Sommers G M, Alfieri A A
Division of Gynecological Oncology, St. Mary's and Christ Hospital, Hoboken, New Jersey, USA.
Cancer Invest. 1998;16(7):462-70. doi: 10.3109/07357909809011700.
The addition of chemotherapy to radiation therapy has the potential to sterilize micrometastases and tumor foci adjacent and peripheral to the treatment field, so as to enhance local control of malignancy and improve primary and salvage therapy. Studies were done to investigate the effects of combining cisplatin (CP), the most active single agent in squamous-cell cancer of the cervix, with irradiation and the addition of a protein kinase C (PKC) inhibitor. This initial report of these studies describes our experience in exposing human cervical carcinoma (HeLa-S3) cells grown in culture as multicellular tumor spheroids to continuous CP combined with radiation in an attempt to mimic both clinically achievable serum concentrations of CP and a weekly fractionated-dose environment. Radiation-dose-dependent delays of spheroid growth were not significantly increased in the presence of the PKC inhibitor 7-OH-staurosporine (UCN-01) at 1.0 nM and 10.0 nM concentrations. When dose comparisons at 8 Gy alone (2 Gy x 4 fractions) were made for combined therapy with either CP alone (1.0 microgram/ml) or UCN-01 alone, absolute delays in spheroid growth at the highest concentrations used were comparable (range: 37-41 days). Although these data alone would not support minimal chemotherapeutic interaction, it appears that the overall effects observed for combination therapy were predominately radiation-dose dependent. The combination of UCN-01 plus CP (0.5 and 1.0 mu/ml, respectively) was effective in increasing the cytostatic and cytotoxic effects of irradiation at 4 Gy (2 Gy x 2 fractions). Observations made as early as day 4 and day 7 posttreatment were indicative of > or = 40% and 60%, respectively, of morphological damage. Spheroid growth was essentially static at these doses over the evaluation time of 60 days. Intracellular junctions were disorganized, and spheroid swelling was evident and contributed to the modest dimensional changes observed after treatment. No surviving fractions could be generated from spheroids that were mechanically disrupted, trypsinized, and plated at day 7 after the initiation of treatment. At 2 months, 88% (14/16) and 94% (15/16) of the multimodality treatment groups (4 Gy + UCN-01 + CP [0.5 and 1.0 mu/ml], respectively) had sterilized spheroids, indicating that the CP concentration dependence may not be a sole determinant of efficacy. Our therapeutic strategy for combining irradiation with CP was based on the contemporary use of CP as the most successful agent in producing high survival rates in gynecological malignancy. The combination of UCN-01 with CP and irradiation may, however, represent a more effective strategy for enhancing future cisplatin-based chemotherapy regimens.
在放射治疗中加入化疗有可能使微转移灶以及治疗区域附近和周边的肿瘤病灶失活,从而增强对恶性肿瘤的局部控制,并改善初始治疗和挽救治疗效果。开展了多项研究,以探讨顺铂(CP)(子宫颈鳞状细胞癌中最有效的单一药物)与放疗联合应用以及添加蛋白激酶C(PKC)抑制剂的效果。这些研究的这份初步报告描述了我们将培养成多细胞肿瘤球体的人子宫颈癌(HeLa-S3)细胞暴露于持续CP联合放疗的经验,旨在模拟临床上可达到的CP血清浓度和每周分次给药环境。在浓度为1.0 nM和10.0 nM的PKC抑制剂7-羟基星孢菌素(UCN-01)存在的情况下,球体生长的放射剂量依赖性延迟未显著增加。当单独比较8 Gy(2 Gy×4分次)与单独使用CP(1.0微克/毫升)或单独使用UCN-01联合治疗时,所用最高浓度下球体生长的绝对延迟相当(范围:37 - 41天)。尽管仅凭这些数据不能支持最低限度的化疗相互作用,但联合治疗观察到的总体效果似乎主要取决于放射剂量。UCN-01加CP(分别为0.5和1.0微升/毫升)的联合在增加4 Gy(2 Gy×2分次)照射的细胞生长抑制和细胞毒性作用方面是有效的。早在治疗后第4天和第7天的观察结果分别表明形态损伤>或 = 40%和60%。在60天的评估时间内,这些剂量下球体生长基本处于静止状态。细胞内连接紊乱,球体肿胀明显,这导致了治疗后观察到的适度尺寸变化。在治疗开始后第7天,对机械破坏、胰蛋白酶消化并接种的球体无法产生存活分数。在2个月时,多模式治疗组(分别为4 Gy + UCN-01 + CP [0.5和1.0微升/毫升])中88%(14/16)和94%(15/16)的球体已失活,这表明CP浓度依赖性可能不是疗效的唯一决定因素。我们将放疗与CP联合的治疗策略基于当前将CP用作在妇科恶性肿瘤中产生高生存率最成功药物的应用。然而,UCN-01与CP和放疗的联合可能代表了一种更有效的策略,用于增强未来基于顺铂的化疗方案。
