多聚ADP核糖聚合酶抑制剂(PARPi)与化疗联合治疗复发性卵巢癌的疗效和安全性对比:系统综述。

Shittu Muhammad Adamu, Olaoye Stephen Oyewole, Umar Farouk Kabir
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引用次数: 0

摘要

手术细胞减灭术后的铂类化疗是治疗晚期卵巢癌(OC)的通用疗法,然而,约 80% 的患者会复发,无进展生存期仍然很短。治疗后一年内复发的患者最终会对二线化疗产生耐药性。多ADP核糖聚合酶抑制剂是一类新型靶向疗法,可通过增强其他细胞毒药物的化疗活性来克服这些挑战。我们在《护理与专职医疗文献累积索引》(CINHAL)、Cochrane和PubMed数据库中搜索了2011年至2022年期间报道PARP抑制剂与化疗联合治疗复发性OC的疗效和安全性的潜在相关主要出版物,并对其进行了综述。定性评估的相关结果是无进展生存期(PFS)和3级或以上不良事件(AEs),分别作为疗效和安全性的衡量标准。系统性综述共纳入了八项随机对照试验(RCT),对PARP抑制剂的疗效和安全性进行了评估:Olaparib、niraparib和veliparib与贝伐珠单抗、卡铂、顺铂、塞地拉尼、环磷酰胺和紫杉醇联合使用。824名患者有33个BRCA基因突变,1430名患者有野生型BRCA基因突变,这种等位基因会增加患癌症的风险。大多数患者患有对铂类药物敏感的癌症。在所有纳入的试验中,PARP抑制剂与化疗的联合应用与化疗相比,PFS明显延长,只有一项试验除外,该试验将veliparib与环磷酰胺联合应用。BRCA基因突变患者的PFS延长更为明显,野生型BRCA患者的PFS延长也偶尔出现。尼拉帕利和veliparib明显与3级或3级以上贫血、中性粒细胞减少和血小板减少有关,奥拉帕利会引起疲劳和胃肠功能紊乱,而贝伐单抗和西地尼布会引起高血压。本综述认为,与化疗相比,PARP抑制剂和化疗联合使用可明显延长无进展生存期,尤其是在BRCA基因突变患者中,而且联合治疗是安全的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Efficacy and safety of combination of poly-ADP-ribose polymerase inhibitor (PARPi) and chemotherapy compared with chemotherapy alone in treatment of recurrent ovarian carcinoma: a systematic review.

Platinum-based chemotherapy after surgical cytoreduction is the universal treatment for advanced ovarian cancer (OC), however, about eighty percent of patients experienced relapse and progression-free survival remained poor. Patients who relapsed within one year of treatment eventually become resistant to second-line chemotherapy. Poly-ADP-ribose polymerase inhibitors are a novel class of targeted therapy that could overcome these challenges by augmenting the chemotherapeutic activity of other cytotoxic agents. Cumulative Index to Nursing and Allied Health Literature (CINHAL), Cochrane and PubMed databases were searched for potentially relevant primary publications from 2011 to 2022 reporting on efficacy and safety of combination of a PARP inhibitor and chemotherapy versus chemotherapy in recurrent OC and reviewed. The outcomes of interest assessed qualitatively were progression-free survival (PFS) and grade 3 or higher adverse events (AEs) as measures of efficacy and safety respectively. Eight randomized controlled trials (RCTs) were included in the systematic review comprising 3,021 patients evaluated efficacy and safety of PARP inhibitors: Olaparib, niraparib and veliparib with combinations of bevacizumab, carboplatin, cisplatin, cediranib, cyclophosphamide and paclitaxel. 824 patients had 33 BRCA mutation while 1,430 had wild-type BRCA, an allele that confers increased risk of cancer. Most patients had platinum-sensitive cancers. There was significant prolongation of PFS with PARP inhibitor and chemotherapy combination compared to chemotherapy in all included trials except one which combined veliparib with cyclophosphamide. The prolongation of PFS was more remarkable in patients with BRCA mutation and occasionally patients with wild-type BRCA. Niraparib and veliparib were notably associated with grade 3 or higher anaemia, neutropenia, and thrombocytopenia, olaparib caused fatigue and gastrointestinal disturbances while bevacizumab and cediranib caused hypertension. This review suggested combined PARP inhibitor and chemotherapy significantly prolonged progression-free survival especially in patients with BRCA mutation compared to chemotherapy and the combined therapy is safe.

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