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Th9 细胞:溃疡性结肠炎发病机制中的可能参与者。

Th9 Cells: Probable players in ulcerative colitis pathogenesis.

机构信息

a Department of Microbiology and Immunology , Faculty of Medicine, Shahrekord University of Medical Sciences , Shahrekord , Iran.

b Department of Dentistry , Department of Medical Microbiology and Immunology , Faculty of Medicine and Dentistry, University of Alberta , Edmonton , Alberta , Canada.

出版信息

Int Rev Immunol. 2018;37(4):192-205. doi: 10.1080/08830185.2018.1457659. Epub 2018 Apr 19.

Abstract

T lymphocytes represent an important part of adaptive immune system undertaking different functions to regulate immune responses. CD4+ T cells are the most important activator cells in inflammatory conditions. Depending on the type of induced cells and inflamed sites, expression and activity of different subtypes of helper T cells are changed. Recent studies have confirmed the existence of a new subset of helper T lymphocytes called Th9. Naive T cells can differentiate into Th9 subtypes if they are exposed simultaneously by interleukin (IL) 4 and transforming growth factor β and also secondary activation of a complicated network of transcription factors such as interferon regulatory factor 4 (IRF4) and Smads which are essential for adequate induction of this phenotype. Th9 cells specifically produce interleukin 9 and their probable roles in promoting intestinal inflammation are being investigated in human subjects and experimental models of ulcerative colitis (UC). Recently, infiltration of Th9 cells, overexpression of IL-9, and certain genes associated with Th9 differentiation have been demonstrated in inflammatory microenvironment of UC. Intestinal oversecretion of IL-9 protein is likely to break down epithelial barriers and compromise tolerance to certain commensal microorganisms which leads to inflammation. Th9 pathogenicity has not yet been adequately explored in UC and they are far from being considered as inflammatory cells in this milieu, therefore precise understanding the role of these newly identified cells in particular their potential role in gut pathogenesis may enable us to develop novel therapeutic approaches for inflammatory bowel disease. So, this article tries to discuss the latest knowledge on the above-mentioned field.

摘要

T 淋巴细胞是适应性免疫系统的重要组成部分,承担着调节免疫反应的不同功能。CD4+T 细胞是炎症状态下最重要的激活细胞。根据诱导细胞的类型和炎症部位的不同,辅助性 T 细胞的不同亚型的表达和活性发生改变。最近的研究证实了一种新的辅助性 T 淋巴细胞亚群的存在,称为 Th9。如果幼稚 T 细胞同时暴露于白细胞介素(IL)4 和转化生长因子β下,并进一步激活干扰素调节因子 4(IRF4)和 Smads 等转录因子的复杂网络,就可以分化为 Th9 亚型,这些转录因子对于充分诱导这种表型是必不可少的。Th9 细胞特异性产生白细胞介素 9,它们在促进肠道炎症中的可能作用正在人类受试者和溃疡性结肠炎(UC)的实验模型中进行研究。最近,在 UC 的炎症微环境中已经证明了 Th9 细胞的浸润、IL-9 的过度表达以及与 Th9 分化相关的某些基因。IL-9 蛋白的肠道过度分泌可能破坏上皮屏障,损害对某些共生微生物的耐受性,从而导致炎症。Th9 的致病性在 UC 中尚未得到充分探讨,它们在这种环境中还远未被认为是炎症细胞,因此,精确了解这些新鉴定的细胞,特别是它们在肠道发病机制中的潜在作用,可能使我们能够为炎症性肠病开发新的治疗方法。因此,本文试图讨论上述领域的最新知识。

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