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分析烟曲霉蛋白质组对卡泊芬净的反应。

Profiling the Aspergillus fumigatus proteome in response to caspofungin.

机构信息

Public Health Research Institute, University of Medicine and Dentistry of New Jersey UMDNJ, New Jersey Medical School, Newark, NJ 07103, USA.

出版信息

Antimicrob Agents Chemother. 2011 Jan;55(1):146-54. doi: 10.1128/AAC.00884-10. Epub 2010 Oct 25.

Abstract

The proteomic response of Aspergillus fumigatus to caspofungin was evaluated by gel-free isobaric tagging for relative and absolute quantitation (iTRAQ) as a means to determine potential biomarkers of drug action. A cell fractionation approach yielding 4 subcellular compartment fractions was used to enhance the resolution of proteins for proteomic analysis. Using iTRAQ, a total of 471 unique proteins were identified in soluble and cell wall/plasma membrane fractions at 24 and 48 h of growth in rich media in a wild-type drug-susceptible strain. A total of 122 proteins showed at least a 2-fold change in relative abundance following exposure to caspofungin (CSF) at just below the minimum effective concentration (0.12 μg/ml). The largest changes were seen in the mitochondrial hypoxia response domain protein (AFUA_1G12250), the level of which decreased >16-fold in the secreted fraction, and ChiA1, the level of which decreased 12.1-fold in the cell wall/plasma membrane fraction. The level of the major allergen and cytotoxin AspF1 was also shown to decrease by 12.1-fold upon the addition of drug. A subsequent iTRAQ analysis of an echinocandin-resistant strain (fks1-S678P) was used to validate proteins specific to drug action. A total of 103 proteins in the 2 fractions tested by iTRAQ were differentially expressed in the wild-type susceptible strain but not significantly changed in the resistant strain. Of these potential biomarkers, 11 had levels that changed at least 12-fold. Microarray analysis of the susceptible strain was performed to evaluate the correlation between proteomics and genomics, with a total of 117 genes found to be changing at least 2-fold. Of these, a total of 22 proteins with significant changes identified by iTRAQ also showed significant gene expression level changes by microarray. Overall, these data have the potential to identify biomarkers that assess the relative efficacy of echinocandin drug therapy.

摘要

采用无标记相对和绝对定量(iTRAQ)的凝胶自由蛋白质组学方法来评估烟曲霉对卡泊芬净的蛋白质组反应,以确定药物作用的潜在生物标志物。采用细胞分级分离方法得到 4 个亚细胞区室级分,以增强蛋白质组分析的分辨率。使用 iTRAQ,在丰富培养基中生长 24 和 48 小时时,在野生型药物敏感株中鉴定出可溶性和细胞壁/质膜级分中 471 个独特的蛋白质。在低于最小有效浓度(0.12μg/ml)的卡泊芬净(CSF)暴露下,共有 122 个蛋白质的相对丰度至少增加了 2 倍。最大的变化发生在线粒体缺氧反应域蛋白(AFUA_1G12250),其在分泌级分中的水平降低了 16 倍以上,以及 ChiA1,其在细胞壁/质膜级分中的水平降低了 12.1 倍。添加药物后,主要过敏原和细胞毒素 AspF1 的水平也降低了 12.1 倍。随后对棘白菌素耐药株(fks1-S678P)进行 iTRAQ 分析,以验证特定于药物作用的蛋白质。通过 iTRAQ 测试的 2 个级分中的总共 103 个蛋白质在敏感野生型株中差异表达,但在耐药株中没有显著变化。在这些潜在的生物标志物中,有 11 个的水平变化至少 12 倍。对敏感株进行微阵列分析以评估蛋白质组学和基因组学之间的相关性,共发现 117 个基因的表达水平至少变化了 2 倍。在这些基因中,iTRAQ 鉴定出的总共 22 个具有显著变化的蛋白质也通过微阵列显示出显著的基因表达水平变化。总的来说,这些数据有可能确定评估棘白菌素药物治疗相对疗效的生物标志物。

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