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Extended-schedule oral etoposide in selected neoplasms and overview of administration and scheduling issues.

机译:某些肿瘤的延长时间表口服依托泊苷,以及给药和时间表问题概述。

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Extended schedules of oral etoposide have been evaluated in many types of advanced cancer. In addition to their use in the common solid tumours, extended schedules have been employed in Kaposi's sarcoma (both AIDS-related and endemic types), medulloblastoma, glioma, and hepatocellular carcinoma. Single agent activity was demonstrated in all of these tumour subtypes. For patients with carcinoma of unknown primary site, we have recently incorporated a 10-day oral etoposide schedule into a combination regimen that also includes paclitaxel and carboplatin. With this regimen we achieved a 47% response rate in a group of 53 evaluable patients, with a median survival of 13.4 months. Patients with adenocarcinoma and poorly differentiated carcinoma of unknown primary site had comparable response rates and survival. According to a large number of clinical trials and pharmacokinetic data, a daily oral etoposide dose of 50 mg/m2 consistently produces serum concentrations >1 mg/L for several hours each day. Lower doses fail to consistently produce this serum concentration, which is considered necessary for optimum tumoricidal activity. Optimal dose duration is 10 to 14 days, particularly when combination regimens are being employed. Oral etoposide has an established role as a single agent in patients with low grade non-Hodgkin's lymphoma, Kaposi's sarcoma, and testicular cancer (if residual carcinoma is resected after first-line treatment). The optimal use of extended-schedule etoposide in combination regimens is not defined but is being evaluated in a number of etoposide-sensitive malignancies.
机译:在许多类型的晚期癌症中已经评估了口服依托泊苷的时间表。除了在常见的实体瘤中使用外,在卡波西氏肉瘤(与艾滋病有关的和地方性的两种类型),髓母细胞瘤,神经胶质瘤和肝细胞癌中也采用了延长的治疗方案。在所有这些肿瘤亚型中均证明了单药活性。对于原发灶未知的癌症患者,我们最近将10天口服依托泊苷方案纳入了包括紫杉醇和卡铂的联合治疗方案中。通过这种方案,我们在53名可评估患者中实现了47%的缓解率,中位生存期为13.4个月。腺癌和原发部位未知的低分化癌患者的缓解率和生存率相当。根据大量的临床试验和药代动力学数据,每日口服依托泊苷剂量为50 mg / m2,每天持续数小时,其血清浓度始终> 1 mg / L。较低剂量不能持续产生该血清浓度,这被认为是最佳杀肿瘤活性所必需的。最佳剂量持续时间为10到14天,尤其是在采用联合治疗方案时。口服依托泊苷已在低级非霍奇金淋巴瘤,卡波济肉瘤和睾丸癌(如果在一线治疗后切除残留癌)中作为单一药物已确立作用。延长方案依托泊苷在联合用药方案中的最佳用法尚未确定,但正在许多依托泊苷敏感的恶性肿瘤中进行评估。

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