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首页> 外文期刊>Molecular Metabolism >Quantitative mass spectrometry for human melanocortin peptides in?vitro and in?vivo suggests prominent roles for β-MSH and desacetyl α-MSH in energy homeostasis
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Quantitative mass spectrometry for human melanocortin peptides in?vitro and in?vivo suggests prominent roles for β-MSH and desacetyl α-MSH in energy homeostasis

机译:体外和体内人类黑皮质素肽的定量质谱表明,β-MSH和脱乙酰α-MSH在能量稳态中具有重要作用

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Objective The lack of pro-opiomelanocortin (POMC)-derived melanocortin peptides results in hypoadrenalism and severe obesity in both humans and rodents that is treatable with synthetic melanocortins. However, there are significant differences in POMC processing between humans and rodents, and little is known about the relative physiological importance of POMC products in the human brain. The aim of this study was to determine which POMC-derived peptides are present in the human brain, to establish their relative concentrations, and to test if their production is dynamically regulated. Methods We analysed both fresh post-mortem human hypothalamic tissue and hypothalamic neurons derived from human pluripotent stem cells (hPSCs) using liquid chromatography tandem mass spectrometry (LC-MS/MS) to determine the sequence and quantify the production of hypothalamic neuropeptides, including those derived from POMC. Results In both in?vitro and in?vivo hypothalamic cells, LC-MS/MS revealed the sequence of hundreds of neuropeptides as a resource for the field. Although the existence of β-melanocyte stimulating hormone (MSH) is controversial, we found that both this peptide and desacetyl α-MSH (d-α-MSH) were produced in considerable excess of acetylated α-MSH. In hPSC-derived hypothalamic neurons, these POMC derivatives were appropriately trafficked, secreted, and their production was significantly (P? Conclusions Our findings challenge the assumed pre-eminence of α-MSH and suggest that in humans, d-α-MSH and β-MSH are likely to be the predominant physiological products acting on melanocortin receptors.
机译:目的缺乏源自前opiomelanocortin(POMC)的melanocortin肽,可导致人类和啮齿类动物的肾上腺皮质功能减退和严重肥胖,可以用合成的melanocortins治疗。但是,人与啮齿动物之间在POMC加工方面存在显着差异,对POMC产品在人脑中的相对生理重要性知之甚少。这项研究的目的是确定人脑中存在哪些POMC衍生肽,确定其相对浓度,并测试其产生是否受到动态调节。方法我们使用液相色谱串联质谱(LC-MS / MS)分析了新鲜的人体死后丘脑下丘脑组织和源自人多能干细胞(hPSCs)的丘脑下丘脑神经元,以确定其序列并定量了下丘脑神经肽的产生,包括那些源自POMC。结果在体外和体内下丘脑细胞中,LC-MS / MS揭示了数百种神经肽的序列,可作为该领域的资源。尽管β-黑素细胞刺激激素(MSH)的存在存在争议,但我们发现该肽和脱乙酰基α-MSH(d-α-MSH)都产生了大量过量的乙酰化α-MSH。在hPSC衍生的下丘脑神经元中,这些POMC衍生物被适当地贩运,分泌,并且其产生显着(P?结论)我们的发现挑战了假定的α-MSH优势,并提示在人中d-α-MSH和β -MSH可能是作用于黑皮质素受体的主要生理产物。

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