Cell migration and chimerism after whole-organ transplantation: The basis of graft acceptance

Thomas E. Starzl; Anthony J. Demetris; Massimo Trucco; Noriko Murase; Camillo Ricordi; Suzanne T. Ildstad; Hector C. Ramos; Satoru Todo; Andreas Tzakis; John J. Fung; Michael A. Nalesnik; Adriana Zeevi; William A. Rudert; Mirjana Kočova

doi:10.1002/hep.1840170629

Cell migration and chimerism after whole-organ transplantation: The basis of graft acceptance

Thomas E. Starzl(University of Pittsburgh), Anthony J. Demetris(University of Pittsburgh), Massimo Trucco(University of Pittsburgh), Noriko Murase(University of Pittsburgh), Camillo Ricordi(University of Pittsburgh), Suzanne T. Ildstad(University of Pittsburgh), Hector C. Ramos(University of Pittsburgh), Satoru Todo(University of Pittsburgh), Andreas Tzakis(University of Pittsburgh), John J. Fung(University of Pittsburgh), Michael A. Nalesnik(University of Pittsburgh), Adriana Zeevi(University of Pittsburgh), William A. Rudert(University of Pittsburgh), Mirjana Kočova(University of Pittsburgh)

Hepatology

June 1, 1993

10.1002/hep.1840170629

Cited by 810Open Access

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Abstract

Improvements in the prevention or control of rejection of the kidney and liver have been largely interchangeable (1, 2) and then applicable, with very little modification, to thoracic and other organs. However, the mechanism by which anti rejection treatment permits any of these grafts to be "accepted" has been an immunological enigma (3, 4). We have proposed recently that the exchange of migratory leukocytes between the transplant and the recipient with consequent long-term cellular chimerism in both is the basis for acceptance of all whole-organ allografts and xenografts (5). Although such chimerism was demonstrated only a few months ago, the observations have increased our insight into transplantation immunology and have encouraged the development of alternative therapeutic strategies (6).

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