A practical approach to curate clonal hematopoiesis of indeterminate potential in human genetic datasets

外显子组 外显子组测序 生物 人口 遗传学 生命银行 DNA微阵列 生殖系 计算生物学 医学 突变 基因 环境卫生 基因表达
作者
Caitlyn Vlasschaert,Taralynn Mack,J. Brett Heimlich,Abhishek Niroula,Md Mesbah Uddin,Joshua S. Weinstock,Brian Sharber,Alexander J. Silver,Yaomin Xu,Michael R. Savona,Christopher J. Gibson,Matthew B. Lanktree,Michael J. Rauh,Benjamin L. Ebert,Pradeep Natarajan,Siddhartha Jaiswal,Alexander G. Bick
出处
期刊:Blood [Elsevier BV]
卷期号:141 (18): 2214-2223 被引量:135
标识
DOI:10.1182/blood.2022018825
摘要

Clonal hematopoiesis of indeterminate potential (CHIP) is a common form of age-related somatic mosaicism that is associated with significant morbidity and mortality. CHIP mutations can be identified in peripheral blood samples that are sequenced using approaches that cover the whole genome, the whole exome, or targeted genetic regions; however, differentiating true CHIP mutations from sequencing artifacts and germ line variants is a considerable bioinformatic challenge. We present a stepwise method that combines filtering based on sequencing metrics, variant annotation, and population-based associations to increase the accuracy of CHIP calls. We apply this approach to ascertain CHIP in ∼550 000 individuals in the UK Biobank complete whole exome cohort and the All of Us Research Program initial whole genome release cohort. CHIP ascertainment on this scale unmasks recurrent artifactual variants and highlights the importance of specialized filtering approaches for several genes, including TET2 and ASXL1. We show how small changes in filtering parameters can considerably increase CHIP misclassification and reduce the effect size of epidemiological associations. Our high-fidelity call set refines previous population-based associations of CHIP with incident outcomes. For example, the annualized incidence of myeloid malignancy in individuals with small CHIP clones is 0.03% per year, which increases to 0.5% per year among individuals with very large CHIP clones. We also find a significantly lower prevalence of CHIP in individuals of self-reported Latino or Hispanic ethnicity in All of Us, highlighting the importance of including diverse populations. The standardization of CHIP calling will increase the fidelity of CHIP epidemiological work and is required for clinical CHIP diagnostic assays.
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