犬齿鱼胰高血糖素类似物可降低高血糖,并增强饮食诱导肥胖型糖尿病小鼠的胰岛素分泌和作用。
Dogfish glucagon analogues counter hyperglycaemia and enhance both insulin secretion and action in diet-induced obese diabetic mice.
机构信息
School of Biomedical Sciences, Saad Centre for Pharmacy and Diabetes, University of Ulster, Coleraine, UK.
出版信息
Diabetes Obes Metab. 2016 Oct;18(10):1013-24. doi: 10.1111/dom.12713. Epub 2016 Aug 15.
AIMS
To investigate the antidiabetic actions of three dogfish glucagon peptide analogues [known glucagon-like peptide-1 and glucagon receptor co-agonists] after chronic administration in diet-induced high-fat-diet-fed diabetic mice.
MATERIALS AND METHODS
National Institutes of Health Swiss mice were pre-conditioned to a high-fat diet (45% fat) for 100 days, and control mice were fed a normal diet (10% fat). Normal diet control and high-fat-fed control mice received twice-daily intraperitoneal (i.p.) saline injections, while the high-fat-fed treatment groups (n = 8) received twice-daily injections of exendin-4(1-39), [S2a]dogfish glucagon, [S2a]dogfish glucagon exendin-4(31-39) or [S2a]dogfish glucagon-Lys(30) -γ-glutamyl-PAL (25 nmol/kg body weight) for 51 days.
RESULTS
After dogfish glucagon analogue treatment, there was a rapid and sustained decrease in non-fasting blood glucose and an associated insulinotropic effect (analysis of variance, p < .05 to <.001) compared with saline-treated high-fat-fed controls. All peptide treatments significantly improved i.p. and oral glucose tolerance with concomitant increased insulin secretion compared with saline-treated high-fat-fed controls (p <.05 to <.001). After chronic treatment, no receptor desensitization was observed but insulin sensitivity was enhanced for all peptide-treated groups (p < .01 to <.001) except [S2a]dogfish glucagon. Both exendin-4 and [S2a]dogfish glucagon exendin-4(31-39) significantly reduced plasma triglyceride concentrations compared with those found in lean controls (p = .0105 and p = .0048, respectively). Pancreatic insulin content was not affected by peptide treatments but [S2a]dogfish glucagon and [S2a]dogfish glucagon exendin-4(31-39) decreased pancreatic glucagon by 28%-34% (p = .0221 and p = .0075, respectively). The percentage of β-cell area within islets was increased by exendin-4 and peptide analogue treatment groups compared with high-fat-fed controls and the β-cell area decreased (p < .05 to <.01).
CONCLUSIONS
Overall, dogfish glucagon co-agonist analogues had several beneficial metabolic effects, showing therapeutic potential for type 2 diabetes.
目的
研究三种狗鲨胰高血糖素肽类似物[已知的胰高血糖素样肽-1 和胰高血糖素受体共激动剂]在慢性给药于饮食诱导的高脂肪饮食喂养的糖尿病小鼠后的抗糖尿病作用。
材料和方法
美国国立卫生研究院瑞士小鼠预先适应高脂肪饮食(45%脂肪)100 天,对照小鼠喂食正常饮食(10%脂肪)。正常饮食对照组和高脂肪喂养对照组接受每日两次腹腔内(i.p.)生理盐水注射,而高脂肪喂养治疗组(n=8)接受每日两次 exendin-4(1-39)、[S2a]狗鲨胰高血糖素、[S2a]狗鲨胰高血糖素 exendin-4(31-39)或[S2a]狗鲨胰高血糖素-Lys(30)-γ-谷氨酰基-PAL(25 nmol/kg 体重)治疗 51 天。
结果
与生理盐水治疗的高脂肪喂养对照组相比,狗鲨胰高血糖素类似物治疗后,非空腹血糖迅速且持续下降,同时具有胰岛素促分泌作用(方差分析,p<.05 至<.001)。与生理盐水治疗的高脂肪喂养对照组相比,所有肽类治疗均显著改善了腹腔内和口服葡萄糖耐量,同时胰岛素分泌增加(p<.05 至<.001)。在慢性治疗后,没有观察到受体脱敏,但所有肽类治疗组的胰岛素敏感性都增强(p<.01 至<.001),除[S2a]狗鲨胰高血糖素外。与瘦对照组相比,exendin-4 和[S2a]狗鲨胰高血糖素 exendin-4(31-39)均显著降低了血浆甘油三酯浓度(p=.0105 和 p=.0048)。肽类治疗并未影响胰腺胰岛素含量,但[S2a]狗鲨胰高血糖素和[S2a]狗鲨胰高血糖素 exendin-4(31-39)使胰腺胰高血糖素降低了 28%-34%(p=.0221 和 p=.0075)。与高脂肪喂养对照组相比,exendin-4 和肽类似物治疗组的胰岛内β细胞面积增加,β细胞面积减少(p<.05 至<.01)。
结论
总体而言,狗鲨胰高血糖素共激动剂类似物具有多种有益的代谢作用,显示出治疗 2 型糖尿病的潜力。
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