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白细胞介素 4 诱导基因 1:负性免疫检查点控制 B 细胞分化和激活。

IL-4-Induced Gene 1: A Negative Immune Checkpoint Controlling B Cell Differentiation and Activation.

机构信息

INSERM, U1016, Institut Cochin, 75014 Paris, France.

CNRS, UMR8104, 75014 Paris, France.

出版信息

J Immunol. 2018 Feb 1;200(3):1027-1038. doi: 10.4049/jimmunol.1601609. Epub 2017 Dec 29.

Abstract

Emerging data highlight the crucial role of enzymes involved in amino acid metabolism in immune cell biology. IL-4-induced gene-1 (IL4I1), a secreted l-phenylalanine oxidase expressed by APCs, has been detected in B cells, yet its immunoregulatory role has only been explored on T cells. In this study, we show that IL4I1 regulates multiple steps in B cell physiology. Indeed, IL4I1 knockout mice exhibit an accelerated B cell egress from the bone marrow, resulting in the accumulation of peripheral follicular B cells. They also present a higher serum level of natural Igs and self-reactive Abs. We also demonstrate that IL4I1 produced by B cells themselves controls the germinal center reaction, plasma cell differentiation, and specific Ab production in response to T dependent Ags, SRBC, and NP-KLH. In vitro, IL4I1-deficient B cells proliferate more efficiently than their wild-type counterparts in response to BCR cross-linking. Moreover, the absence of IL4I1 increases activation of the Syk-Akt-S6kinase signaling pathway and calcium mobilization, and inhibits SHP-1 activity upon BCR engagement, thus supporting that IL4I1 negatively controls BCR-dependent activation. Overall, our study reveals a new perspective on IL4I1 as a key regulator of B cell biology.

摘要

新兴数据强调了参与氨基酸代谢的酶在免疫细胞生物学中的关键作用。IL-4 诱导基因-1(IL4I1)是一种由 APC 表达的分泌型 l-苯丙氨酸氧化酶,已在 B 细胞中检测到,但它在 T 细胞上的免疫调节作用仅被探索过。在这项研究中,我们表明 IL4I1 调节 B 细胞生理学的多个步骤。事实上,IL4I1 敲除小鼠表现出 B 细胞从骨髓中更快地流出,导致外周滤泡 B 细胞的积累。它们还表现出更高的血清天然 Igs 和自身反应性 Abs 水平。我们还证明,B 细胞自身产生的 IL4I1 控制生发中心反应、浆细胞分化和对 T 依赖性抗原、SRBC 和 NP-KLH 的特异性 Ab 产生。在体外,与野生型相比,IL4I1 缺陷型 B 细胞在 BCR 交联时更有效地增殖。此外,缺乏 IL4I1 增加了 Syk-Akt-S6kinase 信号通路的激活和钙动员,并抑制了 BCR 结合时 SHP-1 的活性,因此支持 IL4I1 负调控 BCR 依赖性激活。总体而言,我们的研究揭示了 IL4I1 作为 B 细胞生物学关键调节剂的新视角。

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