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基于噻吩并嘧啶的单膦酸酯(ThP-MP)对人法尼基焦磷酸合酶抑制剂的药效团映射

Pharmacophore Mapping of Thienopyrimidine-Based Monophosphonate (ThP-MP) Inhibitors of the Human Farnesyl Pyrophosphate Synthase.

作者信息

Park Jaeok, Leung Chun Yuen, Matralis Alexios N, Lacbay Cyrus M, Tsakos Michail, Fernandez De Troconiz Guillermo, Berghuis Albert M, Tsantrizos Youla S

机构信息

Department of Biochemistry, McGill University , 3649 Promenade Sir William Osler, Montreal, QC H3G 0B1, Canada.

Department of Chemistry, McGill University , 801 Sherbrooke Street West, Montreal, QC H3A 0B8, Canada.

出版信息

J Med Chem. 2017 Mar 9;60(5):2119-2134. doi: 10.1021/acs.jmedchem.6b01888. Epub 2017 Feb 28.

Abstract

The human farnesyl pyrophosphate synthase (hFPPS), a key regulatory enzyme in the mevalonate pathway, catalyzes the biosynthesis of the C-15 isoprenoid farnesyl pyrophosphate (FPP). FPP plays a crucial role in the post-translational prenylation of small GTPases that perform a plethora of cellular functions. Although hFPPS is a well-established therapeutic target for lytic bone diseases, the currently available bisphosphonate drugs exhibit poor cellular uptake and distribution into nonskeletal tissues. Recent drug discovery efforts have focused primarily on allosteric inhibition of hFPPS and the discovery of non-bisphosphonate drugs for potentially treating nonskeletal diseases. Hit-to-lead optimization of a new series of thienopyrimidine-based monosphosphonates (ThP-MPs) led to the identification of analogs with nanomolar potency in inhibiting hFPPS. Their interactions with the allosteric pocket of the enzyme were characterized by crystallography, and the results provide further insight into the pharmacophore requirements for allosteric inhibition.

摘要

人法尼基焦磷酸合酶(hFPPS)是甲羟戊酸途径中的关键调节酶,催化C-15类异戊二烯法尼基焦磷酸(FPP)的生物合成。FPP在执行多种细胞功能的小GTP酶的翻译后异戊二烯化中起关键作用。尽管hFPPS是溶骨性骨疾病公认的治疗靶点,但目前可用的双膦酸盐药物在细胞摄取和向非骨骼组织的分布方面表现不佳。最近的药物研发工作主要集中在hFPPS的变构抑制以及发现用于潜在治疗非骨骼疾病的非双膦酸盐药物。对一系列基于噻吩并嘧啶的单膦酸盐(ThP-MPs)进行从苗头化合物到先导化合物的优化,得到了对hFPPS具有纳摩尔级抑制效力的类似物。通过晶体学表征了它们与该酶变构口袋的相互作用,结果为变构抑制的药效团要求提供了进一步的见解。

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