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卵巢特异性启动子 OSP-2 驱动的 survivin 转移对 CHO 细胞的保护作用。

Protection of CHO cells by transfer of survivin driven by ovarian-specific promoter OSP-2.

机构信息

Department of Obstetrics and Gynecology, The First Affiliated Hospital of Nanchang University, No. 17 Yongwaizheng Street, Nanchang, 330006, China.

出版信息

Mol Biol Rep. 2011 Apr;38(4):2323-8. doi: 10.1007/s11033-010-0365-y. Epub 2010 Nov 14.

Abstract

Chemotherapy is the major therapy for cancer in clinic. However, chemotherapeutic agents can harm the other tissues/organs besides cancer. Thus, there are great interests in protecting the innocents by the transfer of protective genes. There are two problems to be solved, one is the selection of protective genes and the other is the orientation of the exotic genes. Recent researches demonstrated that the principal mechanism of chemotherapeutics was through apoptosis. Hereby, introduction of anti-apoptosis genes might interrupt the processes of apoptosis to avoid side effect from chemotherapeutics. On the other hand, tissue-specific promoters, which control gene expression in a tissue-specific manner, might be an alternative tool to guarantee the location of target genes. In this research, we applied gene therapy to chemoprotection using anti-apoptosis gene survivin and ovarian-specific promoter OSP-2. The results showed that OSP-2 could specifically drive the expression of survivin in ovarian cells and survivin could protect cells via inhibiting apoptosis. This might put a light on the future of chemoprotective gene therapy.

摘要

化疗是癌症临床治疗的主要手段。然而,化疗药物除了能杀伤肿瘤细胞外,还会对其他组织或器官造成损伤。因此,人们对通过转移保护性基因来保护正常组织有着浓厚的兴趣。目前有两个问题亟待解决,一是保护性基因的选择,二是外源基因的定向导入。最近的研究表明,化疗药物的主要作用机制是通过细胞凋亡来实现的。因此,导入抗凋亡基因可能会中断细胞凋亡的过程,从而避免化疗药物的副作用。另一方面,组织特异性启动子可以特异性地控制基因在特定组织中的表达,这可能是一种保证目的基因靶向定位的替代工具。在本研究中,我们应用抗凋亡基因 survivin 和卵巢特异性启动子 OSP-2 进行化疗保护的基因治疗研究。结果表明,OSP-2 可以特异性地驱动 survivin 在卵巢细胞中的表达,并且 survivin 可以通过抑制细胞凋亡来保护细胞。这可能为未来的化疗保护基因治疗指明了方向。

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