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维生素E动力学与生育酚调节蛋白的功能

Vitamin E kinetics and the function of tocopherol regulatory proteins.

作者信息

Blatt D H, Leonard S W, Traber M G

机构信息

Linus Pauling Institute, Oregon State University, Corvallis, OR 97331-6512, USA.

出版信息

Nutrition. 2001 Oct;17(10):799-805. doi: 10.1016/s0899-9007(01)00637-2.

Abstract

Plasma and tissue alpha-tocopherol concentrations are remarkably stable, which suggests that they are regulated. alpha-Tocopherol transfer protein, tocopherol-associated protein, and tocopherol-binding protein bind alpha-tocopherol. These proteins might function as tocopherol regulatory proteins, although only tocopherol transfer protein has been shown to influence plasma and tissue alpha-tocopherol concentrations. Tissue alpha-tocopherol concentrations likely depend on tocopherol regulatory protein function and tissue lipid content, vitamin E uptake and efflux, oxidative stress, and interactions between vitamin E and other antioxidants. Pharmacokinetic models often divide tissues into rapidly perfused, slowly perfused, and very slowly perfused compartments. Tissue vitamin E concentrations might equilibrate more rapidly in tissues with greater perfusion, greater vitamin E uptake, increased amounts or activities of tocopherol regulatory protein, and lower lipid contents. The rate at which tissue concentrations approach equilibrium, however, does not predict the final equilibrium concentrations because of redistribution among tissues. Redistribution of vitamin E to adipose tissue from other tissues may be significant. Intracellular trafficking of vitamin E might occur in conjunction with membrane recycling because membrane constituents rapidly recycle between the plasma membrane and intracellular endocytic compartments. Thus, tocopherol regulatory proteins may modulate rather than directly regulate vitamin E tissue distribution and intracellular trafficking.

摘要

血浆和组织中的α-生育酚浓度非常稳定,这表明它们受到调控。α-生育酚转运蛋白、生育酚相关蛋白和生育酚结合蛋白可结合α-生育酚。这些蛋白可能作为生育酚调节蛋白发挥作用,尽管只有生育酚转运蛋白已被证明会影响血浆和组织中的α-生育酚浓度。组织中的α-生育酚浓度可能取决于生育酚调节蛋白的功能、组织脂质含量、维生素E的摄取和流出、氧化应激以及维生素E与其他抗氧化剂之间的相互作用。药代动力学模型通常将组织分为快速灌注、缓慢灌注和非常缓慢灌注的区室。在灌注量更大、维生素E摄取量更高、生育酚调节蛋白的量或活性增加以及脂质含量更低的组织中,组织维生素E浓度可能更快达到平衡。然而,由于组织间的再分布,组织浓度达到平衡的速率并不能预测最终的平衡浓度。维生素E从其他组织向脂肪组织的再分布可能很显著。维生素E的细胞内运输可能与膜循环同时发生,因为膜成分在质膜和细胞内吞区室之间快速循环。因此,生育酚调节蛋白可能调节而非直接调控维生素E的组织分布和细胞内运输。

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