Thymic Function after Hematopoietic Stem-Cell Transplantation for the Treatment of Severe Combined Immunodeficiency

doi:10.1056/NEJM200005043421804

Volume 342:1325-1332		May 4, 2000		Number 18

Thymic Function after Hematopoietic Stem-Cell Transplantation for the Treatment of Severe Combined Immunodeficiency

Dhavalkumar D. Patel, M.D., Ph.D., Maria E. Gooding, B.A., Roberta E. Parrott, B.S., Kimberly M. Curtis, B.S., Barton F. Haynes, M.D., and Rebecca H. Buckley, M.D.

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ABSTRACT

Background Immune function can be restored in infants with severecombined immunodeficiency by transplantation of unfractionatedbone marrow from HLA-identical donors or T-cell–depletedmarrow stem cells from haploidentical donors, with whom thereis a single haplotype mismatch, without the need for chemotherapybefore transplantation or prophylaxis against graft-versus-hostdisease. The role of the thymus in this process is unknown.

Methods We analyzed the phenotypes of circulating T cells andthe proliferative responses of peripheral-blood mononuclearcells to phytohemagglutinin in 83 patients with severe combinedimmunodeficiency who received allogeneic marrow transplantswithout T-cell ablation from related donors over an 18-yearperiod. We also tested for the presence of episomes of T-cellantigen receptors (extrachromosomal DNA circles formed duringintrathymic T-cell development) to assess thymus-dependent T-cellreconstitution.

Results Before and early after transplantation, the numbersof circulating T cells were low, with a predominance of matureCD45RO+ T cells (primarily resulting from the transplacentaltransfer of maternal cells); T-cell antigen-receptor episomeswere undetectable in peripheral-blood mononuclear cells. In73 of the infants, thymus-derived T cells expressing CD45RAand T-cell antigen-receptor episomes were detected within threeto six weeks after transplantation. The mean (±SD) valuefor thymus-dependent T-cell antigen-receptor episomes peaked(at 7311±8652 per microgram of peripheral-blood mononuclear-cellDNA) 1 to 2 years after transplantation and declined to lowlevels (less than 100 episomes per microgram of DNA) within14 years, as compared with a gradual decline from birth to theage of about 80 years in normal subjects.

Conclusions The vestigial thymus in infants with severe combinedimmunodeficiency is functional and can produce enough T cellsafter bone marrow transplantation to provide normal immune function.

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From the Departments of Medicine (D.D.P., M.E.G., B.F.H.), Immunology (D.D.P., B.F.H., R.H.B.), and Pediatrics (R.E.P., K.M.C., R.H.B.) and the Human Vaccine Institute (D.D.P., B.F.H.), Duke University Medical Center, Durham, N.C.

Address reprint requests to Dr. Patel at Box 3258, Duke University Medical Center, Durham, NC 27710, or at patel003{at}mc.duke.edu.

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