卵巢癌综合治疗的进展与现状

卵巢上皮癌是妇科恶性肿瘤中最致命的恶性肿瘤。诊断时75％的病人已有盆腹腔广泛转移。这些病人的治疗需要适当的应用综合治疗方法。近年来卵巢上皮癌的治疗方法不断进展。本文复习近年来主要的与治疗和进展有关的文献,包括全身和腹腔化疗、新辅助化疗、间隔减瘤术,复发卵巢癌的化疗和二次减瘤术的作用等,特别强调卵巢上皮癌处理过程中化疗和手术的相互依赖作用。

Mechanisms of acquired resistance of BRCA1/2-driven tumors to platinum compounds and PARP inhibitors

Molecular pathogenesis of tumors arising in BRCA1/2 germ-line mutation carriers usually includes somatic inactivation of the remaining allele of the involved gene.Consequently,BRCA1/2-driven cancers are sensitive to platinum-based therapy and poly(ADP-ribose)polymerase inhibitors(PARPi).Long-term exposure to these drugs may result in the emergence of secondary BRCA1/2 mutations,which restore the open-reading frame of the affected allele.This platinum/PARPi crossresistance mechanism applies both for BRCA1 and BRCA2 genes and has been repeatedly validated in various laboratory models and multiple clinical studies.There are some other routes associated with the partial rescue of BRCA1/2 function or the development of BRCA1/2-independent pathways for genomic maintenance;however,their actual clinical relevance remains to be established.In addition,studies on the short-term neoadjuvant therapy for ovarian cancer revealed that even chemonaive BRCA1-driven tumors contain a small proportion of BRCA1-proficient cells.These pre-existing cells with retained BRCA1 heterozygosity rapidly repopulate the tumor mass during platinum exposure,but become outcompeted by BRCA1-deficient cells during therapy holidays.Understanding of the platinum/PARPi resistance pathways has led to the development of novel therapeutic approaches,which aim to improve the management of BRCA1/2-related cancers and are currently undergoing preclinical and clinical evaluation.

铂类敏感型复发性卵巢癌不同治疗方案疗效比较研究

目的:通过对广西医科大学附属肿瘤医院132例铂类敏感型复发性卵巢癌(platinum-sensitive recurrent ovarian cancer, PSROC)进行回顾性病例分析,研究不同临床特征对PSROC患者的总生存期(overall survival, OS)的影响,探讨影响PSROC患者生存情况的因素以及不同治疗方案对PSROC患者的预后影响,从而优化复发型卵巢癌的治疗。方法:收集2010年7月至2018年8月广西医科大学附属肿瘤医院现有电子病历数据132例PSROC患者的临床资料,包括患者复发年龄、FIGO分期、组织病理类型、无铂治疗间期(platinum-free intervals, PFI)、复发时CA125值、复发病灶、腹水这7个因素,探讨PSROC患者生存情况的影响因素并构建预后预测模型。结果:单因素分析表明:PFI、复发时CA125值、复发病灶、腹水与PSROC患者OS相关(P<0.05);复发年龄、FIGO分期、组织病理类型与OS无关(P>0.05)。COX多因素分析表明,PFI、复发时CA125值和复发病灶是PSROC患者预后的独立危险因素(P<0.05)。预后预测模型列线图可用于预测PSROC患者不同时间生存概率。本组PSROC患者随访时间2至108个月,中位随访时间33.5个月。终点分析显示:(1)中位OS在二次肿瘤细胞减灭术(secondary cytoreductive surgery, SCS)组和单纯化疗组分别为51.0个月vs 29.0个月(HR=0.45,95%CI:0.27~0.77,P=0.003),SCS组中位OS延长了22个月,差异有统计学意义(P<0.05);(2)中位OS在肿瘤残余病灶<1 cm组和肿瘤残留病灶≥1 cm组分别为55.0 vs 36.0个月(HR=0.40,95%CI:0.18~0.89,P=0.024),肿瘤残余病灶<1 cm组中位OS延长了19个月,差异有统计学意义(P<0.05);(3)中位OS在以铂类为基础的二次新辅助化疗(secondary neoadjuvant chemotherapy, SNACT)+SCS组和直接行SCS组分别为38.0个月vs 56.0个月(HR=2.02,95%CI:0.95~4.29,P=0.066),两组间差异无统计学意义;(4)中位OS在含顺铂/卡铂为主的方案(常规化疗组)化疗与其他铂类为主方案化疗疗效分别为49.0个月vs 30.5个月(HR=0.62,95%CI:0.41~0.95,P=0.029),常规化疗组中位OS延长了18.5个月,差异有统计学意义(P<0.05);(5)中位OS在含顺铂/卡铂+血管抑制剂组和含顺铂/卡铂组分别为35.0个月vs 49.0个月(HR=1.52, 95%CI:0.65~3.57,P=0.332),非靶向治疗组中位OS延长了14个月,差异无统计学意义(P>0.05);(6)中位OS在疗程<4疗程组、4~6疗程组、疗程>6疗程组分别为29.5个月vs 42.0个月vs 38.0个月(HR=0.74,95%CI:0.41~1.34,P=0.053),3组间差异无统计学意义(P>0.05)。结论:对于PSROC患者,满意的SCS给患者带来显著生存获益。对于不能直接行SCS患者,SNACT未尝不是一种可选择的治疗方式。含顺铂或卡铂的联合化疗仍是PSROC患者的首选治疗方案。