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Ultra-high frequency ultrasound biomicroscopy and high throughput cardiovascular phenotyping in a large scale mouse mutagenesis screen

机译:大规模小鼠诱变筛选中的超高频超声生物显微镜和高通量心血管表型

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Ultrasound biomicroscopy (UBM) is ideally suited for phenotyping fetal mice for congenital heart disease (CHD), as imaging can be carried out noninvasively to provide both hemodynamic and structural information essential for CHD diagnosis. Using the UBM (Vevo 2100; 40Hz) in conjunction with the clinical ultrasound system (Acuson Sequioa C512; 15Hz), we developed a two-step screening protocol to scan thousands fetuses derived from ENU mutagenized pedigrees. A wide spectrum of CHD was detected by the UBM, which were subsequently confirmed with follow-up necropsy and histopathology examination with episcopic fluorescence image capture. CHD observed included outflow anomalies, left/right heart obstructive lesions, septal/valvular defects and cardiac situs anomalies. Meanwhile, various extracardiac defects were found, such as polydactyly, craniofacial defects, exencephaly, omphalocele, cleft palate, most of which were associated with cardiac defects. Our analyses showed the UBM was better at assessing cardiac structure and blood flow profiles, while conventional ultrasound allowed higher throughput low-resolution screening. Our study showed the integration of conventional clinical ultrasound imaging with the UBM for fetal mouse cardiovascular phenotyping can maximize the detection and recovery of CHD mutants.
机译:超声生物显微镜(UBM)非常适合先天性心脏病(CHD)的胎鼠表型分析,因为可以无创地进行成像以提供CHD诊断必不可少的血液动力学和结构信息。我们将UBM(Vevo 2100; 40Hz)与临床超声系统(Acuson Sequioa C512; 15Hz)结合使用,开发了两步筛选方案,可扫描成千上万来自ENU诱变家系的胎儿。 UBM检测到了广泛的冠心病,随后通过尸检和组织病理学检查(通过镜射荧光图像捕获)进行了确认。观察到的冠心病包括流出异常,左/右心脏梗阻性病变,间隔/瓣膜缺损和心脏部位异常。同时,发现了多种心脏外缺陷,例如多指,颅面缺陷,脑电,卵裂,卵裂,pa裂,其中大多数与心脏缺陷有关。我们的分析表明,UBM可以更好地评估心脏结构和血流状况,而常规超声可以进行更高通量的低分辨率筛查。我们的研究表明,将常规临床超声成像与UBM整合用于胎鼠心血管表型可以最大程度地检测和恢复CHD突变体。

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