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Unique remodeling processes after vascular injury in intracranial arteries: analysis using a novel mouse model

机译:颅内动脉血管损伤后的独特重塑过程:使用新型小鼠模型的分析

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摘要

The effectiveness of angioplasty and stenting in intracranial atherosclerotic diseases is controversial due to high rates of delayed restenosis and hemorrhage compared with extracranial arteries. However, the mechanisms underlying these differences are still unclear, because their pathophysiology is yet to be examined. To address this issue, we established a novel vascular injury model in the intracranial internal carotid arteries (IICAs) in mice, and analyzed the remodeling process in comparison to that of the femoral arteries (FAs). In IICAs, neointimal hyperplasia was observed from day 14 and grew until day 56. Although smooth muscle cells (SMCs) emerged in the neointima from day 28, SMCs in the injured media were continuously lost with eventual extinction of the media. Re-endothelialization was started from day 7 and completed on day 28. Accumulation of macrophages was continued in the adventitia until day 56. Compared with FAs, the following points are unique in IICAs: (1) delayed continuous formation of neointima; (2) accumulation of macrophages in the media on day 14; (3) continuous loss of SMCs in the media followed by extinction of the media itself; and (4) continuously growing adventitia. These pathophysiologic differences might be associated with unfavorable outcomes in percutaneous transluminal angioplasty and stenting in intracranial arteries.
机译:与颅外动脉相比,由于延迟再狭窄和出血的发生率高,在颅内动脉粥样硬化疾病中血管成形术和支架置入术的有效性引起争议。但是,尚不清楚这些差异的潜在机制,因为尚未对其病理生理学进行检查。为了解决这个问题,我们在小鼠的颅内颈内动脉(IICAs)中建立了一种新型的血管损伤模型,并与股动脉(FAs)进行了对比分析。在IICA中,从第14天开始观察到新内膜增生,并一直持续到第56天。尽管从第28天起在新内膜中出现了平滑肌细胞(SMC),但受伤的培养基中的SMC不断丢失,最终培养基消失了。重新内皮化从第7天开始并在第28天完成。外膜中巨噬细胞的积累一直持续到第56天。与FAs相比,在IICAs中有以下几点独特之处:(1)延迟了新内膜的连续形成; (2)在第14天,巨噬细胞在培养基中积累; (3)培养基中SMC的连续损失,然后培养基本身灭绝; (4)外膜不断增长。这些病理生理差异可能与颅内动脉经皮腔内血管成形术和支架置入术的不良结果有关。

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