低密度脂蛋白受体相关蛋白1的平滑肌细胞缺失会加剧血管紧张素II诱导的肠系膜上动脉和升主动脉瘤形成。
Smooth muscle cell deletion of low-density lipoprotein receptor-related protein 1 augments angiotensin II-induced superior mesenteric arterial and ascending aortic aneurysms.
作者信息
Davis Frank M, Rateri Debra L, Balakrishnan Anju, Howatt Deborah A, Strickland Dudley K, Muratoglu Selen C, Haggerty Christopher M, Fornwalt Brandon K, Cassis Lisa A, Daugherty Alan
机构信息
From the Saha Cardiovascular Research Center (F.M.D., D.L.R., A.B., D.A.H., C.M.H., B.K.F., A.D.), Department of Pediatrics (B.K.F.), Department of Pharmacology and Nutritional Sciences (L.A.C.), University of Kentucky, Lexington; and Center for Vascular and Inflammatory Diseases, University of Maryland School of Medicine, Baltimore (D.K.S., S.C.M.).
出版信息
Arterioscler Thromb Vasc Biol. 2015 Jan;35(1):155-62. doi: 10.1161/ATVBAHA.114.304683. Epub 2014 Nov 13.
OBJECTIVE
Low-density lipoprotein receptor-related protein 1 (LRP1), a multifunctional protein involved in endocytosis and cell signaling pathways, leads to several vascular pathologies when deleted in vascular smooth muscle cells (SMCs). The purpose of this study was to determine whether LRP1 deletion in SMCs influenced angiotensin II-induced arterial pathologies.
APPROACH AND RESULTS
LRP1 protein abundance was equivalent in selected arterial regions, but SMC-specific LRP1 depletion had no effect on abdominal and ascending aortic diameters in young mice. To determine the effects of LRP1 deficiency on angiotensin II vascular responses, SMC-specific LRP1 (smLRP1(+/+)) and smLRP1-deficient (smLRP1(-/-)) mice were infused with saline, angiotensin II, or norepinephrine. Several smLRP(-/-) mice died of superior mesenteric arterial (SMA) rupture during angiotensin II infusion. In surviving mice, angiotensin II profoundly augmented SMA dilation in smLRP1(-/-) mice. SMA dilation was blood pressure dependent as demonstrated by a similar response during norepinephrine infusion. SMA dilation was also associated with profound macrophage accumulation, but minimal elastin fragmentation. Angiotensin II infusion led to no significant differences in abdominal aorta diameters between smLRP1(+/+) and smLRP1(-/-) mice. In contrast, ascending aortic dilation was exacerbated markedly in angiotensin II-infused smLRP1(-/-) mice, but norepinephrine had no significant effect on either aortic region. Ascending aortas of smLRP1(-/-) mice infused with angiotensin II had minimal macrophage accumulation but significantly increased elastin fragmentation and mRNA abundance of several LRP1 ligands including MMP-2 (matrix metalloproteinase-2) and uPA (urokinase plasminogen activator).
CONCLUSIONS
smLRP1 deficiency had no effect on angiotensin II-induced abdominal aortic aneurysm formation. Conversely, angiotensin II infusion in smLRP1(-/-) mice exacerbated SMA and ascending aorta dilation. Dilation in these 2 regions had differential association with blood pressure and divergent pathological characteristics.
目的
低密度脂蛋白受体相关蛋白1(LRP1)是一种参与内吞作用和细胞信号通路的多功能蛋白,在血管平滑肌细胞(SMC)中缺失时会导致多种血管病变。本研究的目的是确定SMC中LRP1的缺失是否会影响血管紧张素II诱导的动脉病变。
方法与结果
在选定的动脉区域,LRP1蛋白丰度相当,但SMC特异性LRP1缺失对年轻小鼠的腹主动脉和升主动脉直径没有影响。为了确定LRP1缺乏对血管紧张素II血管反应的影响,对SMC特异性LRP1(smLRP1(+/+))和smLRP1缺陷(smLRP1(-/-))小鼠输注生理盐水、血管紧张素II或去甲肾上腺素。在血管紧张素II输注期间,几只smLRP(-/-)小鼠死于肠系膜上动脉(SMA)破裂。在存活的小鼠中,血管紧张素II显著增强了smLRP1(-/-)小鼠的SMA扩张。去甲肾上腺素输注期间的类似反应表明,SMA扩张与血压有关。SMA扩张还与大量巨噬细胞积聚有关,但弹性蛋白断裂最少。血管紧张素II输注导致smLRP1(+/+)和smLRP1(-/-)小鼠的腹主动脉直径没有显著差异。相反,在血管紧张素II输注的smLRP1(-/-)小鼠中,升主动脉扩张明显加剧,但去甲肾上腺素对两个主动脉区域均无显著影响。输注血管紧张素II的smLRP1(-/-)小鼠的升主动脉巨噬细胞积聚最少,但弹性蛋白断裂显著增加,包括基质金属蛋白酶-2(MMP-2)和尿激酶型纤溶酶原激活剂(uPA)在内的几种LRP1配体的mRNA丰度也显著增加。
结论
smLRP1缺乏对血管紧张素II诱导的腹主动脉瘤形成没有影响。相反,在smLRP1(-/-)小鼠中输注血管紧张素II会加剧SMA和升主动脉扩张。这两个区域的扩张与血压有不同的关联,且病理特征不同。
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