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A Murine Model of Arterial Restenosis: Technical Aspects of Femoral Wire Injury

机译:小鼠动脉再狭窄模型:股线损伤的技术方面

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摘要

Cardiovascular disease caused by atherosclerosis is the leading cause of death in the developed world. Narrowing of the vessel lumen, due to atherosclerotic plaque development or the rupturing of established plaques, interrupts normal blood flow leading to various morbidities such as myocardial infarction and stroke. In the clinic endovascular procedures such as angioplasty are commonly performed to reopen the lumen. However, these treatments inevitably damage the vessel wall as well as the vascular endothelium, triggering an excessive healing response and the development of a neointimal plaque that extends into the lumen causing vessel restenosis (re-narrowing). Restenosis remains a major cause of failure of endovascular treatments for atherosclerosis. Thus, preclinical animal models of restenosis are vitally important for investigating the pathophysiological mechanisms as well as translational approaches to vascular interventions. Among several murine experimental models, femoral artery wire injury is widely accepted as the most suitable for studies of post-angioplasty restenosis because it closely resembles the angioplasty procedure that injures both endothelium and vessel wall. However, many researchers have difficulty utilizing this model due to its high degree of technical difficulty. This is primarily because a metal wire needs to be inserted into the femoral artery, which is approximately three times thinner than the wire, to generate sufficient injury to induce prominent neointima. Here, we describe the essential surgical details to effectively overcome the major technical difficulties of this model. By following the presented procedures, performing the mouse femoral artery wire injury becomes easier. Once familiarized, the whole procedure can be completed within 20 min.
机译:由动脉粥样硬化引起的心血管疾病是发达国家的主要死亡原因。由于动脉粥样硬化斑块的发展或已建立的斑块的破裂,血管腔的狭窄会中断正常的血液流动,从而导致各种疾病,例如心肌梗塞和中风。在临床中,通常进行诸如血管成形术的血管内手术以重新打开管腔。然而,这些治疗不可避免地损害了血管壁和血管内皮,触发了过度的愈合反应,并形成了延伸至管腔的新内膜斑块,从而引起血管再狭窄(再狭窄)。再狭窄仍然是动脉粥样硬化血管内治疗失败的主要原因。因此,再狭窄的临床前动物模型对于研究病理生理机制以及血管干预的转化方法至关重要。在几种鼠类实验模型中,股动脉钢丝损伤被广泛认为是最适合于血管成形术后再狭窄的研究,因为它非常类似于会损伤内皮和血管壁的血管成形术。但是,由于该模型的技术难度很高,因此许多研究人员难以使用该模型。这主要是因为需要将一根金属线插入到股动脉中,该金属线的厚度大约是该线的三倍,以产生足够的损伤以引起明显的新内膜。在这里,我们描述了必要的手术细节,以有效克服该模型的主要技术难题。通过遵循提出的程序,执行小鼠股动脉钢丝损伤变得更加容易。熟悉后,整个过程可以在20分钟内完成。

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