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New insights into mineral and skeletal regulation by active forms of vitamin D

机译:维生素D活性形式对矿物质和骨骼调节的新见解

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Recent studies in mice using genetic approaches have shed new light on the physiological effects of 1,25-dihydroxyvitamin D (1,25(OH)2D) and the vitamin D receptor (VDR) in skeletal and mineral homeostasis, and on their interaction with calcium. These studies in mice with targeted deletion of the 25-hydroxyvitamin D-1-hydroxylase (1(OH)ase), and of the VDR or of double mutants, have shown the discrete effects of calcium in inhibiting parathyroid hormone secretion and in enhancing bone mineralization, but overlapping effects of calcium and 1,25(OH)2D on inhibiting parathyroid growth and on normal development of the cartilaginous growth plate. The 1,25(OH)2D/VDR system is essential, however, in enhancing intestinal calcium absorption and in optimally increasing osteoclastic activation. In addition, the 1,25(OH)2D/VDR system has important anabolic effects on bone, thus defining a dual role for this system in bone turnover. These studies are revealing functions of the vitamin D/VDR system which have relevance for new concepts of the pathophysiology of renal bone disease and, in particular, of the adynamic bone disorder, and for the development of new analogs of the active form of vitamin D, which have less calcemic activity and greater skeletal anabolic effects.
机译:使用遗传学方法对小鼠进行的最新研究为1,25-二羟基维生素D(1,25(OH)2D)和维生素D受体(VDR)在骨骼和矿物质体内稳态中的生理作用以及与它们的相互作用提供了新的思路。钙。这些针对25-羟基维生素D-1-羟化酶(1(OH)ase)和VDR或双重突变体的靶向缺失的小鼠的研究表明,钙在抑制甲状旁腺激素分泌和增强骨骼方面具有离散作用。矿化,但钙和1,25(OH)2D对抑制甲状旁腺生长和对软骨生长板正常发育有重叠作用。 1,25(OH)2D / VDR系统是必不可少的,但是,对于增强肠道钙的吸收和最佳地增加破骨细胞的活化来说,这是必不可少的。此外,1,25(OH)2D / VDR系统对骨骼具有重要的合成代谢作用,因此定义了该系统在骨骼更新中的双重作用。这些研究揭示了维生素D / VDR系统的功能,这些功能与肾骨疾病的病理生理学新概念有关,尤其是与无动力性骨病有关,并且与维生素D活性形式的新类似物的开发有关,具有较少的钙减少活性和更大的骨骼合成代谢作用。

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