Cathepsin L-dependent positive selection shapes clonal composition and functional fitness of CD4+ T cells

IF 27.7 1区 医学 Q1 IMMUNOLOGY
Elisabetta Petrozziello, Amina Sayed, João A. Freitas, Christine Federle, Jelena Nedjic, Sarina Ravens, Batuhan Akçabozan, Anna M. Schulz, Dietmar Zehn, Marc Schmidt-Supprian, Reinhard Obst, Immo Prinz, Martijn Verdoes, Jan Kisielow, Thomas Reinheckel, Tobias Straub, Stephen R. Daley, Ludger Klein
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Abstract

The physiological significance of thymic positive selection and its reliance on a single stromal cell type, cortical thymic epithelial cells, remain incompletely understood. The lysosomal cysteine protease cathepsin L (CTSL) has been implicated in generating major histocompatibility complex class II-bound peptides in cortical thymic epithelial cells for efficient CD4+ T cell differentiation. Here, we addressed the extent and nature of the CD4+ T cell repertoire changes associated with CTSL deficiency. In the absence of CTSL, a highly selective loss of T cell receptors resulted in a markedly reduced repertoire diversity. However, a similarly large proportion of nominally ‘CTSL-independent’ T cell receptors were retained. Clones representative of the second category experienced weaker positive selection signals in the absence of CTSL, which were sufficient for further maturation yet imprinted aberrant responsiveness to agonist stimulation and impaired homeostatic behavior. Together, these findings demonstrate that CTSL is crucial for both shaping full repertoire diversity and optimizing CD4+ T cell functionality.

Abstract Image

组织蛋白酶l依赖的阳性选择决定了CD4+ T细胞的克隆组成和功能适应性
胸腺阳性选择的生理意义及其对单一基质细胞类型——胸腺皮质上皮细胞的依赖,仍不完全清楚。溶酶体半胱氨酸蛋白酶组织蛋白酶L (CTSL)在胸腺皮质上皮细胞中产生主要的组织相容性复合体ii类结合肽,以促进CD4+ T细胞的有效分化。在这里,我们讨论了与CTSL缺陷相关的CD4+ T细胞库变化的程度和性质。在缺乏CTSL的情况下,T细胞受体的高度选择性损失导致库多样性显着降低。然而,同样大比例的名义上“ctsl独立”的T细胞受体被保留。在缺乏CTSL的情况下,第二类克隆的阳性选择信号较弱,这足以使其进一步成熟,但却对激动剂刺激产生异常反应,损害了体内平衡行为。总之,这些发现表明,CTSL对于形成全库多样性和优化CD4+ T细胞功能至关重要。
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来源期刊
Nature Immunology
Nature Immunology 医学-免疫学
CiteScore
40.00
自引率
2.30%
发文量
248
审稿时长
4-8 weeks
期刊介绍: Nature Immunology is a monthly journal that publishes the highest quality research in all areas of immunology. The editorial decisions are made by a team of full-time professional editors. The journal prioritizes work that provides translational and/or fundamental insight into the workings of the immune system. It covers a wide range of topics including innate immunity and inflammation, development, immune receptors, signaling and apoptosis, antigen presentation, gene regulation and recombination, cellular and systemic immunity, vaccines, immune tolerance, autoimmunity, tumor immunology, and microbial immunopathology. In addition to publishing significant original research, Nature Immunology also includes comments, News and Views, research highlights, matters arising from readers, and reviews of the literature. The journal serves as a major conduit of top-quality information for the immunology community.
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