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Treatment with a β-2-adrenoceptor agonist stimulates glucose uptake in skeletal muscle and improves glucose homeostasis, insulin resistance and hepatic steatosis in mice with diet-induced obesity.

Anastasia KalinovichNodi DehvariAlice ÅslundSten van BeekCarina HalleskogJessica OlsenElisabete ForsbergEvelyn ZacharewiczGert SchaartMia RindeAnna SandströmRoger BerlinClaes-Goran OstensonJoris HoeksTore Bengtsson
Published in: Diabetologia (2020)
Clenbuterol improved glucose tolerance after 4 days of treatment and these effects were maintained for up to 42 days. Effects were achieved with doses in a clinically relevant microgram range. Mechanistically, prolonged treatment with a low dose of clenbuterol improved glucose homeostasis in insulin resistant mice, most likely by stimulating glucose uptake in skeletal muscle and improving whole-body insulin sensitivity as well as by reducing hepatic lipids and glycogen. We conclude that selective β2-adrenergic agonists might be an attractive potential treatment for type 2 diabetes. This remains to be confirmed in humans. Graphical abstract.
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