1. Phenotype and molecular signature of CD8+ T cell subsets in T cell- mediated rejections after kidney transplantation.
- Author
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Ko, Eun Jeong, Seo, Jung-Woo, Kim, Kyoung Woon, Kim, Bo-Mi, Cho, Jang-Hee, Kim, Chan-Duck, Seok, Junhee, Yang, Chul Woo, Lee, Sang-Ho, and Chung, Byung Ha
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KIDNEY transplantation ,PHENOTYPES ,GENE expression - Abstract
We investigated the phenotype and molecular signatures of CD8
+ T cell subsets in kidney-transplant recipients (KTRs) with biopsy-proven T cell-mediated rejection (TCMR). We included 121 KTRs and divided them into three groups according to the pathologic or clinical diagnosis: Normal biopsy control (NC)(n = 32), TCMR (n = 50), and long-term graft survival (LTGS)(n = 39). We used flowcytometry and microarray to analyze the phenotype and molecular signatures of CD8+ T cell subsets using peripheral blood from those patients and analyzed significant gene expressions according to CD8+ T cell subsets. We investigated whether the analysis of CD8+ T cell subsets is useful for predicting the development of TCMR. CCR7+ CD8+ T cells significantly decreased, but CD28null CD57+ CD8+ T cells and CCR7- CD45RA+ CD8+ T cells showed an increase in the TCMR group compared to other groups (p<0.05 for each); hence CCR7+ CD8+ T cells showed significant negative correlations to both effector CD8+ T cells. We identified genes significantly associated with the change of CCR7+ CD8+ T, CCR7- CD45RA+ CD8+ T, and CD28null CD57+ CD8+ T cells in an ex vivo study and found that most of them were included in the significant genes on in vitro CCR7+ CD8+ T cells. Finally, the decrease of CCR7+ CD8+ T cells relative to CD28null CD57+ T or CCR7- CD45RA+ CD8+ T cells can predict TCMR significantly in the whole clinical cohort. In conclusion, phenotype and molecular signature of CD8+ T subsets showed a significant relationship to the development of TCMR; hence monitoring of CD8+ T cell subsets may be a useful for predicting TCMR in KTRs. [ABSTRACT FROM AUTHOR]- Published
- 2020
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