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Synchrotron microCT imaging of soft tissue in juvenile zebrafish reveals retinotectal projections

机译:少年斑马鱼的软组织的同步rotron microct成像揭示了视网膜营投影

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Biomedical research and clinical diagnosis would benefit greatly from full volume determinations of anatomical phenotype. Comprehensive tools for morphological phenotyping are central for the emerging field of phenomics, which requires high-throughput, systematic, accurate, and reproducible data collection from organisms affected by genetic, disease, or environmental variables. Theoretically, complete anatomical phenotyping requires the assessment of every cell type in the whole organism, but this ideal is presently untenable due to the lack of an unbiased 3D imaging method that allows histopathological assessment of any cell type despite optical opacity. Histopathology, the current clinical standard for diagnostic phenotyping, involves the microscopic study of tissue sections to assess qualitative aspects of tissue architecture, disease mechanisms, and physiological state. However, quantitative features of tissue architecture such as cellular composition and cell counting in tissue volumes can only be approximated due to characteristics of tissue sectioning, including incomplete sampling and the constraints of 2D imaging of 5 micron thick tissue slabs. We have used a small, vertebrate organism, the zebrafish, to test the potential of microCT for systematic macroscopic and microscopic morphological phenotyping. While cell resolution is routinely achieved using methods such as light sheet fluorescence microscopy and optical tomography, these methods do not provide the pancellular perspective characteristic of histology, and are constrained by the limited penetration of visible light through pigmented and opaque specimens, as characterizes zebrafish juveniles. Here, we provide an example of neuroanatomy that can be studied by microCT of stained soft tissue at 1.43 micron isotropic voxel resolution. We conclude that synchrotron microCT is a form of 3D imaging that may potentially be adopted towards more reproducible, large-scale, morphological phenotyping of optically opaque tissues. Further development of soft tissue microCT, visualization and quantitative tools will enhance its utility.
机译:生物医学研究和临床诊断将从解剖学表型的全批量测定中受益匪浅。形态学表型的综合工具是表达的新兴领域的核心,这需要从受遗传,疾病或环境变量影响的生物体的高通量,系统,准确和可重复的数据收集。理论上,完全解剖表型需要评估整个生物体中的每种细胞类型,但由于缺乏无偏见的3D成像方法,这种理想是允许允许任何细胞类型的无偏见的3D成像方法,尽管光不透明度。组织病理学,目前的诊断表型临床标准涉及组织切片的微观研究,以评估组织结构,疾病机制和生理状态的定性方面。然而,组织体积中的组织结构的定量特征,例如在组织体积中计数,只能近似由于组织切片的特征,包括不完全采样和5微米厚组织板的2D成像的约束。我们使用了一个小脊椎动物,斑马鱼,以测试Microct用于系统宏观和微观形态表型的潜力。虽然使用诸如光片荧光显微镜和光学断层扫描的方法常规实现细胞分辨率,但这些方法不提供组织学的雌孔透视特性,并且受到可见光通过着色和不透明标本的有限渗透的限制,如斑马鱼幼年症所表征。在这里,我们提供了神经肿瘤的举例,其可以通过染色的软组织的Microct在1.43微米各向同性体素分辨率中研究。我们得出结论,同步rotron Microct是3D成像的形式,可能潜在地朝着更可重现的光学不透明组织的更可重复,大规模的形态学表型。进一步发展软组织MicroCT,可视化和定量工具将增强其实用性。

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