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对酿酒酵母进行全基因组筛选,以鉴定真核生物抗生素不敏感性所需的基因。

Genome-wide screening of Saccharomyces cerevisiae to identify genes required for antibiotic insusceptibility of eukaryotes.

作者信息

Blackburn Alexandra S, Avery Simon V

机构信息

School of Life and Environmental Sciences, University of Nottingham, University Park, Nottingham NG7 2RD, United Kingdom.

出版信息

Antimicrob Agents Chemother. 2003 Feb;47(2):676-81. doi: 10.1128/AAC.47.2.676-681.2003.

Abstract

The adverse reactions provoked by many antibiotics in humans are well documented but are generally poorly understood at the molecular level. To elucidate potential genetic defects that could give rise to susceptibility to prokaryote-specific antibiotics in eukaryotes, we undertook genome-wide screens using the yeast Saccharomyces cerevisiae as a model of eukaryotes; our previous work with a small number of yeast mutants revealed some specific gene functions required for oxytetracycline resistance. Here, the complete yeast deletion strain collection was tested for growth in the presence of a range of antibiotics. The sensitivities of mutants revealed by these screens were validated in independent tests. None of the approximately 4,800 defined deletion strains tested were found to be sensitive to amoxicillin, penicillin G, rifampin, or vancomycin. However, two of the yeast mutants were tetracycline sensitive and four were oxytetracycline sensitive; encompassed among the latter were mutants carrying deletions in the same genes that we had characterized previously. Seventeen deletion strains were found to exhibit growth defects in the presence of gentamicin, with MICs for the strains being as low as 32 micro g ml(-1) (the wild type exhibited no growth defects at any gentamicin concentration tested up to 512 micro g ml(-1)). Strikingly, 11 of the strains that were most sensitive to gentamicin carried deletions in genes whose products are all involved in various aspects of vacuolar and Golgi complex (or endoplasmic reticulum) function. Therefore, these and analogous organelles, which are also the principal sites of gentamicin localization in human cells, appear to be essential for normal resistance to gentamicin in eukaryotes. The approach and data described here offer a new route to gaining insight into the potential genetic bases of antibiotic insusceptibilities in eukaryotes.

摘要

许多抗生素在人体中引发的不良反应已有充分记录,但在分子水平上通常了解甚少。为了阐明可能导致真核生物对原核生物特异性抗生素敏感的潜在基因缺陷,我们以酿酒酵母作为真核生物模型进行了全基因组筛选;我们之前对少数酵母突变体的研究揭示了一些四环素抗性所需的特定基因功能。在此,我们测试了完整的酵母缺失菌株库在一系列抗生素存在下的生长情况。通过这些筛选揭示的突变体敏感性在独立测试中得到了验证。在测试的约4800个明确的缺失菌株中,没有一个对阿莫西林、青霉素G、利福平或万古霉素敏感。然而,有两个酵母突变体对四环素敏感,四个对土霉素敏感;在后者中包括携带与我们之前鉴定的相同基因缺失的突变体。发现有17个缺失菌株在庆大霉素存在下表现出生长缺陷,这些菌株的最低抑菌浓度低至32μg/ml(野生型在高达512μg/ml的任何测试庆大霉素浓度下均未表现出生长缺陷)。引人注目的是,对庆大霉素最敏感的11个菌株携带的基因缺失,其产物都参与液泡和高尔基体复合体(或内质网)功能的各个方面。因此,这些以及类似的细胞器,它们也是庆大霉素在人体细胞中的主要定位位点,似乎对真核生物对庆大霉素的正常抗性至关重要。本文所述的方法和数据为深入了解真核生物抗生素不敏感性的潜在遗传基础提供了一条新途径。

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