The allosteric inhibitor ABL001 enables dual targeting of BCR–ABL1

伊马替尼 变构调节 医学 阿布勒 甲磺酸伊马替尼 药理学 癌症研究 化学 髓系白血病 酪氨酸激酶 信号转导 生物化学
作者
Andrew A. Wylie,Joseph Schoepfer,Wolfgang Jahnke,Sandra W. Cowan‐Jacob,Alice Loo,Pascal Furet,Andreas L. Marzinzik,Xavier Pellé,Jerry Donovan,Wenjing Zhu,Silvia Buonamici,Amr Hassan,Franco Lombardo,Varsha Iyer,Michael R. Palmer,Giuliano Berellini,Stephanie Dodd,Sanjeev Thohan,Hans Bitter,Susan Branford
出处
期刊:Nature [Nature Portfolio]
卷期号:543 (7647): 733-737 被引量:589
标识
DOI:10.1038/nature21702
摘要

The selective allosteric ABL1 inhibitor ABL001 (asciminib) represents a new inhibitory mechanism for BCR–ABL1-driven malignancies, and its efficacy and evolving mechanisms of resistance do not overlap with those of other BCR–ABL1 kinase inhibitors. Current inhibitors targeting the BCR–ABL1 mutation have saved many lives but their application is limited by resistance-driving mutations. Here, the authors report the characterization of ABL001, a new allosteric ABL inhibitor. The compound represents a new inhibitory enzymatic mechanism for BCR–ABL-driven malignancies and could be applied for cases of resistance. The authors note that its efficacy and evolving mechanisms of resistance do not overlap with other BCR–ABL kinase inhibitors. Chronic myeloid leukaemia (CML) is driven by the activity of the BCR–ABL1 fusion oncoprotein. ABL1 kinase inhibitors have improved the clinical outcomes for patients with CML, with over 80% of patients treated with imatinib surviving for more than 10 years1. Second-generation ABL1 kinase inhibitors induce more potent molecular responses in both previously untreated and imatinib-resistant patients with CML2. Studies in patients with chronic-phase CML have shown that around 50% of patients who achieve and maintain undetectable BCR–ABL1 transcript levels for at least 2 years remain disease-free after the withdrawal of treatment3,4. Here we characterize ABL001 (asciminib), a potent and selective allosteric ABL1 inhibitor that is undergoing clinical development testing in patients with CML and Philadelphia chromosome-positive (Ph+) acute lymphoblastic leukaemia. In contrast to catalytic-site ABL1 kinase inhibitors, ABL001 binds to the myristoyl pocket of ABL1 and induces the formation of an inactive kinase conformation. ABL001 and second-generation catalytic inhibitors have similar cellular potencies but distinct patterns of resistance mutations, with genetic barcoding studies revealing pre-existing clonal populations with no shared resistance between ABL001 and the catalytic inhibitor nilotinib. Consistent with this profile, acquired resistance was observed with single-agent therapy in mice; however, the combination of ABL001 and nilotinib led to complete disease control and eradicated CML xenograft tumours without recurrence after the cessation of treatment.
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