前列腺癌相关雄激素受体突变体的促细胞增殖效应  被引量:4

Cell growth promoting of the androgen receptor mutation

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作  者:武国军[1] 王禾[1] 李晓武[1] 袁建林[1] 于磊[1] 张波[1] 

机构地区:[1]第四军医大学西京医院泌尿外科,陕西西安710033

出  处:《中国医学工程》2006年第1期4-7,10,共5页China Medical Engineering

摘  要:目的评价前列腺癌相关雄激素受体突变体(mtAR)对细胞生长的促进作用。方法利用三种腺病毒表达载体:野生型雄激素受体(Ad-wtAR);一个被广泛研究的前列腺癌(CaP)相关的mtAR(Ad-mtAR,T877A);以及作为对照的腺病毒载体,我们评价并比较了野生型AR及mtAR的促细胞生长效应。结果相对于被野生型或者对照的腺病毒转染的LNCaP、PC3细胞,转染mtAR的LNCaP、PC3细胞无论有无合成的雄激素(R1881)存在的情况下均显示出更强的细胞增殖作用。并且,用腺病毒载体转染T877A的LNCaP和PC3细胞显示了对R1881更强的反应性。结论这些发现提出了崭新的关于mtAR在CaP细胞中作用的细胞生物学方面的见解,并且表明mtAR(T877A)可能为前列腺癌病程的进展提供了选择性的细胞生长的便利。[Objective] To evaluate the cell growth promoting effects of mutant androgen receptor (tatAR). [Methods] By sing adenovirus expression vectors of: the wild type AR (Ad-wtAR); a widely studied prostate cancer (CAP) associated tatAR (Ad-mtAR, T877A); and the control adenovirus vector (Ad-eontrol), we have evaluated and compared cell biologic effects of wtAR and tatAR. [Results] In comparison to the Ad-wtAR or Ad-eontrol infected LNCaP and PC3 cells, Ad-mtAR (T877A) infected LNCuP and PC3 cells exhibited enhanced cell growth in the presence or absence of synthetic androgen, R1881. Furthermore, Ad-mtAR (T877A) infected LNCaP and PC3 cells showed increased androgen responsiveness to R1881. [Conclusion] These findings provide novel cell biologic insights into effects of the AR mutations in CaP cells and suggest that mtARs with properties of AR (T877A) may provide selective cell growth advantages in the progression of CaP.

关 键 词:雄激素受体 雄激素爱体突变体 细胞增殖 

分 类 号:R392.11[医药卫生—免疫学] R737.25[医药卫生—基础医学]

 

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