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一种研究大鼠肝脏中内分泌调节的自噬和蛋白质降解的新方法。

A new method for the investigation of endocrine-regulated autophagy and protein degradation in rat liver.

作者信息

Bergamini E, Del Roso A, Fierabracci V, Gori Z, Masiello P, Masini M, Pollera M

机构信息

Instituto di Patologia Generale, Università di Pisa, Italy.

出版信息

Exp Mol Pathol. 1993 Aug;59(1):13-26. doi: 10.1006/exmp.1993.1023.

Abstract

The effect of the antilipolytic agent 3,5-dimethylpyrazole (DMP) on liver autophagy and protein degradation was studied on male young adult rats (200 g body wt) of the Sprague-Dawley strain by electron microscopy and short-term single-pass liver perfusion and HPLC amino acid assay in the perfusate. Treatment with DMP (12 mg/kg body wt) enlarged the lysosomal-autophagic compartment in liver cells in 30 min and increased significantly the concentrations of valine and total amino acid in blood plasma (taken at sacrifice) and valine concentration in the liver perfusate in 60 min. These effects of DMP stimulating liver were secondary to the metabolic and endocrine effects of the drug (which caused a decrease in FFA, glucose, and insulin and an increase in glucagon and corticosterone plasma levels with a shorter latency, about 15 min). The effects of DMP were compared to those of other treatments inducing liver autophagy and protein degradation in vivo. Alterations after DMP or glucagon injections were similar, but they were larger and lasted for a longer time with DMP administration. Treatment with vinblastine or chloroquine enlarged the lysosomal-autophagic compartment without increasing protein breakdown.

摘要

采用电子显微镜、短期单次肝脏灌注及灌注液中HPLC氨基酸分析方法,研究了解脂药物3,5 - 二甲基吡唑(DMP)对Sprague-Dawley品系雄性成年幼鼠(体重200 g)肝脏自噬和蛋白质降解的影响。用DMP(12 mg/kg体重)处理30分钟后,肝细胞内溶酶体自噬区室增大,60分钟时,血浆(处死时采集)中缬氨酸和总氨基酸浓度以及肝脏灌注液中缬氨酸浓度显著升高。DMP对肝脏的这些作用继发于该药物的代谢和内分泌作用(导致游离脂肪酸、葡萄糖和胰岛素水平降低,胰高血糖素和皮质酮血浆水平升高,潜伏期较短约15分钟)。将DMP的作用与其他在体内诱导肝脏自噬和蛋白质降解的处理方法的作用进行了比较。注射DMP或胰高血糖素后的变化相似,但DMP给药后的变化更大且持续时间更长。用长春碱或氯喹处理可使溶酶体自噬区室增大,但不会增加蛋白质分解。

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