Pegylated Liposomal Doxorubicin for Advanced Ovarian Cancer in Women who are Refractory to Both Platinum- and Paclitaxel-Based Chemotherapy Regimens

T. Sugiyama, S. Kumagai
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引用次数: 1

Abstract

Pegylated liposomal doxorubicin (PLD) is doxorubicin HCl encapsulated in long-circulating STEALTH® liposomes (Doxil®). PLD achieves good response rates and many patients maintain long-lasting stable disease (SD), which is one of the advantages. In addition, the clinical benefit is high in platinum-resistant disease, and PLD is thus considered to be the first option. PLD is associated with a number of adverse events, but these events are mild to moderate. PLD is safer for heavily pretreated patients than topotecan and gemcitabine due to mild bone-marrow toxicity, but that nonhematotoxity, such as PPE, stomatitis, mucositis, and other cutaneous reactions were the most common side effects attributable to PLD. Based on a review of previous studies, there are no differences in efficacy between 50 and 40 mg/m2 of PLD, therefore, a dose of 40 mg/m2 is preferable in patients with platinum-resistant disease to reduce adverse events. The 1-hour infusion schedule every 4 weeks makes PLD easy to administer. A rational approach to combine PLD with other drugs should take the slow accumulation and delayed peak of PLD in tumors into consideration. When combined with other useful agents, the lower dose of PLD (30 to 35 mg/m2) with a 3-week schedule may reduce severe PPE and stomatitis with negligible effects on the level of DI and the therapeutic efficacy.
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聚乙二醇脂质体阿霉素对铂类和紫杉醇类化疗方案均难治的晚期卵巢癌患者的治疗
聚乙二醇脂质体阿霉素(PLD)是阿霉素HCl封装在长循环的STEALTH®脂质体(Doxil®)。PLD具有良好的应答率,许多患者保持了长期稳定的疾病(SD),这是其优势之一。此外,铂耐药疾病的临床获益较高,因此PLD被认为是首选。PLD与许多不良事件有关,但这些事件是轻微到中度的。由于轻度骨髓毒性,PLD对于重度预处理患者比拓扑替康和吉西他滨更安全,但非血液毒性,如PPE、口腔炎、粘膜炎和其他皮肤反应是PLD最常见的副作用。根据对以往研究的回顾,50mg /m2和40mg /m2的PLD在疗效上没有差异,因此,40mg /m2的剂量对铂耐药患者更可取,以减少不良事件。每4周1小时的输注计划使PLD易于管理。考虑到PLD在肿瘤内蓄积缓慢、峰值延迟的特点,合理联合其他药物治疗。当与其他有用的药物联合使用时,低剂量的PLD(30至35 mg/m2), 3周的疗程可以减少严重的PPE和口炎,对DI水平和治疗效果的影响可以忽略不计。
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