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Can Xanthophyll-Membrane Interactions Explain Their Selective Presence in the Retina and Brain?

机译:叶黄素-膜相互作用可以解释其在视网膜和大脑中的选择性存在吗?

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Epidemiological studies demonstrate that a high dietary intake of carotenoids may offer protection against age-related macular degeneration, cancer and cardiovascular and neurodegenerative diseases. Humans cannot synthesize carotenoids and depend on their dietary intake. Major carotenoids that have been found in human plasma can be divided into two groups, carotenes (nonpolar molecules, such as β-carotene, α-carotene or lycopene) and xanthophylls (polar carotenoids that include an oxygen atom in their structure, such as lutein, zeaxanthin and β-cryptoxanthin). Only two dietary carotenoids, namely lutein and zeaxanthin (macular xanthophylls), are selectively accumulated in the human retina. A third carotenoid, meso -zeaxanthin, is formed directly in the human retina from lutein. Additionally, xanthophylls account for about 70% of total carotenoids in all brain regions. Some specific properties of these polar carotenoids must explain why they, among other available carotenoids, were selected during evolution to protect the retina and brain. It is also likely that the selective uptake and deposition of macular xanthophylls in the retina and brain are enhanced by specific xanthophyll-binding proteins. We hypothesize that the high membrane solubility and preferential transmembrane orientation of macular xanthophylls distinguish them from other dietary carotenoids, enhance their chemical and physical stability in retina and brain membranes and maximize their protective action in these organs. Most importantly, xanthophylls are selectively concentrated in the most vulnerable regions of lipid bilayer membranes enriched in polyunsaturated lipids. This localization is ideal if macular xanthophylls are to act as lipid-soluble antioxidants, which is the most accepted mechanism through which lutein and zeaxanthin protect neural tissue against degenerative diseases.
机译:流行病学研究表明,饮食中摄入大量的类胡萝卜素可以预防与年龄有关的黄斑变性,癌症以及心血管和神经退行性疾病。人类无法合成类胡萝卜素,只能依靠饮食摄入。人类血浆中发现的主要类胡萝卜素可分为两组,类胡萝卜素(非极性分子,例如β-胡萝卜素,α-胡萝卜素或番茄红素)和叶黄素(结构中包含氧原子的极性类胡萝卜素,例如叶黄素) ,玉米黄质和β-隐黄质)。在人的视网膜中,只有两种饮食类胡萝卜素,即叶黄素和玉米黄质(黄体叶黄素)选择性地积累。第三种类胡萝卜素,中观玉米黄质,是由叶黄素直接在人视网膜中形成的。此外,叶黄素在所有大脑区域中约占类胡萝卜素总量的70%。这些极性类胡萝卜素的某些特殊性质必须解释为什么为什么在进化过程中选择了其他可用的类胡萝卜素来保护视网膜和大脑。叶黄素结合蛋白可以增强黄斑叶黄素在视网膜和大脑中的选择性摄取和沉积。我们假设黄斑叶黄素的高膜溶解度和优先的跨膜方向使它们与其他饮食类胡萝卜素区分开来,增强了它们在视网膜和脑膜中的化学和物理稳定性,并使它们在这些器官中的保护作用最大化。最重要的是,叶黄素选择性地富集在富含多不饱和脂质的双层脂质膜的最脆弱区域中。如果黄斑叶黄素充当脂溶性抗氧化剂,则这种定位是理想的,这是叶黄素和玉米黄质保护神经组织免受退行性疾病侵害的最广泛接受的机制。

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