[Regulatory T cells].

Q4 Medicine Acta Medica Croatica Pub Date : 2006-12-01 DOI:10.1142/9789813231719_0008
I. Marinić, A. Gagro, S. Rabatić
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引用次数: 1

Abstract

Regulatory T-cells are a subset of T cells that have beene extensively studied in modern immunology. They are important for the maintenance of peripheral tolerance, and have an important role in various clinical conditions such as allergy, autoimmune disorders, tumors, infections, and in transplant medicine. Basically, this population has a suppressive effect on the neighboring immune cells, thus contributing to the local modulation and control of immune response. There are two main populations of regulatory T cells - natural regulatory T cells, which form a distinct cellular lineage, develop in thymus and perform their modulatory action through direct intercellular contact, along with the secreted cytokines; and inducible regulatory T cells, which develop in the periphery after contact with the antigen that is presented on the antigen presenting cell, and their primary mode of action is through the interleukin 10 (IL-10) and transforming growth factor beta (TGF-alpha) cytokines. Natural regulatory T cells are activated through T cell receptor after contact with specific antigen and inhibit proliferation of other T cells in an antigen independent manner. One of the major difficulties in the research of regulatory T cells is the lack of specific molecular markers that would identify these cells. Natural regulatory T cells constitutively express surface molecule CD25, but many other surface and intracellular molecules (HLA-DR, CD122, CD45RO, CD62, CTLA-4, GITR, PD-1, Notch, FOXP3, etc.) are being investigated for further phenotypic characterization of these cells. Because regulatory T cells have an important role in establishing peripheral tolerance, their importance is manifested in a number of clinical conditions. In the IPEX syndrome (immunodysregulation, polyendocrinopathy and enteropathy, X-linked), which is caused by mutation in Foxp3 gene that influences the development and function of regulatory T cells, patients develop severe autoimmune reactions that involve autoimmune endocrine disorders (type 1 diabetes, thyroiditis), respiratory and nutritive allergy, eczema and severe infections. In different types of allergy (pollen allergy, dust mite, nutritive allergens, contact hypersensitivity, etc.) and autoimmune diseases (such as rheumatoid arthritis, multiple sclerosis and type 1 diabetes) a lower number or decreased functional capability of regulatory T cells have been described. In inflammatory conditions and infections, this cell population has an important task in restricting immune response and protecting the host from excessive damage. This ability of regulatory T cells can be used by some pathogens (Epstein Barr virus, Mycobacterium tuberculosis, Leishmania major, etc.) and tumor cells to avoid host response and therefore contribute to the development of some pathological conditions. The knowledge gained on the phenotype and function of regulatory T cells could be useful in many medical conditions. In allergy, autoimmune diseases and in transplant procedures in medicine it would be desirable to increase their function, thus to partially suppress the immune system activity. On the other hand, in some infections and tumors, it would be preferable to decrease the activity of regulatory T cells and boost the function of effector T cells. Regulatory T cells comprise a very active field of immunology, therefore monitoring and modulating of their activity is of great potential significance in a broad spectrum of clinical conditions. By developing and standardizing methods for their monitoring, it would be possible to follow additional parameters of certain clinical conditions and possibly utilize them in therapy.
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调节性T细胞。
调节性T细胞是T细胞的一个子集,在现代免疫学中得到了广泛的研究。它们对于外周耐受性的维持很重要,并且在各种临床疾病如过敏、自身免疫性疾病、肿瘤、感染和移植医学中发挥重要作用。基本上,这个群体对邻近的免疫细胞有抑制作用,从而有助于局部调节和控制免疫反应。调节性T细胞主要有两种:自然调节性T细胞,它们形成独特的细胞谱系,在胸腺中发育,并通过直接的细胞间接触以及分泌的细胞因子来发挥调节作用;和诱导调节性T细胞,它们与抗原呈递细胞上的抗原接触后在外周发育,它们的主要作用方式是通过白细胞介素10 (IL-10)和转化生长因子β (tgf - α)细胞因子。自然调节性T细胞与特异性抗原接触后,通过T细胞受体被激活,并以不依赖抗原的方式抑制其他T细胞的增殖。调节性T细胞研究的主要困难之一是缺乏特异性分子标记来识别这些细胞。自然调节性T细胞组成性地表达表面分子CD25,但许多其他表面和细胞内分子(HLA-DR、CD122、CD45RO、CD62、CTLA-4、GITR、PD-1、Notch、FOXP3等)正在被研究以进一步表征这些细胞的表型。由于调节性T细胞在建立外周耐受性方面起着重要作用,它们的重要性在许多临床条件中得到体现。IPEX综合征(免疫失调、多内分泌病和肠病,x连锁)是由Foxp3基因突变影响调节性T细胞的发育和功能引起的,患者会出现严重的自身免疫反应,包括自身免疫性内分泌紊乱(1型糖尿病、甲状腺炎)、呼吸和营养过敏、湿疹和严重感染。在不同类型的过敏(花粉过敏、尘螨、营养性过敏原、接触性超敏反应等)和自身免疫性疾病(如类风湿关节炎、多发性硬化症和1型糖尿病)中,调节性T细胞数量较少或功能能力下降已被描述。在炎症条件和感染中,这些细胞群在限制免疫反应和保护宿主免受过度损伤方面具有重要作用。调节性T细胞的这种能力可以被一些病原体(爱泼斯坦巴尔病毒、结核分枝杆菌、利什曼原虫等)和肿瘤细胞利用,以避免宿主反应,从而促进一些病理状况的发展。关于调节性T细胞的表型和功能的知识在许多医疗条件下可能是有用的。在过敏、自身免疫性疾病和医学上的移植手术中,希望增加它们的功能,从而部分抑制免疫系统的活性。另一方面,在某些感染和肿瘤中,最好是降低调节性T细胞的活性,增强效应T细胞的功能。调节性T细胞是一个非常活跃的免疫学领域,因此监测和调节其活性在广泛的临床条件下具有重要的潜在意义。通过开发和标准化监测方法,可以跟踪某些临床条件的附加参数,并可能将其用于治疗。
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 Medica Croatica
Acta Medica Croatica Medicine-Medicine (all)
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期刊介绍: ACTA MEDICA CROATICA publishes original contributions to medical sciences, that have not been previously published. All manuscripts should be written in English.
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