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Long-term complications of chemotherapy for germ cell tumours.

机译:生殖细胞肿瘤化疗的长期并发症。

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Testicular cancer is the most common solid tumour among young males aged 15-35 years. Cisplatin-based combination chemotherapy has changed the outlook of this disease. Disseminated testicular cancer, once uniformly fatal, now has a cure rate of more than 80% with combination chemotherapy. Systematic randomised trials have shown that cisplatin, etoposide and bleomycin (PEB) combination chemotherapy remains the mainstay of treatment. While there is a high cure rate with chemotherapy in patients with this disease, some long-term complications from chemotherapy have now been recognised, including secondary leukaemia, therapy-related solid tumours, nephrotoxicity, neurotoxicity, pulmonary toxicity, vascular toxicity and infertility. Etoposide, a DNA topoisomerase II inhibitor, is a significant risk factor for developing leukaemia; the risk appears to be correlated with the total dose given. Patients receiving cisplatin-based combination chemotherapy for testicular cancer also appear to have a higher relative risk for developing second non-germ cell malignancies; the greatest risks for therapy-related solid tumours were seen with a combination of radiation therapy plus chemotherapy. Long-term vascular toxicities associated with chemotherapy include Raynaud's phenomenon, acute myocardial infarction and cerebrovascular events. Bleomycin is thought to be the most important drug in the pathogenesis of Raynaud's phenomenon, while cisplatin is the most likely agent involved in myocardial infarction. Peripheral neuropathy is the most common form of neurotoxicity observed with cisplatin-based chemotherapy. Risk factors for the development of neural damage include a high cumulative dose of cisplatin, the use of vinblastine and the concomitant development of Raynaud's phenomenon. Cisplatin is also well known to cause significant nephrotoxicity. Approximately 25% of patients present with azoospermia after undergoing combination chemotherapy with a follow up of 2-5 years. Physician awareness of complications associated with chemotherapy is vital to maximise efficacy, minimise toxicity, and preserve quality of life after treatment. Sperm cryopreservation should be considered for patients who desire children. Close monitoring during therapy allows for the early diagnosis of complications, and close follow up of patients after the completion of therapy is necessary to monitor for relapse and development of long-term complications such as myelodysplastic syndrome and leukaemia. Despite these complications, given the potential for cure rates in this young group of patients, the benefits far outweigh the risks.
机译:睾丸癌是15-35岁的年轻男性中最常见的实体瘤。基于顺铂的联合化疗改变了这种疾病的面貌。曾经一度致命的播散性睾丸癌现在通过联合化疗治愈率超过80%。系统性随机试验表明,顺铂,依托泊苷和博来霉素(PEB)联合化疗仍是治疗的主要手段。尽管该疾病患者的化疗治愈率很高,但现已认识到化疗带来的一些长期并发症,包括继发性白血病,与治疗有关的实体瘤,肾毒性,神经毒性,肺毒性,血管毒性和不育。依托泊苷,一种DNA拓扑异构酶II抑制剂,是发生白血病的重要危险因素。风险似乎与给定的总剂量有关。接受以顺铂为基础的联合化疗治疗睾丸癌的患者似乎也有较高的相对危险性发展为第二种非生殖细胞恶性肿瘤。放疗加化疗相结合,发现与治疗相关的实体瘤的最大风险。与化学疗法有关的长期血管毒性包括雷诺现象,急性心肌梗塞和脑血管事件。博来霉素被认为是雷诺现象发病机理中最重要的药物,而顺铂是最可能参与心肌梗塞的药物。周围神经病变是基于顺铂的化学疗法观察到的最常见的神经毒性形式。神经损伤发生的危险因素包括顺铂的高累积剂量,长春碱的使用以及雷诺现象的伴随发展。众所周知,顺铂会引起明显的肾毒性。约有25%的患者在接受联合化疗并随访2-5年后出现无精症。医生对与化学疗法相关的并发症的意识对于最大化疗效,最小化毒性以及维持治疗后的生活质量至关重要。对于需要孩子的患者,应考虑精子冷冻保存。治疗期间应密切监测,以便及早诊断出并发症,治疗结束后应密切随访患者,以监测长期并发症如骨髓增生异常综合症和白血病的复发和发展。尽管存在这些并发症,但考虑到这一年轻患者治愈率的潜力,其收益远大于风险。

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