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鉴定出一种可预防氨基糖苷类毒性的过表达酵母基因。

Identification of an overexpressed yeast gene which prevents aminoglycoside toxicity.

作者信息

Prezant T R, Chaltraw W E, Fischel-Ghodsian N

机构信息

Ahmanson Department of Pediatrics, Steven Spielberg Pediatric Research Center, Los Angeles, CA, USA.

出版信息

Microbiology (Reading). 1996 Dec;142 ( Pt 12):3407-14. doi: 10.1099/13500872-142-12-3407.

Abstract

Aminoglycoside antibiotics, used to treat bacterial infections by interfering with proofreading during protein synthesis, cause sensorineural hearing loss in genetically susceptible individuals. The only aminoglycoside-hypersensitivity mutations which have been described in humans are in the mitochondrial 125 rRNA gene, potentially allowing increased antibiotic binding to mitochondrial ribosomes. To identify additional predisposing mutations, a yeast model system was used to isolate genes which interact with or bypass the effects of aminoglycoside antibiotics. A novel yeast gene was isolated which, in high copy, confers neomycin resistance to yeast transformants. The neomycin-resistance 1 gene (NEO1) encodes a potential 1151 as integral membrane protein, most homologous to the yeast DRS2 gene product, a Ca(2+)-ATPase involved in cytoplasmic ribosome assembly. The N-terminus of Neo1p is partially homologous to abrin A-chain, another protein which interacts with cytoplasmic ribosomes. Mutagenesis experiments demonstrate that the NEO1 product is essential for vegetative growth and that the drug-resistance phenotype requires ATPase function.

摘要

氨基糖苷类抗生素通过干扰蛋白质合成过程中的校对来治疗细菌感染,会使具有遗传易感性的个体发生感音神经性听力损失。人类中已描述的唯一氨基糖苷类超敏突变存在于线粒体125 rRNA基因中,这可能会增加抗生素与线粒体核糖体的结合。为了鉴定其他易感突变,使用酵母模型系统来分离与氨基糖苷类抗生素相互作用或绕过其作用的基因。分离出一个新的酵母基因,该基因以高拷贝形式赋予酵母转化体新霉素抗性。新霉素抗性1基因(NEO1)编码一种潜在的1151个氨基酸的整合膜蛋白,与酵母DRS2基因产物最同源,DRS2基因产物是一种参与细胞质核糖体组装的Ca(2+) -ATP酶。Neo1p的N末端与相思豆毒素A链部分同源,相思豆毒素A链是另一种与细胞质核糖体相互作用的蛋白质。诱变实验表明,NEO1产物对营养生长至关重要,且耐药表型需要ATP酶功能。

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