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由于E6和E7癌蛋白表达降低以及凋亡增强,HPV阳性头颈部癌细胞系对X射线照射±顺铂的敏感性增加。

Increased sensitivity of HPV-positive head and neck cancer cell lines to x-irradiation ± Cisplatin due to decreased expression of E6 and E7 oncoproteins and enhanced apoptosis.

作者信息

Ziemann Frank, Arenz Andrea, Preising Stefanie, Wittekindt Claus, Klussmann Jens P, Engenhart-Cabillic Rita, Wittig Andrea

机构信息

Department of Radiotherapy and Radiooncology, Philipps-University, University Hospital Gießen and Marburg Marburg, Germany.

Department of Otorhinolaryngology and Head and Neck Surgery, Justus Liebig University, University Hospital Gießen and Marburg Giessen, Germany.

出版信息

Am J Cancer Res. 2015 Feb 15;5(3):1017-31. eCollection 2015.

Abstract

Squamous cell carcinoma of the head and neck region (HNSCC), which is related to an infection with human papilloma virus (HPV), responds better to simultaneous radio-chemotherapy with Cisplatin based regimens than HPV-negative tumors. The underlying molecular mechanisms for this clinical observation are not fully understood. Therefore, the response of four HPV-positive (HPV+) (UM-SCC-47, UM-SCC-104, 93-VU-147T, UPCI:SCC152) and four HPV-negative (HPV-) (UD-SCC-1, UM-SCC-6, UM-SCC-11b, UT-SCC-33) HNSCC cell lines to x-irradiation ± Cisplatin incubation in terms of clonogenic survival, cell cycle progression, protein expression (cyclin A2, cyclin E2, E6, E7, p53) and induction of apoptosis, was investigated. HPV+ cells were more radio- and chemosensitive and were more effectively sensitized to x-irradiation by simultaneous Cisplatin incubation than HPV- cell lines. HPV+ cell lines revealed an increased and prolonged G2/M arrest after irradiation, whereas Cisplatin induced a blockage of cells in S phase. In comparison to irradiation only, addition of Cisplatin significantly enhanced apoptosis especially in HPV+ cell lines. While irradiation alone increased the amount of HPV E6 and E7 proteins, both were down-regulated by Cisplatin incubation either alone or in combination with x-rays, which however did not increase the expression of endogenous p53. Our results demonstrate that cell cycle deregulation together with downregulation of HPV E6 and E7 proteins facilitating apoptosis after Cisplatin incubation promote the enhanced sensitivity of HPV+ HNSCC cells to simultaneous radio-chemotherapy. Combined effects of irradiation and Cisplatin appear to be relevant in mediating the enhanced therapeutic response of HPV-related HNSCC and are indicative of the benefit of combined modality approaches in future treatment optimization strategies.

摘要

头颈部区域的鳞状细胞癌(HNSCC)与人乳头瘤病毒(HPV)感染有关,相较于HPV阴性肿瘤,其对基于顺铂方案的同步放化疗反应更佳。这一临床观察结果背后的分子机制尚未完全明确。因此,研究了四种HPV阳性(HPV+)(UM-SCC-47、UM-SCC-104、93-VU-147T、UPCI:SCC152)和四种HPV阴性(HPV-)(UD-SCC-1、UM-SCC-6、UM-SCC-11b、UT-SCC-33)HNSCC细胞系在克隆存活、细胞周期进程、蛋白质表达(细胞周期蛋白A2、细胞周期蛋白E2、E6、E7、p53)以及凋亡诱导方面对X射线照射±顺铂孵育的反应。HPV+细胞系对放疗和化疗更敏感,与HPV-细胞系相比,同步顺铂孵育能更有效地使其对X射线照射敏感。HPV+细胞系在照射后显示出G2/M期阻滞增加且持续时间延长,而顺铂则诱导细胞在S期阻滞。与仅照射相比,添加顺铂显著增强了凋亡,尤其是在HPV+细胞系中。单独照射会增加HPV E6和E7蛋白的量,但顺铂单独孵育或与X射线联合孵育均会使其下调,不过这并未增加内源性p53的表达量。我们的结果表明,细胞周期失调以及顺铂孵育后HPV E6和E7蛋白的下调促进凋亡,从而提高了HPV+ HNSCC细胞对同步放化疗的敏感性。照射和顺铂的联合作用似乎与介导HPV相关HNSCC增强的治疗反应有关,这表明联合治疗方法在未来治疗优化策略中具有益处。

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