首页> 美国卫生研究院文献>British Journal of Cancer >Persistent gestational trophoblastic disease: results of MEA (methotrexate etoposide and dactinomycin) as first-line chemotherapy in high risk disease and EA (etoposide and dactinomycin) as second-line therapy for low risk disease
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Persistent gestational trophoblastic disease: results of MEA (methotrexate etoposide and dactinomycin) as first-line chemotherapy in high risk disease and EA (etoposide and dactinomycin) as second-line therapy for low risk disease

机译:持续性妊娠滋养细胞疾病:作为高危疾病一线化疗的MEA(甲氨蝶呤依托泊苷和放线菌素)和作为低危疾病二线治疗的EA(依托泊苷和放线菌素)作为结果

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摘要

Persistent gestational trophoblastic disease is potentially fatal, but the majority of patients are cured with chemotherapy. Any developments in treatment are therefore being directed towards maintaining efficacy and reducing toxicity. We evaluated efficacy and toxicity of methotrexate, etoposide and dactinomycin (MEA) as first-line therapy for high risk disease and etoposide and dactinomycin (EA) as second-line therapy for methotrexate-refractory low risk disease in a retrospective analysis of 73 patients (38 MEA, 35 EA) treated since 1986 at a supra-regional centre. The median follow-up period was 5.5 years and the median number of cycles received was 7. The overall complete response rate was 85% (97% for EA, 75% for MEA). Of eight patients who failed to respond, four have since died and four were cured with platinum-based chemotherapy. Alopecia was universal. Grade II or worse nausea, emesis, or stomatitis was observed in 29%, 30% and 37% respectively. Fifty-one per cent experienced grade II/III anaemia, 8% grade II or higher thrombocytopenia and 64% grade III or IV neutropenia; in six cases this was complicated by sepsis. Fifty-four per cent of patients went on to have a normal pregnancy. No patient has developed a second malignancy. In conclusion, the MEA and EA chemotherapy regimens for persistent trophoblastic disease are very well tolerated, do not appear to affect future fertility and are associated with excellent, sustained complete response rates. © 2000 Cancer Research Campaign
机译:持续性妊娠滋养细胞疾病可能致命,但大多数患者可通过化学疗法治愈。因此,治疗方面的任何发展都致力于维持功效和降低毒性。我们对73例患者进行了回顾性分析,评估了甲氨蝶呤,依托泊苷和放线菌素(MEA)作为高危疾病的一线治疗的疗效和毒性,而依托泊苷和放线菌素(EA)作为甲氨蝶呤难治性低危疾病的二线治疗的疗效和毒性(自1986年以来,在上述区域中心对38 MEA,35 EA)进行了治疗。中位随访期为5.5年,中位周期数为7。总的完全缓解率为85%(EA为97%,MEA为75%)。在八名未能缓解的患者中,有四名已经死亡,四名已通过铂类化学疗法治愈。脱发是普遍的。观察到II级或更严重的恶心,呕吐或口腔炎分别占29%,30%和37%。 51%经历过II / III级贫血,8%达到II级或更高的血小板减少症和64%达到III级或IV级中性粒细胞减少症;在六例中,这是由败血症引起的。 54%的患者继续正常妊娠。没有患者发生第二次恶性肿瘤。总之,针对持续性滋养细胞疾病的MEA和EA化疗方案具有很好的耐受性,似乎不会影响未来的生育能力,并且具有出色的持续完全缓解率。 ©2000癌症研究运动

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