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四膜虫的溶酶体生理学。3. 关于酸性水解酶释放以及二甲基苯并蒽颗粒摄取与排出的药理学研究。

Lysosomal physiology in Tetrahymena. 3. Pharmacological studies on acid hydrolase release and the ingestion and egestion of dimethylbenzanthracene particles.

作者信息

Rothstein T L, Blum J J

出版信息

J Cell Biol. 1974 Sep;62(3):844-59. doi: 10.1083/jcb.62.3.844.

Abstract

The ingestion of (14)C-labeled 9,10-dimethyl-1,2-benzanthracene particles, the extracellular release of acid phosphatase, ribonuclease, and alpha-glucosidase, and the egestion of preingested dimethylbenzanthracene particles by Tetrahymena taken from logarithmically growing cultures and resuspended in a dilute salt solution were followed in the presence of several pharmacologic agents. Serotonin, caffeine, and, to a lesser extent, dibutyryl cyclic AMP increased the rate of particle ingestion, but did not alter the rate of release of the three acid hydrolases studied. Added catecholamines did not affect either particle ingestion or acid hydrolase release, but particle ingestion was inhibited by the catecholamine antagonists, dichloroisoproterenol, desmethylimipramine, reserpine, and phenoxybenzamine. These drugs also increased the release of acid phosphatase and ribonuclease in 5-h incubations. Desmethylimipramine acted within 1 h to increase acid hydrolase release, but the effect of dichloroisoproterenol developed more slowly and was secondary to a change in cellular content of the hydrolases. Desmethylimipramine increased the energy of activation for the release of acid phosphatase, while dichloroisoproterenol did not. Both of these drugs enhanced the egestion of preingested dimethylbenzanthracene particles, supporting the view that acid hydrolase release occurs through a cytoproct egestion mechanism. Particle ingestion was also inhibited by colchicine, vinblastine, and cytochalasin B, but these agents had no effect on acid hydrolase release, thus further differentiating the properties of the ingestion mechanism from those of the egestion mechanism. It appears that both microtubules and microfilaments play a role in the ingestion process and that this process may be controlled in part by a cyclic AMP-mediated serotoninergic and adrenergic system.

摘要

在几种药理剂存在的情况下,追踪来自对数生长期培养物并重悬于稀盐溶液中的四膜虫对(14)C标记的9,10 - 二甲基 - 1,2 - 苯并蒽颗粒的摄取、酸性磷酸酶、核糖核酸酶和α - 葡萄糖苷酶的细胞外释放,以及预先摄取的二甲基苯并蒽颗粒的排出。血清素、咖啡因,以及在较小程度上的二丁酰环磷酸腺苷增加了颗粒摄取速率,但并未改变所研究的三种酸性水解酶的释放速率。添加的儿茶酚胺对颗粒摄取或酸性水解酶释放均无影响,但颗粒摄取受到儿茶酚胺拮抗剂二氯异丙肾上腺素、去甲丙咪嗪、利血平和酚苄明的抑制。这些药物在5小时孵育中也增加了酸性磷酸酶和核糖核酸酶的释放。去甲丙咪嗪在1小时内起作用增加酸性水解酶释放,但二氯异丙肾上腺素的作用发展较慢,且是水解酶细胞内含量变化的继发结果。去甲丙咪嗪增加了酸性磷酸酶释放的活化能,而二氯异丙肾上腺素则没有。这两种药物均增强了预先摄取的二甲基苯并蒽颗粒的排出,支持酸性水解酶释放通过胞肛排出机制发生的观点。秋水仙碱、长春碱和细胞松弛素B也抑制颗粒摄取,但这些药剂对酸性水解酶释放无影响,从而进一步区分了摄取机制与排出机制的特性。似乎微管和微丝在摄取过程中均起作用,并且该过程可能部分受环磷酸腺苷介导的血清素能和肾上腺素能系统控制。

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