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Three-Dimensional Microtumors for Probing Heterogeneity of Invasive Bladder Cancer

机译:用于探测侵入性膀胱癌的异质性的三维显微镜

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摘要

Bladder cancer is an increasingly common malignancy, and muscle invasive bladder cancer is associated with particularly high rates of morbidity and mortality. The morpho- logic and molecular diversity of bladder cancer poses significant challenges in elucidating the invasion mechanisms responsible for disease progression. Furthermore, conventional invasion assays do not provide a physiological context for studying bladder cancer invasion within 3D microenvironments and have limited ability to capture the contribution of cellular phenotypic heterogeneity to disease progression. Here, we describe the development of a 3D microtumor invasion model suitable for the analysis of cellular phenotypic heterogeneity in cell lines and primary tumor cells from bladder cancer patients. This model incorporates a self-assembly approach for recapitulating features of bladder cancer invasion in 3D microenvironments and probing the invasive cell subpopulations. The gene expression profiles of invading microtumors were analyzed by incorporating a gold nanorod-locked nucleic acid biosensor. The incorporation of the single cell biosensor and transient gene knockdown into the system revealed the formation of invasive leader cells with upregulated Delta-like ligand 4 (DLL4) expression as well as the role of NOTCH1-DLL4 signaling in collective bladder cancer invasion. The involvement of DLL4 expressing cells in bladder cancer invasion was also observed in patient samples obtained from transurethral resection. Collectively, our study demonstrates a 3D microtumor invasion model for investigating intracellular heterogeneity of bladder cancer invasion and analyzing patient derived samples toward personalized medicine applications.
机译:膀胱癌是一种越来越常见的恶性肿瘤,肌肉侵袭性膀胱癌与特别高的发病率和死亡率有关。膀胱癌的形态逻辑和分子多样性阐述了阐明疾病进展的侵袭机制的重大挑战。此外,常规的侵袭测定不能提供用于研究3D微环境内的膀胱癌侵袭的生理背景,并具有捕获细胞表型异质性对疾病进展的贡献的有限能力。这里,我们描述了适用于分析来自膀胱癌患者细胞系细胞系和原代肿瘤细胞细胞表型异质性的3D微型侵袭模型的发展。该模型包括一种自组装方法,用于重新携带3D微环境中膀胱癌侵袭的特征,探测侵入性细胞群。通过掺入金纳米杆锁定的核酸生物传感器来分析入侵微型器的基因表达谱。将单细胞生物传感器和瞬时基因敲入系统的掺入揭示了具有上调的δ样配体4(DLL4)表达的侵入式领导细胞以及Notch1-DLL4信号传导在集体膀胱癌侵袭中的作用。在从经尿道切除术中获得的患者样品中也观察到DLL4表达细胞在膀胱癌侵袭中的参与。集体,我们的研究表明,用于研究膀胱癌侵袭的细胞内异质性和分析患者衍生样品对个性化药物应用的3D微量侵袭模型。

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  • 来源
    《Analytical chemistry》 |2020年第13期|共8页
  • 作者单位

    Penn State Univ Dept Mech Engn University Pk PA 16802 USA;

    Penn State Univ Dept Biomed Engn University Pk PA 16802 USA;

    Penn State Hlth Milton S Hershey Med Ctr Dept Pathol &

    Lab Med Hershey PA 17033 USA;

    Penn State Hlth Milton S Hershey Med Ctr Dept Surg Div Urol Hershey PA 17033 USA;

    Penn State Hlth Milton S Hershey Med Ctr Dept Surg Div Urol Hershey PA 17033 USA;

    Penn State Hlth Milton S Hershey Med Ctr Div Urol Dept Surg Dept Pathol &

    Lab Med Hershey PA 17033 USA;

    Penn State Univ Dept Mech Engn University Pk PA 16802 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
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