首页> 外文会议>IEEE International Symposium on Biomedical Imaging >CARDIAC TISSUE AND ERYTHROCYTE SEPARATION IN BRIGHT-FIELD MICROSCOPY IMAGES OF THE EMBRYONIC ZEBRAFISH HEART FOR MOTION ESTIMATION
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CARDIAC TISSUE AND ERYTHROCYTE SEPARATION IN BRIGHT-FIELD MICROSCOPY IMAGES OF THE EMBRYONIC ZEBRAFISH HEART FOR MOTION ESTIMATION

机译:心脏组织和红细胞分离在胚胎斑马鱼心脏的明场显微镜图像中的运动估计

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Bright-field (BF) microscopy enables imaging the beating embryonic zebrafish heart at high frame rates, thereby revealing motion of both tissues that form the heart and red blood cells (RBCs). However, single-channel BF images lack the specificity seen in multi-color fluorescence microscopy since all structures in the field of view contribute similarly to image contrast. We discuss an algorithm that overcomes this limitation by separating a BF sequence of the beating heart into two distinct image sequences: one showing only the heart and surrounding tissues and the other showing only the transient structures such as RBCs. These sequences can be analyzed separately to characterize heart wall and RBCs motion using common optical flow techniques (e.g. Lucas-Kanade method). We validate our technique on a synthetically generated image sequence and show its potential for facilitating quantitative characterization of heart function during cardiac morphogenesis by examining experimental BF images of the beating embryonic zebrafish heart.
机译:明亮场(BF)显微镜使得能够以高帧速率对搅拌胚胎斑马鱼心脏成像,从而揭示了形成心脏和红细胞(RBC)的两种组织的运动。然而,单通道BF图像缺乏多色荧光显微镜中看到的特异性,因为视野中的所有结构与图像对比度类似地贡献。我们讨论一种算法,通过将跳动心脏分离成两个不同的图像序列来克服这种限制:仅显示心脏和周围组织,另一个仅显示诸如RBC的瞬态结构。可以单独分析这些序列,以使用常见的光学流动技术表征心脏壁和RBC运动(例如Lucas-Kanade方法)。我们在合成生成的图像序列上验证了我们的技术,并通过检查搅拌胚胎斑马皮心脏的实验性BF图像促进心脏形态发生期间促进心脏功能的定量表征的可能性。

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