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高水平的葡萄糖-6-磷酸酶基因和蛋白表达反映了增殖性肝脏和糖尿病中的一种适应性反应。

High levels of glucose-6-phosphatase gene and protein expression reflect an adaptive response in proliferating liver and diabetes.

作者信息

Haber B A, Chin S, Chuang E, Buikhuisen W, Naji A, Taub R

机构信息

Department of Genetics, Children's Hospital of Philadelphia, Pennsylvania.

出版信息

J Clin Invest. 1995 Feb;95(2):832-41. doi: 10.1172/JCI117733.

Abstract

The regenerating liver after partial hepatectomy is one of the few physiologic models of cellular proliferation in the adult animal. During hepatic regeneration, the animal is able to maintain metabolic homeostasis despite the acute loss of two thirds of hepatic tissue. In examining the molecular mechanisms regulating hepatic regeneration, we isolated novel immediate-early genes that are rapidly induced as the remnant liver undergoes the transition from its normal quiescent state into the G1 phase of the cell cycle. One of the most rapidly and highly induced genes which we initially termed RL-1, encodes rat glucose-6-phosphatase (rG6Pase). G6Pase mRNA peaks at 30 min and 36-48 h after hepatectomy correlating with the first and second rounds of cell division. This finding is compatible with studies that showed that G6Pase enzyme activity increases during liver regeneration. However, the increase in G6Pase mRNA is much more dramatic, indicating that it is a more sensitive indicator of this regulation. G6Pase gene expression peaks in the perinatal time period in the liver and remains elevated during the first month of life. The expression of the G6Pase gene is also dramatically elevated in BB diabetic rats, again higher than the enzyme elevation, and its relative induction after partial hepatectomy is blunted in these animals. Insulin treatment of partially hepatectomized diabetic animals downregulates the expression of G6Pase mRNA. Using specific antibodies against G6Pase, we detect a 36-kD G6Pase protein, and its level is elevated in regenerating and diabetic livers. The pattern of G6Pase mRNA expression appears to reflect similar changes in insulin and glucagon levels which accompany diabetes and hepatic proliferation. The elevation of G6Pase expression in these conditions is indicative of its importance as a regulator of glucose homeostasis in normal and abnormal physiologic states.

摘要

部分肝切除术后再生的肝脏是成年动物中少数细胞增殖的生理模型之一。在肝脏再生过程中,尽管三分之二的肝组织急性丧失,动物仍能够维持代谢稳态。在研究调节肝脏再生的分子机制时,我们分离出了新的即刻早期基因,这些基因在残余肝脏从正常静止状态转变为细胞周期的G1期时被迅速诱导。我们最初称为RL-1的诱导最快且诱导程度最高的基因之一,编码大鼠葡萄糖-6-磷酸酶(rG6Pase)。肝切除术后30分钟和36 - 48小时,G6Pase mRNA达到峰值,这与第一轮和第二轮细胞分裂相关。这一发现与表明肝脏再生期间G6Pase酶活性增加的研究结果一致。然而,G6Pase mRNA的增加更为显著,表明它是这种调节的更敏感指标。G6Pase基因在肝脏围产期表达达到峰值,并在出生后的第一个月内保持升高。在BB糖尿病大鼠中,G6Pase基因的表达也显著升高,同样高于酶的升高水平,并且在这些动物中部分肝切除术后其相对诱导作用减弱。对部分肝切除的糖尿病动物进行胰岛素治疗可下调G6Pase mRNA的表达。使用针对G6Pase的特异性抗体,我们检测到一种36-kD的G6Pase蛋白,其水平在再生肝脏和糖尿病肝脏中升高。G6Pase mRNA的表达模式似乎反映了伴随糖尿病和肝脏增殖的胰岛素和胰高血糖素水平的类似变化。在这些情况下G6Pase表达的升高表明其作为正常和异常生理状态下葡萄糖稳态调节因子的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ac5/295564/402d95bdd985/jcinvest00024-0403-a.jpg

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