Survival analysis in second-line and third-line chemotherapy with irinotecan followed by topotecan or topotecan followed by irinotecan for extensive-stage small-cell lung cancer patients: a single-center retrospective study

Gokmen Aktas; Tulay Kus; Mehmet Emin Kalender; Alper Sevinc; Celaletdin Camci; Seval Kul

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Survival analysis in second-line and third-line chemotherapy with irinotecan followed by topotecan or topotecan followed by irinotecan for extensive-stage small-cell lung cancer patients: a single-center retrospective study

机译：单中心回顾性研究：伊立替康，托泊替康或托泊替康，伊立替康二线和三线化疗对广泛期小细胞肺癌患者的生存分析：单中心回顾性研究

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Purpose: The number of patients who make it to receive third-line chemotherapy is increasing owing to the improvements in adverse-event management of chemotherapy for small-cell lung cancer (SCLC). Sequencing of optimal treatment for SCLC is still a challenge for oncologists. In this paper, we aim to present a different approach to the treatment of SCLC. Methods: Between January 2008 and July 2014, all patients diagnosed with extensive-stage SCLC and treated with third-line chemotherapy at Gaziantep University Oncology Hospital were analyzed retrospectively. Disease control rates and progression-free survival (PFS) for first-, second-, and third-line chemotherapy, and overall survival (OS) were recorded. Survival analysis was calculated by using Kaplan–Meier method. Results: A total of 255 SCLC patients were screened, and 25 of those patients who received third-line chemotherapy were included in this study. Median age was 57±10.131 years (range:?39–74 years). Disease control rates at first-, second-, and third-line chemotherapy were 92%, 68%, and 44%, respectively. Fourteen patients received irinotecan followed by topotecan, and eleven patients received topotecan followed by irinotecan. Second-line median PFS was statistically better in patients treated with irinotecan at second-line compared with those treated with topotecan (21 vs 12 weeks, P =0.018). Comparison of third-line median PFS of the two groups was not statistically significant (14 vs 12 weeks, P =0.986). Median OS was not statistically significant in patients who received irinotecan followed by topotecan vs those who received topotecan followed by irinotecan (18 vs 14 months, P =0.112). Conclusion: Sequential monotherapy with topotecan and irinotecan provides a considerable contribution to OS, and second-line irinotecan showed a better PFS, despite a similar OS, compared with topotecan.

机译：目的：由于小细胞肺癌（SCLC）化疗不良事件管理的改善，使其接受三线化疗的患者数量正在增加。对SCLC的最佳治疗顺序仍然是肿瘤学家所面临的挑战。在本文中，我们旨在提出一种不同的SCLC治疗方法。方法：回顾性分析2008年1月至2014年7月在加济安泰普大学肿瘤医院接受诊断的广泛期SCLC并接受三线化疗的所有患者。记录一线，二线和三线化疗的疾病控制率和无进展生存期（PFS），以及总生存期（OS）。生存分析采用Kaplan–Meier方法进行计算。结果：总共筛选了255名SCLC患者，该研究中包括了接受三线化疗的患者中的25名。中位年龄为57±10.131岁（范围：？39-74岁）。一线，二线和三线化疗的疾病控制率分别为92％，68％和44％。十四名患者接受了伊立替康，之后是托泊替康，十一名患者接受了拓扑替康，然后是伊立替康。与伊曲替康组相比，二线伊立替康组患者的二线中位PFS统计学上更好（21 vs 12周，P = 0.018）。两组三线中位PFS的比较无统计学意义（14周与12周，P = 0.986）。接受伊立替康+拓扑替康治疗的患者与接受伊立替康+依立替康治疗的患者的中位OS差异无统计学意义（18个月对14个月，P = 0.112）。结论：拓扑替康和伊立替康的序贯单药治疗对OS有相当大的贡献，尽管OS与托泊替康相似，但二线伊立替康显示出更好的PFS，尽管OS相似。

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《OncoTargets and therapy》 |2016年第2期|共6页
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Gokmen Aktas; Tulay Kus; Mehmet Emin Kalender; Alper Sevinc; Celaletdin Camci; Seval Kul;
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1. Combined chemotherapy with cisplatin, etoposide, and irinotecan versus topotecan alone as second-line treatment for patients with sensitive relapsed small-cell lung cancer (JCOG0605): a multicentre, open-label, randomised phase 3 trial [J] . Goto Koichi, Ohe Yuichiro, Shibata Taro, The lancet oncology . 2016,第8期

机译：联合化疗联合顺铂，依托泊苷和伊立替康与伊泊替康相比单独使用拓扑替康作为敏感性复发小细胞肺癌患者的二线治疗（JCOG0605）：一项多中心，开放标签，随机3期试验
2. E5501: Phase II study of topotecan sequenced with etoposide/cisplatin, and irinotecan/cisplatin sequenced with etoposide for extensive-stage small-cell lung cancer [J] . OwonikokoT.K., AisnerJ., WangX.V., Cancer chemotherapy and pharmacology. . 2014,第1期

机译：E5501：依托泊苷/顺铂测序的拓扑替康和依托泊苷测序的伊立替康/顺铂用于广泛期小细胞肺癌的II期研究
3. Apatinib in patients with extensive-stage small-cell lung cancer after second-line or third-line chemotherapy: a phase II, single-arm, multicentre, prospective study [J] . Yanjun Xu, Zhiyu Huang, Hongyang Lu, British Journal of Cancer . 2019,第8期

机译：Apatinib患者在二线或第三线化疗后广泛的小细胞肺癌：II期，单臂，多环境，前瞻性研究
4. Efficacy of combination chemotherapy with docetaxel and irinotecan as first- or second-line treatment for advanced gastric cancer [C] . K. Sugiyama, A. Ishikawa, T. Watanabe International Gastric Cancer Congress . 2009

机译：组合化疗与多西紫杉醇和伊替康的疗效，作为晚期胃癌的第一或二线治疗
5. Patient Derived Xenograft Models of Small-cell Lung Cancer Provide Molecular Insights into Mechanisms of Chemotherapy Cross-resistance [D] . Myers, David T. 2018

机译：小细胞肺癌的患者衍生异种移植模型为化学疗法交叉耐药机制提供分子见解
6. Survival analysis in second-line and third-line chemotherapy with irinotecan followed by topotecan or topotecan followed by irinotecan for extensive-stage small-cell lung cancer patients: a single-center retrospective study [O] . Gokmen Aktas, Tulay Kus, Mehmet Emin Kalender, 2016

机译：单中心回顾性研究：伊立替康托泊替康或托泊替康伊立替康二线和三线化疗对广泛期小细胞肺癌患者的生存分析：单中心回顾性研究
7. Survival analysis in second-line and third-line chemotherapy with irinotecan followed by topotecan or topotecan followed by irinotecan for extensive-stage small-cell lung cancer patients: a single-center retrospective study [O] . gokmen aktas, Kuş Tulay, mehmet emin kalender, 2016

机译：二线和第三线化疗的生存分析与Irinotecan之后是Topotecan或Topotecan，然后是Irinotecan进行广泛的小型细胞肺癌患者：单中心回顾性研究

Survival analysis in second-line and third-line chemotherapy with irinotecan followed by topotecan or topotecan followed by irinotecan for extensive-stage small-cell lung cancer patients: a single-center retrospective study

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