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具有延长的胰高血糖素样肽-1受体激动剂和胰高血糖素受体拮抗剂活性的双功能肽,用于治疗2型糖尿病。

Dual-acting peptide with prolonged glucagon-like peptide-1 receptor agonist and glucagon receptor antagonist activity for the treatment of type 2 diabetes.

作者信息

Claus Thomas H, Pan Clark Q, Buxton Joanne M, Yang Ling, Reynolds Jennifer C, Barucci Nicole, Burns Michael, Ortiz Astrid A, Roczniak Steve, Livingston James N, Clairmont Kevin B, Whelan James P

机构信息

Bayer HealthCare, Biotechnology, 800 Dwight Way, Berkeley, CA 94701, USA.

出版信息

J Endocrinol. 2007 Feb;192(2):371-80. doi: 10.1677/JOE-06-0018.

DOI:10.1677/JOE-06-0018
PMID:17283237
Abstract

Type 2 diabetes is characterized by reduced insulin secretion from the pancreas and overproduction of glucose by the liver. Glucagon-like peptide-1 (GLP-1) promotes glucose-dependent insulin secretion from the pancreas, while glucagon promotes glucose output from the liver. Taking advantage of the homology between GLP-1 and glucagon, a GLP-1/glucagon hybrid peptide, dual-acting peptide for diabetes (DAPD), was identified with combined GLP-1 receptor agonist and glucagon receptor antagonist activity. To overcome its short plasma half-life DAPD was PEGylated, resulting in dramatically prolonged activity in vivo. PEGylated DAPD (PEG-DAPD) increases insulin and decreases glucose in a glucose tolerance test, evidence of GLP-1 receptor agonism. It also reduces blood glucose following a glucagon challenge and elevates fasting glucagon levels in mice, evidence of glucagon receptor antagonism. The PEG-DAPD effects on glucose tolerance are also observed in the presence of the GLP-1 antagonist peptide, exendin(9-39). An antidiabetic effect of PEG-DAPD is observed in db/db mice. Furthermore, PEGylation of DAPD eliminates the inhibition of gastrointestinal motility observed with GLP-1 and its analogues. Thus, PEG-DAPD has the potential to be developed as a novel dual-acting peptide to treat type 2 diabetes, with prolonged in vivo activity, and without the GI side-effects.

摘要

2型糖尿病的特征是胰腺胰岛素分泌减少以及肝脏葡萄糖过度生成。胰高血糖素样肽-1(GLP-1)促进胰腺葡萄糖依赖性胰岛素分泌,而胰高血糖素促进肝脏葡萄糖输出。利用GLP-1与胰高血糖素之间的同源性,鉴定出一种GLP-1/胰高血糖素杂合肽,即糖尿病双效肽(DAPD),它具有GLP-1受体激动剂和胰高血糖素受体拮抗剂的联合活性。为克服其血浆半衰期短的问题,DAPD进行了聚乙二醇化修饰,从而显著延长了其体内活性。聚乙二醇化DAPD(PEG-DAPD)在葡萄糖耐量试验中可增加胰岛素分泌并降低血糖,这是GLP-1受体激动作用的证据。在给予胰高血糖素刺激后,它还能降低小鼠血糖并提高空腹胰高血糖素水平,这是胰高血糖素受体拮抗作用的证据。在存在GLP-1拮抗剂肽艾塞那肽(9-39)的情况下,也观察到了PEG-DAPD对葡萄糖耐量的影响。在db/db小鼠中观察到了PEG-DAPD的抗糖尿病作用。此外,DAPD的聚乙二醇化消除了GLP-1及其类似物所观察到的对胃肠动力的抑制作用。因此,PEG-DAPD有潜力被开发成为一种新型双效肽,用于治疗2型糖尿病,具有延长的体内活性且无胃肠道副作用。

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