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首页> 外文期刊>Journal of Medicinal Chemistry >Re-emerging Aspartic Protease Targets: Examining Cryptococcus neoformans Major Aspartyl Peptidase 1 as a Target for Antifungal Drug Discovery
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Re-emerging Aspartic Protease Targets: Examining Cryptococcus neoformans Major Aspartyl Peptidase 1 as a Target for Antifungal Drug Discovery

机译:重新涌现天冬氨酸蛋白酶靶标:将密集的Crypoccus Neoformans主要阿氨酰肽酶1作为抗真菌药物发现的靶标

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摘要

Cryptococcosis is an invasive infection that accounts for 15% of AIDS-related fatalities. Still, treating cryptococcosis remains a significant challenge due to the poor availability of effective antifungal therapies and emergence of drug resistance. Interestingly, protease inhibitor components of antiretroviral therapy regimens have shown some clinical benefits in these opportunistic infections. We investigated Major aspartyl peptidase 1 (May1), a secreted Cryptococcus neoformans protease, as a possible target for the development of drugs that act against both fungal and retroviral aspartyl proteases. Here, we describe the biochemical characterization of May1, present its high-resolution X-ray structure, and provide its substrate specificity analysis. Through combinatorial screening of 11,520 compounds, we identified a potent inhibitor of May1 and HIV protease. This dual-specificity inhibitor exhibits antifungal activity in yeast culture, low cytotoxicity, and low off-target activity against host proteases and could thus serve as a lead compound for further development of May1 and HIV protease inhibitors.
机译:隐球菌病是一种侵袭性感染,占艾滋病相关死亡人数的15%。尽管如此,由于有效的抗真菌疗法的缺乏和耐药性的出现,治疗隐球菌病仍然是一个重大挑战。有趣的是,抗逆转录病毒治疗方案中的蛋白酶抑制剂成分在这些机会性感染中显示出一些临床益处。我们研究了主要天冬氨酸肽酶1(May1),一种分泌的新生隐球菌蛋白酶,作为开发同时作用于真菌和逆转录病毒天冬氨酸蛋白酶的药物的可能靶点。在这里,我们描述了May1的生化特性,展示了它的高分辨率X射线结构,并提供了它的底物特异性分析。通过对11520个化合物的组合筛选,我们确定了一种有效的May1和HIV蛋白酶抑制剂。这种双特异性抑制剂在酵母培养物中表现出抗真菌活性、低细胞毒性和对宿主蛋白酶的低脱靶活性,因此可以作为进一步开发May1和HIV蛋白酶抑制剂的先导化合物。

著录项

  • 来源
    《Journal of Medicinal Chemistry 》 |2021年第10期| 共14页
  • 作者单位

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Wroclaw Univ Sci &

    Technol Dept Chem Biol &

    Bioimaging PL-50370 Wroclaw Poland;

    Wroclaw Univ Sci &

    Technol Dept Chem Biol &

    Bioimaging PL-50370 Wroclaw Poland;

    Univ Calif San Francisco Dept Biochem &

    Biophys UCSF Genetech Hall San Francisco CA 94158 USA;

    Wroclaw Univ Sci &

    Technol Dept Chem Biol &

    Bioimaging PL-50370 Wroclaw Poland;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

    Univ Calif San Francisco Dept Biochem &

    Biophys UCSF Genetech Hall San Francisco CA 94158 USA;

    Univ Calif San Francisco Dept Pharmaceut Chem UCSF Genetech Hall San Francisco CA 94158 USA;

    Czech Acad Sci Inst Organ Chem &

    Biochem Prague 16610 6 Czech Republic;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学 ;
  • 关键词

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