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Apolipoprotein A-I mimetic peptides and their role in atherosclerosis prevention.

机译:载脂蛋白A-1模拟肽及其在预防动脉粥样硬化中的作用。

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The importance of apolipoprotein A-I (apoA-I) in atherosclerosis was established by testing in animal models, and its potential usefulness in humans has been confirmed in preliminary studies. ApoA-I is a large protein comprising 243 amino acids, which means that venous administration is necessary. In addition, manufacture of apoA-I is difficult and expensive. Research has, therefore, been directed towards finding smaller peptide mimetics that produce similar results to apoA-I, but that are easier to manufacture and administer. The earliest peptides mimicked some of the lipid-binding properties of apoA-I but did not prevent atherosclerosis in mice. A detailed study of the physical-chemical characteristics of these peptides led to the realization that the hydrophobic region of the peptide was critical in determining bioactivity. A potent peptide, 4F, which was synthesized wholly from D-amino acids, could be given orally. Use of 4F significantly improved the function of HDL in mice and monkeys. When 4F was administered in combination with a statin, lesion size and macrophage content were reduced in mice with atherosclerosis, and lesions regressed in older mice. Vasoreactivity and endothelial sloughing were also improved in other rodent studies. Early human clinical trials are now being carried out on 4F. Here, we review the studies on apoA-I mimetic peptides that have been carried out so far.
机译:载脂蛋白A-I(apoA-I)在动脉粥样硬化中的重要性已通过在动物模型中的测试确定,并且其在人体中的潜在用途已在初步研究中得到证实。 ApoA-I是一种包含243个氨基酸的大蛋白,这意味着需要静脉给药。另外,制造apoA-1是困难且昂贵的。因此,研究针对寻找较小的肽模拟物,其产生与apoA-I相似的结果,但是更易于制造和施用。最早的肽模拟了apoA-I的某些脂质结合特性,但不能预防小鼠的动脉粥样硬化。对这些肽的物理化学特征的详细研究导致人们认识到,肽的疏水区对于确定生物活性至关重要。可以口服完全由D-氨基酸合成的有效肽4F。 4F的使用显着改善了HDL在小鼠和猴子中的功能。当将4F与他汀类药物联合给药时,动脉粥样硬化小鼠的病变大小和巨噬细胞含量减少,而老年小鼠则病变消退。在其他啮齿动物研究中,血管反应性和内皮脱落也得到了改善。现在正在4F上进行早期人体临床试验。在这里,我们回顾了迄今为止已进行的关于apoA-I模拟肽的研究。

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