同源重组缺陷检测告知患者对高级别浆液性或子宫内膜样上皮性卵巢癌尼拉帕尼维持治疗的决定:一项健康技术评估

Q1 Medicine
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Based on two studies that evaluated patients and oncologists' preferences for maintenance therapy with a PARP inhibitor in the recurrent setting, a decrease in moderate to severe adverse events was more important for patients than an improvement in progression-free survival; however, improvement in progression-free survival was more important for oncologists. Both patients and oncologists accepted some trade-offs between efficacy and safety. The people with ovarian cancer we spoke with demonstrated a shared value for access to information, prevention of cancer recurrence, and overall survival with minimal adverse effects. This was consistent with findings from another survey in patients with ovarian cancer and at least one episode of recurrence, which suggest that patients prioritize treatment benefit over some treatment adverse events in the context of niraparib maintenance therapy. 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引用次数: 0

摘要

背景:卵巢癌影响卵巢细胞,上皮性癌是最常见的恶性卵巢癌类型。同源重组修复途径可以实现DNA双链断裂的无错误修复。与该途径相关的关键基因的损伤导致同源重组缺陷(HRD),从而导致DNA未修复并可能导致癌症。HRD的肿瘤被认为对多磷酸腺苷(ADP)-核糖聚合酶(PARP)抑制剂(如尼拉帕尼)治疗敏感。我们进行了一项健康技术评估,以评估HRD测试的临床效用和成本效益,以告知患者对高级别浆液性或子宫内膜样上皮性卵巢癌患者使用尼拉帕尼维持治疗的决定。我们还评估了尼拉帕尼维持治疗在HRD或同源重组能力(HRP)患者中的有效性和安全性、HRD检测的成本效益、公共资助HRD检测的预算影响以及患者的偏好和价值观。方法:对临床证据进行系统的文献检索。我们使用Cochrane随机试验风险偏倚工具第2版评估了每个纳入研究的偏倚风险,并根据建议评估、发展和评价分级(GRADE)工作组标准评估了证据体的质量。我们进行了系统的经济文献检索,并从公共付款人的角度进行了5年时间范围的成本效用分析。我们还分析了安大略省对卵巢癌患者进行HRD检测的公共资助对预算的影响。我们进行了文献检索,寻找患者和提供者对HRD检测和PARP抑制剂维持治疗的偏好的定量证据。为了了解HRD检测的潜在价值,我们采访了卵巢癌患者。结果:临床证据综述包括两项高级别上皮性卵巢癌的研究(一项为新诊断的晚期病例,另一项为复发性癌症患者)。这些研究评估了尼拉帕尼维持治疗与无维持治疗的比较,并根据HRD状态使用HRD测试对患者进行分组。与安慰剂相比,尼拉帕尼维持治疗提高了新诊断和复发卵巢癌患者以及HRD或HRP (GRADE: High)肿瘤患者的无进展生存期,但研究没有比较HRD组和HRP组之间的结果。尼拉帕尼组不良事件发生频率较高。我们没有发现评估HRD检测临床应用的研究。我们进行了初步的经济评估,以评估HRD检测对安大略省新诊断的卵巢癌患者的成本效益。我们的分析采用了5年的时间跨度。HRD测试(针对所有符合条件的患者或仅针对BRCA野生型患者)导致接受尼拉帕尼维持治疗的患者比例较低,从而降低了成本和更少的质量调整生命年(QALYs)。未进行HRD检测的患者平均总成本为131375美元,仅BRCA野生型患者进行HRD检测的患者平均总成本为126867美元,所有符合条件的患者进行HRD检测的患者平均总成本为127746美元。每位患者未进行HRD检测的平均总质量年为2.087,仅BRCA野生型患者进行HRD检测的平均总质量年为1.971,所有符合条件的患者进行HRD检测的平均总质量年为1.971。我们的预算影响分析表明,假设高接受率,公共资助对新诊断的卵巢癌患者进行HRD检测将导致在未来5年内总计节省900万美元(如果为所有人提供HRD检测资金)至1267万美元(如果为BRCA野生型患者提供HRD检测资金)。为复发性癌症患者提供HRD检测的公共资金将在未来5年内节省1631万美元(如果为所有人提供HRD检测资金)至2167万美元(如果为BRCA野生型患者提供HRD检测资金)。我们没有发现评估HRD测试的定量偏好的研究。两项研究评估了复发患者和肿瘤学家对PARP抑制剂维持治疗的偏好,对患者来说,中度至重度不良事件的减少比无进展生存期的改善更重要;然而,对肿瘤学家来说,无进展生存期的改善更为重要。患者和肿瘤学家都接受了疗效和安全性之间的一些权衡。与我们交谈的卵巢癌患者在获取信息、预防癌症复发和不良反应最小的总体生存方面表现出了共同的价值。 这与另一项针对至少一次复发的卵巢癌患者的调查结果一致,该调查表明,在尼拉帕尼维持治疗的背景下,患者优先考虑治疗益处而不是一些治疗不良事件。受访者还强调了医患伙伴关系、获得当地保健服务和患者教育的重要性。结论:在新诊断(晚期)或复发的高级别浆液性或子宫内膜样卵巢癌患者中,与无维持治疗相比,尼拉帕尼维持治疗可改善HRD或HRP肿瘤(GRADE: High)的无进展生存期。因为我们没有发现关于HRD检测临床应用的研究,所以我们不能评论它将如何影响患者的决定和临床结果。在5年的时间跨度内,对野生型BRCA患者进行HRD检测可以为每人节省4,509美元,并导致0.116 QALY的损失。我们的经济分析结果依赖于HRD测试后关于尼拉帕尼使用的假设。我们估计,公共资助HRD检测将为新诊断的癌症节省900万至1267万美元,并在5年内为复发癌症节省1631万至2167万美元,假设在HRD检测后尼拉帕尼维持治疗的使用将减少。患者优先考虑降低PARP抑制剂维持治疗中中度至重度不良事件的风险,而不是改善无进展生存期,肿瘤学家优先考虑改善无进展生存期,而不是降低中度至重度不良事件的风险。然而,患者和肿瘤学家都对治疗效果和毒性之间的某些权衡持开放态度。我们采访的人都有过卵巢癌和基因检测的经历,他们都很重视HRD检测对自己和家人的潜在临床益处。他们强调患者教育是安大略省公共资金的重要考虑因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Homologous Recombination Deficiency Testing to Inform Patient Decisions About Niraparib Maintenance Therapy for High-Grade Serous or Endometrioid Epithelial Ovarian Cancer: A Health Technology Assessment.

Background: Ovarian cancer affects the cells of the ovaries, and epithelial cancer is the most common type of malignant ovarian cancer. The homologous recombination repair pathway enables error-free repair of DNA double-strand breaks. Damage of key genes associated with this pathway leads to homologous recombination deficiency (HRD), which results in unrepaired DNA and can lead to cancer. Tumours with HRD are believed to be sensitive to treatment with poly-adenosine diphosphate (ADP)-ribose polymerase (PARP) inhibitors, such as niraparib. We conducted a health technology assessment to evaluate the clinical utility and cost-effectiveness of HRD testing to inform patient decisions about the use of niraparib maintenance therapy for patients with high-grade serous or endometrioid epithelial ovarian cancer. We also evaluated the efficacy and safety of niraparib maintenance therapy in patients with HRD or homologous recombination proficiency (HRP), the cost-effectiveness of HRD testing, the budget impact of publicly funding HRD testing, and patient preferences and values.

Methods: We performed a systematic literature search of the clinical evidence. We assessed the risk of bias of each included study using the Cochrane risk-of-bias tool for randomized trials version 2, and the quality of the body of evidence according to the Grading of Recommendations Assessment, Development, and Evaluation (GRADE) Working Group criteria. We performed a systematic economic literature search and conducted a cost-utility analysis with a 5-year time horizon from a public payer perspective. We also analyzed the budget impact of publicly funding HRD testing in people with ovarian cancer in Ontario. We performed a literature search for quantitative evidence of patient and provider preferences with respect to HRD testing and maintenance therapy with PARP inhibitors. To contextualize the potential value of HRD testing, we spoke with people with ovarian cancer.

Results: The clinical evidence review included two studies in high-grade epithelial ovarian cancer (one in patients with newly diagnosed advanced cases and one in patients with recurrent cancer). The studies evaluated niraparib maintenance therapy compared with no maintenance therapy and used HRD testing to group patients according to HRD status. Compared to placebo, niraparib maintenance therapy improved progression-free survival in patients with newly diagnosed and recurrent ovarian cancer, and in tumours with HRD or HRP (GRADE: High), but the studies did not compare the results between the HRD and HRP groups. The frequency of adverse events was higher in the niraparib group. We identified no studies that evaluated the clinical utility of HRD testing.We conducted a primary economic evaluation to evaluate the cost-effectiveness of HRD testing for people with newly diagnosed ovarian cancer in an Ontario setting. Our analysis used a 5-year time horizon. HRD testing (for all eligible people or only for people with BRCA wild type) resulted in a lower proportion of patients receiving niraparib maintenance therapy, leading to lower costs and fewer quality-adjusted life-years (QALYs). The average total cost per patient was $131,375 for no HRD testing, $126,867 for HRD testing only in people with BRCA wild type, and $127,746 for HRD testing in all eligible people. The average total QALYs per patient were 2.087 for no HRD testing, 1.971 for HRD testing only in people with BRCA wild type, and 1.971 for HRD testing in all eligible people. Our budget impact analysis suggested that assuming a high uptake rate, publicly funding HRD testing for people with newly diagnosed ovarian cancer would lead to a total saving of $9.00 million (if HRD testing were funded for all) to $12.67 million (if HRD testing were funded for people with BRCA wild type) over the next 5 years. Publicly funding HRD testing for people with recurrent cancer would lead to a total saving of $16.31 million (if HRD testing were funded for all) to $21.67 million (if HRD testing were funded for people with BRCA wild type) over the next 5 years.We identified no studies that evaluated quantitative preferences for HRD testing. Based on two studies that evaluated patients and oncologists' preferences for maintenance therapy with a PARP inhibitor in the recurrent setting, a decrease in moderate to severe adverse events was more important for patients than an improvement in progression-free survival; however, improvement in progression-free survival was more important for oncologists. Both patients and oncologists accepted some trade-offs between efficacy and safety. The people with ovarian cancer we spoke with demonstrated a shared value for access to information, prevention of cancer recurrence, and overall survival with minimal adverse effects. This was consistent with findings from another survey in patients with ovarian cancer and at least one episode of recurrence, which suggest that patients prioritize treatment benefit over some treatment adverse events in the context of niraparib maintenance therapy. Interviewees also emphasized the importance of the patient-doctor partnership, access to local health care services, and patient education.

Conclusions: In patients with newly diagnosed (advanced) or recurrent high-grade serous or endometrioid ovarian cancer, niraparib maintenance therapy improved progression-free survival compared with no maintenance therapy in tumours with HRD or HRP (GRADE: High). Because we identified no studies on the clinical utility of HRD testing, we cannot comment on how it would affect patient decisions and clinical outcomes.Over a 5-year time horizon, HRD testing for people with BRCA wild type could save $4,509 per person and lead to a loss of 0.116 QALY. The findings of our economic analyses are dependent on assumptions about the use of niraparib following HRD testing. We estimate that publicly funding HRD testing would lead to a total saving of $9 million to $12.67 million for newly diagnosed cancer, and a total saving of $16.31 million to $21.67 million for recurrent cancer over 5 years, assuming the use of niraparib maintenance therapy would be reduced following HRD testing.Patients prioritized decreasing the risk of moderate to severe adverse events of maintenance therapy with PARP inhibitors over improving progression-free survival, and oncologists prioritized improving progression-free survival over decreasing the risk of moderate to severe adverse events. However, both patients and oncologists were open to accepting certain trade-offs between treatment efficacy and toxicity. The people we interviewed, who had lived experience with ovarian cancer and genetic testing, valued the potential clinical benefits of HRD testing for themselves and their family members. They emphasized patient education as an important consideration for public funding in Ontario.

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Ontario Health Technology Assessment Series
Ontario Health Technology Assessment Series Medicine-Medicine (miscellaneous)
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