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培养中的人成骨细胞将1α,25 - 二羟基维生素D3及其前体25 - 羟基维生素D3都代谢为它们各自的内酯。

Human osteoblasts in culture metabolize both 1 alpha, 25-dihydroxyvitamin D3 and its precursor 25-hydroxyvitamin D3 into their respective lactones.

作者信息

Siu-Caldera M L, Zou L, Ehrlich M G, Schwartz E R, Ishizuka S, Reddy G S

机构信息

Department of Pediatrics, Women and Infants Hospital of Rhode Island, Providence 02905, USA.

出版信息

Endocrinology. 1995 Oct;136(10):4195-203. doi: 10.1210/endo.136.10.7664636.

Abstract

1 alpha, 25-Dihydroxyvitamin D3 [1 alpha, 25-(OH)2D3], the hormonal form of vitamin D3, is further metabolized in the kidney and intestine through the carbon 24 (C-24) oxidation pathway initiated by C-24 hydroxylation, and the carbon 23 (C-23) oxidation pathway initiated by C-23 hydroxylation. The C-24 oxidation pathway leading to the formation of calcitroic acid has been previously reported to be present in bone cells, but the C-23 oxidation pathway leading to the formation of 1 alpha, 25-(OH)2D3-26,23-lactone has not been described in bone cells, even though 1 alpha, 25-(OH)2D3-26,23-lactone is noted to have a significant effect on bone formation. Therefore, in the present study, we investigated the production of 1 alpha, 25-(OH)2D3-26,23-lactone in normal human osteoblasts, and our studies revealed that human osteoblasts possess the activity of both 24- and 23-hydroxylases constitutively. Thus, 1 alpha, 24(R),25-(OH)3D3, 1 alpha, 25-(OH)2-24-oxo-D3, 1 alpha, 23(S), 25-(OH)3-24-oxo-D3, 1 alpha, 23-(OH)2-24,25,26,27-tetranor D3, and calcitroic acid formed through the C-24 oxidation pathway and 1 alpha, 23(S),25-(OH)3D3 and 1 alpha, 25-(OH)2D3-26,23-lactone formed through the C-23 oxidation pathway were detected under basal conditions. Also, the synthesis of these metabolites was increased significantly when the cells were treated with 1 alpha, 25-(OH)2D3 (50 nM) for 24 h before incubation with the tracer. As 25-hydroxyvitamin D3 (25OHD3) follows similar side-chain modifications as 1 alpha, 25-(OH)2D3, the metabolism of 25OHD3 in normal human osteoblasts was studied under basal conditions. We found that 25OHD3 was also metabolized through both C-24 and C-23 oxidation pathways, resulting in significant synthesis of 24(R),25-(OH)2D3 along with 25OH-24-oxo-D3, 23(S),25-(OH)2-24-oxo-D3, 23(S),25-(OH)2D3, and 25OHD3-26,23-lactone. Under the same experimental conditions, we looked for 1 alpha, 25-(OH)2D3 synthesis, as earlier studies have shown production of 1 alpha, 25-(OH)2D3 in human bone cells. During a time-course study ranging from 1-24 h, we found that by 2 h, the 24(R), 25-(OH)2D3 concentration rose and accumulated considerably during the following 24 h, but 1 alpha, 25-(OH)2D3 did not accumulate at any time. However, other 1-hydroxylated metabolites, 1 alpha, 23(S),25-(OH)3D3, 1 alpha, 23(S),25-(OH)3-24-oxo-D3, as well as 1 alpha, 25-(OH)2D3-26,23-lactone were detected.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

1α,25 - 二羟基维生素D3[1α,25 - (OH)2D3],即维生素D3的激素形式,在肾脏和肠道中通过由C - 24羟基化启动的碳24(C - 24)氧化途径以及由C - 23羟基化启动的碳23(C - 23)氧化途径进一步代谢。先前报道导致骨化三醇酸形成的C - 24氧化途径存在于骨细胞中,但导致1α,25 - (OH)2D3 - 26,23 - 内酯形成的C - 23氧化途径在骨细胞中尚未见描述,尽管1α,25 - (OH)2D3 - 26,23 - 内酯被认为对骨形成有显著影响。因此,在本研究中,我们研究了正常人成骨细胞中1α,25 - (OH)2D3 - 26,23 - 内酯的产生,我们的研究表明人成骨细胞组成性地具有24 - 和23 - 羟化酶的活性。因此,在基础条件下检测到了通过C - 24氧化途径形成的1α,24(R),25 - (OH)3D3、1α,25 - (OH)2 - 24 - 氧代 - D3、1α,23(S),25 - (OH)3 - 24 - 氧代 - D3、1α,23 - (OH)2 - 24,25,26,27 - 四去甲D3和骨化三醇酸,以及通过C - 23氧化途径形成的1α,23(S),25-(OH)3D3和1α,25 - (OH)2D3 - 26,23 - 内酯。此外,在用示踪剂孵育前,当细胞用1α,25 - (OH)2D3(50 nM)处理24小时时,这些代谢产物的合成显著增加。由于25 - 羟基维生素D3(25OHD3)与1α,25 - (OH)2D3具有相似的侧链修饰,因此在基础条件下研究了正常人成骨细胞中25OHD3的代谢。我们发现25OHD3也通过C - 24和C - 23氧化途径代谢,导致24(R),25 - (OH)2D3以及25OH - 24 - 氧代 - D3、23(S),25 - (OH)2 - 24 - 氧代 - D3、23(S),25 - (OH)2D3和25OHD3 - 26,23 - 内酯的显著合成。在相同的实验条件下,我们寻找1α,25 - (OH)2D3的合成,因为早期研究表明人骨细胞中产生1α,25 - (OH)2D3。在1 - 24小时的时间进程研究中,我们发现到2小时时,24(R),25 - (OH)2D3浓度升高并在接下来的24小时内大量积累,但1α,25 - (OH)2D3在任何时候都没有积累。然而,检测到了其他1 - 羟化代谢产物,1α,23(S),25 - (OH)3D3、1α,23(S),25 - (OH)3 - 24 - 氧代 - D3以及1α,25 - (OH)2D3 - 26,23 - 内酯。(摘要截断于400字)

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