Perfused Three-dimensional Organotypic Culture of Human Cancer Cells for Therapeutic Evaluation

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作者
Xiao Wan
Steven Ball
Frances Willenbrock
Shaoyang Yeh
Nikola Vlahov
Delia Koennig
Marcus Green
Graham Brown
Sanjeeva Jeyaretna
Zhaohui Li
Zhanfeng Cui
Hua Ye
Eric O’Neill
机构
[1] CRUK/MRC Oxford Institute of Radiation Biology,Department of Neurosurgery
[2] University of Oxford,undefined
[3] ORCRB Research Building,undefined
[4] Roosevelt Drive,undefined
[5] Oxford Instruments Nanoscience,undefined
[6] Tubney Woods,undefined
[7] Institute of Biomedical Engineering,undefined
[8] Department of Engineering Science,undefined
[9] University of Oxford,undefined
[10] Old Road Campus Research Building,undefined
[11] John Radcliffe Hospital,undefined
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Pharmaceutical research requires pre-clinical testing of new therapeutics using both in-vitro and in-vivo models. However, the species specificity of non-human in-vivo models and the inadequate recapitulation of physiological conditions in-vitro are intrinsic weaknesses. Here we show that perfusion is a vital factor for engineered human tissues to recapitulate key aspects of the tumour microenvironment. Organotypic culture and human tumour explants were allowed to grow long-term (14–35 days) and phenotypic features of perfused microtumours compared with those in the static culture. Differentiation status and therapeutic responses were significantly different under perfusion, indicating a distinct biological response of cultures grown under static conditions. Furthermore, heterogeneous co-culture of tumour and endothelial cells demonstrated selective cell-killing under therapeutic perfusion versus episodic delivery. We present a perfused 3D microtumour culture platform that sustains a more physiological tissue state and increased viability for long-term analyses. This system has the potential to tackle the disadvantages inherit of conventional pharmaceutical models and is suitable for precision medicine screening of tumour explants, particularly in hard-to-treat cancer types such as brain cancer which suffer from a lack of clinical samples.
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