MAdCAM-1 co-stimulation combined with retinoic acid and TGF-β induces blood CD8+ T cells to adopt a gut CD101+ TRM phenotype

IF 7.9 2区 医学 Q1 IMMUNOLOGY
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引用次数: 0

Abstract

Resident memory T cells (TRMs) help control local immune homeostasis and contribute to tissue-protective immune responses. The local cues that guide their differentiation and localization are poorly defined. We demonstrate that mucosal vascular addressin cell adhesion molecule 1, a ligand for the gut-homing receptor α4β7 integrin, in the presence of retinoic acid and transforming growth factor-β (TGF-β) provides a co-stimulatory signal that induces blood cluster of differentiation (CD8+ T cells to adopt a TRM-like phenotype. These cells express CD103 (integrin αE) and CD69, the two major TRM cell-surface markers, along with CD101. They also express C-C motif chemokine receptors 5 (CCR5) , C-C motif chemokine receptors 9 (CCR9), and α4β7, three receptors associated with gut homing. A subset also expresses E-cadherin, a ligand for αEβ7. Fluorescent lifetime imaging indicated an αEβ7 and E-cadherin cis interaction on the plasma membrane. This report advances our understanding of the signals that drive the differentiation of CD8+ T cells into resident memory T cells and provides a means to expand these cells in vitro, thereby affording an avenue to generate more effective tissue-specific immunotherapies.

MAdCAM-1 与维甲酸和 TGF-β 共同刺激可诱导血液 CD8+ T 细胞形成肠道 CD101+ TRM 表型。
驻留记忆 T 细胞(TRMs)有助于控制局部免疫平衡,并促进组织保护性免疫反应。指导其分化和定位的局部线索尚未明确。我们证明,MAdCAM-1(肠道归巢受体α4β7整合素的配体)在视黄酸和 TGF-β 的存在下提供了一种成本刺激信号,诱导血液 CD8+ T 细胞采用类似 TRM 的表型。这些细胞表达 CD103(整合素 αE)和 CD69,这是两个主要的 TRM 细胞表面标志物,同时还表达 CD101。它们还表达 CCR5、CCR9 和 α4β7 这三种与肠道归巢相关的受体。其中一部分还表达 E-cadherin,这是 αEβ7 的配体。荧光寿命成像显示,αEβ7 和 E-cadherin 在质膜上存在顺式相互作用。该报告加深了我们对驱动 CD8+ T 细胞分化为 TRMs 的信号的理解,并提供了体外扩增这些细胞的方法,从而为产生更有效的组织特异性免疫疗法提供了途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Mucosal Immunology
Mucosal Immunology 医学-免疫学
CiteScore
16.60
自引率
3.80%
发文量
100
审稿时长
12 days
期刊介绍: Mucosal Immunology, the official publication of the Society of Mucosal Immunology (SMI), serves as a forum for both basic and clinical scientists to discuss immunity and inflammation involving mucosal tissues. It covers gastrointestinal, pulmonary, nasopharyngeal, oral, ocular, and genitourinary immunology through original research articles, scholarly reviews, commentaries, editorials, and letters. The journal gives equal consideration to basic, translational, and clinical studies and also serves as a primary communication channel for the SMI governing board and its members, featuring society news, meeting announcements, policy discussions, and job/training opportunities advertisements.
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