Title of Invention

COMPOSITIONS, APPARATUS AND METHODS FOR FACILITATING SURGICAL PROCEDURES

Abstract Methods are provided for conducting surgical procedures in a patient wherein, during the surgical procedure, autonomous ventricular electrical conductivity and escape beats are reversibly and transiently suppressed to facilitate the surgical procedure. Also provided are compositions which are capable of inducing ventricular asystole in a patient. The compositions may include an AV node blocker. In one embodiment, compositions including an atrioventricular (AV) node blocker and a b-blocker are provided, wherein the b-blocker is present in an amount sufficient to substantially reduce the amount of AV node blocker required to induce ventricular asystole in the patient. The compositions and methods may be used for inducing temporary ventricular asystole in a beating heart, and to facilitate the performance of a variety of surgical techniques, including minimally invasive microsurgical techniques. Methods for performing a surgical procedure on a human patient are provided wherein a composition capable of inducing transient reversible ventricular asystole is administered to the heart, for example by intracoronary injection. The heart then is electrically paced using an electrical pacing system, thereby to maintain the patient's blood circulation. The electrical pacing then is selectively intermittently stopped to allow ventricular asystole to occur, and the steps of the surgical or therapeutic procedure, such as suturing, are conducted during the time that the electrical pacing is intermittently stopped. The methods and compositions advantageously may be used in a range of different surgical procedures including cardiac, vascular and neurosurgical procedures.
Full Text COMPOSITIONS, APPARATUS AND METHODS FOR FACILITATING
SURGICAL PROCEDURES
CROSS REFERENCE TO RELATED APPLICATIONS
This application claims the benefit of U.S. Provisional Application Serial
No. 60/055,127, filed August 8, 1997, the disclosure of which is incorporated herein
by reference.
TECHNICAL FIELD
The present invention relates to compositions and methods that facilitate the
performance of medical and surgical therapeutic procedures, particularly cardiac
surgical procedures, in one embodiment, methods and compositions are provided
which facilitate the performance of minimally invasive coronary bypass surgery.
BACKGROUND ART
Heart attacks and angina pectoris (chest pain) are caused by occlusions in the
coronary arteries. Atherosclerosis, the major cause of coronary artery occlusions, is
characterized by deposits of fatty substances, cholesterol, calcium and fibrin within
the arterial wall. As the coronary arteries narrow, blood flow is reduced depriving
the heart of much needed oxygen. This occurrence is called myocardial ischemia.
Severe and prolonged myocardial ischemia produces irreparable damage to the heart
muscle, pronounced cardiac dysfunction, and possibly death. Apart from medical
therapy, atherosclerosis is treated with coronary artery bypass graft surgery (CABG),
percutaneous transluminal coronary angioplasty (PTCA), stents, atherectomy, and
transmyocardial laser revascularization (TMLR).
In patients where PTCA, stents, and atherectomy are unsuitable or
unsuccessful, CABG is the procedure of choice. In the conventional CABG
operation, a long vertical incision is made in the chest, the sternum is split
longitudinally and the halves are spread apart to provide access to the heart. Two
large bore tubes, or cannulas, are then inserted directly into the right atrium and the
aorta in order to establish cardiopulmonary bypass (CPB). The aorta is occluded
with an external clamp placed proximal to the aortic cannula. A third cannula is
inserted proximal to the aortic clamp, and is used for the delivery of a cardioplegic
solution into the coronary arteries. The hyperkalemic cardioplegic solution protects
the heart by stopping atrial and ventricular contraction, thereby reducing its
metabolic demand. When the heart is not beating, blood flow to the rest of the body
is provided by means of CPB. Cardiopulmonary bypass involves removing
deoxygenated blood through the cannula in the right atrium, infusing the blood with
oxygen, and then returning it through the cannula in the aorta to the patient. With the
heart motionless, the surgeon augments blood flow to the ischemic heart muscle by
redirecting blood around the coronary artery occlusion. Although there are several
methods to bypass an occlusion, the most important method involves using the left
internal thoracic artery (LITA). The LITA normally originates from the left
subclavian artery and courses along the anterior chest wall just lateral of the sternum.
For this operation, the LITA is mobilized from the chest wall and, with its proximal
origin left intact, the distal end is divided and sewn to the coronary artery beyond the
site of occlusion (most commonly the left anterior descending coronary artery).
After the LITA anastomosis is completed and any further arterial or vein grafts are
completed, CPB is weaned as the heart resumes its normal rhythm. The cannulae are
removed, temporary pacing wires are sewn to the heart, and plastic tubes are passed
through the chest wall and positioned near the heart to drain any residual fluid
collection. The two halves of the sternum are approximated using steel wire.
Because the traditional method of performing CABG involves significant
operative trauma and morbidity to the patient, attention has been directed to
developing less invasive surgical techniques that avoid splitting the sternum. The
new techniques are performed with or without CPB through smaller incisions placed
between the ribs. One method, called port-access, utilizes groin cannulation to
establish CPB, while another, called minimally invasive direct coronary artery
bypass or MIDCAB, is performed on the beating heart and therefore does not require
CPB. Insofar as these techniques succeed in achieving less operative trauma
compared to conventional CABG, postoperative pain is improved, the length of
hospitalization is shortened, and the return to normal activity is hastened.
The port-access approach avoids the sternal splitting incision by employing femoral
venoarterial CPB and an intraaortic (endoaortic) balloon catheter that functions as an
aortic clamp by means of an expandable balloon at its distal end (Daniel S. Schwartz
et al. "Minimally Invasive Cardiopulmonary Bypass With Cardioplegic Arrest: A
Closed Chest Technique With Equivalent Myocardial Protection." Journal of
Thoracic & Cardiovascular Surgery 1996; 111:556-566. John H. Stevens et al.
"Port-Access Coronary Artery Bypass Grafting: A Proposed Method." Journal of
Thoracic & Cardiovascular Surgery 1996; 111:567-573. John H. Stevens et al.
"Port-Access Coronary Artery Bypass With Cardioplegic Arrest: Acute and Chronic
Canine Studies." Annals of Thoracic Surgery 1996; 62:435-441). This catheter also
includes a separate lumen for the delivery of cardioplegic solution and venting of the
aortic root. Alternatively, a different catheter may be placed percutaneously into the
internal jugular vein and positioned in the coronary sinus for delivery of retrograde
cardioplegic solution. Coronary bypass grafting is performed through a separate
limited left anterior thoracotomy incision with dissection of the LITA and
anastomosis to the atherosclerotic coronary artery under direct vision. Other bypass
grafts to coronary arteries can be accomplished using radial artery sewn to the LITA.
A full description of the port-access technique is found in U.S. Patent
No. 5,452,733, the complete disclosure of which is incorporated herein by reference.
Thus, the port-access approach focuses on avoiding the sternal splitting incision
while maintaining a motionless heart to facilitate a precise coronary anastomosis as
the primary means to reduce operative trauma and morbidity. Compelling evidence
to support this contention, however, is scarce. Furthermore, no evidence exists
regarding the effectiveness of the coronary anastomosis performed through the
limited incision, nor the safety of the intraaortic balloon clamp and the vascular
sequelae of groin cannulation. Finally, the port-access approach does not avoid the
damaging effects of cardiopulmonary bypass, which include: 1) a systemic
inflammatory response; 2) interstitial pulmonary edema; 3) neuropsychological
impairment; 4) acute renal insufficiency; and 5) nonmechanical microvascular
hemorrhage.
The MIDCAB approach also avoids the sternal splitting incision, favoring
instead a limited left anterior thoracotomy incision (Tea E. Acuff et al. "Minimally
Invasive Coronary Artery Bypass Grafting." Annals of Thoracic Surgery 1996;
61:135-7. Federico J. Benetti and Carlos Ballester, "Use Of Thoracoscopy And A
Minimal Thoracotomy, In Mammary-Coronary Bypass To Left Anterior Descending
Artery, Without Extracorporeal Circulation." Journal of Cardiovascular Surgery
1995; 36:159-61. Federico J. Benetti et al. "Video Assisted Coronary Bypass
Surgery." Journal of Cardiac Surgery 1995; 10:620-625). Similarly, dissection of
the LITA and anastomosis to the coronary artery are then performed under direct
vision. The principal difference between the MIDCAB and port-access techniques,
however, involves the utilization of cardioplegic solution and CPB (Denton A.
Cooley, "Limited Access Myocardial Revascularization" Texas Heart Institute
Journal 1996; 23:81-84; and Antonio M. Calafiore et al., "Left Anterior Descending Coronary Artery Grafting via Left Anterior Small Thoracotomy without
Cardiopulmonary Bypass," Annals of Thoracic Surgery 1996; 61:1658-65). Because
MIDCAB is performed on the beating heart, cardioplegic solution, aortic cross-
clamping and CPB are not required. This approach therefore focuses on the
avoidance of cardiopulmonary bypass and aortic cross-clamp and the sternal splitting
incision as the primary means to reduce operative trauma and morbidity after
conventional CABG.
The potential advantages of MIDCAB compared to conventional CABG
include: 1) the avoidance of CPB and aortic cross-clamping; 2) fewer embolic
strokes; 3) less blood loss, hence a decreased transfusion requirement; 4) fewer
perioperative supraventricular arrhythmias; 5) earlier separation from mechanical
ventilatory support; 6) decreased or eliminated intensive care unit stay; 7) shorter
length of hospitalization; 8) reduced total convalescence with earlier return to
preoperative activity level; and 9) lower overall cost. Despite these potential
benefits, however, the durability of the LITA to coronary artery anastomosis is
uncertain. At the recent American Heart Association 69th Annual Scientific Session,
the Mayo Clinic group reported on 15 patients undergoing MIDCAB. Of these 15
patients, three or 20% required reoperation to revise the anastomosis during the same
hospitalization (Hartzell V. Schaff et al., "Minimal Thoracotomy For Coronary
Artery Bypass: Value Of Immediate Postprocedure Graft Angiography," Abstract
presented at the American Heart Association, 69th Scientific Sessions,
November 10-13, 1996, Atlanta, GA). Of greater significance, however, was a report
from Loma Linda University Medical Center that demonstrated a seven-year LITA to
left anterior descending coronary artery patency rate of 42% in a subset of patients
who underwent beating heart surgery and presented with recurrent angina. In
contrast, the patency rate in an age-, sex- and disease severity-matched control group
was 92% (Steven R. Gundry et al, "Coronary Artery Bypass with and Without the
Heart-Lung Machine: A Case Matched 6-year Follow-up," Abstract presented at the
American Heart Association, 69th Scientific Sessions, November 10-13, 1996,
Atlanta, GA). Finally, because the MIDCAB approach is restricted mostly to
patients with isolated disease of the left anterior descending coronary artery, the vast
majority of patients with atherosclerotic heart disease are not appropriate candidates.
Thus, despite the potential benefits of MIDCAB, its safety, efficacy, and
applicability remain uncertain.
There are major obstacles to precise coronary anastomosis during MIDCAB.
The constant translational motion of the heart and bleeding from the opening in the
coronary artery hinder precise suture placement in the often tiny coronary vessel.
Although bleeding can be reduced by using proximal and distal coronary occluders,
by excluding diagonal and septal branches near the arterial opening when possible,
and by continuous saline irrigation or humidified carbon dioxide insufflation, the
incessant motion of the beating heart remains the Achilles" heel of minimally
invasive coronary artery bypass.
In summary, although port-access and minimally invasive direct coronary
artery bypass techniques avoid the operative trauma and morbidity associated with
the sternal splitting incision, both have serious disadvantages. The port-access
approach is encumbered by the morbidity of cardiopulmonary bypass and aortic
cross-clamping and the cost of the apparatus. Furthermore, the safety of the
intraaortic balloon clamp and the vascular sequelae of groin cannulation are
unresolved issues. The MIDCAB approach is imperiled by the constant motion of
the beating heart which precludes a precise coronary anastomosis. Reports of poor
graft patency rates and the need for early reoperation in a significant proportion of
patients after MIDCAB attests to the technical difficulty of the procedure.
Conventional CABG requires arrest of the heart through the use of
cardioplegic agents, aortic cross-clamping and cardiopulmonary bypass. These
cardioplegic agents stop the beating heart to thereby allow precise suture placement
and other surgical procedures. A mixture of magnesium sulfate, potassium citrate,
and neostigmine has been used to induce cardioplegia during cardiopulmonary
bypass. Sealy et al. "Potassium, Magnesium, And Neostigmine For Controlled
Cardioplegia: A Report Of Its Use In 34 Patients," Journal of Thoracic Surgery
1959, 37:655-59. Although both magnesium and potassium remain integral
components of modern cardioplegic solutions, neostigmine was ultimately
eliminated. Potassium citrate is currently the most commonly used cardioplegic
agent. Potassium impedes excitation-contraction coupling, however, making it
impossible to pace the heart by electrical stimulation and necessitating the use of a
cardiopulmonary bypass system to sustain the patient. Other chemical agents that
have been used in human cardiac operations to slow the rate of ventricular
contraction include acetylcholine, neostigmine, adenosine, lignocaine, and esmolol.
Another agent, carbachol or carbamyl choline, has been used to induce cardiac arrest
in experimental animals. Broadley and Rothaul, Pflugers Arch., 391:147-153
(1981).
Acetylcholine has been used as a cardioplegic agent during cardiopulmonary
bypass. Lam et al., "Induced Cardiac Arrest In Intracardiac Procedures, An
Experimental Study," Journal of Thoracic Surgery 1955; 30:620-25; Lam et al.,
"Clinical Experiences With Induced Cardiac Arrest During Intracardiac Surgical
Procedures," Annals of Surgery 1957; 146:439-49; Lam et al., "Induced Cardiac
Arrest (Cardioplegia) In Open Heart Procedures," Surgery 1958; 43:7-13; and Lam
et al., "Acetylcholine-induced Asystole. An adjunct In Open Heart Operations With
Extracorporeal Circulation," in Extracorporeal Circulation 1958, pp. 451-48;
Lillehei et al., "The Direct Vision Correction Of Calcific Aortic Stenosis By Means
Of A Pump Oxygenator And Retrograde Coronary Sinus Perfusion," Disease Of The
Chest, 1956, 30:123-132; Lillehei et al., "Clinical Experience With Retrograde
Perfusion Of The Coronary Sinus For Direct Vision Aortic Valve Surgery With
Observations Upon Use of Elective Asystole Or Temporary Coronary Ischemia," in
Extracorporeal Circulation, 1958, pp. 466-85; Lillehei et al., "The Surgical
Treatment Of Stenotic Or Regurgitant Lesions Of The Mitral And Aortic Valves By
Direct Vision Utilizing A Pump Oxygenator," Journal of Thoracic &
Cardiovascular Surgery, 1958; 35:154-91. Conrad R. Lam, et al. Annals of Surgery
1957; 146:439-49. Intravenous adenosine has been used to facilitate MIDCAB.
M. Clive Robinson, First International Live Teleconference. Least-Invasive
Coronary Surgery, The John Radcliffe Hospital, Oxford, England, March 21 and 22,
1996.
Ventricular asystole has been achieved by direct injection of lignocaine into
the interventricular septum. Khanna and Cullen, "Coronary Artery Surgery With
Induced Temporary Asystole And Intermittent Ventricular Pacing: An Experimental
Study," Cardiovascular Surgery 1996; 4(2):231-236. Epicardial pacing wires were
placed, and ventricular pacing was employed to maintain an adequate cardiac output.
Esmolol has been used as a cardioplegic agent during cardiopulmonary bypass.
Mauricio Ede et al., "Beyond Hyperkalemia: Beta-Blocker-Induced Cardiac Arrest
For Normothermic Cardiac Operations," Annals of Thoracic Surgery, 1997; 63:721-
727.
In summary, there is a need for a surgical approach that avoids the risks and
costs of cardiopulmonary bypass while preserving the benefits of a motionless
operative field to achieve a precise coronary anastomosis. There is a further need for
methods and compositions that enable predictable, controllable, transient arrest of the
heart, which stop or slow the beating heart with acceptable half-life and quick onset
of effect. There is a need for compositions and methods for transient arrest of the
heart which can be used in a variety of surgical procedures conducted on the heart,
vascular system, brain, or other major organs, where pulsatile flow, movement
associated with arterial pulsations, or bleeding is undesirable during the procedure.
SUMMARY OF THE INVENTION
Methods, compositions and apparatus are provided which are useful for
medical and surgical therapeutic applications. The methods and compositions are
useful for cardiac surgery and other procedures, such as neurosurgery and vascular
surgery, which require precise control of cardiac contraction. Other applications
include non-invasive procedures such as percutaneous aortic aneurysm graft
placement, and invasive procedures such as brain surgery. Using the methods and
compositions disclosed herein for conducting a surgical procedure, such as a
coronary bypass, a substantially motionless operative field is provided.
In one aspect, there is provided a method of inducing reversible ventricular
asystole in a beating heart in a human patient, the method comprising administering a
compound and a ß-blocker to the heart of the patient in an amount effective to induce
ventricular asystole, while maintaining the ability of the heart to be electrically
paced, wherein the ß-blocker is administered in amount sufficient to substantially
reduce the amount of compound required to induce ventricular asystole. In one
embodiment, the compound may be an atrioventricular (AV) node blocker. The ß-
blocker may be administered in an amount sufficient to reduce the amount of AV
node blocker, which is required to induce ventricular asystole, to, for example, about
50% or less by weight of the amount of AV node blocker alone required to induce
ventricular asystole. The compound may be a cholinergic receptor agonist, such as
carbachol. The cholinergic receptor agonist, such as carbachol, may be administered
in an amount, for example, of about 0.1 to 4.8 µg/kg body weight/min. The ß-
blocker, may be, for example, propranolol. The propranolol may be administered,
for example, in an amount of about 0.01 to 0.07 mg/kg body weight. In one
embodiment, the ß-blocker is propranolol and the AV node blocker is carbachol, and
the propranolol is administered prior to or during administration of the carbachol.
The propranolol and the carbachol may be administered, for example, to the coronary
artery of the patient.
In another embodiment, there is provided a method of inducing reversible
ventricular asystole in a beating heart in a human patient, the method comprising
administering a cholinergic receptor agonist and a ß-blocker to the heart of the
patient in an amount effective to induce ventricular asystole, wherein the amount
administered of the cholinergic receptor agonist alone or the ß-blocker alone is not
sufficient to induce ventricular asystole.
In another embodiment, there is provided a method of conducting a surgical
procedure on a human patient comprising: administering a ß-blocker and an AV
node blocker to the heart of a human patient to induce reversible ventricular asystole
while maintaining the ability of the heart to be electrically paced; electrically pacing
the heart with an electrical pacing system; selectively intermittently stopping the
electrical pacing to allow ventricular asystole; and conducting the surgical procedure
during the time that the electrical pacing is intermittently stopped. In one
embodiment, the ß-blocker is administered prior to the AV node blocker. The AV
node blocker may be a cholinergic agent, such as carbachol. The ß-blocker may be
administered in an amount sufficient to substantially reduce the amount of AV node
blocker required to induce ventricular asystole. The surgical procedure may be, for
example, a cardiac surgical procedure. In one embodiment, the electrical pacing is
selectively intermittently interrupted by a surgeon conducting the surgical procedure
by selectively manipulating a control that is functionally coupled to the electrical
pacing system. The ß-blocker and the cholinergic agent and the ß-blocker may be
administered, for example, sequentially or simultaneously, and may be administered,
for example, to the left ventricle, the aorta, the right ventricle, the pulmonary artery,
the pulmonary vein, or the coronary sinus. The cholinergic receptor agonist, such as
carbachol, may be administered, for example, in an amount of about 0.1 to 4.8 µg/kg
body weight/min. The ß-blocker, may be, for example, propranolol, which may be
administered, for example, in an amount of about 0.01 to 0.07 mg/kg body weight.
In one embodiment, the ß-blocker is propranolol and the AV node blocker is
carbachol, and the propranolol is administered prior to or during administration of
the carbachol.
In one embodiment, the propranolol is administered by a single bolus
injection in the coronary artery, prior to the administration of carbachol, and the
carbachol is administered by a single bolus injection followed by continuous infusion
into the coronary artery to maintain the ventricular asystole. Surgical procedures that
may be conducted include minimally invasive coronary bypass procedure,
neurological procedures and endovascular procedures. Other surgical procedures
include treatment of injuries to the liver, spleen, heart, lungs, and major blood
vessels, as well as electrophysiologic procedures and cardiac surgery with or without
cardiopulmonary bypass.
In another embodiment, there is provided a method of inducing reversible
ventricular asystole in a human patient comprising administering carbachol to the
heart of the patient. The carbachol may be administered, for example, to the
coronary sinus, or may be administered intraventricularly, or to the aortic root or
coronary artery of the patient. Optionally, propranolol also may be administered to
the heart of the patient. The propranolol may be administered, for example, prior to
or during the administration of the carbachol.
In a further embodiment, there is provided a method of inducing reversible
ventricular asystole in the heart of a human patient comprising administering
carbachol to the patient at a dosage of about 1 to 15 mg, for example, about 1 to 12
mg. In another embodiment, there is provided a method of inducing reversible
ventricular asystole in the heart of a human patient, the method comprising
administering carbachol to the patient at a rate of 0.1 to 4.8 µg/kg body weight/min.
In another embodiment, there is provided a method of inducing reversible
ventricular asystole in the heart of a human patient, the method comprising:
administering an initial intracoronary bolus of carbachol of about 0.1 to 10 µg/kg
body weight of the patient; and administering a continuous intracoronary infusion of
carbachol at a rate of about 0.1-4.8 µg/kg body weight/min. The initial intracoronary
bolus of carbachol is administered, for example, over about 1-5 minutes. The
intracoronary infusion of carbachol is administered, for example, over a time period
of about 5 to 120 minutes. The initial intracoronary bolus may comprise, or example
about 0.1 to 5 µg carbachol/kg body weight, and may be provided in a suitable
pharmaceutically acceptable carrier.
In a further embodiment, there is provided a method of inducing reversible
ventricular asystole in a human patient comprising: administering an intracoronary
bolus injection of about 0.01 to 0.5 mg of carbachol over about 0.5 to 3 minutes; and
administering an intracoronary infusion of carbachol at a rate of about 0.01 to 0.3
mg/min over about 30 to 90 minutes.
In a further embodiment, there is provided a method of inducing reversible
ventricular asystole of a heart of a human patient while maintaining the ability of the
heart to be electrically paced comprising: administering at least a first compound to
the heart of the patient which is capable of inducing third-degree AV block of the
heart; and administering at least a second compound to the heart of the patient which
alone or in combination with the first compound is capable of substantially
suppressing ectopic ventricular beats in the heart while maintaining the ability of the
heart to be electrically paced.
In another embodiment, there is provided a method of inducing reversible
ventricular asystole in the heart of a patient, while maintaining the ability of the heart
to be electrically paced comprising: administering an AV-node blocker and a
compound to the heart of the patient in an amount effective to induce ventricular
asystole, while maintaining the ability of the heart to be electrically paced, wherein
the compound is administered in an amount sufficient to reduce the amount of AV-
node blocker required to induce ventricular asystole.
In a further embodiment, a method of performing a surgical procedure on a
human patient is provided, the method comprising: administering an effective
amount of a composition capable of inducing reversible ventricular asystole to the
patient, while maintaining the ability of the heart to be electrically paced; electrically
pacing the heart with an electrical pacing system, thereby to maintain the patient"s
blood circulation; selectively intermittently stopping the electrical pacing to allow
ventricular asystole; and conducting the surgical procedure during the time that the
electrical pacing is intermittently stopped. The composition capable of inducing
ventricular asystole may comprise, in one embodiment, an atrioventricular (AV)
node blocker. The composition may further comprise a ß-blocker, wherein the b-
blocker is present in an amount sufficient to substantially reduce the amount of AV
node blocker required to induce ventricular asystole. In another embodiment, the
composition may comprise a cholinergic agent and a ß-blocker, wherein the amount
by weight administered of either the cholinergic agent alone or the ß-blocker alone is
not sufficient to induce complete heart block and suppression of ventricular escape
beats, but in combination, due to a synergistic effect, is effective to induce
ventricular asystole.
According to another aspect of the invention, a cardiac surgical procedure is
conducted by inducing reversible ventricular asystole in the heart of a human patient
without cardiopulmonary bypass, and/or without aortic cross-clamping.
According to another aspect, a composition is provided that is capable of
inducing reversible ventricular asystole in a patient, while maintaining the ability of
the heart to be electrically paced. The composition may include an atrioventricular
(AV) node blocker. In one embodiment, the composition may include a compound
capable of inducing reversible ventricular asystole in a patient and a ß-blocker in an
amount sufficient to substantially reduce the amount of the compound required to
induce ventricular asystole in the patient. The composition may include, for
example, an atrioventricular (AV) node blocker, such as carbachol and a ß-blocker,
such as propranolol. The ß-blocker is provided in one embodiment in an amount
sufficient to substantially reduce the amount of AV node blocker required to induce
ventricular asystole. For example, the AV node blocker may be present in the
composition in an amount which is 50% or less by weight, or optionally about 1 to
20 % by weight of the amount of AV node blocker alone required to induce
ventricular asystole. The composition may comprise, for example carbachol in a
pharmaceutically acceptable solution at a dosage amount of about 1 to 20 mg. The
comopsition may include propranolol in a pharmaceutically acceptable carrier in a
dosage form for administration to a patient in an amount of about 0.01 to 0.07 mg/kg
body weight of the patient. In one embodiment, the composition may comprise
propranolol present in a pharmaceutically acceptable solution at a dosage amount of
about 1 to 10 mg. Methods are provided for administering an effective amount of the
compositions to a patient to induce reversible ventricular asystole during a surgical
procedure.
In another embodiment, a composition is provided which is capable of
inducing ventricular asystole in a patient, while maintaining the ability of the heart to
be electrically paced, comprising a cholinergic receptor agonist and a ß-blocker. In
one embodiment, the amount of either the cholinergic receptor agonist alone or the
ß-blocker alone in the composition is not sufficient to induce ventricular asystole in
the patient.
In another embodiment, a sterile dosage form of carbachol is provided, which
may be provided in form suitable for use in a surgical procedure. The dosage form
of carbachol may be in a pharmaceutically acceptable form for parenteral
administration, for example to the cardiovascular system, or directly to the heart.
The carbachol may be provided in a variety of pharmaceutically acceptable carriers.
In one embodiment, a sterile dosage form of carbachol is provided comprising about
1-20 mg of carbachol in a pharmaceutically acceptable carrier. Carriers include
aqueous solutions including saline, aqueous solutions including dextrose, water and
buffered aqueous solutions.
In yet another embodiment, the invention provides the use of a ß-blocker in
the manufacture of a medicament for use in conjunction with a compound capable of
inducing reversible ventricular asystole in the heart of a patient, for use in a method
of inducing transient reversible ventricular asystole in the heart of a patient, while
maintaining the ability of the heart be electrically paced, the amount of ß-blocker
being sufficient to reduce substantially the amount of the compound required to
induce ventricular asystole.
There is further provided the use of a compound capable of inducing
reversible ventricular asystole in the manufacture of a medicament for use in
conjunction with a ß-blocker for use in a method of inducing transient reversible
ventricular asystole in the heart of a patient, while maintaining the ability of the heart
be electrically paced, the amount of ß-blocker being sufficient to reduce substantially
the amount of the compound required to induce ventricular asystole.
In another embodiment, there is provided the use of a ß-blocker in the
manufacture of a medicament for use in conjunction with a cholinergic receptor
agonist, for use in a method of inducing transient reversible ventricular asystole in
the heart of a patient, while maintaining the ability of the heart to be electrically
paced, the amount of the cholinergic receptor agonist administered alone or the
ß-blocker administered alone not being sufficient to induce ventricular asystole in the
heart of the patient.
In another aspect, there is provided the use of a cholinergic receptor agonist
in the manufacture of a medicament for use in conjunction with a ß-blocker, for use
in a method of inducing transient reversible ventricular asystole in the heart of a
patient, while maintaining the ability of the heart to be electrically paced, the amount
of cholinergic receptor agonist administered alone or the ß-blocker administered
alone not being sufficient to induce ventricular asystole in the heart of the patient.
According to another aspect of the invention, a patient may be prepared for
coronary artery bypass by placing at least a portion of a delivery device in a coronary
vessel of the patient"s heart and delivering a cardioplegic agent to the AV node of the
patient via coronary vessel with the device, which may be a catheter, for example. In
one embodiment, the device is placed in the right coronary artery of the heart of the
patient. In another embodiment, it is placed in the left coronary artery of the heart of
the patient. The device may include an outlet and the outlet placed in the right
coronary artery of the heart of the patient and immediately proximal to the AV nodal
branch artery. In another embodiment, the device outlet may be placed in the AV
nodal branch artery. In further embodiments, the device may be placed in the middle
vein of the heart of the patient or in an ostium of a right or left coronary artery of the
heart of the patient. In another embodiment, the device may be introduced through
the femoral artery. The device also may be introduced through an incision in the
aorta of the patient.
According to another aspect of the invention, a kit is provided comprising
one or more agents capable of inducing ventricular asystole. For example, the kit
may include separate containers of an AV node blocker and a ß-blocker. In one
embodiment, the kit is provided with a first container comprising a dosage amount of
a cholinergic receptor agonist and a second container comprising a dosage amount of
a ß-blocker. Dosage amounts of cholinergic receptor agonist and ß-blocker may be
included that are suitable for simultaneous, separate or sequential use in a surgical
procedure for inducing transient reversible ventricular asystole in a patient. In one
embodiment, the cholinergic receptor agonist is carbachol and the ß-blocker is
propranolol. The carbachol and/or propranolol may be in a pharmaceutically
acceptable carrier. According to one embodiment, the first container contains about
1 to 20 mg of carbachol, and the second container contains about 1 to 10 mg of
propranolol. Other possible components of the kit include pacing electrodes, drug
delivery devices and catheters. The electrodes may be, for example, epicardial or
endocardial pacing electrodes. Other components of the kit can include pacing
catheters and devices, and coronary perfusion catheters and devices, catheter
introducers, a pump system and/or tubes, or other surgical devices. The drug
delivery device may be in various forms including a catheter, such as a drug deliver}"
catheter or guide catheter, a cannula or a syringe and needle assembly. The drug
delivery catheter may include an expandable member, and a shaft having a distal
portion, wherein the expandable member is disposed along the distal portion. The
expandable member may be a low-pressure balloon. The kit may be in packaged
combination, such as in a pouch, bag or the like. The kit may further include
instructions for the use of components of the kit in a surgical procedure, such as
instructions for use of compounds to induce transient reversible ventricular asystole
in the heart of a patient undergoing a surgical procedure.
According to another aspect of the invention, a pacing system is provided
comprising an extracorporeal pacer for delivering pacing signals to a human heart, a
switch coupled to the pacer, and a switch actuator arranged remote from the pacer.
The pacing system may include pacing leads coupled to the switch and adapted for
coupling to the heart of the patient. The switch may remote from the pacer. The
actuator may be remote from the switch. Further, the actuator may take various
forms. For example, in one embodiment, the actuator may comprise a foot pedal an
in another, it may comprise a needle holder.
The above is a brief description of some deficiencies in the prior art and
advantages of the present invention. Other features, advantages and embodiments of
the invention will be apparent to those skilled in the art from the following
description, accompanying drawings and appended claims.
BRIEF DESCRIPTION OF THE DRAWINGS
Figure 1 diagramatically shows a pacing system in accordance with the
principles of the invention;
Figure 1A and 1B are circuit diagrams of a control switch and an actuator
used in the pacing system of Figure 1;
Figure 1C is a schematic representation of a control box according to the
present invention;
Figure 1D diagrammatically shows one outlet lead arrangement coupled to
the heart of a patient;
Figure 1E diagrammatically shows another outlet lead arrangement coupled
to the heart of a patient;
Figure 2 illustrates a drug delivery catheter prior to insertion into the
coronary sinus in accordance with the invention;
Figure 2A is a sectional view of the catheter of Figure 2 taken along line
2A - 2A;
Figure 3 illustrates placement of the distal end portion of the catheter of
Figure 2 in the coronary sinus;
Figure 3 A is a sectional view of the distal portion of the catheter of Figure 3;
Figure 4 illustrates another coronary sinus catheter configuration;
Figure 5 depicts a drug delivery catheter positioned for intra-aortic drug
delivery in accordance with the present invention;
Figure 6 illustrates a drug delivery catheter positioned for drug delivery local
to the AV node branch in accordance with the present invention;
Figure 7 illustrates another embodiment of the catheter of Figure 6 showing a
curved distal end portion for directing fluid toward the AV node; and
Figure 8 depicts the catheter of Figure 7 with its bent distal end portion
directed toward the AV node branch.
DETAILED DESCRIPTION
Compositions and methods are provided which are useful for medical and
surgical therapeutic applications. The compositions and methods are useful for
cardiac surgery and other procedures such as neurosurgery and vascular surgery
which require precise control of cardiac contraction. In one embodiment, the
compositions and methods are useful for coronary artery bypass procedures, with or
without cardiopulmonary bypass. Using the methods and compositions for
conducting a coronary artery bypass disclosed herein, a motionless operative field is
provided.
The methods and compositions of the invention are useful for any procedure
which requires controlled temporary complete heart block and suppression of
ventricular escape beats. Examples of such procedures include coronary bypass
surgery (with full or partial sternotomy or thoracotomy), transmyocardial laser
revascularization, tachyarrhythmia operations such as electrophysiology lab
procedures (diagnostic and therapeutic ablation of arrhythmias), imaging procedures

of the heart and great vessels such as CAT scan or MRI procedures, percutaneous
transluminal coronary angioplasty, placement of stents such as coronary or aortic
stents, operations where uncontrollable hemorrhage is present or anticipated or
control of significant hemorrhage is required during the surgical procedure (for
example, treatment of injuries to the liver, spleen, heart, lungs, or major blood
vessels, including iatrogenic and traumatic injuries to such organs or structures),
other procedures including percutaneous aortic aneurysm graft placement, and
neurosurgical procedures, such as aneurysm repair. The methods and compositions
are useful for any surgical procedure or intervention on the heart, vascular system,
brain, or other major organs, where pulsatile flow, movement associated with arterial
pulsations, or bleeding prevents successful completion of the operative procedure.
The compositions and methods can be used to induce ventricular asystole in a
patient, for example, prior to a surgical procedure. The term "ventricular asystole" as
used herein refers to a state wherein autonomous electrical conduction and escape
rhythms in the ventricle are suppressed. Preferably, a state of the heart is induced
wherein the heart beats less than about 25 beats per minute, for example, less than
about 12 beats per minute. The induced ventricular asystole is reversible and after
reversal, the heart functions are restored, and the heart is capable of continuing
autonomous function. Preferred are pharmaceutically acceptable compositions
which are capable of inducing transient reversible ventricular asystole reliably and
predictably.
The compositions capable of suppressing autonomous ventrical electrical
conduction and escape rhythms may in one embodiment comprise an atrioventricular
(AV) node blocker. As used herein, the term "AV node blocker" refers to a
compound capable of reversibly suppressing autonomous electrical conduction at the
AV node, while still allowing the heart to be electrically paced to maintain cardiac
output. Preferably, the AV node blocker, or composition comprising the AV node
blocker, reduces or blocks ventricular escape beats and cardiac impulse transmission
at the AV node of the heart, while the effect on depolarization of the pacemaker cells
of the heart is minimal or non-existent. The AV node blocker preferably induces
third degree, or complete AV block, or significantly slows AV conduction to the
point where the ventricular beat is less than about 25 beats per minute, for example
less than about 12 beats per minute. The AV node blocker, or composition
comprising the AV node blocker, preferably induces reversible ventricular asystole,
and renders the heart totally pacemaker dependent for a limited period of time, such
that a pacemaker may be used to maintain pacing and to intermittently stop pacing
during a surgical step. After the surgical procedure is completed, for example, less
than about 2 hours, the heart then can be returned to its normal intrinsic rhythm.
Exemplary AV node blockers include calcium channel blockers, adenosine
A1 receptor agonists, adenosine deaminase inhibitors, cholinesterase inhibitors,
monoamine oxidase inhibitors, serotoninergic agonists, antiarrythmics, cardiac
glycosides, local anesthetics and combinations thereof. Examples of AV node
blockers include adenosine, digoxin, digitalis, procaine, lidocaine, procainamide,
quinidine, verapamil, chloroquine, amiodarone, ethmozine, propafenone, flecainide,
encainide, pilocarpine, diltiazem, dipyridamole, ibutilide, zapranest, sotalol and
metoclopromide and combinations thereof. AV node blocking also can be achieved
by other methods including direct electrical stimulation, vagal nerve stimulation,
stimulation with ultrasonic energy, and temporary cooling of the AV node using a
cryonic agent. Cryonic agents include devices, such as cryostats, and cryogenic
chemicals which are capable of inducing low temperatures at the AV node.
The AV node blocker, capable of causing ventricular asystole, in a preferred
embodiment is a cholinergic agent. As used herein, the term "cholinergic agent""
refers to a cholinergic receptor modulator, which is preferably an agonist. The
cholinergic agent in a preferred embodiment is carbachol (carbamyl choline
chloride). Other cholinergic agents which may be used include any naturally
occurring cholinergic (acetylcholine) receptor agonists or synthetic derivatives.
Exemplary cholinergic agents include acetylcholine, methacholine, bethanechol,
arecoline, norarecoline, pyridostigmine, neostigmine, and other.agents that increase
cyclic GMP levels by direct or indirect receptor stimulation.
In one embodiment, compositions and methods are provided which are
capable of slowing or preventing autonomous conduction of electrical impulses from
the sinoatrial node to the ventricle, with suppression of escape beats in the AV node
and the ventricle. Preferably, a state of the heart is induced wherein the heart beats
less than about 25 beats per minute, for example, less than about 12 beats per minute.
As used herein, the term "ß-adrenergic blocking agent," also referred to as a
"ß-blocker", is defined as an agent which is capable of blocking ß-adrenergic
receptor sites. In a preferred embodiment, the ß-blocker is propranolol. Other b-
blockers which can be used include atenolol, acebutolol, labetalol, metoprolol,
nadolol, oxprenolol, penbutolol, pindolol, sotalol and timolol. Other exemplary b-
blockers include celiprolol, betaxolol, bevantolol, bisoprolol, esmolol, alprenolol,
carterolol, nadolol or teratoid, and mixtures thereof. The ß-blocker may be any
naturally occurring or synthetic analogue capable of blocking ß-adrenergic receptor
sites.
In one embodiment, reversible ventricular asystole in a beating heart in a
human patient is induced by administering to a patient a composition capable of
suppressing autonomous ventricular electrical conduction and escape rhythms. In
one embodiment, the composition capable of inducing ventricular asystole may
comprise a first compound capable of inducing ventricular asystole, such as an AV
node blocker, and a ß-blocker present in an amount sufficient to substantially reduce
the amount of the compound required to induce ventricular asystole. In one
embodiment, the combination of the compound, such as an AV node blocker
together with the ß-blocker provides a synergistic effect such that the amount of AV
node blocker required to induce reversible ventricular asystole may be reduced in
comparison to the amount of AV node blocker required alone. Methods also are
provided wherein the ß-blocker is administered either prior to or contemporaneously
with the compound capable of inducing ventricular asystole, in an amount effective
to substantially reduce the amount of the compound required to be administered to
induce ventricular asystole.
In a particular embodiment, ventricular asystole is induced in a beating heart
in a human patient by administering a cholinergic receptor agonist and a ß-blocker to
the heart of the patient in an effective amount to induce ventricular asystole, wherein
the amount administered of the cholinergic receptor agonist alone or the ß-blocker
alone is not sufficient to induce ventricular asystole. In one embodiment, the coadministration
of the ß-blocker with the cholinergic agent provides a synergistic
effect, such that the amount of cholinergic agent which is administered to induce
reversible ventricular asystole can be reduced.
Reversible ventricular asystole in the heart of a human patient thus may be
induced by administration of an AV node blocker, or mixture of AV node blockers,
to the heart of the patient. Reversible ventricular asystole optionally is induced by
administration of the combination of an AV node blocker, such as a cholinergic
agent, and one or more ß-blockers to the heart of the patient. The ß-blocker is
preferably administered either prior to or contemporaneously with the AV node
blocker.
In an embodiment wherein a surgical procedure is to be conducted, after
inducing reversible ventricular asystole, the method further includes electrically
pacing the heart with an electrical pacing system, thereby to maintain the patient"s
blood circulation; selectively intermittently stopping the electrical pacing to allow
ventricular asystole; and conducting the surgical procedure during the intervals of
time that the electrical pacing is intermittently stopped.
The method may be used, for example, in a cardiac surgical procedure.
Electrical pacing may be controlled by a surgeon conducting the surgical procedure
by selectively manipulating a control that is functionally coupled to the electrical
pacing system. Once reversible ventricular asystole is achieved, pacing of the heart
may be implemented using a external pacemaker connected to the heart, and the
pacemaker may be periodically deactuated, for example by way of a foot switch, to
allow reversible ventricular asystole, thereby facilitating the performance of coronary
artery bypass, with or without cardiopulmonary bypass, or other procedures
elsewhere in the body of the patient.
For example, to conduct a coronary artery bypass, the patient"s heart is
provided with ventricular pacing electrodes connected to an electrical pacing device,
which is controlled by the surgeon. A composition, for example, comprising an AV
node blocker and a ß-blocker, then is administered to the patient to induce reversible
ventricular asystole. The surgeon then employs the pacing device to pace the heart
and sustain the patient"s circulation. The surgeon intermittently stops the electrical
pacing for a few seconds to place a single suture, and re-starts it after each successive
suture, thus permitting a precise coronary anastomosis to be performed. In this
method, the ventricles (and/or atria) are electrically paced and maintain a normal
cardiac output except for the brief periods of time that are required to accurately
place a single suture in the coronary artery, preferably about 2 to 15 seconds, and
more preferably about 2 to 5 seconds. Using the methods and compositions
described herein, the rate and timing of ventricular contraction can be directly
controlled.
In the method, the composition inducing ventricular asystole, such as an AV
node blocker in combination with a ß-blocker or AV node blocker administered after
a ß-blocker, may be infused through a catheter placed into the right coronary artery.
In one embodiment, the composition is delivered locally to the AV node of
the heart upon which it acts via the AV nodal branch artery of the heart. Preferably
the composition is delivered to the right coronary artery which feeds blood to the AV
nodal branch artery. In a majority of patients, the right coronary artery is the main
vessel supplying blood to the right side of the heart and to the AV node. However,
where the right coronary artery is substantially totally occluded, and in a small subset
of about 20% of patients, the first septal branch of the left anterior descending artery
which originates from the left coronary artery may be the vessel which delivers blood
to the AV node and can be selected as the delivery conduit for delivering the
composition to the AV node. Additionally, other possible routes of administration to
the AV node may include Kugel"s artery and the right superior descending artery.
Preferably, the composition is delivered to the right coronary artery or left coronary
artery at a location near the bifurcation to the AV nodal branch artery and proximal
to the right coronary artery"s bifurcation into the posterior descending artery by any
one of a number of drug delivery means, such as a drug delivery catheter suitably
positioned within the right coronary artery. Other methods of administration may be
used including hypodermic needle injection into, for example, any of the vessels
noted above which may supply blood to the AV node, such as the right coronary
artery or the first septal branch. Other methods of administration include needle
injection into the aorta, needle injection directly into the AV node artery or the AV
node itself, a transepicardial absorption pad, i.e., a myocardial patch which slowly
releases the composition directly into the heart"s myocardium, and for example, an
intraoperative cannula or other similar guide introducer or sheath which can be
surgically placed by a surgeon into the aorta or the ostium of a coronary vessel
without the need for X-ray fluoroscopy.
As the composition achieves the desired effect of ventricular asystole, the
ventricle is electrically paced to maintain a stable rhythm and blood pressure. To
interrupt the electrical pacing of the heart, the surgeon uses a convenient control
means, such as a foot pedal or hand held actuator, as shown in Figure 1, and is
thereby able to stop the heart as sutures are placed in the coronary arterial wall.
Because the heart is motionless during the critical period as the surgeon places
sutures, precision and safety are enhanced. The time required to place a single suture
into the coronary artery preferably does not exceed 15 seconds, and is preferably
about 2 to 5 seconds, most preferably about 2 to 4 seconds. Thus, the compositions
can permit the elimination of the translational motion of the beating heart.
Compositions capable of inducing ventricular asystole in a patient are
provided which in one embodiment include a cholinergic receptor agonist and a b-
blocker, wherein the amount of the cholinergic receptor agonist alone or the b-
blocker alone in the composition is not sufficient to induce ventricular asystole in the
patient. Methods are provided wherein the cholinergic receptor agonist and the b-
blocker may be administered, either sequentially or together, thereby to induce
ventricular asystole in a patient, wherein the amount of the cholinergic receptor
agonist administered alone or the ß-blocker administered alone is not sufficient to
induce ventricular asystole in the patient.
In one embodiment, wherein a cholinergic agent and a ß-blocker are
administered to the heart of a human patient to induce reversible ventricular asystole,
when the ß-blocker used is propranolol and the cholinergic receptor agonist used is
carbachol, a continuous infusion rate of about 0.1 to 4.8 µg/kg/min of carbachol can
be used, e.g., an infusion rate of carbachol of 0.1 to 2.1 µg/kg/min, or about 0.1
µg/kg/min to 2.1, or in one preferred embodiment, about 1.5 to 2.1 µg/kg/min. When
an initial bolus of propranolol is administered prior to or during administration of an
initial bolus of carbachol, the ratio by weight of propranolol to carbachol in the bolus
injections can range, for example, from about 1:2 to 35:1, or, in another embodiment,
from about 1:1 to 15:1, or, in another embodiment, from about 2:1 to 10:1, or, in
another embodiment, is about 5:1.
In another embodiment, compositions capable of inducing ventricular
asystole in a patient are provided, comprising a compound, such as an
atrioventricular (AV) node blocker, and a ß-blocker, wherein the ß-blocker is present
in an amount sufficient to substantially reduce the amount of the compound required
to induce ventricular asystole in the patient. The AV node blocker is preferably a
cholinergic agent. Due to the synergistic effect of the presence of the ß-blocker, the
cholinergic agent may be present in the composition in a reduced amount which is,
for example, about 1-90%, about 1-50%, or about 1-20%, or for example, about 2-
14%, or in another embodiment about 80% or less, for example about 50% or less, or
about 10% or less by weight of the amount of the cholinergic agent alone required to
induce ventricular asystole in the patient. Advantageously, the co-administration of
the ß-blocker with the AV node blocker provides a synergistic effect, such that the
amount of AV node blocker which is administered to induce ventricular asystole may
be reduced.
Additionally, in the methods disclosed herein, ventricular asystole may be
induced in a patient by administration, together, or sequentially, of a compound, such
as an AV node blocker, together with a ß-blocker, wherein the ß-blocker is
administered in an amount sufficient to substantially reduce the amount of the
compound required to induce ventricular asystole in the patient. In a preferred
embodiment, the compound is a cholinergic agent, such as carbachol. Due to the
synergistic effect of the administration of the ß-blocker, the cholinergic agent may be
administered in reduced amount which is, for example, about 1-90%, about 1-50%.
or about 1-20%, or in one embodiment, about 2-14%, or in another embodiment
about 80% or less, about 50% or less, or about 10% or less by weight of the amount
of the cholinergic agent alone required to induce ventricular asystole in the patient.
Additionally, due to the synergistic effect, the ß-blocker may be present in
combination with other compounds capable of inducing ventricular asystole, in an
amount effective to reduce the amount of the compound required to induce
ventricular asystole, for example to about 5-90%, e.g., 30-50% or less by weight of
the amount alone required to induce ventricular asystole.
The administration of the ß-blocker is preferably prior to, or
contemporaneously with, the administration of the cholinergic agent, and in one
embodiment results in a synergistic effect between the ß-blocker and the cholinergic
agent. The amount of ß-blocker present is preferably not sufficient to induce
ventricular asystole by itself, and is sufficient only to cause a local ß-blockade, but
has a minimal effect on electrical conduction of the heart, or is low enough to cause
only a first degree heart block.
In another embodiment, in order to induce reversible ventricular asystole in
the heart of a patient, while maintaining the ability of the heart to be electrically
paced, an AV node blocker is administered in combination with an effective amount
of a second compound, such as a ß-blocker to reduce or suppress ectopic ventricular
activity while maintaining the ability of the heart to be electrically paced. In one
embodiment, the ß-blocker, alone or in combination with the AV node blocker, is
capable of substantially suppressing ectopic ventricular beats in the heart while
maintaining the ability of the heart to be electrically paced. For example, an AV
node blocker, such as an antiarrythmic, such as flecainide, and a ß-blocker, such as
propranolol, may be administered. In one preferred embodiment, the ß-blocker is
administered prior to the AV node blocker. In another embodiment, a composition is
provided that includes an AV node blocker and a ß-blocker in an amount effective to
induce reversible ventricular asystole and wherein the ß-blocker is present in an
amount effective to reduce or suppress ectopic ventricular activity after
administration.
The use of a cholinergic agent, such as carbachol, in combination with a b-
blocker, such as propranolol, preferably produces ventricular asystole at significantly
reduced dosages of the cholinergic agent, while maintaining a short half-life and
rapid onset of effect. A preferred half-life is on the order of about one to ten
minutes. A preferred onset of effect is less than one minute after administration. It
is possible to induce onset of ventricular asystole within about thirty seconds after
administration of carbachol and propranolol to the heart.
The compositions preferably are capable of inducing reversible transient
ventricular asystole of a beating heart to facilitate the performance of minimally
invasive surgical procedures, while still permitting the heart to be electrically paced.
The compositions, including for example a cholinergic agent, preferably can reliably
and in a dose-dependent fashion produce extended periods of reversible ventricular
asystole, for example, for up to about two hours upon either administration of a
single dose, or continuous infusion, depending upon the composition. In preferred
embodiments, the ventricular asystole is chemically reversible. For example, in the
case of carbachol, the ventricular asystole can be reversed by administering atropine,
for example by an intravenous bolus injection, providing an important advantage of
safety during the procedure.
In one preferred embodiment, to induce ventricular asystole, the ß-blocker is
administered to the heart before the cholinergic agent. For example, the ß-blocker in
one embodiment is administered in a single bolus injection into the coronary artery,
and then the cholinergic agent is administered by a single bolus injection followed by
continuous infusion throughout the surgical procedure, to maintain the ventricular
asystole. In another embodiment, where the ß-blocker has a relatively short half life.
such as esmolal, the ß-blocker may be administered by continuous infusion, or a
plurality of bolus infusions. The ventricular asystole continues as long as
administration of the cholinergic agent is continued. In a preferred embodiment, due
to the prior administration of the ß-blocker, it is possible to administer a significantly
reduced amount of the cholinergic agent and thereby reduce the occurrence of side-
effects such as systemic hypotension. Moreover, depolarization of the pacemaker
cells of the heart by the administered composition is preserved, thereby making it
possible to selectively electrically pace the heart to permit the performance of a
surgical procedure while the heart is under transient ventricular asystole.
The time between administration of the ß-blocker and the cholinergic agent is
preferably long enough to permit the ß-blocker to cause a local ß-blockade of the
pacemaker cells of the heart. After bolus administration, the time interval can be, for
example about two minutes. In the case of intravenous or other forms of
administration, several minutes or even hours may be required to permit the ß-
blocker to affect the pacemaker cells of the heart. The subsequent administration of
the cholinergic agent may be controlled by the surgeon. Bolus infusion of higher
doses can be used to give a dose dependent effect, while continuous infusion of
lower doses also may be given to maintain ventricular asystole. In another
embodiment, the ß-blocker may be administered by an initial intracoronary bolus
followed by a continuous infusion.
In one embodiment, the AV node blocker, such as a cholinergic agent, such
as carbachol, is administered in an initial intracoronary bolus of about 0.1 to 150
µg/kg body weight of patient, or about 2 to 20 µg/kg body weight of patient, for
example, about 4 to 16 µg/kg, or about 6 to 14 µg/kg, or in one embodiment, about 8
to 12 µg/kg body weight, in a suitable pharmaceutically acceptable carrier. The AV
node blocker, such as carbachol, is preferably administered over a time period of
about 0.1 to 3 minutes, preferably about 0.5 to 1 minute. In a preferred embodiment.
the AV node blocker, such as a cholinergic agent, such as carbachol, is administered
in an intracoronary bolus of about 0.10 to 10 µg/kg body weight of patient, for
example about 0.10 to 5.0 µg/kg body weight in a pharmaceutically acceptable
carrier over a time period of about 0.1 to 3 minutes, preferably about 0.5 to 1 minute.
The bolus infusion of the AV node blocker such as a cholinergic agent is in
one embodiment followed by a continuous intracoronary infusion at about 0.1 -5
µg/kg body weight/ min of the AV node blocker, which in a preferred embodiment is
a cholinergic agent. The infusion rate in one embodiment is about 0.1 -4.8 µg/kg
body weight of patient/min, for example about 0.1 -2.1 µg/kg/min, or about 0.1 -1.5
µg/kg/min, or about 0.1 -1.0 µg/kg/min, or in another embodiment, about 0.1 -0.5
µg/kg/min. Optionally, the cholinergic agent is combined with a ß-blocker. In one
embodiment, a typical total adult dosage of an AV node blocker, such as a
cholinergic agent, such as carbachol, is about 1 mg to 15 mg. This dosage can
produce reversible ventricular asystole, for example, for a time period of about 5 to
120 minutes, for example, about 5 to 90 minutes, preferably about 30 to 90 minutes,
e.g., about 75 minutes. The dosage may also be, for example, about 1 to 12 mg, or
about 1 to 10 mg, or in one embodiment about 1 to 5 mg. The dosage may be
adjusted depending on the surgical procedure.
The ß-blocker, such as propranolol, in one embodiment is administered
through the right or left coronary artery in a dosage of about 0.01 to 0.07 mg/kg body
weight of patient, for example, 0.01 to 0.05 mg/kg, or about 0.01 to 0.04 mg/kg. The
total amount of propranolol administered is in one embodiment about 1 mg to 6 mg,
e.g., about 1 mg to 5 mg, or, for example, about 2 to 4 mg, or about 3 mg.
For example, one embodiment to induce transient reversible ventricular
asystole in a patient is as follows. An intracoronary injection of 0.5 to 4 mg, e.g.,
about 1.0 mg, of propranolol is administered by intracoronary infusion through a
drug delivery catheter positioned in the right coronary artery just proximate to the
AV node artery, over a time period of about 0.5-3 minutes, e.g., about 1 minute,
preferably followed by a saline flush, such as a 2 mL saline flush. This is followed
by an intracoronary bolus injection of about 0.01 to 0.5 mg, e.g., about 0.025 to 0.3
mg, e.g., about 0.1 mg carbachol administered over about 0.5 to 3 minutes, e.g.,
about 1 minute, and then by an intracoronary infusion of carbachol at a rate of about
0.01 to 0.3 mg/min, e.g., about 0.025 to 0.3 mg/min, for example, about 0.01 to 0.1
mg/min, or, e.g., about 0.05 to 0.1 mg/min, e.g. about 0.0825 mg/min, for a time
period of about 5 to 90 minutes, preferably about 30 to 90 minutes, e.g., about 75
minutes. A dosage amount of phenylephrine in the range of about 0.1 to 1.0 mg if
needed may be administered to counteract any hypotension effects associated with
carbachol administration. Additionally, nitroglycerine may be required in some
patients to counteract the coronary vasodilator effects of systemic phenylephrine
administration.
Additionally, in one embodiment, where the patient is under prior therapeutic
treatment with a ß-blocker, lower amounts of ß-blocker, or alternatively no ß-blocker
may be required prior to the surgical procedure. Moreover, in certain situations
overdrive suppression (i.e., pacing at about 90 to 110 beats/min for about 10 seconds
may be used in addition to the initial intracoronary bolus of carbachol and
propranolol to initiate ventricular asystole prior to carbachol continuous infusion.
Compositions may be administered by intravenous, intracoronary and
intraventricular administration in a suitable carrier. Compositions may be
administered locally to the heart, for example, by direct infusion to the right coronary
artery as a single bolus injection, continuous infusion, or combination thereof. This
can be achieved, for example by administration to the proximal or ostial portion of
the right coronary artery, using a guiding catheter or drug delivery catheter, or by
administration just proximal to the AV branch by means of a drug delivery catheter
positioned in the right coronary artery. Intraventricular (left side) injection also may
be used. Continuous infusion can be continued as long as necessary to complete the
procedure. In one embodiment, the infusion rate can range from about 0.01 to 0.5
mg-min-1, e.g., about 0.01 to 0.3 mg-min-1, or about 0.015 to 0.15 mg-min-1, for
example about 0.016 to 0.12 mg-min-1. Methods of administration include
intravenous, intra-atrial, intra-aortic, and administration via the aortic root, or
coronary artery. Administration may be via any suitable route, for example via the
left or right ventricle, for example proximal to the AV node artery, or via the aorta,
pulmonary artery, pulmonary vein, central vein, right atrium or the coronary sinus.
In another embodiment, administration may be by direct administration into the AV
node artery or AV node. In one embodiment, administration may be via a
hypodermic needle to the AV node.
In addition to local delivery, systemic delivery routes of administration
known in the art may be used, such as oral, transdermal, intranasal, suppository and
inhalation. For example, in addition to injection as described above, the ß-blocker
may be administered orally in a suitable carrier for oral administration. The patient
also may be on therapeutic treatment with a ß-blocker prior to the surgical procedure
and thus may require lower amounts, or even no additional ß-blocker prior to the
surgery.
The compositions capable of inducing ventricular asystole, such as an AV
node blocker and ß-blocker, may be provided in pharmaceutically acceptable carriers
including diluents. A variety of carriers may be used that are known in the art,
preferably in sterile form. Suitable carriers include sterile water, aqueous normal
saline solutions, and aqueous solutions such as lactated Ringer"s solution, or a
solution of a sugar such as dextrose, for example 5% dextrose in water or saline.
Other possible carriers, which may be provided, for example, in an aqueous solution,
include sodium citrate, citric acid, amino acids, lactate, mannitol, maltose, glycerol,
sucrose, ammonium chloride, NaCl, KCl, CaCl2, sodium lactate, and sodium
bicarbonate. In one embodiment, the carrier may be D5 W, a solution of 5% dextrose
in water. Other carriers include buffered aqueous solutions, such as an acqueous
solution comprising 5 mM HEPES (N-[2-hydroxyethyl)piperazine-N"-[2-
ethanesulfonic acid]). Antioxidants or preservatives such as ascorbic acid also may
be provided in the compositions. Carriers known in the art, for example, for
injection, oral delivery, delivery via a suppository, transdermal delivery and
inhalation also may be used.
In one embodiment, compositions are provided which include an AV node
blocker, such as a cholinergic agent and ß-blocker either together or separately in a
pharmaceutically acceptable carrier. In another embodiment, containers containing
unit dosage forms of the AV node blocker, such as a cholinergic agent and the b-
blocker, either in separate containers or in a single container are provided. In one
embodiment, unit dosage forms of carbachol and propranolol are provided either in
separate containers or in a single container for administration to a patient, optionally
in combination with a pharmaceutically acceptable carrier. For example, carbachol
can be present in a pharmaceutically acceptable carrier in a dosage form for
administration to a patient in an amount of about 5 to 150 µg/kg body weight of the
patient, or in a total amount of from about 1 to 20 mg, or in a total amount of about 5
to 10 mg. The propranolol can be present in a pharmaceutically acceptable carrier in
a dosage form for administration to a patient in an amount of about 0.01 to 0.07
mg/kg body weight of the patient, or in a total amount of about 1 to 10 mg, or in a
total amount of about 1 to 5 mg. Carbachol is available commercially from Sigma
Chemical Company, St. Louis, MO.
Thus, in one aspect of the invention, there is provided a composition
comprising an AV node blocker or a ß-blocker, or a combination thereof, in a
pharmaceutically acceptable carrier. The composition, may be provided for example
as an aqueous solution, or in the form of a suspension or emulsion. Optionally, the
composition may include a mixture of AV node blockers and/or a mixture of b-
blockers. The composition may be provided in a form suitable for parenteral
administration. In the embodiment wherein the composition comprises water, the
water is preferably processed, for example by compression distillation, to ensure that
it is sufficiently purified to be suitable for parenteral administration. Methods for
making compositions of a quality suitable for parenteral administration are disclosed
for example, in Gennaro, "Remington: The Science and Practice of Pharmacy,"
Mack Publishing Co., Easton, Pennsylvania, 1995, Vol. 2, Chapter 87, the disclosure
of which is incorporated herein. In one embodiment, the composition is provided in
a form suitable for administration to the cardiovascular system during a surgical
procedure. In one embodiment, the AV node blocker is a cholinergic agent. In a
preferred embodiment, the AV node blocker is carbachol. The pharmaceutically
acceptable composition comprising the AV node blocker or ß-blocker, or
combination thereof, may be provided, for example in an aqueous solution, in a
container, such as a vial, at a concentration suitable for direct administration to a
patient, or may be diluted, for example with saline.
In one embodiment, a pharmaceutically acceptable composition comprising
an AV node blocker, such as cholinergic agent, is provided, which may be used to
permit local cardiac administration of the AV node blocker. In one embodiment,
there is provided a pharmaceutically acceptable composition comprising carbachol,
wherein the composition is suitable for parenteral administration. Preferably, the
carrier is suitable for intracoronary administration. The carbachol may be provided
in an aqueous carrier, such as water. In the composition, which optionally may be
diluted prior to local cardiac administration, the concentration of carbachol may
range, for example, from about 0.01 mg/mL to 2.55 mg/mL, e.g., about 0.1 to 1.0
mg/mL. In one embodiment, the composition may further comprise a ß-blocker.
such as propranolol, at a concentration, for example, of about 0.5 to 6 mg/mL, for
example about, 0.5 to 3 mg/mL, or, e.g., about 1.0 to 2.0 mg/mL or about 1.0
mg/mL. If needed, the composition may be diluted to a concentration suitable for
local administration to the heart, e.g., via an intracoronary bolus or infusion.
Pharmaceutically acceptable compositions also are provided including an AV
node blocker, such as a cholinergic agent and/or a ß-blocker that are suitable for
direct local cardiac administration. In one embodiment, there is provided a
pharmaceutically acceptable composition comprising carbachol, wherein the
composition is suitable for direct local administration, for example, to a coronary
vessel such as the right coronary artery. The carbachol is, for example, provided in
an aqueous carrier, such as water. In one embodiment, the carbachol is provided in
physiologic saline. In the composition, the concentration of carbachol may range, for
example, from about 0.001 to 2.55 mg/mL, for example, about 0.01 to 2.5 mg/mL, or
about 0.05 to 1.0 mg/mL, e.g., about 0.01 to 0.5 mg/mL, for example, about 0.05
mg/mL to 0.2 mg/mL, or e.g., about 0.1 to 0.2 mg/mL, or about 0.075 mg/mL. The
composition may optionally further comprise a ß-blocker, such as propranolol, at a
concentration, for example, of about 0.05 to 6.0 mg/ml, for example, 0.05 to 3.0
mg/ml, or, e.g., about 1.0 to 2.0 mg/ml, or about 1.0 mg/mL. In this embodiment,
the composition is suitable without dilution for local administration to the heart, e.g.,
via an intracoronary bolus or infusion.
In another aspect of the invention, there is provided a surgical kit including a
container comprising a dosage of a cholinergic agent, such as carbachol. In one
embodiment, a surgical kit is provided that includes a first container comprising a
cholinergic agent and a second container comprising a ß-blocker, wherein in one
preferred embodiment, the cholinergic agent is carbachol and the ß-blocker is
propranolol. The containers may include respectively a preferred dosage form of the
carbachol and of the propranolol. The first container may include a carbachol in a
pharmaceutically acceptable carrier, and the second container may include
propranolol in a pharmaceutically acceptable carrier. Alternatively, the cholinergic
agent and the ß-blocker may be provided in a single container, optionally in
combination with a pharmaceutically acceptable carrier. The kit may further include
epicardial or endocardial pacing electrodes or any other disposable items associated
with the pacemaker. The kit also may include a drug delivery catheter and associated
disposable items.
Referring to the drawings where like numerals indicate like elements, drug
delivery and pacing apparatus are shown in accordance with the principles of the
present invention. The pacing system generally includes pacer, a switch box and an
actuator, which preferably can be readily controlled by the physician to remotely
control the pacer through the switch box. The pacing system will be described with
reference to the example illustrated in Figure 1. However, it should be understood
that other configurations may be used.
Referring to Figure 1, a pacing system configured in accordance with the
present invention is shown. The illustrative system generally includes a pacer 18, a
switch or control box 14, and an actuator 22. Pacer 18 may be a conventional
ventricular demand pacer or dual chamber (atrial-ventricular) pacer. Leads 16 couple
the output of pacer 18 to switch box 14 and leads 12 couple switch box 14 to the
patent"s heart. The latter may be achieved for example, either endocardially or
epicardially. Switch or control box 14 preferably is configured so that when
actuated, it delivers the pacing signals or output of pacer 18 to leads 12. Conductor
or lead 20 couples remote actuator 22 to switch box 14. Although a conventional
foot pedal type actuator is shown, it should be apparent from the foregoing and
following discussion that other actuators such as handle held actuator 24 (shown in
phantom) may be used. Further, as an alternative to epicardially or endocardially
placed pacing leads, the leads may be transvenously delivered for coupling to the
heart. In a further alternative, electrodes, such as transarterial electrodes, can be
incorporated into the drug delivery catheter.
This pacing system of the present invention preferably provides to the
surgeon remote control of the on/off pacing function only. All other parameters
which are user selectable (rate, output, etc.) preferably are not remotely
programmable but must be adjusted by using controls on the pacemaker.
Referring to Figures 1A and 1B, circuit diagrams of the pacing system of
Figure 1 are shown. Switch box 14 includes an electrical or mechanical switch 23 to
which actuator 22 couples. This coupling allows the switch to be energized or
deenergized as would be apparent to one of ordinary skill. Preferably, foot pedal 22
is configured to be in an "Off" (electrically open) position when in its normal state
and to be in an "On" (electrically closed) position to open switch 23 in switch box 14
and interrupt delivery of pacing signals to the heart when the pedal is depressed.
Accordingly, if the power source to the pedal is interrupted, the heart will be paced.
Alternatively, the foot pedal may be configured to be in an "On" position when in its
normal state and to be in an "Off position when the pedal is depressed.
Returning to Figures 1A and 1B, switch box 14 preferably is configured in a
manner to allow the pacing signal to pass through the box, to leads 12 and, thus, to
the patient while actuator 22 is in the "Off position. As shown in Figure 1 A, the
switch box"s switch 23 opens when the actuator is activated (e.g., the foot pedal is
depressed). This opening prevents the pacing signal from going to the patient. On
the other hand, as shown in Figure 1B, the switch box"s switch 23 closes to again
allow the pacing signal to pass through to the patient, when the actuator is released.
Commercially available switch boxes and foot pedal actuators may be used. For
example, a suitable switch box with foot pedal is the Treadlight 2, Catalogue No. T-
91-S manufactured by Line Master Switch Corporation. This switch provides an
open circuit when actuated as shown in Figure 1 A.
Safety features may be incorporated into the switch box. The first is a timer
or override circuit, either programmable or factory set, that limits the time the switch
or control box can interrupt the pacer. This circuit overrides the actuator, if the
actuator should happen to be held down (i.e. in the "On" position) too long, i.e.,
longer than the preset maximum time. The override circuit may be set or configured
to override the activator after an interval of time of about 0.1-60 seconds, more
preferable about 5-30 seconds, or more preferably about 10-15 seconds.
A second safety feature is an indicator (visual and/or audible) that indicates
the pacing signal is not being sent to the patient. A third safety feature is an indicator
(visual or audible) that the pacing signal is going out to the control box, especially to
signify the end of an interruption period (resumption of pacing). Preferably, the
indicator or indicators are audible signals.
The control box could have additional features that may be more useful for
the user than for safety. The first feature would be an indicator, preferably audible,
preparing the user for the resumption of pacing. This could be a beeping tone that
increases in frequency as the interruption period ends. Second, the control panel
should be battery powered either by a disposable or re-chargeable battery. Other
features include a control box that is preferably within 7" x 10" x 5", lightweight,
less than 3 pounds, and easy to use with current pacer and pacing lead designs."
Figure 1C presents one embodiment of the control box as schematically
shown in Figures 1, 1A and 1B. As shown in Figure 1C, a suitable control box 14"
includes debounce circuit 100, pull-down resistor 102, timer select switch 104, first
timer 106, second timer 108, diodes 110, transistor 112, inductive solenoid coil 114,
switches 116, beeper control 118, volume control 120, and speaker 122.
Control box 14" uses debounce circuit 100 to generate a steady signal when
mechanical foot pedal 22 is depressed. Debounce circuit 100 has an input terminal
100A and an output terminal 100B. The input terminal connects to pull-down
resistor 102. This terminal also connects to the foot pedal switch 22A of foot pedal
22. When the foot pedal switch is open as shown in figure 1C (e.g., when the
operator does not depress the foot pedal), the input terminal is pulled to ground
through pull-down resistor 102. On the other hand, when the foot pedal switch
closes (e.g., when the operator depresses the foot pedal), the input terminal connects
to the power supply voltage source through the foot pedal switch 22 in order to
receive the power supply voltage. In response to the power supply voltage provided
by mechanical foot pedal 22, the debounce circuit generates a signal on its output
terminal that it steadily maintains at one level (e.g., the ground level) until the foot
pedal switch opens.
As shown in Figure 1C, the output terminal 100B of the debounce circuit 100
connects to first timer 106. The voltage on this output terminal is usually in a first
level (e.g., the power supply voltage) when the input to the debounce circuit is pulled
to ground (i.e., when the foot pedal has not been depressed). However, this output
terminal"s voltage transitions to a second level (e.g., the ground voltage) when the
input to the debounce circuit transitions to the power supply voltage (i.e., when the
foot pedal has been depressed). As further described below, the voltage at the output
terminal 100B in combination with the signal supplied to the reset pin 106C of the
first timer circuit controls the operation of this timer circuit.
Control box 14" uses first and second timer circuits 106 and 108 in order to
measure the lapse of a selected period of time. The amount of time selected on time
select rotary switch 104 is the maximum amount of time that the physician can
interrupt the supply of the pacing signal to the heart by depressing the foot pedal.
Once the control box 14" determines, through the use of timers 106 and 108. that the
maximum amount of time has expired, then the control box 14" overrides (i.e.,
ignores) the signal generated by the depressed foot pedal and resumes the supply of
the pacing signal to the patient. The second timer counts the last five seconds in the
selected period of time, while the first timer counts the remainder of time.
Both the timers 106 and 108 have reset pins (i.e., reset terminals) 106A and
108A that receive the signal supplied to input terminal 100A of debounce circuit 100.
When the signal supplied to the reset pin of a timer is low (i.e., when the foot pedal
has not been depressed), the timer enters its reset mode and resets its measured time
value to its initial value. Each timer exits its reset mode and enters a standby mode
when the signal supplied to its reset terminal is high (i.e., when the foot pedal has
been depressed).
Also, each timer enters its operational modes when it receives a trigger signal
at its input after it has entered its standby mode. Once the timers are in their
operational modes, they start counting up or down to their expiration values when
they receive an appropriate signal (e.g., a high voltage) on their input terminals
106A, 108A. First timer 106 receives its trigger signal from the output of the
debounce circuit. Thus, the transition of the output of the debounce circuit from one
state to another (e.g., goes from a high level to a low level) triggers the operation of
the first timer 106. Once triggered, the first timer 106 starts to count towards its
expiration value. The physician determines the expiration value of the first timer by
operating the timer select switch 104, which connects to the first timer.
While the first timer operates (i.e., while it counts) and before it has reached
its expiration value, the signal at this timer"s output terminal 106B is at a first
voltage level (e.g., the power supply level). The signal from output terminal 106B
flows through diode 1 lOA and is supplied to the gate of transistor 112 to turn ON
this transistor. Transistor 112 can be any type of transistor. In Figure 1C, this
transistor is an NMOS device.
Once transistor 112 turns ON, it draws current from the power supply "hrough
the inductive solenoid coil 114. This coil serves as a relay (i.e., coil that when
energized operates a mechanical switch). Thus, when current passes through the
solenoid coil, it activates the relay which opens switches 116A-D of patient connect
relay 124. When the relay is deactivated, switches A-D couple the signal from the
pacer to the patient through leads 12.
Referring to the embodiment illustrated in Figure 1C, switch 116A couples a
ventricle inlet (V-IN(-)) to a ventricle outlet (V-OUT(-)). Switch 116B couples a
ventricle inlet (V-IN(+)) to a ventricle outlet (V-OUT(+)). Switch 116C couples an
atrial inlet (A-IN(-)) to an atrial outlet (A-OUT(-)), while switch 116D couples an
atrial inlet (A-IN(+)) to an atrial outlet (A-OUT(+)). The inlets are coupled to the
pacer and the outlets are coupled to the patient. Referring to Figure 1D, a schematic
representation of an endocardial lead arrangement between the control box and the
right atrium of a patient is shown, together with the coupling between the control box
and the pacer. An actuator may be coupled to the control box as described above.
The inlets (A-IN(-), A-IN(+)) may be coupled to the pacer 18 adapter cables and the
outlets (A-OUT(-), A-OUT(+)) may be coupled to the patient with leads as shown in
the drawing and as would be apparent to one of ordinary skill. Specifically, one lead
may be coupled to positive terminal 140, which is in the form of a ring, and the other
lead may be coupled to a negative terminal 142, which may have a generally
hemispherical configuration. A similar arrangement can be used to couple the
control box to the right ventricle. Although an endocardial lead configuration is
shown in Figure 1D, epicardial leads as shown in Figure 1E may be preferred.
Specifically, epicardial leads, which may be sutured to the heart (e.g., right atrium)
as shown in Figure 1E and generally designated with reference character "S",
generally are preferred in open chest procedures since they can be readily sutured to
the heart. Again, a similar arrangement can be used to couple the control box to the
right ventricle.
Although the patient connect relay 124 is shown as a dual chamber pacing
system, it should be understood that single chamber pacing systems can be used to
pace the ventricle as would be apparent to one of ordinary skill in the art (e.g., by
only using switches 16A and B shown in Fig. 1C).
The output of the first timer is also supplretfto a beeper control circuit 118,
which controls the output of a speaker 122. Hence, when the first timer"s output is
active (i.e., its at a first voltage level, such as the power supply level), it turns ON the
beeper control circuit, which in turn generates a first audible signal through speaker
122.
When the first timer expires (i.e., when it has reached its expiration value),
the signal at its output terminal transitions from the first voltage level to a second
voltage level (e.g., transitions from the power supply level to ground level). The first
timer then enters its standby mode, where it will stay until it is reset by the opening
of the foot pedal switch.
The second timer has an edge detector (e.g., a negative edge detector) that
detects this transition. Once it detects this transition, the second timer transitions
into its operation mode, and thereby starts to count towards its expiration value. The
second timer"s expiration value is set at five seconds.
While the second timer is in its operation mode and has not reached its
expiration value, the signal at its output terminal is at a first voltage level (e.g., the
power supply level). In turn, diode 110B supplies this signal to the gate of transistor
112, and thereby keeps this transistor ON. While transistor 112 is ON, it continues
to draw current through the coil 114, which, in turn, keeps switches 116A-D, which
control delivery of the pacer signal to the patient, open.
The output of the second timer is also supplied to a beeper control unit.
Hence, when this output is active (i.e., its at a first voltage level, such as the power
supply level), it turns ON the beeper control unit, which in turn generates a second
audible signal through speaker 122.
Finally, it should be noted that the output of the timers resets to the second
voltage level (e.g., ground) whenever the foot pedal switch opens and the timers are
reset. This resetting operation overrides the counting operation of the timers. Thus,
if the timers are in the process of counting, the opening of the foot pedal makes these
timers stop counting and reset. Any suitable timers may be used such as 555 timers
manufactured by National Semiconductor (Santa Clara, CA).
As an alternative to foot pedal 22, a conventional needle holder 24 can be
used to control the pacer switch box. In this case, the needle holder preferably is of
the standard Castro-Viejo variety. However, any other manual switch actuator
operable by the surgeon for opening and closing the switch in switch box 14 on
demand can be used in accordance with the invention to electrically connect and
disconnect pacer 18 with pacing leads 12. Thus, the actuator can be incorporated in
or on one of the surgeon"s instruments, such as surgical site retractor, or any other
location easily and quickly accessed by the surgeon.
Any conventional pacer suitable for ventricular demand pacing and having
external leads that can be electrically coupled to a switch box 14 may be used. An
example of such a suitable pacer is the Medtronic model 5330 or 5375, Demand
Pulse Generator manufactured by Medtronic Inc. (Mpls, Minn.)
It should be understood that although a particular pacing configuration is
shown, other configurations may be used. For example, the pacer and switch box
may be combined in a single unit. If the switch box is incorporated in a pacer (i.e.,
pacemaker), specifications of the pacemaker should be similar to currently
manufactured external pacemakers (e.g., Ventricular or atrial-ventricular sequential;
Rate range: 30 to 180 ppm (pulses per minute), continuously adjustable or in
increments of 1 ppm; Output current range: 0.1 to 20 mA; Sensitivity range: 1.0
mV(maximum) to asynchronous; Pulse width: 1.8ms maximum).
Pacer 18 preferably is an extracorporeal pacer and differs from implantable
pacemakers in the following ways. Pacer 18 typically will be in excess of
400 grams, can use replaceable (battery life of approximately 500 hours) or
rechargeable batteries (9v), may be line power designed to last several years, and
need not be constructed with a biocompatible exterior shell or be hermetically sealed.
Further, the pacing system may be configured to synchronize activation and
deactivation of the patient"s ventilator (not shown) with pacing. For example, the
control box may be configured for coupling to a ventilator so that pacing and
ventilator signals are simultaneously delivered to the patient leads 12 and the
ventilator when the actuator is in a first state (e.g., when the foot pedal is released).
In this example, the pacing and ventilator signals are simultaneously interrupted
when the actuator is in a second state (e.g., when the foot pedal is depressed). The
synchronization of pacing with a ventilator may minimize or eliminate unwanted
heart motion associated with a patient"s breathing with a ventilator.
With an understanding of the pacing system in hand, drug delivery according
to the principles of the invention will be described with reference to Figures 2- 7.
Generally, Figures 2 and 3 show delivery into the coronary sinus (Figure 4 shows an
alternative balloon configuration); Figure 5 shows intra-aortic delivery; and Figures
6 and 7 show delivery through the right coronary artery. Discussion of a further
delivery procedure in accordance with the present invention, intraventricular
injection, also will be provided.
Coronary Sinus Injection
Referring to Figures 2,2A, 3, and 3A a coronary sinus delivery catheter 30 is
shown according to the present invention for local drug administration into the
coronary sinus (CS) according to the present invention is shown. Coronary sinus
delivery catheter 30 preferably is a medium-diameter, e.g. about 6-8 French, single or
dual lumen, flexible catheter. The tip of catheter 30 may be curved slightly to give ,•!
so-called hockey-stick appearance as shown in the drawings. This configuration
facilitates, for example, introducing the catheter into the coronary sinus from the
atrium as shown in Figure 2 where the distal tip is shown prior to introduction into
the coronary sinus. A low-pressure balloon 32 of up to about 2 cm in diameter is
located near the tip of the catheter. Two ports 34, 36 are present at the proximal
portion of catheter 30 for balloon inflation and drug injection, respectively. Catheter
30 further includes inflation lumen 37 and drug delivery lumen 39 (Figures 2A and
3A) which fluidly couple ports 34 and 36 to balloon 32 and delivery or discharge
opening 38.
Any of three catheter lengths may be used depending on whether the catheter
is introduced into the coronary sinus: (A) through the right atrium or atrial
appendage; (B) via the internal jugular or subclavian vein; or (C) via the femoral
vein. A guidewire (not shown) is used to facilitate transvenous placement, and a
stiffer wire obturator (not shown) is provided for catheter insertion through the right
atrial appendage.
Access to the right atrial appendage (approach A) requires an operative
approach through the right chest or through the mediastinum. A plegeted pursestring
suture (e.g. 4/0 polypropylene), which is conventional in the art, is placed on the
right atrium (RA) or atrial appendage, and catheter 30 is secured in place with a
Rumel-tourniquet. The transvenous approaches (approaches B and C) require
expertise in coronary sinus cannulation over a guidewire using fluoroscopic or
echocardiographic guidance. The internal jugular or subclavian approach accesses
the coronary sinus via the superior vena cava (SVC) as shown in Figure 2. The
femoral vein approach accesses the coronary sinus via the inferior vena cava (IVC).
After the catheter is placed in the coronary sinus using any of the three
approaches described above, the guidewire or obturator, which was used to introduce
the catheter into the coronary sinus, is removed. Injection port 36 is then connected
to a three-way stopcock (not shown) for intermittent measurement of coronary sinus
pressure and administration of the composition(s) provided in accordance with the
present invention. With inflation of the low-pressure balloon within the coronary
sinus (Figure 3), a right ventricular pressure wave form is observed. The inventive
composition(s) is then administered as a bolus injection through drug injection port
36 so as to be delivered at the delivery port 38. Coronary sinus pressure during bolus
injection generally should not exceed about 30 mm Hg. Alternatively, the
composition(s) may be administered as a bolus injection followed by continuous
infusion or as a continuous infusion alone. Balloon inflation may be rapid
inflation/deflation balloon synchronized with the electrocardiogram (ECG).
Alternatively, the coronary sinus may be occluded, partially or completely, for a
period of about one or two hours. Balloon 32 may have a much thinner wall
construction than balloon 42 (discussed below) because it need not expand against
arterial pressure. Previously placed pacing leads 12 permit ventricular pacing during
drug induced ventricular asystole. Removal of the catheter simply requires deflation
of the balloon and closure of the atriotomy with the pursestring suture.
Referring to Figure 4, another coronary sinus catheter configuration is shown.
Catheter 30" is provided with laterally spaced balloons 32" which are fluidly coupled
to inflation lumen 39". Drug delivery lumen 37" opens in a region between the
balloons.
Intraventricular Injection
Another drug administration approach is intraventricular injection into the
left ventricle via a catheter (not shown). With this approach, the catheter may be
delivered in retrograde fashion through the arterial system, aorta and through the
aortic valve into the left ventricle. In the alternative, a catheter or cannula may be
inserted directly into the left ventricle (preferably the apex) through a hole made by
the surgeon. In a further alternative, a needle may be inserted directly into the left
ventricle.
Aortic Root Injection
Another drug administration approach is injection of drug into the aortic root
with, for example, an intra-aortic delivery catheter 40 as shown in Figure 5. This
permits direct aortic administration of compositions in accordance with the invention
during diastole while providing ventricular support analogous to an intra-aortic
counterpulsation device. Catheter 40 preferably is a dual lumen catheter provided for
rapid inflation and deflation of a durable, low-pressure balloon 42 arranged to inflate
in synchronization with heart beat (e.g., electronically synchronized with ECG "P"
waves so that balloon 42 inflates during diastole and deflates just before systole).
Importantly, complete occlusion of the aorta by the catheter balloon 42 is not
required for proper functioning of the device. Thus, risk of injury to the aortic wall,
for example, the aortic dissection, is minimized. As in the embodiment discussed above, a balloon inflation port 44 and a drug injection port 46 are provided. Catheter
40 a drug delivery and inflation lumens similar to catheter 30 with the exception that
the drug delivery lumen in catheter 40 terminates with a discharge opening 48
proximal to balloon 42 this configuration facilitates delivery of drugs in the vicinity
of the coronary arteries. Catheter 40 may be inserted through a hole made by the
surgeon in the wall of the aorta as shown in figure 5, for example, or endovascularly
delivered via a percutaneously catheter insertion in the femoral artery. However, if a
catheter is desired to be delivered in a retrograde fashion through the arterial system
(e.g. femoral artery and the aorta), the balloon and lumen configuration of catheter 30
or 30", for example, is preferred. The balloon diameter may be larger to correspond with the larger size of the aorta and the balloon walls also may be constructed to
withstand the greater pressures in the aorta.
Returning to Figure 5, which illustrates placement of catheter 40, a
pursestring suture (not shown) is placed on the aortic root and catheter 40 is inserted
into the ascending aorta and secured with a Rumel tourniquet. The intra-aortic
balloon is inflated during diastole and deflated during systole, using the patient"s
ECG signal for synchronization. Drug delivery is given with a bolus infusion and/or
continuous infusion. With drug induced ventricular asystole, the heart is electrically
paced, as detailed herein below, permitting continued intra-aortic counterpulsation.
In the case of where the accompanying procedure is a coronary artery bypass
procedure, catheter 40 is removed after the distal anastomosis is completed. Then, a
partially occluding clamp is placed on the aorta, and the aortitomy may be used for
the proximal aortosaphenous anastomosis. Alternatively, the catheter 40 may be
removed and the aortic pursestring simply tied.
Direct Infusion Into Right Coronary Artery
Another drug administration approach is direct infusion into the right
coronary artery (RCA). This approach advantageously delivers drug more local to
the AV node than the approaches described above. Other methods are generally less
efficient because when-mixed in the aorta, ventricle, or other parts of the
cardiovascular system, significant drug dilution occurs by the time it reaches the AV
branch of the RCA.
This approach can be achieved by either injection into the proximal or ostial
portion of the RCA, by use of a guide catheter or drug delivery catheter, or by
injection just proximal to the branch perfusing the \V node (AV node artery) by
means of a drug delivery catheter positioned in the RCA as shown in Figure 6.
Alternatively, the drug delivery catheter can be positioned directly in the AV nodal
artery through the RCA to delivery the drug more locally to the AV node. The
catheter may be introduced into the coronary artery via the arterial system (femoral,
radial, subclavian) with a larger diameter coronary guiding catheter. In cases of a left
dominant system anatomy or occluded RCA, the catheter may be used in a similar
fashion to deliver the drug into the left coronary artery to, for example, the
circumflex branch.
Referring to Figure 6, an exemplary catheter design as shown in the
drawings. Catheter 50 is a small diameter (for example, about 3-4 French) single
lumen catheter with a drug delivery opening 58 located at the distal end of the
catheter to provide selective coronary artery drug delivery. By avoiding the need for
a separate channel for balloon inflation, catheter 50 maximizes the volume of
catheter lumen dedicated to drug delivery while minimizing catheter diameter.
In use, catheter 50 is introduced into the right coronary artery under
flouroscopic guidance through a larger diameter (6-8 French) coronary guiding
catheter 56, which is positioned at the ostium, and over a guidewire which is placed
distally in the RCA.
After appropriate positioning of the catheter tip, just proximal to or within the
take-off of the artery to the atrioventricular node branch (B) the guiding catheter is
pulled back from the ostium of the RCA to provide blood flow to the RCA, the
guidewire is removed, and a bolus dose is given. Alternatively, a continuous
infusion of drugs can be administered into the distal right coronary artery. Coronary
catheter 50 is small enough that blood flow is not significantly impeded to the RCA.
Referring to Figures 7 and 8, another embodiment for the coronary delivery
catheter is shown. Catheter 60 is the same as catheter 50 with the exception that
catheter 60 has a bent distal end portion 62. Catheter 50 or portion 62 can be
positioned within the branch (B) to the AV node. The bent distal end configuration
minimizes or eliminates the possibility of the catheter entering the branch going
down a posterior left ventricular branch.
Although particular drug administration routes have been described, it should
be understood that other routes may be used including, without limitation, needle
injection into the aorta, needle injection into the AV node, and trans-epicardial
absorption (e.g., a trans-myocardial patch which slowly releases pharmaceutical
agents into the myocardium).
Pacing
Prior to drug delivery, the heart is prepared for cardiac pacing as discussed
above. In general, leads 12 may be temporarily affixed to the right ventricle of the
heart such as by suturing or other manner as would be apparent to one of skill in the
art. Drugs are administered to the heart through, for example, any one of catheters
30, 40, 50 or 60 to induce ventricular asystole. Pacing of the heart is established and
maintained. The pacing can be transiently interrupted by temporarily deactivating
the pacemaker using, for example, foot pedal 22. When the foot pedal is in its
deactuated, raised position, the switch in the pacer switch box is closed, and current
flows from the ventricular demand pacer 18, through the switch box 14 and the
pacing wires 12 to the heart 10 without impediment. During this time, the heart
preferably is paced at a rate between 90 to 110 beats/minute. When complete heart
block is necessary, to enable a surgical procedure to be performed, pacing is disabled
by depressing the foot pedal. In the illustrated and currently preferred embodiment,
this opens the switch in pacer switch box 14, stopping the current flow from pacer 18
to pacing leads 12. Since no current reaches the heart while the foot pedal is
depressed, ventricular asystole occurs, thus allowing precise suturing or other
manipulative procedures to be performed. Once, e.g., a suture has been applied, the
pacer may be reactuated by releasing the foot pedal, thereby to reestablish the
electrical connection between the pacer 18 and the pacing wires 12 and resuming
pacing of the heart at the prescribed rate until another precise manipulation is
required. By providing a surgeon-controlled device, such as with a foot pedal, remote
from the pacer for controlling the pacer, the surgeon can have complete and
immediate control over when pacing is interrupted, even though the surgeon also has
surgical instruments in his or her hands. This allows the surgeon to coordinate
precisely the pacing of the heart to the manipulative step, thereby minimizing
unnecessary and undesired cardiac arrest.
The pacer control box also may be configured to control interruption of a
patient"s ventilator so that the pacing may be synchronized (e.g., the actuator
activates pacing and ventilating equipment (not shown) simultaneously and
deactivates pacing and the ventilating equipment simultaneously). Thus, the switch
box can be electrically coupled to a ventilator so that when the foot pedal described
above is depressed pacing and ventilation are deactivated and when it is released,
pacing and ventilation resume. This arrangement may eliminate some small motions
of the heart associated with a patient"s breathing during a surgical procedure.
The invention will now be described in more detail by reference to the
following non-limiting examples.
Example 1 - In Vivo Studies
The following comparative in vivo studies demonstrated the synergistic effect
of the use of the cholinergic agent carbachol in combination with the ß-blocker
propranolol in stimulating ventricular asystole according to the present invention.
Eleven male crossbred swine weighing 20-25 kg were studied, eight of which
received carbachol alone and three of which received carbachol plus propranolol.
The swine were sedated using 10 mg/kg IV ketamine. After 20 minutes, the animals
were induced with 10 mg/kg IV thiopental sodium and orotracheally intubated. The
proper anesthetic plane was maintained with 1 % Isoflurane. Periodic arterial blood
gas samples were obtained to guide ventilator management. The electrocardiograph
was continuously monitored. Through a 7 Fr sheath in the left femoral artery,
arterial blood samples were obtained and amicromanometer was inserted to monitor
central aortic blood pressure (Millar Instruments, Inc., Houston, TX). The heart was
exposed through a median sternotomy and suspended in a pericardial cradle. Two
temporary epicardial pacing wires were affixed to the right ventricle and connected
to an external pacemaker (Medtronic, Inc., Minneapolis, MN). The pacemaker was
modified to permit deactuation by means of depressing a foot pedal. Through the
femoral sheath, an AR-1 guide (Cordis Corp., Miami Lakes, FL.) was placed into the
right coronary artery. An 0.014-inch floppy guide wire was then advanced into the
right coronary artery to the level of the posterior descending coronary artery. The
AR-1 guide was removed and a 2.5 Fr Tracker (Cordis Corp., Miami Lakes, FL.)
catheter was inserted over the guide wire. Using dye injection, the catheter was
positioned just proximal to the take-off of the atrioventricular nodal artery.
Carbachol (Sigma St. Louis, MO) solution was prepared the day of the experiment
and infused at a constant rate using a Harvard pump.
Animals received either carbachol alone or carbachol in combination with
propranolol (Inderal®, Wyeth Ayerst, Philadelphia, PA). All animals were
instrumented and allowed 10 minutes of hemodynamic stability. Before carbachol
was administered, each subject received a 500 ml IV bolus of 0.9% sodium chloride.
In the animals receiving carbachol alone, carbachol was continuously infused
through the Tracker catheter at increasing doses of 0.44, 0.62,0.88, and 1.72
mg/min, until ventricular asystole was observed.
In the animals receiving carbachol plus propranolol, a 1 mg dose of
propranolol (0.04-0.05 mg/kg) was administered through the Tracker catheter.
Carbachol was then administered as a 0.5 mg intracoronary bolus (0.02 mg/kg)
followed by a constant infusion. The infusion rate necessary to achieve ventricular
asystole was 0.03 mg/min (1.1 to 1.2 µg/kg/min). After carbachol-mediated
ventricular asystole was observed, the heart was paced at 100 beats/minute. At 60-
second intervals, the pacemaker was turned off for five seconds to determine the
underlying cardiac rate and rhythm. The SBP, DBP, and MAP were recorded every
five minutes. The duration of ventricular asystole, defined in this example as a heart
rate less than twelve beats per minute, was recorded. Profound hypotension (SBP
intravenous bolus injections of phenylephrine (0.02 mg/kg), or both. After 75
minutes, the carbachol infusion was stopped and the time required to return to
normal sinus rhythm was recorded. The results are set forth in Table 1 below.
Example 2 - Treatment of Human Patients
Ten human patients were treated pursuant to an investigational new drug
clinical trial following Institutional Review Board and FDA approval and informed
consent.
Repair of a leaky distal anastomosis was performed on 9 human patients
(designated patients 101-109) with stable coronary artery disease (CAD) following
open-chest coronary artery bypass graft (CABG) surgery. The study was conducted
to assess the ability to induce pacemaker-dependent reversible ventricular asystole in
patients on cardiopulmonary bypass (CPB) utilizing an aortic cross clamp
undergoing an open-chest CABG procedure. Established institutional techniques for
preparation and conduct of CABG were used. At the end of the surgical procedure,
and after the aortic cross clamp was removed, the AV-node blocker carbachol and
the beta-blocker propranolol were serially administered to the patients to induce
pacemaker-dependent ventricular asystole. In patients 101-109, the propranolol and
carbachol were used at the end of the CABG surgery only during repair of leaking
distal vascular anastomoses, while the patients were still on cardiopulmonary bypass
(CPB) subsequent to the removal of the aortic cross clamp. In the tenth patient
(designated patient 201), the carbachol and propranolol drugs and temporary pacing
were used for the CABG procedure itself, and the aortic cross clamp was avoided.
The patients were selected based on the following key criteria. Patients were
selected ranging between 18 and 70 years in age with a normal sinus rhythm with P-
wave-R-wave interval not exceeding 0.16 sec. Men or women were selected who
had a stable coronary artery disease and were undergoing elective CABG
revascularization of distal target(s) in the left anterior descending (LAD) artery
system, right coronary artery (RCA) and/or the left circumflex (LCX) artery.
Patients were selected with right dominant coronary circulation or an expectation that
their AV node was supplied by the RCA, and with the presence of at least two of the
following angiographic criteria: (1) coronary arteries greater than 2 mm in diameter,
(2) noncalcified coronary arteries, or (3) an LAD that was not intramyocardial.
Patients with any of the following conditions were intended to be excluded
from the study: (1) significant left main coronary artery stenosis, (2) left dominant coronary circulation, (3) RCA with proximal chronic total occlusion or inability to
pass drug infusion catheter past proximal RCA stenosis, (4) presence of any
significant hemodynamic instability, including, but not limited to, unstable angina or
active ischemia requiring maximal medical management, malignant ventricular
arrhythmias currently requiring medical management or cardiogenic shock requiring
blood pressure support, (5) presence of any significant condition that increases the
risk of the CABG procedure or other study procedure, including but not limited to, a
history of peripheral vascular disease, hypertensive heart disease, cardiomyopathy.
New York Health Association (NYHA) Class 3 or 4 congestive heart failure, chronic
renal insufficiency or failure, prior CABG, valvular heart disease, unusual body
habitus (e.g., morbid obesity), presence of acute pulmonary infection/pneumonia,
metastatic cancer, thyrotoxicosis, sepsis, history of stroke or transient ischemic attack
(TIA) or asymptomatic carotid bruit, (6) recent (within 2 weeks) acute myocardial
infarction, (7) documented cardiac ejection fraction procedure, (8) presence of any significant condition that would make the
determination of the efficacy and/or safety endpoints of the study more difficult,
including, but not limited to, first or second degree heart block, left or right bundle
branch block or other IVCD, (9) presence of any significant condition that increases
the risk of exposure to any of the components of the drugs as follows: Propranolol -
This includes, but is not limited to, significant asthma, obstructive lung disease,
congestive heart failure, hypersensitivity to propranolol or other beta-adrenergic
antagonists; Carbachol - This includes, but is not limited to, asthma, obstructive lung
disease, epilepsy, Parkinsonism, peptic ulcer disease, hepatic insufficiency,
hypersensitivity to carbachol or other cholinergic agonists (i.e., cholinomimetics or
acetyl-cholinesterase inhibitors), (10) presence of any significant condition that
increases the risk of use of a temporary pacemaker. This includes, but is not limited
to, implanted permanent pacemaker, history of ventricular tachycardia or fibrillation
requiring current antiarrhythmic therapy, other arrhythmia or condition that increases
the risk of cardiac pacing, e.g., Wolfe-Parkinson-White syndrome, and (11) pregnant
or nursing women.
For the first 9 patients, CABG surgery was performed using well established
traditional methods. Patients were placed on CPB, the aorta was cross-clamped and
cardioplegic arrest was administered. After distal and (if applicable) proximal
anastomoses were sutured, the cross-clamp was removed and (if necessary) the heart
defibrillated with patients still on CPB. When a leak requiring repair was detected at
the distal anastomotic site(s), epicardial pacemaker leads were sewn into place on the
ventricles and, optionally, the right atrium, of the patients and the pacing thresholds
determined and recorded. A temporary pacemaker was connected to the epicardial
leads. The pacing voltage was set at 10 times the pacing threshold. The pacemaker
was first placed in ventricular-ventricular inhibited (VVI) mode with a rate of 60±l 5
bpm and pacing ensued for 2 minutes. Hemodynamic acceptability of the VVI-paced
rhythm was assessed. The pacemaker was then set in ventricular-atrial triggered
(VAT) mode and pacing ensued for another 2 minutes. Hemodynamic acceptability
of the VAT-paced rhythm was assessed.
During surgery and prior to administration of the drug protocol, fluoroscopy
was used to position an appropriate catheter, e.g., a Tracker™ (Target Therapeutics,
Freemont, CA) catheter with an appropriate guide wire, in the proximal right
coronary artery. This catheter was used for intracoronary administration of the study
drugs. If at any time during the procedure, catheter displacement was noted, repeat
angiography was used to reposition the catheter. Adequate supplies of
phenylephrine, other adrenergic agents and volume repletion fluids were available at
the bedside during and following drug administration in the event of unexpected
adverse events, to control blood pressure, and/or to protect against inadvertent
overdose.
The propranolol solution used was an injectable solution of Inderal® (Wyeth-
Ayerst, Philadelphia, PA). The initial propranolol dose was 1 mg of a 1 mg/mL
solution. Carbachol was provided in a vial containing 6 mL of a 0.255% solution
(mg/dL). Each vial contained 2.55 mg/ml of carbachol in 5 mM sodium citrate and
was adjusted to pH=7.0 using citric acid. The carbachol infusion solution was
prepared by adding 5 mL of this solution to 250 mL of sterile saline. After
reconstitution, the resulting concentration of the carbachol solution was 0.005%, or
0.05 mg/mL. The initial dose of carbachol was 0.025 mg or 0.5 mL and the initial
infusion rate was 0.025 mg/min or 0.5 mL/min of the 0.005% solution.
A loading dose of propranolol ranging between 1-6 mg first was given to
patients over a period of 1-3 minutes. Carbachol was administered as an
intracoronary low dose bolus and as an infusion. For Patients 101-108, the bolus
dose of carbachol used to initiate reversible ventricular asystole was in the range of
0.05-0.225 mg and the sustained infusion of carbachol used to maintain ventricular
asystole was in the range of 0.05-0.15 mg/min. In one of the patients studied,
overdrive pacing was used in conjunction with the loading dose of carbachol to
induce ventricular asystole. Once complete heart block was achieved with no
ventricular escape beats, and a pacemaker-dependent rhythm established, for patients
101-108 the distal anastomosis(es) were repaired during brief (up to 5 seconds)
interruptions of pacing.
For patient 201, the drugs and temporary pacing were used for the CABG
procedure itself. A loading dose of 4 mg propranolol and 0.15 mg of carbachol were
administered via intracoronary delivery to Patient 201 to initiate reversible
ventricular asystole. Subsequently, an infusion of carbachol at a rate of 0.1 mg/min
was given via intracoronary delivery to the patient to maintain ventricular asytole for
a period of about 45 minutes. During this arrest period, a left internal mammary
artery and obtuse marginal graft procedure were performed by the surgeon using
intermittent pacing interruptions to successfully place the graft sutures in a
substantially still rather than moving heart, producing the benefit of an improved
technical result and avoidance of cross-clamping of the aorta.
A dose of phenylephrine ranging between about 0.24-0.32 mg was
administered to Patients 101, 103, 105-109 and 201 to control hypotension. When a
satisfactory technical result had been achieved, the drug infusion was stopped and
atropine was administered to determine the reliability of pharmacologic reversal of
complete heart block with the exception of Patient 201, who was allowed to return to
normal sinus rhythm naturally, over less than 15 minutes. The dosage amount of
atropine used to reverse arrest in Patients 101-108 was about 1.0 mg. At the close of
the pharmacologic protocol, after resumption of normal A-V conduction, CPB was
removed. Established procedures for closing of the chest were followed.
In one patient, 109, no arrest was achieved, however this is believed to be
because the patient was a left dominant patient, i.e., having the AV node fed from the
left coronary artery rather than the right coronary artery, where the catheter was
placed. Transesophageal echocardiography (TEE) revealed normal left and right
ventricular function, i.e., with no reported global or regional wall motion
abnormalities in each patient in which arrest was achieved.
The results are shown in Table 2 below.
Although the foregoing invention has been described in some detail by way
of illustration and example for purposes of clarity and understanding, it will be
apparent to those skilled in the art that certain changes and modifications may be
practiced. Therefore, the description and examples should not be construed as
limiting the scope of the invention.
WE CLAIM:
1. A composition capable of inducing transient reversible ventricular
asystole in a patient, while maintaining the ability of the heart to be
electrically paced, comprising;
a compound capable of inducing reversible ventricular asystole in a
patient; and
a ß-blocker in an amount sufficient to substantially reduce the amount
of the compound required to induce ventricular asystole in the patient
2. The composition as claimed in claim 1 wherein the compound is an
atrioventricular (AV) node blocker,
3. The composition as claimed in claim 2, wherein the AV node blocker is
present in an amount which is about 50% or less by weight of the
amount of AV node blocker alone required to induce ventricular
asystole.
4. The composition as claimed in claim 1, wherein the compound is a
cholinergic receptor agonist selected from the group consisting of
bethanechol, arecoline, norarecoline, and neostigmine.
5. The composition as claimed in claim 1, wherein the compound is
carbachol
6. The composition as claimed in claim 5, wherein the carbachol is
present in a pharmaceutically acceptable carrier in a dosage form for
administration to a patient.
7. The composition as claimed in claim 5, wherein the carbachol is
present in a pharmaceutically acceptable solution at a dosage amount
of about 1 to 20 mg,
3. The composition as claimed in claim 1, wherein the ß-blocker is
selected from the group consisting of atenolol, acebutolol, labetalol,
metoprolol, nadolol, oxprenolol, penbutoiof, pindolol, sotalol, timolol,
celiprolol, betaxolol, bevantolol, bisoprotol, esmolol, alprenolol,
carterotol, nadolol and teratolol.
9. The composition as claimed in claim 1, wherein the ß-blocker is
propranolol,
10. The composition as claimed in claim 9, wherein the propranolol is
present in a pharmaceutically acceptable carrier in a dosage form for
administration to a patient in an amount of 0.01 to 0.07 mg/kg body
weight of the patient.
11. The composition as claimed in claim 9, wherein the propranolol is
present in a pharmaceutically acceptable solution at a dosage amount
of about 1 to 10 mg.
12. The composition as claimed in claim 1, wherein the compound is
carbachol and the ß-blocker is propranolol.
13. A composition capable of inducing ventricular asystole in a patient,
while maintaining the ability of the heart to be electrically paced,
comprising:
a cholinergic receptor agonist; and
a ß-biocker;
wherein the amount of the cholinergic receptor agonist alone or the b-
blocker alone in the composition is not sufficient to induce ventricular
asystole in the patient.
14. A sterile pharmaceutically acceptable form of carbachol comprising
about 1-20 mg of carbachol in a pharmaceutically acceptable carrier
selected from the group consisting of saline, aqueous dextrose and
water.
15. A pharmaceutically acceptable composition suitable for parenteral
administration to a human patient comprising carbachol and a carrier
selected from the group consisting of dextrose, saline and a buffered
aqueous solution.
16. The composition as claimed in claim 15, wherein the composition is
suitable for administration to the heart.
17. A kit for conducting a surgical procedure comprising:
a first container comprising a dosage amount of a cholinergic receptor
agonist; and
a second container comprising a dosage amount of a ß-blocker.
18. The kit as claimed in claim 17, wherein the cholinergic receptor agonist
is carbachol and the ß-blocker is propranolol.
19. The kit as claimed in claim 18, wherein the first container comprises
carbachol in a pharmaceutically acceptable carrier; and
wherein the second container comprises propranolol in a
pharmaceutically acceptable carrier.
20. The kit as claimed in claim 19, wherein
the first container contains about 1 to 20 mg of carbachol; and
wherein the second container contains about 1 to 10 mg of
propranolol.
21. The kit as claimed in claim 18 further comprising epicardial or
endocardial pacing electrodes.
22. The kit as claimed in claim 18 further comprising a drug delivery
catheter.
23. The kit as claimed in claim 22 wherein said drug delivery catheter
further includes an expandable member, said catheter including a shaft
having a distal portion and said expandable member being disposed
along said distal portion.
24. The kit as claimed in claim 23 wherein said expandable member
comprises a low-pressure balloon.
25. The kit as claimed in claim 17 further comprising a guide catheter.
26. The kit as claimed in claim 17 further comprising a cannula.
27. The kit as claimed in claim 17 further comprising a syringe and needle
assembly.
28. A pacing system comprising:
an extracorporeal pacer for delivering pacing signals to a human heart;
a switch coupled to said pacer;
and an actuator arranged remote from said pacer and coupled to said
switch.
29. The pacing system as claimed in claim 28 including pacing leads
coupled to said switch.
30. The pacing system as claimed in claim 29, wherein said pacing leads
are adapted for coupling to the heart of a patient.
31. The pacing system as claimed In claim 28, wherein said actuator
comprises a foot pedal.
32. The pacing system as claimed in claim 28, wherein said actuator
comprises a needle holder.
33. The pacing system as claimed in claim 28, wherein the switch is
arranged remote from the pacer.
34. The pacing system as claimed in claim 28, wherein the actuator is
arranged remote from the switch.
Methods are provided for conducting surgical procedures in a patient
wherein, during the surgical procedure, autonomous ventricular electrical
conductivity and escape beats are reversibly and transiently suppressed to facilitate
the surgical procedure. Also provided are compositions which are capable of
inducing ventricular asystole in a patient. The compositions may include an AV
node blocker. In one embodiment, compositions including an atrioventricular (AV)
node blocker and a ß-blocker are provided, wherein the ß-blocker is present in an
amount sufficient to substantially reduce the amount of AV node blocker required to
induce ventricular asystole in the patient. The compositions and methods may be
used for inducing temporary ventricular asystole in a beating heart, and to facilitate
the performance of a variety of surgical techniques, including minimally invasive
microsurgical techniques. Methods for performing a surgical procedure on a human
patient are provided wherein a composition capable of inducing transient reversible
ventricular asystole is administered to the heart, for example by intracoronary
injection. The heart then is electrically paced using an electrical pacing system.
thereby to maintain the patient"s blood circulation. The electrical pacing then is
selectively intermittently stopped to allow ventricular asystole to occur, and the steps
of the surgical or therapeutic procedure, such as suturing, are conducted during the
time that the electrical pacing is intermittently stopped. The methods and
compositions advantageously may be used in a range of different surgical procedures
including cardiac, vascular and neurosurgical procedures.

Documents:

1419-cal-1998-granted-abstract.pdf

1419-cal-1998-granted-claims.pdf

1419-cal-1998-granted-correspondence.pdf

1419-cal-1998-granted-description (complete).pdf

1419-cal-1998-granted-drawings.pdf

1419-cal-1998-granted-form 1.pdf

1419-cal-1998-granted-form 18.pdf

1419-cal-1998-granted-form 2.pdf

1419-cal-1998-granted-form 3.pdf

1419-cal-1998-granted-form 5.pdf

1419-cal-1998-granted-letter patent.pdf

1419-cal-1998-granted-pa.pdf

1419-cal-1998-granted-reply to examination report.pdf

1419-cal-1998-granted-specification.pdf

1419-cal-1998-granted-translated copy of priority document.pdf


Patent Number 212584
Indian Patent Application Number 1419/CAL/1998
PG Journal Number 49/2007
Publication Date 07-Dec-2007
Grant Date 04-Dec-2007
Date of Filing 07-Aug-1998
Name of Patentee DUKE UNIVERSITY
Applicant Address ERWIN ROAD, DURHAM, NORTH CAROLINA 27708
Inventors:
# Inventor's Name Inventor's Address
1 FRANCIS G. DUHAYLONGSOD 4218 TROTTER RIDGE ROAD, DURHAM, NORTH CAROLINA 27707
PCT International Classification Number A 61 K 31/27
PCT International Application Number N/A
PCT International Filing date
PCT Conventions:
# PCT Application Number Date of Convention Priority Country
1 60/055,127 1997-08-08 U.S.A.