Federico M, Alberts D S, Garcia D J, Emerson J, Fanta P, Liu R, Salmon S E
Arizona Cancer Center, College of Medicine, University of Arizona, Tucson 85724.
Gynecol Oncol. 1994 Dec;55(3 Pt 2):S156-63. doi: 10.1006/gyno.1994.1356.
The purpose of this study was to assess the prognostic value of in vitro drug chemosensitivity testing using the Hamburger-Salmon human tumor colony-forming assay (HTCA) in fresh tumor samples obtained from newly diagnosed patients with stage II-IV ovarian cancer undergoing maximum cytoreductive surgery and prior to platinum-based chemotherapy. The HTCA was performed on fresh ovarian cancers obtained from 93 patients at their initial exploratory laparotomy to evaluate in vitro sensitivity to cisplatin, carboplatin, and cyclophosphamide following a 1-hr drug exposure. Prospective clinical follow-up was performed on all patients with the primary study endpoints being pathologically proven complete response at second-look surgery and disease-free and overall survival durations. In vitro drug sensitivity was strongly dose-dependent. At a concentration of 5 micrograms/ml only 23% of tumor samples were sensitive (as defined by a > or = 50% decrease in tumor colony-forming units compared to controls) to cisplatin; 13% of tumors were sensitive to carboplatin at a concentration of 50 micrograms/ml and 11% to 4-OH-cyclophosphamide at a concentration of 1 microgram/ml. At doses which were 10 times the previously stated concentrations, the sensitivity rates to cisplatin, carboplatin, and 4-OH-cyclophosphamide increased to 72, 63, and 53%, respectively. Subjects were categorized as having drug-sensitive disease if HTCA results showed in vitro drug sensitivity to at least one of the agents used in their primary chemotherapy. Multivariate analysis failed to show any advantage in clinical response rate, progression-free interval, or survival duration for patients with drug-sensitive disease compared to drug-resistant disease; however, there was evidence of a trend toward an enhanced pathologically proven complete response rate in patients who had chemosensitive tumors in vitro. Second-look surgery was performed in 28 of 55 patients with optimal surgical resections and no clinical evidence of disease at the completion of their primary chemotherapy. Fifty percent (5/10) of patients with drug-sensitive disease achieved a pathologic complete response, while only 3/18 (17%) patients with drug-resistant tumors had a documented pathologic complete response (P = 0.13). As reported in other ovarian cancer studies, patient characteristics which were found to be significantly associated with survival were stage of disease (II-III vs IV), optimal primary surgical resection (i.e., < 1 cm2 residual tumor) vs suboptimal resection, clinical measurability of disease at initiation of chemotherapy, and response to primary chemotherapy. In conclusion, in vitro drug sensitivity, as measured by the HTCA, does not appear to be an independent prognostic factor for survival in patients with stage II-IV epithelial ovarian cancer who undergo standard treatment with tumor debulking surgery and primary platinum-based chemotherapy.(ABSTRACT TRUNCATED AT 400 WORDS)
本研究的目的是评估使用汉堡-萨蒙人肿瘤集落形成试验(HTCA)对从新诊断的II-IV期卵巢癌患者获取的新鲜肿瘤样本进行体外药物化学敏感性检测的预后价值,这些患者即将接受最大限度的肿瘤细胞减灭术且在铂类化疗之前。对93例患者在初次剖腹探查时获取的新鲜卵巢癌组织进行HTCA,以评估在药物暴露1小时后对顺铂、卡铂和环磷酰胺的体外敏感性。对所有患者进行前瞻性临床随访,主要研究终点为二次探查手术时病理证实的完全缓解以及无病生存期和总生存期。体外药物敏感性呈强烈的剂量依赖性。在浓度为5微克/毫升时,只有23%的肿瘤样本对顺铂敏感(定义为与对照组相比肿瘤集落形成单位减少≥50%);在浓度为50微克/毫升时,13%的肿瘤对卡铂敏感,在浓度为1微克/毫升时,11%的肿瘤对4-羟基环磷酰胺敏感。在上述浓度的10倍剂量下,对顺铂、卡铂和4-羟基环磷酰胺的敏感率分别增至72%、63%和53%。如果HTCA结果显示对其一线化疗中使用的至少一种药物有体外药物敏感性,则将受试者归类为患有药物敏感型疾病。多变量分析未显示药物敏感型疾病患者与耐药型疾病患者在临床缓解率、无进展间期或生存期方面有任何优势;然而,有证据表明体外肿瘤对化疗敏感的患者病理证实的完全缓解率有升高趋势。55例初次手术切除效果最佳且在一线化疗结束时无疾病临床证据的患者中有28例接受了二次探查手术。药物敏感型疾病患者中有50%(5/10)达到病理完全缓解,而耐药型肿瘤患者中只有3/18(17%)有记录的病理完全缓解(P = 0.13)。正如其他卵巢癌研究报告的那样,发现与生存显著相关的患者特征包括疾病分期(II-III期与IV期)、初次手术切除是否最佳(即残留肿瘤<1平方厘米)与非最佳切除、化疗开始时疾病的临床可测量性以及对一线化疗的反应。总之,对于接受肿瘤减灭术和一线铂类化疗标准治疗的II-IV期上皮性卵巢癌患者,通过HTCA测定的体外药物敏感性似乎不是生存的独立预后因素。(摘要截短至400字)
