The FANC pathway and BLM collaborate during mitosis to prevent micro-nucleation and chromosome abnormalities

Naim, Valeria; Rosselli, Filippo

doi:10.1038/ncb1883

Cited by 287 publications

(376 citation statements)

References 31 publications

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“…In the absence of these proteins a nuclease activity involving Mre11 degrades the regressed fork leading to the generation of broken ends and genomic instability. Finally, FA proteins are also localized to the anaphase bridges, where they cooperate with the DNA helicase BLM in the resolution of these structures [49,50]. All of the above indicate a key role for the FA pathway in the suppression of RS and replication-borne genomic instability.…”

Section: Rs As a Fuel Of Tumorogenesismentioning

confidence: 95%

“…Additionally, they work on fork regression and restoration of chicken foot structures to normal forks that may be generated by lesions such as ICL [53]. In fact, the absence of these proteins increases genome instability as reflected by the expression of common fragile sites, along with increased sister chromatid exchanges and anaphase bridges [49,50,54]. Defects in BLM, WRN and RECQL4 cause Bloom, Werner and Rothmund-Thomson syndromes, respectively, which are associated with cancer and accelerated ageing phenotypes.…”

Section: Rs As a Fuel Of Tumorogenesismentioning

confidence: 99%

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Replication stress and cancer: It takes two to tango

Lecona

Fernández-Capetillo

2014

Experimental Cell Research

119

107

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Problems arising during DNA replication require the activation of the ATR-CHK1 pathway to ensure the stabilization and repair of the forks, and to prevent the entry into mitosis with unreplicated genomes. Whereas the pathway is essential at the cellular level, limiting its activity is particularly detrimental for some cancer cells. Here we review the links between replication stress (RS) and cancer, which provide a rationale for the use of ATR and Chk1 inhibitors in chemotherapy. First, we describe how the activation of oncogene-induced RS promotes genome rearrangements and chromosome instability, both of which could potentially fuel carcinogenesis. Next, we review the various pathways that contribute to the suppression of RS, and how mutations in these components lead to increased cancer incidence and/or accelerated ageing. Finally, we summarize the evidence showing that tumours with high levels of RS are dependent on a proficient RS-response, and therefore vulnerable to ATR or Chk1 inhibitors.

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Section: Rs As a Fuel Of Tumorogenesismentioning

confidence: 95%

Section: Rs As a Fuel Of Tumorogenesismentioning

confidence: 99%

Replication stress and cancer: It takes two to tango

Lecona

Fernández-Capetillo

2014

Experimental Cell Research

119

107

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“…17 In favor of this last hypothesis, it has been recently suggested that sister chromatid disjunction at the NPM origin is frequently incomplete in human cells, but Fanconi proteins and BLM play a cooperative role in resolving these DNA links. 9,10 However, this pathway seems to be at least partially functional in MKs, as both This abnormality corresponds to nucleoplasmic bridges (NPM), as staining with TOTO revealed the presence of DNA. Sometimes, the connection was so thin that TOTO staining was not obvious but could be observed after overexposing the images ( Fig.…”

Section: Discussionmentioning

confidence: 99%

Presence of a defect in karyokinesis during megakaryocyte endomitosis

et al. 2012

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“…treatment with the DNA polymerase inhibitor aphidicolin). The Fanconi anemia proteins, FANCI and FANCD2 associate with CFSs after replication stress and localize to the termini of FS-UFBs [8,12–14]. Finally, telomeric UFBs (T-UFBs) can be induced by interfering with the replication of telomeres or by overexpression of the shelterin component TRF2 that induces chromosome end-to-end fusions [15–17].…”

Section: Introductionmentioning

confidence: 99%

A new class of ultrafine anaphase bridges generated by homologous recombination

Chan

West

2018

Cell Cycle

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Ultrafine anaphase bridges (UFBs) are a potential source of genome instability that is a hallmark of cancer. UFBs can arise from DNA catenanes at centromeres/rDNA loci, late replication intermediates induced by replication stress, and DNA linkages at telomeres. Recently, it was reported that DNA intertwinements generated by homologous recombination give rise to a new class of UFBs, which have been termed homologous recombination ultrafine bridges (HR-UFBs). HR-UFBs are decorated with PICH and BLM in anaphase, and are subsequently converted to RPA-coated, single-stranded DNA bridges. Breakage of these sister chromatid entanglements leads to DNA damage that can be repaired by non-homologous end joining in the next cell cycle, but the potential consequences include DNA rearrangements, chromosome translocations and fusions. Visualisation of these HR-UFBs, and knowledge of how they arise, provides a molecular basis to explain how upregulation of homologous recombination or failure to resolve recombination intermediates leads to the development of chromosomal instability observed in certain cancers.

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The FANC pathway and BLM collaborate during mitosis to prevent micro-nucleation and chromosome abnormalities

Cited by 287 publications

References 31 publications

Replication stress and cancer: It takes two to tango

Replication stress and cancer: It takes two to tango

Presence of a defect in karyokinesis during megakaryocyte endomitosis

A new class of ultrafine anaphase bridges generated by homologous recombination

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