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首页> 外文期刊>Ultrasound in Medicine and Biology >QUANTIFICATION OF ENDOTHELIAL alpha(V)beta(3) EXPRESSION WITH HIGH-FREQUENCY ULTRASOUND AND TARGETED MICROBUBBLES: IN VITRO AND IN VIVO STUDIES
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QUANTIFICATION OF ENDOTHELIAL alpha(V)beta(3) EXPRESSION WITH HIGH-FREQUENCY ULTRASOUND AND TARGETED MICROBUBBLES: IN VITRO AND IN VIVO STUDIES

机译:高频和靶向微泡对内皮α(V)beta(3)表达的定量:体外和体内研究

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摘要

Angiogenesis is a critical feature of plaque development in atherosclerosis and might play a key role in both the initiation and later rupture of plaques. The precursory molecular or cellular pro-angiogenic events that initiate plaque growth and that ultimately contribute to plaque instability, however, cannot be detected directly with any current diagnostic modality. This study was designed to investigate the feasibility of ultrasound molecular imaging of endothelial alpha(v)beta(3) expression in vitro and in vivo using alpha(v)beta(3)-targeted ultrasound contrast agents (UCAs). In the in vitro study, alpha(v)beta(3) expression was confirmed by immunofluorescence in a murine endothelial cell line and detected using the targeted UCA and ultrasound imaging at 18-MHz transmit frequency. In the in vivo study, expression of endothelial alpha(v)beta(3) integrin in murine carotid artery vessels and microvessels of the salivary gland was quantified using targeted UCA and high-frequency ultrasound in seven animals. Our results indicated that endothelial avb3 expression was significantly higher in the carotid arterial wall containing atherosclerotic lesions than in arterial segments without any lesions. We also found that the salivary gland can be used as an internal positive control for successful binding of targeted UCA to avb3 integrin. In conclusion, avb3-targeted UCA allows non-invasive assessment of the expression levels of alpha(v)beta(3) on the vascular endothelium and may provide potential insights into early atherosclerotic plaque detection and treatment monitoring. (C) 2016 World Federation for Ultrasound in Medicine & Biology.
机译:血管生成是动脉粥样硬化斑块发展的关键特征,并且可能在斑块的起始和随后破裂中均起关键作用。然而,用任何当前的诊断方法都不能直接检测到启动斑块生长并最终导致斑块不稳定性的前体分子或细胞促血管生成事件。这项研究旨在调查在体内和体外使用α(v)beta(3)靶向超声造影剂(UCA)对内皮α(v)beta(3)表达进行超声分子成像的可行性。在体外研究中,通过免疫荧光在鼠内皮细胞系中确认了alpha(v)beta(3)表达,并使用靶向UCA和超声成像以18 MHz的发射频率进行了检测。在体内研究中,使用靶向UCA和高频超声在7只动物中定量了鼠颈动脉血管和唾液腺微血管中内皮α(v)beta(3)整合素的表达。我们的结果表明,在含有动脉粥样硬化病变的颈动脉壁中,血管内皮avb3的表达明显高于没有任何病变的动脉段。我们还发现,唾液腺可以用作内部阳性对照,成功地将靶向UCA与avb3整联蛋白结合。总之,以avb3为靶点的UCA可以无创地评估血管内皮上alpha(v)beta(3)的表达水平,并可能为早期动脉粥样硬化斑块的检测和治疗监测提供潜在的见解。 (C)2016世界医学与生物学超声联合会。

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