Children's Health Queensland Clinical Unit, School of Clinical Medicine, Faculty of Medicine, Mater Research, University of Queensland, St. Lucia, Brisbane, QLD, Australia.
School of Biomedical Sciences, Faculty of Medicine, University of Queensland, St. Lucia, Brisbane, QLD, Australia.
Front Immunol. 2021 Feb 11;11:624597. doi: 10.3389/fimmu.2020.624597. eCollection 2020.
The immune system has evolved to protect the host from the pathogens and allergens surrounding their environment. The immune system develops in such a way to recognize self and non-self and develops self-tolerance against self-proteins, nucleic acids, and other larger molecules. However, the broken immunological self-tolerance leads to the development of autoimmune or autoinflammatory diseases. Pattern-recognition receptors (PRRs) are expressed by immunological cells on their cell membrane and in the cytosol. Different Toll-like receptors (TLRs), Nod-like receptors (NLRs) and absent in melanoma-2 (AIM-2)-like receptors (ALRs) forming inflammasomes in the cytosol, RIG (retinoic acid-inducible gene)-1-like receptors (RLRs), and C-type lectin receptors (CLRs) are some of the PRRs. The DNA-sensing receptor cyclic GMP-AMP synthase (cGAS) is another PRR present in the cytosol and the nucleus. The present review describes the role of ALRs (AIM2), TLR9, and cGAS in recognizing the host cell DNA as a potent damage/danger-associated molecular pattern (DAMP), which moves out to the cytosol from its housing organelles (nucleus and mitochondria). The introduction opens with the concept that the immune system has evolved to recognize pathogens, the idea of ,and its failure due to the emergence of autoimmune diseases (ADs), and the discovery of PRRs revolutionizing immunology. The second section describes the cGAS-STING signaling pathway mediated cytosolic self-DNA recognition, its evolution, characteristics of self-DNAs activating it, and its role in different inflammatory conditions. The third section describes the role of TLR9 in recognizing self-DNA in the endolysosomes during infections depending on the self-DNA characteristics and various inflammatory diseases. The fourth section discusses about AIM2 (an ALR), which also binds cytosolic self-DNA (with 80-300 base pairs or bp) that inhibits cGAS-STING-dependent type 1 IFN generation but induces inflammation and pyroptosis during different inflammatory conditions. Hence, this trinity of PRRs has evolved to recognize self-DNA as a potential DAMP and comes into action to guard the cellular galaxy. However, their dysregulation proves dangerous to the host and leads to several inflammatory conditions, including sterile-inflammatory conditions autoinflammatory and ADs.
免疫系统的进化是为了保护宿主免受周围环境中的病原体和过敏原的侵害。免疫系统的发展方式是识别自我和非自我,并对自我蛋白、核酸和其他较大分子产生自身耐受性。然而,免疫自身耐受性的破坏导致自身免疫或自身炎症性疾病的发展。模式识别受体 (PRRs) 表达在免疫细胞的细胞膜和细胞质中。不同的 Toll 样受体 (TLRs)、Nod 样受体 (NLRs) 和黑色素瘤 2 (AIM-2) 样受体 (ALRs) 在细胞质中形成炎性体,RIG (视黄酸诱导基因)-1 样受体 (RLRs) 和 C 型凝集素受体 (CLRs) 是一些 PRRs。细胞质和核中存在另一种 PRR 环状 GMP-AMP 合酶 (cGAS)。本综述描述了 ALRs (AIM2)、TLR9 和 cGAS 在识别宿主细胞 DNA 作为一种有效的损伤/危险相关分子模式 (DAMP) 方面的作用,该模式从其细胞器 (核和线粒体) 转移到细胞质。引言以免疫系统进化为背景,介绍了识别病原体的概念,由于自身免疫性疾病 (AD) 的出现导致该系统失效的观点,以及 PRRs 的发现对免疫学的革命性影响。第二部分描述了 cGAS-STING 信号通路介导的细胞质自身 DNA 识别,其进化、激活它的自身 DNA 特征及其在不同炎症条件下的作用。第三部分描述了 TLR9 在感染期间在内体溶酶体中识别自身 DNA 的作用,这取决于自身 DNA 的特征和各种炎症性疾病。第四部分讨论了 AIM2(一种 ALR),它也与细胞质自身 DNA(80-300 个碱基对或 bp)结合,抑制 cGAS-STING 依赖性 I 型 IFN 的产生,但在不同的炎症条件下诱导炎症和细胞焦亡。因此,这三种 PRRs 的进化是为了识别自身 DNA 作为一种潜在的 DAMP,并发挥作用来保护细胞星系。然而,它们的失调对宿主是危险的,并导致几种炎症条件,包括无菌性炎症条件、自身炎症性疾病和 AD。
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