首页> 外文期刊>Phytomedicine : >Stevioside induces antihyperglycaemic, insulinotropic and glucagonostatic effects in vivo: studies in the diabetic Goto-Kakizaki (GK) rats.
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Stevioside induces antihyperglycaemic, insulinotropic and glucagonostatic effects in vivo: studies in the diabetic Goto-Kakizaki (GK) rats.

机译:甜菊糖在体内诱导抗高血糖,促胰岛素和促胰高血糖素作用:在糖尿病Goto-Kakizaki(GK)大鼠中的研究。

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摘要

Extracts of leaves from the plant Stevia rebaudiana Bertoni have been used in the traditional treatment of diabetes in Paraguay and Brazil. Recently, we demonstrated a direct insulinotropic effect in isolated mouse islets and the clonal beta cell line INS-1 of the glycoside stevioside that is present in large quantity in these leaves. Type 2 diabetes is a chronic metabolic disorder that results from defects in both insulin and glucagon secretion as well as insulin action. In the present study we wanted to unravel if stevioside in vivo exerts an antihyperglycaemic effect in a nonobese animal model of type 2 diabetes. An i.v. glucose tolerance test (IVGT) was carried out with and without stevioside in the type 2 diabetic Goto-Kakizaki (GK) rat, as well as in the normal Wistar rat. Stevioside (0.2 g/kg BW) and D-glucose (2.0 g/kg BW) were administered as i.v. bolus injections in anaesthetized rats. Stevioside significantly suppressed the glucose response to the IVGT in GK rats (incremental area under the curve (IAUC): 648 +/- 50 (stevioside) vs 958 +/- 85 mM x 120 min (control); P < 0.05) and concomitantly increased the insulin response (IAUC: 51116 +/- 10967 (stevioside) vs 21548 +/- 3101 microU x 120 min (control); P < 0.05). Interestingly, the glucagon level was suppressed by stevioside during the IVGT, (total area under the curve (TAUC): 5720 +/- 922 (stevioside) vs 8713 +/- 901 pg/ml x 120 min (control); P < 0.05). In the normal Wistar rat stevioside enhanced insulin levels above basal during the IVGT (IAUC: 79913 +/- 3107 (stevioside) vs 17347 +/- 2882 microU x 120 min (control); P < 0.001), however, without altering the blood glucose response (IAUC: 416 +/- 43 (stevioside) vs 417 +/- 47 mM x 120 min (control)) or the glucagon levels (TAUC: 5493 +/- 527 (stevioside) vs 5033 +/- 264 pg/ml x 120 min (control)). In conclusion, stevioside exerts antihyperglycaemic, insulinotropic, and glucagonostatic actions in the type 2 diabetic GK rat, and may have the potential of becoming a new antidiabetic drug for use in type 2 diabetes.
机译:来自甜叶菊甜叶菊的叶子的提取物已在巴拉圭和巴西用于糖尿病的传统治疗。最近,我们证明了在分离的小鼠胰岛和糖苷甜菊糖苷的克隆β细胞系INS-1中具有直接的促胰岛素作用,而这些甜叶菊糖苷在这些叶片中大量存在。 2型糖尿病是一种慢性代谢性疾病,由胰岛素和胰高血糖素分泌以及胰岛素作用的缺陷引起。在本研究中,我们想弄清楚甜菊糖在体内是否在2型糖尿病的非肥胖动物模型中具有降血糖作用。 i.v.在2型糖尿病Goto-Kakizaki(GK)大鼠以及正常Wistar大鼠中,在有和没有甜菊糖的情况下进行了葡萄糖耐量试验(IVGT)。静脉注射甜菊糖苷(0.2 g / kg体重)和D-葡萄糖(2.0 g / kg体重)。麻醉大鼠大剂量注射。甜菊糖苷可显着抑制GK大鼠对IVGT的葡萄糖反应(曲线下的增量面积(IAUC):648 +/- 50(甜菊糖苷)vs 958 +/- 85 mM x 120分钟(对照组); P <0.05)增加了胰岛素反应(IAUC:51116 +/- 10967(甜菊糖苷)与21548 +/- 3101 microU x 120分钟(对照); P <0.05)。有趣的是,IVGT期间甜菊糖苷抑制了胰高血糖素水平(曲线下总面积(TAUC):5720 +/- 922(甜菊糖苷)与8713 +/- 901 pg / ml x 120分钟(对照); P <0.05 )。在正常Wistar大鼠中,甜菊糖苷在IVGT期间将胰岛素水平提高至高于基础水平(IAUC:79913 +/- 3107(甜菊糖苷)与17347 +/- 2882 microU x 120分钟(对照); P <0.001),但未改变血液葡萄糖反应(IAUC:416 +/- 43(甜菊糖苷)vs 417 +/- 47 mM x 120分钟(对照))或胰高血糖素水平(TAUC:5493 +/- 527(甜菊糖苷)vs 5033 +/- 264 pg / ml x 120分钟(对照))。总之,甜菊糖苷在2型糖尿病GK大鼠中具有降血糖,促胰岛素和促胰高血糖素的作用,并且可能具有成为2型糖尿病中使用的新型抗糖尿病药的潜力。

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