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移植后肠道内同种异体反应性 T 细胞克隆的可塑性与移植结局相关。

Plasticity of intragraft alloreactive T cell clones in human gut correlates with transplant outcomes.

机构信息

Department of Medicine, Columbia Center for Translational Immunology, Columbia University, New York, NY, USA.

Department of Systems Biology, Center for Computational Biology and Bioinformatics, Columbia University, New York, NY, USA.

出版信息

J Exp Med. 2024 Jan 1;221(1). doi: 10.1084/jem.20230930. Epub 2023 Dec 13.

Abstract

The site of transition between tissue-resident memory (TRM) and circulating phenotypes of T cells is unknown. We integrated clonotype, alloreactivity, and gene expression profiles of graft-repopulating recipient T cells in the intestinal mucosa at the single-cell level after human intestinal transplantation. Host-versus-graft (HvG)-reactive T cells were mainly distributed to TRM, effector T (Teff)/TRM, and T follicular helper compartments. RNA velocity analysis demonstrated a trajectory from TRM to Teff/TRM clusters in association with rejection. By integrating pre- and post-transplantation (Tx) mixed lymphocyte reaction-determined alloreactive repertoires, we observed that pre-existing HvG-reactive T cells that demonstrated tolerance in the circulation were dominated by TRM profiles in quiescent allografts. Putative de novo HvG-reactive clones showed a transcriptional profile skewed to cytotoxic effectors in rejecting grafts. Inferred protein regulon network analysis revealed upstream regulators that accounted for the effector and tolerant T cell states. We demonstrate Teff/TRM interchangeability for individual T cell clones with known (allo)recognition in the human gut, providing novel insight into TRM biology.

摘要

组织驻留记忆 (TRM) 和循环 T 细胞表型之间的转换位点尚不清楚。我们在人肠移植后,在单细胞水平上整合了移植后肠道黏膜中再定植受体 T 细胞的克隆型、同种异体反应性和基因表达谱。宿主对移植物 (HvG) 反应性 T 细胞主要分布于 TRM、效应 T (Teff)/TRM 和 T 滤泡辅助区。RNA 速度分析表明,与排斥反应相关,存在从 TRM 到 Teff/TRM 簇的轨迹。通过整合移植前和移植后 (Tx) 混合淋巴细胞反应确定的同种反应性库,我们观察到在循环中表现出耐受的预先存在的 HvG 反应性 T 细胞在静止的同种异体移植物中主要表现为 TRM 谱。推定的新出现的 HvG 反应性克隆在排斥的移植物中显示出偏向细胞毒性效应器的转录谱。推断的蛋白质调控网络分析揭示了导致效应和耐受 T 细胞状态的上游调节剂。我们证明了个体 T 细胞克隆在人类肠道中具有已知 (同种异体) 识别的 Teff/TRM 可互换性,为 TRM 生物学提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a7e3/10720543/c8942e4a7bb0/JEM_20230930_Fig1.jpg

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