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Differential Effects of Camel Milk on Insulin Receptor Signaling – Toward Understanding the Insulin-Like Properties of Camel Milk

机译:骆驼奶对胰岛素受体信号转导的差异作用–旨在了解骆驼奶的胰岛素样特性

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Previous studies on the Arabian camel ( Camelus dromedarius ) showed beneficial effects of its milk reported in diverse models of human diseases, including a substantial hypoglycemic activity. However, the cellular and molecular mechanisms involved in such effects remain completely unknown. In this study, we hypothesized that camel milk may act at the level of human insulin receptor (hIR) and its related intracellular signaling pathways. Therefore, we examined the effect of camel milk on the activation of hIR transiently expressed in human embryonic kidney 293 (HEK293) cells using bioluminescence resonance energy transfer (BRET) technology. BRET was used to assess, in live cells and real-time, the physical interaction between hIR and insulin receptor signaling proteins (IRS1) and the growth factor receptor-bound protein 2 (Grb2). Our data showed that camel milk did not promote any increase in the BRET signal between hIR and IRS1 or Grb2 in the absence of insulin stimulation. However, it significantly potentiated the maximal insulin-promoted BRET signal between hIR and Grb2 but not IRS1. Interestingly, camel milk appears to differentially impact the downstream signaling since it significantly activated ERK1/2 and potentiated the insulin-induced ERK1/2 but not Akt activation. These observations are to some extent consistent with the BRET data since ERK1/2 and Akt activation are known to reflect the engagement of Grb2 and IRS1 pathways, respectively. The preliminary fractionation of camel milk suggests the peptide/protein nature of the active component in camel milk. Together, our study demonstrates for the first time an allosteric effect of camel milk on insulin receptor conformation and activation with differential effects on its intracellular signaling. These findings should help to shed more light on the hypoglycemic activity of camel milk with potential therapeutic applications.
机译:先前对阿拉伯骆驼(Camelus dromedarius)的研究表明,在多种人类疾病模型中报道了其牛奶的有益作用,包括大量降糖活动。但是,涉及这种作用的细胞和分子机制仍然完全未知。在这项研究中,我们假设骆驼奶可能在人类胰岛素受体(hIR)及其相关的细胞内信号通路中起作用。因此,我们使用生物发光共振能量转移(BRET)技术检查了骆驼奶对人胚肾293(HEK293)细胞中瞬时表达的hIR活化的影响。 BRET用于在活细胞中实时评估hIR与胰岛素受体信号蛋白(IRS1)和生长因子受体结合蛋白2(Grb2)之间的物理相互作用。我们的数据显示,在没有胰岛素刺激的情况下,骆驼奶不会促进hIR与IRS1或Grb2之间的BRET信号增加。但是,它显着增强了hIR和Grb2之间的最大胰岛素促进BRET信号,但不能增强IRS1。有趣的是,骆驼奶似乎显着地影响下游信号,因为它显着激活了ERK1 / 2,并增强了胰岛素诱导的ERK1 / 2,但未激活Akt。这些观察结果在一定程度上与BRET数据一致,因为已知ERK1 / 2和Akt激活分别反映了Grb2和IRS1途径的参与。骆驼奶的初步分馏表明,骆驼奶中活性成分的肽/蛋白质性质。总之,我们的研究首次证明了骆驼奶对胰岛素受体构象和活化的变构作用,并对其细胞内信号传导产生不同的影响。这些发现应有助于进一步揭示骆驼奶的降血糖活性及其潜在的治疗应用。

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