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首页> 外文期刊>Cancer gene therapy >Long term follow-up of patients with recurrent ovarian cancer after Ad p53 gene replacement with SCH 58500
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Long term follow-up of patients with recurrent ovarian cancer after Ad p53 gene replacement with SCH 58500

机译:SCH 58500替代Ad p53基因后对复发性卵巢癌患者的长期随访

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Objective: We have previously reported the safety, efficient gene transfer, and favorable CA125 responses of individuals with recurrent ovarian cancer treated by p53 gene replacement with the adenoviral vector SCH 58500. The purpose of the present investigation was to evaluate the long-term follow-up of these heavily pretreated patients subsequent to SCH 58500 dosing. Methods: Patients (n=36) were treated with either single-dose SCH 58500 in the phase I study or with multiple doses (MD) of SCH 58500 over multiple cycles in combination of platinum-based chemotherapy in the phase I/II portion of the study. Five patients were initially treated in the single-dose group and re-enrolled in the MD group. The MD group was evaluated both without the re-enrolled patients as MD1 (n=19), and as MD2 (n=24), which included them. Patients who were only treated on the single-dose arm were designated as SD (n=12). Most patients received additional chemotherapy at the discretion of their physicians on completion of the trial. The current analysis is a retrospective sequential cohort survival analysis. Results: The first patient was treated in March 1997 and the last patient completed SCH 58500 in September 1998. There was no difference in age at diagnosis, Karnofsky performance status, interval between diagnosis to SCH 58500, prior cycles or regimen of chemotherapy, platinum-free interval, percent platinum refractory patients, pretreatment CA125, or largest tumor volume between groups. Both MD groups had a slightly longer chemotherapy-free interval before SCH 58500 than the SD group. Median survival of individuals who received MD SCH 58500 with chemotherapy was 12–13.0 months, compared to only 5 months for those treated with SD SCH 58500. There are 10 long-term survivors more than 20 months after MD treatment for recurrent disease compared to only 2 long-term survivors after SD SCH 58500. Conclusion: The 12- to 13.0-month median survival in a heavily pretreated population with recurrent ovarian cancer compares favorably to the 16-month median survival for individuals treated with paclitaxel at the time of initial recurrence of this disease and is more than double the 5-month survival seen with palliative radiotherapy or paclitaxel failure. These data suggest that further study of SCH58500 is clearly indicated.
机译:目的:我们先前已报道了用腺病毒载体SCH 58500替代p53基因替代治疗的复发性卵巢癌患者的安全性,有效的基因转移和有利的CA125反应。本研究的目的是评估长期随访-这些严重预处理的患者在SCH 58500给药后服用。方法:在I期研究中,对36例患者采用单剂量SCH 58500或在多个周期中对SCH 58500进行多剂量(MD)治疗,在I / II期患者中联合铂类化疗。研究。五例患者最初在单剂量组接受治疗,然后重新纳入MD组。在没有重新入组患者的情况下,将MD组评估为MD1(n = 19)和MD2(n = 24),其中包括他们。仅在单剂量手臂上接受治疗的患者被指定为SD(n = 12)。在试验完成后,大多数患者应由医师决定是否接受其他化疗。当前的分析是回顾性连续队列生存分析。结果:首例患者于1997年3月接受治疗,最后一名患者于1998年9月完成SCH58500。在诊断年龄,卡诺夫斯基机能状态,诊断到SCH 58500的间隔,先前的化疗周期或化疗方案,铂-间隔,铂难治性患者百分比,CA125预处理或两组之间最大的肿瘤体积。两组MD组在SCH 58500之前的无化疗间隔都比SD组更长。接受MD SCH 58500化疗的患者的中位生存期为12–13.0个月,而接受SD SCH 58500治疗的患者的中位生存期仅为5个月。接受MD SCH 58500治疗的复发性疾病超过20个月的长期存活者为10个SD SCH 58500之后有2位长期幸存者。结论:经过大量预处理的患有复发性卵巢癌的人群中位生存期为12到13.0个月,与紫杉醇在初次复发时的16个月中位生存期相比具有优势。这种疾病的发生率是姑息放疗或紫杉醇治疗失败后5个月生存率的两倍以上。这些数据表明明确指示了对SCH58500的进一步研究。

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