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携带R因子的铜绿假单胞菌对新型半合成抗生素阿米卡星的乙酰化作用。

Acetylation of amikacin, a new semisynthetic antibiotic, by Pseudomonas aeruginosa carrying an R factor.

作者信息

Kawabe H, Naito T, Mitsuhashi S

出版信息

Antimicrob Agents Chemother. 1975 Jan;7(1):50-4. doi: 10.1128/AAC.7.1.50.

Abstract

A clinical isolate Pseudomonas aeruginosa GN315 resistant to amikacin (AK), a new semisynthetic antibiotic, inactivated AK by acetylation. The acetylating enzyme was purified approximately 146-fold from a crude extract of GN315 by affinity chromatography. Fractionated samples obtained by affinity chromatography showed almost the same inactivation curves toward 3',4'-dideoxykanamycin B (DKB) and AK. Partially purified AK-acetylating enzyme inactivated DKB and kanamycin A but could not inactivate gentamicin C(1). The optimal pH for their inactivation was 6.0 to 7.0, and the pH curves for the inactivation of both drugs were almost the same. These facts indicate that AK and DKB are inactivated by the same aminoglycoside-acetylating enzyme. Through elemental analysis, the inactivated AK was found to be a monoacetylated product of AK. A sample of inactivated AK was purified and compared with a synthetic 6'-N-acetyl AK by thin-layer chromatography, and the results indicated that AK was inactivated by acetylation of the 6'-NH(2) group. The ultraviolet, infrared, and nuclear magnetic resonance spectra of the inactivated AK showed that AK was inactivated by the enzyme through acetylation of the amino group of 6'-amino-6'-deoxy-d-glucose moiety of AK. This enzyme, mediated by R factor, is capable of conferring resistance to AK, DKB, kanamycin, gentamicin, and sulfanilamide.

摘要

临床分离的对新型半合成抗生素阿米卡星(AK)耐药的铜绿假单胞菌GN315,通过乙酰化作用使AK失活。通过亲和层析从GN315的粗提物中纯化出乙酰化酶,纯化倍数约为146倍。亲和层析得到的分级分离样品对3',4'-二脱氧卡那霉素B(DKB)和AK显示出几乎相同的失活曲线。部分纯化的AK-乙酰化酶使DKB和卡那霉素A失活,但不能使庆大霉素C(1)失活。它们失活的最适pH为6.0至7.0,两种药物失活的pH曲线几乎相同。这些事实表明AK和DKB被同一种氨基糖苷乙酰化酶失活。通过元素分析,发现失活的AK是AK的单乙酰化产物。纯化失活的AK样品并通过薄层色谱与合成的6'-N-乙酰AK进行比较,结果表明AK通过6'-NH(2)基团的乙酰化而失活。失活的AK的紫外、红外和核磁共振光谱表明,AK通过该酶对AK的6'-氨基-6'-脱氧-D-葡萄糖部分的氨基进行乙酰化而失活。这种由R因子介导的酶能够赋予对AK、DKB、卡那霉素、庆大霉素和磺胺类药物的耐药性。

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