重组载脂蛋白a -米兰诺输注兔颈动脉快速去除脂肪条纹中的脂质

G. Chiesa, E. Monteggia, M. Marchesi, P. Lorenzon, M. Laucello, V. Lorusso, C. Di Mario, E. Karvouni, R. Newton, C. Bisgaier, G. Franceschini, C. Sirtori
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引用次数: 202

摘要

载脂蛋白a - imilano (AIM)是人类载脂蛋白a - i的一种天然变体,赋予携带者对血管疾病的重要保护作用。在先前的研究中,给高胆固醇血症家兔注射重组aim -磷脂(AIM-PL)复合物可显著抑制动脉损伤后新内膜的形成;此外,在apoe缺陷小鼠中反复注射AIM-PL可显著降低动脉粥样硬化的进展。本研究的目的是确定AIM-PL复合物的单次局部输注是否可以促进斑块的消退。采用血管周围电损伤法,在25只家兔的颈总动脉上产生富含脂质的动脉粥样硬化斑块,随后给予1.5%胆固醇饮食90天。兔通过位于右颈动脉起始处的血管内超声(IVUS)导管输注生理盐水、磷脂囊泡或3种不同剂量的AIM-PL(250、500或1000 mg蛋白质)。因此,左颈动脉病变被全身暴露在药物下。通过IVUS分析,注射2个最高剂量的AIM-PL在注射90分钟结束时导致右颈动脉斑块面积减少。在治疗开始72小时后,颈动脉直接(500和1000 mg剂量)和全身(500 mg剂量)给药的组织学证实斑块面积消退。斑块脂质含量与两条动脉的油红O染色显著相似的降低有关。这些结果表明AIM-PL复合物增强动脉脂质去除是导致观察到的斑块变化的机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Recombinant Apolipoprotein A-IMilano Infusion Into Rabbit Carotid Artery Rapidly Removes Lipid From Fatty Streaks
Apolipoprotein A-IMilano (AIM), a natural variant of human apolipoprotein A-I, confers to carriers a significant protection against vascular disease. In previous studies, administration of recombinant AIM-phospholipid (AIM-PL) complexes to hypercholesterolemic rabbits markedly inhibited neointimal formation after arterial injury; moreover, repeated injections of AIM-PL in apoE-deficient mice significantly reduced atherosclerosis progression. The objective of the present study was to determine if a single localized infusion of AIM-PL complexes administered directly to atheromatous lesions could promote plaque regression. Lipid-rich, atheromatous plaques were generated at both common carotid arteries of 25 rabbits by applying a perivascular electric injury, followed by 1.5% cholesterol diet for 90 days. Rabbits were infused with either saline, phospholipid vesicles, or 3 different AIM-PL doses (250, 500, or 1000 mg of protein) delivered through an intravascular ultrasound (IVUS) catheter positioned at the origin of the right carotid. The lesions at the left carotid artery were therefore exposed to the agents systemically. Infusion of AIM-PL at the 2 highest doses caused reduction of right carotid artery plaque area by the end a 90-minute infusion as assessed by IVUS analysis. Plaque area regression was confirmed by histology in carotid arteries receiving direct (500 and 1000 mg doses) and systemic (500 mg dose) delivery, 72 hours after the start of the treatment. Plaque lipid content was associated with significant and similar decreases in Oil Red O staining in both arteries. These results suggest AIM-PL complexes enhanced lipid removal from arteries is the mechanism responsible for the observed plaque changes.
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