Department of Pediatrics, Division of Hematology and Oncology, Washington University School of Medicine, Saint Louis, MO.
Center for Genome Sciences and Systems Biology, Washington University School of Medicine, Saint Louis, MO.
Haematologica. 2019 Dec;104(12):2410-2417. doi: 10.3324/haematol.2018.215269. Epub 2019 Apr 19.
Nearly all adults harbor acute myeloid leukemia (AML)-related clonal hematopoietic mutations at a variant allele fraction (VAF) of ≥0.0001, yet relatively few develop hematologic malignancies. We conducted a nested analysis in the Nurses' Health Study and Health Professionals Follow-Up Study blood subcohorts, with up to 22 years of follow up to investigate associations of clonal mutations of ≥0.0001 allele frequency with future risk of AML. We identified 35 cases with AML that had pre-diagnosis peripheral blood samples and matched two controls without history of cancer per case by sex, age, and ethnicity. We conducted blinded error-corrected sequencing on all study samples and assessed variant-associated risk using conditional logistic regression. We detected AML-associated mutations in 97% of all participants (598 mutations, 5.8/person). Individuals with mutations ≥0.01 variant allele fraction had a significantly increased AML risk (OR 5.4, 95%CI: 1.8-16.6), as did individuals with higher-frequency clones and those with R882H/C mutations. The risk of lower-frequency clones was less clear. In the 11 case-control sets with samples banked ten years apart, clonal mutations rarely expanded over time. Our findings are consistent with published evidence that detection of clonal mutations ≥0.01 VAF identifies individuals at increased risk for AML. Further study of larger populations, mutations co-occurring within the same pre-leukemic clone and other risk factors (lifestyle, epigenetics, etc.), are still needed to fully elucidate the risk conferred by low-frequency clonal hematopoiesis in asymptomatic adults.
几乎所有成年人的造血细胞中都存在着急性髓系白血病(AML)相关的克隆性突变,其等位基因变异分数(VAF)≥0.0001,但只有相对较少的人会发展为血液系统恶性肿瘤。我们对护士健康研究和健康专业人员随访研究的血液子队列进行了一项嵌套分析,随访时间长达 22 年,以研究等位基因频率≥0.0001 的克隆突变与未来 AML 风险之间的关联。我们在诊断前外周血样本中鉴定了 35 例 AML 病例,并按性别、年龄和种族与每个病例匹配了两名无癌症病史的对照者。我们对所有研究样本进行了盲法纠错测序,并使用条件逻辑回归评估了与变异相关的风险。我们在所有参与者中检测到 97%的 AML 相关突变(598 个突变,5.8/人)。突变等位基因分数≥0.01 的个体 AML 风险显著增加(OR 5.4,95%CI:1.8-16.6),高频克隆和 R882H/C 突变的个体也是如此。低频克隆的风险则不太明确。在 11 个病例对照样本组中,样本相隔十年保存,克隆突变很少随时间扩展。我们的研究结果与已发表的证据一致,即检测到等位基因变异分数≥0.01 的克隆突变可识别出 AML 风险增加的个体。进一步对更大人群、同一白血病前克隆内共同发生的突变以及其他风险因素(生活方式、表观遗传学等)进行研究,仍然需要充分阐明无症状成年人中低频克隆性造血所带来的风险。
