SGLT2 inhibition reprograms systemic metabolism via FGF21-dependent and -independent mechanisms

Osataphan S.; Macchi C.; Singhal G.; Chimene-Weiss J.; Sales V.; Kozuka C.; Dreyfuss J.M.; Pan H.; Tangcharoenpaisan Y.; Morningstar J.; Gerszten R.; Patti M.-E.

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dc.contributor.author	Osataphan S.
dc.contributor.author	Macchi C.
dc.contributor.author	Singhal G.
dc.contributor.author	Chimene-Weiss J.
dc.contributor.author	Sales V.
dc.contributor.author	Kozuka C.
dc.contributor.author	Dreyfuss J.M.
dc.contributor.author	Pan H.
dc.contributor.author	Tangcharoenpaisan Y.
dc.contributor.author	Morningstar J.
dc.contributor.author	Gerszten R.
dc.contributor.author	Patti M.-E.
dc.date.accessioned	2021-04-05T03:03:33Z
dc.date.available	2021-04-05T03:03:33Z
dc.date.issued	2019
dc.identifier.issn	23793708
dc.identifier.other	2-s2.0-85062630085
dc.identifier.uri	https://ir.swu.ac.th/jspui/handle/123456789/12462
dc.identifier.uri	https://www.scopus.com/inward/record.uri?eid=2-s2.0-85062630085&doi=10.1172%2fjci.insight.123130&partnerID=40&md5=c24313c08333eed7ffc7fdbc42af7302
dc.description.abstract	Pharmacologic inhibition of the renal sodium/glucose cotransporter-2 induces glycosuria and reduces glycemia. Given that SGLT2 inhibitors (SGLT2i) reduce mortality and cardiovascular risk in type 2 diabetes, improved understanding of molecular mechanisms mediating these metabolic effects is required. Treatment of obese but nondiabetic mice with the SGLT2i canagliflozin (CANA) reduces adiposity, improves glucose tolerance despite reduced plasma insulin, increases plasma ketones, and improves plasma lipid profiles. Utilizing an integrated transcriptomic-metabolomics approach, we demonstrate that CANA modulates key nutrient-sensing pathways, with activation of 5' AMP-activated protein kinase (AMPK) and inhibition of mechanistic target of rapamycin (mTOR), independent of insulin or glucagon sensitivity or signaling. Moreover, CANA induces transcriptional reprogramming to activate catabolic pathways, increase fatty acid oxidation, reduce hepatic steatosis and diacylglycerol content, and increase hepatic and plasma levels of FGF21. Given that these phenotypes mirror the effects of FGF21 to promote lipid oxidation, ketogenesis, and reduction in adiposity, we hypothesized that FGF21 is required for CANA action. Using FGF21-null mice, we demonstrate that FGF21 is not required for SGLT2i-mediated induction of lipid oxidation and ketogenesis but is required for reduction in fat mass and activation of lipolysis. Taken together, these data demonstrate that SGLT2 inhibition triggers a fasting-like transcriptional and metabolic paradigm but requires FGF21 for reduction in adiposity.
dc.subject	canagliflozin
dc.subject	diacylglycerol
dc.subject	fibroblast growth factor
dc.subject	fibroblast growth factor 21
dc.subject	hydroxymethylglutaryl coenzyme A reductase kinase
dc.subject	insulin
dc.subject	ketone
dc.subject	lipid
dc.subject	rapamycin
dc.subject	Slc5a2 protein, mouse
dc.subject	sodium glucose cotransporter 2
dc.subject	animal
dc.subject	blood
dc.subject	C57BL mouse
dc.subject	diet restriction
dc.subject	drug effect
dc.subject	energy metabolism
dc.subject	fatty liver
dc.subject	genetics
dc.subject	glucose blood level
dc.subject	knockout mouse
dc.subject	lipid metabolism
dc.subject	liver
dc.subject	male
dc.subject	metabolism
dc.subject	mouse
dc.subject	non insulin dependent diabetes mellitus
dc.subject	nuclear reprogramming
dc.subject	obesity
dc.subject	pathology
dc.subject	pharmacology
dc.subject	signal transduction
dc.subject	Adiposity
dc.subject	AMP-Activated Protein Kinases
dc.subject	Animals
dc.subject	Blood Glucose
dc.subject	Canagliflozin
dc.subject	Cellular Reprogramming
dc.subject	Diabetes Mellitus, Type 2
dc.subject	Diglycerides
dc.subject	Energy Metabolism
dc.subject	Fasting
dc.subject	Fatty Liver
dc.subject	Fibroblast Growth Factors
dc.subject	Insulin
dc.subject	Ketones
dc.subject	Lipid Metabolism
dc.subject	Lipids
dc.subject	Liver
dc.subject	Male
dc.subject	Mice
dc.subject	Mice, Inbred C57BL
dc.subject	Mice, Knockout
dc.subject	Obesity
dc.subject	Signal Transduction
dc.subject	Sirolimus
dc.subject	Sodium-Glucose Transporter 2
dc.subject	Sodium-Glucose Transporter 2 Inhibitors
dc.title	SGLT2 inhibition reprograms systemic metabolism via FGF21-dependent and -independent mechanisms
dc.type	Article
dc.rights.holder	Scopus
dc.identifier.bibliograpycitation	JCI insight. Vol 4, No.5 (2019)
dc.identifier.doi	10.1172/jci.insight.123130