Peptide Sharing Between CMV and Mismatched HLA Class I Peptides Promotes Early T-Cell-Mediated Rejection After Kidney Transplantation

IF 5.9 4区 医学 Q2 CELL BIOLOGY
HLA Pub Date : 2024-10-22 DOI:10.1111/tan.15719
Emma T. M. Peereboom, Renato de Marco, Kirsten Geneugelijk, Jasvir Jairam, Frans M. Verduyn Lunel, Anna J. Blok, José Medina-Pestana, Maria Gerbase-DeLima, Arjan D. van Zuilen, Eric Spierings
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Abstract

Cytomegalovirus (CMV) infection is related to acute rejection and graft loss after kidney transplantation, though the underlying mechanism remains largely unknown. Some CMV strains produce a peptide that is identical to a peptide sequence found in the leader peptide of specific HLA-A and -C alleles. In this retrospective study of 351 kidney transplantations, we explored whether CMV-seropositive recipients without the VMAPRTLIL, VMAPRTLLL or VMAPRTLVL HLA class I leader peptide receiving a transplant from a donor with this peptide, faced an increased risk of T-cell-mediated rejection (TCMR) in the first 90 days after transplantation. An independent case–control cohort was used for validation (n = 122). The combination of recipient CMV seropositivity with the VMAPRTLIL peptide mismatch was associated with TCMR with a hazard ratio (HR) of 3.06 (p = 0.001) in a multivariable analysis. Similarly, the VMAPRTLLL peptide mismatch was associated with TCMR revealing a HR of 2.61 (p = 0.008). Transplantations featuring either a VMAPRTLIL or a VMAPRTLLL peptide mismatch had a significantly higher cumulative TCMR incidence (p < 0.0001), with the primary impact observed in the first 2 weeks post-transplantation. The findings could be validated in an independent cohort. Together, our data strongly suggest that CMV-positive recipients without an HLA peptide identical to a CMV peptide yet transplanted with a donor who does possess this peptide, have a significantly increased risk of early TCMR. Considering the prevention of such an leader peptide mismatch in these patients or adjusting immunosuppression protocols accordingly may hold promise in reducing the incidence of early TCMR.

Abstract Image

CMV与不匹配的HLA I类肽之间的肽共享会促进肾移植后T细胞介导的早期排斥反应。
巨细胞病毒(CMV)感染与肾移植后的急性排斥反应和移植物损失有关,但其根本机制仍不清楚。一些 CMV 株系会产生一种肽,这种肽与特定 HLA-A 和 -C 等位基因领导肽中的肽序列相同。在这项对 351 例肾移植进行的回顾性研究中,我们探讨了没有 VMAPRTLIL、VMAPRTLLL 或 VMAPRTLVL HLA I 类头端肽的 CMV 血清阳性受者在接受带有该肽的供体的移植后,在移植后的前 90 天内发生 T 细胞介导的排斥反应(TCMR)的风险是否会增加。一个独立的病例对照队列被用于验证(n = 122)。受体CMV血清阳性与VMAPRTLIL肽错配的组合与TCMR相关,多变量分析的危险比(HR)为3.06(P = 0.001)。同样,VMAPRTLLL 肽错配也与 TCMR 有关,其危险比为 2.61(p = 0.008)。具有 VMAPRTLIL 或 VMAPRTLLL 肽错配的移植,其累积 TCMR 发生率显著较高(p=0.008)。
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来源期刊
HLA
HLA Immunology and Microbiology-Immunology
CiteScore
3.00
自引率
28.80%
发文量
368
期刊介绍: HLA, the journal, publishes articles on various aspects of immunogenetics. These include the immunogenetics of cell surface antigens, the ontogeny and phylogeny of the immune system, the immunogenetics of cell interactions, the functional aspects of cell surface molecules and their natural ligands, and the role of tissue antigens in immune reactions. Additionally, the journal covers experimental and clinical transplantation, the relationships between normal tissue antigens and tumor-associated antigens, the genetic control of immune response and disease susceptibility, and the biochemistry and molecular biology of alloantigens and leukocyte differentiation. Manuscripts on molecules expressed on lymphoid cells, myeloid cells, platelets, and non-lineage-restricted antigens are welcomed. Lastly, the journal focuses on the immunogenetics of histocompatibility antigens in both humans and experimental animals, including their tissue distribution, regulation, and expression in normal and malignant cells, as well as the use of antigens as markers for disease.
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