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首页> 外文期刊>Journal of Medicinal Chemistry >Des-acyl ghrelin fragments and analogues promote survival of pancreatic β-cells and human pancreatic islets and prevent diabetes in streptozotocin-treated rats
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Des-acyl ghrelin fragments and analogues promote survival of pancreatic β-cells and human pancreatic islets and prevent diabetes in streptozotocin-treated rats

机译:脱酰基生长素释放肽片段和类似物可促进链脲佐菌素治疗的大鼠胰腺β细胞和人类胰岛的存活并预防糖尿病

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摘要

Des-acyl ghrelin, although devoid of binding to ghrelin receptor (GRLN), exerts many biological effects, including regulation of glucose and lipid metabolism. Indeed, des-acyl ghrelin promotes pancreatic β-cell and human islet cell survival and prevents diabetes in streptozotocin (STZ) treated rats. We investigated whether des-acyl ghrelin fragments excluding serine ~3, which is essential for binding to GRLN, would display similar actions. Among the different compounds tested, des-acyl ghrelin _((6-13)) and des-acyl ghrelin _((6-13)) with alanine substitutions or cyclization, but not with d-amino acid substitutions, showed the best survival effect, similar to des-acyl ghrelin. Des-acyl ghrelin _((6-13)) even prevented diabetes in STZ-treated rats and protected human circulating angiogenic cells from oxidative stress and senescence, similar to des-acyl ghrelin. These results suggest that not only full-length des-acyl ghrelin but also short des-acyl ghrelin fragments have clear beneficial effects on several tissues in vitro and in vivo.
机译:脱酰基生长素释放肽尽管缺乏与生长素释放肽受体(GRLN)的结合,但发挥了许多生物学作用,包括调节葡萄糖和脂质代谢。实际上,去酰基生长素释放肽可促进链脲佐菌素(STZ)治疗的大鼠的胰腺β细胞和人类胰岛细胞存活,并预防糖尿病。我们研究了除丝氨酸〜3外的去酰基生长素释放肽片段是否对结合GRLN至关重要,而丝氨酸〜3除外。在测试的不同化合物中,具有丙氨酸取代或环化作用但不具有d-氨基酸取代作用的去酰基ghrelin _((6-13))和去酰基ghrelin _((6-13))显示了最佳的存活率效果类似于去酰基生长素释放肽。与去酰基生长素释放肽类似,去酰基生长激素释放肽_((6-13))甚至可以预防经STZ处理的大鼠的糖尿病,并保护人体循环血管生成细胞免受氧化应激和衰老。这些结果表明,不仅全长的脱酰基生长素释放肽,而且短的脱酰基生长素释放肽片段在体外和体内对几种组织都有明显的有益作用。

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