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翻译抑制剂环己酰亚胺、依米丁和嘌呤霉素在体内抑制小鼠肝实质细胞和胰腺腺泡细胞的细胞自噬。

Translational inhibitors cycloheximide, emetine, and puromycin inhibit cellular autophagy in mouse liver parenchymal and pancreatic acinar cells in vivo.

作者信息

Oliva O, László L, Pálfia Z, Réz G

机构信息

Dept. of General Zoology, Eötvös Univ. Budapest, Hungary.

出版信息

Acta Morphol Hung. 1991;39(2):79-85.

PMID:1789148
Abstract

The protein synthesis inhibitor cycloheximide is widely used (in vitro or in vivo) to inhibit the autophagic degradation of endogenous cellular proteins. Circumstantial evidence has been obtained largely from in vitro experiments for a similar effect of other translational inhibitors. In the present study, the in vivo effects of cycloheximide, emetine and puromycin on autophagy in murine exocrine pancreatic and liver cells were tested using electron microscopic morphometry. The experiments were based on the assumption that the autophagic compartment will regress if the formation of the vacuoles is blocked while degradation in the pre-existing vacuoles goes on. To make the measurements easier, autophagic compartment of the cells was greatly enlarged in both cell types by administering vinblastine (10 mg/kg b. wt.) for 2 h when the inhibitors were set on for an additional 30 min. During this half-an-hour, cycloheximide (0.2 mg/g b. wt.), emetine (0.12 mg/g b. wt.) and puromycin (0.2 mg/g b. wt.), respectively caused 58.5, 35.6, and 69.5% regression of the pancreatic and 46.7, 64.2, and 54.2% of the hepatocytic autophagic vacuole compartment. Thus, similarly to cycloheximide, both emetine and puromycin have proved to be inhibitors of autophagy in vivo. The results argue for a possible relationship between the synthesis and degradation of endogenous cellular proteins.

摘要

蛋白质合成抑制剂放线菌酮被广泛用于(体外或体内)抑制内源性细胞蛋白质的自噬降解。间接证据主要来自体外实验,表明其他翻译抑制剂也有类似作用。在本研究中,使用电子显微镜形态计量学检测了放线菌酮、吐根碱和嘌呤霉素对小鼠外分泌胰腺细胞和肝细胞自噬的体内作用。实验基于这样的假设:如果液泡形成受阻而先前存在的液泡中的降解仍在继续,自噬区室将会消退。为了便于测量,在加入抑制剂后再持续30分钟时,通过给予长春碱(10毫克/千克体重)2小时,使两种细胞类型的细胞自噬区室都大大扩大。在这半小时内,放线菌酮(0.2毫克/克体重)、吐根碱(0.12毫克/克体重)和嘌呤霉素(0.2毫克/克体重)分别使胰腺自噬泡区室消退58.5%、35.6%和69.5%,使肝细胞自噬泡区室消退46.7%、64.2%和54.2%。因此,与放线菌酮类似,吐根碱和嘌呤霉素在体内也被证明是自噬抑制剂。这些结果表明内源性细胞蛋白质的合成与降解之间可能存在关联。

相似文献

1
Translational inhibitors cycloheximide, emetine, and puromycin inhibit cellular autophagy in mouse liver parenchymal and pancreatic acinar cells in vivo.翻译抑制剂环己酰亚胺、依米丁和嘌呤霉素在体内抑制小鼠肝实质细胞和胰腺腺泡细胞的细胞自噬。
Acta Morphol Hung. 1991;39(2):79-85.
2
Effect of different protein synthesis inhibitors on the exocrine pancreatocytic autophagocytosis in vivo.不同蛋白质合成抑制剂对体内外分泌胰腺细胞自噬作用的影响
Acta Biol Hung. 1991;42(1-3):127-32.
3
Time course of vinblastine-induced cellular autophagy in the murine pancreatic acinar cells in vivo. Different regression rates of the autophagic compartment caused by cycloheximide given different times after the vinca alkaloid. A morphometric study.长春碱诱导的小鼠胰腺腺泡细胞体内细胞自噬的时间进程。在长春花生物碱给药后不同时间给予放线菌酮导致自噬区室的不同消退率。一项形态计量学研究。
Acta Biol Hung. 1991;42(1-3):119-26.
4
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Regression of autophagic vacuoles in pancreatic acinar, seminal vesicle epithelial, and liver parenchymal cells: a comparative morphometric study of the effect of vinblastine and leupeptin followed by cycloheximide treatment.胰腺腺泡细胞、精囊上皮细胞和肝实质细胞中自噬泡的消退:长春碱和亮抑酶肽联合环己酰亚胺处理效果的比较形态计量学研究
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