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首页> 外文期刊>Kidney International: Official Journal of the International Society of Nephrology >Parathyroid-specific interaction of the calcium-sensing receptor and G alpha q.
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Parathyroid-specific interaction of the calcium-sensing receptor and G alpha q.

机译:钙敏感受体和 G α q 的甲状旁腺特异性相互作用。

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摘要

The calcium-sensing receptor regulates various parathyroid gland functions, including hormone secretion, gene transcription, and chief cell hyperplasia through G alpha q- and G alpha i-dependent signaling pathways. To determine the specific function of G alpha q in these processes, we generated transgenic mice using the human parathyroid hormone promoter to drive overexpression of a dominant negative G alpha q loop minigene to selectively disrupt G alpha q function in the parathyroid gland. The G alpha q loop mRNA was highly expressed in the parathyroid gland but not in other tissues of these transgenic mice. Gross appearance, body weight, bone mineral density, and survival of the transgenic mice were indistinguishable from those of their wild-type littermates. Adult transgenic mice, however, exhibited an increase in parathyroid hormone mRNA and in its basal serum level as well as in gland size. The response of the parathyroid gland to hypocalcemia was found to be reduced in sensitivity in the transgenic mice when compared to their wild-type controls. Abnormalities of the parathyroid gland function in these transgenic mice were similar to those of heterozygous G alpha q(+/-) and calcium sensing receptor(+/-) mice. These studies demonstrate the feasibility of selectively targeting the parathyroid gland to investigate signaling mechanisms downstream of the calcium receptor.
机译:钙敏感受体通过 G α q- 和 G α i 依赖性信号通路调节各种甲状旁腺功能,包括激素分泌、基因转录和主细胞增生。为了确定 G α q 在这些过程中的特定功能,我们使用人甲状旁腺激素启动子生成转基因小鼠,以驱动显性阴性 G α q 环微基因的过表达,以选择性地破坏甲状旁腺中的 G α q 功能。G α q 环 mRNA 在甲状旁腺中高度表达,但在这些转基因小鼠的其他组织中不高表达。转基因小鼠的粗体外观、体重、骨密度和存活率与野生型同窝小鼠没有区别。然而,成年转基因小鼠表现出甲状旁腺激素mRNA及其基础血清水平以及腺体大小的增加。与野生型对照组相比,发现转基因小鼠对甲状旁腺对低钙血症的反应在敏感性上降低。这些转基因小鼠的甲状旁腺功能异常与杂合子G α q(+/-)和钙敏感受体(+/-)小鼠相似。这些研究证明了选择性靶向甲状旁腺以研究钙受体下游信号传导机制的可行性。

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