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人生长激素和胰岛素样生长因子I对全身亮氨酸及蛋白质代谢评估的影响。

Effect of human growth hormone and insulin-like growth factor I on whole-body leucine and estimates of protein metabolism.

作者信息

Haymond M W, Horber F F, De Feo P, Kahn S E, Mauras N

机构信息

Nemours Children's Clinic, Jacksonville, FL 32207.

出版信息

Horm Res. 1993;40(1-3):92-4. doi: 10.1159/000183773.

DOI:10.1159/000183773
PMID:8300055
Abstract

Recombinant human growth hormone (rhGH) administration to normal volunteers increases estimates of whole-body and forearm protein synthesis but has little effect on rates of proteolysis in both the postabsorptive state and during meal absorption. In contrast, insulin decreases estimates of whole-body and forearm proteolysis while decreasing or, in the presence of infused (or ingested) amino acids, sustaining estimates of protein synthesis. We have used high-dose prednisone as a controlled model for protein catabolism in normal volunteers and demonstrated that glucocorticosteroids increase estimates of whole-body proteolysis and the oxidation of leucine with little or no effect on estimates of whole-body protein synthesis. We have recently demonstrated that high-dose rhGH together with prednisone prevents the protein-catabolic effects observed with treatment with prednisone alone, while inducing insulin resistance and increased secretion of proinsulin. GH is thought to mediate its effects via the generation of insulin-like growth factor I (IGF-I). However, high rates of infusion of rhIGF-I induce hypoglycemia and decrease estimates of whole-body proteolysis and suppress the secretion of GH, insulin and glucagon, suggesting a predominant insulin-like effect on protein and glucose metabolism. When rhIGF-I is infused at a rate that achieves plasma IGF-I concentrations similar to those observed during rhGH treatment and yet avoids hypoglycemia, estimates of proteolysis and protein synthesis were not affected in the absence or presence of prednisone treatment. When rhGH and rhIGF-I are administered simultaneously, nitrogen balance is remarkably improved. Thus, the mechanism of action of both rhGH and/or rhIGF-I on body protein metabolism remains to be elucidated.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

对正常志愿者给予重组人生长激素(rhGH)可提高全身和前臂蛋白质合成的估计值,但对吸收后状态及进餐吸收期间的蛋白水解速率影响甚微。相比之下,胰岛素可降低全身和前臂蛋白水解的估计值,同时在降低或(在输注或摄入氨基酸的情况下)维持蛋白质合成的估计值。我们使用高剂量泼尼松作为正常志愿者蛋白质分解代谢的对照模型,并证明糖皮质激素可提高全身蛋白水解的估计值以及亮氨酸的氧化,而对全身蛋白质合成的估计值影响很小或没有影响。我们最近证明,高剂量rhGH与泼尼松联合使用可预防单独使用泼尼松治疗时观察到的蛋白质分解代谢作用,同时诱导胰岛素抵抗并增加胰岛素原的分泌。生长激素被认为是通过产生胰岛素样生长因子I(IGF-I)来介导其作用的。然而,高剂量输注rhIGF-I会导致低血糖,并降低全身蛋白水解的估计值,抑制生长激素、胰岛素和胰高血糖素的分泌,这表明对蛋白质和葡萄糖代谢具有主要的胰岛素样作用。当以达到与rhGH治疗期间观察到的血浆IGF-I浓度相似但又避免低血糖的速率输注rhIGF-I时,无论是否进行泼尼松治疗,蛋白水解和蛋白质合成的估计值均不受影响。当同时给予rhGH和rhIGF-I时,氮平衡会显著改善。因此,rhGH和/或rhIGF-I对身体蛋白质代谢的作用机制仍有待阐明。(摘要截短至250字)

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