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完整细胞中胰岛素受体与跨膜蛋白酪氨酸磷酸酶LAR之间的功能关联。

Functional association between the insulin receptor and the transmembrane protein-tyrosine phosphatase LAR in intact cells.

作者信息

Ahmad F, Goldstein B J

机构信息

Dorrance H. Hamilton Research Laboratories, Department of Medicine, Jefferson Medical College of Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA.

出版信息

J Biol Chem. 1997 Jan 3;272(1):448-57.

PMID:8995282
Abstract

The receptor-type protein-tyrosine phosphatase LAR (for leukocyte common antigen-related) has been implicated as a physiological regulator of the insulin receptor. To demonstrate a functional interaction between LAR and the insulin receptor, we incubated CHO cells overexpressing the human insulin receptor with an antibody to the extracellular domain of LAR and found a 47% decrease in insulin receptor autophosphorylation and kinase activity. A physical association between LAR and the insulin receptor was then shown by immunoprecipitation of LAR from cell lysates and immunoblotting with antibody to the insulin receptor, or vice versa. Up to 11.8% of the LAR protein in the lysates of CHO cells overexpressing both the insulin receptor and LAR co-immunoprecipitated with the insulin receptor. The LAR/insulin receptor association was related to the level of LAR or insulin receptor overexpression and was increased 6.5-fold by chemical cross-linking and 3.9-fold by treatment with insulin, suggesting that receptor activation influences the affinity of LAR for the insulin receptor. In insulin-stimulated rat liver, LAR was temporally enriched in endosomes with the insulin receptor, and incubation of endosomes with neutralizing LAR antibodies decreased insulin receptor dephosphorylation in situ by 28% (p = 0.01 versus control). These data provide more direct evidence of a role for LAR in the physiological regulation of insulin action at the receptor level.

摘要

受体型蛋白酪氨酸磷酸酶LAR(白细胞共同抗原相关)被认为是胰岛素受体的一种生理调节因子。为了证明LAR与胰岛素受体之间存在功能相互作用,我们用针对LAR细胞外结构域的抗体孵育过表达人胰岛素受体的CHO细胞,发现胰岛素受体自身磷酸化和激酶活性降低了47%。然后通过从细胞裂解物中免疫沉淀LAR并用胰岛素受体抗体进行免疫印迹,或反之亦然,证明了LAR与胰岛素受体之间存在物理关联。在同时过表达胰岛素受体和LAR的CHO细胞裂解物中,高达11.8%的LAR蛋白与胰岛素受体共免疫沉淀。LAR/胰岛素受体的关联与LAR或胰岛素受体的过表达水平有关,通过化学交联增加了6.5倍,通过胰岛素处理增加了3.9倍,这表明受体激活会影响LAR对胰岛素受体的亲和力。在胰岛素刺激的大鼠肝脏中,LAR与胰岛素受体在内涵体中暂时富集,用中和性LAR抗体孵育内涵体可使原位胰岛素受体去磷酸化降低28%(与对照相比,p = 0.01)。这些数据为LAR在受体水平对胰岛素作用的生理调节中的作用提供了更直接的证据。

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