Suicide gene therapy of ovarian cancer; an experimental study in rats using retroviral-mediated transfer of herpes simplex virus thymidine kinase gene

被引:0
|
作者
Nagy, HJ
Panis, Y
Fabre, M
Klatzmann, D
Houssin, D
Soubrane, O
机构
[1] Univ Paris, Hop Cochin, Lab Rech Chirurg, F-75252 Paris, France
[2] Hop Kremlin Bicetre, Serv Anatomocytopathol, Paris, France
[3] Hop La Pitie Salpetriere, Lab Biol & Genet Pathol Immunitaires, CNRS, URA 1463, Paris, France
关键词
ovarian cancer; gene therapy; retrovirus; thymidine kinase; ganciclovir;
D O I
暂无
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: This study evaluated the potential of gene therapy against ovarian cancer usin the retroviral transfer. of the herpes simplex type 1 thymidine kinase gene (HSV1-TK) followed by ganciclovir treatment. Materials and Methods: The sensitivity of 4 different ovarian cancer cell lines (rat ar human) to in vitro infection by recombinant retroviruses were evaluated. Then, their HSV1-TK expressing derivatives were tested for their sensitivity to ganciclovir. One of them, DMBA-OC-1-TK+ was used to generate experimental ovarian cancer in 13 WKY female rats. After 14 days, tl rats received ganciclovir for 12 days (n=6). The results were expressed in mean+/-ES and were evaluated with the Mann-Whitney test. Results: All cell lines analyzed in this study were sensitive to retroviral mediated gene transfe although with significant variations. The HSV1-TK expressing derivatives of these cells were 300 7,000-fold more sensitive to ganciclovir; than the parental cells. The ganciclovir dramatically reduced the size of HSV1-TK+ tumors compared to untreated control ruts (0 mm(3) vs 2,594 mm(3), p<0.001) with complete tumor regression and residual fibrotic scars on pathological examination. Control tumors showed a poorly-differentiated epithelial adenocarcinoma of the ovary. Conclusion: In a clinical perspective, the good tolerance and the significant antitumoral effects of retroviral-mediated transfer of HSV1-TK gene in animals were encouraging. It remains to set up gene transfer methods that will allow efficient targeting of the ovarian cancer in vivo.
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页码:4633 / 4638
页数:6
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