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中性粒细胞和免疫及炎症中的残留清除。

Neutrophil and remnant clearance in immunity and inflammation.

机构信息

Pharmacology Division, CSIR-Central Drug Research Institute, Lucknow, Uttar Pradesh, India.

Academy of Scientific and Innovative Research (AcSIR), Postal Staff College Area, Ghaziabad, Uttar Pradesh, India.

出版信息

Immunology. 2022 Jan;165(1):22-43. doi: 10.1111/imm.13423. Epub 2021 Nov 9.

Abstract

Neutrophil-centred inflammation and flawed clearance of neutrophils cause and exuberate multiple pathological conditions. These most abundant leukocytes exhibit very high daily turnover in steady-state and stress conditions. Various armours including oxidative burst, NETs and proteases function against pathogens, but also dispose neutrophils to spawn pro-inflammatory responses. Neutrophils undergo death through different pathways upon ageing, infection, executing the intruder's elimination. These include non-lytic apoptosis and other lytic deaths including NETosis, necroptosis and pyroptosis with distinct disintegration of the cellular membrane. This causes release and presence of different intracellular cytotoxic, and tissue-damaging content as cell remnants in the extracellular environment. The apoptotic cells and apoptotic bodies get cleared with non-inflammatory outcomes, while lytic deaths associated remnants including histones and cell-free DNA cause pro-inflammatory responses. Indeed, the enhanced frequencies of neutrophil-associated proteases, cell-free DNA and autoantibodies in diverse pathologies including sepsis, asthma, lupus and rheumatoid arthritis, imply disturbed neutrophil resolution programmes in inflammatory and autoimmune diseases. Thus, the clearance mechanisms of neutrophils and associated remnants are vital for therapeutics. Though studies focused on clearance mechanisms of senescent or apoptotic neutrophils so far generated a good understanding of the same, clearance of neutrophils undergoing distinct lytic deaths, including NETs, are being the subjects of intense investigations. Here, in this review, we are providing the current updates in the clearance mechanisms of apoptotic neutrophils and focusing on not so well-defined recognition, uptake and degradation of neutrophils undergoing lytic death and associated remnants that may provide new therapeutic approaches in inflammation and autoimmunity.

摘要

中性粒细胞为中心的炎症和清除缺陷的中性粒细胞导致并加剧多种病理状况。这些最丰富的白细胞在稳态和应激条件下表现出非常高的每日周转率。各种防御机制包括氧化爆发、NETs 和蛋白酶,既能对抗病原体,也能引发促炎反应。中性粒细胞在衰老、感染、执行清除入侵者的过程中,通过不同的途径死亡。这些途径包括非溶细胞性凋亡和其他溶细胞性死亡,包括 NETosis、坏死性凋亡和细胞焦亡,细胞膜有明显的破裂。这导致不同的细胞内细胞毒性和组织损伤内容物作为细胞残骸释放并存在于细胞外环境中。凋亡细胞和凋亡小体以非炎症的方式被清除,而与溶细胞性死亡相关的残留物质,包括组蛋白和无细胞 DNA,会引起促炎反应。事实上,在包括脓毒症、哮喘、狼疮和类风湿关节炎在内的多种病理中,中性粒细胞相关蛋白酶、无细胞 DNA 和自身抗体的频率增加,意味着炎症和自身免疫性疾病中中性粒细胞的清除程序受到干扰。因此,中性粒细胞及其相关残留物质的清除机制对治疗至关重要。尽管目前的研究集中在衰老或凋亡中性粒细胞的清除机制上,已经对其有了很好的了解,但对经历不同溶细胞性死亡的中性粒细胞的清除,包括 NETosis,仍在进行深入研究。在这篇综述中,我们提供了凋亡中性粒细胞清除机制的最新进展,并重点关注尚未充分定义的识别、摄取和降解经历溶细胞性死亡和相关残留的中性粒细胞,这可能为炎症和自身免疫提供新的治疗方法。

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