氟达拉滨在急性髓系白血病治疗中的应用。

Graham H Jackson
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引用次数: 21

摘要

急性髓性白血病(AML)是一种疾病,如果不及时治疗,总是致命的。这种疾病在老年人中更常见,由于不良预后因素的发生率更高,老年人的病情也比年轻AML患者更差,如表现不佳、多种合共病、对治疗的耐受性降低、“不利的”染色体异常和多药耐药蛋白-1表达。虽然许多患者完全缓解,但复发率高,复发后预后很差。近年来,使用含氟达拉滨的联合治疗AML,最常见的是氟达拉滨+阿糖胞苷+粒细胞集落刺激因子(G-CSF) [FLAG], FLAG +米托沙酮(FLANG)或FLAG +伊达柔比星(FLAG- ida)。这种组合最大化了阿糖胞苷和G-CSF之间以及阿糖胞苷和氟达拉滨之间有利的细胞毒性相互作用。在小型研究中,这些联合治疗作为二线治疗的完全缓解率(CR)为36-59%。早期回顾性分析表明,难治性AML患者的CR率高于复发性AML患者,但这一观察结果尚未在最近的前瞻性试验中得到证实。含氟达拉滨的联合治疗也被评估为高危患者的一线治疗,CR率为34-70%,中位生存期为7 - 16个月。目前的大型MRC随机高风险研究将提供关于在预后不良的AML患者中使用含氟达拉滨方案的进一步数据。进一步的研究正在调查氟达拉滨与其他药物(如吉妥珠单抗ozogamicin和吉西他滨)在AML患者中的联合使用。
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Use of fludarabine in the treatment of acute myeloid leukemia.

Acute myeloid leukemia (AML) is a disease, which when left untreated, is invariably fatal. The disease is more common in elderly people, who also fare worse than younger patients with AML due to a higher rate of unfavorable prognostic factors, such as poor performance status, multiple comorbidities, reduced tolerance to treatment, 'unfavorable' chromosomal abnormalities and multidrug resistant protein-1 expression. While many patients achieve a complete remission, the rate of relapse is high and prognosis after relapse very poor. Promising results have been published in recent years using fludarabine-containing combination therapy for AML, most commonly fludarabine +cytarabine + granulocyte colony-stimulating factor (G-CSF) [FLAG], FLAG + mitoxantrone (FLANG), or FLAG + idarubicin (FLAG-Ida). Such combinations maximize favorable cytotoxic interactions between cytarabine and G-CSF, and between cytarabine and fludarabine. In small studies, such combinations used as second-line therapy have resulted in complete response (CR) rates of 36-59%. Early retrospective analyses suggested higher CR rates in patients with refractory AML than in those with relapsed AML, but this observation has not been confirmed in recent prospective trials. Fludarabine-containing combinations have also been evaluated as first-line therapy in high-risk patients and resulted in CR rates of 34-70%, with median survival from 7 to 16 months. The current large MRC randomized high-risk study will provide further data on the use of fludarabine-containing regimens in patients with poor prognosis AML. Further studies are investigating the use of fludarabine in combination with other agents, such as gemtuzumab ozogamicin and gemcitabine, in patients with AML.

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