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Stress protein expression in primary and immortalized cultures of human thyroid cells: a model system for the study of stress proteins in the pathogenesis of autoimmune thyroid disease

机译:人甲状腺细胞原代培养和永生培养中的应激蛋白表达:自身免疫性甲状腺疾病发病机理中应激蛋白研究的模型系统

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摘要

Stress has, for many years, been linked to the onset of autoimmune disease and, in particular, autoimmune thyroid disease (AITD). Whilst the exact mechanism of this association is unknown, it is clear that episodes of stress can induce profound changes in the immune system. More specifically, recent studies from several laboratories have shown an association between the expression of stress proteins and, particularly, the Hsp70 family with AITD. Our own studies describe a thyroid-specific Hsp70 which shares antigenicity with the key thyroid autoantigen, thyroid peroxidase. Further studies on the molecular basis for this observation are, however, hampered by the lack of a suitably validated thyroid cell model. In this paper we compare the response of primary cultures of human thyrocytes to hyperthermia with the response seen in the immortalized human thyroid cell line HTori3. Both cell types responded in a broadly similar manner, synthesizing proteins from two of the major stress protein families, Hsp70 and Hsp90. In the primary human thyrocyte cultures the 70 kDa proteins showed a 7.5-fold increase and the 90 kDa proteins a 2.7-fold increase with hyperthermia whilst in the HTori3 cells the increases in response to hyperthermia were 10- and 6.5-fold, respectively. We also show a dose-dependent stress response in HTori3 cells cultured in the presence of arsenite ions. We conclude that the response of this highly differentiated and stable thyroid cell line to stress is similar to that seen in primary cultures of human thyroid cells and that these immortalized cells will afford a convenient and effective model for the further study of the role of stress in the pathology of AITD.
机译:多年来,压力与自身免疫性疾病特别是自身免疫性甲状腺疾病(AITD)的发作有关。虽然这种关联的确切机制尚不清楚,但很明显,压力发作可以诱发免疫系统的深刻变化。更具体地说,来自几个实验室的最新研究表明,应激蛋白的表达与AITD特别是Hsp70家族之间存在关联。我们自己的研究描述了一种甲状腺特异性Hsp70,它与关键的甲状腺自身抗原甲状腺过氧化物酶具有抗原性。但是,由于缺乏适当验证的甲状腺细胞模型,因此无法在分子基础上进行进一步的研究。在本文中,我们将人类甲状腺细胞原代培养物对热疗的反应与永生化的人类甲状腺细胞系HTori3的反应进行了比较。两种细胞类型都以大致相似的方式做出反应,合成了来自两个主要应激蛋白家族Hsp70和Hsp90的蛋白。在原代人甲状腺细胞培养物中,随着热疗,70 kDa蛋白显示增加了7.5倍,而90 kDa蛋白则显示了2.7倍的增加,而在HTori3细胞中,对热疗的响应分别增加了10倍和6.5倍。我们还显示了在砷离子存在下培养的HTori3细胞中的剂量依赖性应激反应。我们得出的结论是,这种高度分化和稳定的甲状腺细胞系对应激的反应与人类甲状腺细胞原代培养中所见相似,并且这些永生化的细胞将为进一步研究应激在小鼠体内的作用提供方便和有效的模型。 AITD的病理学。

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