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非肥胖糖尿病小鼠自身免疫的机制:炎症高峰期效应细胞/调节细胞平衡

Mechanisms of autoimmunity in the non-obese diabetic mouse: effector/regulatory cell equilibrium during peak inflammation.

作者信息

Askenasy Nadir

机构信息

The Leah and Edward M. Frankel Laboratory of Experimental Bone Marrow Transplantation, Petach Tikva, Israel.

出版信息

Immunology. 2016 Apr;147(4):377-88. doi: 10.1111/imm.12581. Epub 2016 Feb 8.

Abstract

Immune imbalance in autoimmune disorders such as type 1 diabetes may originate from aberrant activities of effector cells or dysfunction of suppressor cells. All possible defective mechanisms have been proposed for diabetes-prone species: (i) quantitative dominance of diabetogenic cells and decreased numbers of regulatory T cells, (ii) excessive aggression of effectors and defective function of suppressors, (iii) perturbed interaction between effector and suppressor cells, and (iv) variations in sensitivity to negative regulation. The experimental evidence available to date presents conflicting information on these mechanisms, with identification of perturbed equilibrium on the one hand and negation of critical role of each mechanism in propagation of diabetic autoimmunity on the other hand. In our analysis, there is no evidence that inherent abnormalities in numbers and function of effector and suppressor T cells are responsible for the immune imbalance responsible for propagation of type 1 diabetes as a chronic inflammatory process. Possibly, the experimental tools for investigation of these features of immune activity are still underdeveloped and lack sufficient resolution, in the presence of the extensive biological viability and functional versatility of effector and suppressor elements.

摘要

自身免疫性疾病(如1型糖尿病)中的免疫失衡可能源于效应细胞的异常活动或抑制细胞的功能障碍。针对易患糖尿病的物种,人们提出了所有可能的缺陷机制:(i)致糖尿病细胞的数量优势和调节性T细胞数量减少,(ii)效应细胞过度攻击和抑制细胞功能缺陷,(iii)效应细胞与抑制细胞之间的相互作用紊乱,以及(iv)对负调节的敏感性变化。迄今为止获得的实验证据在这些机制方面呈现出相互矛盾的信息,一方面确定了平衡紊乱,另一方面又否定了每种机制在糖尿病自身免疫传播中的关键作用。在我们的分析中,没有证据表明效应性和抑制性T细胞数量及功能的内在异常是导致1型糖尿病作为慢性炎症过程传播的免疫失衡的原因。可能是,在效应细胞和抑制细胞具有广泛的生物学活性和功能多样性的情况下,用于研究免疫活动这些特征的实验工具仍然不够发达,缺乏足够的分辨率。

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