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曼氏血吸虫NAD⁺分解代谢酶强效抑制剂的发现

Discovery of Potent Inhibitors of Schistosoma mansoni NAD⁺ Catabolizing Enzyme.

作者信息

Jacques Sylvain A, Kuhn Isabelle, Koniev Oleksandr, Schuber Francis, Lund Frances E, Wagner Alain, Muller-Steffner Hélène, Kellenberger Esther

机构信息

†Laboratoire des Systèmes Chimiques Fonctionnels, MEDALIS Drug Discovery Center, Faculté de Pharmacie, CAMB UMR7199 CNRS/Université de Strasbourg, 67401 Illkirch, France.

‡Laboratoire d'Innovation Thérapeutique, MEDALIS Drug Discovery Center, Faculté de Pharmacie, LIT UMR7200 CNRS/Université de Strasbourg, 74 Route du Rhin, 67401 Illkirch, France.

出版信息

J Med Chem. 2015 Apr 23;58(8):3582-92. doi: 10.1021/acs.jmedchem.5b00203. Epub 2015 Apr 1.

Abstract

The blood fluke Schistosoma mansoni is the causative agent of the intestinal form of schistosomiasis (or bilharzia). Emergence of Schistosoma mansoni with reduced sensitivity to praziquantel, the drug currently used to treat this neglected disease, has underlined the need for development of new strategies to control schistosomiasis. Our ability to screen drug libraries for antischistosomal compounds has been hampered by the lack of validated S. mansoni targets. In the present work, we describe a virtual screening approach to identify inhibitors of S. mansoni NAD(+) catabolizing enzyme (SmNACE), a receptor enzyme suspected to be involved in immune evasion by the parasite at the adult stage. Docking of commercial libraries into a homology model of the enzyme has led to the discovery of two in vitro micromolar inhibitors. Further structure-activity relationship studies have allowed a 3-log gain in potency, accompanied by a largely enhanced selectivity for the parasitic enzyme over the human homologue CD38.

摘要

曼氏血吸虫是肠道型血吸虫病(或血吸虫病)的病原体。对目前用于治疗这种被忽视疾病的药物吡喹酮敏感性降低的曼氏血吸虫的出现,凸显了开发控制血吸虫病新策略的必要性。由于缺乏经过验证的曼氏血吸虫靶点,我们筛选抗血吸虫化合物药物库的能力受到了阻碍。在目前的工作中,我们描述了一种虚拟筛选方法,以鉴定曼氏血吸虫NAD(+)分解代谢酶(SmNACE)的抑制剂,该受体酶被怀疑在寄生虫成虫阶段参与免疫逃避。将商业库对接至该酶的同源模型中,发现了两种体外微摩尔级抑制剂。进一步的构效关系研究使效力提高了3个对数级,同时对寄生酶的选择性大大高于人类同源物CD38。

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