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中性粒细胞和S100A9蛋白对肉芽肿形成起着关键调节作用。

Neutrophils and the S100A9 protein critically regulate granuloma formation.

作者信息

Yoshioka Yuya, Mizutani Tatsuaki, Mizuta Satoshi, Miyamoto Ayumi, Murata Satoru, Ano Toshiaki, Ichise Hiroshi, Morita Daisuke, Yamada Hiroyuki, Hoshino Yoshihiko, Tsuruyama Tatsuaki, Sugita Masahiko

机构信息

Laboratory of Cell Regulation, Institute for Virus Research, and.

Laboratory of Cell Regulation and Molecular Network, Graduate School of Biostudies, Kyoto University, Kyoto, Japan.

出版信息

Blood Adv. 2016 Dec 14;1(3):184-192. doi: 10.1182/bloodadvances.2016000497. eCollection 2016 Dec 27.

Abstract

Macrophages have the potential to undergo cellular transformation into epithelioid cells, and their concentric accumulation in tissues results in the development of granulomas. Although epithelioid cells are an essential and dominant component of granulomas, other cell types have also been detected, which may contribute to the establishment of well-organized granulomas, as observed in human granulomatous diseases. We herein demonstrated that neutrophils may mediate these functions. By taking advantage of the guinea pig pulmonary granuloma model, we obtained a rat monoclonal antibody with unique reactivity to granuloma cells. This antibody, termed G213, reacted with clusters of neutrophils located in the central area of granulomas, and a biochemical analysis identified the G213-reactive antigen as S100A9, a calcium-binding protein of the S100 family, which was expressed abundantly in neutrophils. Consistent with the multifaceted functions attributed to S100A9, including its role in neutrophil extravasation and macrophage activation, the blockade of S100A9 functions with the specific inhibitor, tasquinimod, impaired the formation of organized granulomas with neutrophil cores. These results demonstrate the critical role of neutrophils and the S100A9 protein in granuloma formation. Because intragranuloma S100A9 neutrophils were also detected in humans, these results indicate the potential of tasquinimod, a new anticancer drug candidate, for manipulating human granulomatous diseases.

摘要

巨噬细胞有潜力发生细胞转化成为上皮样细胞,并且它们在组织中的同心性聚集会导致肉芽肿的形成。尽管上皮样细胞是肉芽肿的重要且主要成分,但也检测到了其他细胞类型,这些细胞类型可能有助于形成结构良好的肉芽肿,正如在人类肉芽肿性疾病中所观察到的那样。我们在此证明中性粒细胞可能介导这些功能。利用豚鼠肺部肉芽肿模型,我们获得了一种对肉芽肿细胞具有独特反应性的大鼠单克隆抗体。这种名为G213的抗体与位于肉芽肿中心区域的中性粒细胞簇发生反应,生化分析确定G213反应性抗原为S100A9,它是S100家族的一种钙结合蛋白,在中性粒细胞中大量表达。与归因于S100A9的多方面功能一致,包括其在中性粒细胞渗出和巨噬细胞激活中的作用,用特异性抑制剂他喹莫德阻断S100A9的功能会损害具有中性粒细胞核心的有组织肉芽肿的形成。这些结果证明了中性粒细胞和S100A9蛋白在肉芽肿形成中的关键作用。因为在人类中也检测到了肉芽肿内的S100A9阳性中性粒细胞,这些结果表明新型抗癌候选药物他喹莫德在治疗人类肉芽肿性疾病方面的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/26e2/5737174/7608f4d405ee/advances000497absf1.jpg

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