Cardiac retransplantation is an efficacious therapy for primary cardiac allograft failure

The International Society for Heart Lung Transplantation (ISHLT) estimates that over 65,000 heart transplants have been performed worldwide. With the increasing population of heart transplant patients there is an associated large population of patients suffering from allograft failure resulting from 3 major categories: acute rejection, primary graft failure, and transplant arteriopathy. Several clinical and experimental strategies to treat graft failure have been proposed, but these options have not yet proven to be long-term clinical solutions. Cardiac retransplantation remains the only viable long-term treatment for end-stage cardiac allograft failure.

A few studies have evaluated outcomes following cardiac retransplantation and have demonstrated good results [1‐4]. Unfortunately, the long-term efficacy of heart retransplantation remains unclear with several studies suggesting significantly worse outcomes [5‐8]. Over the past two decades we have accumulated a significant degree of expertise in pre-, intra-, and post-operative management of heart transplant patients at our institution. Our results have been significantly better than the international mean. We undertook this retrospective study with the goal of evaluating cardiac retransplantation outcomes at a high volume center with good results. It is our hope that further evaluation of outcomes will elucidate the viability of orthotopic cardiac retransplantation as therapy for cardiac allograft failure.

As demonstrated in this study, cardiac retransplantation can be safely performed in appropriately selected patients with good outcomes. We have demonstrated long term viability following cardiac retransplantation that approaches that of primary cardiac transplantation. With appropriate patient selection, meticulous intra- and post-operative care, and careful myocardial surveillance cardiac retransplantation is a very effective and viable treatment strategy.

Alternate therapeutic options for cardiac allograft failure are limited as minimal benefits have been demonstrated with percutaneous coronary interventions, coronary artery bypass grafting, valvular repair, plasmapheresis, or medical management [12‐15]. There are several promising experimental strategies, including myocardial regeneration and vasculogenesis that may provide novel and minimally invasive means of salvaging failing, end-stage cardiac allografts [16‐19]. To date, however, these therapies remain experimental and are beyond the current clinical scope. Therefore, the only viable therapy for end-stage heart failure following a cardiac transplant remains cardiac retransplantation. Roughly 2.0% of all heart transplants performed annually are cardiac retransplants[11].

The literature on cardiac retransplantation is ambiguous with several studies reporting divergent findings. Shuhaiber and colleagues in a retrospective review evaluating cardiac retransplants found a higher risk of death after retransplantation when compared to primary allograft failure. Risk factors for cardiac retransplantation were ischemic time, age, and ventilator dependence at the time of transplant, these were similar risk factors for cardiac transplantation[6]. Optimizing these risk factors with appropriate patient selection can significantly improve retransplantation outcomes. Similarly, a smaller study by Schnetzler and colleagues demonstrated 1- and 4-year survivals of 61.5% and 46% respectively. Interestingly, the initial transplant patients in this study had 1 year survival rates close to 70%, a finding that is significantly lower than the 85% international average reported by the ISHLT registry[11]; thereby putting in to question the overall comparability of the data.

A high volume transplant center published a retrospective review of their retransplant experience and reported slightly lower but beneficial short- and long-term results following cardiac retransplantation[8]. This finding was corroborated by both a multi-institutional study and single center experience that found cardiac retransplantation to be a viable option for allograft failure secondary to vasculopathy[1, 3]. Our findings in this study, from a high volume center with extensive heart transplant experience and very good long-term results, further support cardiac retransplantation for allograft failure following a heart transplant. Admittedly this study is limited by the small number of patients and retrospective analysis of the data. Even with this limitation, we have extracted valuable outcomes that support relisting appropriate patients for cardiac retransplantation. A large prospective study is warranted and should be performed, but given the small number of cardiac retransplantations performed internationally a study of this magnitude would take several years to complete.

From a theoretical and immunologic standpoint, retransplantation in a patient with long standing immunosuppression may actually provide the appropriate milieu for diminished rejection, decreased coronary vasculopathy, and longer allograft survival. One of the most controversial post-transplant issues has been the utilization of induction therapy with cytolytic anti-lymphocyte antibodies such as OKT3 and thymoglobulin. Encouragingly, induction therapy has been associated with decreased rates of allograft rejection[20, 21]. But, on the other hand, utilization of anti-lymphocyte antibodies has been associated with 9 fold higher rates of lymphoproliferative disorders, bacterial and viral infections, meningitis, and respiratory distress[22, 23]. Based, on this information one could surmise that a pre-existing immunosuppressed status would potentiate the beneficial decrease in rejection seen with induction therapy while avoiding the negative side effects associated with cytolytic antibodies. If this theory holds true, then retransplantation from a purely immunological standpoint would confer greater long term graft viability.

Along similar lines retransplantation in patients with prolonged initial graft survival, ie. greater than 15 years, will likely have longer retransplant graft function as compared to patients who suffer hyperacute rejection or repeated bouts of rejection and rapid onset allograft dysfunction. Rapid rejection implies a profound immunologic response with less tolerance of allogenic grafts. A large, multi-institutional retrospective study found worse survival in patients undergoing cardiac retransplantation for early graft failure and acute rejection; with survival rates for patients that underwent retransplantation <6 months after initial transplant manifesting worse survival[3]. Therefore, retranplantation performed in a semi-elective setting for transplant arteriopathy will likely confer better results than emergent retransplantation performed for acute rejection. Recipient age does not appear to affect long-term survival[3].

Cardiac retransplantation raises further interesting management questions. For instance, does it matter if we do not resect all of the previous heart? The renal transplant literature suggests that the presence of multiple organs from different donors increases the risk of organ rejection. One can theorize that this situation would hold true for cardiac retransplants with residual tissue from the initial donor as well as a heart from a second donor. Therefore, if a patient has had a biatrial anastomosis at the initial transplant, should all of the initial donor aorta, pulmonary artery, and atria be resected to decrease immunogenicity and rejection associated with the "chimera"? The literature in both clinical and experimental cardiac transplant models thus far fails to answer these issues. These questions exemplify our basic understanding of cardiac retransplantation and the need to expand our knowledge so that we can optimize outcomes.

In conclusion, cardiac retransplantation is an efficacious treatment strategy for cardiac allograft failure with good long-term results.