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慢性骨髓纤维化相非 JAK 抑制剂的研究。

Investigational non-JAK inhibitors for chronic phase myelofibrosis.

机构信息

Medical Oncology and Hematology, Princess Margaret Cancer Center , Toronto, Ontario, Canada.

出版信息

Expert Opin Investig Drugs. 2020 May;29(5):461-474. doi: 10.1080/13543784.2020.1751121. Epub 2020 Apr 29.

DOI:10.1080/13543784.2020.1751121
PMID:32245330
Abstract

INTRODUCTION

Patients with myelofibrosis (MF) have no effective treatment option after the failure of approved JAK inhibitor (JAKi) therapy. Non-JAK inhibitors (non-JAKi) that target non-canonical molecular pathways are undergoing clinical evaluations to optimize efficacy and/or to reduce hematological toxicity of JAKi.

AREA COVERED

This article reviews the efficacy data from completed and ongoing early phase clinical trials of non-JAKi agents for chronic phase MF. The article also illuminates some of the challenges of myelofibrosis drug development.

EXPERT OPINION

Most non-JAKi agents tested so far have shown modest benefit in improving the efficacy of ruxolitinib. Several novel agents such as BET inhibitor- CPI-0610, activin receptor ligand trap- luspatercept, recombinant pentraxin-PRM-151, telomerase inhibitor- imetelstat and bcl-2 inhibitor- navitoclax, have shown promising activity; however, they require vigorous evaluation in randomized controlled trials to understand the clinical benefit. Drugs that target new molecular pathways (MDM2, p-selectin, TIM-3, TGF-β, aurora kinase) and immune-based strategies (CALR vaccine, anti-PD-1, allogeneic cord blood regulatory T cells) are in early phase trials. Further translational studies to target leukemic stem cells, improvement in trial designs by incorporating control arm and survival endpoints, and patient-focused collaborations among all stakeholders could pave a way for future success in MF drug development.

摘要

简介

接受 JAK 抑制剂(JAKi)治疗失败后的骨髓纤维化(MF)患者,目前尚无有效的治疗方案。目前正在进行临床试验评估,以评估非 JAK 抑制剂(non-JAKi)针对非经典分子通路的疗效,旨在优化疗效和/或降低 JAKi 的血液学毒性。

涵盖领域

本文综述了已完成和正在进行的非 JAKi 药物治疗慢性期 MF 的早期临床试验的疗效数据。本文还阐明了 MF 药物开发面临的一些挑战。

专家意见

迄今为止,大多数已测试的非 JAKi 药物在改善 ruxolitinib 的疗效方面显示出适度的益处。几种新型药物,如 BET 抑制剂-CPI-0610、激活素受体配体陷阱-luspatercept、重组 pentraxin-PRM-151、端粒酶抑制剂-imetelstat 和 bcl-2 抑制剂-navitoclax,已显示出有希望的活性;然而,它们需要在随机对照试验中进行强有力的评估,以了解临床获益。靶向新分子通路(MDM2、p-选择素、TIM-3、TGF-β、极光激酶)和免疫策略(CALR 疫苗、抗 PD-1、同种异体脐带血调节性 T 细胞)的药物正在早期临床试验中。进一步的转化研究旨在靶向白血病干细胞,通过纳入对照臂和生存终点来改进试验设计,以及所有利益相关者之间以患者为中心的合作,可能为 MF 药物开发的未来成功铺平道路。

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