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Transplantation Biology Research Center, Massachusetts General Hospital and Harvard Medical School, Boston, MA 02129
Donor/recipient MHC class II matching is beneficial to the survival
of allogeneic kidneys in humans and swine. In the latter, tolerance to
class I-disparate grafts can be induced by a short course of
immunosuppression, a peripheral mechanism that implicates regulatory T
cells. Absence of treatment will lead to prompt rejection. Rejected
grafts are infiltrated by dominant alloaggressive T cells, whereas
there is still speculation on the specificity and function of T cells
invading accepted tissues. To characterize the TCR repertoire of
graft-infiltrating T cells (GITC) in accepted kidneys, we have used the
RT-PCR-based spectratyping technique to assess the length polymorphism
of the porcine TCR
chain complementary-determining region 3 (CDR3).
Results show that T cells infiltrating accepted kidneys
(n = 5) express a restricted polymorphism of the
CDR3 length, whereas PBL from the same animal have the polymorphic
distribution of CDR3 lengths found in naive animals; that the skewed
V
repertoire in accepted grafts involved distinct V
subfamilies
in otherwise MHC-identical recipient animals; that GITC clonal
dominance is not caused by immunosuppression because a second kidney,
accepted without drug treatment, exhibits the same TCR V
CDR3
profiles than those detected in the first graft; and that intragraft
clonal dominance intensifies with time, indicating progressive
preeminence of nonaggressive GITC clones. Collectively, these data
represent the first example, in a preclinical model, of the emergence
of nonaggressive intragraft clones, which may be involved in the
induction/maintenance of local tolerance to allogeneic
tissues.
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