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奇霉素能大幅降低大肠杆菌延伸因子Tu对氨酰tRNA的亲和力。

Kirromycin drastically reduces the affinity of Escherichia coli elongation factor Tu for aminoacyl-tRNA.

作者信息

Abrahams J P, van Raaij M J, Ott G, Kraal B, Bosch L

机构信息

Department of Biochemistry, Leiden University, The Netherlands.

出版信息

Biochemistry. 1991 Jul 9;30(27):6705-10. doi: 10.1021/bi00241a010.

Abstract

We have studied the interaction between EF-Tu-GDP or EF-Tu-GTP in complex with kirromycin or aurodox (N1-methylkirromycin) and aminoacyl-tRNA, N-acetylaminoacyl-tRNA, or deacylated tRNA. Three independent methods were used: zone-interference gel electrophoresis, GTPase stimulation, and fluorescence. All three methods revealed that kirromycin induces a severe drop in the stability of the complex of EF-Tu-GTP and aminoacyl-tRNA of about 3 orders of magnitude. The affinities of EF-Tu-kirromycin-GTP and EF-Tu-kirromycin-GDP for aa-tRNA were found to be of about the same order of magnitude. We conclude that kirromycin and related compounds do not induce a so-called GTP-like conformation of EF-Tu with respect to tRNA binding. The findings shed new light on the mechanism of action of the antibiotic during the elongation cycle. In contrast to indirect evidence previously obtained in our laboratory [Van Noort et al. (1982) EMBO J. 1, 1199-1205; Van Noort et al. (1986) Proc. Natl. Acad. Sci. U.S.A. 71, 4910-4914], we were unable to demonstrate complexes of EF-Tu-aurodox-GTP/GDP with N-acetylaminoacyl-tRNA or deacylated tRNA by direct detection using zone-interference gel electrophoresis. Modification with N-tosyl-L-phenylalanine chloromethyl ketone (TPCK) decreases the affinity of EF-Tu-kirromycin-GTP for aminoacyl-tRNA, just like it does in the absence of the antibiotic.

摘要

我们研究了与奇霉素或奥多霉素(N1-甲基奇霉素)结合的EF-Tu-GDP或EF-Tu-GTP与氨酰-tRNA、N-乙酰氨酰-tRNA或脱酰基tRNA之间的相互作用。使用了三种独立的方法:区带干涉凝胶电泳、GTP酶刺激和荧光法。所有这三种方法均表明,奇霉素会使EF-Tu-GTP与氨酰-tRNA复合物的稳定性急剧下降约3个数量级。发现EF-Tu-奇霉素-GTP和EF-Tu-奇霉素-GDP对氨酰-tRNA的亲和力处于相同的数量级。我们得出结论,就tRNA结合而言,奇霉素及相关化合物不会诱导EF-Tu呈现所谓的GTP样构象。这些发现为抗生素在延伸循环中的作用机制提供了新的线索。与我们实验室之前获得的间接证据[Van Noort等人(1982年),《欧洲分子生物学组织杂志》1,1199 - 1205;Van Noort等人(1986年),《美国国家科学院院刊》71,4910 - 4914]相反,我们无法通过区带干涉凝胶电泳直接检测到EF-Tu-奥多霉素-GTP/GDP与N-乙酰氨酰-tRNA或脱酰基tRNA的复合物。用N-甲苯磺酰-L-苯丙氨酸氯甲基酮(TPCK)修饰会降低EF-Tu-奇霉素-GTP对氨酰-tRNA的亲和力,就如同在没有抗生素的情况下一样。

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