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Sarcoidosis and the mTOR, Rac1, and Autophagy Triad

机译:结节病和MTOR,RAC1和自噬三合一

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摘要

Sarcoidosis is an enigmatic multisystem disease characterized by the development and accumulation of granulomas: a compact collection of macrophages that have differentiated into epithelioid cells and which are associated with T helper (Th)1 and Th17 cells. Although no single causative factor has been shown to underlie sarcoidosis in humans, its etiology has been related to microbial, environmental, and genetic factors. We examine how these factors play a role in sarcoidosis pathogenesis. Specifically, we propose that dysfunction of mTOR, Rac1, and autophagy-related pathways not only hampers pathogen or nonorganic particle clearance but also participates in T cell and macrophage dysfunction, driving granuloma formation. This concept opens new avenues for potentially treating sarcoidosis and may serve as a blueprint for other granulomatous disorders.
机译:结节病是一种神秘的多系统疾病,其特征在于肉芽肿的开发和积累:巨大的巨噬细胞收集,其具有与上皮细胞分化并与T辅助剂(TH)1和TH17细胞相关。 虽然人类在人类的结利术中没有出现单一的致病因素,但其病因与微生物,环境和遗传因素有关。 我们研究这些因素如何在顺节病发病机制中发挥作用。 具体而言,我们提出了MTOR,RAC1和自噬相关途径的功能障碍不仅妨碍了病原体或非无限颗粒间隙,而且还参与了T细胞和巨噬细胞功能障碍,驱动肉芽肿形成。 这一概念打开了新的途径,以潜在地治疗结节病,可以作为其他肉芽肿性疾病的蓝图。

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  • 来源
    《Trends in immunology》 |2020年第4期|共14页
  • 作者单位

    Lyon 1 Claude Bernard Univ South Med Univ Hosp Inflammat &

    Immun Resp Epithelium EA7426 PI3;

    Med Univ Vienna Ctr Pathobiochem &

    Genet Inst Med Genet Vienna Austria;

    Med Univ Vienna Ctr Pathobiochem &

    Genet Inst Med Genet Vienna Austria;

    Univ Paris 13 Avicenne Hosp AP HP Dept Pulmonol EA 2363 Bobigny France;

    Hosp Civils Lyon Univ Hosp Dept Mol &

    Med Genet Bron France;

    Lyon 1 Claude Bernard Univ South Med Univ Hosp Inflammat &

    Immun Resp Epithelium EA7426 PI3;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医学免疫学;
  • 关键词

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