重组腺相关病毒介导的单纯疱疹病毒胸苷激酶基因转移,通过瘤内直接注射和四环素调控用于植入的人乳腺癌。
Recombinant AAV-mediated HSVtk gene transfer with direct intratumoral injections and Tet-On regulation for implanted human breast cancer.
作者信息
Li Zi-Bo, Zeng Zhao-Jun, Chen Qian, Luo Sai-Qun, Hu Wei-Xin
机构信息
Molecular Biology Research Center, Xiangya Medical College, Central South University, Changsha, Hunan 410078, PR China.
出版信息
BMC Cancer. 2006 Mar 16;6:66. doi: 10.1186/1471-2407-6-66.
BACKGROUND
HSVtk/ganciclovir (GCV) gene therapy has been extensively studied in tumors and relies largely on the gene expression of HSVtk. Most studies, however, have failed to demonstrate any significant benefit of a controlled gene expression strategy in cancer treatment. The Tet-On system is commonly used to regulate gene expression following Dox induction. We have evaluated the antitumor effect of HSVtk/ganciclovir gene therapy under Tet-On regulation by means of adeno-associated virus-2 (AAV-2)-mediated HSVtk gene transfer with direct intratumoral injections in mice bearing breast cancer tumors.
METHODS
Recombinant adeno-associated virus-2 (rAAV) was constructed and transduced into MCF-7 cell line. GCV treatment to the rAAV infected MCF-7 cells was performed by MTT assay under the doxycycline (Dox) induction or without Dox induction at a vp (viral particle) number of > or =10(4)/cell. The virus was administered intratumorally to nude mice that had also received GCV intraperitoneally. The antitumor effects were evaluated by measuring tumor regression and histological analysis.
RESULTS
We have demonstrated that GCV treatment to the infected MCF-7 cells under the Dox induction was of more inhibited effects than those without Dox induction at > or =10(4) vp/cell. In ex vivo experiments, tumor growth of BALB/C nude mice breast cancer was retarded after rAAV-2/HSVtk/Tet-On was injected into the tumors under the Dox induction. Infiltrating cells were also observed in tumors after Dox induction followed by GCV treatment and cells were profoundly damaged. The expression of HSVtk gene in MCF-7 cells and BALB/C nude mice tumors was up-regulated by Tet-On under Dox induction with reverse transcription-PCR (RT-PCR) analysis.
CONCLUSION
The antitumor effect of rAAV-mediated HSVtk/GCV gene therapy under the Dox induction with direct intratumoral injections may be a useful treatment for breast cancer and other solid tumors.
背景
单纯疱疹病毒胸苷激酶/更昔洛韦(HSVtk/GCV)基因疗法已在肿瘤研究中得到广泛应用,且很大程度上依赖于HSVtk的基因表达。然而,大多数研究未能证明可控基因表达策略在癌症治疗中有任何显著益处。Tet-On系统常用于在强力霉素(Dox)诱导后调节基因表达。我们通过腺相关病毒2型(AAV-2)介导的HSVtk基因直接瘤内注射,评估了在Tet-On调控下HSVtk/GCV基因疗法对荷乳腺癌小鼠的抗肿瘤作用。
方法
构建重组腺相关病毒2型(rAAV)并转导至MCF-7细胞系。在强力霉素(Dox)诱导或无Dox诱导的情况下,以病毒粒子数≥10⁴/细胞,通过MTT法对rAAV感染的MCF-7细胞进行GCV处理。将病毒瘤内注射给同样接受了腹腔内注射GCV的裸鼠。通过测量肿瘤消退情况和组织学分析评估抗肿瘤效果。
结果
我们已证明,在≥10⁴病毒粒子/细胞时,Dox诱导下对感染的MCF-7细胞进行GCV处理比无Dox诱导时具有更强的抑制作用。在体外实验中,Dox诱导下将rAAV-2/HSVtk/Tet-On注射到BALB/C裸鼠乳腺癌肿瘤后,肿瘤生长受到抑制。Dox诱导后接着进行GCV处理,肿瘤中也观察到浸润细胞,且细胞受到严重损伤。通过逆转录-聚合酶链反应(RT-PCR)分析,Tet-On在Dox诱导下上调了MCF-7细胞和BALB/C裸鼠肿瘤中HSVtk基因的表达。
结论
Dox诱导下直接瘤内注射的rAAV介导的HSVtk/GCV基因疗法的抗肿瘤作用可能是乳腺癌和其他实体瘤的一种有效治疗方法。
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