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Development of a locally advanced orthotopic prostate tumor model in rats for assessment of combined modality therapy
Author(s) -
Vasu Tumati,
Sanjeev Kumar Mathur,
Kwang Hyun Song,
JerTsong Hsieh,
Dawen Zhao,
Masaya Takahashi,
Timothy Dobin,
Leah Gandee,
Timothy D. Solberg,
Amyn A. Habib,
Debabrata Saha
Publication year - 2013
Publication title -
international journal of oncology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.405
H-Index - 122
ISSN - 1019-6439
DOI - 10.3892/ijo.2013.1858
Subject(s) - prostate cancer , prostate , radiation therapy , medicine , fiducial marker , ultrasound , cancer research , cancer , radiation treatment planning , oncogene , radiology , oncology , cell cycle
The purpose of this study was to develop an aggressive locally advanced orthotopic prostate cancer model for assessing high-dose image-guided radiation therapy combined with biological agents. For this study, we used a modified human prostate cancer (PCa) cell line, PC3, in which we knocked down a tumor suppressor protein, DAB2IP (PC3‑KD). These prostate cancer cells were implanted into the prostate of nude or Copenhagen rats using either open surgical implantation or a minimally invasive procedure under ultrasound guidance. We report that: i) these DAB2IP-deficient PCa cells form a single focus of locally advanced aggressive tumors in both nude and Copenhagen rats; ii) the resulting tumors are highly aggressive and are poorly controlled after treatment with radiation alone; iii) ultrasound-guided tumor cell implantation can be used successfully for tumor development in the rat prostate; iv) precise measurement of the tumor volume and the treatment planning for radiation therapy can be obtained from ultrasound and MRI, respectively; and v) the use of a fiducial marker for enhanced radiotherapy localization in the rat orthotopic tumor. This model recapitulates radiation-resistant prostate cancers which can be used to demonstrate and quantify therapeutic response to combined modality treatments.

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