Regulation of glucokinase in pancreatic islets by prolactin: a mechanism for increasing glucose-stimulated insulin secretion during pregnancy

doi:10.1677/JOE-07-0043

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Regulation of glucokinase in pancreatic islets by prolactin: a mechanism for increasing glucose-stimulated insulin secretion during pregnancy

Anthony J Weinhaus, Laurence E Stout¹, Nicholas V Bhagroo¹, T Clark Brelje¹ and Robert L Sorenson¹

Department of Integrative Biology and Physiology, University of Minnesota, 6-125 Jackson Hall, 321 Church St SE, Minneapolis, Minnesota 55455-0303, USA
¹ Department of Genetics, Cell Biology and Development, University of Minnesota, Minneapolis, Minnesota, USA

(Requests for offprints should be addressed to R L Sorenson; Email: soren001{at}umn.edu)

Glucokinase activity is increased in pancreatic islets duringpregnancy and in vitro by prolactin (PRL). The underlying mechanismsthat lead to increased glucokinase have not been resolved. Sinceglucose itself regulates glucokinase activity in ß-cells,it was unclear whether the lactogen effects are direct or occurthrough changes in glucose metabolism. To clarify the rolesof glucose metabolism in this process, we examined the interactionsbetween glucose and PRL on glucose metabolism, insulin secretion,and glucokinase expression in insulin 1 (INS-1) cells and ratislets. Although the PRL-induced changes were more pronouncedafter culture at higher glucose concentrations, an increasein glucose metabolism, insulin secretion, and glucokinase expressionoccurred even in the absence of glucose. The presence of comparablelevels of insulin secretion at similar rates of glucose metabolismfrom both control and PRL-treated INS-1 cells suggests the PRL-inducedincrease in glucose metabolism is responsible for the increasein insulin secretion. Similarly, increases in other known PRLresponsive genes (e.g. the PRL receptor, glucose transporter-2,and insulin) were also detected after culture without glucose.We show that the upstream glucokinase promoter contains multipleSTAT5 binding sequences with increased binding in response toPRL. Corresponding increases in glucokinase mRNA and proteinsynthesis were also detected. This suggests the PRL-inducedincrease in glucokinase mRNA and its translation are sufficientto account for the elevated glucokinase activity in ß-cellswith lactogens. Importantly, the increase in islet glucokinaseobserved with PRL is in line with that observed in islets duringpregnancy.

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				S. Rieck, P. White, J. Schug, A. J. Fox, O. Smirnova, N. Gao, R. K. Gupta, Z. V. Wang, P. E. Scherer, M. P. Keller, et al. The Transcriptional Response of the Islet to Pregnancy in Mice Mol. Endocrinol., October 1, 2009; 23(10): 1702 - 1712. [Abstract] [Full Text] [PDF]

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