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关于源自牛血清白蛋白胰蛋白酶消化产物的胰岛素刺激肽生物活性的研究。

Studies on the biological activity of an insulin-stimulating peptide from a tryptic digest of bovine serum albumin.

作者信息

Ueno A, Arakaki N, Oribe T, Takeda Y

出版信息

Mol Cell Biochem. 1986 May;70(2):121-30. doi: 10.1007/BF00229427.

DOI:10.1007/BF00229427
PMID:3523209
Abstract

A two-chain polypeptide, which corresponds to amino acid residues 115-143 and 144-184(185) of bovine serum albumin, connected to each other by a disulfide bridge, potentiated the effects of insulin on glucose transport and glucose metabolism in isolated rat adipocytes. Although the peptide alone had little activity, it shifted the concentration-response curves of insulin-stimulated D-[1-14C]glucose oxidation, 2-deoxyglucose transport, and lipid synthesis from D-[U-14C]glucose to lower insulin concentrations. It also increased the maximal responses of these parameters to insulin. However, it did not affect insulin binding to adipocytes. The peptide protected insulin considerably from degradation, but this effect alone cannot account for its effect in increasing the maximal responses to the hormone, and even when degradation of a submaximal concentration of insulin was suppressed by bacitracin, the peptide still had an enhancing effect. These results suggest not only that the peptide influences a step distal to receptor-mediated insulin binding but also that inhibition of insulin degradation alone cannot explain its total effect. The peptide lost its insulin-stimulating activity completely when it was further digested with V8 or lysine-specific endopeptidase, or when it was reduced and then carboxamidomethylated or oxidized with performic acid. Similar active tryptic fragments were obtained from human and rat albumins. Insulin-stimulating peptides should be useful in studies on the mechanisms of insulin action including both the sensitivities and responsiveness of target cells to the hormone.

摘要

一种由两条链组成的多肽,对应于牛血清白蛋白的115 - 143和144 - 184(185)位氨基酸残基,通过二硫键相互连接,可增强胰岛素对分离的大鼠脂肪细胞中葡萄糖转运和葡萄糖代谢的作用。尽管该肽单独作用时活性很小,但它可将胰岛素刺激的D - [1 - 14C]葡萄糖氧化、2 - 脱氧葡萄糖转运以及从D - [U - 14C]葡萄糖合成脂质的浓度 - 反应曲线向较低的胰岛素浓度方向移动。它还增加了这些参数对胰岛素的最大反应。然而,它并不影响胰岛素与脂肪细胞的结合。该肽能显著保护胰岛素不被降解,但仅这一作用不能解释其增加对该激素最大反应的作用,即使杆菌肽抑制了次最大浓度胰岛素的降解,该肽仍有增强作用。这些结果表明,该肽不仅影响受体介导的胰岛素结合的下游步骤,而且仅抑制胰岛素降解不能解释其全部作用。当该肽用V8或赖氨酸特异性内肽酶进一步消化,或还原后进行羧甲基化或用过甲酸氧化时,它完全失去了胰岛素刺激活性。从人白蛋白和大鼠白蛋白中也获得了类似的活性胰蛋白酶片段。胰岛素刺激肽在胰岛素作用机制的研究中应是有用的,包括靶细胞对该激素的敏感性和反应性。

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Studies on the biological activity of an insulin-stimulating peptide from a tryptic digest of bovine serum albumin.关于源自牛血清白蛋白胰蛋白酶消化产物的胰岛素刺激肽生物活性的研究。
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引用本文的文献

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本文引用的文献

1
METABOLISM OF ISOLATED FAT CELLS. I. EFFECTS OF HORMONES ON GLUCOSE METABOLISM AND LIPOLYSIS.分离脂肪细胞的代谢。I. 激素对葡萄糖代谢和脂肪分解的影响。
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Microdetermination of long-chain fatty acids in plasma and tissues.血浆和组织中长链脂肪酸的微量测定
J Biol Chem. 1960 Sep;235:2595-9.
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Quantitative aspects of the reaction between insulin and insulin-binding antibody.胰岛素与胰岛素结合抗体之间反应的定量方面
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Effect of insulin fragments on biological activity of insulin and desoctapeptide insulin. II. Enhanced binding and mechanism studies.胰岛素片段对胰岛素及去八肽胰岛素生物活性的影响。II. 增强的结合作用及机制研究。
J Biol Chem. 1981 Sep 25;256(18):9445-9.
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Effect of insulin fragments on biological activity of insulin and desoctapeptide insulin. I. Potentiation of biological activities.胰岛素片段对胰岛素及去八肽胰岛素生物活性的影响。I. 生物活性的增强作用。
J Biol Chem. 1981 Sep 25;256(18):9441-4.
6
In vitro effects of a sulfonylurea on insulin action in adipocytes. Potentiation of insulin-stimulated hexose transport.一种磺脲类药物对脂肪细胞胰岛素作用的体外效应。增强胰岛素刺激的己糖转运。
J Clin Invest. 1981 Jul;68(1):85-90. doi: 10.1172/jci110257.
7
Evidence for modulation of insulin action and degradation independently of insulin binding.胰岛素作用和降解的调节与胰岛素结合无关的证据。
Am J Physiol. 1981 Mar;240(3):E325-32. doi: 10.1152/ajpendo.1981.240.3.E325.
8
The minimal amino acid sequence of the insulin-potentiating fragments of human growth hormone: its mechanism of action.人生长激素胰岛素增敏片段的最小氨基酸序列:其作用机制。
Diabetes. 1980 Oct;29(10):782-7. doi: 10.2337/diacare.20.10.782.
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Enhanced specific insulin binding and insulin action with C-terminal B-chain pentapeptide derived from insulin.源自胰岛素的B链C端五肽增强特异性胰岛素结合及胰岛素作用。
FEBS Lett. 1980 Sep 22;119(1):161-4. doi: 10.1016/0014-5793(80)81021-0.
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Mol Pharmacol. 1982 Nov;22(3):614-8.