首页> 美国卫生研究院文献>Journal of Lipid Research >Oral administration of L-mR18L a single domain cationic amphipathic helical peptide inhibits lesion formation in ApoE null mice
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Oral administration of L-mR18L a single domain cationic amphipathic helical peptide inhibits lesion formation in ApoE null mice

机译:口服L-mR18L(单结构域阳离子两亲性螺旋肽)可抑制ApoE null小鼠的病变形成

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摘要

We have shown that Ac-hE18A-NH2, a dual-domain cationic apolipoprotein-mimetic peptide, reduces plasma cholesterol levels in dyslipidemic mice. Two single-domain cationic peptides based on the lytic class L peptide 18L were developed to test the hypothesis that a single-domain cationic amphipathic peptide can reduce atherosclerosis in apolipoprotein (apo)E null mice when orally administered. To incorporate anti-inflammatory properties, aromatic residues were clustered in the nonpolar face similar to peptide 4F, resulting in modified 18L (m18L). To reduce lytic properties, the Lys residues of 18L were replaced with Arg with the resulting peptide called modified R18L (mR18L). Biophysical studies showed that mR18L had stronger interactions with lipids than did m18L. Peptide mR18L was also more effective than m18L in promoting LDL uptake by HepG2 cells. ApoE null mice received normal chow or chow containing m18L or mR18L for six weeks. A significant reduction in plasma cholesterol and aortic sinus lesion area was seen only in the mR18L group. Plasma from mice administered mR18L, unlike those from the control and m18L groups, did not enhance monocyte adhesion to endothelial cells. Thus oral administration of mR18L reduces plasma cholesterol and lesion formation and inhibits monocyte adhesion.
机译:我们已经表明,Ac-hE18A-NH2,一个双域阳离子载脂蛋白模拟肽,可以降低血脂异常小鼠的血浆胆固醇水平。开发了两种基于溶解性L类肽18L的单域阳离子肽,以测试以下假设:口服时,单域阳离子两亲肽可以减少载脂蛋白(apo)E缺失小鼠的动脉粥样硬化。为了结合抗炎特性,类似于肽4F,芳香族残基聚集在非极性面上,从而产生修饰的18L(m18L)。为了降低裂解特性,将18L的Lys残基替换为Arg,得到的肽称为修饰的R18L(mR18L)。生物物理研究表明,mR18L与脂质的相互作用比m18L更强。肽mR18L在促进HepG2细胞摄取LDL方面也比m18L更有效。 ApoE null小鼠接受正常食物或含有m18L或mR18L的食物六周。仅在mR18L组中,血浆胆固醇和主动脉窦病变区域显着减少。与对照组和m18L组的小鼠不同,施用mR18L的小鼠的血浆不能增强单核细胞与内皮细胞的粘附。因此,口服mR18L可降低血浆胆固醇和病变的形成,并抑制单核细胞粘附。

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