基于结构的线粒体 α 碳酸酐酶抑制剂的探索作为抗肥胖药物开发的潜在先导物。
Structure based exploration of mitochondrial alpha carbonic anhydrase inhibitors as potential leads for anti-obesity drug development.
机构信息
Department of Pharmaceutical Chemistry, School of Pharmaceutical Sciences, Siksha 'O' Anusandhan (Deemed to be University), Bhubaneswar, 751003, Odisha, India.
School of Pharmaceutical Sciences and Research, Chhatrapati Shivaji Maharaj University, Panvel, Navi Mumbai, Maharashtra, 410221, India.
出版信息
Daru. 2024 Dec;32(2):907-924. doi: 10.1007/s40199-024-00535-w. Epub 2024 Sep 14.
BACKGROUND
Obesity has emerged as a major health challenge globally in the last two decades. Dysregulated fatty acid metabolism and de novo lipogenesis are prime causes for obesity development which ultimately trigger other co-morbid pathological conditions thereby risking life longevity. Fatty acid metabolism and de novo lipogenesis involve several biochemical steps both in cytosol and mitochondria. Reportedly, the high catalytically active mitochondrial carbonic anhydrases (CAVA/CAVB) regulate the intercellular depot of bicarbonate ions and catalyze the rapid carboxylation of pyruvate and acetyl-co-A to acetyl-co-A and malonate respectively, which are the precursors of fatty acid synthesis and lipogenesis. Several in vitro and in vivo investigations indicate inhibition of mitochondrial carbonic anhydrase isoforms interfere in the functioning of pyruvate, fatty acid and succinate pathways. Targeting of mitochondrial carbonic anhydrase isoforms (CAVA/CAVB) could thereby modulate gluconeogenetic as well as lipogenetic pathways and pave way for designing of novel leads in the development pipeline of anti-obesity medications.
METHODS
The present review unveils a diverse chemical space including synthetic sulphonamides, sulphamates, sulfamides and many natural bioactive molecules which selectively inhibit the mitochondrial isoform CAVA/CAVB with an emphasis on major state-of-art drug design strategies.
RESULTS
More than 60% similarity in the structural framework of the carbonic anhydrase isoforms has converged the drug design methods towards the development of isoform selective chemotypes. While the benzene sulphonamide derivatives selectively inhibit CAVA/CAVB in low nanomolar ranges depending on the substitutions on the phenyl ring, the sulpamates and sulpamides potently inhibit CAVB. The virtual screening and drug repurposing methods have also explored many non-sulphonamide chemical scaffolds which can potently inhibit CAVA.
CONCLUSION
The review could pave way for the development of novel and effective anti-obesity drugs which can modulate the energy metabolism.
背景
在过去的二十年中,肥胖已成为全球主要的健康挑战。脂肪酸代谢失调和从头合成脂肪是肥胖发展的主要原因,最终会引发其他合并病理状况,从而危及寿命。脂肪酸代谢和从头合成脂肪涉及细胞质和线粒体中的几个生化步骤。据报道,高催化活性的线粒体碳酸酐酶(CAVA/CAVB)调节细胞间的碳酸氢盐离子库,并催化丙酮酸和乙酰辅酶 A 的快速羧化,分别生成脂肪酸合成和脂肪生成的前体丙二酸盐和丙二酸盐。一些体外和体内研究表明,抑制线粒体碳酸酐酶同工型会干扰丙酮酸、脂肪酸和琥珀酸途径的功能。靶向线粒体碳酸酐酶同工型(CAVA/CAVB)可以调节糖异生和脂肪生成途径,并为开发抗肥胖药物的新先导化合物铺平道路。
方法
本综述揭示了一个多样化的化学空间,包括合成的磺胺类、硫酸盐、磺胺类和许多天然生物活性分子,它们选择性地抑制线粒体同工型 CAVA/CAVB,并重点介绍了主要的最新药物设计策略。
结果
碳酸酐酶同工型在结构框架上有超过 60%的相似性,这使得药物设计方法朝着开发同工型选择性化学型的方向发展。苯磺酰胺衍生物根据苯环上的取代基选择性地在纳摩尔范围内抑制 CAVA/CAVB,而磺酸盐和磺酰胺则强烈抑制 CAVB。虚拟筛选和药物再利用方法也探索了许多能够强烈抑制 CAVA 的非磺胺化学支架。
结论
该综述为开发能够调节能量代谢的新型有效抗肥胖药物铺平了道路。
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