Discovery of an Orally Bioavailable Benzimidazole Diacylglycerol Acyltransferase 1 (DGAT1) Inhibitor That Suppresses Body Weight Gain in Diet-Induced Obese Dogs and Postprandial Triglycerides in Humans.
Katsumasa NakajimaRicardo ChatelainKevin B ClairmontRenee CommerfordGary M CoppolaThomas DanielsCornelia J ForsterThomas A GilmoreYongjin GongMonish JainAaron KanterYoungshin KwakJingzhou LiCharles D MeyersAlan D NeubertPaul SzklennikVivienne TedescoJames ThompsonDavid TruongQing YangBrian K HubbardMichael H Serrano-WuPublished in: Journal of medicinal chemistry (2017)
Modification of a gut restricted class of benzimidazole DGAT1 inhibitor 1 led to 9 with good oral bioavailability. The key structural changes to 1 include bioisosteric replacement of the amide with oxadiazole and α,α-dimethylation of the carboxylic acid, improving DGAT1 potency and gut permeability. Since DGAT1 is expressed in the small intestine, both 1 and 9 can suppress postprandial triglycerides during acute oral lipid challenges in rats and dogs. Interestingly, only 9 was found to be effective in suppressing body weight gain relative to control in a diet-induced obese dog model, suggesting the importance of systemic inhibition of DGAT1 for body weight control. 9 has advanced to clinical investigation and successfully suppressed postprandial triglycerides during an acute meal challenge in humans.
Keyphrases
- weight gain
- weight loss
- body mass index
- body weight
- birth weight
- liver failure
- blood glucose
- adipose tissue
- respiratory failure
- molecular docking
- signaling pathway
- metabolic syndrome
- high density
- drug induced
- type diabetes
- bariatric surgery
- small molecule
- high throughput
- hepatitis b virus
- skeletal muscle
- insulin resistance
- intensive care unit
- fatty acid
- blood pressure
- acute respiratory distress syndrome
- mechanical ventilation