西多福韦的选择性基于正常细胞和癌细胞对 DNA 损伤的不同反应。
Cidofovir selectivity is based on the different response of normal and cancer cells to DNA damage.
机构信息
Rega Institute for Medical Research, Laboratory of Virology and Chemotherapy, KU Leuven, Leuven, Belgium.
出版信息
BMC Med Genomics. 2013 May 23;6:18. doi: 10.1186/1755-8794-6-18.
BACKGROUND
Cidofovir (CDV) proved efficacious in treatment of human papillomaviruses (HPVs) hyperplasias. Antiproliferative effects of CDV have been associated with apoptosis induction, S-phase accumulation, and increased levels of tumor suppressor proteins. However, the molecular mechanisms for the selectivity and antitumor activity of CDV against HPV-transformed cells remain unexplained.
METHODS
We evaluated CDV drug metabolism and incorporation into cellular DNA, in addition to whole genome gene expression profiling by means of microarrays in two HPV(+) cervical carcinoma cells, HPV- immortalized keratinocytes, and normal keratinocytes.
RESULTS
Determination of the metabolism and drug incorporation of CDV into genomic DNA demonstrated a higher rate of drug incorporation in HPV(+) tumor cells and immortalized keratinocytes compared to normal keratinocytes. Gene expression profiling clearly showed distinct and specific drug effects in the cell types investigated. Although an effect on inflammatory response was seen in all cell types, different pathways were identified in normal keratinocytes compared to immortalized keratinocytes and HPV(+) tumor cells. Notably, Rho GTPase pathways, LXR/RXR pathways, and acute phase response signaling were exclusively activated in immortalized cells. CDV exposed normal keratinocytes displayed activated cell cycle regulation upon DNA damage signaling to allow DNA repair via homologous recombination, resulting in genomic stability and survival. Although CDV induced cell cycle arrest in HPV- immortalized cells, DNA repair was not activated in these cells. In contrast, HPV(+) cells lacked cell cycle regulation, leading to genomic instability and eventually apoptosis.
CONCLUSIONS
Taken together, our data provide novel insights into the mechanism of action of CDV and its selectivity for HPV-transformed cells. The proposed mechanism suggests that this selectivity is based on the inability of HPV(+) cells to respond to DNA damage, rather than on a direct anti-HPV effect. Since cell cycle control is deregulated by the viral oncoproteins E6 and E7 in HPV(+) cells, these cells are more susceptible to DNA damage than normal keratinocytes. Our findings underline the therapeutic potential of CDV for HPV-associated malignancies as well as other neoplasias.
背景
西多福韦(CDV)已被证明可有效治疗人类乳头瘤病毒(HPV)增生。CDV 的抗增殖作用与诱导细胞凋亡、S 期积累和肿瘤抑制蛋白水平升高有关。然而,CDV 对 HPV 转化细胞的选择性和抗肿瘤活性的分子机制仍不清楚。
方法
我们评估了 CDV 的药物代谢和在两种 HPV(+)宫颈癌细胞、HPV-永生化角质形成细胞和正常角质形成细胞中的细胞 DNA 掺入,此外还通过微阵列进行了全基因组基因表达谱分析。
结果
CDV 代谢和药物掺入到基因组 DNA 的测定表明,HPV(+)肿瘤细胞和永生化角质形成细胞的药物掺入率高于正常角质形成细胞。细胞类型研究中的基因表达谱分析清楚地显示了不同的、特定的药物作用。虽然所有细胞类型都观察到对炎症反应的影响,但在正常角质形成细胞与永生化细胞和 HPV(+)肿瘤细胞之间鉴定出不同的途径。值得注意的是,Rho GTPase 途径、LXR/RXR 途径和急性期反应信号转导仅在永生化细胞中被激活。CDV 暴露的正常角质形成细胞在 DNA 损伤信号下显示出激活的细胞周期调节,以允许通过同源重组进行 DNA 修复,从而导致基因组稳定性和存活。尽管 CDV 诱导 HPV-永生化细胞中的细胞周期停滞,但这些细胞中未激活 DNA 修复。相反,HPV(+)细胞缺乏细胞周期调节,导致基因组不稳定并最终导致细胞凋亡。
结论
综上所述,我们的数据为 CDV 的作用机制及其对 HPV 转化细胞的选择性提供了新的见解。所提出的机制表明,这种选择性是基于 HPV(+)细胞无法对 DNA 损伤做出反应,而不是直接的抗 HPV 作用。由于 HPV(+)细胞中的病毒癌蛋白 E6 和 E7 使细胞周期调控失调,这些细胞比正常角质形成细胞更容易受到 DNA 损伤。我们的研究结果强调了 CDV 在 HPV 相关恶性肿瘤以及其他肿瘤中的治疗潜力。
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