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Cyclophosphamide and etoposide for non-small cell and small cell lung cancer.

机译:环磷酰胺和依托泊苷用于非小细胞和小细胞肺癌。

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摘要

Oral chemotherapeutic regimens with limited toxicity are desirable in that quality of life can be maintained and clinic/hospital visits minimised during therapy. We have investigated the use of extended courses of oral cyclophosphamide and oral etoposide for the treatment of non-small cell lung cancer (NSCLC) and small cell lung cancer (SCLC). A 14-day course of oral combination chemotherapy every 28 days resulted in a 12% response rate and a median survival of 6 months (1-year survival, 26%) in stage IV NSCLC. This regimen could not be intensified with carboplatin because of synergistic granulocytopenia. A 14-day course every 28 days resulted in a 40% response rate and a median survival of 7 months in poor-prognosis extensive-disease SCLC. Pharmacodynamic modelling revealed that the granulocyte nadir could be predicted from a single plasma etoposide level drawn on the second day of therapy, potentially allowing dose adjustment during the treatment cycle. Oral chemotherapy remains a promising route for the treatment of lung cancer.
机译:具有毒性有限的口服化疗方案是理想的,因为在治疗过程中可以维持生活质量并最大程度地减少临床/医院就诊次数。我们已经研究了口服环磷酰胺和口服依托泊苷的扩展疗程用于非小细胞肺癌(NSCLC)和小细胞肺癌(SCLC)的治疗。 IV期NSCLC每28天进行14天的口服联合化疗疗程可导致12%的缓解率和6个月的中位生存期(1年生存率26%)。由于协同性粒细胞减少症,不能用卡铂加强该方案。每28天进行14天的疗程可导致预后不良的广泛疾病SCLC的缓解率达到40%,中位生存期为7个月。药效学模型揭示,可以从治疗第二天抽取的血浆血浆依托泊苷水平预测粒细胞最低点,从而有可能在治疗周期内调整剂量。口服化疗仍然是治疗肺癌的有前途的途径。

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