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A novel human receptor involved in bitter tastant detection identified using Dictyostelium discoideum

机译:使用Disctyostelium Discoideum鉴定的一种涉及苦味剂检测的新型人类受体

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Detection of substances tasting bitter to humans occurs in diverse organisms including the social amoeba Dictyostelium discoideum. To establish a molecular mechanism for bitter tastant detection in Dictyostelium, we screened a mutant library for resistance to a commonly used bitter standard, phenylthiourea. This approach identified a G-protein-coupled receptor mutant, grlJ- , which showed a significantly increased tolerance to phenylthiourea in growth, survival and movement. This mutant was not resistant to a structurally dissimilar potent bitter tastant, denatonium benzoate, suggesting it is not a target for at least one other bitter tastant. Analysis of the cell-signalling pathway involved in the detection of phenylthiourea showed dependence upon heterotrimeric G protein and phosphatidylinositol 3- kinase activity, suggesting that this signalling pathway is responsible for the cellular effects of phenylthiourea. This is further supported by a phenylthiourea-dependent block in the transient cAMP-induced production of phosphatidylinositol (3,4,5)-trisphosphate (PIP3) in wild-type but not grlJ- cells. Finally, we have identified an uncharacterized human protein γ-aminobutyric acid (GABA) type B receptor subunit 1 isoform with weak homology to GrlJ that restored grlJ- sensitivity to phenylthiourea in cell movement and PIP3 regulation. Our results thus identify a novel pathway for the detection of the standard bitter tastant phenylthiourea in Dictyostelium and implicate a poorly characterized human protein in phenylthiourea-dependent cell responses
机译:品尝到对人有苦味的物质的检测发生在各种生物中,包括社交变形​​虫盘基网柄菌Discoyostelium discoideum。为了建立双歧杆菌中苦味剂检测的分子机制,我们筛选了对常用苦味标准苯硫脲具有抗性的突变体文库。该方法鉴定了G蛋白偶联的受体突变体grlJ-,其显示出对苯硫脲在生长,存活和运动中的耐受性显着提高。该突变体对结构上不同的强效苦味剂苯甲酸地那铵没有抗性,表明它不是至少一种其他苦味剂的靶标。对参与苯硫脲检测的细胞信号通路的分析表明,它依赖于异三聚体G蛋白和磷脂酰肌醇3-激酶活性,这表明该信号通路对苯硫脲的细胞作用负责。这在野生型而不是grlJ-细胞中由c硫代磷酸酯依赖性的暂时性cAMP诱导的磷脂酰肌醇(3,4,5)-三磷酸(PIP3)的瞬时产生中进一步受到支持。最后,我们鉴定了与GrlJ同源性较弱的未表征的人蛋白质γ-氨基丁酸(GABA)B型受体亚基1亚型,可恢复细胞运动和PIP3调节对苯硫脲的grlJ敏感性。因此,我们的结果确定了一种检测Dictyostelium中的标准苦味味苯基硫脲的新途径,并暗示了表征不佳的人类蛋白质对苯硫脲的依赖

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