作者
Jennifer A Locke, Emma S Guns, Amy A Lubik, Hans H Adomat, Stephen C Hendy, Catherine A Wood, Susan L Ettinger, Martin E Gleave, Colleen C Nelson
发表日期
2008/8/1
期刊
Cancer research
卷号
68
期号
15
页码范围
6407-6415
出版商
American Association for Cancer Research
简介
Although systemic androgen deprivation prolongs life in advanced prostate cancer, remissions are temporary because patients almost uniformly progress to a state of a castration-resistant prostate cancer (CRPC) as indicated by recurring PSA. This complex process of progression does not seem to be stochastic as the timing and phenotype are highly predictable, including the observation that most androgen-regulated genes are reactivated despite castrate levels of serum androgens. Recent evidence indicates that intraprostatic levels of androgens remain moderately high following systemic androgen deprivation therapy, whereas the androgen receptor (AR) remains functional, and silencing the AR expression following castration suppresses tumor growth and blocks the expression of genes known to be regulated by androgens. From these observations, we hypothesized that CRPC progression is not …
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