合理设计多肽受体激动剂治疗糖尿病和肥胖症。

Endocrine development Pub Date : 2017-01-01 Epub Date: 2017-08-15 DOI:10.1159/000475737
Noushafarin Khajavi, Heike Biebermann, Matthias Tschöp, Richard DiMarchi
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引用次数: 15

摘要

肥胖及其合并症,如2型糖尿病,构成了全球主要的健康威胁,确定有效的医疗干预措施已成为全球的优先事项。历史上抗肥胖治疗的有限效果通常归因于疾病的复杂性和维持体重的代谢调节机制的冗余。肥胖研究的前沿是开发联合药物治疗,同时针对多种调节途径,促进功能失调的代谢。最近,据报道,分子制造的单分子“多激动剂”在参与代谢的3个关键受体,特别是胰高血糖素样肽(GLP)-1受体,葡萄糖依赖性胰岛素性多肽(GIP)受体和胰高血糖素受体的平衡活性上优于传统的单激动剂治疗。这些混合肽激动剂旨在药理学上整合GLP-1的促胰岛素和厌氧作用,胰高血糖素的产热和溶脂活性,以及GIP的促胰岛素和胰岛素增敏特性。这些有目的的混杂配体的分子机制尚不完全清楚,然而,最近在胰腺β细胞中的研究指出了一个复杂的信号网络的前景,该网络可以放大多激动剂配体的信号。这种信号体的激活可能解释了通过多种代谢受体同时激活细胞所固有的额外治疗益处。
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Treatment of Diabetes and Obesity by Rationally Designed Peptide Agonists Functioning at Multiple Metabolic Receptors.

Obesity and its comorbidities such as type 2 diabetes constitute major worldwide health threats, and the identification of an effective medical intervention has emerged as a global priority. The limited effectiveness of historical, anti-obesity treatments is commonly attributed to the complexity of the disease and the redundancy of metabolic regulatory mechanisms that sustain body weight. At the forefront of obesity research is the development of combinational drug therapies that simultaneously target multiple regulatory pathways, which promote dysfunctional metabolism. Recently, molecularly crafted unimolecular "multi-agonism" of balanced activity at 3 key receptors involved in metabolism and specifically the glucagon-like peptide (GLP)-1 receptor, glucose-dependent insulinotropic polypeptide (GIP) receptor and glucagon receptor was reported as superior to conventional monoagonist therapy. These mixed peptide agonists are designed to pharmacologically integrate the insulinotropic and anorexigenic effects of GLP-1, the thermogenic and lipolytic activities of glucagon, and the insulinotropic and insulin sensitizing properties of GIP. The molecular mechanism of these purposefully promiscuous ligands is not completely understood, however, recent studies in pancreatic beta cells point to the prospect of a complex signaling network that can magnify the signaling of multi-agonist ligands. The activation of this signalosome might explain the additional therapeutic benefit inherent to simultaneous cellular activation through multiple metabolic receptors.

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