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体内生长激素处理对大鼠肝细胞体外甘油三酯合成的刺激作用。

Stimulation of in vitro triglyceride synthesis in the rat hepatocyte by growth hormone treatment in vivo.

作者信息

Elam M B, Simkevich C P, Solomon S S, Wilcox H G, Heimberg M

机构信息

Veterans Administration Hospital Research Service, Memphis, Tennessee.

出版信息

Endocrinology. 1988 Apr;122(4):1397-402. doi: 10.1210/endo-122-4-1397.

Abstract

Hepatic fatty acid metabolism in the rat is sexually differentiated. Rates of esterification by the liver of fatty acid into triglyceride and other esterification products (phospholipid, diglyceride, cholesteryl esters) are higher in the female than in the male. There is evidence to suggest that GH feminizes other hepatic systems that exhibit sexual dimorphism, including hepatic steroid metabolism, PRL receptors, and estrogen binding. To investigate the role of GH in maintenance of the high rates of fatty acid esterification observed in the female, we assessed rates of [1-14C]oleic acid utilization by hepatocytes prepared from hypophysectomized (hypox) cortisol/T3-replaced female rats with an without continuous in vivo infusion of human (h) GH (5 micrograms/h). In addition, we assessed the effect of in vivo hGH treatment (5 micrograms/h) on [1-14C]oleic acid utilization in the normal male rat. Hypophysectomy was accompanied by a reduction in incorporation of [1-14C]oleic acid into products of esterification (triglyceride, phospholipid, diglyceride) and oxidation (CO2, ketone bodies). Continuous infusion of hGH (5 micrograms/h; 14 days) restored rates of fatty acid esterification in the hypox-cortisol/T3-replaced female rat, with the exception of cholesteryl esters. hGH infusion partially restored rates of fatty acid oxidation in the hypox cortisol/T3-replaced female rat. Treatment of the adult male rat with continuous infusion of hGH (5 micrograms/h; 7 days) resulted in increased rates of incorporation of [1-14C] oleic acid into triglyceride. In contrast, incorporation of oleic acid into phospholipid, diglyceride, and cholesteryl esters was unaltered. These results suggest that GH may be an important regulator of hepatic fatty acid metabolism.

摘要

大鼠肝脏脂肪酸代谢存在性别差异。雌性大鼠肝脏将脂肪酸酯化生成甘油三酯和其他酯化产物(磷脂、甘油二酯、胆固醇酯)的速率高于雄性。有证据表明,生长激素(GH)使其他表现出性别二态性的肝脏系统女性化,包括肝脏类固醇代谢、催乳素(PRL)受体和雌激素结合。为了研究GH在维持雌性大鼠中观察到的高脂肪酸酯化率中的作用,我们评估了从垂体切除(hypox)并用皮质醇/T3替代的雌性大鼠制备的肝细胞在有无连续体内输注人(h)GH(5微克/小时)的情况下对[1-14C]油酸的利用率。此外,我们评估了体内hGH治疗(5微克/小时)对正常雄性大鼠中[1-14C]油酸利用率的影响。垂体切除伴随着[1-14C]油酸掺入酯化产物(甘油三酯、磷脂、甘油二酯)和氧化产物(CO2、酮体)的减少。连续输注hGH(5微克/小时;14天)恢复了hypox-皮质醇/T3替代的雌性大鼠中脂肪酸酯化率,但胆固醇酯除外。hGH输注部分恢复了hypox皮质醇/T3替代的雌性大鼠中脂肪酸氧化率。对成年雄性大鼠连续输注hGH(5微克/小时;7天)导致[1-14C]油酸掺入甘油三酯的速率增加。相反,油酸掺入磷脂、甘油二酯和胆固醇酯的情况未改变。这些结果表明,GH可能是肝脏脂肪酸代谢的重要调节因子。

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