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从一名格雷夫斯病患者体内开发出一种人单克隆抗体,该抗体可识别一种新型甲状腺膜抗原。

Development of a human monoclonal antibody from a Graves' disease patient that identifies a novel thyroid membrane antigen.

作者信息

Baker J R, Saunders N B, Kaulfersch W, Burman K D

机构信息

Transplant Immunology Service, Walter Reed Army Medical Center, Washington, DC 20307.

出版信息

J Immunol. 1988 Apr 15;140(8):2593-9.

PMID:2895790
Abstract

To investigate the interaction between antibodies and the thyroid gland in Graves' disease, PBL were harvested from seven Graves' disease patients and transformed into lymphoblasts by the addition of EBV in the presence of cyclosporine A. These lymphoblasts were cloned by limiting dilution and then assayed for binding activity to human thyroglobulin, thyroid-stimulating hormone, thyroid microsome, and thyroid as well as guinea pig fat cell membranes. Four patients' cells produced antibody that bound to at least one of the Ag; a single clone from one patient that bound equally well to both thyroid and guinea pig fat cell membranes (but not to other thyroid Ag) was selected for further evaluation. Fusion of these cells with SHM-D33 heteromyeloma cells yielded three cell lines that produced genetically identical mAb. Immunostaining of human thyrocytes with this mAb demonstrated an Ag present on both nuclear and cell membranes. This Ag was identified as an 18,000 m.w. protein band on Western blots of both human thyroid and guinea pig fat cell membranes. The mAb was also able to alter thyrocyte physiology as the short term incubation of this mAb with FRTL-5 cells in vitro inhibited thyroid-stimulating hormone-mediated production of cAMP. Thus, this mAb and the Ag it identifies may be relevant to Graves' disease.

摘要

为了研究格雷夫斯病中抗体与甲状腺之间的相互作用,从7例格雷夫斯病患者身上采集外周血淋巴细胞(PBL),并在环孢素A存在的情况下加入EBV将其转化为淋巴母细胞。通过有限稀释法对这些淋巴母细胞进行克隆,然后检测其与人甲状腺球蛋白、促甲状腺激素、甲状腺微粒体、甲状腺以及豚鼠脂肪细胞膜的结合活性。4例患者的细胞产生了与至少一种抗原结合的抗体;从一名患者中选择了一个与甲状腺和豚鼠脂肪细胞膜结合能力相同(但不与其他甲状腺抗原结合)的单克隆进行进一步评估。这些细胞与SHM-D33异骨髓瘤细胞融合产生了三个产生基因相同单克隆抗体(mAb)的细胞系。用该单克隆抗体对人甲状腺细胞进行免疫染色显示,在细胞核膜和细胞膜上均存在一种抗原。在人甲状腺和豚鼠脂肪细胞膜的蛋白质印迹上,这种抗原被鉴定为一条分子量为18,000的蛋白带。该单克隆抗体还能够改变甲状腺细胞的生理功能,因为在体外将该单克隆抗体与FRTL-5细胞短期孵育可抑制促甲状腺激素介导的环磷酸腺苷(cAMP)生成。因此,这种单克隆抗体及其识别的抗原可能与格雷夫斯病有关。

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