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奥昔康唑,一种新型咪唑衍生物。体外和体内抗真菌活性评估。

Oxiconazole, a new imidazole derivative. Evaluation of antifungal activity in vitro and in vivo.

作者信息

Polak A

出版信息

Arzneimittelforschung. 1982;32(1):17-24.

PMID:7037014
Abstract

The new imidazole derivative Z-[2,4-dichloro-2-imidazol-1-yl)acetophenone]-O-(2,4-dichlorobenzyl)-oxime nitrate (oxiconazole, Ro 13-8996) is characterized by a broad fungistatic spectrum against the agents of human mycoses in vitro. In addition, fungicidal activity of various degree was found in selected species (Aspergillus fumigatus, Cryptococcus neoformans, Candida albicans and Trichophyton mentagrophytes). Synthesis of DNA was inhibited by subinhibitory concentrations of oxiconazole in parallel to cell multiplication, whereas synthesis of RNA, protein and carbohydrate was decreased to a lesser extent. The most relevant findings was high topical activity in both trichophytosis in the guinea-pig and vaginal candidiasis in the rat. In these 2 models, oxiconazole proved to be more potent than several reference compounds from the group of imidazole antimycotics. Systemic oral activity of oxiconazole was also found in three mouse models, namely in dermal infection with T. mentagrophytes var. quinckeanum, systemic histoplasmosis and, just to a low degree, systemic candidiasis, but the compound proved to be inactive in cryptococcosis and aspergillosis in the mouse. Based on our findings, a clinical evaluation of oxiconazole as a topical antimycotic in human superficial mycosis, seems to be justified.

摘要

新型咪唑衍生物Z-[(2,4-二氯-2-咪唑-1-基)苯乙酮]-O-(2,4-二氯苄基)肟硝酸盐(奥昔康唑,Ro 13-8996)的特点是在体外对人类真菌病病原体具有广泛的抑菌谱。此外,在某些特定菌种(烟曲霉、新型隐球菌、白色念珠菌和须癣毛癣菌)中发现了不同程度的杀菌活性。亚抑制浓度的奥昔康唑在抑制细胞增殖的同时也抑制了DNA的合成,而RNA、蛋白质和碳水化合物的合成减少程度较小。最相关的发现是其在豚鼠皮肤癣菌病和大鼠阴道念珠菌病中均具有较高的局部活性。在这两种模型中,奥昔康唑被证明比咪唑类抗真菌药组中的几种对照化合物更有效。在三种小鼠模型中也发现了奥昔康唑的全身口服活性,即须癣毛癣菌变种昆克氏菌引起的皮肤感染、系统性组织胞浆菌病以及程度较低的系统性念珠菌病,但该化合物在小鼠隐球菌病和曲霉病中无活性。基于我们的研究结果,对奥昔康唑作为人类浅表真菌病局部抗真菌药进行临床评估似乎是合理的。

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