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基于宿主-病原体相互作用模型的筛选检测方法鉴定了一组新型抗真菌苯并咪唑衍生物。

A screening assay based on host-pathogen interaction models identifies a set of novel antifungal benzimidazole derivatives.

机构信息

Fraunhofer Institute for Interfacial Engineering and Biotechnology, Nobelstr. 12, 70569 Stuttgart, Germany.

出版信息

Antimicrob Agents Chemother. 2011 Oct;55(10):4789-801. doi: 10.1128/AAC.01657-10. Epub 2011 Jul 11.

Abstract

Fungal infections are a serious health problem in clinics, especially in the immune-compromised patient. Disease ranges from widespread superficial infections like vulvovaginal infections to life-threatening systemic candidiasis. Especially for systemic mycoses, only a limited arsenal of antifungals is available. The most commonly used classes of antifungal compounds used include azoles, polyenes, and echinocandins. Due to emerging resistance to standard therapy, significant side effects, and high costs for several antifungals, there is a medical need for new antifungals in the clinic and general practice. In order to expand the arsenal of compounds with antifungal activities, we screened a compound library including more than 35,000 individual compounds derived from organic synthesis as well as combinatorial compound collections representing mixtures of compounds for antimycotic activity. In total, more than 100,000 compounds were screened using a new type of activity-selectivity assay, analyzing both the antifungal activity and the compatibility with human cells at the same time. One promising hit, an (S)-2-aminoalkyl benzimidazole derivative, was developed among a series of lead compounds showing potent antifungal activity. (S)-2-(1-Aminoisobutyl)-1-(3-chlorobenzyl) benzimidazole showed the highest antifungal activity and the best compatibility with human cells in several cell culture models and against a number of clinical isolates of several species of pathogenic Candida yeasts. Transcriptional profiling indicates that the newly discovered compound is a potential inhibitor of the ergosterol pathway, in contrast to other benzimidazole derivatives, which target microtubules.

摘要

真菌感染是临床中的一个严重健康问题,特别是在免疫功能低下的患者中。疾病范围从广泛的浅表感染,如外阴阴道感染,到危及生命的系统性念珠菌病。特别是对于系统性真菌感染,只有有限的抗真菌药物可供使用。最常用的抗真菌化合物类别包括唑类、多烯类和棘白菌素类。由于对标准治疗的耐药性不断出现、许多抗真菌药物的副作用显著且成本高昂,临床上和一般实践中都需要新的抗真菌药物。为了扩大具有抗真菌活性的化合物库,我们筛选了一个化合物库,其中包括超过 35000 种源自有机合成的单个化合物,以及代表抗真菌活性的化合物混合物的组合化合物库。总共使用一种新型的活性选择性测定法筛选了超过 100000 种化合物,同时分析了抗真菌活性和与人细胞的相容性。在一系列表现出强大抗真菌活性的先导化合物中,一种(S)-2-氨基烷基苯并咪唑衍生物是一种很有前途的候选药物。(S)-2-(1-氨基异丁基)-1-(3-氯苄基)苯并咪唑在几种细胞培养模型中和针对几种致病性念珠菌属酵母的一些临床分离株中表现出最高的抗真菌活性和与人细胞的最佳相容性。转录谱分析表明,这种新发现的化合物是一种潜在的麦角甾醇途径抑制剂,与其他靶向微管的苯并咪唑衍生物不同。

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