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维生素 D 和 DBP:游离激素假说再探。

Vitamin D and DBP: the free hormone hypothesis revisited.

机构信息

Orthopaedic Hospital Research Center, University of California Los Angeles, Los Angeles, CA 90095, USA.

Department of Mathematics and Statistics, University of Maryland, Baltimore County, Baltimore, MD 21250, USA.

出版信息

J Steroid Biochem Mol Biol. 2014 Oct;144 Pt A:132-7. doi: 10.1016/j.jsbmb.2013.09.012. Epub 2013 Oct 4.

Abstract

The last five years have witnessed a remarkable renaissance in vitamin D research and a complete re-evaluation of its benefits to human health. Two key factors have catalyzed these changes. First, it now seems likely that localized, tissue-specific, conversion of 25-hydroxyvitamin D (25OHD) to 1,25-dihydroxyvitamin D (1,25(OH)2D) drives many of the newly recognized effects of vitamin D on human health. The second key factor concerns the ongoing discussion as to what constitutes adequate or optimal serum vitamin D (25OHD) status, with the possibility that vitamin D-deficiency is common to communities across the globe. These two concepts appear to be directly linked when low serum concentrations of 25OHD compromise intracrine generation of 1,25(OH)2D within target tissues. But, is this an over-simplification? Pro-hormone 25OHD is a lipophilic molecule that is transported in the circulation bound primarily to vitamin D binding protein (DBP). While the association between 25OHD and DBP is pivotal for renal handling of 25OHD and endocrine synthesis of 1,25(OH)2D, what is the role of DBP for extra-renal synthesis of 1,25(OH)2D? We hypothesize that binding to DBP impairs delivery of 25OHD to the vitamin D-activating enzyme 1α-hydroxylase in some target cells. Specifically, it is unbound, 'free' 25OHD that drives many of the non-classical actions of vitamin D. Levels of 'free' 25OHD are dependent on the concentration of DBP and alternative serum binding proteins such as albumin, but will also be influenced by variations in DBP binding affinity for specific vitamin D metabolites. The aim of this review will be to discuss the merits of 'free 25OHD' as an alternative marker of vitamin D status, particularly in the context of non-classical responses to vitamin D. This article is part of a Special Issue entitled '16th Vitamin D Workshop'.

摘要

在过去的五年中,维生素 D 研究取得了显著的复兴,人们对其对人类健康的益处进行了全面重新评估。有两个关键因素促成了这些变化。首先,现在看来,25-羟维生素 D(25OHD)在局部组织中的特异性转化为 1,25-二羟维生素 D(1,25(OH)2D)可能驱动了维生素 D 对人类健康的许多新的认知作用。第二个关键因素涉及到什么构成了足够或最佳的血清维生素 D(25OHD)状态的持续讨论,有可能维生素 D 缺乏在全球社区中很普遍。当低血清 25OHD 浓度使靶组织内的 1,25(OH)2D 的内源性生成受到损害时,这两个概念似乎直接相关。但是,这是否过于简单化了呢?前激素 25OHD 是一种亲脂性分子,在循环中主要与维生素 D 结合蛋白(DBP)结合运输。虽然 25OHD 与 DBP 的结合对于 25OHD 的肾脏处理和 1,25(OH)2D 的内分泌合成至关重要,但 DBP 对于 1,25(OH)2D 的肾外合成有何作用?我们假设,在某些靶细胞中,与 DBP 的结合会损害 25OHD 向维生素 D 激活酶 1α-羟化酶的传递。具体而言,是未结合的“游离”25OHD 驱动了维生素 D 的许多非经典作用。“游离”25OHD 的水平取决于 DBP 的浓度和替代的血清结合蛋白(如白蛋白),但也会受到 DBP 对特定维生素 D 代谢物的结合亲和力变化的影响。本综述的目的将是讨论“游离 25OHD”作为维生素 D 状态替代标志物的优点,特别是在维生素 D 的非经典反应方面。本文是题为“第 16 届维生素 D 研讨会”的特刊的一部分。

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