Antidiabetic activity of Vaccinium vitis-idaea, a medicinal plant from the traditional pharmacopeia of the James Bay Cree.

摘要

Type 2 diabetes in Canadian First Nations is three times higher than the national average. Poor prognosis is partly attributed to cultural inappropriateness of pharmaceutical products. Our project aims to develop culturally adapted diabetes treatment based on traditional medicine pharmacopoeia. Our team has identified 17 plants used to treat the symptoms of diabetes by the Cree of Eeyou Istchee (James Bay, Quebec). Among them, the ethanol extract of Vaccinium vitis-idaea berries was found to have an important stimulatory effect on glucose uptake in cultured skeletal muscle cells and adipocytes. The goal of this thesis was to elucidate the mechanisms of action of this plant product as well as to isolate and identify its active constituents using a bioassay-guided fractionation approach and finally to validate the antidiabetic activity in vivo. The extract of V.vitis enhanced glucose uptake in cultured C2C12 and L6 skeletal muscle cells and stimulated the translocation of GLUT4 transporters to the cell membrane of L6 cells. It mildly inhibited ADP-stimulated oxygen consumption in isolated rat liver mitochondria, an effect similar to that of metformin and consistent with metabolic stress and the consecutive activation of AMP-activated protein kinase (AMPK) pathway. The insulin pathway does not seem to be involved in V.vitis signaling.;Fractionation of this plant extract, guided by glucose uptake activity, resulted in the isolation of the active principles, quercetin-3-O -galactoside, quercetin, and quercetin-3-O-glucoside. Similar to the crude extract, the quercetin glycosides and the aglycone stimulated the AMPK pathway. However, only the aglycone inhibited ATP synthase in isolated mitochondria.;To validate the effect of V.vitis in vivo, the extract (1% in drinking water) was administered to KKAy mice for 10 days. Glycemia and body weight were significantly reduced by V.vitis . These effects were associated with decrease of food intake, suggesting that V.vitis reduces the appetite. The pair-fed study confirmed that the previous effects of V.vitis are almost mediated by its appetite reducing action. In addition, V. vitis-treatment increased the content of GLUT4 protein in skeletal muscle, stimulated the phosphorylation of ACC and increased the levels of PPAR-alpha in the liver of KKAy mice. These effects could be additives to the apetite controling effect of V. vitis.;In the course of bioguided-fractionation, caffeic acid methyl ester (CAME), a by-product of fractionation procedure, has been shown to potently stimulate glucose uptake in cultured skeletal muscle cells and therefore to have anti-diabetic potential. To identify other active caffeic acid (CA) derivatives and to elucidate their structure--activity and structure-toxicity relationships, twenty CA derivatives were tested. In addition to CAME, four compounds were found to stimulate glucose uptake and activate AMPK. Uncoupling of mitochondrial oxidative phosphorylation by these compounds resulted in metabolic stress which could explain the activation of AMPK. The activity required an intact caffeic acid moiety devoid of strongly ionized groups and was well correlated with lipophilicity and toxicity.;The results of the present thesis support a therapeutic potential for V.vitis, and its active compounds, as well as the CA family of compounds for the prevention and treatment of diabetes.;Keywords: Vaccinium vitis, type 2 diabetes, AMPK, ACC, PPAR-alpha, OPD, KKAy, GLUT4, natural health products, traditional medicine, Canadian boreal forest, Aboriginal populations of North America.