Insights into clonal haematopoiesis from 8,342 mosaic chromosomal alterations

Loh, Po−Ru; Genovese, Giulio; Handsaker, Robert E.; Finucane, Hilary; Reshef, Yakir; Palamara, Pier Francesco; Birmann, Brenda M.; Talkowski, Michael E.; Bakhoum, Samuel F.; McCarroll, Steven A.; Price, Alkes L.

doi:10.1038/s41586-018-0321-x

Cited by 303 publications

(448 citation statements)

References 71 publications

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“…Recently, single-nucleotide polymorphism array analysis identified mosaic chromosomal aberrations in 7484 of 151 202 (4.9%) persons without a diagnosis of a hematologic neoplasm. 32 In the majority of these individuals, the estimated cell fraction harboring the CNA or LOH was below 5%. Small deletions frequently affected chromosomal regions 13q14, 2p (DNMT3A), and 4q (TET2).…”

Section: Beyond Gene Mutations: Detection Of Ch By Means Of Chromosmentioning

confidence: 93%

“…Besides skewed X‐chromosome inactivation and gene mutations, CH can also become evident through gross chromosomal aberrations resulting in copy number alterations (CNA) or loss of heterozygosity (LOH). Recently, single‐nucleotide polymorphism array analysis identified mosaic chromosomal aberrations in 7484 of 151 202 (4.9%) persons without a diagnosis of a hematologic neoplasm . In the majority of these individuals, the estimated cell fraction harboring the CNA or LOH was below 5%.…”

Section: Beyond Gene Mutations: Detection Of Ch By Means Of Chromosommentioning

confidence: 99%

“…31 Finally, several lines of evidence, including analyses of sibling pairs and genetic analyses, now provide evidence that there are hereditary traits leading to a predisposition to develop CH with specific genetic lesions, including TET2 mutations. 22,32,33…”

Section: Identification Of Clonal Hematopoiesismentioning

confidence: 99%

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Clonal hematopoiesis and preleukemia—Genetics, biology, and clinical implications

Hartmann

Metzeler

2019

Genes Chromosomes & Cancer

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Myeloid neoplasms including myelodysplastic syndromes and acute myeloid leukemia (AML) originate from hematopoietic stem cells through sequential acquisition of genetic and epigenetic alterations that ultimately cause the disease‐specific phenotype of impaired differentiation and increased proliferation. It has become clear that preleukemic clonal hematopoiesis (CH), characterized by an expansion of stem and progenitor cells that carry somatic mutations but are still capable of normal differentiation, can precede the development of clinically overt myeloid neoplasia by many years. CH commonly develops in the aging hematopoietic system, yet progression to myelodysplasia or AML is rare. The discovery that myeloid neoplasms frequently develop from premalignant precursor conditions that are detectable in many healthy individuals has important consequences for the diagnosis, and potentially for the treatment of these disorders. In this review, we summarize the current knowledge on CH as a precursor of myeloid cancers and the implications of CH‐related gene mutations in the diagnostic workup of patients with suspected myelodysplastic syndrome. We will discuss the risk of progression associated with CH in healthy persons and in patients undergoing chemotherapy for a non‐hematologic cancer, and the significance of CH in autologous and allogeneic stem cell transplantation. Finally, we will review the significance of preleukemic clones in AML and their persistence in patients who achieve a remission after chemotherapeutic treatment.

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Section: Beyond Gene Mutations: Detection Of Ch By Means Of Chromosmentioning

confidence: 93%

Section: Beyond Gene Mutations: Detection Of Ch By Means Of Chromosommentioning

confidence: 99%

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Clonal hematopoiesis and preleukemia—Genetics, biology, and clinical implications

Hartmann

Metzeler

2019

Genes Chromosomes & Cancer

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“…This variant was previously significantly associated with increased leukocyte telomere length. 15 This variant was also associated with myeloproliferative neoplasms (MPN, see Bao et al, co-submitted manuscript) and clonal chromosomal mosaicism 13 . In a phenome-wide association analysis (PheWAS) of rs34002450 in UK Biobank, we identified significant increased risk of MPN (p=2.6 x 10 -13 ), uterine leiomyoma (p=3.2 x 10 -9 ), brain cancer (p=3.6 x 10 -8 ) and a decreased risk of Seborrheic keratosis (p=1.4 x 10 -7 ).…”

mentioning

confidence: 98%

“…Germline genetic variants have been previously associated with clonal hematopoiesis, defined either by somatic mosaicism of SNVs and indels 12 or by chromosomal rearrangements with appreciable clonal fraction 13 , in individuals of European ancestry, and identified variants at a single locus, TERT, that associates with clonal hematopoiesis. Given the distinct association of clonal hematopoiesis with known leukemogenic mutations (i.e., CHIP) with both cancer 14 and atherosclerotic cardiovascular disease 5 , we sought to specifically discover germline genetic variations conferring increased risk for CHIP acquisition.…”

mentioning

confidence: 99%

Inherited Causes of Clonal Hematopoiesis of Indeterminate Potential in TOPMed Whole Genomes

Bick¹,

Weinstock²,

Nandakumar³

et al. 2019

Preprint

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Age is the dominant risk factor for most chronic human diseases; yet the mechanisms by which aging confers this risk are largely unknown. 1 Recently, the age-related acquisition of somatic mutations in regenerating hematopoietic stem cell populations was associated with both hematologic cancer incidence 2-4 and coronary heart disease prevalence. 5 Somatic mutations with leukemogenic potential may confer selective cellular advantages leading to clonal expansion, a phenomenon termed 'Clonal Hematopoiesis of Indeterminate Potential' (CHIP). 6 Simultaneous germline and somatic whole genome sequence analysis now provides the opportunity to identify root causes of CHIP. Here, we analyze high-coverage whole genome sequences from 97,691 participants of diverse ancestries in the NHLBI TOPMed program and identify 4,229 individuals with CHIP. We identify associations with blood cell, lipid, and inflammatory traits specific to different CHIP genes. Association of a genome-wide set of germline genetic variants identified three genetic loci associated with CHIP status, including one locus at TET2 that was African ancestry specific. In silico-informed in vitro evaluation of the TET2 germline locus identified a causal variant that disrupts a TET2 distal enhancer. Aggregates of rare germline loss-of-function variants in CHEK2, a DNA damage repair gene, predisposed to CHIP acquisition. Overall, we observe that germline genetic variation altering hematopoietic stem cell function and the fidelity of DNA-damage repair increase the likelihood of somatic mutations leading to CHIP.

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Clonal Hematopoiesis in Cancer

Rauch¹,

Steensma²

2022

Holland‐Frei Cancer Medicine

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Overview Clonal hematopoiesis represents a precursor syndrome to development of hematologic malignancy. The discovery of clonal hematopoiesis resulted from improvement in next‐generation sequencing that allows identification of low‐variant allele frequency mutations in select genes that provide hematopoietic stem cells a growth advantage over time as compared to un‐mutated stem cells. Clonal hematopoiesis results from acquisition of mutations over time in hematopoietic stem cells as individuals age. Clonal hematopoiesis is not only a risk factor for the development of hematologic malignancies but also to many other processes involving inflammation that ultimately have the potential to impact patient survival. Strategies to both utilize the presence of clonal hematopoiesis in risk assessment for cancer, cardiovascular mortality, and to potentially intervene to prevent these outcomes yet to be developed.

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Insights into clonal haematopoiesis from 8,342 mosaic chromosomal alterations

Cited by 303 publications

References 71 publications

Clonal hematopoiesis and preleukemia—Genetics, biology, and clinical implications

Clonal hematopoiesis and preleukemia—Genetics, biology, and clinical implications

Inherited Causes of Clonal Hematopoiesis of Indeterminate Potential in TOPMed Whole Genomes

Clonal Hematopoiesis in Cancer

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