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甲状旁腺激素(PTH)相关蛋白通过在血管平滑肌细胞中稳定表达的重组PTH/PTHrP受体进行细胞特异性信号转导。

Cell-specific signal transduction of parathyroid hormone (PTH)-related protein through stably expressed recombinant PTH/PTHrP receptors in vascular smooth muscle cells.

作者信息

Maeda S, Wu S, Jüppner H, Green J, Aragay A M, Fagin J A, Clemens T L

机构信息

Department of Medicine, University of Cincinnati College of Medicine, Ohio 45267, USA.

出版信息

Endocrinology. 1996 Aug;137(8):3154-62. doi: 10.1210/endo.137.8.8754733.

DOI:10.1210/endo.137.8.8754733
PMID:8754733
Abstract

PTH-related protein activates a G protein-coupled PTH/PTHrP receptor in many cell types and produces diverse biological actions. To study the signal transduction events associated with biological activity of the PTH/PTHrP receptor in vascular smooth muscle, a principal PTHrP-responsive tissue, rat aortic smooth muscle cells (A10) were stably transfected with a plasmid encoding a PTH/PTHrP receptor and tested for ligand binding, PTHrP-(1-34)-induced cAMP levels, inositol phosphate production, and cytosolic calcium transients. Of nineteen G418-resistant lines recovered, all exhibited high affinity binding [approximately dissociation constant (Kd) > 10(-10)) of iodinated [Tyr36]hPTHrP(1-36)NH2 and ligand-induced cAMP accumulation (2- to 100-fold), which was directly proportional to PTH/PTHrP receptor number (range 4 x 10(3) to 7 x 10(7) sites/cell]. PTHrP had no effect on intracellular calcium or inositol phosphate formation in any cell line regardless of receptor number despite the presence of detectable G alpha q). Transient overexpression of individual G alpha q proteins (G alpha q, G alpha 11 or G alpha 14) into PTH/PTHrP receptor-expressing A10 cells conferred the ability of PTHrP to increase intracellular calcium and inositol phosphate formation. Ligand activation of the recombinant PTH/PTHrP receptor elicited appropriate downstream biological effects in A10 cells including inhibition of DNA synthesis and osteopontin messenger RNA (mRNA) expression. Thus, a single PTH/PTHrP receptor, though capable of coupling to different G proteins, signals exclusively through a cAMP-dependent pathway in vascular smooth muscle.

摘要

甲状旁腺激素相关蛋白(PTHrP)在多种细胞类型中激活G蛋白偶联的甲状旁腺激素/甲状旁腺激素相关蛋白(PTH/PTHrP)受体,并产生多种生物学作用。为了研究与血管平滑肌(一种主要的PTHrP反应性组织)中PTH/PTHrP受体生物学活性相关的信号转导事件,用编码PTH/PTHrP受体的质粒稳定转染大鼠主动脉平滑肌细胞(A10),并检测其配体结合、PTHrP-(1-34)诱导的cAMP水平、肌醇磷酸生成和胞质钙瞬变。在回收的19个对G418耐药的细胞系中,所有细胞系均表现出对碘化的[Tyr36]hPTHrP(1-36)NH2的高亲和力结合[解离常数(Kd)约>10(-10)]以及配体诱导的cAMP积累(2至100倍),这与PTH/PTHrP受体数量直接相关(范围为4×10(3)至7×10(7)个位点/细胞)。尽管存在可检测到的Gαq,但无论受体数量如何,PTHrP对任何细胞系中的细胞内钙或肌醇磷酸形成均无影响。将单个Gαq蛋白(Gαq、Gα11或Gα14)瞬时过表达至表达PTH/PTHrP受体的A10细胞中,赋予了PTHrP增加细胞内钙和肌醇磷酸形成的能力。重组PTH/PTHrP受体的配体激活在A10细胞中引发了适当的下游生物学效应,包括抑制DNA合成和骨桥蛋白信使核糖核酸(mRNA)表达。因此,单个PTH/PTHrP受体虽然能够与不同的G蛋白偶联,但在血管平滑肌中仅通过cAMP依赖性途径发出信号。

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