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含哌啶酸的放线菌素类似物:结构与生物活性的关系。

Actinomycin analogues containing pipecolic acid: relationship of structure to biological activity.

作者信息

Formica J V, Shatkin A J, Katz E

出版信息

J Bacteriol. 1968 Jun;95(6):2139-50. doi: 10.1128/jb.95.6.2139-2150.1968.

DOI:10.1128/jb.95.6.2139-2150.1968
PMID:4174667
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC315146/
Abstract

Streptomyces antibioticus synthesizes a mixture of actinomycins which differ at the "imino acid" site of the peptide chains. In the presence of exogenous pipecolic acid, several new actinomycins were synthesized and 70% of the proline in the antibiotic mixture was replaced by the analogue. Three new antibiotics (designated Pip 1alpha, Pip 1beta, and Pip 2) were isolated from culture filtrates, purified, and crystallized. The molar ratio of pipecolic acid to proline was: Pip 1alpha, 1:0; Pip 1beta, 1:1; Pip 2, 2:0. These compounds inhibited the growth and cell division of gram-positive, but not gram-negative, bacteria. The relative inhibitory activity against bacteria, Escherichia coli deoxyribonucleic acid (DNA)-dependent ribonucleic acid (RNA) polymerase in vitro, and RNA synthesis in Bacillus subtilis and mouse L-929 cells was: actinomycin IV = Pip 1beta > Pip 2 > Pip 1alpha. Protein synthesis in B. subtilis was less affected, and DNA synthesis was inhibited only at higher concentrations of antibiotic tested. In L cells, DNA formation was reduced less than RNA synthesis, whereas protein synthesis was not blocked under the experimental conditions employed. Kinetic studies with B. subtilis revealed that RNA synthesis was inhibited rapidly followed by an inhibition of protein synthesis. All four antibiotics markedly inhibited the replication of vaccinia virus and reovirus in tissue culture cells, but the production of poliovirus was resistant to the antibiotics. These actinomycins bind to DNA, resulting in an elevation of its T(m) and a decrease in the peak extinction of the actinomycins. The mode of action, as well as the structure-activity relationships among the actinomycins, are discussed relative to a previously proposed model of binding.

摘要

抗生链霉菌合成了多种在肽链“亚氨基酸”位点存在差异的放线菌素混合物。在外源哌啶酸存在的情况下,合成了几种新的放线菌素,抗生素混合物中70%的脯氨酸被该类似物取代。从培养滤液中分离出三种新抗生素(分别命名为Pip 1α、Pip 1β和Pip 2),并进行了纯化和结晶。哌啶酸与脯氨酸的摩尔比为:Pip 1α,1:0;Pip 1β,1:1;Pip 2,2:0。这些化合物抑制革兰氏阳性菌的生长和细胞分裂,但对革兰氏阴性菌无此作用。它们对细菌、体外大肠杆菌脱氧核糖核酸(DNA)依赖性核糖核酸(RNA)聚合酶以及枯草芽孢杆菌和小鼠L - 929细胞中RNA合成的相对抑制活性为:放线菌素IV = Pip 1β > Pip 2 > Pip 1α。枯草芽孢杆菌中的蛋白质合成受影响较小,只有在测试的抗生素浓度较高时DNA合成才受到抑制。在L细胞中,DNA形成的减少程度小于RNA合成,而在所采用的实验条件下蛋白质合成未被阻断。对枯草芽孢杆菌的动力学研究表明,RNA合成被迅速抑制,随后蛋白质合成也受到抑制。所有这四种抗生素都能显著抑制痘苗病毒和呼肠孤病毒在组织培养细胞中的复制,但脊髓灰质炎病毒的产生对这些抗生素具有抗性。这些放线菌素与DNA结合,导致其解链温度升高,同时放线菌素的峰值消光降低。结合先前提出的结合模型,讨论了放线菌素的作用方式以及它们之间的构效关系。

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引用本文的文献

1
Spectroscopic analysis of the equilibrium and kinetic DNA binding properties of several actinomycin analogs.几种放线菌素类似物的平衡及动力学DNA结合特性的光谱分析
Nucleic Acids Res. 1980 Mar 11;8(5):1121-32. doi: 10.1093/nar/8.5.1121.
2
Effect of pipecolic acid isomers on the biogenesis of actinomycins.哌可酸异构体对放线菌素生物合成的影响。
Antimicrob Agents Chemother. 1974 Mar;5(3):296-301. doi: 10.1128/AAC.5.3.296.
3
Novel actinomycins formed by biosynthetic incorporation of cis- and trans-4-methylproline.通过顺式和反式-4-甲基脯氨酸的生物合成掺入形成的新型放线菌素。
Antimicrob Agents Chemother. 1977 Jun;11(6):1056-63. doi: 10.1128/AAC.11.6.1056.
4
Production, isolation, and properties of azetomycins.氮杂霉素的制备、分离及性质
Antimicrob Agents Chemother. 1976 Feb;9(2):214-21. doi: 10.1128/AAC.9.2.214.
5
Glutamate-induced uptake of proline by Streptomyces antibioticus.谷氨酸诱导抗生链霉菌对脯氨酸的摄取。
J Bacteriol. 1978 May;134(2):546-54. doi: 10.1128/jb.134.2.546-554.1978.

本文引用的文献

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