T. Walsh, M. Kasai, A. Francesconi, D. Landsman, S. Chanock
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引用次数: 39
Abstract
Emergence of resistance of Candida albicans to antifungal triazoles is increasingly recognized as an important cause of refractory mucosal candidiasis in HIV-infected patients. Recently, CDR1, which is thought to be analogous to the human MDR-1 P-glycoprotein, has been cloned in C. albicans. It has been proposed that its expression is partially responsible for fluconazole resistance in C. albicans. This gene is characterized by the presence of an ATP binding cassette (ABC) region and is distinct from the BENr gene which does not encode such a functional domain. As the molecular basis for fluconazole resistance appears to be multifactorial, we considered that there may be other ATP binding cassette-containing MDR genes that may potentially contribute to antifungal azole resistance in C. albicans. We therefore sought to identify potential target sequences that may be derived from candidate genes that share homology with the ATP binding cassette region of the human MDR-1 P-glycoprotein. Degenerate oligonucleotide primers based on the known sequence from the ATP binding cassette region of the human MDR-1 P-glycoprotein were used to amplify PCR products within the range of 100 bp in length from C. albicans isolates (3 fluconazole-susceptible and 3 fluconazole-resistant). Sequence analysis of individually subcloned PCR products, derived from the six isolates revealed 34 sequences in total. The results of our study identified 14 clones (with at least one per isolate) with a high degree of homology to the ATP binding cassette of the human MDR-1 P-glycoprotein. The BLAST search did not disclose homology of these new sequences to the C. albicans CDR1 gene, suggesting that C. albicans may possess more than one MDR-like gene. We conclude that C. albicans may possess one or more additional genes encoding ATP binding cassette MDR-like proteins that are distinct from CDR 1 and which could participate in the development of fluconazole resistance.
白色念珠菌对抗真菌三唑的耐药性越来越被认为是hiv感染患者难治性粘膜念珠菌病的重要原因。最近,被认为与人类MDR-1 p -糖蛋白类似的CDR1在白色念珠菌中被克隆。有人提出它的表达是白色念珠菌对氟康唑耐药的部分原因。该基因的特点是存在ATP结合盒(ABC)区域,与不编码这种功能区域的BENr基因不同。由于氟康唑耐药的分子基础似乎是多因素的,我们认为可能存在其他含有ATP结合盒的MDR基因,可能有助于白色念珠菌抗真菌唑耐药。因此,我们试图确定可能来源于候选基因的潜在靶序列,这些候选基因与人MDR-1 p糖蛋白的ATP结合盒区具有同源性。利用人MDR-1 p -糖蛋白ATP结合盒区已知序列的退化寡核苷酸引物扩增白色念珠菌分离株(3株氟康唑敏感和3株氟康唑耐药)长度为100 bp的PCR产物。对6株分离株的亚克隆PCR产物进行序列分析,共发现34个序列。我们的研究结果确定了14个克隆(每个分离物至少一个)与人MDR-1 p -糖蛋白的ATP结合盒高度同源。BLAST搜索未发现这些新序列与白色念珠菌CDR1基因的同源性,这表明白色念珠菌可能拥有不止一个耐多药样基因。我们得出结论,白色念珠菌可能拥有一个或多个编码ATP结合盒耐多药样蛋白的额外基因,这些基因与CDR 1不同,可能参与氟康唑耐药的发展。
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