CTGF公司
心脏病学
动脉瘤
表型
氧化应激
主动脉瘤
主动脉
动脉瘤
内科学
血管平滑肌
胸主动脉
医学
解剖
生物
外科
生长因子
遗传学
受体
基因
平滑肌
作者
Emanuela Branchetti,Paolo Poggio,Rachana Sainger,Eric K. Shang,Juan B. Grau,Benjamin M. Jackson,Edward K. Lai,Michael S. Parmacek,Robert C. Gorman,Joseph H. Gorman,Joseph E. Bavaria,Giovanni Ferrari
出处
期刊:Cardiovascular Research
[Oxford University Press]
日期:2013-08-28
卷期号:100 (2): 316-324
被引量:103
摘要
Dissection and rupture of the ascending aorta are life-threatening conditions resulting in 80% mortality. Ascending aortic replacement in patients presenting with thoracic aortic aneurysm (TAA) is determined by metric measurement. However, a significant number of dissections occur outside of the parameters suggested by the current guidelines. We investigate the correlation among altered haemodynamic condition, oxidative stress, and vascular smooth muscle cell (VSMC) phenotype in controlling tissue homoeostasis.We demonstrate using finite element analysis (FEA) based on computed tomography geometries that TAA patients have higher wall stress in the ascending aorta than non-dilated patients. We also show that altered haemodynamic conditions are associated with increased levels of reactive oxygen species (ROS), direct regulators of the VSMC phenotype in the microregional area of the ascending aorta. Using in vitro and ex vivo studies on human tissues, we show that ROS accumulation correlates with media layer degeneration and increased connective tissue growth factor (CTGF) expression, which modulate the synthetic VSMC phenotype. Results were validated by a murine model of TAA (C57BL/6J) based on Angiotensin II infusion showing that medial thickening and luminal expansion of the proximal aorta is associated with the VSMC synthetic phenotype as seen in human specimens.Increased peak wall stress correlates with change in VSMC towards a synthetic phenotype mediated by ROS accumulation via CTGF. Understanding the molecular mechanisms that regulate VSMC towards a synthetic phenotype could unveil new regulatory pathways of aortic homoeostasis and impact the risk-stratification tool for patients at risk of aortic dissection and rupture.
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