[Design of Novel Carboxamides of Eremomycin and Vancomycin with 4- or 3-Amino Methyl Phenyl Boric Acid and Their Investigation].

Q4 Medicine Antibiotiki i Khimioterapiya Pub Date : 2015-01-01
E N Bychkova, A M Korolev, E N Olsufyeva, E P Mirchink, E B Isakova
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引用次数: 0

Abstract

Amidation of the end carboxyl group of eremomycin and vancomycin by pinacolinic 4- or 3-amino methyl phenyl boron acids esters in the presence of the condensing reagent PyBOP resulted in formation of novel carboxamides of the antibiotics (IIIa-VIa). After elimination of the pinacolinic group under mild hydrolysis in weak acid aqueous medium there formed the respective derivatives with a residue of the nonprotected boric acid (III-VI). It was shown that the activity of the 4-substituted derivatives of the borole-containing eremomycin and vancomycin practically was the same as that of the initial antibiotics, while higher than that of the respective 3-substituted derivatives of the borole-containing derivatives against 8 strains of grampositive bacteria.

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[4-或3-氨基甲基苯基硼酸的新型埃雷霉素和万古霉素羧胺的设计与研究]。
在冷凝试剂PyBOP的作用下,4-或3-氨基甲基苯基硼酸酯对伊雷霉素和万古霉素的末端羧基进行酰胺化反应,形成新型抗生素(IIIa-VIa)。在弱酸性水介质中轻度水解,消去了pinacolinic基团后,形成了相应的衍生物,其残基为无保护硼酸(III-VI)。结果表明,含硼罗勒衍生物的4-取代衍生物对8株革兰氏阳性菌的活性与初始抗生素基本相同,但高于含硼罗勒衍生物的3-取代衍生物。
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来源期刊
Antibiotiki i Khimioterapiya
Antibiotiki i Khimioterapiya Medicine-Infectious Diseases
CiteScore
0.80
自引率
0.00%
发文量
46
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