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HDL from apoA1 transgenic mice expressing the 4WF isoform is resistant to oxidative loss of function

机译:表达4WF亚型的apoA1转基因小鼠的HDL抵抗氧化功能丧失

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摘要

HDL functions are impaired by myeloperoxidase (MPO), which selectively targets and oxidizes human apoA1. We previously found that the 4WF isoform of human apoA1, in which the four tryptophan residues are substituted with phenylalanine, is resistant to MPO-mediated loss of function. The purpose of this study was to generate 4WF apoA1 transgenic mice and compare functional properties of the 4WF and wild-type human apoA1 isoforms in vivo. Male mice had significantly higher plasma apoA1 levels than females for both isoforms of human apoA1, attributed to different production rates. With matched plasma apoA1 levels, 4WF transgenics had a trend for slightly less HDL-cholesterol versus human apoA1 transgenics. While 4WF transgenics had 31% less reverse cholesterol transport (RCT) to the plasma compartment, equivalent RCT to the liver and feces was observed. Plasma from both strains had similar ability to accept cholesterol and facilitate ex vivo cholesterol efflux from macrophages. Furthermore, we observed that 4WF transgenic HDL was partially (∼50%) protected from MPO-mediated loss of function while human apoA1 transgenic HDL lost all ABCA1-dependent cholesterol acceptor activity. In conclusion, the structure and function of HDL from 4WF transgenic mice was not different than HDL derived from human apoA1 transgenic mice.
机译:髓过氧化物酶(MPO)会损害HDL功能,而髓过氧化物酶会选择性地靶向并氧化人apoA1。我们以前发现人apoA1的4WF同工型,其中四个色氨酸残基被苯丙氨酸取代,对MPO介导的功能丧失具有抵抗力。这项研究的目的是生成4WF apoA1转基因小鼠,并比较4WF和野生型人apoA1同工型在体内的功能特性。对于人类apoA1的两种同工型,雄性小鼠的血浆apoA1水平明显高于雌性,这归因于不同的生产率。在血浆apoA1水平匹配的情况下,与人类apoA1转基因相比,4WF转基因的HDL-胆固醇含量略有降低。尽管4WF转基因产品向血浆区室的反向胆固醇转运(RCT)减少了31%,但观察到与肝脏和粪便相当的RCT。两种菌株的血浆具有相似的接受胆固醇的能力,并促进巨噬细胞的离体胆固醇流出。此外,我们观察到4WF转基因HDL被部分保护(〜50%)免受MPO介导的功能丧失,而人apoA1转基因HDL失去了所有ABCA1依赖性胆固醇受体活性。总之,来自4WF转基因小鼠的HDL的结构和功能与源自人apoA1转基因小鼠的HDL没有区别。

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