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Optical Diagnostics of Osteoblast Cells and Osteogenic Drug Screening

机译:成骨细胞的光学诊断和成骨药物筛选

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摘要

Microfluidic device based diagnostics involving optical fibre path, in situ imaging and spectroscopy are gaining importance due to recent advances in diagnostics instrumentation and methods, besides other factors such as low amount of reagent required for analysis, short investigation times, and potential possibilities to replace animal model based study in near future. It is possible to grow and monitor tissues in vitro in microfluidic lab-on-chip. It may become a transformative way of studying how cells interact with drugs, pathogens and biomaterials in physiologically relevant microenvironments. To a large extent, progress in developing clinically viable solutions has been constrained because of (ⅰ) contradiction between in vitro and in vivo results and (ⅱ) animal model based and clinical studies which is very expensive. Our study here aims to evaluate the usefulness of microfluidic device based 3D tissue growth and monitoring approach to better emulate physiologically and clinically relevant microenvironments in comparison to conventional in vitro 2D culture. Moreover, the microfluidic methodology permits precise high-throughput investigations through real-time imaging while using very small amounts of reagents and cells. In the present study, we report on the details of an osteoblast cell based 3D microfluidic platform which we employ for osteogenic drug screening. The drug formulation is functionalized with fluorescence and other biomarkers for imaging and spectroscopy, respectively. Optical fibre coupled paths are used to obtain insight regarding the role of stress/flow pressure fluctuation and nanoparticle-drug concentration on the osteoblast growth and osteogenic properties of bone.
机译:由于诊断仪器和方法的最新进展,基于微流体设备的诊断方法涉及光纤路径,原位成像和光谱学正变得越来越重要,此外还有其他因素,例如分析所需的试剂量少,研究时间短以及替换动物的潜在可能性。基于模型的研究在不久的将来。在微流控芯片实验室中可以体外生长和监测组织。它可能成为研究细胞在生理相关的微环境中如何与药物,病原体和生物材料相互作用的一种变革方式。在很大程度上,由于(ⅰ)体外和体内结果之间的矛盾以及(ⅱ)基于动物模型和临床研究的成本很高,因此,临床上可行的解决方案的开发受到了限制。我们的研究旨在评估基于微流体设备的3D组织生长和监测方法的有效性,与常规的体外2D培养相比,该方法可以更好地模拟生理和临床相关的微环境。此外,微流体方法允许通过实时成像进行精确的高通量研究,同时使用非常少量的试剂和细胞。在本研究中,我们报告了基于成骨细胞的3D微流体平台的详细信息,我们将其用于成骨药物筛选。分别用荧光和其他生物标记功能对药物制剂进行成像和光谱分析。光纤耦合路径用于获得有关应力/流量压力波动和纳米颗粒药物浓度对成骨细胞生长和骨骼成骨特性的作用的见解。

著录项

  • 来源
    《Photonic therapeutics and diagnostics XII》|2016年|96894I.1-96894I.6|共6页
  • 会议地点 San Francisco CA(US)
  • 作者单位

    Laboratory for Integrative Multiscale Engineering Materials and Systems, Department of Aerospace Engineering, Indian Institute of Science, Bangalore 560012, India;

    Laboratory for Integrative Multiscale Engineering Materials and Systems, Department of Aerospace Engineering, Indian Institute of Science, Bangalore 560012, India;

    Laboratory for Integrative Multiscale Engineering Materials and Systems, Department of Aerospace Engineering, Indian Institute of Science, Bangalore 560012, India;

    Laboratory for Integrative Multiscale Engineering Materials and Systems, Department of Aerospace Engineering, Indian Institute of Science, Bangalore 560012, India;

  • 会议组织
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Osteoblast cells; microfluidic; drug screening; scaffold; tissue engineering; spectroscopy; fluorescence imaging;

    机译:成骨细胞;微流体药物筛选脚手架;组织工程;光谱学荧光成像;
  • 入库时间 2022-08-26 13:45:07

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