2018
DOI: 10.1002/ijc.31259
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Rare missense mutations in RECQL and POLG associate with inherited predisposition to breast cancer

Abstract: Several known breast cancer susceptibility genes with moderate-to-high risk alleles encode proteins involved in DNA damage response (DDR). As these explain less than half of the hereditary breast cancer cases, additional predisposing alleles are likely to be discovered. Many of the previous studies utilizing massive parallel sequencing have focused on the protein-truncating variants, and the role of rare missense mutations has remained poorly addressed. To identify novel susceptibility factors, we have systema… Show more

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Cited by 15 publications
(8 citation statements)
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“…Maintenance of mitochondrial dNTP pools is critical for proper mtDNA function. Alterations in nuclear genes involved in transport of cytosolic dNTPs (e.g., SLC25A4), the salvage nucleotide biosynthesis in the inner mitochondrial membrane (e.g., TK2 and DGUOK), and genes involved in mtDNA replication (e.g., TWNK and POLG) are implicated in both cancer and metabolic syndromes ( 63 , 68 , 77 79 , 130 133 ). Moreover, dysfunction in the electron transport chain induces oxidative stress, which has been associated with impaired one-carbon metabolism ( 134 , 135 ), an essential anapleurotic pathway for both purine and pyrimidine nucleotides.…”
Section: Impaired Nucleotide Metabolism In Cancer and Metabolic Diseamentioning
confidence: 99%
“…Maintenance of mitochondrial dNTP pools is critical for proper mtDNA function. Alterations in nuclear genes involved in transport of cytosolic dNTPs (e.g., SLC25A4), the salvage nucleotide biosynthesis in the inner mitochondrial membrane (e.g., TK2 and DGUOK), and genes involved in mtDNA replication (e.g., TWNK and POLG) are implicated in both cancer and metabolic syndromes ( 63 , 68 , 77 79 , 130 133 ). Moreover, dysfunction in the electron transport chain induces oxidative stress, which has been associated with impaired one-carbon metabolism ( 134 , 135 ), an essential anapleurotic pathway for both purine and pyrimidine nucleotides.…”
Section: Impaired Nucleotide Metabolism In Cancer and Metabolic Diseamentioning
confidence: 99%
“…Besides well‐described mutations in AML, we found mutations in POLG , which is responsible for mitochondrial DNA replication 47 as well as mutations in MLH1 , which belongs to the DNA mismatch repair system and plays an important role in maintaining genomic stability 48–52 . Whereas both mutations were described to increase the risk of hereditary and sporadic cancers, 48,50,52,53 their incidence and clinical impact in AML are less well defined. Both mutations were not described by Ley et al ., who performed WGS or whole‐exome sequencing on 200 adult, de novo AML patients, along with RNA and microRNA sequencing and DNA‐methylation analysis 54 .…”
Section: Discussionmentioning
confidence: 88%
“…There are conflicting studies investigating germline variants in RECQL1 as a cancer susceptibility gene. Germline missense, truncating, and splice site variants in RECQL1 have been enriched in participants with breast cancer in five different ethnic groups ( Cybulski et al, 2015 ; Sun et al, 2015 ; Kwong et al, 2016 ; Sun et al, 2017 ; Tervasmaki et al, 2018 ). However, there have been a few subsequent studies with conflicting evidence, such that RECQL1 appears to be a moderate breast cancer risk gene that needs further study ( Bogdanova et al, 2017 ; Li et al, 2018a ; Nguyen-Dumont et al, 2018 ).…”
Section: Overview Of Dna Recq Helicases In Cancermentioning
confidence: 99%