基底上皮干细胞是前列腺癌起始的有效靶点。
Basal epithelial stem cells are efficient targets for prostate cancer initiation.
机构信息
Department of Microbiology, The Howard Hughes Medical Institute, University of California, Los Angeles, CA 90095, USA.
出版信息
Proc Natl Acad Sci U S A. 2010 Feb 9;107(6):2610-5. doi: 10.1073/pnas.0913873107. Epub 2010 Jan 25.
Abstract
Prevailing theories suggest that luminal cells are the origin of prostate cancer because it is histologically defined by basal cell loss and malignant luminal cell expansion. We introduced a series of genetic alterations into prospectively identified populations of murine basal/stem and luminal cells in an in vivo prostate regeneration assay. Stromal induction of FGF signaling, increased expression of the ETS family transcription factor ERG1, and constitutive activation of PI3K signaling were evaluated. Combination of activated PI3K signaling and heightened androgen receptor signaling, which is associated with disease progression to androgen independence, was also performed. Even though luminal cells fail to respond, basal/stem cells demonstrate efficient capacity for cancer initiation and can produce luminal-like disease characteristic of human prostate cancer in multiple models. This finding provides evidence in support of basal epithelial stem cells as one target cell for prostate cancer initiation and demonstrates the propensity of primitive cells for tumorigenesis.
摘要
目前的理论认为,腔细胞是前列腺癌的起源,因为它在组织学上的定义是基底细胞丢失和恶性腔细胞扩张。我们在体内前列腺再生试验中,向预先确定的小鼠基底/干细胞和腔细胞群体中引入了一系列遗传改变。评估了成纤维细胞生长因子信号的基质诱导、ETS 家族转录因子 ERG1 的表达增加以及 PI3K 信号的组成性激活。还进行了激活的 PI3K 信号和增强的雄激素受体信号的组合,这与疾病进展到雄激素非依赖性相关。尽管腔细胞不能响应,但基底/干细胞表现出有效的癌症起始能力,并能在多种模型中产生类似于人类前列腺癌的腔样疾病。这一发现为基底上皮干细胞作为前列腺癌起始的靶细胞提供了证据,并证明了原始细胞的致瘤倾向。
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