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首页> 外文期刊>The biochemical journal >Endogenously produced lipoprotein lipase enhances the binding and cell association of native, mildly oxidized and moderately oxidized low-density lipoprotein in mouse peritoneal macrophages
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Endogenously produced lipoprotein lipase enhances the binding and cell association of native, mildly oxidized and moderately oxidized low-density lipoprotein in mouse peritoneal macrophages

机译:内源性脂蛋白脂肪酶增强了小鼠腹膜巨噬细胞中天然,轻度氧化和中度氧化的低密度脂蛋白的结合和细胞缔合

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pIt has been well established that purified lipoprotein lipase (LPL) can facilitate the cellular uptake of various native and modified lipoproteins when added exogenously to macrophages. Because activated macrophages express LPL endogenously, it was the aim of this study to investigate the effect of macrophage-produced LPL on the uptake of native low-density lipoprotein (LDL) and LDL that has been modified to various degrees by Cusup2+/sup-mediated oxidation. Cell binding and uptake of Eusup3+/sup-labelled native and oxidized LDL was determined in mouse peritoneal macrophages (MPM) from normal mice and induced mutant mice that lack LPL expression in MPM. We found that LPL expressed by MPM was able to increase cell binding and association of native LDL (by 121% and 101% respectively), mildly oxidized LDL (by 47% and 43%) and moderately oxidized LDL (by 30% and 22%). With increased levels of lipoprotein oxidation, the relative proportion of LPL-mediated LDL uptake decreased. This decrease was not due to weakened binding of LPL to oxidized LDL. The drastically increased uptake of highly oxidized LDL in MPM by scavenger-receptor-mediated pathways might dominate the simultaneous exogenous or endogenous LPL-mediated uptake of this lipoprotein. Competition experiments with positively charged poly(amino acids) furthermore suggested that histidine, arginine and lysine residues in LPL are important for the interaction between LDL and LPL. Our results imply that physiological levels of LPL produced by macrophages facilitate the uptake of native LDL as well as mildly and moderately oxidized LDL. This process might, in the micro-environment of arteries, contribute to the accumulation of macrophage lipids and the formation of foam cells./p
机译:众所周知,纯化的脂蛋白脂肪酶(LPL)外源添加到巨噬细胞后,可以促进细胞摄取各种天然和修饰的脂蛋白。因为活化的巨噬细胞内源性表达LPL,所以本研究的目的是研究巨噬细胞产生的LPL对天然低密度脂蛋白(LDL)和被Cu 2修饰到不同程度的LDL摄取的影响。 + 介导的氧化。在正常小鼠和在MPM中缺乏LPL表达的诱导突变小鼠的小鼠腹膜巨噬细胞(MPM)中,测定了Eu 3 + 标记的天然LDL和氧化LDL的细胞结合和摄取。我们发现,由MPM表达的LPL能够增加天然LDL(分别增加121%和101%),轻度氧化的LDL(分别增加47%和43%)和中度氧化的LDL(分别增加30%和22%)的细胞结合和缔合)。随着脂蛋白氧化水平的提高,LPL介导的LDL摄取的相对比例降低。这种减少不是由于LPL与氧化LDL的结合减弱所致。通过清除剂-受体介导的途径,MPM中高度氧化的LDL的摄取急剧增加,可能占该脂蛋白同时外源或内源LPL介导的摄取的主导。带正电荷的聚氨基酸的竞争实验进一步表明,LPL中的组氨酸,精氨酸和赖氨酸残基对于LDL和LPL之间的相互作用很重要。我们的结果暗示巨噬细胞产生的LPL的生理水平有助于摄取天然LDL以及轻度和中度氧化的LDL。在动脉的微环境中,该过程可能有助于巨噬细胞脂质的积累和泡沫细胞的形成。

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