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与一名HIV感染患者的白色念珠菌亚菌株相关的稳定唑类耐药性。

Stable azole drug resistance associated with a substrain of Candida albicans from an HIV-infected patient.

作者信息

White T C, Pfaller M A, Rinaldi M G, Smith J, Redding S W

机构信息

Seattle Biomedical Research Institute, WA 98109, USA.

出版信息

Oral Dis. 1997 May;3 Suppl 1:S102-9. doi: 10.1111/j.1601-0825.1997.tb00336.x.

Abstract

Oral candidiasis is one of the earliest and most frequent complications of a failing immune system in HIV-infected individuals. For several years, oral candidiasis has been treated effectively with azole drugs, the one most frequently used is fluconazole. Unfortunately, extensive use of the drug for treatment and prophylaxis has led to treatment failure in an increasing number of patients. In most of these cases, strains of C. albicans isolated from the infection are less susceptible to fluconazole. The development of azole resistance in strains of C. albicans has been studied biochemically and more recently with molecular techniques. One excellent example of the development of azole resistance in C. albicans has been documented in a series of 17 C. albicans isolates from a single patient over a 2-year period. During this time, the patient experienced 14 episodes of oral candidiasis and was treated with increasing doses of fluconazole. Molecular and biochemical analyses confirms that the isolates are the same strain of C. albicans and that the resistance in these isolates is stable over 600 generations, suggesting that the changes in this strain are genetic in nature. In addition, the development of resistance is correlated with the identification of a substrain or variant of the original strain, as identified by restriction fragment length polymorphism (RFLP) analysis with the moderately repetitive probe, Ca3. The analysis of this series of isolates demonstrates that azole drug resistance is associated with several small genetic changes, each of which contributes to the overall resistance of the strain. Clearly, continual use of azole drugs by a patient can select for genetic changes that render oral candidiasis refractory to treatment.

摘要

口腔念珠菌病是人类免疫缺陷病毒(HIV)感染者免疫系统功能衰退最早且最常见的并发症之一。多年来,唑类药物一直有效地用于治疗口腔念珠菌病,其中最常用的是氟康唑。不幸的是,该药物在治疗和预防方面的广泛使用已导致越来越多的患者治疗失败。在大多数此类病例中,从感染中分离出的白色念珠菌菌株对氟康唑的敏感性降低。白色念珠菌菌株中唑类耐药性的产生已通过生化方法进行了研究,最近也采用了分子技术。在一名患者两年期间分离出的一系列17株白色念珠菌中,记录了一个白色念珠菌产生唑类耐药性的典型例子。在此期间,该患者经历了14次口腔念珠菌病发作,并接受了剂量递增的氟康唑治疗。分子和生化分析证实,这些分离株是同一株白色念珠菌,并且这些分离株的耐药性在600代中保持稳定,这表明该菌株的变化本质上是遗传性的。此外,耐药性的产生与通过使用中度重复探针Ca3进行限制性片段长度多态性(RFLP)分析鉴定出的原始菌株的一个亚菌株或变体相关。对这一系列分离株的分析表明,唑类药物耐药性与几个小的基因变化有关,每个变化都对菌株的总体耐药性有贡献。显然,患者持续使用唑类药物会选择导致口腔念珠菌病难以治疗的基因变化。

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