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游离脂肪酸在有或无生长激素的情况下对人类禁食期间蛋白质保存的决定性作用。

The decisive role of free fatty acids for protein conservation during fasting in humans with and without growth hormone.

作者信息

Nørrelund Helene, Nair K Sreekumaran, Nielsen Steen, Frystyk Jan, Ivarsen Per, Jørgensen Jens Otto Lunde, Christiansen Jens Sandahl, Møller Niels

机构信息

Medical Department M (Endocrinology and Diabetes), Aarhus University Hospital, DK-8000 Aarhus C, Denmark.

出版信息

J Clin Endocrinol Metab. 2003 Sep;88(9):4371-8. doi: 10.1210/jc.2003-030267.

DOI:10.1210/jc.2003-030267
PMID:12970312
Abstract

During fasting, a lack of GH increases protein loss by close to 50%, but the underlying mechanisms remain uncertain. The present study tests the hypothesis that the anabolic actions of GH depend on mobilization of lipids. Seven normal subjects were examined on four occasions during a 37-h fast with infusion of somatostatin, insulin, and glucagon for the final 15 h: 1) with GH replacement, 2) with GH replacement and antilipolysis with acipimox, 3) without GH and with antilipolysis, and 4) with GH replacement, antilipolysis, and infusion of intralipid. Urinary urea excretion, serum urea concentrations, and muscle protein breakdown (assessed by labeled phenylalanine) increased by almost 50% during fasting with suppression of lipolysis. Addition of GH during fasting with antilipolysis did not influence indexes of protein degradation, whereas restoration of high FFA levels regenerated proportionally low concentrations of urea and decreased whole body protein degradation (phenylalanine to tyrosine conversion) by 10-15%, but failed to affect muscle protein metabolism. Thus, the present data provide strong evidence that FFA are important protein-sparing agents during fasting. The finding that inhibition of lipolysis eliminates the ability of GH to restrict fasting protein loss indicates that stimulation of lipolysis is the principal protein-conserving mechanism of GH.

摘要

在禁食期间,生长激素(GH)缺乏会使蛋白质损失增加近50%,但其潜在机制仍不确定。本研究检验了GH的合成代谢作用依赖于脂质动员这一假说。在37小时禁食期间,对7名正常受试者进行了4次检查,在最后15小时输注生长抑素、胰岛素和胰高血糖素:1)给予GH替代;2)给予GH替代并使用阿西莫司进行抗脂解;3)不给予GH但进行抗脂解;4)给予GH替代、抗脂解并输注脂肪乳剂。在禁食期间抑制脂解时,尿尿素排泄、血清尿素浓度和肌肉蛋白质分解(通过标记苯丙氨酸评估)增加了近50%。在禁食且进行抗脂解时添加GH并不影响蛋白质降解指标,而恢复高游离脂肪酸(FFA)水平可使尿素浓度相应降低,并使全身蛋白质降解(苯丙氨酸向酪氨酸转化)减少10 - 15%,但未能影响肌肉蛋白质代谢。因此,目前的数据提供了强有力的证据,表明FFA在禁食期间是重要的蛋白质节省剂。抑制脂解会消除GH限制禁食蛋白质损失的能力这一发现表明,刺激脂解是GH的主要蛋白质保护机制。

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