Complete morphologic response to gilteritinib in ALK-rearranged acute myeloid leukemia

IF 6.8 1区 医学 Q1 ONCOLOGY
Jacob J. Adashek, Max Brodsky, Mark J. Levis
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Abstract

The cytogenetic abnormality inv(2)(p23q13) in acute myeloid leukemia (AML) results in a fusion of RANBP2 with ALK. This fusion makes ALK constitutively active and acts as a driver for the proliferation of AML cell lines. Gilteritinib, a FLT3 inhibitor approved in AML, also can inhibit ALK among other receptor tyrosine kinases. A 75-year-old-woman with a history of essential thrombocythemia (ET) and a presumed germline DDX41 mutation developed ALK-fusion positive AML and despite standard therapies was transfusion-dependent and globally declining. The patient has been on gilteritinib with an ongoing response of more than one year with near normal blood counts and no evidence of AML. The fact that she was found to harbor a presumed germline DDX41 alteration may account for why she developed, and yet survived, two myeloid neoplasms (ET and AML). Additionally, this demonstrates that gilteritinib is clinically active as an ALK inhibitor, and could be considered for use in any AML patient presenting with an inv(2(p23q13)) translocation. Finally, it is an example of using a disease-agnostic, precision medicine approach to arrive at a beneficial treatment.

Abstract Image

Abstract Image

ALK 重排急性髓性白血病患者对吉特替尼的完全形态学反应
急性髓性白血病(AML)的细胞遗传异常 inv(2)(p23q13)导致 RANBP2 与 ALK 融合。这种融合使 ALK 具有组成性活性,并成为急性髓性白血病细胞系增殖的驱动力。吉罗替尼(Gilteritinib)是一种获准用于治疗急性髓细胞性白血病的FLT3抑制剂,它也能抑制ALK和其他受体酪氨酸激酶。一位 75 岁的女性患者曾患有原发性血小板增多症(ET),并推测存在种系 DDX41 基因突变,后来患上了 ALK 融合阳性的急性髓细胞性白血病,尽管接受了标准疗法,但仍需依赖输血,且病情全面恶化。患者使用吉特替尼治疗一年多后,血细胞计数接近正常,没有发现急性髓细胞性白血病的迹象。她被发现携带假定的种系 DDX41 基因改变,这可能是她罹患两种骨髓性肿瘤(ET 和 AML)但却存活下来的原因。此外,这表明吉特替尼作为 ALK 抑制剂具有临床活性,可考虑用于任何出现 inv(2(p23q13)) 易位的 AML 患者。最后,这也是使用疾病诊断、精准医疗方法来实现有益治疗的一个范例。
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来源期刊
CiteScore
9.90
自引率
1.30%
发文量
87
审稿时长
18 weeks
期刊介绍: Online-only and open access, npj Precision Oncology is an international, peer-reviewed journal dedicated to showcasing cutting-edge scientific research in all facets of precision oncology, spanning from fundamental science to translational applications and clinical medicine.
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