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Pathological conditions re-shape physiological Tregs into pathological Tregs

机译:病理状况将生理性Treg重塑为病理性Treg

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CD4+FOXP3+ regulatory T cells (Tregs) are a subset of CD4 T cells that play an essential role in maintaining peripheral immune tolerance, controlling acute and chronic inflammation, allergy, autoimmune diseases, and anti-cancer immune responses. Over the past 20 years, a significant progress has been made since Tregs were first characterized in 1995. Many concepts and principles regarding Tregs generation, phenotypic features, subsets (tTregs, pTregs, iTregs, and iTreg35), tissue specificity (central Tregs, effector Tregs, and tissue resident Tregs), homeostasis (highly dynamic and apoptotic), regulation of Tregs by receptors for PAMPs and DAMPs, Treg plasticity (re-differentiation to other CD4 T helper cell subsets, Th1, Th2, Tfh, and Th17), and epigenetic regulation of Tregs phenotypes and functions have been innovated. In this concise review, we want to briefly analyze these eight new progresses in the study of Tregs. We have also proposed for the first time a novel concept that “physiological Tregs” have been re-shaped into “pathological Tregs” in various pathological environments. Continuing of the improvement in our understanding on this important cellular component about the immune tolerance and immune suppression would lead to the future development of novel therapeutics approaches for acute and chronic inflammatory diseases, allergy, allogeneic transplantation-related immunity, sepsis, autoimmune diseases, and cancers. Keywords Regulatory T cells Immune suppression Epigenetic mechanisms Histone modifications Metabolic cardiovascular diseases
机译:CD4 + FOXP3 + 调节性T细胞(Treg)是CD4 T细胞的一个子集,在维持外周免疫耐受,控制急性和慢性炎症,过敏,自身免疫性疾病和抗癌免疫反应。在过去的20年中,自1995年首次对Tregs进行表征以来,已经取得了重大进展。有关Tregs产生,表型特征,子集(tTregs,pTregs,iTregs和iTreg35),组织特异性(中央Tregs,效应子)的许多概念和原则。 Treg和组织中的Treg),体内稳态(高度动态和凋亡),PAMP和DAMP受体对Treg的调节,Treg可塑性(与其他CD4 T辅助细胞亚群Th1,Th2,Tfh和Th17的再分化), Tregs表型和功能的表观遗传调控已得到创新。在这篇简明的综述中,我们想简要分析一下Tregs研究中的这八项新进展。我们还首次提出了一种新颖的概念,即在各种病理环境中,“生理性Treg”已被重塑为“病理性Treg”。如果我们继续对这种重要的细胞成分的免疫耐受和免疫抑制的认识不断提高,将会导致针对急性和慢性炎性疾病,变态反应,与同种异体移植相关的免疫力,败血症,自身免疫性疾病和癌症。关键词调节性T细胞免疫抑制表观遗传机制组蛋白修饰代谢性心血管疾病

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