首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Recombinant human insulin-like growth factor I induces its own specific carrier protein in hypophysectomized and diabetic rats.
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Recombinant human insulin-like growth factor I induces its own specific carrier protein in hypophysectomized and diabetic rats.

机译:重组人胰岛素样生长因子I在垂体切除和糖尿病大鼠中诱导其自身的特异性载体蛋白。

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摘要

The physiology of the specific serum binding proteins which constitute the main storage pool for insulin-like growth factors (IGFs) in mammals is still incompletely understood. We have, therefore, investigated the regulation of these proteins in (i) hypophysectomized (hypox) rats infused with recombinant human growth hormone (rhGH) or recombinant human IGF 1 (rhIGF I) and (ii) streptozotocin-diabetic rats infused with insulin or rhIGF I. The main carrier protein, a GH-dependent complex of apparent molecular mass 200 kDa, contains N-glycosylated IGF-binding subunits (42, 45, and 49 kDa) that differ in their glycosyl but not in their protein moiety. These subunits are lacking in hypox and diabetic rats. They are induced by GH and insulin, respectively, and appear in the 200-kDa complex. Infusion of rhIGF I induces the subunits in both states; however, only in diabetic, not in hypox, rats do they form the 200-kDa complex. Glycosylated carrier protein subunits do not appear before 8 hr of rhIGF I infusion. During that period, hypox rats may become severely hypoglycemic. After 16 hr, glycosylated subunits are clearly induced, and blood sugar values are normal. We conclude: (i) The N-glycosylated subunits of the 200-kDa complex reflect the IGF I status. (ii) IGF I may mediate the induction of these subunits by GH. (iii) Significant association to the 200-kDa complex occurs only in the presence of GH. It is likely that GH, but not IGF I, induces a component, which itself does not bind IGF, but associates with the glycosylated IGF-binding subunits. (iv) The glycosylated subunits protect against IGF-induced hypoglycemia and may be involved in tissue-specific targeting of IGFs.
机译:尚不完全了解构成哺乳动物胰岛素样生长因子(IGF)主要储存库的特定血清结合蛋白的生理学。因此,我们已经研究了这些蛋白质在(i)注入重组人生长激素(rhGH)或重组人IGF 1(rhIGF I)的经hyphystomtomized(hypox)大鼠中的调节,以及(ii)注入胰岛素或胰岛素的链脲佐菌素糖尿病大鼠rhIGF I.主要载体蛋白是表观分子量为200 kDa的GH依赖性复合物,包含N-糖基化的IGF结合亚基(42、45和49 kDa),其糖基不同,但蛋白质部分不同。缺氧和糖尿病大鼠缺乏这些亚基。它们分别由GH和胰岛素诱导,并以200 kDa的复合物形式出现。输注rhIGF I会在两种状态下诱导亚基。然而,只有在糖尿病大鼠中,而在低氧大鼠中,它们才形成200 kDa的复合物。糖基化的载体蛋白亚基在rhIGF I输注8小时之前不会出现。在此期间,hypox大鼠可能会严重降血糖。 16小时后,明显诱导出糖基化的亚基,血糖值正常。我们得出以下结论:(i)200 kDa复合物的N-糖基化亚基反映了IGF I的状态。 (ii)IGF I可以介导GH诱导这些亚基的诱导。 (iii)仅在GH存在下才与200 kDa复合物显着缔合。 GH可能会诱导一种成分,但它本身不会结合IGF I,但它本身并不结合IGF,而是与糖基化的IGF结合亚基缔合。 (iv)糖基化的亚基可抵抗IGF引起的低血糖症,并可能参与IGF的组织特异性靶向。

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