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Cav 1.3 L型钙通道基因敲除小鼠的骨骼表型

Skeletal phenotype of mice with a null mutation in Cav 1.3 L-type calcium channel.

作者信息

Li J, Zhao L, Ferries I K, Jiang L, Desta M Z, Yu X, Yang Z, Duncan R L, Turner C H

机构信息

Department of Biology, Indiana University Purdue University Indianapolis, Indianapolis, IN 46202, USA.

出版信息

J Musculoskelet Neuronal Interact. 2010 Jun;10(2):180-7.

Abstract

This study aimed to understand the role of Cav1.3, one of the four L-type voltage sensitive calcium channels (VSCC) alpha(1) subunits, in the skeletal response to mechanical loading and intermittent PTH treatment. The Cav1.3 mRNA is expressed in osteoblasts. The Cav1.3 mRNA level in male wild type mice is higher than those in female. Loss of Cav1.3 resulted in a smaller skeleton in male mice as indicated by significantly lower body weight, less bone mineral content and smaller cross-sectional area of femoral midshaft. However, the osteogenic response to mechanical loading of the ulna was normal in Cav1.3(-/-) compared to the normal control mice. Male mice Cav1.3(-/-) were then treated daily with PTH at a dose of 40 microg/kg. A 6-week course of intermittent PTH treatment enhanced bone mineral content and mechanical strength equally in wild type control and Cav1.3 null mice. We also found that Cav1.2 subunit significantly increases in the absence of Cav1.3 gene. In conclusion, Cav1.3 is involved in bone metabolism, especially in male mice. Cav1.3 does not mediate osteoblast response to mechanical loading and PTH. Our data suggest that Cav1.1 and Cav1.2 subunits may substitute for Cav1.3 to maintain bone response to mechanical loading.

摘要

本研究旨在了解四种L型电压敏感性钙通道(VSCC)α(1)亚基之一的Cav1.3在骨骼对机械负荷和间歇性甲状旁腺激素(PTH)治疗反应中的作用。Cav1.3信使核糖核酸(mRNA)在成骨细胞中表达。雄性野生型小鼠的Cav1.3 mRNA水平高于雌性。Cav1.3缺失导致雄性小鼠骨骼较小,表现为体重显著降低、骨矿物质含量减少以及股骨干中段横截面积减小。然而,与正常对照小鼠相比,Cav1.3基因敲除(-/-)小鼠尺骨对机械负荷的成骨反应正常。然后,对雄性Cav1.3(-/-)小鼠每天给予4 μg/kg剂量的PTH治疗。为期6周的间歇性PTH治疗在野生型对照小鼠和Cav1.3基因缺失小鼠中均同等程度地提高了骨矿物质含量和机械强度我们还发现,在缺乏Cav1.3基因的情况下,Cav1.2亚基显著增加。总之,Cav1.3参与骨代谢,尤其是在雄性小鼠中。Cav1.3不介导成骨细胞对机械负荷和PTH的反应。我们的数据表明,Cav1.1和Cav1.2亚基可能替代Cav1.3以维持骨骼对机械负荷的反应。

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