Allogeneic hematopoietic stem cell transplant (allo-HSCT) plays a critical role in the management of acute myeloid leukemia (AML), offering curative potential for patients who have incurable disease with standard forms of chemotherapy. Allo-HSCT incorporates a conditioning regimen of chemotherapy with or without radiation to eradicate residual leukemia and provide recipient immunosuppression. Potent alkylating agents such as busulfan, melphalan, as well as high doses of total-body irradiation (TBI) are highly effective agents against AML, but without marrow rescue with hematopoietic progenitor cells, it can result in prolonged or fatal myelosuppression. Historically, autologous HSCT was studied as a form of consolidation, but improvements over standard consolidation have not been demonstrated.¹ Allogenic transplant requires recipients to be immunosuppressed to limit graft rejection and have additional risks for treatment-related mortality from graft-versus-host disease (GVHD), infection, and primary and secondary graft failure. Nevertheless, allo-HSCT capitalizes on an allogeneic immune effect of graft-versus-leukemia (GVL) that adds synergistically to the cytotoxic effects of the conditioning regimen. Here, we review AML risk stratification, selection of appropriate candidates for allo-HSCT, conditioning regimens, and outcomes of transplantation using matched related or unrelated donors, and alternative donor allo-HSCTs.

The curative potential of allo-HSCT was recognized by early studies showing cures even in a small proportion of refractory patients.² A significant portion of the responses can be attributed to the GVL effect. The earliest implications of this were seen in murine models in which transplanted marrow eliminated leukemia even before cytotoxic irradiation was applied.³ Early studies of sibling donor transplants noted that non–T cell–depleted grafts had improved rates of leukemia relapse.⁴ By the early 1990s retrospective analyses of international transplant registries clearly demonstrated that the presence of acute or chronic GVHD was linked to a reduced risk of relapse.^5,6 Furthermore, the activity of donor lymphocyte infusion (DLI) in treating posttransplant recurrence has further cemented this observation. The concept of “adoptive immunotherapy” was developed by Mathé as he treated a leukemia patient with increasing doses of donor leukocytes.⁷ A syndrome, later recognized to be GVHD, developed, but the patient never relapsed. Susceptibility to the GVL effect may be higher in CML, but still significant in AML.⁸

AML results from clonal proliferation and differentiation blockade of hematopoietic progenitor cells. The resulting cells infiltrate the bone marrow and other tissues and lead to the clinical mani...