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首页> 外文期刊>ACS Chemical Biology >Agouti-related protein segments outside of the receptor binding core are required for enhanced short- and long-term feeding stimulation
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Agouti-related protein segments outside of the receptor binding core are required for enhanced short- and long-term feeding stimulation

机译:受体结合核心以外的刺痛相关蛋白片段是增强短期和长期进食刺激所必需的

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摘要

The agouti-related protein (AgRP) plays a central role in energy balance by reducing signaling through the hypothalamic melanocortin receptors (McRs) 3 and 4, in turn stimulating feeding and decreasing energy expenditure. Mature AgRP(83-132), produced by endoproteolytic processing, contains a central region that folds as an inhibitor cystine knot (ICK) stabilized by a network of disulfide bonds; this domain alone carries the molecular features for high affinity McR binding and inverse agonism. Outside of the ICK domain are two polypeptide segments, an N-terminal extension and a C-terminal loop, both completely conserved but of unknown function. Here we examine the physiological roles of these non-ICK segments by developing a panel of modified AgRPs that were administered to rats through intracerebroventricular (ICV) injection. Analysis of food consumption demonstrates that basic (positively charged) residues are essential for potent short- and long-term AgRP stimulated feeding. Moreover, we demonstrate an approximate linear relationship between protein charge density and 24 h food intake. Next, we developed artificial AgRP(83-132) analogues with increased positive charge and found that these species were substantially more potent than wild type. A single dose of one protein, designated AgRP-4K, results in enhanced feeding for well over a week and weight gain that is nearly double that of AgRP(83-132). These studies suggest new strategies for the development of potent orexigenic species and may serve as leads for the development of therapeutics for treating wasting conditions such as cachexia.
机译:通过减少下丘脑黑皮质素受体(McRs)3和4的信号传导,刺鼠相关蛋白(AgRP)在能量平衡中起着核心作用,进而刺激进食并减少能量消耗。通过内切蛋白水解工艺生产的成熟AgRP(83-132)包含一个中心区域,该区域折叠成通过二硫键网络稳定的抑制剂胱氨酸结(ICK)。该结构域本身具有高亲和力McR结合和反向激动的分子特征。 ICK结构域之外是两个多肽片段,一个N末端延伸和一个C末端环,两者完全保守但功能未知。在这里,我们通过开发一组通过脑室内(ICV)注射给予大鼠的修饰AgRPs来检查这些非ICK片段的生理作用。对食物消耗量的分析表明,碱性(正电荷)残留物对于有效的短期和长期AgRP刺激喂养至关重要。此外,我们证明了蛋白质电荷密度与24小时食物摄入之间的近似线性关系。接下来,我们开发了具有增加的正电荷的人工AgRP(83-132)类似物,发现这些物种比野生型具有更大的效力。单剂量的一种蛋白质称为AgRP-4K,可以使整个星期的进食增加,体重增加几乎是AgRP(83-132)的两倍。这些研究为有效的致病性物种的发展提出了新的策略,并可能为开发治疗消瘦状态(如恶病质)的疗法提供线索。

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