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REGULATION OF F1-ATPASE BETA SUBUNIT CELLULAR LOCATION

机译:F1-ATPaseβ亚基细胞位置的调控

摘要

It has been discovered that the ability of analogues to affect binding of a labeled ?--casomorphin (an enterostatin antagonist) to recombinant rat F1-ATPase ?-subunit was closely correlated with their enterostatin-like biological activity. Using immunohistochemistry and western blots, the presence of the F1- ATPase ?-subunit was demonstrated in plasma membranes of liver, pancreas and amygdala. The effects of enterostatin on the intracellular localization of the proteins were studied using deconvolution or confocal microscopy. Enterostatin did not alter the location of F1-ATPase a-subunit-RFP but induced movement of the F1-ATPase ?-subunit--GFP to the periphery of cells. These studies, showing the plasma membrane localization of the F1-ATPase ?-subunit, the influence of enterostatin on the cellular location of the protein, the appropriate Kd value for binding, together with the previous correlation of binding effects with biological activity for a number of analogues, indicate that this protein is the enterostatin receptor.
机译:已经发现类似物影响标记的β-酪蛋白吗啡(肠抑素拮抗剂)与重组大鼠F1-ATPaseβ-亚基结合的能力与它们的肠抑素样生物学活性密切相关。使用免疫组织化学和蛋白质印迹,在肝,胰腺和杏仁核的质膜中证实了F1-ATPaseβ-亚基的存在。使用去卷积或共聚焦显微镜研究了肠抑素对蛋白质细胞内定位的影响。肠抑素不会改变F1-ATPaseα-亚基-RFP的位置,但会诱导F1-ATPaseβ-亚基-GFP向细胞外围移动。这些研究表明,F1-ATPaseβ-亚基的质膜定位,肠抑素对蛋白质细胞位置的影响,适当的结合Kd值,以及先前结合作用与许多生物学活性的相关性。的类似物表明该蛋白是肠抑素受体。

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