RUNX1 突变与细胞遗传学正常的急性髓系白血病的年轻和老年患者的不良预后相关,并与独特的基因和 MicroRNA 表达特征相关。
RUNX1 mutations are associated with poor outcome in younger and older patients with cytogenetically normal acute myeloid leukemia and with distinct gene and MicroRNA expression signatures.
机构信息
The Ohio State University, Comprehensive Cancer Center, 1216 James Cancer Hospital, 300 West 10th Ave, Columbus, OH 43210, USA.
出版信息
J Clin Oncol. 2012 Sep 1;30(25):3109-18. doi: 10.1200/JCO.2011.40.6652. Epub 2012 Jul 2.
PURPOSE
To determine the association of RUNX1 mutations with therapeutic outcome in younger and older patients with primary cytogenetically normal acute myeloid leukemia (CN-AML) and with gene/microRNA expression signatures.
PATIENTS AND METHODS
Younger (< 60 years; n = 175) and older (≥ 60 years; n = 225) patients with CN-AML treated with intensive cytarabine/anthracycline-based first-line therapy on Cancer and Leukemia Group B protocols were centrally analyzed for RUNX1 mutations by polymerase chain reaction and direct sequencing and for established prognostic gene mutations. Gene/microRNA expression profiles were derived using microarrays.
RESULTS
RUNX1 mutations were found in 8% and 16% of younger and older patients, respectively (P = .02). They were associated with ASXL1 mutations (P < .001) and inversely associated with NPM1 (P < .001) and CEBPA (P = .06) mutations. RUNX1-mutated patients had lower complete remission rates (P = .005 in younger; P = .006 in older) and shorter disease-free survival (P = .058 in younger; P < .001 in older), overall survival (P = .003 in younger; P < .001 in older), and event-free survival (P < .001 for younger and older) than RUNX1 wild-type patients. Because RUNX1 mutations were more common in older patients and almost never coexisted with NPM1 mutations, RUNX1 mutation-associated expression signatures were derived in older, NPM1 wild-type patients and featured upregulation of genes normally expressed in primitive hematopoietic cells and B-cell progenitors, including DNTT, BAALC, BLNK, CD109, RBPMS, and FLT3, and downregulation of promoters of myelopoiesis, including CEBPA and miR-223.
CONCLUSION
RUNX1 mutations are twice as common in older than younger patients with CN-AML and negatively impact outcome in both age groups. RUNX1-mutated blasts have molecular features of primitive hematopoietic and lymphoid progenitors, potentially leading to novel therapeutic approaches.
目的
确定 RUNX1 突变与年轻和老年原发性细胞遗传学正常急性髓系白血病(CN-AML)患者治疗结果的相关性,并与基因/微 RNA 表达特征相关。
方法
根据癌症和白血病组 B 方案,对接受强化阿糖胞苷/蒽环类药物一线治疗的年轻(<60 岁;n=175)和老年(≥60 岁;n=225)CN-AML 患者进行中央 RUNX1 突变聚合酶链反应和直接测序分析,并对已建立的预后基因突变进行分析。使用微阵列获得基因/微 RNA 表达谱。
结果
年轻和老年患者的 RUNX1 突变率分别为 8%和 16%(P=0.02)。它们与 ASXL1 突变相关(P<0.001),与 NPM1(P<0.001)和 CEBPA(P=0.06)突变呈负相关。RUNX1 突变患者的完全缓解率较低(年轻患者 P=0.005;老年患者 P=0.006),无病生存期较短(年轻患者 P=0.058;老年患者 P<0.001),总生存期较短(年轻患者 P=0.003;老年患者 P<0.001),无事件生存期较短(年轻患者和老年患者均 P<0.001)。由于 RUNX1 突变在老年患者中更为常见,并且几乎从不与 NPM1 突变共存,因此在老年、NPM1 野生型患者中衍生了与 RUNX1 突变相关的表达谱,其特征为正常表达于原始造血细胞和 B 细胞前体中的基因上调,包括 DNTT、BAALC、BLNK、CD109、RBPMS 和 FLT3,以及下调髓系生成的启动子,包括 CEBPA 和 miR-223。
结论
CN-AML 患者中 RUNX1 突变在老年患者中比年轻患者常见两倍,且在两个年龄组中均对结果产生负面影响。RUNX1 突变的白血病细胞具有原始造血和淋巴祖细胞的分子特征,可能为新的治疗方法提供线索。
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