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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Oxidative and drug-induced alterations in brush border membrane hemileaflet fluidity, functional consequences for glucose transport
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Oxidative and drug-induced alterations in brush border membrane hemileaflet fluidity, functional consequences for glucose transport

机译:刷状缘膜hemafaflet流动性的氧化和药物诱导改变,葡萄糖转运的功能性后果

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摘要

Oxidation of biological membranes has been suggested as a major pathological process in a variety of disease states including intestinal ischemia and inflammatory bowel disease. Previous studies on the small intestinal brush border membrane have shown that part of the decrease in the activity of the Na~+-dependent glucose transporter (SGLT1) observed after oxidation could be secondary to the derangement in membrane fluidity that accompanied oxidative damage. The present study examined the relationship between oxidative-induced hemileaflet fluidity alterations and the resultant change in Na~+-dependent glucose transport activity. To address this issue, in vitro oxidation of guinea pig brush border membrane vesicles was induced by incubation of the vesicles with ferrous sulfate and ascorbate. We found that oxidation decreased the fluidity of both the outer and inner hemileaflets, the decrease being greater in the outer leaflet. Moreover, the preferential alteration in hemileaflet fluidity was accompanied by a decrease in glucose transport. However, when membrane perturbing agents such as hexanol and A_2C were used to restore membrane fluidity to levels comparable to controls, rates of glucose transport could not be interpreted in terms of variation of bulk membrane fluidity or variation in fluidity of any specific membrane leaflet. On the basis of these experiments, we propose that previous studies that reported coincidental alteration in membrane fluidity and glucose transport cannot be interpreted on the basis of bulk fluidity or hemileaflet fluidity.
机译:已经提出,生物膜的氧化是包括肠缺血和炎性肠病在内的多种疾病状态下的主要病理过程。先前对小肠刷状缘膜的研究表明,氧化后观察到的Na〜+依赖性葡萄糖转运蛋白(SGLT1)活性下降的部分原因可能是膜流动性发生变化并伴有氧化损伤。本研究研究了氧化诱导的hemaflet流动性变化与Na〜+依赖性葡萄糖转运活性的变化之间的关系。为了解决该问题,通过将囊泡与硫酸亚铁和抗坏血酸一起温育来诱导豚鼠刷状缘膜囊泡的体外氧化。我们发现氧化减少了外部和内部hemileaflets的流动性,减少在外部小叶中更大。此外,hemileaflet流动性的优先改变伴随着葡萄糖转运的减少。但是,当使用膜干扰剂(如己醇和A_2C)将膜的流动性恢复到与对照组相当的水平时,无法根据整体膜流动性的变化或任何特定膜小叶的流动性的变化来解释葡萄糖的转运速率。在这些实验的基础上,我们建议以前的报道膜流动性和葡萄糖转运同时发生变化的研究不能基于体积流动性或heafaflet流动性来解释。

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