Cyclophosphamide, doxorubicin, and vincristine in etoposide- and cisplatin-resistant small cell lung cancer.

Cancer treatment reports Pub Date : 1987-10-01
F A Shepherd, W K Evans, R MacCormick, R Feld, J C Yau
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Abstract

For two chemotherapy regimens to be truly non-cross-resistant, each should be active as first-line therapy and also as second-line therapy. The effectiveness of both cyclophosphamide, doxorubicin, and vincristine (CAV) and etoposide and cisplatin (VPP) in previously untreated patients with small cell lung cancer has been well-documented. Also, VPP has caused tumor regression in up to 50% of patients when used as second-line therapy after CAV. The effectiveness of CAV after progression or relapse after VPP has not been documented. We identified 29 patients who received CAV after their tumors failed to respond or relapsed after VPP or etoposide and carboplatin (VPC). There were 21 male and eight female patients (median age, 57 years; range, 30-79). Thirteen patients were treated following failure to respond to VPP or VPC and 16 at the time of relapse. Eight patients had limited disease and 21 had extensive disease. Metastatic sites included liver (11 patients), bone (ten), lymph nodes (seven), bone marrow (three), brain (four), and contralateral lung (one). There were three complete responses (durations of 16, 22, and 26 weeks) and five partial responses (duration, 8+ to 36 weeks). Three patients had stable disease and 18 patients had disease progression while receiving treatment. The median survival of the entire group was 15 weeks. Responding patients had a median survival of 34 weeks (range, 8+ to 72+) and stable and nonresponding patients had a survival of only 9 weeks (range, 2-38). A granulocyte count nadir less than 500 X 10(9)/L was seen after 7.9% of evaluable treatment cycles and a platelet count nadir less than 50,000 X 10(9)/L occurred after only 5.3% of cycles. Five patients required transfusion for anemia, and two patients required dose reduction of vincristine for peripheral neuropathy. This study demonstrates that CAV has limited activity following failure to respond to VPP.

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环磷酰胺、阿霉素和长春新碱在依托泊苷和顺铂耐药小细胞肺癌中的作用。
对于两种真正无交叉耐药的化疗方案,每一种都应该作为一线治疗和二线治疗有效。环磷酰胺、阿霉素和长春新碱(CAV)以及依托泊苷和顺铂(VPP)治疗先前未经治疗的小细胞肺癌患者的有效性已经得到了充分的证明。此外,当VPP作为CAV后的二线治疗时,高达50%的患者肿瘤消退。在VPP进展或复发后CAV的有效性尚未得到证实。我们确定了29例在VPP或依托泊苷加卡铂(VPC)治疗后肿瘤无效或复发后接受CAV治疗的患者。男性21例,女性8例(中位年龄57岁;范围内,30 - 79)。13名患者在VPP或VPC治疗无效后接受治疗,16名患者在复发时接受治疗。局限性病变8例,广泛性病变21例。转移部位包括肝(11例)、骨(10例)、淋巴结(7例)、骨髓(3例)、脑(4例)和对侧肺(1例)。有3个完全缓解(持续时间为16、22和26周)和5个部分缓解(持续时间为8+至36周)。3例病情稳定,18例在治疗过程中病情进展。整个组的中位生存期为15周。应答患者的中位生存期为34周(范围8+至72+),而稳定和无应答患者的生存期仅为9周(范围2-38)。在7.9%的可评估治疗周期后,粒细胞计数最低低于500 X 10(9)/L,血小板计数最低低于50,000 X 10(9)/L仅在5.3%的周期后发生。5例患者因贫血需要输血,2例患者因周围神经病变需要减少长春新碱的剂量。本研究表明,CAV在对VPP无效后活性有限。
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