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Nonmyeloablative haploidentical peripheral blood stem cell transplantation in congenital anemias

$2,829,920ZIAFY2023HLNIH

National Heart, Lung, And Blood Institute

Investigators

Linked publications, trials & patents

Abstract

Based on our murine data, we developed a phase 1 and 2 protocol employing alemtuzumab, 400cGy total body irradiation (TBI), and escalating doses of post-transplant cyclophosphamide (PT-Cy) ranging from 0mg/kg in cohort 1, 50mg/kg in cohort 2, and 100mg/kg in cohort 3. A total of 21 patients with sickle cell disease and 2 patients with beta-thalassemia were transplanted and had baseline complications, including cirrhosis, pulmonary hypertension, heart failure, and end-stage renal disease. The engraftment rate improved from 1/3 (33%) in the first cohort to 5/8 (63%) in the second cohort to 10/12 (83%) in the third cohort. The percentage of donor myeloid and CD3 chimerism also improved with subsequent cohorts. With median follow-up exceeding 8 years, the overall survival is 57.1%; 6 died after the return of their sickle cell disease, and 3 following repeat transplant for sickle cell disease. There was no mortality before 100 days post-transplant. At present, 0% in the first cohort, 12.5% in the second cohort, and 33% in the third cohort remain free of their disease. There was no Grade 2-4 acute or moderate to severe chronic graft-versus-host disease (GVHD). Therefore, we have shown that PT-Cy improves engraftment in patients with SCD who are at high risk for early mortality. 3 patients were re-transplanted with myeloablative conditioning and the same donor, and 2 are alive and free of sickle cell disease. As we reached the stopping rules for the study, we opened a new protocol that added additional immunosuppression in an attempt to improve the success rate while maintaining a low risk of GVHD. Since June 2017, 22 patients have been transplanted. 21 patients achieved high donor chimerism levels. One patient with a history of stroke and chronic thromboembolic pulmonary hypertension on anticoagulation died 60 days after her second transplant. Two patients developed refractory Evans syndrome followed by an unexpected severe hyperinflammatory reaction that led to multi-organ failure in both patients, fatal in both. One patient died from neurotoxicity related to Epstein-Barr Virus-associated post-transplant lymphoproliferative disorder (PTLD). Two patients developed acute GVHD, one Grade 2 and one Grade 4. One patient rejected his graft and required infusion of his backup autologous cells. Two patients with slowly falling donor myeloid chimerism levels experienced the return of their sickle cell disease at 2.5 years post-transplant. Five patients developed PTLD, 2 uncontrolled. Four patients developed autoimmune complications, 2 uncontrolled. Because of the high incidence of unexpected complications, the protocol has recently halted accrual. We have recently submitted a new haploidentical protocol for scientific review. The protocol will enroll patients with severe SCD, including those with compromised organ function. The protocol will include nongenotoxic conditioning with an anti-c-Kit antibody with the goal of maximizing donor chimerism levels long-term while minimizing toxicity. Our clonal hematopoiesis protocol in patients with sickle cell disease and deep phenotyping of major organs in patients with sickle cell disease are enrolling patients to help us identify clinical and genetic risk factors of heart, lung, and kidney disease and myeloid malignancy development after curative therapies for sickle cell disease. We have published one manuscript that described a high incidence of hematologic malignancies after unsuccessful curative therapies and mixed chimerism for sickle cell disease. We also recently reported that cardiac morphology improves in patients with sickle cell disease who underwent nonmyeloablative HLA-matched sibling transplant at one of three sites at 2 years post-transplant.

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