AI Article Synopsis

  • Immune-mediated hemolysis is a significant complication after transplantation, yet mechanisms connecting various cases are often overlooked.
  • The study reviewed three patient cases to highlight different types of immune-mediated red blood cell destruction post-transplantation, illustrating complexities such as autoimmune hemolytic anemia and passenger lymphocyte syndrome.
  • Proper understanding of the causes of posttransplant immune hemolysis is essential for effective management, especially as doctors see more long-term survivors from unrelated bone marrow and peripheral blood transplants.

Article Abstract

Background: Immune-mediated hemolysis is a well-recognized complication of transplantation, but few reports have drawn together the different mechanisms that could be involved.

Study Design And Methods: The clinical and laboratory records of three patients are used to illustrate different types and complexities of posttransplant immune-mediated RBC destruction.

Results: Patient 1 received bone marrow from an HLA-matched, unrelated donor. At 7 months after transplant, his Hb level fell to 50 g per L. The serum contained warm autoantibodies, and the DAT was strongly positive for IgG, IgM, and C3d; an eluate yielded IgG and IgM autoantibodies. Autoimmune hemolytic anemia was diagnosed. Patient 2, blood group A, experienced severe hemolysis 14 days after receiving a lung from a group O donor. The DAT was positive for IgG. Serum and RBC eluate contained anti-A produced by immunocompetent B cells in the transplanted lung-this was the passenger lymphocyte syndrome. Patient 3 experienced posttransplant hemolysis caused by two different immune mechanisms. Originally group A, D- with anti-C, -D, -E, she received a peripheral blood progenitor cell (PBPC) transplant from her HLA-identical group A, D+ son. Six months later, chimerism was evident; the remaining recipient marrow was still producing antibodies that destroyed D+ RBCs made by the transplant. Later, autoimmune hemolytic anemia also developed; the DAT became positive for IgG, and warm autoantibodies were eluted from D- RBCs.

Conclusion: An understanding of the causes and circumstances under which posttransplant immune hemolysis arises is required for proper management. As more patients become long-term survivors of unrelated bone marrow and/or PBPC transplants, chimerism and complex serologic problems will become more common.

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Source
http://dx.doi.org/10.1046/j.1537-2995.2002.00026.xDOI Listing

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