[Novel treatment strategies for polycythemia vera: focus on ropeginterferon alfa-2b].

Keita Kirito
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Abstract

The current main treatment goal of polycythemia vera (PV) is preventing thromboembolic and hemorrhagic complications. However, these therapeutic strategies cannot delay progression of PV. Therefore, there is an unmet need for next-generation therapeutic strategies to slow disease progression and improve survival in patients with PV. One of the most promising agents for modifying the disease course of myeloproliferative neoplasms is interferon alpha, which has been used to treat PV since the 1980s. Notably, it achieved cytogenetic or molecular responses in some patients. However, conventional interferon was not widely used due to its high incidence of adverse events and poor tolerance. Ropeginterferon alfa-2b (ropeg) is a unique, site-selective polyethylene glycol-conjugated form of recombinant interferon alpha. A phase 1/2 study of ropeg for PV patients showed low toxicity and improved tolerability, along with significant molecular response. A phase 3 randomized study (PROUD-PV/CONTINUATION-PV) revealed that treatment with ropeg continuously decreased the JAK2V617F allele burden compared to hydroxyurea and improved event-free survival (with events defined as thromboembolic events, disease progression, or death). A phase 2 study in Japanese patients with PV further confirmed the efficacy of ropeg.

真性红细胞增多症的新治疗策略:关注ropeg干扰素α -2b。
真性红细胞增多症(PV)目前的主要治疗目标是预防血栓栓塞和出血性并发症。然而,这些治疗策略不能延缓PV的进展。因此,对下一代治疗策略的需求尚未得到满足,以减缓PV患者的疾病进展并提高其生存率。干扰素是最有希望改变骨髓增殖性肿瘤病程的药物之一,自20世纪80年代以来一直用于治疗PV。值得注意的是,它在一些患者中取得了细胞遗传学或分子反应。然而,常规干扰素因其不良事件发生率高、耐受性差而未得到广泛应用。ropeg干扰素α -2b (ropeg)是一种独特的、位点选择性的聚乙二醇偶联形式的重组干扰素α。ropeg用于PV患者的1/2期研究显示其毒性低,耐受性提高,分子反应显著。一项3期随机研究(PROUD-PV/ continue - pv)显示,与羟基脲相比,ropeg治疗可持续降低JAK2V617F等位基因负担,并改善无事件生存(事件定义为血栓栓塞事件、疾病进展或死亡)。一项针对日本PV患者的2期研究进一步证实了ropeg的疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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