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Adjuvant therapy for HER2+ breast cancer: practice, perception, and toxicity

机译:HER2 +乳腺癌的辅助治疗:实践,知觉和毒性

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Multiple adjuvant regimens are used for HER2+ breast cancer, but experience in routine practice is not reported. We evaluated whether oncologists’ perceptions of these regimens matches clinical experience. We surveyed Wisconsin medical oncologists throughout the state regarding factors impacting selection of TCH (docetaxel, carboplatin, and trastuzumab) or anthracycline-based therapy. We also reviewed 200 cases of HER2+ breast cancer treated at the University of Wisconsin and the Marshfield Clinic and collected data on patient and tumor characteristics, chemotherapy regimen, and toxicities. Two-thirds of surveyed oncologists prefer anthracycline-based therapy, particularly for node-positive cancers. However, TCH was preferred for early-stage (T1a-bN0) tumors. Half of oncologists use prophylactic G-CSF with TCH. In the 200 cases reviewed at our centers, acute toxicity occurred more frequently with TCH. There were fewer dose modifications or delays for AC-TH (doxorubicin, cyclophosphamide, paclitaxel, and trastuzumab) than TCH (31% vs. 47%, P = 0.07), possibly due to higher use of prophylactic G-CSF with AC-TH (77% vs. 34% with TCH, P < 0.001). Fifteen patients received prophylactic G-CSF during TCH; none developed neutropenic fever. In contrast, 25% developed neutropenic fever during TCH without G-CSF. There were modest declines in median left ventricular ejection fraction reaching 9% with AC-TH and 3% with TCH at 12 months, but early cessation of trastuzumab was similar for both regimens. We conclude that TCH and AC-TH are common adjuvant regimens used for HER2+ breast cancer. The preference of TCH for early-stage disease and anthracycline-based therapy for node-positive disease suggests that many oncologists perceive that TCH is safer and AC-TH more effective. Myelosuppression from TCH is greater than AC-TH, but can be mitigated with routine G-CSF.
机译:多种辅助疗法可用于HER2 +乳腺癌,但尚未报道常规实践的经验。我们评估了肿瘤学家对这些治疗方案的看法是否与临床经验相符。我们调查了威斯康星州全州的肿瘤科医生,了解影响TCH(多西他赛,卡铂和曲妥珠单抗)或蒽环类药物治疗选择的因素。我们还回顾了在威斯康星大学和马什菲尔德诊所治疗的200例HER2 +乳腺癌患者,并收集了有关患者和肿瘤特征,化疗方案和毒性的数据。三分之二的接受调查的肿瘤科医生更喜欢以蒽环类为基础的疗法,特别是对于淋巴结阳性的癌症。但是,TCH对于早期(T1a-bN0)肿瘤是首选。一半的肿瘤科医生对TCH使用预防性G-CSF。在我们中心审查的200例病例中,TCH急性毒性发生的频率更高。 AC-TH(阿霉素,环磷酰胺,紫杉醇和曲妥珠单抗)的剂量修改或延迟时间少于TCH(31%比47%,P = 0.07),这可能是由于预防性G-CSF与AC-TH的使用增加了(77%,而TCH为34%,P <0.001)。 15例患者在TCH期间接受了预防性G-CSF治疗;没有人发生中性粒细胞减少症。相反,没有G-CSF的TCH患者中有25%出现中性白细胞减少症。在12个月时,AC-TH的左心室射血分数中位数有适度下降,而TCH则为3%,但两种方案的曲妥珠单抗的早期停用相似。我们得出结论,TCH和AC-TH是用于HER2 +乳腺癌的常见辅助方案。 TCH对于早期疾病的偏爱和对蒽环类疾病的基于蒽环类的疗法的偏爱表明,许多肿瘤学家认为TCH更安全,AC-TH更有效。 TCH引起的骨髓抑制大于AC-TH,但可以通过常规G-CSF缓解。

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