Novel tricyclic small molecule inhibitors of Nicotinamide N-methyltransferase for the treatment of metabolic disorders

烟酰胺 三环 代谢物 化学 生物化学 调节器 药理学 生物 立体化学 基因
作者
Sven Ruf,Sridharan Rajagopal,Sanjay Venkatachalapathi Kadnur,Mahanandeesha S. Hallur,Shilpa Rani,Rajendra Kristam,S. Srinivasan,Bharat Ravindra Zope,Pavan Kumar Gondrala,Indu N. Swamy,V. P. Rama Kishore Putta,Saravanan Kandan,Gernot Zech,Herman Schreuder,Christine Rudolph,Ralf Elvert,Joerg Czech,Swarnakumari Birudukota,Masood Siddiqui,Niranjan Naranapura Anand
出处
期刊:Scientific Reports [Nature Portfolio]
卷期号:12 (1) 被引量:19
标识
DOI:10.1038/s41598-022-19634-2
摘要

Nicotinamide N-methyltransferase (NNMT) is a metabolic regulator that catalyzes the methylation of nicotinamide (Nam) using the co-factor S-adenosyl-L-methionine to form 1-methyl-nicotinamide (MNA). Overexpression of NNMT and the presence of the active metabolite MNA is associated with a number of diseases including metabolic disorders. We conducted a high-throughput screening campaign that led to the identification of a tricyclic core as a potential NNMT small molecule inhibitor series. Elaborate medicinal chemistry efforts were undertaken and hundreds of analogs were synthesized to understand the structure activity relationship and structure property relationship of this tricyclic series. A lead molecule, JBSNF-000028, was identified that inhibits human and mouse NNMT activity, reduces MNA levels in mouse plasma, liver and adipose tissue, and drives insulin sensitization, glucose modulation and body weight reduction in a diet-induced obese mouse model of diabetes. The co-crystal structure showed that JBSNF-000028 binds below a hairpin structural motif at the nicotinamide pocket and stacks between Tyr-204 (from Hairpin) and Leu-164 (from central domain). JBSNF-000028 was inactive against a broad panel of targets related to metabolism and safety. Interestingly, the improvement in glucose tolerance upon treatment with JBSNF-000028 was also observed in NNMT knockout mice with diet-induced obesity, pointing towards the glucose-normalizing effect that may go beyond NNMT inhibition. JBSNF-000028 can be a potential therapeutic option for metabolic disorders and developmental studies are warranted.
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