前列腺癌中的雄激素剥夺与干细胞标志物
Androgen deprivation and stem cell markers in prostate cancers.
作者信息
Tang Yao, Hamburger Anne W, Wang Linbo, Khan Mohammad Afnan, Hussain Arif
机构信息
Department of Medicine, University of Maryland School of Medicine, Baltimore, Maryland 21201, USA.
出版信息
Int J Clin Exp Pathol. 2009 Nov 10;3(2):128-38.
Abstract
In our previous studies using human LNCaP xenografts and TRAMP (transgenic adenocarcinoma of mouse prostate) mice, androgen deprivation therapy (ADT) resulted in a temporary cessation of prostate cancer (PCa) growth, but then tumors grew faster with more malignant behaviour. To understand whether cancer stem cells might play a role in PCa progression in these animal models, we investigated the expressions of stem cell-related markers in tumors at different time points after ADT. In both animal models, enhanced expressions of stem cell markers were observed in tumors of castrated mice, as compared to non-castrated controls. This increased cell population that expressed stem cell markers is designated as stem-like cells (SLC) in this article. We also observed that the SLC peaked at relatively early time points after ADT, before tumors resumed their growth. These results suggest that the SLC population may play a role in tumor re-growth and disease progression, and that targeting the SLC at their peak-expression time point may prevent tumor recurrence following ADT.
摘要
在我们之前使用人LNCaP异种移植瘤和TRAMP(小鼠前列腺转基因腺癌)小鼠的研究中,雄激素剥夺疗法(ADT)导致前列腺癌(PCa)生长暂时停止,但随后肿瘤生长加快且行为更具侵袭性。为了解癌症干细胞是否可能在这些动物模型的PCa进展中发挥作用,我们研究了ADT后不同时间点肿瘤中干细胞相关标志物的表达。在这两种动物模型中,与未去势对照相比,去势小鼠肿瘤中观察到干细胞标志物表达增强。本文将这种表达干细胞标志物的细胞群体增加称为类干细胞(SLC)。我们还观察到,SLC在ADT后相对较早的时间点达到峰值,然后肿瘤才恢复生长。这些结果表明,SLC群体可能在肿瘤再生长和疾病进展中起作用,并且在其峰值表达时间点靶向SLC可能预防ADT后肿瘤复发。
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