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针对人胰岛素受体不同表位的单克隆抗体的胰岛素样和胰岛素抑制作用。

Insulin-like and insulin-inhibitory effects of monoclonal antibodies for different epitopes on the human insulin receptor.

作者信息

Taylor R, Soos M A, Wells A, Argyraki M, Siddle K

出版信息

Biochem J. 1987 Feb 15;242(1):123-9. doi: 10.1042/bj2420123.

Abstract

Monoclonal antibodies previously shown to react with five distinct epitopes on the human insulin receptor were tested for their metabolic effects on isolated human adipocytes. Two antibodies which reacted with receptor alpha-subunit and completely inhibited 125I-insulin binding mimicked the actions of insulin to stimulate lipogenesis from [14C]glucose and to inhibit catecholamine-induced lipolysis. On a molar basis, these antibodies were comparable in potency with insulin itself. Two other antibodies which decreased insulin binding only slightly or not at all also mimicked these metabolic effects of insulin. One of these antibodies reacted with receptor beta-subunit. In contrast, a further antibody which reacted with alpha-subunit and inhibited insulin binding did not affect basal lipogenesis or catecholamine-induced lipolysis, but was able to antagonize the effects of insulin on these processes. The same antibody antagonized the insulin-like effect of another antibody with which it competed in binding to insulin receptor, but not the effect of an antibody which bound independently to the receptor. It is concluded that binding of ligand at or close to the insulin-binding site is neither necessary nor sufficient to trigger insulin-like metabolic effects, which may rather depend on some general property of antibodies, such as their ability to cross-link and aggregate receptor molecules.

摘要

先前已证明能与人胰岛素受体上五个不同表位发生反应的单克隆抗体,被检测其对分离的人脂肪细胞的代谢作用。两种与受体α亚基反应并完全抑制¹²⁵I胰岛素结合的抗体,模拟了胰岛素刺激[¹⁴C]葡萄糖生成脂肪以及抑制儿茶酚胺诱导的脂肪分解的作用。按摩尔计算,这些抗体的效力与胰岛素本身相当。另外两种仅轻微降低或完全不降低胰岛素结合的抗体,也模拟了胰岛素的这些代谢作用。其中一种抗体与受体β亚基反应。相比之下,另一种与α亚基反应并抑制胰岛素结合的抗体,不影响基础脂肪生成或儿茶酚胺诱导的脂肪分解,但能够拮抗胰岛素对这些过程的作用。同一抗体拮抗了与其在结合胰岛素受体上存在竞争的另一种抗体的胰岛素样作用,但不拮抗独立结合于受体的抗体的作用。得出的结论是,在胰岛素结合位点处或其附近的配体结合,对于触发胰岛素样代谢作用既非必要条件也非充分条件,这些作用可能更多地取决于抗体的某些一般特性,比如它们交联和聚集受体分子的能力。

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