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大鼠体内1α-羟基[6-³H]维生素D₃的合成及其向1α,25-二羟基[6-³H]维生素D₃的代谢

Synthesis of 1alpha-hydroxy [6-3H]vitamin D3 and its metabolism to 1alpha, 25-dihydroxy [6-3H]vitamin D3 in the rat.

作者信息

Holick M F, Tavela T E, Holick S A, Schnoes H K, DeLuca F, Gallagher B M

出版信息

J Biol Chem. 1976 Feb 25;251(4):1020-4.

PMID:1249064
Abstract

1alpha-Hydroxy [6-3H]vitamin D3 has been synthesized with a specific activity of 4 Ci/mmol, and its metabolism in rats has been studied. It is rapidly converted to 1alpha,25-dihydroxy [6-3H]vitamin D3 in vivo. Following an intravenous or oral dose, a maximal concentration of 1alpha,25-dihydroxy [6-3H]vitamin D3 is found 2 and 4 hours, respectively, before the maximal intestinal calcium transport response is observed. Similarly, 1alpha,25-dihydroxy[6-3H]vitamin D3 accumulation in bone precedes the bone calcium mobilization response. It appears, therefore, that the biological activity of 1alpha-hydroxyvitamin D3 is largely, if not exclusively, due to its conversion to 1alpha,25-dihydroxy[6-3H]vitamin D3 1alpha-Hydroxy[6-3H]vitamin D3 and 1alpha,25-dihydroxy[6-3H]vitamin D3 appear in intestine equally well after an oral or an intravenous dose of 1alpha-hydroxy[6-3H]vitamin D3. However, much less of both 1alpha-hydroxy[6-3H]vitamin D3 and 1alpha,25-dihydroxy[6-3H]vitamin D3 appears in bone and blood after an oral than after an intravenous dose. A much reduced bone calcium mobilization response is also noted following an oral dose as compared to an intravenous dose of 1alpha-hydroxyvitamin D3, suggesting that oral 1alpha-hydroxyvitamin D3 is not utilized as well as intravenously administered material.

摘要

已合成比活度为4居里/毫摩尔的1α-羟基[6-³H]维生素D3,并对其在大鼠体内的代谢进行了研究。它在体内迅速转化为1α,25-二羟基[6-³H]维生素D3。静脉注射或口服给药后,分别在观察到最大肠道钙转运反应前2小时和4小时发现1α,25-二羟基[6-³H]维生素D3的最大浓度。同样,骨中1α,25-二羟基[6-³H]维生素D3的蓄积先于骨钙动员反应。因此,看来1α-羟基维生素D3的生物活性即使不是完全也主要是由于其转化为1α,25-二羟基[6-³H]维生素D3。口服或静脉注射1α-羟基[6-³H]维生素D3后,1α-羟基[6-³H]维生素D3和1α,25-二羟基[6-³H]维生素D3在肠道中的出现情况同样良好。然而,口服后骨和血液中出现的1α-羟基[6-³H]维生素D3和1α,25-二羟基[6-³H]维生素D3都比静脉注射后少得多。与静脉注射1α-羟基维生素D3相比,口服给药后骨钙动员反应也明显降低,这表明口服1α-羟基维生素D3的利用率不如静脉给药的物质。

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