Introduction of Androgen Receptor Targeting shRNA Inhibits Tumor Growth in Patient-Derived Prostate Cancer Xenografts

被引:0
|
作者
Thomas, Patrick B. [1 ,2 ,3 ]
Alinezhad, Saeid [1 ,2 ]
Joshi, Andre [1 ,2 ,3 ,4 ]
Sweeney, Katrina [1 ,2 ]
Tse, Brian W. C. [5 ]
Tevz, Gregor [1 ,2 ]
Mcpherson, Stephen [1 ,2 ]
Nelson, Colleen C. [1 ,2 ,6 ]
Williams, Elizabeth D. [1 ,2 ,3 ,6 ]
机构
[1] Queensland Univ Technol QUT, Translat Res Inst TRI, Sch Biomed Sci, Fac Hlth, Brisbane, Qld 4102, Australia
[2] Australian Prostate Canc Res Ctr Queensland, Brisbane, Qld 4102, Australia
[3] Queensland Bladder Canc Initiat QBCI, Brisbane, Qld 4102, Australia
[4] Princess Alexandra Hosp, Dept Urol, Brisbane, Qld 4102, Australia
[5] Translat Res Inst, Preclin Imaging Facil, Brisbane, Qld 4102, Australia
[6] Queensland Univ Technol QUT, Ctr Genom & Personalised Hlth, Brisbane, Qld 4000, Australia
关键词
prostate cancer; organoids; precision medicine; patient-derived xenograft; androgen receptor; DRUG DISCOVERY; STATISTICS; MODEL;
D O I
10.3390/curroncol30110683
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Patient-derived xenograft (PDX) models have been established as important preclinical cancer models, overcoming some of the limitations associated with the use of cancer cell lines. The utility of prostate cancer PDX models has been limited by an inability to genetically manipulate them in vivo and difficulties sustaining PDX-derived cancer cells in culture. Viable, short-term propagation of PDX models would allow in vitro transfection with traceable reporters or manipulation of gene expression relevant to different studies within the prostate cancer field. Here, we report an organoid culture system that supports the growth of prostate cancer PDX cells in vitro and permits genetic manipulation, substantially increasing the scope to use PDXs to study the pathobiology of prostate cancer and define potential therapeutic targets. We have established a short-term PDX-derived in vitro cell culture system which enables genetic manipulation of prostate cancer PDXs LuCaP35 and BM18. Genetically manipulated cells could be re-established as viable xenografts when re-implanted subcutaneously in immunocompromised mice and were able to be serially passaged. Tumor growth of the androgen-dependent LuCaP35 PDX was significantly inhibited following depletion of the androgen receptor (AR) in vivo. Taken together, this system provides a method to generate novel preclinical models to assess the impact of controlled genetic perturbations and allows for targeting specific genes of interest in the complex biological setting of solid tumors.
引用
收藏
页码:9437 / 9447
页数:11
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