黄匹吡醇在慢性淋巴细胞白血病中的作用

Beth A. Christian , Beth Fischer , Kristie A. Blum , Michelle Brooker-McEldowney , Mollie E. Moran , Leslie A. Andritsos , Mitch A. Phelps , James T. Dalton , A. Dimitrios Colevas , John C. Byrd , Michael R. Grever , Thomas S. Lin
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引用次数: 4

摘要

尽管慢性淋巴细胞白血病(CLL)对治疗有反应,但患者总是会复发,许多晚期疾病患者获得p53基因突变或缺失,导致对大多数标准治疗产生耐药性。Alemtuzumab对p53缺陷CLL有活性,但对大体积淋巴结疾病无效,并引起显著的免疫抑制。因此,需要针对高风险、复发性CLL患者的新疗法。人工合成的黄酮黄吡醇体外诱导CLL细胞凋亡,但在临床试验中,连续24 - 72小时静脉输注黄吡醇未观察到临床活性。与人血浆蛋白结合导致游离黄吡醇浓度不足,持续静脉滴注给药。药代动力学模型表明,黄匹立多静脉注射30分钟,然后连续静脉注射4小时,可达到诱导体外细胞凋亡所需的血清浓度。一项I期研究证明了黄匹吡醇这种新型给药方案在复发、遗传高风险CLL患者中的临床活性。剂量限制性毒性为急性肿瘤溶解综合征,导致1例患者高钾血症致死。然而,黄吡醇可以在密切监测和积极干预高钾血症的情况下安全地给予,必要时包括血液透析。I期研究的首批42例患者中有19例部分缓解(45%),包括12例del(17p13)患者中的5例(42%)和18例del(11q22)患者中的13例(72%)。正在进行的II期研究正在研究改进,以优化剂量和给药计划,并尽量减少治疗相关的毒性,如短暂性中性粒细胞减少症和细胞因子释放综合征。黄匹吡醇在急性白血病、淋巴瘤和实体恶性肿瘤中的应用也在研究中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Flavopiridol in Chronic Lymphocytic Leukemia

Whereas chronic lymphocytic leukemia (CLL) responds to therapy, patients invariably experience relapse, and many patients with advanced disease acquire mutation or deletion of the p53 gene, resulting in resistance to most standard therapies. Alemtuzumab is active against p53-deficient CLL but is ineffective against bulky nodal disease and causes significant immunosuppression. Therefore, new therapies for patients with high-risk, relapsed CLL are needed. The synthetic flavone flavopiridol induces apoptosis of CLL cells in vitro, but clinical trials administering flavopiridol by 24–72–hour continuous intravenous (I.V.) infusion observed no clinical activity. Binding to human plasma proteins resulted in inadequate free flavopiridol concentrations with continuous I.V. infusion dosing schedules. Pharmacokinetic modeling indicated that administering flavopiridol by 30-minute I.V. bolus followed by 4-hour continuous I.V. infusion would achieve serum concentrations necessary to induce in vitro apoptosis. A phase I study demonstrated the clinical activity of this novel dosing regimen of flavopiridol in patients with relapsed, genetically high-risk CLL. The dose-limiting toxicity was acute tumor lysis syndrome, which resulted in fatal hyperkalemia in 1 patient. However, flavopiridol can be given safely with close monitoring and aggressive intervention for hyperkalemia, including hemodialysis if necessary. Nineteen of the first 42 patients in the phase I study had a partial response (45%), including 5 of 12 patients (42%) with del(17p13) and 13 of 18 patients (72%) with del(11q22). Ongoing phase II studies are studying modifications to optimize the dose and schedule of administration and to minimize treatment-related toxicities such as transient neutropenia and cytokine release syndrome. Flavopiridol is also being studied in acute leukemias, lymphomas, and solid malignancies.

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