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参与甲状腺自身免疫性疾病的自身抗原的结构特征:甲状腺微粒体/微绒毛抗原。

Structural features of the autoantigens involved in thyroid autoimmune disease: the thyroid microsomal/microvillar antigen.

作者信息

Banga J P, Pryce G, Hammond L, Roitt I M

出版信息

Mol Immunol. 1985 Jun;22(6):629-42. doi: 10.1016/0161-5890(85)90092-6.

Abstract

The microsomal/microvillar antigen of the human thyroid gland which provokes thyroid autoimmunity was characterised by immunoprecipitation studies. Sera from patients with Hashimoto's thyroiditis, primary myxoedema or Graves' disease containing autoanti-microsomal antibody specifically precipitated a component, which under reducing conditions migrates with a mol. wt of 105,000 on SDS-polyacrylamide gel electrophoresis. This protein was absent in auto- or xeno-anti-thyroglobulin precipitates, which under reducing conditions display four polypeptides of Mr 260,000, 230,000, 180,000 and 142,000. Under non-reducing conditions, the microsomal/microvillar antigen displayed a small shift in mobility to a mol. wt of 117,000 suggesting the presence of intrachain disulphide bonds. In contrast, under these conditions, anti-thyroglobulin precipitated components displaying polypeptides of approx. mol. wts in the region of 240,000-260,000, 170,000-180,000 and 140,000. Absorption of thyroiditis sera on thyroglobulin-Sepharose followed by immunoprecipitation abolished the anti-thyroglobulin components without affecting the binding of the 105,000-dalton polypeptide, if the sera contained antimicrosomal antibody. No comparable material was identified in microsomal membrane preparations prepared from the stomach which is also commonly involved in organ-specific autoimmunity. The 105,000-dalton component does not bind to a Lens culinaris lectin affinity column. We conclude that the epitopes of the microsomal/microvillar antigen are presented on a poorly glycosylated peptide of mol. wt 105,000, which is probably stabilised by intrachain disulphide bonds and which does not share serological reactivity with membrane-bound thyroglobulin.

摘要

通过免疫沉淀研究对引发甲状腺自身免疫的人甲状腺微粒体/微绒毛抗原进行了表征。来自桥本甲状腺炎、原发性黏液性水肿或格雷夫斯病患者的血清,含有自身抗微粒体抗体,可特异性沉淀一种成分,在还原条件下,该成分在SDS-聚丙烯酰胺凝胶电泳上的分子量为105,000。这种蛋白质在自身或异种抗甲状腺球蛋白沉淀中不存在,在还原条件下,抗甲状腺球蛋白沉淀显示出分子量分别为260,000、230,000、180,000和142,000的四种多肽。在非还原条件下,微粒体/微绒毛抗原的迁移率略有变化,分子量为117,000,表明存在链内二硫键。相比之下,在这些条件下,抗甲状腺球蛋白沉淀的成分显示出分子量约为240,000 - 260,000、170,000 - 180,000和约140,000的多肽。用甲状腺球蛋白-琼脂糖凝胶吸附甲状腺炎血清后进行免疫沉淀,如果血清中含有抗微粒体抗体,则可消除抗甲状腺球蛋白成分,而不影响105,000道尔顿多肽的结合。在同样常见于器官特异性自身免疫的胃制备的微粒体膜制剂中未鉴定出类似物质。105,000道尔顿的成分不与菜豆凝集素亲和柱结合。我们得出结论,微粒体/微绒毛抗原的表位存在于分子量为105,000的低聚糖肽上,该肽可能由链内二硫键稳定,且与膜结合的甲状腺球蛋白不具有血清学反应性。

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