2021
DOI: 10.1093/narcan/zcaa043
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The HelQ human DNA repair helicase utilizes a PWI-like domain for DNA loading through interaction with RPA, triggering DNA unwinding by the HelQ helicase core

Abstract: Genome instability is a characteristic enabling factor for carcinogenesis. HelQ helicase is a component of human DNA maintenance systems that prevent or reverse genome instability arising during DNA replication. Here, we provide details of the molecular mechanisms that underpin HelQ function—its recruitment onto ssDNA through interaction with replication protein A (RPA), and subsequent translocation of HelQ along ssDNA. We describe for the first time a functional role for the non-catalytic N-terminal region of… Show more

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Cited by 19 publications
(42 citation statements)
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References 72 publications
(83 reference statements)
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“…Roopesh Anand 1,6 , Erika Buechelmaier 2,3,6 , Ondrej Belan 1 , Matthew Newton 1 , Aleksandra Vancevska 1 , Artur Kaczmarczyk 4,5 , Tohru Takaki 1 , David S. Rueda 4,5 ✉ , Simon N. Powell 2 ✉ & Simon J. Boulton 1 ✉ DNA double-stranded breaks (DSBs) are deleterious lesions, and their incorrect repair can drive cancer development 1 . HELQ is a superfamily 2 helicase with 3′ to 5′ polarity, and its disruption in mice confers germ cells loss, infertility and increased predisposition to ovarian and pituitary tumours [2][3][4] .…”
Section: Helq Is a Dual-function Dsb Repair Enzyme Modulated By Rpa And Rad51mentioning
confidence: 99%
See 1 more Smart Citation
“…Roopesh Anand 1,6 , Erika Buechelmaier 2,3,6 , Ondrej Belan 1 , Matthew Newton 1 , Aleksandra Vancevska 1 , Artur Kaczmarczyk 4,5 , Tohru Takaki 1 , David S. Rueda 4,5 ✉ , Simon N. Powell 2 ✉ & Simon J. Boulton 1 ✉ DNA double-stranded breaks (DSBs) are deleterious lesions, and their incorrect repair can drive cancer development 1 . HELQ is a superfamily 2 helicase with 3′ to 5′ polarity, and its disruption in mice confers germ cells loss, infertility and increased predisposition to ovarian and pituitary tumours [2][3][4] .…”
Section: Helq Is a Dual-function Dsb Repair Enzyme Modulated By Rpa And Rad51mentioning
confidence: 99%
“…At the cellular level, defects in HELQ result in hypersensitivity to cisplatin and mitomycin C, and persistence of RAD51 foci after DNA damage 3 , 5 . Notably, HELQ binds to RPA and the RAD51-paralogue BCDX2 complex, but the relevance of these interactions and how HELQ functions in DSB repair remains unclear 3 , 5 , 6 . Here we show that HELQ helicase activity and a previously unappreciated DNA strand annealing function are differentially regulated by RPA and RAD51.…”
mentioning
confidence: 99%
“…The mechanism by which HELQ makes ssDNA available for base-pairing interactions is currently unknown, but primarily because of recent in vitro work we favour a function in removing potentially annealing-interfering ssDNA binding proteins such as RPA or RAD51. HELQ, purified from an archaeal or human source, was found to interact with RPA and able to modulate the RPA-DNA binding including its displacement from ssDNA 57 , 58 ; C. elegans HELQ-1 was shown to promote the disassembly of RAD51 from DNA in vitro 47 . Also, the helicase domain in POLQ, which is highly similar to HELQ, was capable of removing RPA from resected DSB ends in vitro to allow their annealing 37 .…”
Section: Discussionmentioning
confidence: 99%
“…Purified ATPase proficient HELQ protein unwinds model replication fork substrates in vitro [ 49 ] without any of the issues surrounding the low specific activity of the pol θ N-terminal ATPase construct. Additional experimentation will be necessary to clarify why the pol θ ATPase lacks the strong enzymatic activity of HELQ [ 50 ], or the archaeal homolog HEL308, which can break the biotin–streptavidin interaction due to tenacious helicase and protein-stripping functions [ 51 ].…”
Section: Enzymatic Activities Coordinated By Pol θmentioning
confidence: 99%
“…Dimerization is often observed for DNA repair enzymes able to synapse DSBs, such as DNA-PK or LIG4, but functional tetramerization aligns more with helicases catalyzing branch migration of 4-way DNA junctions [ 52 ]. Like the pol θ ATPase, HELQ was also shown to exist in solution as a tetramer by SEC-MALS, but emerging evidence implies that active complexes of the HELQ could exist as dimers, hinting that the tetrameric form might serve a regulatory purpose [ 50 ]. Identifying the functional biological assembly assumed by the pol θ ATPase domain in cells warrants further analysis.…”
Section: Structures Of Template-dependent Dna Polymerase and The Dna-dependent Atpasementioning
confidence: 99%