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干细胞/祖细胞及中间细胞类型与人类前列腺癌的起源

Stem/progenitor and intermediate cell types and the origin of human prostate cancer.

作者信息

Tokar Erik J, Ancrile Brooke B, Cunha Gerald R, Webber Mukta M

机构信息

Department of Zoology, Michigan State University, East Lansing, MI 48824-1312, USA.

出版信息

Differentiation. 2005 Dec;73(9-10):463-73. doi: 10.1111/j.1432-0436.2005.00047.x.

Abstract

Theories of cell lineage in human prostatic epithelium, based on protein expression, propose that basal and luminal cells: 1) are either independently capable of self-renewal or 2) arise from stem cells expressing a full spectrum of proteins (p63, cytokeratins CK5/14, CK8/18, and glutathione-S-transferase-pi [GST-pi]) similar to cells of the embryonic urogenital sinus (UGS). Such embryonic-like stem cells are thought to give rise to mature basal cells and secretory luminal cells. By single cell cloning of an immortalized, normal human prostate-derived, non-tumorigenic RWPE-1 cell line, we isolated and characterized two epithelial cell types, WPE-stem and WPE-int. WPE-stem cells show: i) strong, sixfold greater nuclear expression of p63; ii) nearly twofold greater expression of CK14; iii) threefold less CK18, and iv) low androgen receptor (AR) expression as compared with WPE-int cells. WPE-stem cells are androgen-independent for growth and survival. WPE-int cells express very low p63 and CK5/14, and high CK18. WPE-int cells are androgen-independent for growth and survival but are highly responsive as shown by androgen induction of AR and prostate specific antigen (PSA). Compared with WPE-int cells, WPE-stem cells are smaller and show more rapid growth. WPE-stem cells can grow in an anchorage-independent manner in agar with 4.5-fold greater cloning efficiency and as free floating "prostaspheres" in liquid medium; and express over 40-fold higher matrix metalloproteinase-2 activity. These results indicate that WPE-stem cells express several features characteristic of stem/progenitor cells present in the UGS and in adult prostatic epithelium. In contrast, WPE-int cells have an intermediate, committed phenotype on the pathway to luminal cell differentiation. We propose that in normal prostatic epithelium, cells exist at many stages in a continuum of differentiation progressing from stem cells to definitive basal and luminal cells. Establishment and characterization of clones of human prostatic epithelial cells provide novel models for determining cell lineages, the origin of prostate cancer, and for developing new strategies for tumor prevention and treatment.

摘要

基于蛋白质表达的人类前列腺上皮细胞谱系理论提出,基底细胞和管腔细胞:1)要么各自具有自我更新能力,要么2)起源于表达一系列蛋白质(p63、细胞角蛋白CK5/14、CK8/18和谷胱甘肽 - S - 转移酶 - pi [GST - pi])的干细胞,这些蛋白质与胚胎泌尿生殖窦(UGS)的细胞相似。这种类似胚胎的干细胞被认为可产生成熟的基底细胞和分泌性管腔细胞。通过对永生化、源自正常人类前列腺的非致瘤性RWPE - 1细胞系进行单细胞克隆,我们分离并鉴定了两种上皮细胞类型,即WPE - 干细胞和WPE - 中间细胞。与WPE - 中间细胞相比,WPE - 干细胞表现出:i)p63的核表达强6倍;ii)CK14的表达高近2倍;iii)CK18的表达低3倍,以及iv)雄激素受体(AR)表达低。WPE - 干细胞的生长和存活不依赖雄激素。WPE - 中间细胞p63和CK5/14表达极低,而CK18表达高。WPE - 中间细胞的生长和存活不依赖雄激素,但如AR和前列腺特异性抗原(PSA)的雄激素诱导所示,其反应性很高。与WPE - 中间细胞相比,WPE - 干细胞更小且生长更快。WPE - 干细胞能以不依赖贴壁的方式在琼脂中生长,克隆效率高4.5倍,并能在液体培养基中作为游离漂浮的“前列腺球”生长;且表达的基质金属蛋白酶 - 2活性高40倍以上。这些结果表明,WPE - 干细胞表达了UGS和成人前列腺上皮中存在的干细胞/祖细胞的几个特征。相反,WPE - 中间细胞在向管腔细胞分化的途径上具有中间的、已定向的表型。我们提出,在正常前列腺上皮中,细胞存在于从干细胞到确定的基底细胞和管腔细胞的连续分化的许多阶段。人类前列腺上皮细胞克隆的建立和鉴定为确定细胞谱系、前列腺癌的起源以及开发肿瘤预防和治疗的新策略提供了新的模型。

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