用罗匹干扰素 Alfa-2b 治疗有效控制多发性红细胞症

IF 1.3 Q4 HEMATOLOGY

Journal of hematology Pub Date : 2024-04-01 DOI:10.14740/jh1245

Shan Shan Suo, Rong Feng Fu, A. Qin, Z. H. Shao, Jie Bai, Su Ning Chen, M. Duan, Hu Zhou, Na Xu, Sumei Zhang, Xue Lan Zuo, Xin Du, Li Wang, Pei Li, Xu Han Zhang, Daoxiang Wu, Y. Li, Jing Jing Zhang, Wei Wang, Weihong Shen, O. Zagrijtschuk, Toshiaki Sato, Zhi Jian Xiao, Jie Jin

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Methods Forty-nine patients with PV having HU intolerance from major hospitals in China were treated biweekly with an initial dose of 250 µg, followed by 350 µg and 500 µg thereafter if tolerated. Complete hematological response (CHR) was assessed every 12 weeks based on the European LeukemiaNet criteria. The primary endpoint was the CHR rate at week 24. The secondary endpoints included CHR rates at weeks 12, 36 and 52, changes of JAK2V617F allelic burden, time to first CHR, and safety assessments. Results The CHR rates were 61.2%, 69.4% and 71.4% at weeks 24, 36, and 52, respectively. Mean allele burden of the driver mutation JAK2V617F declined from 58.5% at baseline to 30.1% at 52 weeks. Both CHR and JAK2V617F allele burden reduction showed consistent increases over the 52 weeks of the treatment. Twenty-nine patients (63.0%) achieved partial molecular response (PMR) and two achieved complete molecular response (CMR). The time to CHR was rapid and median time was 5.6 months according to central lab results. The CHRs were durable and median CHR duration time was not reached at week 52. Mean spleen index reduced from 55.6 cm2 at baseline to 50.2 cm2 at week 52. Adverse events (AEs) were mostly mild or moderate. Most common AEs were reversible alanine aminotransferase and aspartate aminotransferase increases, which were not associated with significant elevations in bilirubin levels or jaundice. There were no grade 4 or 5 AEs. Grade 3 AEs were reversible and manageable. Only one AE led to discontinuation. No incidence of thromboembolic events was observed. Conclusion The 250-350-500 µg dosing regimen was well tolerated and effectively induced CHR and MR and managed spleen size increase. 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引用次数: 0

摘要

背景多发性红细胞增多症（PV）是一种骨髓增生性肿瘤。罗匹干扰素 alfa-2b 是一种新一代聚乙二醇结合的脯氨酸干扰素。它被批准用于治疗骨髓增生性肿瘤，起始剂量为100微克（接受羟基脲（HU）治疗的患者为50微克），剂量滴定最高为500微克，每50微克递增一次。该研究旨在评估其在更高起始剂量和更简单的患者剂量递增情况下的疗效和安全性。方法对来自中国各大医院的 49 名不耐受 HU 的 PV 患者进行双周治疗，初始剂量为 250 µg，如患者耐受，随后剂量分别为 350 µg 和 500 µg。根据欧洲白血病网络标准，每12周评估一次完全血液学反应（CHR）。主要终点是第24周时的CHR率。次要终点包括第12、36和52周的CHR率、JAK2V617F等位基因负荷的变化、首次CHR的时间以及安全性评估。结果第24、36和52周的CHR率分别为61.2%、69.4%和71.4%。驱动突变JAK2V617F的平均等位基因负荷从基线时的58.5%降至52周时的30.1%。在52周的治疗过程中，CHR和JAK2V617F等位基因负荷的下降均呈现出持续增长的趋势。29名患者（63.0%）获得了部分分子反应（PMR），2名患者获得了完全分子反应（CMR）。根据中心实验室的结果，CHR的发生时间很快，中位时间为5.6个月。CHR是持久的，中位CHR持续时间在第52周时尚未达到。平均脾脏指数从基线时的 55.6 平方厘米降至第 52 周时的 50.2 平方厘米。不良反应（AEs）大多为轻度或中度。最常见的不良反应是可逆性丙氨酸氨基转移酶和天门冬氨酸氨基转移酶升高，与胆红素水平或黄疸的显著升高无关。没有出现 4 级或 5 级 AE。3级不良反应是可逆和可控的。只有 1 例 AE 导致停药。未观察到血栓栓塞事件。结论 250-350-500 µg 给药方案耐受性良好，能有效诱导 CHR 和 MR，并控制脾脏增大。我们的研究结果表明，采用这种给药方案的索干扰素 alfa-2b 可以有效治疗 PV，并支持将这种给药方案作为一种治疗选择。

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Effective Management of Polycythemia Vera With Ropeginterferon Alfa-2b Treatment

Background Polycythemia vera (PV) is a myeloproliferative neoplasm. Ropeginterferon alfa-2b is a new-generation polyethylene glycol-conjugated proline-interferon. It is approved for the treatment of PV at a starting dose of 100 µg (50 µg for patients receiving hydroxyurea (HU)) and dose titrations up to 500 µg by 50 µg increments. The study was aimed at assessing its efficacy and safety at a higher starting dose and simpler intra-patient dose escalation. Methods Forty-nine patients with PV having HU intolerance from major hospitals in China were treated biweekly with an initial dose of 250 µg, followed by 350 µg and 500 µg thereafter if tolerated. Complete hematological response (CHR) was assessed every 12 weeks based on the European LeukemiaNet criteria. The primary endpoint was the CHR rate at week 24. The secondary endpoints included CHR rates at weeks 12, 36 and 52, changes of JAK2V617F allelic burden, time to first CHR, and safety assessments. Results The CHR rates were 61.2%, 69.4% and 71.4% at weeks 24, 36, and 52, respectively. Mean allele burden of the driver mutation JAK2V617F declined from 58.5% at baseline to 30.1% at 52 weeks. Both CHR and JAK2V617F allele burden reduction showed consistent increases over the 52 weeks of the treatment. Twenty-nine patients (63.0%) achieved partial molecular response (PMR) and two achieved complete molecular response (CMR). The time to CHR was rapid and median time was 5.6 months according to central lab results. The CHRs were durable and median CHR duration time was not reached at week 52. Mean spleen index reduced from 55.6 cm2 at baseline to 50.2 cm2 at week 52. Adverse events (AEs) were mostly mild or moderate. Most common AEs were reversible alanine aminotransferase and aspartate aminotransferase increases, which were not associated with significant elevations in bilirubin levels or jaundice. There were no grade 4 or 5 AEs. Grade 3 AEs were reversible and manageable. Only one AE led to discontinuation. No incidence of thromboembolic events was observed. Conclusion The 250-350-500 µg dosing regimen was well tolerated and effectively induced CHR and MR and managed spleen size increase. Our findings demonstrate that ropeginterferon alfa-2b at this dosing regimen can provide an effective management of PV and support using this dosing regimen as a treatment option.

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Journal of hematology HEMATOLOGY-

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