Markers of Th1 polarized Th17 cells (literature review)

Q4 Immunology and Microbiology Acta Biomedica Scientifica Pub Date : 2023-07-11 DOI:10.29413/abs.2023-8.3.5
E. Kuklina, N. Glebezdina
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Abstract

T helpers (Th) producing IL-17 (Th17) have high plasticity and under the influence of external conditions are able to redifferentiate into cells with a different phenotype, primarily in Th1-lymphocytes, forming a population that combines the characteristics of both Th17 and Th1 and has a high pro-inflammatory potential, as well as a unique ability to overcome histohematic barriers. These cells are currently assigned a key role in the pathogenesis of many inflammatory diseases, including autoimmune ones: they account for up to half of the lymphocytes present in infiltrates of inflamed tissues. The paper discusses the reasons for the increased plasticity of Th17 cells in comparison with the main T helper populations (Th1 and Th2) and considers in detail the mechanisms of formation of IFNγ producing Th17, taking into account not only the redifferentiation of mature Th17, but also possible alternative pathways, in particular, Th1 cell redifferentiation or naive CD4+T lymphocytes direct differentiation into cells with an intermediate Th1/Th17 phenotype. The main inducers of differentiation of IFNγ producing Th17 cells and the reversibility of this process are also discussed. Particular attention is paid to the methods for identifying Th1 polarized Th17 cells: this population is heterogeneous, and its size significantly depends on the type of markers used to characterize these cells – Th1/Th17-associated transcription factors, key cytokines, as well as chemokine receptors and other membrane molecules. As a result, the data in the works on this problem are poorly comparable with each other. The unification of approaches to identifying a population of Th1 like Th17 cells will solve this problem and make it possible to use an assessment of the size and activity of such a population as diagnostic or prognostic markers.
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Th1极化Th17细胞的标记物(文献复习)
产生IL-17 (Th17)的T辅助细胞(Th)具有很高的可塑性,在外界条件的影响下,能够重新分化为具有不同表型的细胞,主要是在Th1淋巴细胞中,形成一个结合了Th17和Th1特征的群体,具有高促炎潜能,以及克服组织血屏障的独特能力。目前,这些细胞在包括自身免疫性疾病在内的许多炎症性疾病的发病机制中起着关键作用:它们占炎症组织浸润物中淋巴细胞的一半。本文讨论了与主要辅助性T细胞群(Th1和Th2)相比,Th17细胞可塑性增加的原因,并详细考虑了产生IFNγ的Th17的形成机制,不仅考虑了成熟Th17的再分化,还考虑了可能的替代途径,特别是Th1细胞再分化或幼稚CD4+T淋巴细胞直接分化为具有中间Th1/Th17表型的细胞。本文还讨论了产生IFNγ的Th17细胞分化的主要诱导剂及其过程的可逆性。特别要注意的是鉴定Th1极化Th17细胞的方法:这个群体是异质的,其大小在很大程度上取决于用于表征这些细胞的标记类型- Th1/Th17相关转录因子,关键细胞因子,以及趋化因子受体和其他膜分子。因此,关于这一问题的研究数据彼此之间的可比性很差。鉴别Th1细胞群(如Th17细胞群)的统一方法将解决这一问题,并使评估此类细胞群的大小和活性成为可能,作为诊断或预后标记。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Acta Biomedica Scientifica
Acta Biomedica Scientifica Immunology and Microbiology-General Immunology and Microbiology
CiteScore
0.40
自引率
0.00%
发文量
106
审稿时长
7 weeks
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