Orthotopic Heart Transplantation

Orthotopic heart transplantation is carried out via a median sternotomy, and the general approach is similar to that used for coronary revascularization or valve replacement. Frequently, patients will have undergone a prior median sternotomy; repeat sternotomy is cautiously performed using an oscillating saw. The groin should be prepped and draped to provide a rapid route for cannulation for cardiopulmonary bypass (CPB) if necessary. After the pericardium is opened, the aorta is cannulated as distally as possible and the IVC and SVC are individually cannulated via the high right atrium. Manipulation of the heart before institution of CPB is limited if thrombus is detected in the heart with transesophageal echocardiography (TEE). After initiation of CPB and cross-clamping of the aorta, the heart is arrested and excised ( Fig. 19.1 ). The aorta and PA are separated and divided just above the level of their respective valves, and the atria are transected at their grooves. A variant of this classic approach totally excises both atria, mandating bicaval anastomoses. This technique may reduce the incidence of atrial arrhythmias, better preserve atrial function by avoiding tricuspid regurgitation, and enhance cardiac output (CO) after transplantation.

Mediastinum after excision of the heart but before allograft placement. Venous cannulas are present in the superior (SVC) and inferior vena cava (IVC) , and the arterial cannula is present in the ascending aorta. (A) Classic orthotopic technique. (B) Bicaval anastomotic technique.

The donor graft then is implanted with every effort to maintain a cold tissue temperature, beginning with the left atrial (LA) anastomosis. If the foramen ovale is patent, it is sutured closed. The donor right atrium is opened by incising it from the IVC to the base of the right atrial (RA) appendage (to preserve the donor sinoatrial node), and the RA anastomosis is constructed. Alternatively, if the bicaval technique is used, individual IVC and SVC anastomoses are sewn. The donor and recipient PAs are then brought together in an end-to-end manner, followed by the anastomosis of the donor to the recipient aorta. After removal of the aortic cross-clamp, the heart is de-aired via a vent in the ascending aorta. Just before weaning from CPB, one of the venous cannulae is withdrawn into the right atrium and the other removed. The patient is then weaned from CPB in the usual manner. After hemostasis is achieved, mediastinal tubes are placed for drainage, the pericardium is left open, and the wound is closed in the standard fashion.

Heterotopic Heart Transplantation

Although orthotopic placement of the cardiac graft is optimal for most patients, certain recipients are not candidates for the orthotopic operation, and instead the graft is placed in the right chest and connected to the circulation in parallel with the recipient heart. The two primary indications for heterotopic placement are significant irreversible pulmonary hypertension and gross size mismatch between the donor and recipient. Heterotopic placement may avoid the development of acute right ventricular (RV) failure in the unconditioned donor heart in the face of acutely increased RV afterload.

Donor harvesting for heterotopic placement is performed in the previously described manner, except that the azygos vein is ligated and divided to increase the length of the donor SVC; the PA is extensively dissected to provide the longest possible main and right PA; and the donor IVC and right pulmonary veins are oversewn, with the left pulmonary veins incised to create a single large orifice. The operation is performed via a median sternotomy in the recipient, but the right pleura is entered and excised. The recipient SVC is cannulated via the RA appendage, and the IVC via the lower right atrium. After arresting the recipient heart, the LA anastomosis is constructed by incising the recipient left atrium near the right superior pulmonary vein and extending this incision inferiorly and then anastomosing the respective left atria. The recipient RA-SVC is then incised and anastomosed to the donor RA-SVC, after which the donor aorta is joined to the recipient aorta in an end-to-side manner. Finally, the donor PA is anastomosed to the recipient main PA in an end-to-side manner if it is sufficiently long; otherwise, they are joined via an interposed vascular graft ( Fig. 19.2 ).

Placement of heterotopic graft in the right chest, with anastomoses to the corresponding native left (LA) and right atria (RA), ascending aorta (AO), and an interposition graft to the native pulmonary artery (PA) . LV, left ventricle; RV, right ventricle; SVC, superior vena cava.

(From Cooper DKC, Lanza LP. Heart Transplantation: The Present Status of Orthotopic and Heterotopic Heart Transplantation . Lancaster, United Kingdom: MTP Press; 1984.)

Special Situations

Mechanical ventricular assist devices have been used successfully to bridge patients who would otherwise die of acute heart failure awaiting transplantation. Although ventricular assist devices may improve the survival of patients awaiting transplantation, complications associated with their use may negatively impact survival after transplantation. The technique of transplantation is virtually identical in such patients to that for ordinary orthotopic transplantation. However, repeat sternotomy is obligatory, and repeat sternotomy is associated with higher morbidity and mortality, as well as higher intraoperative blood use, postoperative length of intensive care unit (ICU) and hospital stays, and frequency of reoperation for bleeding after subsequent heart transplantation.

Rarely, patients will present for cardiac transplantation combined with transplantation of the liver. The cardiac allograft usually is implanted first to better enable the patient to survive potential hemodynamic instability associated with reperfusion of the hepatic allograft. Large-bore intravenous access is mandatory. Conventional full heparinization protocols or low-dose heparin with heparin-bonded circuits may be used. A venous cannula can be left in the right atrium at the completion of the heart transplant procedure to serve as a return site for subsequent venovenous bypass during liver transplantation.

Preoperative Evaluation and Preparation

The preoperative period often is marked by severe time constraints because of the impending arrival of the donor heart. Nevertheless, a rapid history should screen for last oral intake, recent anticoagulant use, intercurrent deterioration of ventricular function, or change in anginal pattern; a physical examination should evaluate present volume status, and a laboratory review (if available) and a chest radiograph should detect the presence of renal, hepatic, or pulmonary dysfunction. Many hospitalized patients will be supported with inotropic infusions and/or an intraaortic balloon pump, and the infusion rates and timing of the latter should be reviewed.

Equipment and drugs similar to those usually used for routine cases requiring CPB should be prepared. A β-agonist such as epinephrine should be readily available both in bolus form and as an infusion to treat ventricular failure rapidly, and an α-agonist such as phenylephrine or norepinephrine is useful to compensate for the vasodilatory effects of anesthetics because even small decreases in preload and afterload can lead to catastrophic changes in CO and coronary perfusion in these patients.

Placement of invasive monitoring before induction will facilitate rapid and accurate response to hemodynamic events during induction. In addition to standard noninvasive monitoring, an arterial catheter and a PA catheter (PAC, with a long sterile sheath to allow partial removal during graft implantation) are placed after judicious use of sedation and local anesthetics. Placing the PAC in a central site rather than the radial artery will avoid the discrepancy between radial and central arterial pressure often seen after CPB, but it also may be necessary to cannulate a femoral artery for arterial inflow for CPB if there has been a prior sternotomy. Floating the PAC into correct position may be difficult because of cardiac chamber dilation and severe tricuspid regurgitation. Large-bore intravenous access is mandatory, especially if a sternotomy has been previously performed, in which case external defibrillator/pacing patches also may be useful. The overall hemodynamic picture should be evaluated and optimized insofar as possible just before induction. If the hemodynamics seem tenuous, then starting or increasing an inotrope infusion may be advisable.

Induction

Most patients presenting for heart transplantation will not be in a fasting state and should be considered to have a full stomach. Therefore the induction technique should aim to rapidly achieve control of the airway to prevent aspiration while avoiding myocardial depression. A regimen combining a short-acting hypnotic with minimal myocardial depression (etomidate, 0.3 mg/kg), a moderate dose of narcotic to blunt the tachycardic response to laryngoscopy and intubation (fentanyl, 10 µg/kg), and succinylcholine (1.5 mg/kg) is popular; high-dose narcotic techniques with or without benzodiazepines also have been advocated. Vasodilation should be countered with an α-agonist. Anesthesia can be maintained with additional narcotic and sedatives (benzodiazepines or scopolamine).

Intraoperative Management

After induction, the stomach can be decompressed with an orogastric tube and a TEE probe introduced while the bladder is catheterized. A complete TEE examination often will reveal useful information not immediately available from other sources, such as the presence of cardiac thrombi, ventricular volume and contractility, and atherosclerosis of the ascending aorta and aortic arch. Crossmatched blood should be immediately available once surgery commences, especially if the patient has had a previous sternotomy; patients not previously exposed to cytomegalovirus should receive blood from donors who are likewise cytomegalovirus negative. Sternotomy and cannulation for CPB are performed as indicated earlier. The period before CPB often is uneventful, apart from arrhythmias and slow recovery of coronary perfusion because of manipulation of the heart during dissection and cannulation. The PAC should be withdrawn from the right heart before completion of bicaval cannulation.

Once CPB is initiated, ventilation is discontinued and the absence of a thrill in the carotid arteries is documented. Most patients will have an excess of intravascular volume, and administration of a diuretic and/or the use of hemofiltration via the pump may be beneficial by increasing the hemoglobin concentration. A dose of glucocorticoid (methylprednisolone, 500 mg) is administered as the last anastomosis is being completed before release of the aortic cross-clamp to attenuate any hyperacute immune response. During the period of reperfusion, an infusion of an inotrope is begun for both inotropy and chronotropy. TEE is used to monitor whether the cardiac chambers are adequately de-aired before weaning from CPB.

Weaning from bypass begins after ventilation is resumed and the cannula in the SVC is removed. The donor heart should be paced if bradycardia is present despite the inotropic infusion. Once the patient is separated from CPB, the PAC can be advanced into position. Patients with increased PVR are at risk for acute RV failure and may benefit from a pulmonary vasodilator such as prostaglandin E ₁ (0.05–0.15 µg/kg/min). Rarely, such patients will require support with a RV assist device. TEE often will provide additional useful information about right- and left-heart function and volume, and document normal flow dynamics through the anastomoses. Unless a bicaval anastomosis was created, a ridge of redundant tissue will be evident in the left atrium and should not cause alarm.

Protamine then is given to reverse the effect of heparin after satisfactory weaning from CPB. Continued coagulopathy despite adequate protamine is common after heart transplantation, especially if there has been a prior sternotomy. Treatment is similar to that used for other postbypass coagulopathies: meticulous attention to surgical hemostasis, empiric administration of platelets, and subsequent addition of fresh-frozen plasma and cryoprecipitate guided by subsequent coagulation studies. After adequate hemostasis is achieved, the wound is closed in standard fashion and the patient transported to the ICU.

Postoperative Management and Complications

Management in the ICU after the conclusion of the procedure essentially is a continuation of the anesthetic management after CPB. The electrocardiogram; arterial, central venous, and/or PA pressures; and arterial oxygen saturation are monitored continuously. Cardiac recipients will continue to require β-adrenergic infusions for chronotropy and inotropy for up to 3 to 4 days. Vasodilators may be necessary to control arterial hypertension and decrease impedance to LV ejection. Patients can be weaned from ventilatory support and extubated when the hemodynamics are stable and hemorrhage has ceased. The immunosuppressive regimen of choice (typically consisting of cyclosporine, azathioprine, and prednisone, or tacrolimus and prednisone) should be started after arrival in the ICU. Invasive monitoring can be withdrawn as the inotropic support is weaned, and mediastinal tubes removed after drainage subsides (usually after 24 hours). Patients usually can be discharged from the ICU after 2 or 3 days.

Early complications after heart transplantation include acute and hyperacute rejection, cardiac failure, systemic and pulmonary hypertension, cardiac arrhythmias, renal failure, and infection. Hyperacute rejection is an extremely rare but devastating syndrome mediated by preformed recipient cytotoxic antibodies against donor heart antigens. The donor heart immediately becomes cyanotic from microvascular thrombosis and ultimately ceases to contract. This syndrome is lethal unless the patient can be supported mechanically until a suitable heart is found. Acute rejection is a constant threat in the early postoperative period and may present in many forms (eg, low CO, arrhythmias). Acute rejection occurs most frequently during the initial 6 months after transplantation, so its presence is monitored by serial endomyocardial biopsies, with additional biopsies to evaluate any acute changes in clinical status. Detection of rejection mandates an aggressive increase in the level of immunosuppression, usually including pulses of glucocorticoid or a change from cyclosporine to tacrolimus. Low CO after transplantation may reflect a number of causative factors: hypovolemia, inadequate adrenergic stimulation, myocardial injury during harvesting, acute rejection, tamponade, or sepsis. Therapy should be guided by invasive monitoring, TEE, and endomyocardial biopsy. Systemic hypertension may be caused by pain, so adequate analgesia should be obtained before treating blood pressure with a vasodilator. Because fixed pulmonary hypertension will have been excluded during the recipient evaluation, pulmonary hypertension after heart transplantation usually will be transient and responsive to vasodilators such as prostaglandin E ₁ , nitrates, or hydralazine after either orthotopic or heterotopic placement. Atrial and ventricular tachyarrhythmias are common after heart transplantation; once rejection has been ruled out as a cause, antiarrhythmics are used for conversion or control (except those acting via indirect mechanisms such as digoxin, or those with negative inotropic properties such as β-blockers and calcium channel blockers). Almost all recipients will require either β-adrenergic agonists or pacing to increase heart rate in the immediate perioperative period, but 10% to 25% of recipients also will require permanent pacing. Renal function often improves immediately after transplantation, but immunosuppressives such as cyclosporine and tacrolimus may impair renal function. Finally, infection is a constant threat to immunosuppressed recipients. Bacterial pneumonia is frequent early in the postoperative period, with opportunistic viral and fungal infections becoming more common after the first several weeks.

Orthotopic Heart Transplantation

Orthotopic heart transplantation is carried out via a median sternotomy, and the general approach is similar to that used for coronary revascularization or valve replacement. Frequently, patients will have undergone a prior median sternotomy; repeat sternotomy is cautiously performed using an oscillating saw. The groin should be prepped and draped to provide a rapid route for cannulation for cardiopulmonary bypass (CPB) if necessary. After the pericardium is opened, the aorta is cannulated as distally as possible and the IVC and SVC are individually cannulated via the high right atrium. Manipulation of the heart before institution of CPB is limited if thrombus is detected in the heart with transesophageal echocardiography (TEE). After initiation of CPB and cross-clamping of the aorta, the heart is arrested and excised ( Fig. 19.1 ). The aorta and PA are separated and divided just above the level of their respective valves, and the atria are transected at their grooves. A variant of this classic approach totally excises both atria, mandating bicaval anastomoses. This technique may reduce the incidence of atrial arrhythmias, better preserve atrial function by avoiding tricuspid regurgitation, and enhance cardiac output (CO) after transplantation.

Mediastinum after excision of the heart but before allograft placement. Venous cannulas are present in the superior (SVC) and inferior vena cava (IVC) , and the arterial cannula is present in the ascending aorta. (A) Classic orthotopic technique. (B) Bicaval anastomotic technique.

The donor graft then is implanted with every effort to maintain a cold tissue temperature, beginning with the left atrial (LA) anastomosis. If the foramen ovale is patent, it is sutured closed. The donor right atrium is opened by incising it from the IVC to the base of the right atrial (RA) appendage (to preserve the donor sinoatrial node), and the RA anastomosis is constructed. Alternatively, if the bicaval technique is used, individual IVC and SVC anastomoses are sewn. The donor and recipient PAs are then brought together in an end-to-end manner, followed by the anastomosis of the donor to the recipient aorta. After removal of the aortic cross-clamp, the heart is de-aired via a vent in the ascending aorta. Just before weaning from CPB, one of the venous cannulae is withdrawn into the right atrium and the other removed. The patient is then weaned from CPB in the usual manner. After hemostasis is achieved, mediastinal tubes are placed for drainage, the pericardium is left open, and the wound is closed in the standard fashion.

Heterotopic Heart Transplantation

Although orthotopic placement of the cardiac graft is optimal for most patients, certain recipients are not candidates for the orthotopic operation, and instead the graft is placed in the right chest and connected to the circulation in parallel with the recipient heart. The two primary indications for heterotopic placement are significant irreversible pulmonary hypertension and gross size mismatch between the donor and recipient. Heterotopic placement may avoid the development of acute right ventricular (RV) failure in the unconditioned donor heart in the face of acutely increased RV afterload.

Donor harvesting for heterotopic placement is performed in the previously described manner, except that the azygos vein is ligated and divided to increase the length of the donor SVC; the PA is extensively dissected to provide the longest possible main and right PA; and the donor IVC and right pulmonary veins are oversewn, with the left pulmonary veins incised to create a single large orifice. The operation is performed via a median sternotomy in the recipient, but the right pleura is entered and excised. The recipient SVC is cannulated via the RA appendage, and the IVC via the lower right atrium. After arresting the recipient heart, the LA anastomosis is constructed by incising the recipient left atrium near the right superior pulmonary vein and extending this incision inferiorly and then anastomosing the respective left atria. The recipient RA-SVC is then incised and anastomosed to the donor RA-SVC, after which the donor aorta is joined to the recipient aorta in an end-to-side manner. Finally, the donor PA is anastomosed to the recipient main PA in an end-to-side manner if it is sufficiently long; otherwise, they are joined via an interposed vascular graft ( Fig. 19.2 ).

Placement of heterotopic graft in the right chest, with anastomoses to the corresponding native left (LA) and right atria (RA), ascending aorta (AO), and an interposition graft to the native pulmonary artery (PA) . LV, left ventricle; RV, right ventricle; SVC, superior vena cava.

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