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KMID : 0620920110430110630
Experimental & Molecular Medicine
2011 Volume.43 No. 11 p.630 ~ p.637
Higher infiltration by Th17 cells compared with regulatory T cells is associated with severe acute T-cell-mediated graft rejection
Chung Byung-Ha

Oh Hye-Jwa
Piao Shang-Guo
Sun In-O
Kang Seok-Hui
Choi Sun-Ryoung
Park Hoon-Suk
Choi Bum-Soon
Choi Yeong-Jin
Park Cheol-Whee
Kim Yong-Soo
Cho Mi-La
Yang Chul-Woo
Abstract
The aim of this study was to evaluate whether the Th17 and Treg cell infiltration into allograft tissue is associated with the severity of allograft dysfunction and tissue injury in acute T cell-mediated rejection (ATCMR). Seventy-one allograft tissues with biopsy-proven ATCMR were included. The biopsy specimens were immunostained for FOXP3 and IL-17. The allograft function was assessed at biopsy by measuring serum creatinine (Scr) concentration, and by applying the modified diet in renal disease (MDRD) formula, which provides the estimated glomerular filtration rate (eGFR). The severity of allograft tissue injury was assessed by calculating tissue injury scores using the Banff classification. The average numbers of infiltrating Treg and Th17 cells were 11.6 ¡¾ 12.2 cells/mm2 and 5.6 ¡¾ 8.0 cells/mm2, respectively. The average Treg/Th17 ratio was 5.6 ¡¾ 8.2. The Treg/Th17 ratio was significantly associated with allograft function (Scr and MDRD eGFR) and with the severity of interstitial injury and tubular injury (P < 0.05, all parameters). In separate analyses of the number of infiltrating Treg and Th17 cells, Th17 cell infiltration was significantly associated with allograft function and the severity of tissue injury. By contrast, Treg cell infiltration was not significantly associated with allograft dysfunction or the severity of tissue injury. The results of this study show that higher infiltration of Th17 cell compared with Treg cell is significantly associated with the severity of allograft dysfunction and tissue injury.
KEYWORD
FOXP3 protein, human, graft rejection, interleukin-17, Th17 cells, T-lymphocytes, regulatory, transplantation, homologous
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