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维生素D及一种具有25-羟胆钙化醇特性的极性代谢物在人血浆中的周转与转运。

The turnover and transport of vitamin D and of a polar metabolite with the properties of 25-hydroxycholecalciferol in human plasma.

作者信息

Smith J E, Goodman D S

出版信息

J Clin Invest. 1971 Oct;50(10):2159-67. doi: 10.1172/JCI106710.

Abstract

Four normal men were injected intravenously with physiological doses (6 mug) of vitamin D(3)-1,2-(3)H. Serial samples of plasma were collected for 50 days. Total lipid extracts were chromatographed on silicic acid columns or thin-layer plates in order to characterize the radioactive components. Labeled vitamin D(3) disappeared rapidly from plasma (initial half-life approximately 12 hr); after 7 days unchanged vitamin D(3) represented less than 1% of circulating radioactivity. Coincident with vitamin D(3) disappearance a more polar labeled metabolite appeared with chromatographic and other properties identical with those of 25-hydroxycholecalciferol. The disappearance of the more polar metabolite was relatively slow with a half-life of 19.6 +/-0.6 days. A similar half-life was seen in a fifth subject, injected with 80 mug of vitamin D(3)-(3)H. Most (approximately 92%) of the plasma total radioactivity was represented by this component throughout the study. Plasma samples collected at various times were adjusted to density (d) 1.21 and were ultracentrifuged to separate plasma lipoproteins from proteins with d > 1.21. In all samples, almost all (mean 94%) of the radioactivity was found in association with proteins of d > 1.21. This observation was confirmed by bioassay, measuring uptake of (45)Ca by intestinal slices. All plasma bioassayable vitamin D was found in association with proteins of d > 1.21; 55% of bioactivity was found in the chromatographic fraction corresponding to 25-hydroxycholecalciferol and 44% in the fractions representing vitamin D(3). Since both vitamin D(3) and its 25-hydroxy metabolite are lipid-soluble sterol derivatives, the finding that these compounds do not circulate in association with the known plasma lipoproteins provides presumptive evidence for the existence of a specific transport protein of d > 1.21. The transport protein for the polar metabolite has been partly characterized by gel filtration on Sephadex G-200 and by electrophoresis on polyacrylamide gel. The protein has an apparent size slightly smaller than plasma albumin (approximate mol wt 50,000-60,000) and an electrophoretic mobility very slightly greater than that of albumin. Studies are in progress to fractionate further and to characterize the transport protein.

摘要

给4名正常男性静脉注射生理剂量(6微克)的维生素D3-1,2-(3)H。连续采集50天的血浆样本。将总脂质提取物在硅酸柱或薄层层析板上进行色谱分析,以鉴定放射性成分。标记的维生素D3从血浆中迅速消失(初始半衰期约为12小时);7天后,未变化的维生素D3占循环放射性的比例不到1%。与维生素D3消失同时出现了一种极性更强的标记代谢物,其色谱和其他性质与25-羟基胆钙化醇相同。这种极性更强的代谢物消失相对较慢,半衰期为19.6±0.6天。在第五名注射了80微克维生素D3-(3)H的受试者中也观察到了类似的半衰期。在整个研究过程中,血浆总放射性的大部分(约92%)由该成分代表。将不同时间采集的血浆样本调整至密度(d)1.21,进行超速离心,以将血浆脂蛋白与密度大于1.21的蛋白质分离。在所有样本中,几乎所有(平均94%)的放射性都与密度大于1.21的蛋白质结合。通过生物测定法,测量肠切片对(45)Ca的摄取,证实了这一观察结果。所有血浆中可进行生物测定的维生素D都与密度大于1.21的蛋白质结合;55%的生物活性存在于与25-羟基胆钙化醇相对应的色谱部分,44%存在于代表维生素D3的部分。由于维生素D3及其25-羟基代谢物都是脂溶性甾醇衍生物,这些化合物不与已知的血浆脂蛋白结合循环这一发现为存在一种密度大于1.21的特异性转运蛋白提供了推测性证据。通过在Sephadex G-200上进行凝胶过滤和在聚丙烯酰胺凝胶上进行电泳,对极性代谢物的转运蛋白进行了部分表征。该蛋白的表观大小略小于血浆白蛋白(近似分子量50,000-60,000),电泳迁移率略大于白蛋白。进一步分离和表征转运蛋白的研究正在进行中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1bd/292150/860fe2ddd87e/jcinvest00198-0168-a.jpg

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