Apoptosis and Thyroiditis

Patricia L. Arscott, James R. Baker Jr.
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引用次数: 75

Abstract

The origin of the various forms of autoimmune thyroiditis remains unclear. Most investigations into the pathogenesis of these disorders have focused on immune abnormalities that might lead to an autoimmune response. However, no unique immune response to thyroid autoantigens has been identified that either is limited to patients with thyroiditis or is absolutely correlated with clinical disease expression. CD8 T-cell-mediated cytotoxicity is thought to be a major cause of thyroid follicular cell damage in thyroiditis. This damage is produced in part through the induction of apoptosis in thyroid cells. Recent studies have demonstrated that programmed cell death is regulated in thyroid cells and that a major pathway for immune-mediated apoptosis, the Fas pathway, is blocked by labile inhibitors in a manner that could prevent cytotoxicity. This review also examines several other types of regulation of apoptotic pathways in thyrocytes. We hypothesize that the regulation of programmed cell death pathways in the thyroid may alter the expression of autoimmune thyroid diseases by modifying the susceptibility of thyroid cells to immune-mediated apoptosis.

细胞凋亡与甲状腺炎
各种形式的自身免疫性甲状腺炎的起源仍不清楚。对这些疾病发病机制的大多数研究都集中在可能导致自身免疫反应的免疫异常上。然而,目前还没有发现对甲状腺自身抗原的独特免疫反应,这种免疫反应要么仅限于甲状腺炎患者,要么与临床疾病表达绝对相关。CD8 t细胞介导的细胞毒性被认为是甲状腺炎中甲状腺滤泡细胞损伤的主要原因。这种损伤部分是通过诱导甲状腺细胞凋亡而产生的。最近的研究表明,程序性细胞死亡在甲状腺细胞中受到调节,免疫介导的凋亡的主要途径Fas途径被不稳定的抑制剂阻断,从而可以防止细胞毒性。本综述还探讨了甲状腺细胞凋亡通路的其他几种调节类型。我们假设,甲状腺细胞程序性死亡通路的调节可能通过改变甲状腺细胞对免疫介导的凋亡的易感性来改变自身免疫性甲状腺疾病的表达。
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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