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人中性粒细胞对微流控装置中补体激活和抑制的反应。

Human Neutrophils Respond to Complement Activation and Inhibition in Microfluidic Devices.

机构信息

BioMEMS Resource Center, Department of Surgery, Massachusetts General Hospital, Harvard Medical School, Boston, MA, United States.

Shriners Burns Hospital, Boston, MA, United States.

出版信息

Front Immunol. 2021 Nov 24;12:777932. doi: 10.3389/fimmu.2021.777932. eCollection 2021.

Abstract

Complement activation is key to anti-microbial defenses by directly acting on microbes and indirectly by triggering cellular immune responses. Complement activation may also contribute to the pathogenesis of numerous inflammatory and immunological diseases. Consequently, intense research focuses on developing therapeutics that block pathology-causing complement activation while preserving anti-microbial complement activities. However, the pace of research is slowed down significantly by the limitations of current tools for evaluating complement-targeting therapeutics. Moreover, the effects of potential therapeutic agents on innate immune cells, like neutrophils, are not fully understood. Here, we employ microfluidic assays and measure chemotaxis, phagocytosis, and swarming changes in human neutrophils in response to various complement-targeting agents. We show that whereas complement factor 5 (C5) cleavage inhibitor eculizumab blocks all neutrophil anti-microbial functions, newer compounds like the C5 cleavage inhibitor RA101295 and C5a receptor antagonist avacopan inhibit chemotaxis and swarming while preserving neutrophil phagocytosis. These results highlight the utility of microfluidic neutrophil assays in evaluating potential complement-targeting therapeutics.

摘要

补体激活是抗微生物防御的关键,它可以直接作用于微生物,也可以通过触发细胞免疫反应间接作用。补体激活也可能导致许多炎症和免疫性疾病的发病机制。因此,人们强烈关注开发能够阻断致病补体激活的治疗方法,同时保留抗微生物补体活性的治疗方法。然而,目前用于评估补体靶向治疗方法的工具存在局限性,这极大地减缓了研究的步伐。此外,潜在治疗剂对先天免疫细胞(如中性粒细胞)的影响还不完全清楚。在这里,我们采用微流控分析方法,测量了人类中性粒细胞对各种补体靶向药物的趋化性、吞噬作用和群集运动变化。我们发现,补体因子 5(C5)裂解抑制剂依库珠单抗阻断了所有中性粒细胞的抗微生物功能,而新型化合物,如 C5 裂解抑制剂 RA101295 和 C5a 受体拮抗剂 avacopan,在抑制趋化性和群集运动的同时,保留了中性粒细胞的吞噬作用。这些结果突出了微流控中性粒细胞分析在评估潜在补体靶向治疗方法中的应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/139b/8653703/ef0eb86c68ef/fimmu-12-777932-g001.jpg

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