Literature DB >> 16778194

EZC-prostate models offer high sensitivity and specificity for noninvasive imaging of prostate cancer progression and androgen receptor action.

Mamatha R Seethammagari1, Xiaoming Xie, Norman M Greenberg, David M Spencer.   

Abstract

In vivo imaging advances have greatly expanded the use of animal cancer models. Herein, we describe two new models that permit prostate imaging ex vivo, in vivo, and in utero. Further, we show the use of these models for detecting small metastasis and testing reagents that modulate the androgen receptor (AR) axis. A luciferase reporter gene was directed to the prostate epithelium using three composite promoters called human kallikrein 2 (hK2)-E3/P, PSA-E2/P, and ARR2PB, derived from hK2, PSA, and rat probasin regulatory elements, to generate the EZC1, EZC2, and EZC3-prostate mice, respectively. EZC2 and EZC3-prostate display robust expression in the prostate with only minimal detectable expression in other organs, including testes and epididymis. Luciferase expression was detected as early as embryonic day 13 (E13) in the urogenital track. To image prostate cancer progression, lines of EZC mice were bred with prostate cancer models TRAMP and JOCK1, and imaged longitudinally. When crossed with prostate cancer models, EZC3 facilitated detection of metastatic lesions although total prostate luciferase expression was static or reduced due to weakening of AR-regulated promoters. Castration reduced luciferase expression by 90% and 97% in EZC2 and EZC3 mice, respectively, and use of GnRH antagonist also led to extensive inhibition of reporter activity. The EZC-prostate model permits prostate imaging in vivo and should be useful for imaging prostate development, growth, metastasis, and response to treatment noninvasively and longitudinally. These models also provide powerful new reagents for developing improved drugs that inhibit the AR axis.

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Year:  2006        PMID: 16778194     DOI: 10.1158/0008-5472.CAN-05-3954

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  9 in total

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3.  Wnt and Notch pathways have interrelated opposing roles on prostate progenitor cell proliferation and differentiation.

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4.  The senescence-associated secretory phenotype promotes benign prostatic hyperplasia.

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6.  Oxidative stress promotes benign prostatic hyperplasia.

Authors:  Paz Vital; Patricia Castro; Michael Ittmann
Journal:  Prostate       Date:  2015-09-29       Impact factor: 4.104

7.  Quantitative volumetric imaging of normal, neoplastic and hyperplastic mouse prostate using ultrasound.

Authors:  Shalini Singh; Chunliu Pan; Ronald Wood; Chiuan-Ren Yeh; Shuyuan Yeh; Kai Sha; John J Krolewski; Kent L Nastiuk
Journal:  BMC Urol       Date:  2015-09-21       Impact factor: 2.264

8.  Multimodal imaging guided preclinical trials of vascular targeting in prostate cancer.

Authors:  James Kalmuk; Margaret Folaron; Julian Buchinger; Roberto Pili; Mukund Seshadri
Journal:  Oncotarget       Date:  2015-09-15

9.  Visualising androgen receptor activity in male and female mice.

Authors:  D Alwyn Dart; Jonathan Waxman; Eric O Aboagye; Charlotte L Bevan
Journal:  PLoS One       Date:  2013-08-07       Impact factor: 3.240

  9 in total

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