HER2 testing to manage patients with breast cancer or other solid tumors.

Jerome Seidenfeld, David J Samsom, Barbara M Rothenberg, Claudia J Bonnell, Kathleen M Ziegler, Naomi Aronson
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Abstract

Objectives: Systematic review of trastuzumab outcomes among breast cancer patients who have negative, equivocal, or discordant HER2 assay results; use of HER2 assay results to predict outcomes of chemotherapy or hormonal therapy regimen for breast cancer; use of serum HER2 to monitor treatment response or disease progression in breast cancer patients; and use of HER2 testing to manage patients with lung, ovarian, prostate, or head and neck tumors. Also, narrative review of concordance of HER2 assays.

Data sources: We abstracted data from: three articles plus one conference abstract on negative, equivocal, or discordant HER2 results; 26 studies on selection of chemotherapy or hormonal therapy; 15 studies on serum HER2; and 26 studies on ovarian, lung, prostate, or head and neck tumors. Foreign-language studies were included.

Review methods: We sought randomized trials or single-arm series (prospective or retrospective) of identically treated patients that presented relevant outcome data associated with HER2 status.

Results: HER2 assay results are influenced by multiple biologic, technical, and performance factors. Many aspects of HER2 assays were standardized only recently, so inconsistencies confound the literature comparing different methods. The evidence is weak on outcomes of trastuzumab added to chemotherapy for HER2-equivocal, -discordant, or -negative patients. Evidence comparing chemotherapy outcomes in HER2-positive and HER2-negative patient subgroups may generate hypotheses, but is too weak to test hypotheses. Only a rigorous test can resolve whether HER2-positive patients (but not HER2-negative patients) benefit from an anthracycline regimen. Evidence is available only from uncontrolled series on whether HER2 status predicts complete pathologic response to neoadjuvant chemotherapy. Evidence also is weak regarding differences by HER2 status for outcomes of chemotherapy for advanced or metastatic disease; with most studies lacking statistical power. Data from studies of tamoxifen and aromatase inhibitors suggest that future studies should examine whether HER2 status predicts response to specific hormonal therapies among estrogen-receptor-positive patients. The evidence is weak on whether serum HER2 predicts outcome after treatment with any regimens in any setting, as is the evidence on use of serum or tissue HER2 testing for malignancies of lung, ovary, head and neck, or prostate.

Conclusions: Overall, few studies directly investigated the key questions of this systematic review. Going forward, cancer therapy trial protocols should incorporate elements to facilitate robust analyses of the use of HER2 status and other biomarkers for managing treatment.

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HER2检测用于治疗乳腺癌或其他实体肿瘤患者。
目的:对HER2检测结果阴性、模棱两可或不一致的乳腺癌患者的曲妥珠单抗结局进行系统评价;使用HER2检测结果预测乳腺癌化疗或激素治疗方案的结果;使用血清HER2监测乳腺癌患者的治疗反应或疾病进展;以及使用HER2检测来管理肺、卵巢、前列腺或头颈部肿瘤患者。此外,对HER2检测的一致性进行了叙述性回顾。数据来源:我们提取的数据来自:三篇文章和一篇关于阴性、模棱两可或不一致HER2结果的会议摘要;26项关于化疗或激素治疗选择的研究;血清HER2研究15项;还有26项关于卵巢,肺,前列腺,头颈部肿瘤的研究。外语学习也包括在内。回顾方法:我们寻找随机试验或单臂系列(前瞻性或回顾性)相同治疗的患者,提供与HER2状态相关的相关结果数据。结果:HER2检测结果受多种生物、技术和性能因素的影响。HER2检测的许多方面直到最近才标准化,因此比较不同方法的文献中存在不一致性。对于her2模棱两可、her2不一致或her2阴性患者,曲妥珠单抗加入化疗的结果证据不足。比较her2阳性和her2阴性患者亚组化疗结果的证据可能会产生假设,但太弱而无法检验假设。只有严格的测试才能确定her2阳性患者(而不是her2阴性患者)是否从蒽环类药物治疗中获益。关于HER2状态是否能预测新辅助化疗的完全病理反应的证据仅来自非对照系列。关于晚期或转移性疾病化疗结果的HER2状态差异的证据也很薄弱;大多数研究缺乏统计能力。来自他莫昔芬和芳香酶抑制剂研究的数据表明,未来的研究应该检查HER2状态是否能预测雌激素受体阳性患者对特定激素治疗的反应。关于血清HER2是否能预测在任何情况下使用任何方案治疗后的预后的证据都很薄弱,就像使用血清或组织HER2检测肺部、卵巢、头颈部或前列腺恶性肿瘤的证据一样。结论:总体而言,很少有研究直接探讨了本系统综述的关键问题。展望未来,癌症治疗试验方案应该包含一些元素,以促进对HER2状态和其他生物标志物的使用进行强有力的分析,以管理治疗。
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