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首页> 外文期刊>American Journal of Physiology >Human calcitonin receptor is directly targeted to and retained in the basolateral surface of MDCK cells.
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Human calcitonin receptor is directly targeted to and retained in the basolateral surface of MDCK cells.

机译:人降钙素受体直接靶向并保留在MDCK细胞的基底外侧表面。

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The human calcitonin receptor (hCTR) is expressed in polarized cells of the kidney, bone, and nervous system. In the kidney, hCTRs are found in cells of the distal nephron to which blood-borne calcitonin has access only at the basolateral surface. We expressed hCTR subtypes 1 and 2 in Madin-Darby canine kidney (MDCK) cells to establish a cell model useful for delineating the molecular mechanisms underlying hCTR polarity. Selective cell surface incubation demonstrated functional polarity of hCTRs by equilibrium binding or cross-linking of radioiodinated salmon calcitonin (125I-sCT) and cAMP accumulation stimulated by sCT. We estimated that at the steady state there are 40-fold more hCTRs on the basolateral than on the apical side. Domain-selective cell surface biotinylation followed by immunoblotting of streptavidin-agarose-fractionated biotinylated glycoproteins independently confirmed the polarized distribution of FLAG epitope-tagged hCTR-2 in the basolateral domain. Confocal microscopy of immunostained receptors revealed that hCTRs are concentrated on a lateral subdomain of the basolateral membrane. Cell surface arrival assay of newly formed receptors demonstrated that direct delivery to the basolateral domain is the mechanism by which hCTRs become polarized. Measurement of receptor turnover on the basolateral surface showed that retention contributes to hCTR distribution at the steady state.
机译:人降钙素受体(hCTR)在肾脏,骨骼和神经系统的极化细胞中表达。在肾脏中,hCTRs在远端肾单位的细胞中发现,血液中的降钙素只能在基底外侧表面进入。我们在Madin-Darby犬肾(MDCK)细胞中表达了hCTR亚型1和2,以建立可用于描述hCTR极性基础的分子机制的细胞模型。选择性细胞表面孵育通过放射性碘化鲑鱼降钙素(125I-sCT)和sCT刺激的cAMP积累的平衡结合或交联证明了hCTR的功能极性。我们估计,在稳态下,基底外侧的hCTR比顶端高40倍。域选择性细胞表面生物素化和链霉亲和素-琼脂糖分离的生物素化糖蛋白的免疫印迹独立地证实了基底外侧域中带有FLAG表位标记的hCTR-2的极化分布。免疫染色受体的共聚焦显微镜显示,hCTRs集中在基底外侧膜的外侧亚结构域上。新形成的受体的细胞表面到达测定表明,直接递送至基底外侧结构域是hCTRs极化的机制。测量基底外侧表面上的受体周转率表明,保留在稳态下有助于hCTR分布。

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