Transrectal gene therapy of the prostate in the canine model

被引:0
|
作者
Kyle J Weld
Brant E Mayher
James A Allay
Jody L Cockroft
Christopher P Reed
Mildred M Randolph
Yi Lu
Mitchell S Steiner
Jeffrey R Gingrich
机构
[1] Urologic Research Laboratories,Department of Comparative Medicine
[2] University of Tennessee,undefined
[3] GTx Inc.,undefined
[4] University of Tennessee,undefined
来源
Cancer Gene Therapy | 2002年 / 9卷
关键词
gene therapy; prostate; adenovirus; β-galactosidase;
D O I
暂无
中图分类号
学科分类号
摘要
Direct transrectal delivery of therapeutic genes utilizing adenoviral vectors for advanced prostate cancer may offer effective treatment at the molecular level. Large animal models to assess feasibility and the intraprostatic and systemic dissemination patterns of these vectors have not been reported. For these studies, a replication-deficient (E1−/E3−) recombinant adenovirus (AdRSVlacZ) expressing bacterial β-galactosidase (β-gal) was delivered under transrectal ultrasound guidance. Two prostate biopsies, followed by concurrent injection of 4.8×109 pfu of the adenoviral vector divided into either 1 or 2 mL of diluent, were performed (n=4). Swabs of the rectum, sputum, and urine were collected and after 72 hours, the animals were sacrificed. Specimens were assayed for the presence of virus and β-gal activity. Rectal swabs were transiently positive, whereas urine and sputum samples showed no detectable vector throughout the experiment. β-gal activity was observed at the prostate injection sites with detectable activity noted up to 7.5 mm away from the injection site. Systemic dissemination was observed regardless of the injected volume. In conclusion, transrectal prostate biopsy with concurrent prostate injection is a feasible method to deliver therapeutic adenoviral vectors for the treatment of prostate cancer; however, systemic distribution and temporary rectal shedding of virus should be anticipated.
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页码:189 / 196
页数:7
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