1. Haploinsufficiency of CYP8B1 associates with increased insulin sensitivity in humans
- Author
-
Zhong, Shiqi, Chevre, Raphael, Mayan, David Castano, Corliano, Maria, Cochran, Blake J., Sem, Kai Ping, van Dijk, Theo H., Peng, Jianhe, Tan, Liang Juin, Hartimath, Siddesh V., Ramasamy, Boominathan, Cheng, Peter, Groen, Albert K., Kuipers, Folkert, Goggi, Julian L., Drum, Chester, van Dam, Rob M., Tan, Ru San, Rye, Kerry-Anne, Hayden, Michael R., Cheng, Ching-Yu, Chacko, Shaji, Flannick, Jason, Sim, Xueling, Tan, Hong Chang, and Singaraja, Roshni R.
- Subjects
Insulin resistance -- Risk factors -- Development and progression ,Chenodeoxycholic acid -- Physiological aspects -- Health aspects ,Cytochrome P-450 -- Genetic aspects -- Physiological aspects -- Health aspects ,Muscles -- Health aspects -- Physiological aspects ,Health care industry - Abstract
BACKGROUND. Cytochrome P450 family 8 subfamily B member 1 (CYP8B1) generates 12[alpha]-hydroxylated bile acids (BAs) that are associated with insulin resistance in humans. METHODS. To determine whether reduced CYP8B1 activity improves insulin sensitivity, we sequenced CYP8B1 in individuals without diabetes and identified carriers of complete loss-of-function (CLOF) mutations utilizing functional assays. RESULTS. Mutation carriers had lower plasma 12[alpha]-hydroxylated/non-12[alpha]-hydroxylated BA and cholic acid (CA)/ chenodeoxycholic acid (CDCA) ratios compared with age-, sex-, and BMI-matched controls. During insulin clamps, hepatic glucose production was suppressed to a similar magnitude by insulin, but glucose infusion rates to maintain euglycemia were higher in mutation carriers, indicating increased peripheral insulin sensitivity. Consistently, a polymorphic CLOF CYP8B1 mutation associated with lower fasting insulin in the AMP-T2D-GENES study. Exposure of primary human muscle cells to mutationcarrier CA/CDCA ratios demonstrated increased FOXO1 activity, and upregulation of both insulin signaling and glucose uptake, which were mediated by increased CDCA. Inhibition of FOXO1 attenuated the CDCA-mediated increase in muscle insulin signaling and glucose uptake. We found that reduced CYP8B1 activity associates with increased insulin sensitivity in humans. CONCLUSION. Our findings suggest that increased circulatory CDCA due to reduced CYP8B1 activity increases skeletal muscle insulin sensitivity, contributing to increased whole-body insulin sensitization. FUNDING. Biomedical Research Council/National Medical Research Council of Singapore., Introduction Bile acids (BAs) are products of cholesterol catabolism, accounting for approximately 50% of daily cholesterol turnover in humans, and act as surfactants to promote intestinal lipid absorption (1). The [...]
- Published
- 2022
- Full Text
- View/download PDF