Highly altered Vβ repertoire of T cells infiltrating long-term rejected kidney allografts

被引:53
作者
Gagne, K
Brouard, S
Giral, M
Sebille, F
Moreau, A
Guillet, M
Bignon, JD
Imbert, BM
Cuturi, MC
Soulillou, JP
机构
[1] INSERM, U437, F-44093 Nantes 01, France
[2] CHU Nantes, Hotel Dieu, Inst Transplantat & Rech Transplantat, F-44035 Nantes 01, France
[3] Etab Transfus Sanguine, Nantes, France
[4] Harvard Univ, Sch Med, Beth Israel Deaconess Med Ctr, Boston, MA 02215 USA
[5] CHU Nantes, Hotel Dieu, Serv Anatomopathol, F-44035 Nantes 01, France
[6] Inst Biol, Serv Virol, Nantes, France
关键词
D O I
10.4049/jimmunol.164.3.1553
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Chronic rejection represents a major cause of Long-term kidney graft loss. T cells that are predominant in long-term rejected kidney allografts (35 +/- 10% of area infiltrate) may thus be instrumental in this phenomenom, which is likely to be dependant on the indirect pathway of allorecognition only, We have analyzed the variations in T cell repertoire usage of the V beta chain at the complementary determining region 3 (CDR3) level in 18 human kidney grafts lost due to chronic rejection. We observed a strongly biased intragraft TCR V beta usage for the majority of V beta families and also a very high percentage (55%) of V beta families exhibiting common and oligoclonal V beta-C beta rearrangements in the grafts of patients with chronic rejection associated with superimposed histologically acute lesions. Furthermore, V beta 8 and V beta 23 families exhibited common and oligoclonal V beta-J beta rearrangements in 4 of 18 patients (22%). Several CDR3 amino acid sequences were found for the common and oligoclonal V beta 8-J beta 1.4 rearrangement. Quantitative PCR showed that biased V beta transcripts were also overexpressed in chronically rejected kidneys with superimposed acute lesions. In contrast, T lymphocytes infiltrating rejected allografts with chronic rejection only showed an unaltered Gaussian-type CDR3 length distribution. This pattern suggests that late graft failure associated with histological lesions restricted to Banff-defined chronic rejection does not involve T cell-mediated injury. Thus, our observation suggests that a limited number of determinants stimulates the recipient immune system in long-term allograft failure. The possibility of a local response against viral or parenchymatous cell-derived determinants is discussed.
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页码:1553 / 1563
页数:11
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