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格雷夫斯病血清中的抗促甲状腺素受体自身抗体与新生的、体外翻译的促甲状腺素受体的结合:绘制抗体识别表位的能力。

Binding of antithyrotropin receptor autoantibodies in Graves' disease serum to nascent, in vitro translated thyrotropin receptor: ability to map epitopes recognized by antibodies.

作者信息

Morgenthaler N G, Tremble J, Huang G, Scherbaum W A, McGregor A M, Banga J P

机构信息

Department of Medicine, King's College School of Medicine, London, United Kingdom.

出版信息

J Clin Endocrinol Metab. 1996 Feb;81(2):700-6. doi: 10.1210/jcem.81.2.8636291.

DOI:10.1210/jcem.81.2.8636291
PMID:8636291
Abstract

The binding of Graves' disease autoantibodies and xenogeneic antibodies to the human TSH receptor (TSH-R) has been studied using receptor preparations generated in an in vitro transcription and translation reaction. The complementary DNAs encoding for the full-length (764 amino acids) and the extracellular region of TSH-R (amino acids 20-414, lacking the signal sequence) were used to generate the translated receptor antigen. Stable [35S]methionine-labeled nascent protein for full-length and extracellular regions of TSH-R of approximate size 87 and 50 kDa, respectively, together with other smaller proteins were generated. The 87- and 50-kDa translated receptor proteins react by immunoprecipitation analysis with monoclonal antibodies, polyclonal antisera, and unfractionated Graves' disease serum containing autoantibody to TSH-R. The translated products of the extracellular TSH-R were examined in detail. Using three well characterized murine monoclonal antibodies whose epitopes encompass the amino-, central, and carboxyl-terminals of the extracellular region of the receptor led to immunochemical identification of the smaller translated products to derive from internal methionine start sites of TSH-R. These smaller, N-terminal-truncated translated proteins were also recognized by polyclonal antisera generated against recombinant TSH-R, thus allowing epitope mapping of some antibodies. A large proportion of Graves' disease autoantibodies (> 70%) bind to the translated extracellular region of TSH-R. This indicates that the majority of pathogenic anti-TSH-R autoantibody binds the nascent translated extracellular region of TSH-R, which is not influenced by the lack of glycosylation of the receptor.

摘要

利用体外转录和翻译反应产生的受体制剂,研究了格雷夫斯病自身抗体和异种抗体与人促甲状腺激素受体(TSH-R)的结合。编码全长(764个氨基酸)和TSH-R细胞外区域(氨基酸20 - 414,缺少信号序列)的互补DNA用于产生翻译后的受体抗原。分别产生了大小约为87 kDa和50 kDa的TSH-R全长和细胞外区域的稳定[35S]甲硫氨酸标记的新生蛋白,以及其他较小的蛋白。通过免疫沉淀分析,87 kDa和50 kDa的翻译后受体蛋白可与单克隆抗体、多克隆抗血清以及含有TSH-R自身抗体的未分级格雷夫斯病血清发生反应。对细胞外TSH-R的翻译产物进行了详细研究。使用三种特征明确的鼠单克隆抗体,其表位涵盖受体细胞外区域的氨基末端、中央区域和羧基末端,通过免疫化学鉴定发现较小的翻译产物源自TSH-R的内部甲硫氨酸起始位点。这些较小的、N末端截短的翻译蛋白也被针对重组TSH-R产生的多克隆抗血清所识别,从而实现了一些抗体的表位定位。很大一部分(> 70%)格雷夫斯病自身抗体与翻译后的TSH-R细胞外区域结合。这表明大多数致病性抗TSH-R自身抗体与TSH-R新生的翻译后细胞外区域结合,而这不受受体糖基化缺失的影响。

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Binding of antithyrotropin receptor autoantibodies in Graves' disease serum to nascent, in vitro translated thyrotropin receptor: ability to map epitopes recognized by antibodies.格雷夫斯病血清中的抗促甲状腺素受体自身抗体与新生的、体外翻译的促甲状腺素受体的结合:绘制抗体识别表位的能力。
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