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Merck

Nogo-A downregulation improves insulin secretion in mice.

Diabetes (2013-01-01)
Claire B Bonal, Delphine E Baronnier, Caroline Pot, Mahdia Benkhoucha, Martin E Schwab, Patrice H Lalive, Pedro L Herrera
要旨

Type 2 diabetes (T2D) is characterized by β-cell dysfunction and the subsequent depletion of insulin production, usually in a context of increased peripheral insulin resistance. T2D patients are routinely treated with oral antidiabetic agents such as sulfonylureas or dipeptidyl peptidase-4 antagonists, which promote glucose- and incretin-dependent insulin secretion, respectively. Interestingly, insulin secretion may also be induced by neural stimulation. Here we report the expression of Nogo-A in β-cells. Nogo-A is a membrane protein that inhibits neurite outgrowth and cell migration in the central nervous system. We observed that Nogo-A-deficient mice display improved insulin secretion and glucose clearance. This was associated with a stronger parasympathetic input and higher sensitivity of β-cells to the cholinergic analog carbachol. Insulin secretion was also improved in diabetic db/db mice treated with neutralizing antibody against Nogo-A. Together, these findings suggest that promoting the vagal stimulation of insulin secretion through the selective inhibition of Nogo-A could be a novel therapeutic approach in T2D.

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Sigma-Aldrich
塩化カルバモイルコリン, ≥98% (titration), crystalline
塩化カルバモイルコリン, European Pharmacopoeia (EP) Reference Standard