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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Translocation of pyrene-labeled phosphatidylserine from the plasma membrane to mitochondria diminishes systematically with molecular hydrophobicity: implications on the maintenance of high phosphatidylserine content in the inner leaflet of the plasma
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Translocation of pyrene-labeled phosphatidylserine from the plasma membrane to mitochondria diminishes systematically with molecular hydrophobicity: implications on the maintenance of high phosphatidylserine content in the inner leaflet of the plasma

机译:molecular标记的磷脂酰丝氨酸从质膜向线粒体的转运随着分子疏水性系统性减少:对维持血浆内小叶中磷脂酰丝氨酸含量高的影响

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摘要

To study the translocation of phosphatidylserine (PS) from plasma membrane to mitochondria, dipyrene PS molecules (diPyr_nPS; n=acyl chain length) were introduced to the plasma membrane of baby hamster kidney cells (BHK cells) using either cyclodextrin-mediated monomer transfer or fusion of cationic vesicles. Translocation of diPyrnPS to mitochondria was assessed based on decarboxylation by mitochondrial PS decarboxylase (PSD). It was found that the rate of translocation diminishes systematically with acyl chain length (molecular hydrophobicity) of diPyr_nPS. Using an in vitro assay, it was shown that the spontaneous translocation rates of long-chain diPyr_nPS species are similar to those of common natural PS species, thus supporting the biological relevance of the data. These results, and other data arguing against the involvement of vesicular traffic and lipid transfer proteins, imply that spontaneous monomeric diffusion via the cytoplasm is the main mechanism of PS movement from the plasma membrane to mitochondria. This finding could explain why a major fraction of PS synthesized by DHK cells consists of hydrophobic species: such species have little tendency to efflux from the plasma membrane to mitochondria where they would be decarboxylated. Thus, adequate molecular hydrophobicity seems to be crucial for the maintenance of high PS content in the inner leaflet of the plasma membrane.
机译:为了研究磷脂酰丝氨酸(PS)从质膜到线粒体的转运,使用环糊精介导的单体转移或阳离子囊泡的融合。基于线粒体PS脱羧酶(PSD)的脱羧作用,评估diPyrnPS向线粒体的转运。已经发现,易位的速率随着diPyr_nPS的酰基链长度(分子疏水性)而逐渐降低。使用体外试验表明,长链diPyr_nPS物种的自发易位率与普通天然PS物种的自发易位率相似,从而支持了数据的生物学相关性。这些结果以及其他有关囊泡运输和脂质转移蛋白参与的数据表明,通过细胞质的自发性单体扩散是PS从质膜向线粒体运动的主要机制。这一发现可以解释为什么DHK细胞合成的PS的大部分由疏水性物质组成:此类物质几乎没有从质膜流出到线粒体的趋势,在那里它们会被羧化。因此,足够的分子疏水性对于维持质膜内小叶中的高PS含量似乎至关重要。

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