首页> 外文期刊>Lung cancer: Journal of the International Association for the Study of Lung Cancer >Clinical outcomes in extracranial tumor sites and unusual toxicities with concurrent whole brain radiation (WBRT) and Erlotinib treatment in patients with non-small cell lung cancer (NSCLC) with brain metastasis.
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Clinical outcomes in extracranial tumor sites and unusual toxicities with concurrent whole brain radiation (WBRT) and Erlotinib treatment in patients with non-small cell lung cancer (NSCLC) with brain metastasis.

机译:非转移性非小细胞肺癌(NSCLC)患者的颅外肿瘤部位的临床结果以及同时全脑放射(WBRT)和厄洛替尼治疗的异常毒性。

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BACKGROUND: Thirty percent of newly diagnosed NSCLC patients present with synchronous brain metastases, most of whom are treated with whole brain radiation. Systemic chemotherapy is usually avoided during WBRT due to concerns regarding toxicity. However, concurrent administration of targeted agents, such as Erlotinib, during WBRT may address systemic disease without causing toxicity. We report our institutional data on outcomes and toxicities with this treatment approach. MATERIALS AND METHODS: Medical records of patients with newly diagnosed NSCLC and brain metastases receiving concurrent WBRT and Erlotinib treatment were reviewed. Radiographic response to therapy and toxicities were analyzed. RESULT: Eight patients were identified and 7 were evaluable for response. All patients had intracranial disease control. In the extracranial sites, 3 (37.5%, intent-to-treat) showed partial response (PR), 2 (25%) had stable disease (SD), 1 (12.5%) had progression (PD) and 1 (12.5%) had new air space disease obscuring tumor response assessment. Among the three responders, two were female never smokers, while one was a female current smoker. Unanticipated grade 3 hepatotoxitity, hyponatremia, mental status changes, grade 3 and 4 thrombocytopenia, and grade 4 neutropenia with sepsis were observed. Three deaths occurred without clear signs of disease progression: one from neutropenic sepsis, one from wide spread air space disease, and one from neurologic deterioration. CONCLUSION: Our data demonstrates a high percentage of extracranial tumor response rates with first line Erlotinib in selected NSCLC patients. We observed unexpected serious complications and postulate possible mechanisms. We recommend caution to be exercised when considering Erlotinib treatment during WBRT, particularly in regard to drug-drug interactions and infection control. Data from prospective trials are needed to determine the benefits and toxicities of Erlotinib during WBRT.
机译:背景:新诊断的NSCLC患者中有30%出现同步脑转移,其中大多数接受全脑放射治疗。由于担心毒性,通常在WBRT期间避免全身化疗。但是,在WBRT期间同时施用靶向药物(例如厄洛替尼)可以解决全身性疾病而不会引起毒性。我们用这种治疗方法报告了关于结局和毒性的机构数据。材料与方法:回顾了新诊断为NSCLC并伴有WBRT和厄洛替尼治疗的脑转移患者的病历。分析了放射线对治疗和毒性的反应。结果:确定了8例患者,其中7例可评估反应。所有患者均进行了颅内疾病控制。在颅外部位,有3例(37.5%,意向性治疗)显示部分缓解(PR),2例(25%)患有稳定疾病(SD),1例(12.5%)患有进展(PD),1例(12.5%) )进行了新的航空疾病掩盖了肿瘤反应的评估。在这三个响应者中,有两个是从未吸烟的女性,而一个是目前吸烟的女性。观察到出乎意料的3级肝毒性,低血钠症,精神状态变化,3级和4级血小板减少症和4级中性粒细胞减少伴脓毒症。发生了三例死亡,但没有明确的疾病进展迹象:一例是中性粒细胞减少性败血症,一例是广泛空域疾病,另一例是神经系统恶化。结论:我们的数据表明,在某些非小细胞肺癌患者中,第一线厄洛替尼对颅外肿瘤的反应率很高。我们观察到了意想不到的严重并发症,并推测了可能的机制。我们建议在进行WBRT期间考虑厄洛替尼治疗时要特别小心,尤其是在药物相互作用和感染控制方面。需要前瞻性试验的数据来确定厄洛替尼在WBRT期间的益处和毒性。

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