单细胞转录组测序部分揭示了肾脏衰老早期T细胞的变化。

IF 3.2 3区 医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular immunology Pub Date : 2024-07-25 DOI:10.1016/j.molimm.2024.06.005
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引用次数: 0

摘要

衰老是一个渐进的、不可避免的生理过程。器官衰老与慢性炎症的持续存在有关,但目前还缺乏对肾脏衰老过程中炎症状态的了解。研究人员对衰老小鼠肾脏进行了单细胞转录组测序,以揭示不同细胞类型的分子表型和组成变化。在衰老早期,肾脏中的免疫细胞(如 T 细胞、B 细胞和单核巨噬细胞)增多。衰老肾脏中 T 细胞的分子状态发生了变化,并出现了极化。其中,我们发现了一组高表达 Eomes、Pdcd1 和 Ifng 的 GZMK+ CD8 + T 细胞,以及一组高表达 Il17a 和 Il23r 的 Il17a+ T 细胞。此外,细胞因子和炎症最终会加重组织损伤。此外,我们还发现不同类型的上皮细胞和 T 细胞之间的相互作用在肾脏衰老过程中有所增加。这些结果表明了T细胞在肾脏衰老早期的变化,并提示GZMK+CD8+ T细胞可能是改善与年龄相关的肾脏功能障碍的潜在靶点(图解摘要)。
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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Single-cell transcriptome sequencing partially revealed the changes of T cells in the early stage of aging kidney

Aging is a gradual, inevitable physiologic process. The organ aging is related to the persistence of chronic inflammation, but the understanding of inflammatory state during renal aging is lacking currently. Single-cell transcriptome sequencing was performed on aging mouse kidney to reveal the molecular phenotype and composition changes of different cell types. In the early stage of aging, immune cells such as T, B cells and mononuclear macrophages increased in kidney. The molecular state of T cells in aging kidney changed and polarized. Among them, we identified a group of GZMK+ CD8 + T cells with high expression of Eomes, Pdcd1 and Ifng and a group of Il17a+ T cells with high expression of Il17a and Il23r. Moreover, the cytokines and inflammations can aggravate tissue damage eventually. Furthermore, we found the interaction between different types of epithelial cells and T cells increased during the renal aging. These results identify the changes of T cells in the early stage of aging kidney and suggest that GZMK+CD8+ T cells might be a potential target to ameliorate age-associated dysfunctions of kidney(Graphical Abstract).

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来源期刊
Molecular immunology
Molecular immunology 医学-免疫学
CiteScore
6.90
自引率
2.80%
发文量
324
审稿时长
50 days
期刊介绍: Molecular Immunology publishes original articles, reviews and commentaries on all areas of immunology, with a particular focus on description of cellular, biochemical or genetic mechanisms underlying immunological phenomena. Studies on all model organisms, from invertebrates to humans, are suitable. Examples include, but are not restricted to: Infection, autoimmunity, transplantation, immunodeficiencies, inflammation and tumor immunology Mechanisms of induction, regulation and termination of innate and adaptive immunity Intercellular communication, cooperation and regulation Intracellular mechanisms of immunity (endocytosis, protein trafficking, pathogen recognition, antigen presentation, etc) Mechanisms of action of the cells and molecules of the immune system Structural analysis Development of the immune system Comparative immunology and evolution of the immune system "Omics" studies and bioinformatics Vaccines, biotechnology and therapeutic manipulation of the immune system (therapeutic antibodies, cytokines, cellular therapies, etc) Technical developments.
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