Congenital Diseases of DNA Replication: Clinical Phenotypes and Molecular Mechanisms

Schmit, Megan; Bielinsky, Anja‐Katrin

doi:10.3390/ijms22020911

Cited by 24 publications

(14 citation statements)

References 210 publications

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“…Because genome-instability is a hallmark of cancer, the findings described here support a previously proposed model that WASp functions within the “tumor-suppressor” apparatus in normal lymphocytes 49 , and that its loss triggers replication dysfunction and genome-instability contributing to oncogenesis in WAS. Notably, immunodeficiencies frequently occur in certain congenital diseases arising from mutations in essential replication genes 50 . In this connection, multiple WAS mutations/ variants (p.D485G; p.E486K; p.D489N; p.D493N; p.D497E; pD497Y) are reported in the public WAS-databases that occur in/or around RBM1, which could potentially disrupt RPA1-activity directly.…”

Section: Discussionmentioning

confidence: 99%

WASp modulates RPA function on single-stranded DNA in response to replication stress and DNA damage

et al. 2022

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Perturbation in the replication-stress response (RSR) and DNA-damage response (DDR) causes genomic instability. Genomic instability occurs in Wiskott-Aldrich syndrome (WAS), a primary immunodeficiency disorder, yet the mechanism remains largely uncharacterized. Replication protein A (RPA), a single-strand DNA (ssDNA) binding protein, has key roles in the RSR and DDR. Here we show that human WAS-protein (WASp) modulates RPA functions at perturbed replication forks (RFs). Following genotoxic insult, WASp accumulates at RFs, associates with RPA, and promotes RPA:ssDNA complexation. WASp deficiency in human lymphocytes destabilizes RPA:ssDNA-complexes, impairs accumulation of RPA, ATR, ETAA1, and TOPBP1 at genotoxin-perturbed RFs, decreases CHK1 activation, and provokes global RF dysfunction. las17 (yeast WAS-homolog)-deficient S. cerevisiae also show decreased ScRPA accumulation at perturbed RFs, impaired DNA recombination, and increased frequency of DNA double-strand break (DSB)-induced single-strand annealing (SSA). Consequently, WASp (or Las17)-deficient cells show increased frequency of DSBs upon genotoxic insult. Our study reveals an evolutionarily conserved, essential role of WASp in the DNA stress-resolution pathway, such that WASp deficiency provokes RPA dysfunction-coupled genomic instability.

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Section: Discussionmentioning

confidence: 99%

WASp modulates RPA function on single-stranded DNA in response to replication stress and DNA damage

et al. 2022

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“…The region encompasses three candidate genes involved in pharyngeal arches development, including HIC2, YPEL1, and MAPK1. However, the typical auricular phenotype in these patients is preauricular tags but not microtia (Schmit & Bielinsky, 2021). One OAVS patient with central 22q11.2 deletion between LCR22B-D was reported.…”

Section: Discussionmentioning

confidence: 98%

“…The loss of cell division cycle 45 gene (CDC45, MIM *603465) embedded in 22q11.2 has been reported to be related to craniofacial malformations, as in Meier-Gorlin syndrome and craniosynostosis (Miller et al, 2017;Parker et al, 2018). As one of the components in replicative helicase Cdc45-MCM2-7-GINS (CMG), CDC45 functions in DNA replication which is crucial in many developmental processes (Schmit & Bielinsky, 2021;Tognetti et al, 2015). We therefore speculate that the loss of CDC45 on 22q11.2 is an important causal mutation for ear malformation.…”

Section: Introductionmentioning

confidence: 99%

De novo 22q11.2 deletions and auricular findings in two Chinese patients with microtia

Zhang

Huang

et al. 2021

Molec Gen & Gen Med

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“…Nevertheless, it is widely accepted that acquisition and sustenance of an infinite replicative potential are key factors for carcinogenesis. Retarded growth potential of human cells deficient in BLM, WRN, and RecQL4 gave a general indication that RecQ helicases participate in DNA replication [Bennett and Keck, 2004;Burla et al, 2018;Schmit and Bielinsky, 2021]. Since this review is focused on RecQL4, much of the discussion is confined only to RecQL4 and its associated activities in DNA replication.…”

Section: Sustained Proliferation Capacity In Recql4 Overexpressing Cancer Cellsmentioning

confidence: 99%

Human RecQL4 as a Novel Molecular Target for Cancer Therapy

Balajee¹

2021

Cytogenet Genome Res

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Human RecQ helicases play diverse roles in the maintenance of genomic stability. Inactivating mutations in 3 of the 5 human RecQ helicases are responsible for the pathogenesis of Werner syndrome (WS), Bloom syndrome (BS), Rothmund-Thomson syndrome (RTS), RAPADILINO, and Baller-Gerold syndrome (BGS). WS, BS, and RTS patients are at increased risk for developing many age-associated diseases including cancer. Mutations in RecQL1 and RecQL5 have not yet been associated with any human diseases so far. In terms of disease outcome, RecQL4 deserves special attention because mutations in RecQL4 result in 3 autosomal recessive syndromes (RTS type II, RAPADILINO, and BGS). RecQL4, like other human RecQ helicases, has been demonstrated to play a crucial role in the maintenance of genomic stability through participation in diverse DNA metabolic activities. Increased incidence of osteosarcoma in RecQL4-mutated RTS patients and elevated expression of RecQL4 in sporadic cancers including osteosarcoma suggest that loss or gain of RecQL4 expression is linked with cancer susceptibility. In this review, current and future perspectives are discussed on the potential use of RecQL4 as a novel cancer therapeutic target.

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Congenital Diseases of DNA Replication: Clinical Phenotypes and Molecular Mechanisms

Cited by 24 publications

References 210 publications

WASp modulates RPA function on single-stranded DNA in response to replication stress and DNA damage

WASp modulates RPA function on single-stranded DNA in response to replication stress and DNA damage

De novo 22q11.2 deletions and auricular findings in two Chinese patients with microtia

Human RecQL4 as a Novel Molecular Target for Cancer Therapy

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