A novel TARP-promoter-based adenovirus against hormone-dependent and hormone-refractory prostate cancer

被引:34
作者
Cheng, WS
Kraaij, R
Nilsson, B
van der Weel, L
de Ridder, CMA
Tötterman, TH
Essand, M [1 ]
机构
[1] Uppsala Univ, Rudbeck Lab, SE-75185 Uppsala, Sweden
[2] Erasmus Med Ctr, Dept Urol, Josephine Nefkens Inst, Sect Oncol Urol, Rotterdam, Netherlands
关键词
TARP; promoter; PPT; prostate cancer; adenovirus; gene therapy;
D O I
10.1016/j.ymthe.2004.05.022
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
TARP (T cell receptor T-chain alternate reading frame protein) is a protein that in males is uniquely expressed in prostate epithelial cells and prostate cancer cells. We have previously shown that the transcriptional activity of a chimeric sequence comprising the TARP promoter (TARPp) and the PSA enhancer (PSAe) is strictly controlled by testosterone and highly restricted to cells of prostate origin. Here we report that a chimeric sequence comprising TARPp and the PSMA enhancer (PSMAe) is highly active in testosterone-deprived prostate cancer cells, while a regulatory sequence comprising PSAe, PSMAe, and TARPp (PPT) has high prostate-specific activity both in the presence and in the absence of testosterone. Therefore, the PPT sequence may, in a gene therapy setting, be beneficial to prostate cancer patients that have been treated with androgen withdrawal. A recombinant adenovirus vector with the PPT sequence, shielded from interfering adenoviral sequences by the mouse H19 insulator, yields high and prostate-specific transgene expression both in cell cultures and when prostate cancer, PC-346C, tumors were grown orthotopically in nude mice. Intravenous virus administration reveals both higher activity and higher selectivity for the insulator-shielded PPT sequence than for the immediate-early CMV promoter. Therefore, we believe that an adenovirus with therapeutic gene expression controlled by an insulator-shielded PPT sequence is a promising candidate for gene therapy of prostate cancer.
引用
收藏
页码:355 / 364
页数:10
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