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右旋苯丙胺抑制蛋白质合成的机制。

Mechanism of D-amphetamine inhibition of protein synthesis.

作者信息

Baliga B S, Zähringer J, Trachtenberg M, Moskowitz M A, Munro H N

出版信息

Biochim Biophys Acta. 1976 Aug 18;442(2):239-50. doi: 10.1016/0005-2787(76)90494-9.

Abstract

At 1 h after intraperitoneal administration of D-amphetamine sulphate (15 mg/kg), rat brain polyribosomes show disaggregation accompanied by reduced capacity for in vitro peptide chain elongation. The direct action of amphetamine on cell-fine protein-synthesizing systems was therefore explored. When brain or liver polyribosomes from untreated rats were incubated with pH 5 enzyme, peptide chain elongation was not inhibited by the addition 4 mM amphetamine to the medium. On the other hand, an initiation-dependent system consisting of rat liver of brain mRNA and wheat germ S-30 fraction showed inhibition of [3H]leucine incorporation by 50% when 4 mM amphetamine were added. The metabolites of amphetamine, p-hydroxyamphetamine and p-hydroxynorephedrine, had no inhibitory action in either system, but the potent neurotoxin p-chloroamphetamine was a more powerful inhibitor of initiation than amphetamine. By using [3H]amphetamine, it was shown that amphetamine binds to the 80-S ribosomes of the wheat germ system. This binding depended on the presence in the system of natural liver or brain mRNA or several synthetic mRNAs, but was not promoted by polyuridylic acid as the messenger. Significantly, polyuridylic acid-dependent polyphenylalanine synthesis by the wheat germ system was not inhibited by amphetamine or p-chloroamphetamine. Therefore, it was concluded that amphetamine inhibits protein synthesis by interfering with initiation through a step related to formation of the mRNA ribosome complex.

摘要

腹腔注射硫酸右苯丙胺(15毫克/千克)1小时后,大鼠脑多核糖体出现解聚,同时体外肽链延伸能力降低。因此,研究了苯丙胺对细胞精细蛋白质合成系统的直接作用。当将未处理大鼠的脑或肝多核糖体与pH 5酶一起孵育时,向培养基中添加4毫摩尔苯丙胺不会抑制肽链延伸。另一方面,由大鼠肝脑mRNA和小麦胚芽S-30组分组成的起始依赖性系统,当添加4毫摩尔苯丙胺时,[3H]亮氨酸掺入受到50%的抑制。苯丙胺的代谢产物对羟基苯丙胺和对羟基去甲麻黄碱在这两种系统中均无抑制作用,但强效神经毒素对氯苯丙胺是比苯丙胺更强的起始抑制剂。通过使用[3H]苯丙胺,表明苯丙胺与小麦胚芽系统的80-S核糖体结合。这种结合取决于系统中天然肝或脑mRNA或几种合成mRNA的存在,但不受聚尿苷酸作为信使的促进。值得注意的是,小麦胚芽系统中聚尿苷酸依赖性多聚苯丙氨酸合成不受苯丙胺或对氯苯丙胺的抑制。因此,得出结论,苯丙胺通过干扰与mRNA核糖体复合物形成相关的步骤来抑制蛋白质合成。

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