Blood：口服MDM2蛋白拮抗剂Idasanutlin用于真性红细胞增多症的疗效评估

2019-06-06 QQ MedSci原创

治疗真性红细胞增多症(PV)和原发性血小板增多症（ET）的药物数量有限。John Mascarenhas等研究人员尝试寻找可靶向恶性造血干细胞/祖细胞 (HSC/HPC)的替代药物。已有研究表明MDM2蛋白在PV/ET CD34+细胞中的表达水平上调，暴露于MDM2拮抗剂nutlin中，可诱导激活TP53信号通路，选择性耗竭PV HPC/HSCs。这种抗克隆活性由p53上调介导，并可通过添加干扰素

中心点：

MDM2在PV患者中的表达水平升高，为MDM2拮抗剂药物干预的治疗靶点。

MDM2拮抗剂idasanutlin，用于PV患者耐受性良好，表现出靶向p53激活和临床活性。

摘要：

治疗真性红细胞增多症(PV)和原发性血小板增多症（ET）的药物数量有限。John Mascarenhas等研究人员尝试寻找可靶向恶性造血干细胞/祖细胞 (HSC/HPC)的替代药物。

已有研究表明MDM2蛋白在PV/ET CD34+细胞中的表达水平上调，暴露于MDM2拮抗剂nutlin中，可诱导激活TP53信号通路，选择性耗竭PV HPC/HSCs。这种抗克隆活性由p53上调介导，并可通过添加干扰素-α-2a而增强。

因此，John等人开展一1期试验，研究口服MDM2拮抗剂 idasanutlin用于既往治疗失败的高危型PV/ET患者的疗效和安全性。招募了13位携带JAK2V617F阳性的PV/ET患者，其中12位（11位PV患者、1位ET患者）接受idasanutlin治疗，100mg/日或150mg/日，连续服用5天，28天一疗程。

Idasanutlin的安全性良好，试验期间未观察到剂量限制性毒性，但常见低级别的胃肠毒性。idasanutlin单药治疗6个疗程后，总体缓解率为58%（7/12），与其他药物联合治疗的总体缓解率为50%（2/4）。缓解持续的中位时间位16.8个月（3.5-26.7）。患者血液学、症状、病理性和分子缓解均有获得。

综上所述，本研究表明idasanutlin是一种有望用于PV的新药物，目前关于idasanutlin的全球2期试验正在进行中。

原始出处：

John Mascarenhas， et al. Oral Idasanutlin in Patients with Polycythemia Vera. Blood 2019 ：blood.2018893545； doi： https：//doi.org/10.1182/blood.2018893545

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2020-02-18 wangyang7970

#MDM2#

89 0
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2019-07-28 lvygwyt2781

#ASA#

88 0
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2020-02-12 zxxiang

#疗效评估#

59 0
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2020-02-16 仁心济世

#Idasanutlin#

119 0
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2019-06-08 kord1982

#红细胞#

70 0
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2019-06-08 ms5236388012055669

#拮抗剂#

77 0
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2019-06-08 linlin2317

#红细胞增多症#

81 0
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2019-06-06 内科新手

谢谢梅斯提供这么好的信息，学到很多

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