Your search keyword '"DNA Helicases metabolism"' showing total 286 results

1. The ARK2N-CK2 complex initiates transcription-coupled repair through enhancing the interaction of CSB with lesion-stalled RNAPII.

Author

Luo Y, Li J, Li X, Lin H, Mao Z, Xu Z, Li S, Nie C, Zhou XA, Liao J, Xiong Y, Xu X, and Wang J

Subjects

Humans, Animals, Mice, Transcription, Genetic, Phosphorylation, Casein Kinase II metabolism, Casein Kinase II genetics, Mice, Knockout, DNA Damage, ATPases Associated with Diverse Cellular Activities metabolism, ATPases Associated with Diverse Cellular Activities genetics, Chromatin metabolism, Ubiquitination, Excision Repair, DNA Repair Enzymes metabolism, DNA Repair Enzymes genetics, RNA Polymerase II metabolism, RNA Polymerase II genetics, Poly-ADP-Ribose Binding Proteins metabolism, Poly-ADP-Ribose Binding Proteins genetics, DNA Repair, DNA Helicases metabolism, DNA Helicases genetics, Cockayne Syndrome genetics, Cockayne Syndrome metabolism

Abstract

Transcription is extremely important for cellular processes but can be hindered by RNA polymerase II (RNAPII) pausing and stalling. Cockayne syndrome protein B (CSB) promotes the progression of paused RNAPII or initiates transcription-coupled nucleotide excision repair (TC-NER) to remove stalled RNAPII. However, the specific mechanism by which CSB initiates TC-NER upon damage remains unclear. In this study, we identified the indispensable role of the ARK2N-CK2 complex in the CSB-mediated initiation of TC-NER. The ARK2N-CK2 complex is recruited to damage sites through CSB and then phosphorylates CSB. Phosphorylation of CSB enhances its binding to stalled RNAPII, prolonging the association of CSB with chromatin and promoting CSA-mediated ubiquitination of stalled RNAPII. Consistent with this finding, Ark2n -/- mice exhibit a phenotype resembling Cockayne syndrome. These findings shed light on the pivotal role of the ARK2N-CK2 complex in governing the fate of RNAPII through CSB, bridging a critical gap necessary for initiating TC-NER., Competing Interests: Competing interests statement:The authors declare no competing interest.

Published

2024

2. Frequent nonhomologous replacement of replicative helicase loaders by viruses in Vibrionaceae .

Author

Tominaga K, Ozaki S, Sato S, Katayama T, Nishimura Y, Omae K, and Iwasaki W

Subjects

Bacterial Proteins metabolism, Bacterial Proteins genetics, Viral Proteins genetics, Viral Proteins metabolism, Bacteriophages genetics, Bacteriophages enzymology, Evolution, Molecular, Genome, Bacterial, DnaB Helicases metabolism, DnaB Helicases genetics, Vibrio genetics, Vibrio enzymology, Vibrionaceae genetics, Vibrionaceae enzymology, DNA Helicases metabolism, DNA Helicases genetics, DNA Replication, Phylogeny

Abstract

Several microbial genomes lack textbook-defined essential genes. If an essential gene is absent from a genome, then an evolutionarily independent gene of unknown function complements its function. Here, we identified frequent nonhomologous replacement of an essential component of DNA replication initiation, a replicative helicase loader gene, in Vibrionaceae . Our analysis of Vibrionaceae genomes revealed two genes with unknown function, named vdhL1 and vdhL2 , that were substantially enriched in genomes without the known helicase-loader genes. These genes showed no sequence similarities to genes with known function but encoded proteins structurally similar with a viral helicase loader. Analyses of genomic syntenies and coevolution with helicase genes suggested that vdhL1/2 encodes a helicase loader. The in vitro assay showed that Vibrio harveyi VdhL1 and Vibrio ezurae VdhL2 promote the helicase activity of DnaB. Furthermore, molecular phylogenetics suggested that vdhL1 / 2 were derived from phages and replaced an intrinsic helicase loader gene of Vibrionaceae over 20 times. This high replacement frequency implies the host's advantage in acquiring a viral helicase loader gene., Competing Interests: Competing interests statement:The authors declare no competing interest.

Published

2024

3. An iron-sulfur cluster in the zinc-binding domain of the SARS-CoV-2 helicase modulates its RNA-binding and -unwinding activities.

Author

Maio N, Raza MK, Li Y, Zhang DL, Bollinger JM Jr, Krebs C, and Rouault TA

Subjects

Humans, COVID-19 Drug Treatment, DNA Helicases metabolism, RNA, Sulfur, Viral Nonstructural Proteins metabolism, RNA Helicases genetics, SARS-CoV-2 genetics, COVID-19

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the causative agent of COVID-19, uses an RNA-dependent RNA polymerase along with several accessory factors to replicate its genome and transcribe its genes. Nonstructural protein (nsp) 13 is a helicase required for viral replication. Here, we found that nsp13 ligates iron, in addition to zinc, when purified anoxically. Using inductively coupled plasma mass spectrometry, UV-visible absorption, EPR, and Mössbauer spectroscopies, we characterized nsp13 as an iron-sulfur (Fe-S) protein that ligates an Fe 4 S 4 cluster in the treble-clef metal-binding site of its zinc-binding domain. The Fe-S cluster in nsp13 modulates both its binding to the template RNA and its unwinding activity. Exposure of the protein to the stable nitroxide TEMPOL oxidizes and degrades the cluster and drastically diminishes unwinding activity. Thus, optimal function of nsp13 depends on a labile Fe-S cluster that is potentially targetable for COVID-19 treatment.

Published

2023

4. Unlicensed origin DNA melting by MCV and SV40 polyomavirus LT proteins is independent of ATP-dependent helicase activity.

Author

Wan L, Toland S, Robinson-McCarthy LR, Lee N, Schaich MA, Hengel SR, Li X, Bernstein KA, Van Houten B, Chang Y, and Moore PS

Subjects

Nucleic Acid Denaturation, Adenylyl Imidodiphosphate, DNA Replication, DNA genetics, DNA metabolism, DNA Helicases genetics, DNA Helicases metabolism, DNA, Single-Stranded, DNA, Viral genetics, DNA, Viral metabolism, Antigens, Polyomavirus Transforming genetics, Antigens, Polyomavirus Transforming metabolism, Simian virus 40 genetics, Simian virus 40 metabolism

Abstract

Cellular eukaryotic replication initiation helicases are first loaded as head-to-head double hexamers on double-stranded (ds) DNA origins and then initiate S-phase DNA melting during licensed (once per cell cycle) replication. Merkel cell polyomavirus (MCV) large T (LT) helicase oncoprotein similarly binds and melts its own 98-bp origin but replicates multiple times in a single cell cycle. To examine the actions of this unlicensed viral helicase, we quantitated multimerization of MCV LT molecules as they assembled on MCV DNA origins using real-time single-molecule microscopy. MCV LT formed highly stable double hexamers having 17-fold longer mean lifetime (τ, >1,500 s) on DNA than single hexamers. Unexpectedly, partial MCV LT assembly without double-hexamer formation was sufficient to melt origin dsDNA as measured by RAD51, RPA70, or S1 nuclease cobinding. DNA melting also occurred with truncated MCV LT proteins lacking the helicase domain, but was lost from a protein without the multimerization domain that could bind only as a monomer to DNA. SV40 polyomavirus LT also multimerized to the MCV origin without forming a functional hexamer but still melted origin DNA. MCV origin melting did not require ATP hydrolysis and occurred for both MCV and SV40 LT proteins using the nonhydrolyzable ATP analog, adenylyl-imidodiphosphate (AMP-PNP). LT double hexamers formed in AMP-PNP, and melted DNA, consistent with direct LT hexamer assembly around single-stranded (ss) DNA without the energy-dependent dsDNA-to-ssDNA melting and remodeling steps used by cellular helicases. These results indicate that LT multimerization rather than helicase activity is required for origin DNA melting during unlicensed virus replication.

Published

2023

5. Targeting SWI/SNF ATPases in H3.3K27M diffuse intrinsic pontine gliomas.

Author

Mota M, Sweha SR, Pun M, Natarajan SK, Ding Y, Chung C, Hawes D, Yang F, Judkins AR, Samajdar S, Cao X, Xiao L, Parolia A, Chinnaiyan AM, and Venneti S

Subjects

Humans, Child, Histones genetics, Adenosine Triphosphatases metabolism, Lysine genetics, Chromatin, Mutation, DNA Helicases metabolism, Nuclear Proteins metabolism, Transcription Factors metabolism, Diffuse Intrinsic Pontine Glioma, Glioma genetics, Brain Neoplasms genetics

Abstract

Diffuse midline gliomas (DMGs) including diffuse intrinsic pontine gliomas (DIPGs) bearing lysine-to-methionine mutations in histone H3 at lysine 27 (H3K27M) are lethal childhood brain cancers. These tumors harbor a global reduction in the transcriptional repressive mark H3K27me3 accompanied by an increase in the transcriptional activation mark H3K27ac. We postulated that H3K27M mutations, in addition to altering H3K27 modifications, reprogram the master chromatin remodeling switch/sucrose nonfermentable (SWI/SNF) complex. The SWI/SNF complex can exist in two main forms termed BAF and PBAF that play central roles in neurodevelopment and cancer. Moreover, BAF antagonizes PRC2, the main enzyme catalyzing H3K27me3. We demonstrate that H3K27M gliomas show increased protein levels of the SWI/SNF complex ATPase subunits SMARCA4 and SMARCA2, and the PBAF component PBRM1. Additionally, knockdown of mutant H3K27M lowered SMARCA4 protein levels. The proteolysis targeting chimera (PROTAC) AU-15330 that simultaneously targets SMARCA4, SMARCA2, and PBRM1 for degradation exhibits cytotoxicity in H3.3K27M but not H3 wild-type cells. AU-15330 lowered chromatin accessibility measured by ATAC-Seq at nonpromoter regions and reduced global H3K27ac levels. Integrated analysis of gene expression, proteomics, and chromatin accessibility in AU-15330-treated cells demonstrated reduction in the levels of FOXO1, a key member of the forkhead family of transcription factors. Moreover, genetic or pharmacologic targeting of FOXO1 resulted in cell death in H3K27M cells. Overall, our results suggest that H3K27M up-regulates SMARCA4 levels and combined targeting of SWI/SNF ATPases in H3.3K27M can serve as a potent therapeutic strategy for these deadly childhood brain tumors.

Published

2023

6. "Helicase" Activity promoted through dynamic interactions between a ssDNA translocase and a diffusing SSB protein.

Author

Mersch KN, Sokoloski JE, Nguyen B, Galletto R, and Lohman TM

Subjects

Humans, Protein Binding genetics, Replication Protein A metabolism, DNA, Single-Stranded metabolism, DNA metabolism, Adenosine Triphosphate metabolism, DNA Helicases metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism

Abstract

Replication protein A (RPA) is a eukaryotic single-stranded (ss) DNA-binding (SSB) protein that is essential for all aspects of genome maintenance. RPA binds ssDNA with high affinity but can also diffuse along ssDNA. By itself, RPA is capable of transiently disrupting short regions of duplex DNA by diffusing from a ssDNA that flanks the duplex DNA. Using single-molecule total internal reflection fluorescence and optical trapping combined with fluorescence approaches, we show that S. cerevisiae Pif1 can use its ATP-dependent 5' to 3' translocase activity to chemomechanically push a single human RPA (hRPA) heterotrimer directionally along ssDNA at rates comparable to those of Pif1 translocation alone. We further show that using its translocation activity, Pif1 can push hRPA from a ssDNA loading site into a duplex DNA causing stable disruption of at least 9 bp of duplex DNA. These results highlight the dynamic nature of hRPA enabling it to be readily reorganized even when bound tightly to ssDNA and demonstrate a mechanism by which directional DNA unwinding can be achieved through the combined action of a ssDNA translocase that pushes an SSB protein. These results highlight the two basic requirements for any processive DNA helicase: transient DNA base pair melting (supplied by hRPA) and ATP-dependent directional ssDNA translocation (supplied by Pif1) and that these functions can be unlinked by using two separate proteins.

Published

2023

7. Yin and yang regulation of stress granules by Caprin-1.

Author

Song D, Kuang L, Yang L, Wang L, Li H, Li X, Zhu Z, Shi C, Zhu H, and Gong W

Subjects

RNA Recognition Motif Proteins metabolism, Poly-ADP-Ribose Binding Proteins metabolism, Cytoplasmic Granules metabolism, Stress Granules, GTPase-Activating Proteins metabolism, Ubiquitin-Specific Proteases metabolism, RNA Helicases metabolism, DNA Helicases metabolism

Abstract

Stress granules (SGs) are cytoplasmic biomolecular condensates containing proteins and RNAs in response to stress. Ras-GTPase-activating protein binding protein 1 (G3BP1) is a core SG protein. Caprin-1 and ubiquitin specific peptidase 10 (USP10) interact with G3BP1, facilitating and suppressing SG formation, respectively. The crystal structures of the nuclear transport factor 2-like (NTF2L) domain of G3BP1 in complex with the G3BP1-interacting motif (GIM) of Caprin-1 and USP10 show that both GIMs bind to the same hydrophobic pocket of G3BP1. Moreover, both GIMs suppressed the liquid-liquid phase separation (LLPS) of G3BP1, suggesting that Caprin-1 likely facilitates SG formation via other mechanisms. Thus, we dissected various domains of Caprin-1 and investigated their role in LLPS in vitro and SG formation in cells. The C-terminal domain of Caprin-1 underwent spontaneous LLPS, whereas the N-terminal domain and GIM of Caprin-1 suppressed LLPS of G3BP1. The opposing effect of the N- and C-terminal domains of Caprin-1 on SG formation were demonstrated in cells with or without the endogenous Caprin-1. We propose that the N- and C-terminal domains of Caprin-1 regulate SG formation in a "yin and yang" fashion, mediating the dynamic and reversible assembly of SGs.

Published

2022

8. Global profiling of arginine dimethylation in regulating protein phase separation by a steric effect-based chemical-enrichment method.

Author

Wang Q, Li Z, Zhang S, Li Y, Wang Y, Fang Z, Ma Y, Liu Z, Zhang W, Li D, Liu C, and Ye M

Subjects

Animals, Humans, RNA Recognition Motif Proteins metabolism, DNA Helicases metabolism, Poly-ADP-Ribose Binding Proteins metabolism, RNA Helicases metabolism, Proteome metabolism, Mammals metabolism, DNA-Binding Proteins metabolism, RNA-Binding Proteins metabolism, Adaptor Proteins, Signal Transducing metabolism, Arginine metabolism, Cytoplasmic Granules metabolism

Abstract

Protein arginine methylation plays an important role in regulating protein functions in different cellular processes, and its dysregulation may lead to a variety of human diseases. Recently, arginine methylation was found to be involved in modulating protein liquid-liquid phase separation (LLPS), which drives the formation of different membraneless organelles (MLOs). Here, we developed a steric effect-based chemical-enrichment method (SECEM) coupled with liquid chromatography-tandem mass spectrometry to analyze arginine dimethylation (DMA) at the proteome level. We revealed by SECEM that, in mammalian cells, the DMA sites occurring in the RG/RGG motifs are preferentially enriched within the proteins identified in different MLOs, especially stress granules (SGs). Notably, global decrease of protein arginine methylation severely impairs the dynamic assembly and disassembly of SGs. By further profiling the dynamic change of DMA upon SG formation by SECEM, we identified that the most dramatic change of DMA occurs at multiple sites of RG/RGG-rich regions from several key SG-contained proteins, including G3BP1, FUS, hnRNPA1, and KHDRBS1. Moreover, both in vitro arginine methylation and mutation of the identified DMA sites significantly impair LLPS capability of the four different RG/RGG-rich regions. Overall, we provide a global profiling of the dynamic changes of protein DMA in the mammalian cells under different stress conditions by SECEM and reveal the important role of DMA in regulating protein LLPS and SG dynamics.

Published

2022

9. Sequence-dependent mechanochemical coupling of helicase translocation and unwinding at single-nucleotide resolution.

Author

Laszlo AH, Craig JM, Gavrilov M, Tippana R, Nova IC, Huang JR, Kim HC, Abell SJ, deCampos-Stairiker M, Mount JW, Bowman JL, Baker KS, Higinbotham H, Bobrovnikov D, Ha T, and Gundlach JH

Subjects

Adenosine Triphosphate metabolism, DNA metabolism, DNA, Single-Stranded, Kinetics, DNA Helicases metabolism, Nucleotides

Abstract

We used single-molecule picometer-resolution nanopore tweezers (SPRNT) to resolve the millisecond single-nucleotide steps of superfamily 1 helicase PcrA as it translocates on, or unwinds, several kilobase-long DNA molecules. We recorded more than two million enzyme steps under various assisting and opposing forces in diverse adenosine tri- and diphosphate conditions to comprehensively explore the mechanochemistry of PcrA motion. Forces applied in SPRNT mimic forces and physical barriers PcrA experiences in vivo , such as when the helicase encounters bound proteins or duplex DNA. We show how PcrA's kinetics change with such stimuli. SPRNT allows for direct association of the underlying DNA sequence with observed enzyme kinetics. Our data reveal that the underlying DNA sequence passing through the helicase strongly influences the kinetics during translocation and unwinding. Surprisingly, unwinding kinetics are not solely dominated by the base pairs being unwound. Instead, the sequence of the single-stranded DNA on which the PcrA walks determines much of the kinetics of unwinding.

Published

2022

10. Structural insight and characterization of human Twinkle helicase in mitochondrial disease.

Author

Riccio AA, Bouvette J, Perera L, Longley MJ, Krahn JM, Williams JG, Dutcher R, Borgnia MJ, and Copeland WC

Subjects

DNA Replication, DNA, Mitochondrial biosynthesis, Humans, Mass Spectrometry, Molecular Dynamics Simulation, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Mutant Proteins ultrastructure, Cryoelectron Microscopy, DNA Helicases chemistry, DNA Helicases genetics, DNA Helicases metabolism, DNA Helicases ultrastructure, Mitochondrial Diseases genetics, Mitochondrial Proteins chemistry, Mitochondrial Proteins genetics, Mitochondrial Proteins metabolism, Mitochondrial Proteins ultrastructure, Protein Multimerization

Abstract

Twinkle is the mammalian helicase vital for replication and integrity of mitochondrial DNA. Over 90 Twinkle helicase disease variants have been linked to progressive external ophthalmoplegia and ataxia neuropathies among other mitochondrial diseases. Despite the biological and clinical importance, Twinkle represents the only remaining component of the human minimal mitochondrial replisome that has yet to be structurally characterized. Here, we present 3-dimensional structures of human Twinkle W315L. Employing cryo-electron microscopy (cryo-EM), we characterize the oligomeric assemblies of human full-length Twinkle W315L, define its multimeric interface, and map clinical variants associated with Twinkle in inherited mitochondrial disease. Cryo-EM, crosslinking-mass spectrometry, and molecular dynamics simulations provide insight into the dynamic movement and molecular consequences of the W315L clinical variant. Collectively, this ensemble of structures outlines a framework for studying Twinkle function in mitochondrial DNA replication and associated disease states.

Published

2022

11. Computationally exploring the mechanism of bacteriophage T7 gp4 helicase translocating along ssDNA.

Author

Jin S, Bueno C, Lu W, Wang Q, Chen M, Chen X, Wolynes PG, and Gao Y

Subjects

Adenosine Diphosphate metabolism, Adenosine Triphosphate metabolism, DNA Primase metabolism, Protein Conformation, Bacteriophage T7 enzymology, Bacteriophage T7 genetics, DNA Helicases metabolism, DNA, Single-Stranded

Abstract

Bacteriophage T7 gp4 helicase has served as a model system for understanding mechanisms of hexameric replicative helicase translocation. The mechanistic basis of how nucleoside 5'-triphosphate hydrolysis and translocation of gp4 helicase are coupled is not fully resolved. Here, we used a thermodynamically benchmarked coarse-grained protein force field, Associative memory, Water mediated, Structure and Energy Model (AWSEM), with the single-stranded DNA (ssDNA) force field 3SPN.2C to investigate gp4 translocation. We found that the adenosine 5'-triphosphate (ATP) at the subunit interface stabilizes the subunit-subunit interaction and inhibits subunit translocation. Hydrolysis of ATP to adenosine 5'-diphosphate enables the translocation of one subunit, and new ATP binding at the new subunit interface finalizes the subunit translocation. The LoopD2 and the N-terminal primase domain provide transient protein-protein and protein-DNA interactions that facilitate the large-scale subunit movement. The simulations of gp4 helicase both validate our coarse-grained protein-ssDNA force field and elucidate the molecular basis of replicative helicase translocation.

Published

2022

12. The structure and activities of the archaeal transcription termination factor Eta detail vulnerabilities of the transcription elongation complex.

Author

Marshall CJ, Qayyum MZ, Walker JE, Murakami KS, and Santangelo TJ

Subjects

Crystallography, DNA-Directed RNA Polymerases metabolism, Protein Domains, Archaeal Proteins chemistry, Archaeal Proteins metabolism, DNA Helicases chemistry, DNA Helicases metabolism, Thermococcus enzymology, Thermococcus genetics, Transcription Factors chemistry, Transcription Factors metabolism, Transcription Termination, Genetic

Abstract

Transcription must be properly regulated to ensure dynamic gene expression underlying growth, development, and response to environmental cues. Regulation is imposed throughout the transcription cycle, and while many efforts have detailed the regulation of transcription initiation and early elongation, the termination phase of transcription also plays critical roles in regulating gene expression. Transcription termination can be driven by only a few proteins in each domain of life. Detailing the mechanism(s) employed provides insight into the vulnerabilities of transcription elongation complexes (TECs) that permit regulated termination to control expression of many genes and operons. Here, we describe the biochemical activities and crystal structure of the superfamily 2 helicase Eta, one of two known factors capable of disrupting archaeal transcription elongation complexes. Eta retains a twin-translocase core domain common to all superfamily 2 helicases and a well-conserved C terminus wherein individual amino acid substitutions can critically abrogate termination activities. Eta variants that perturb ATPase, helicase, single-stranded DNA and double-stranded DNA translocase and termination activities identify key regions of the C terminus of Eta that, when combined with modeling Eta-TEC interactions, provide a structural model of Eta-mediated termination guided in part by structures of Mfd and the bacterial TEC. The susceptibility of TECs to disruption by termination factors that target the upstream surface of RNA polymerase and potentially drive termination through forward translocation and allosteric mechanisms that favor opening of the clamp to release the encapsulated nucleic acids emerges as a common feature of transcription termination mechanisms.

Published

2022

13. Viral evasion of PKR restriction by reprogramming cellular stress granules.

Author

Gao P, Liu Y, Wang H, Chai Y, Weng W, Zhang Y, Zhou L, Ge X, Guo X, Han J, and Yang H

Subjects

Animals, Swine, Virus Replication, Antiviral Restriction Factors metabolism, DNA Helicases metabolism, Immune Evasion, Poly-ADP-Ribose Binding Proteins metabolism, Porcine respiratory and reproductive syndrome virus genetics, Porcine respiratory and reproductive syndrome virus metabolism, RNA Helicases metabolism, RNA Recognition Motif Proteins metabolism, Stress Granules virology, Viral Nonstructural Proteins metabolism, eIF-2 Kinase metabolism

Abstract

Protein kinase R (PKR) is a critical host restriction factor against invading viral pathogens. However, this molecule is inactivated in the cells infected with porcine reproductive and respiratory syndrome virus (PRRSV), an economically devastating pathogen to the world swine industry. Here, we report that this event is to suppress cellular inflammation and is mediated by the viral replicase protein nsp1β. We show that nsp1β is a stress-responsive protein, enters virus-induced stress granules (SGs) during infection, and repurposes SGs into a proviral platform, where it co-opts the SG core component G3BP1 to interact with PKR in a regulated manner. RNA interference silencing of G3BP1 or mutation of specific nsp1β residues (VS19GG) can abolish the antagonization of PKR activation. The viral mutant carrying the corresponding mutations induces elevated level of PKR phosphorylation and pronounced production of inflammatory cytokines (e.g., tumor necrosis factor-α, interleukin [IL]-6, and IL-8), whereas small-interfering RNA knockdown of PKR or treatment with C16, a PKR inhibitor, blocks this effect. Thus, PRRSV has evolved a unique strategy to evade PKR restriction to suppress host inflammatory responses.

Published

2022

14. Human HELB is a processive motor protein that catalyzes RPA clearance from single-stranded DNA.

Author

Hormeno S, Wilkinson OJ, Aicart-Ramos C, Kuppa S, Antony E, Dillingham MS, and Moreno-Herrero F

Subjects

Adenosine Triphosphate chemistry, Adenosine Triphosphate metabolism, Humans, Hydrolysis, Protein Binding, DNA Helicases chemistry, DNA Helicases metabolism, DNA, Single-Stranded chemistry, DNA, Single-Stranded metabolism, Molecular Motor Proteins chemistry, Molecular Motor Proteins metabolism, Replication Protein A metabolism

Abstract

Human DNA helicase B (HELB) is a poorly characterized helicase suggested to play both positive and negative regulatory roles in DNA replication and recombination. In this work, we used bulk and single-molecule approaches to characterize the biochemical activities of HELB protein with a particular focus on its interactions with Replication Protein A (RPA) and RPA–single-stranded DNA (ssDNA) filaments. HELB is a monomeric protein that binds tightly to ssDNA with a site size of ∼20 nucleotides. It couples ATP hydrolysis to translocation along ssDNA in the 5′ to 3′ direction accompanied by the formation of DNA loops. HELB also displays classical helicase activity, but this is very weak in the absence of an assisting force. HELB binds specifically to human RPA, which enhances its ATPase and ssDNA translocase activities but inhibits DNA unwinding. Direct observation of HELB on RPA nucleoprotein filaments shows that translocating HELB concomitantly clears RPA from ssDNA. This activity, which can allow other proteins access to ssDNA intermediates despite their shielding by RPA, may underpin the diverse roles of HELB in cellular DNA transactions.

Published

2022

15. The CHARGE syndrome ortholog CHD-7 regulates TGF-β pathways in Caenorhabditis elegans .

Author

Jofré DM, Hoffman DK, Cervino AS, Hahn GM, Grundy M, Yun S, Amrit FRG, Stolz DB, Godoy LF, Salvatore E, Rossi FA, Ghazi A, Cirio MC, Yanowitz JL, and Hochbaum D

Subjects

Animals, Caenorhabditis elegans metabolism, DNA Helicases genetics, DNA Helicases metabolism, Larva, Signal Transduction, Transforming Growth Factor beta genetics, Transforming Growth Factor beta metabolism, Caenorhabditis elegans Proteins metabolism, CHARGE Syndrome

Abstract

CHARGE syndrome is a complex developmental disorder caused by mutations in the chromodomain helicase DNA-binding protein-7 (CHD7) and characterized by retarded growth and malformations in the heart and nervous system. Despite the public health relevance of this disorder, relevant cellular pathways and targets of CHD7 that relate to disease pathology are still poorly understood. Here we report that chd-7, the nematode ortholog of Chd7, is required for dauer morphogenesis, lifespan determination, stress response, and body size determination. Consistent with our discoveries, we found chd-7 to be allelic to scd-3, a previously identified dauer suppressor from the DAF-7/ tumor growth factor-β (TGF-β) pathway. Epistatic analysis places CHD-7 at the level of the DAF-3/DAF-5 complex, but we found that CHD-7 also directly impacts the expression of multiple components of this pathway. Transcriptomic analysis revealed that chd-7 mutants fail to repress daf-9 for execution of the dauer program. In addition, CHD-7 regulates the DBL-1/BMP pathway components and shares roles in male tail development and cuticle synthesis. To explore a potential conserved function for chd-7 in vertebrates, we used Xenopus laevis embryos, an established model to study craniofacial development. Morpholino-mediated knockdown of Chd7 led to a reduction in col2a1 messenger RNA (mRNA) levels, a collagen whose expression depends on TGF-β signaling. Both embryonic lethality and craniofacial defects in Chd7-depleted tadpoles were partially rescued by overexpression of col2a1 mRNA. We suggest that Chd7 has conserved roles in regulation of the TGF-β signaling pathway and pathogenic Chd7 could lead to a defective extracellular matrix deposition.

Published

2022

16. ΔNp63-Senataxin circuit controls keratinocyte differentiation by promoting the transcriptional termination of epidermal genes.

Author

Gatti V, Fierro C, Compagnone M, La Banca V, Mauriello A, Montanaro M, Scalera S, De Nicola F, Candi E, Ricci F, Fania L, Melino G, and Peschiaroli A

Subjects

DNA Helicases genetics, Humans, Keratin-1 biosynthesis, Keratin-1 genetics, MCF-7 Cells, Multifunctional Enzymes genetics, RNA Helicases genetics, Transcription Factors biosynthesis, Transcription Factors genetics, Tumor Suppressor Proteins biosynthesis, Tumor Suppressor Proteins genetics, Cell Differentiation, DNA Helicases metabolism, Epidermis metabolism, Keratinocytes metabolism, Multifunctional Enzymes metabolism, RNA Helicases metabolism, Transcription Factors metabolism, Transcription Termination, Genetic, Tumor Suppressor Proteins metabolism

Abstract

SignificanceΔNp63 is a master regulator of skin homeostasis since it finely controls keratinocyte differentiation and proliferation. Here, we provide cellular and molecular evidence demonstrating the functional role of a ΔNp63 interactor, the R-loop-resolving enzyme Senataxin (SETX), in fine-tuning keratinocyte differentiation. We found that SETX physically binds the p63 DNA-binding motif present in two early epidermal differentiation genes, Keratin 1 (KRT1) and ZNF750, facilitating R-loop removal over their 3' ends and thus allowing efficient transcriptional termination and gene expression. These molecular events translate into the inability of SETX-depleted keratinocytes to undergo the correct epidermal differentiation program. Remarkably, SETX is dysregulated in cutaneous squamous cell carcinoma, suggesting its potential involvement in the pathogenesis of skin disorders.

Published

2022

17. Mycobacterium tuberculosis DNA repair helicase UvrD1 is activated by redox-dependent dimerization via a 2B domain cysteine.

Author

Chadda A, Jensen D, Tomko EJ, Ruiz Manzano A, Nguyen B, Lohman TM, and Galburt EA

Subjects

Bacterial Proteins genetics, Cysteine chemistry, DNA genetics, DNA metabolism, DNA Damage, DNA Helicases genetics, DNA Repair genetics, DNA, Bacterial metabolism, DNA, Single-Stranded, Dimerization, Oxidation-Reduction, Protein Binding, Protein Domains genetics, Bacterial Proteins metabolism, DNA Helicases metabolism, DNA Repair physiology, Mycobacterium tuberculosis genetics

Abstract

Mycobacterium tuberculosis ( Mtb ) causes tuberculosis and, during infection, is exposed to reactive oxygen species and reactive nitrogen intermediates from the host immune response that can cause DNA damage. UvrD-like proteins are involved in DNA repair and replication and belong to the SF1 family of DNA helicases that use ATP hydrolysis to catalyze DNA unwinding. In Mtb , there are two UvrD-like enzymes, where UvrD1 is most closely related to other family members. Previous studies have suggested that UvrD1 is exclusively monomeric; however, it is well known that Escherichia coli UvrD and other UvrD family members exhibit monomer-dimer equilibria and unwind as dimers in the absence of accessory factors. Here, we reconcile these incongruent studies by showing that Mtb UvrD1 exists in monomer, dimer, and higher-order oligomeric forms, where dimerization is regulated by redox potential. We identify a 2B domain cysteine, conserved in many Actinobacteria, that underlies this effect. We also show that UvrD1 DNA-unwinding activity correlates specifically with the dimer population and is thus titrated directly via increasing positive (i.e., oxidative) redox potential. Consistent with the regulatory role of the 2B domain and the dimerization-based activation of DNA unwinding in UvrD family helicases, these results suggest that UvrD1 is activated under oxidizing conditions when it may be needed to respond to DNA damage during infection., Competing Interests: The authors declare no competing interest.

Published

2022

18. Rad54 and Rdh54 prevent Srs2-mediated disruption of Rad51 presynaptic filaments.

Author

Meir A, Crickard JB, Kwon Y, Sung P, and Greene EC

Subjects

Cell Cycle Proteins metabolism, DNA Damage physiology, DNA Helicases physiology, DNA Repair genetics, DNA Repair Enzymes genetics, DNA Repair Enzymes physiology, DNA Topoisomerases physiology, DNA, Single-Stranded metabolism, DNA-Binding Proteins metabolism, Homologous Recombination genetics, Protein Binding genetics, Rad51 Recombinase metabolism, Rad51 Recombinase physiology, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae Proteins genetics, Saccharomyces cerevisiae Proteins physiology, DNA Helicases metabolism, DNA Repair Enzymes metabolism, DNA Topoisomerases metabolism, Saccharomyces cerevisiae Proteins metabolism

Abstract

Srs2 is a superfamily 1 (SF1) helicase that participates in several pathways necessary for the repair of damaged DNA. Srs2 regulates formation of early homologous recombination (HR) intermediates by actively removing the recombinase Rad51 from single-stranded DNA (ssDNA). It is not known whether and how Srs2 itself is down-regulated to allow for timely HR progression. Rad54 and Rdh54 are two closely related superfamily 2 (SF2) motor proteins that promote the formation of Rad51-dependent recombination intermediates. Rad54 and Rdh54 bind tightly to Rad51-ssDNA and act downstream of Srs2, suggesting that they may affect the ability of Srs2 to dismantle Rad51 filaments. Here, we used DNA curtains to determine whether Rad54 and Rdh54 alter the ability of Srs2 to disrupt Rad51 filaments. We show that Rad54 and Rdh54 act synergistically to greatly restrict the antirecombinase activity of Srs2. Our findings suggest that Srs2 may be accorded only a limited time window to act and that Rad54 and Rdh54 fulfill a role of prorecombinogenic licensing factors., Competing Interests: The authors declare no competing interest., (Copyright © 2022 the Author(s). Published by PNAS.)

Published

2022

19. Integrated genome and transcriptome analyses reveal the mechanism of genome instability in ataxia with oculomotor apraxia 2.

Author

Kanagaraj R, Mitter R, Kantidakis T, Edwards MM, Benitez A, Chakravarty P, Fu B, Becherel O, Yang F, Lavin MF, Koren A, Stewart A, and West SC

Subjects

Animals, Apraxias genetics, Ataxia genetics, Cell Line, Cerebellar Ataxia genetics, DNA Helicases genetics, DNA Repair genetics, Gene Expression Profiling methods, Genomic Instability genetics, Genomics methods, Humans, Mice, Mouse Embryonic Stem Cells, Multifunctional Enzymes genetics, Mutation genetics, Neurodegenerative Diseases genetics, Primary Cell Culture, Promoter Regions, Genetic genetics, RNA Helicases genetics, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias physiopathology, Transcriptome genetics, Chromosomal Instability genetics, DNA Helicases metabolism, Multifunctional Enzymes metabolism, RNA Helicases metabolism, Spinocerebellar Ataxias congenital

Abstract

Mutations in the SETX gene, which encodes Senataxin, are associated with the progressive neurodegenerative diseases ataxia with oculomotor apraxia 2 (AOA2) and amyotrophic lateral sclerosis 4 (ALS4). To identify the causal defect in AOA2, patient-derived cells and SETX knockouts (human and mouse) were analyzed using integrated genomic and transcriptomic approaches. A genome-wide increase in chromosome instability (gains and losses) within genes and at chromosome fragile sites was observed, resulting in changes to gene-expression profiles. Transcription stress near promoters correlated with high GCskew and the accumulation of R-loops at promoter-proximal regions, which localized with chromosomal regions where gains and losses were observed. In the absence of Senataxin, the Cockayne syndrome protein CSB was required for the recruitment of the transcription-coupled repair endonucleases (XPG and XPF) and RAD52 recombination protein to target and resolve transcription bubbles containing R-loops, leading to genomic instability. These results show that transcription stress is an important contributor to SETX mutation-associated chromosome fragility and AOA2., Competing Interests: The authors declare no competing interest., (Copyright © 2022 the Author(s). Published by PNAS.)

Published

2022

20. CMG helicase can use ATPγS to unwind DNA: Implications for the rate-limiting step in the reaction mechanism.

Author

Yao NY, Zhang D, Yurieva O, and O'Donnell ME

Subjects

Adenosine Triphosphate chemistry, Adenosine Triphosphate metabolism, Cell Cycle Proteins metabolism, DNA chemistry, DNA Helicases genetics, DNA Replication, DNA-Binding Proteins metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism, Adenosine Triphosphate analogs & derivatives, DNA Helicases metabolism, Multiprotein Complexes metabolism

Abstract

The adenosine triphosphate (ATP) analog ATPγS often greatly slows or prevents enzymatic ATP hydrolysis. The eukaryotic CMG (Cdc45, Mcm2 to 7, GINS) replicative helicase is presumed unable to hydrolyze ATPγS and thus unable to perform DNA unwinding, as documented for certain other helicases. Consequently, ATPγS is often used to "preload" CMG onto forked DNA substrates without unwinding before adding ATP to initiate helicase activity. We find here that CMG does hydrolyze ATPγS and couples it to DNA unwinding. Indeed, the rate of unwinding of a 20- and 30-mer duplex fork of different sequences by CMG is only reduced 1- to 1.5-fold using ATPγS compared with ATP. These findings imply that a conformational change is the rate-limiting step during CMG unwinding, not hydrolysis. Instead of using ATPγS for loading CMG onto DNA, we demonstrate here that nonhydrolyzable adenylyl-imidodiphosphate (AMP-PNP) can be used to preload CMG onto a forked DNA substrate without unwinding., Competing Interests: The authors declare no competing interest., (Copyright © 2022 the Author(s). Published by PNAS.)

Published

2022

21. Multiple roles for PARP1 in ALC1-dependent nucleosome remodeling.

Author

Ooi SK, Sato S, Tomomori-Sato C, Zhang Y, Wen Z, Banks CAS, Washburn MP, Unruh JR, Florens L, Conaway RC, and Conaway JW

Subjects

Cell Line, Tumor, Chromatin Assembly and Disassembly, DNA Repair, Humans, DNA Helicases metabolism, DNA-Binding Proteins metabolism, Nucleosomes metabolism, Poly (ADP-Ribose) Polymerase-1 metabolism

Abstract

The SNF2 family ATPase Amplified in Liver Cancer 1 (ALC1) is the only chromatin remodeling enzyme with a poly(ADP-ribose) (PAR) binding macrodomain. ALC1 functions together with poly(ADP-ribose) polymerase PARP1 to remodel nucleosomes. Activation of ALC1 cryptic ATPase activity and the subsequent nucleosome remodeling requires binding of its macrodomain to PAR chains synthesized by PARP1 and NAD + A key question is whether PARP1 has a role(s) in ALC1-dependent nucleosome remodeling beyond simply synthesizing the PAR chains needed to activate the ALC1 ATPase. Here, we identify PARP1 separation-of-function mutants that activate ALC1 ATPase but do not support nucleosome remodeling by ALC1. Investigation of these mutants has revealed multiple functions for PARP1 in ALC1-dependent nucleosome remodeling and provides insights into its multifaceted role in chromatin remodeling., Competing Interests: The authors declare no competing interest.

Published

2021

22. Natural variation identifies SNI1, the SMC5/6 component, as a modifier of meiotic crossover in Arabidopsis .

Author

Zhu L, Fernández-Jiménez N, Szymanska-Lejman M, Pelé A, Underwood CJ, Serra H, Lambing C, Dluzewska J, Bieluszewski T, Pradillo M, Henderson IR, and Ziolkowski PA

Subjects

Arabidopsis genetics, Arabidopsis Proteins genetics, DNA Helicases genetics, Gene Expression Regulation, Plant, Nuclear Proteins genetics, Protein Domains, Arabidopsis metabolism, Arabidopsis Proteins metabolism, Crossing Over, Genetic physiology, DNA Helicases metabolism, Genetic Variation, Meiosis physiology, Nuclear Proteins metabolism

Abstract

The frequency and distribution of meiotic crossovers are tightly controlled; however, variation in this process can be observed both within and between species. Using crosses of two natural Arabidopsis thaliana accessions, Col and L er , we mapped a crossover modifier locus to semidominant polymorphisms in SUPPRESSOR OF NPR1-1 INDUCIBLE 1 ( SNI1 ), which encodes a component of the SMC5/6 complex. The sni1 mutant exhibits a modified pattern of recombination across the genome with crossovers elevated in chromosome distal regions but reduced in pericentromeres. Mutations in SNI1 result in reduced crossover interference and can partially restore the fertility of a Class I crossover pathway mutant, which suggests that the protein affects noninterfering crossover repair. Therefore, we tested genetic interactions between SNI1 and both RECQ4 and FANCM DNA helicases, which showed that additional Class II crossovers observed in the sni1 mutant are FANCM independent. Furthermore, genetic analysis of other SMC5/6 mutants confirms the observations of crossover redistribution made for SNI1 The study reveals the importance of the SMC5/6 complex in ensuring the proper progress of meiotic recombination in plants., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

23. The intra-S phase checkpoint directly regulates replication elongation to preserve the integrity of stalled replisomes.

Author

Liu Y, Wang L, Xu X, Yuan Y, Zhang B, Li Z, Xie Y, Yan R, Zheng Z, Ji J, Murray JM, Carr AM, and Kong D

Subjects

Alleles, DNA Helicases metabolism, Hydroxyurea pharmacology, Models, Biological, Multiprotein Complexes metabolism, Mutation genetics, Phosphorylation drug effects, Schizosaccharomyces drug effects, Schizosaccharomyces pombe Proteins genetics, Schizosaccharomyces pombe Proteins metabolism, DNA Replication drug effects, DNA-Directed DNA Polymerase metabolism, Multienzyme Complexes metabolism, S Phase Cell Cycle Checkpoints drug effects, Schizosaccharomyces metabolism

Abstract

DNA replication is dramatically slowed down under replication stress. The regulation of replication speed is a conserved response in eukaryotes and, in fission yeast, requires the checkpoint kinases Rad3 ATR and Cds1 Chk2 However, the underlying mechanism of this checkpoint regulation remains unresolved. Here, we report that the Rad3 ATR -Cds1 Chk2 checkpoint directly targets the Cdc45-MCM-GINS (CMG) replicative helicase under replication stress. When replication forks stall, the Cds1 Chk2 kinase directly phosphorylates Cdc45 on the S275, S322, and S397 residues, which significantly reduces CMG helicase activity. Furthermore, in cds1 Chk2 -mutated cells, the CMG helicase and DNA polymerases are physically separated, potentially disrupting replisomes and collapsing replication forks. This study demonstrates that the intra-S phase checkpoint directly regulates replication elongation, reduces CMG helicase processivity, prevents CMG helicase delinking from DNA polymerases, and therefore helps preserve the integrity of stalled replisomes and replication forks., Competing Interests: The authors declare no competing interest.

Published

2021

24. Prespacers formed during primed adaptation associate with the Cas1-Cas2 adaptation complex and the Cas3 interference nuclease-helicase.

Author

Musharova O, Medvedeva S, Klimuk E, Guzman NM, Titova D, Zgoda V, Shiriaeva A, Semenova E, Severinov K, and Savitskaya E

Subjects

CRISPR-Cas Systems, DNA Helicases metabolism, Endonucleases metabolism, Escherichia coli metabolism, Escherichia coli Proteins metabolism

Abstract

For Type I CRISPR-Cas systems, a mode of CRISPR adaptation named priming has been described. Priming allows specific and highly efficient acquisition of new spacers from DNA recognized (primed) by the Cascade-crRNA (CRISPR RNA) effector complex. Recognition of the priming protospacer by Cascade-crRNA serves as a signal for engaging the Cas3 nuclease-helicase required for both interference and primed adaptation, suggesting the existence of a primed adaptation complex (PAC) containing the Cas1-Cas2 adaptation integrase and Cas3. To detect this complex in vivo, we here performed chromatin immunoprecipitation with Cas3-specific and Cas1-specific antibodies using cells undergoing primed adaptation. We found that prespacers are bound by both Cas1 (presumably, as part of the Cas1-Cas2 integrase) and Cas3, implying direct physical association of the interference and adaptation machineries as part of PAC., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

25. Structural basis for backtracking by the SARS-CoV-2 replication-transcription complex.

Author

Malone B, Chen J, Wang Q, Llewellyn E, Choi YJ, Olinares PDB, Cao X, Hernandez C, Eng ET, Chait BT, Shaw DE, Landick R, Darst SA, and Campbell EA

Subjects

Adenosine Monophosphate pharmacology, Antiviral Agents pharmacology, COVID-19 genetics, COVID-19 metabolism, Coronavirus RNA-Dependent RNA Polymerase metabolism, Cryoelectron Microscopy methods, DNA Helicases metabolism, Genome, Viral, Humans, Molecular Dynamics Simulation, RNA Helicases metabolism, RNA, Viral genetics, RNA, Viral metabolism, RNA-Dependent RNA Polymerase metabolism, RNA-Dependent RNA Polymerase physiology, SARS-CoV-2 drug effects, SARS-CoV-2 genetics, Viral Nonstructural Proteins genetics, COVID-19 virology, SARS-CoV-2 physiology, Virus Replication genetics

Abstract

Backtracking, the reverse motion of the transcriptase enzyme on the nucleic acid template, is a universal regulatory feature of transcription in cellular organisms but its role in viruses is not established. Here we present evidence that backtracking extends into the viral realm, where backtracking by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) RNA-dependent RNA polymerase (RdRp) may aid viral transcription and replication. Structures of SARS-CoV-2 RdRp bound to the essential nsp13 helicase and RNA suggested the helicase facilitates backtracking. We use cryo-electron microscopy, RNA-protein cross-linking, and unbiased molecular dynamics simulations to characterize SARS-CoV-2 RdRp backtracking. The results establish that the single-stranded 3' segment of the product RNA generated by backtracking extrudes through the RdRp nucleoside triphosphate (NTP) entry tunnel, that a mismatched nucleotide at the product RNA 3' end frays and enters the NTP entry tunnel to initiate backtracking, and that nsp13 stimulates RdRp backtracking. Backtracking may aid proofreading, a crucial process for SARS-CoV-2 resistance against antivirals., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

26. DDX11 loss causes replication stress and pharmacologically exploitable DNA repair defects.

Author

Jegadesan NK and Branzei D

Subjects

Antineoplastic Agents, Cisplatin, Genes, BRCA1, Genes, BRCA2, HeLa Cells, Humans, Poly(ADP-ribose) Polymerase Inhibitors, DEAD-box RNA Helicases metabolism, DNA Helicases metabolism, DNA Repair, Drug Resistance, Neoplasm, Molecular Targeted Therapy

Abstract

DDX11 encodes an iron-sulfur cluster DNA helicase required for development, mutated, and overexpressed in cancers. Here, we show that loss of DDX11 causes replication stress and sensitizes cancer cells to DNA damaging agents, including poly ADP ribose polymerase (PARP) inhibitors and platinum drugs. We find that DDX11 helicase activity prevents chemotherapy drug hypersensitivity and accumulation of DNA damage. Mechanistically, DDX11 acts downstream of 53BP1 to mediate homology-directed repair and RAD51 focus formation in manners nonredundant with BRCA1 and BRCA2. As a result, DDX11 down-regulation aggravates the chemotherapeutic sensitivity of BRCA1 / 2 -mutated cancers and resensitizes chemotherapy drug-resistant BRCA1 / 2 -mutated cancer cells that regained homologous recombination proficiency. The results further indicate that DDX11 facilitates recombination repair by assisting double strand break resection and the loading of both RPA and RAD51 on single-stranded DNA substrates. We propose DDX11 as a potential target in cancers by creating pharmacologically exploitable DNA repair vulnerabilities., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

27. Helicase-like functions in phosphate loop containing beta-alpha polypeptides.

Author

Vyas P, Trofimyuk O, Longo LM, Deshmukh FK, Sharon M, and Tawfik DS

Subjects

Amino Acid Motifs physiology, Amino Acid Sequence genetics, DNA Helicases metabolism, DNA Helicases physiology, DNA, Single-Stranded chemistry, DNA, Single-Stranded metabolism, Models, Molecular, Nucleoside-Triphosphatase chemistry, Peptides chemistry, Phosphates chemistry, Protein Conformation, alpha-Helical physiology, Protein Conformation, beta-Strand physiology, Proteins chemistry, RNA chemistry, Rec A Recombinases metabolism, AAA Domain genetics, AAA Domain physiology

Abstract

The P-loop Walker A motif underlies hundreds of essential enzyme families that bind nucleotide triphosphates (NTPs) and mediate phosphoryl transfer (P-loop NTPases), including the earliest DNA/RNA helicases, translocases, and recombinases. What were the primordial precursors of these enzymes? Could these large and complex proteins emerge from simple polypeptides? Previously, we showed that P-loops embedded in simple βα repeat proteins bind NTPs but also, unexpectedly so, ssDNA and RNA. Here, we extend beyond the purely biophysical function of ligand binding to demonstrate rudimentary helicase-like activities. We further constructed simple 40-residue polypeptides comprising just one β-(P-loop)-α element. Despite their simplicity, these P-loop prototypes confer functions such as strand separation and exchange. Foremost, these polypeptides unwind dsDNA, and upon addition of NTPs, or inorganic polyphosphates, release the bound ssDNA strands to allow reformation of dsDNA. Binding kinetics and low-resolution structural analyses indicate that activity is mediated by oligomeric forms spanning from dimers to high-order assemblies. The latter are reminiscent of extant P-loop recombinases such as RecA. Overall, these P-loop prototypes compose a plausible description of the sequence, structure, and function of the earliest P-loop NTPases. They also indicate that multifunctionality and dynamic assembly were key in endowing short polypeptides with elaborate, evolutionarily relevant functions., Competing Interests: The authors declare no competing interest.

Published

2021

28. Super-resolution mapping of cellular double-strand break resection complexes during homologous recombination.

Author

Whelan DR and Rothenberg E

Subjects

BRCA1 Protein metabolism, Cell Line, Tumor, DNA Helicases metabolism, DNA Repair Enzymes metabolism, DNA, Single-Stranded metabolism, Endodeoxyribonucleases metabolism, Exodeoxyribonucleases metabolism, Humans, MRE11 Homologue Protein metabolism, Multiprotein Complexes metabolism, RecQ Helicases metabolism, Tumor Suppressor p53-Binding Protein 1 metabolism, DNA Breaks, Double-Stranded, Homologous Recombination, Recombinational DNA Repair, Single Molecule Imaging

Abstract

Homologous recombination (HR) is a major pathway for repair of DNA double-strand breaks (DSBs). The initial step that drives the HR process is resection of DNA at the DSB, during which a multitude of nucleases, mediators, and signaling proteins accumulates at the damage foci in a manner that remains elusive. Using single-molecule localization super-resolution (SR) imaging assays, we specifically visualize the spatiotemporal behavior of key mediator and nuclease proteins as they resect DNA at single-ended double-strand breaks (seDSBs) formed at collapsed replication forks. By characterizing these associations, we reveal the in vivo dynamics of resection complexes involved in generating the long single-stranded DNA (ssDNA) overhang prior to homology search. We show that 53BP1, a protein known to antagonize HR, is recruited to seDSB foci during early resection but is spatially separated from repair activities. Contemporaneously, CtBP-interacting protein (CtIP) and MRN (MRE11-RAD51-NBS1) associate with seDSBs, interacting with each other and BRCA1. The HR nucleases EXO1 and DNA2 are also recruited and colocalize with each other and with the repair helicase Bloom syndrome protein (BLM), demonstrating multiple simultaneous resection events. Quantification of replication protein A (RPA) accumulation and ssDNA generation shows that resection is completed 2 to 4 h after break induction. However, both BRCA1 and BLM persist later into HR, demonstrating potential roles in homology search and repair resolution. Furthermore, we show that initial recruitment of BRCA1 and removal of Ku are largely independent of MRE11 exonuclease activity but dependent on MRE11 endonuclease activity. Combined, our observations provide a detailed description of resection during HR repair., Competing Interests: The authors declare no competing interest.

Published

2021

29. Clutch mechanism of chemomechanical coupling in a DNA resecting motor nuclease.

Author

Unciuleac MC, Meir A, Xue C, Warren GM, Greene EC, and Shuman S

Subjects

Adenosine Triphosphate metabolism, Bacterial Proteins chemistry, Bacterial Proteins genetics, Bacterial Proteins metabolism, Cryoelectron Microscopy, DNA Breaks, Double-Stranded, DNA Helicases chemistry, DNA Helicases genetics, DNA Repair, DNA, Single-Stranded metabolism, Endodeoxyribonucleases chemistry, Endodeoxyribonucleases genetics, Hydrolysis, Mutation, Mycobacterium enzymology, Mycobacterium genetics, Protein Binding, Protein Domains, DNA Helicases metabolism, DNA, Bacterial metabolism, Endodeoxyribonucleases metabolism

Abstract

Mycobacterial AdnAB is a heterodimeric helicase-nuclease that initiates homologous recombination by resecting DNA double-strand breaks (DSBs). The N-terminal motor domain of the AdnB subunit hydrolyzes ATP to drive rapid and processive 3' to 5' translocation of AdnAB on the tracking DNA strand. ATP hydrolysis is mechanically productive when oscillating protein domain motions synchronized with the ATPase cycle propel the DNA tracking strand forward by a single-nucleotide step, in what is thought to entail a pawl-and-ratchet-like fashion. By gauging the effects of alanine mutations of the 16 amino acids at the AdnB-DNA interface on DNA-dependent ATP hydrolysis, DNA translocation, and DSB resection in ensemble and single-molecule assays, we gained key insights into which DNA contacts couple ATP hydrolysis to motor activity. The results implicate AdnB Trp325, which intercalates into the tracking strand and stacks on a nucleobase, as the singular essential constituent of the ratchet pawl, without which ATP hydrolysis on ssDNA is mechanically futile. Loss of Thr663 and Thr118 contacts with tracking strand phosphates and of His665 with a nucleobase drastically slows the AdnAB motor during DSB resection. Our findings for AdnAB prompt us to analogize its mechanism to that of an automobile clutch., Competing Interests: The authors declare no competing interest.

Published

2021

30. Zinc finger protein E4F1 cooperates with PARP-1 and BRG1 to promote DNA double-strand break repair.

Author

Moison C, Chagraoui J, Caron MC, Gagné JP, Coulombe Y, Poirier GG, Masson JY, and Sauvageau G

Subjects

Breast Neoplasms genetics, Cell Proliferation, Cell Survival, Chromatin Assembly and Disassembly, DNA Damage, Gene Expression Regulation, Neoplastic, Gene Silencing, Homologous Recombination, Humans, Protein Binding, Repressor Proteins deficiency, Signal Transduction, Ubiquitin-Protein Ligases deficiency, DNA Breaks, Double-Stranded, DNA Helicases metabolism, DNA Repair, Nuclear Proteins metabolism, Poly (ADP-Ribose) Polymerase-1 metabolism, Repressor Proteins metabolism, Transcription Factors metabolism, Ubiquitin-Protein Ligases metabolism

Abstract

Zinc finger (ZnF) proteins represent one of the largest families of human proteins, although most remain uncharacterized. Given that numerous ZnF proteins are able to interact with DNA and poly(ADP ribose), there is growing interest in understanding their mechanism of action in the maintenance of genome integrity. We now report that the ZnF protein E4F transcription factor 1 (E4F1) is an actor in DNA repair. Indeed, E4F1 is rapidly recruited, in a poly(ADP ribose) polymerase (PARP)-dependent manner, to DNA breaks and promotes ATR/CHK1 signaling, DNA-end resection, and subsequent homologous recombination. Moreover, we identify E4F1 as a regulator of the ATP-dependent chromatin remodeling SWI/SNF complex in DNA repair. E4F1 binds to the catalytic subunit BRG1/SMARCA4 and together with PARP-1 mediates its recruitment to DNA lesions. We also report that a proportion of human breast cancers show amplification and overexpression of E4F1 or BRG1 that are mutually exclusive with BRCA1 / 2 alterations. Together, these results reveal a function of E4F1 in the DNA damage response that orchestrates proper signaling and repair of double-strand breaks and document a molecular mechanism for its essential role in maintaining genome integrity and cell survival., Competing Interests: The authors declare no competing interest.

Published

2021

31. The Srs2 helicase dampens DNA damage checkpoint by recycling RPA from chromatin.

Author

Dhingra N, Kuppa S, Wei L, Pokhrel N, Baburyan S, Meng X, Antony E, and Zhao X

Subjects

Chromatin metabolism, DNA Helicases genetics, DNA Repair, DNA, Single-Stranded metabolism, Replication Protein A genetics, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae Proteins genetics, Chromatin genetics, DNA Damage, DNA Helicases metabolism, DNA, Single-Stranded genetics, Replication Protein A metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism

Abstract

The DNA damage checkpoint induces many cellular changes to cope with genotoxic stress. However, persistent checkpoint signaling can be detrimental to growth partly due to blockage of cell cycle resumption. Checkpoint dampening is essential to counter such harmful effects, but its mechanisms remain to be understood. Here, we show that the DNA helicase Srs2 removes a key checkpoint sensor complex, RPA, from chromatin to down-regulate checkpoint signaling in budding yeast. The Srs2 and RPA antagonism is supported by their numerous suppressive genetic interactions. Importantly, moderate reduction of RPA binding to single-strand DNA (ssDNA) rescues hypercheckpoint signaling caused by the loss of Srs2 or its helicase activity. This rescue correlates with a reduction in the accumulated RPA and the associated checkpoint kinase on chromatin in srs2 mutants. Moreover, our data suggest that Srs2 regulation of RPA is separable from its roles in recombinational repair and critically contributes to genotoxin resistance. We conclude that dampening checkpoint by Srs2-mediated RPA recycling from chromatin aids cellular survival of genotoxic stress and has potential implications in other types of DNA transactions., Competing Interests: The authors declare no competing interest.

Published

2021

32. The Cockayne syndrome group A and B proteins are part of a ubiquitin-proteasome degradation complex regulating cell division.

Author

Paccosi E, Costanzo F, Costantino M, Balzerano A, Monteonofrio L, Soddu S, Prantera G, Brancorsini S, Egly JM, and Proietti-De-Santis L

Subjects

DNA Helicases genetics, DNA Repair Enzymes genetics, Fluorescent Antibody Technique, Humans, Mitosis, Poly-ADP-Ribose Binding Proteins genetics, Protein Binding, Protein Transport, Proteolysis, Spindle Apparatus, Transcription Factors genetics, Ubiquitination, Cell Division, DNA Helicases metabolism, DNA Repair Enzymes metabolism, Poly-ADP-Ribose Binding Proteins metabolism, Proteasome Endopeptidase Complex metabolism, Transcription Factors metabolism, Ubiquitin metabolism

Abstract

Cytokinesis is monitored by a molecular machinery that promotes the degradation of the intercellular bridge, a transient protein structure connecting the two daughter cells. Here, we found that CSA and CSB, primarily defined as DNA repair factors, are located at the midbody, a transient structure in the middle of the intercellular bridge, where they recruit CUL4 and MDM2 ubiquitin ligases and the proteasome. As a part of this molecular machinery, CSA and CSB contribute to the ubiquitination and the degradation of proteins such as PRC1, the Protein Regulator of Cytokinesis, to ensure the correct separation of the two daughter cells. Defects in CSA or CSB result in perturbation of the abscission leading to the formation of long intercellular bridges and multinucleated cells, which might explain part of the Cockayne syndrome phenotypes. Our results enlighten the role played by CSA and CSB as part of a ubiquitin/proteasome degradation process involved in transcription, DNA repair, and cell division., Competing Interests: The authors declare no competing interest.

Published

2020

33. CHD7 regulates cardiovascular development through ATP-dependent and -independent activities.

Author

Yan S, Thienthanasit R, Chen D, Engelen E, Brühl J, Crossman DK, Kesterson R, Wang Q, Bouazoune K, and Jiao K

Subjects

Adenosine Triphosphate metabolism, Alleles, Animals, CHARGE Syndrome genetics, Chromatin Assembly and Disassembly genetics, DNA Helicases metabolism, Disease Models, Animal, Embryo, Mammalian metabolism, Gene Expression Regulation, Developmental genetics, Heart Defects, Congenital genetics, Mice, Mice, Knockout, Mutation, Neural Crest embryology, Neural Crest metabolism, Organogenesis physiology, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Heart embryology

Abstract

CHD7 encodes an ATP-dependent chromatin remodeling factor. Mutation of this gene causes multiple developmental disorders, including CHARGE (Coloboma of the eye, Heart defects, Atresia of the choanae, Retardation of growth/development, Genital abnormalities, and Ear anomalies) syndrome, in which conotruncal anomalies are the most prevalent form of heart defects. How CHD7 regulates conotruncal development remains unclear. In this study, we establish that deletion of Chd7 in neural crest cells (NCCs) causes severe conotruncal defects and perinatal lethality, thus providing mouse genetic evidence demonstrating that CHD7 cell-autonomously regulates cardiac NCC development, thereby clarifying a long-standing controversy in the literature. Using transcriptomic analyses, we show that CHD7 fine-tunes the expression of a gene network that is critical for cardiac NCC development. To gain further molecular insights into gene regulation by CHD7, we performed a protein-protein interaction screen by incubating recombinant CHD7 on a protein array. We find that CHD7 directly interacts with several developmental disorder-mutated proteins including WDR5, a core component of H3K4 methyltransferase complexes. This direct interaction suggested that CHD7 may recruit histone-modifying enzymes to target loci independently of its remodeling functions. We therefore generated a mouse model that harbors an ATPase-deficient allele and demonstrates that mutant CHD7 retains the ability to recruit H3K4 methyltransferase activity to its targets. Thus, our data uncover that CHD7 regulates cardiovascular development through ATP-dependent and -independent activities, shedding light on the etiology of CHD7-related congenital disorders. Importantly, our data also imply that patients carrying a premature stop codon versus missense mutations will likely display different molecular alterations; these patients might therefore require personalized therapeutic interventions., Competing Interests: The authors declare no competing interest.

Published

2020

34. Cockayne syndrome B protein acts as an ATP-dependent processivity factor that helps RNA polymerase II overcome nucleosome barriers.

Author

Xu J, Wang W, Xu L, Chen JY, Chong J, Oh J, Leschziner AE, Fu XD, and Wang D

Subjects

Adenosine Triphosphatases genetics, Adenosine Triphosphatases metabolism, DNA Helicases genetics, DNA Repair Enzymes genetics, DNA, Fungal, Escherichia coli, Gene Expression Regulation, Enzymologic, Gene Expression Regulation, Fungal, Models, Molecular, Mutation, Poly-ADP-Ribose Binding Proteins genetics, Protein Conformation, RNA Polymerase II genetics, Saccharomyces cerevisiae Proteins genetics, Saccharomyces cerevisiae Proteins metabolism, Schizosaccharomyces metabolism, Adenosine Triphosphate metabolism, DNA Helicases metabolism, DNA Repair Enzymes metabolism, Nucleosomes metabolism, Poly-ADP-Ribose Binding Proteins metabolism, RNA Polymerase II metabolism

Abstract

While loss-of-function mutations in Cockayne syndrome group B protein (CSB) cause neurological diseases, this unique member of the SWI2/SNF2 family of chromatin remodelers has been broadly implicated in transcription elongation and transcription-coupled DNA damage repair, yet its mechanism remains largely elusive. Here, we use a reconstituted in vitro transcription system with purified polymerase II (Pol II) and Rad26, a yeast ortholog of CSB, to study the role of CSB in transcription elongation through nucleosome barriers. We show that CSB forms a stable complex with Pol II and acts as an ATP-dependent processivity factor that helps Pol II across a nucleosome barrier. This noncanonical mechanism is distinct from the canonical modes of chromatin remodelers that directly engage and remodel nucleosomes or transcription elongation factors that facilitate Pol II nucleosome bypass without hydrolyzing ATP. We propose a model where CSB facilitates gene expression by helping Pol II bypass chromatin obstacles while maintaining their structures., Competing Interests: The authors declare no competing interest.

Published

2020

35. Lsh/HELLS is required for B lymphocyte development and immunoglobulin class switch recombination.

Author

He Y, Ren J, Xu X, Ni K, Schwader A, Finney R, Wang C, Sun L, Klarmann K, Keller J, Tubbs A, Nussenzweig A, and Muegge K

Subjects

Animals, Cell Line, DNA Helicases genetics, Gene Silencing, Humans, Immunoglobulins genetics, Mice, Mice, Knockout, Mutation, B-Lymphocytes physiology, DNA Helicases metabolism, Immunoglobulins metabolism

Abstract

Mutation of HELLS (Helicase, Lymphoid-Specific)/Lsh in human DNA causes a severe immunodeficiency syndrome, but the nature of the defect remains unknown. We assessed here the role of Lsh in hematopoiesis using conditional Lsh knockout mice with expression of Mx1 or Vav Cre-recombinase. Bone marrow transplantation studies revealed that Lsh depletion in hematopoietic stem cells severely reduced B cell numbers and impaired B cell development in a hematopoietic cell-autonomous manner. Lsh-deficient mice without bone marrow transplantation exhibited lower Ig levels in vivo compared to controls despite normal peripheral B cell numbers. Purified B lymphocytes proliferated normally but produced less immunoglobulins in response to in vitro stimulation, indicating a reduced capacity to undergo class switch recombination (CSR). Analysis of germline transcripts, examination of double-stranded breaks using biotin-labeling DNA break assay, and End-seq analysis indicated that the initiation of the recombination process was unscathed. In contrast, digestion-circularization PCR analysis and high-throughput sequencing analyses of CSR junctions and a chromosomal break repair assay indicated an impaired ability of the canonical end-joining pathway in Lsh-deficient B cells. Our data suggest a hematopoietic cell-intrinsic role of Lsh in B cell development and in CSR providing a potential target for immunodeficiency therapy., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

36. Structural mechanism of helicase loading onto replication origin DNA by ORC-Cdc6.

Author

Yuan Z, Schneider S, Dodd T, Riera A, Bai L, Yan C, Magdalou I, Ivanov I, Stillman B, Li H, and Speck C

Subjects

Binding Sites, Cryoelectron Microscopy, Minichromosome Maintenance Complex Component 6 chemistry, Minichromosome Maintenance Complex Component 6 metabolism, Molecular Docking Simulation, Molecular Dynamics Simulation, Origin Recognition Complex, Protein Binding, Protein Conformation, Structure-Activity Relationship, Cell Cycle Proteins chemistry, Cell Cycle Proteins metabolism, DNA Helicases chemistry, DNA Helicases metabolism, DNA Replication, Replication Origin, Saccharomyces cerevisiae Proteins chemistry, Saccharomyces cerevisiae Proteins metabolism

Abstract

DNA replication origins serve as sites of replicative helicase loading. In all eukaryotes, the six-subunit origin recognition complex (Orc1-6; ORC) recognizes the replication origin. During late M-phase of the cell-cycle, Cdc6 binds to ORC and the ORC-Cdc6 complex loads in a multistep reaction and, with the help of Cdt1, the core Mcm2-7 helicase onto DNA. A key intermediate is the ORC-Cdc6-Cdt1-Mcm2-7 (OCCM) complex in which DNA has been already inserted into the central channel of Mcm2-7. Until now, it has been unclear how the origin DNA is guided by ORC-Cdc6 and inserted into the Mcm2-7 hexamer. Here, we truncated the C-terminal winged-helix-domain (WHD) of Mcm6 to slow down the loading reaction, thereby capturing two loading intermediates prior to DNA insertion in budding yeast. In "semi-attached OCCM," the Mcm3 and Mcm7 WHDs latch onto ORC-Cdc6 while the main body of the Mcm2-7 hexamer is not connected. In "pre-insertion OCCM," the main body of Mcm2-7 docks onto ORC-Cdc6, and the origin DNA is bent and positioned adjacent to the open DNA entry gate, poised for insertion, at the Mcm2-Mcm5 interface. We used molecular simulations to reveal the dynamic transition from preloading conformers to the loaded conformers in which the loading of Mcm2-7 on DNA is complete and the DNA entry gate is fully closed. Our work provides multiple molecular insights into a key event of eukaryotic DNA replication., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

37. Epstein-Barr virus co-opts TFIIH component XPB to specifically activate essential viral lytic promoters.

Author

Verma D, Church TM, and Swaminathan S

Subjects

Cell Line, Tumor, DNA Helicases genetics, DNA-Binding Proteins genetics, Epstein-Barr Virus Infections drug therapy, Epstein-Barr Virus Infections virology, Gene Expression Regulation, Viral drug effects, Humans, Promoter Regions, Genetic genetics, Proteolysis drug effects, RNA, Small Interfering metabolism, Spironolactone pharmacology, Spironolactone therapeutic use, Transcriptional Activation drug effects, Virion drug effects, Virion metabolism, DNA Helicases metabolism, DNA-Binding Proteins metabolism, Herpesvirus 4, Human genetics, Host-Pathogen Interactions genetics, Phosphoproteins metabolism, Trans-Activators metabolism

Abstract

Epstein-Barr virus (EBV) is associated with epithelial and lymphoid malignancies, establishes latent infection in memory B cells, and intermittently produces infectious virions through lytic replication. Released virions play a key role in latent reservoir maintenance and transmission. Lytic EBV transcription differs from cellular transcription in requiring a virus-encoded preinitiation complex that binds to TATT motifs unique to EBV late lytic promoters. Expression of 15 late lytic genes that are important for virion production and infectivity is particularly dependent on the EBV SM protein, a nuclear protein expressed early during lytic reactivation that binds to viral RNAs and enhances RNA stability. We recently discovered that spironolactone blocks EBV virion production by inhibiting EBV SM function. Since spironolactone causes degradation of xeroderma pigmentosum group B-complementing protein (XPB), a component of human transcription factor TFIIH, in both B lymphocytes and epithelial cells, we hypothesized that SM utilizes XPB to specifically activate transcription of SM target promoters. While EBV SM has been thought to act posttranscriptionally, we provide evidence that SM also facilitates EBV gene transcription. We demonstrate that SM binds and recruits XPB to EBV promoters during lytic replication. Depletion of XPB protein, by spironolactone treatment or by siRNA transfection, inhibits SM-dependent late lytic gene transcription but not transcription of other EBV genes or cellular genes. These data indicate that SM acts as a transcriptional activator that has co-opted XPB to specifically target 15 EBV promoters that have uniquely evolved to require XPB for activity, providing an additional mechanism to differentially regulate EBV gene expression., Competing Interests: The authors declare no competing interest.

Published

2020

38. Direct observation of helicase-topoisomerase coupling within reverse gyrase.

Author

Yang X, Garnier F, Débat H, Strick TR, and Nadal M

Subjects

Adenosine Triphosphate metabolism, DNA, Bacterial metabolism, DNA-Binding Proteins metabolism, Models, Molecular, Protein Conformation, Protein Domains, Thermus genetics, DNA metabolism, DNA Helicases metabolism, DNA Topoisomerases metabolism, DNA Topoisomerases, Type I metabolism

Abstract

Reverse gyrases (RGs) are the only topoisomerases capable of generating positive supercoils in DNA. Members of the type IA family, they do so by generating a single-strand break in substrate DNA and then manipulating the two single strands to generate positive topology. Here, we use single-molecule experimentation to reveal the obligatory succession of steps that make up the catalytic cycle of RG. In the initial state, RG binds to DNA and unwinds ∼2 turns of the double helix in an ATP-independent fashion. Upon nucleotide binding, RG then rewinds ∼1 turn of DNA. Nucleotide hydrolysis and/or product release leads to an increase of 2 units of DNA writhe and resetting of the enzyme, for a net change of topology of +1 turn per cycle. Final dissociation of RG from DNA results in rewinding of the 2 turns of DNA that were initially disrupted. These results show how tight coupling of the helicase and topoisomerase activities allows for induction of positive supercoiling despite opposing torque., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

39. CtIP promotes the motor activity of DNA2 to accelerate long-range DNA end resection.

Author

Ceppi I, Howard SM, Kasaciunaite K, Pinto C, Anand R, Seidel R, and Cejka P

Subjects

Acid Anhydride Hydrolases metabolism, Adenosine Triphosphate metabolism, Animals, Cell Cycle Proteins metabolism, DNA Breaks, Double-Stranded, DNA-Binding Proteins metabolism, Enzyme Assays, Hydrolysis, MRE11 Homologue Protein metabolism, Nuclear Proteins metabolism, Protein Domains, Recombinant Proteins metabolism, Sf9 Cells, DNA Helicases metabolism, DNA, Single-Stranded metabolism, Endodeoxyribonucleases metabolism, Recombinational DNA Repair

Abstract

To repair a DNA double-strand break by homologous recombination, 5'-terminated DNA strands must first be resected to reveal 3'-overhangs. This process is initiated by a short-range resection catalyzed by MRE11-RAD50-NBS1 (MRN) stimulated by CtIP, which is followed by a long-range step involving EXO1 or DNA2 nuclease. DNA2 is a bifunctional enzyme that contains both single-stranded DNA (ssDNA)-specific nuclease and motor activities. Upon DNA unwinding by Bloom (BLM) or Werner (WRN) helicase, RPA directs the DNA2 nuclease to degrade the 5'-strand. RPA bound to ssDNA also represents a barrier, explaining the need for the motor activity of DNA2 to displace RPA prior to resection. Using ensemble and single-molecule biochemistry, we show that CtIP also dramatically stimulates the adenosine 5'-triphosphate (ATP) hydrolysis-driven motor activity of DNA2 involved in the long-range resection step. This activation in turn strongly promotes the degradation of RPA-coated ssDNA by DNA2. Accordingly, the stimulatory effect of CtIP is only observed with wild-type DNA2, but not the helicase-deficient variant. Similarly to the function of CtIP to promote MRN, also the DNA2 stimulatory effect is facilitated by CtIP phosphorylation. The domain of CtIP required to promote DNA2 is located in the central region lacking in lower eukaryotes and is fully separable from domains involved in the stimulation of MRN. These results establish how CtIP couples both MRE11-dependent short-range and DNA2-dependent long-range resection and define the involvement of the motor activity of DNA2 in this process. Our data might help explain the less severe resection defects of MRE11 nuclease-deficient cells compared to those lacking CtIP., Competing Interests: The authors declare no competing interest.

Published

2020

40. Caenorhabditis elegans ADAR editing and the ERI-6/7/MOV10 RNAi pathway silence endogenous viral elements and LTR retrotransposons.

Author

Fischer SEJ and Ruvkun G

Subjects

Adenosine Deaminase genetics, Adenosine Deaminase metabolism, Animals, Caenorhabditis elegans virology, Caenorhabditis elegans Proteins metabolism, DNA Helicases metabolism, DNA, Viral metabolism, Endoplasmic Reticulum Stress genetics, Gene Expression Regulation, Viral, Genes, Viral genetics, Humans, RNA, Double-Stranded metabolism, RNA, Viral metabolism, Sequence Homology, Amino Acid, Terminal Repeat Sequences genetics, Unfolded Protein Response genetics, Caenorhabditis elegans genetics, Endogenous Retroviruses genetics, Host Microbial Interactions genetics, RNA Interference, Retroelements genetics

Abstract

Endogenous retroviruses and long terminal repeat (LTR) retrotransposons are mobile genetic elements that are closely related to retroviruses. Desilenced endogenous retroviruses are associated with human autoimmune disorders and neurodegenerative diseases. Caenorhabditis elegans and related Caenorhabditis spp. contain LTR retrotransposons and, as described here, numerous integrated viral genes including viral envelope genes that are part of LTR retrotransposons. We found that both LTR retrotransposons and endogenous viral elements are silenced by ADARs [adenosine deaminases acting on double-stranded RNA (dsRNA)] together with the endogenous RNA interference (RNAi) factor ERI-6/7, a homolog of MOV10 helicase, a retrotransposon and retrovirus restriction factor in human. siRNAs corresponding to integrated viral genes and LTR retrotransposons, but not to DNA transposons, are dependent on the ADARs and ERI-6/7. siRNAs corresponding to palindromic repeats are independent of the ADARs and ERI-6/7, and are in fact increased in adar- and eri-6/7- defective mutants because of an antiviral RNAi response to dsRNA. Silencing of LTR retrotransposons is dependent on downstream RNAi factors and P granule components but is independent of the viral sensor DRH-1/RIG-I and the nuclear Argonaute NRDE-3. The activation of retrotransposons in the ADAR- and ERI-6/7/MOV10-defective mutant is associated with the induction of the unfolded protein response (UPR), a common response to viral infection. The overlap between genes induced upon viral infection and infection with intracellular pathogens and genes coexpressed with retrotransposons suggests that there is a common response to different types of foreign elements that includes a response to proteotoxicity presumably caused by the burden of replicating pathogens and expressed retrotransposons., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

41. Multivalent interaction of ESCO2 with the replication machinery is required for sister chromatid cohesion in vertebrates.

Author

Bender D, Da Silva EML, Chen J, Poss A, Gawey L, Rulon Z, and Rankin S

Subjects

Animals, Cell Cycle Proteins metabolism, Chondroitin Sulfate Proteoglycans metabolism, DNA Helicases metabolism, HeLa Cells, Humans, Nuclear Proteins metabolism, Proliferating Cell Nuclear Antigen metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism, Vertebrates genetics, Cohesins, Acetyltransferases metabolism, Chromatids metabolism, Chromosomal Proteins, Non-Histone metabolism, Chromosome Segregation physiology, DNA Replication physiology

Abstract

The tethering together of sister chromatids by the cohesin complex ensures their accurate alignment and segregation during cell division. In vertebrates, sister chromatid cohesion requires the activity of the ESCO2 acetyltransferase, which modifies the Smc3 subunit of cohesin. It was shown recently that ESCO2 promotes cohesion through interaction with the MCM replicative helicase. However, ESCO2 does not significantly colocalize with the MCM complex, suggesting there are additional interactions important for ESCO2 function. Here we show that ESCO2 is recruited to replication factories, sites of DNA replication, through interaction with PCNA. We show that ESCO2 contains multiple PCNA-interaction motifs in its N terminus, each of which is essential to its ability to establish cohesion. We propose that multiple PCNA-interaction motifs embedded in a largely flexible and disordered region of the protein underlie the unique ability of ESCO2 to establish cohesion between sister chromatids precisely as they are born during DNA replication., Competing Interests: The authors declare no competing interest.

Published

2020

42. Branched unwinding mechanism of the Pif1 family of DNA helicases.

Author

Singh SP, Soranno A, Sparks MA, and Galletto R

Subjects

Adenosine Triphosphate metabolism, DNA chemistry, DNA metabolism, Fluorescence Resonance Energy Transfer, Kinetics, Saccharomyces cerevisiae chemistry, Schizosaccharomyces chemistry, DNA Helicases chemistry, DNA Helicases metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins chemistry, Saccharomyces cerevisiae Proteins metabolism, Schizosaccharomyces metabolism, Schizosaccharomyces pombe Proteins chemistry, Schizosaccharomyces pombe Proteins metabolism

Abstract

Members of the Pif1 family of helicases function in multiple pathways that involve DNA synthesis: DNA replication across G-quadruplexes; break-induced replication; and processing of long flaps during Okazaki fragment maturation. Furthermore, Pif1 increases strand-displacement DNA synthesis by DNA polymerase δ and allows DNA replication across arrays of proteins tightly bound to DNA. This is a surprising feat since DNA rewinding or annealing activities limit the amount of single-stranded DNA product that Pif1 can generate, leading to an apparently poorly processive helicase. In this work, using single-molecule Förster resonance energy transfer approaches, we show that 2 members of the Pif1 family of helicases, Pif1 from Saccharomyces cerevisiae and Pfh1 from Schizosaccharomyces pombe , unwind double-stranded DNA by a branched mechanism with 2 modes of activity. In the dominant mode, only short stretches of DNA can be processively and repetitively opened, with reclosure of the DNA occurring by mechanisms other than strand-switching. In the other less frequent mode, longer stretches of DNA are unwound via a path that is separate from the one leading to repetitive unwinding. Analysis of the kinetic partitioning between the 2 different modes suggests that the branching point in the mechanism is established by conformational selection, controlled by the interaction of the helicase with the 3' nontranslocating strand. The data suggest that the dominant and repetitive mode of DNA opening of the helicase can be used to allow efficient DNA replication, with DNA synthesis on the nontranslocating strand rectifying the DNA unwinding activity., Competing Interests: The authors declare no competing interest.

Published

2019

43. Asymmetric base-pair opening drives helicase unwinding dynamics.

Author

Colizzi F, Perez-Gonzalez C, Fritzen R, Levy Y, White MF, Penedo JC, and Bussi G

Subjects

Bacteria enzymology, Bacteria genetics, Bacteria metabolism, Bacterial Proteins genetics, Base Pairing, Base Sequence, DNA Helicases genetics, DNA, Bacterial chemistry, Kinetics, RNA, Bacterial genetics, RNA, Bacterial metabolism, Bacterial Proteins metabolism, DNA Helicases metabolism, DNA, Bacterial genetics

Abstract

The opening of a Watson-Crick double helix is required for crucial cellular processes, including replication, repair, and transcription. It has long been assumed that RNA or DNA base pairs are broken by the concerted symmetric movement of complementary nucleobases. By analyzing thousands of base-pair opening and closing events from molecular simulations, here, we uncover a systematic stepwise process driven by the asymmetric flipping-out probability of paired nucleobases. We demonstrate experimentally that such asymmetry strongly biases the unwinding efficiency of DNA helicases toward substrates that bear highly dynamic nucleobases, such as pyrimidines, on the displaced strand. Duplex substrates with identical thermodynamic stability are thus shown to be more easily unwound from one side than the other, in a quantifiable and predictable manner. Our results indicate a possible layer of gene regulation coded in the direction-dependent unwindability of the double helix., Competing Interests: The authors declare no competing interest., (Copyright © 2019 the Author(s). Published by PNAS.)

Published

2019

44. Replication fork stalling elicits chromatin compaction for the stability of stalling replication forks.

Author

Feng G, Yuan Y, Li Z, Wang L, Zhang B, Luo J, Ji J, and Kong D

Subjects

Acetylation, DNA Helicases metabolism, DNA Methylation genetics, DNA-Directed DNA Polymerase metabolism, Histone Code genetics, Histones metabolism, Nucleosomes genetics, S Phase Cell Cycle Checkpoints, Schizosaccharomyces metabolism, Schizosaccharomyces pombe Proteins metabolism, DNA Replication, Nucleosomes metabolism, Schizosaccharomyces genetics

Abstract

DNA replication forks in eukaryotic cells stall at a variety of replication barriers. Stalling forks require strict cellular regulations to prevent fork collapse. However, the mechanism underlying these cellular regulations is poorly understood. In this study, a cellular mechanism was uncovered that regulates chromatin structures to stabilize stalling forks. When replication forks stall, H2BK33, a newly identified acetylation site, is deacetylated and H3K9 trimethylated in the nucleosomes surrounding stalling forks, which results in chromatin compaction around forks. Acetylation-mimic H2BK33Q and its deacetylase clr6 - 1 mutations compromise this fork stalling-induced chromatin compaction, cause physical separation of replicative helicase and DNA polymerases, and significantly increase the frequency of stalling fork collapse. Furthermore, this fork stalling-induced H2BK33 deacetylation is independent of checkpoint. In summary, these results suggest that eukaryotic cells have developed a cellular mechanism that stabilizes stalling forks by targeting nucleosomes and inducing chromatin compaction around stalling forks. This mechanism is named the "Chromsfork" control: Chromatin Compaction Stabilizes Stalling Replication Forks., Competing Interests: The authors declare no conflict of interest.

Published

2019

45. Molecular basis of chromatin remodeling by Rhp26, a yeast CSB ortholog.

Author

Wang W, Xu J, Limbo O, Fei J, Kassavetis GA, Chong J, Kadonaga JT, Russell P, Li B, and Wang D

Subjects

Chromatin metabolism, DNA Repair, Epitopes, Histones metabolism, Schizosaccharomyces, Chromatin Assembly and Disassembly, DNA Helicases metabolism, Schizosaccharomyces pombe Proteins metabolism

Abstract

CSB/ERCC6 belongs to an orphan subfamily of SWI2/SNF2-related chromatin remodelers and plays crucial roles in gene expression, DNA damage repair, and the maintenance of genome integrity. The molecular basis of chromatin remodeling by Cockayne syndrome B protein (CSB) is not well understood. Here we investigate the molecular mechanism of chromatin remodeling by Rhp26, a Schizosaccharomyces pombe CSB ortholog. The molecular basis of chromatin remodeling and nucleosomal epitope recognition by Rhp26 is distinct from that of canonical chromatin remodelers, such as imitation switch protein (ISWI). We reveal that the remodeling activities are bidirectionally regulated by CSB-specific motifs: the N-terminal leucine-latch motif and the C-terminal coupling motif. Rhp26 remodeling activities depend mainly on H4 tails and to a lesser extent on H3 tails, but not on H2A and H2B tails. Rhp26 promotes the disruption of histone cores and the release of free DNA. Finally, we dissected the distinct contributions of two Rhp26 C-terminal regions to chromatin remodeling and DNA damage repair., Competing Interests: The authors declare no conflict of interest.

Published

2019

46. Regulatory control of Sgs1 and Dna2 during eukaryotic DNA end resection.

Author

Xue C, Wang W, Crickard JB, Moevus CJ, Kwon Y, Sung P, and Greene EC

Subjects

Homologous Recombination, Nucleosomes metabolism, Replication Protein A metabolism, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae metabolism, Single Molecule Imaging methods, DNA Breaks, Double-Stranded, DNA Helicases metabolism, DNA Repair, RecQ Helicases metabolism, Saccharomyces cerevisiae Proteins metabolism

Abstract

In the repair of DNA double-strand breaks by homologous recombination, the DNA break ends must first be processed into 3' single-strand DNA overhangs. In budding yeast, end processing requires the helicase Sgs1 (BLM in humans), the nuclease/helicase Dna2, Top3-Rmi1, and replication protein A (RPA). Here, we use single-molecule imaging to visualize Sgs1-dependent end processing in real-time. We show that Sgs1 is recruited to DNA ends through Top3-Rmi1-dependent or -independent means, and in both cases Sgs1 is maintained in an immoble state at the DNA ends. Importantly, the addition of Dna2 triggers processive Sgs1 translocation, but DNA resection only occurs when RPA is also present. We also demonstrate that the Sgs1-Dna2-Top3-Rmi1-RPA ensemble can efficiently disrupt nucleosomes, and that Sgs1 itself possesses nucleosome remodeling activity. Together, these results shed light on the regulatory interplay among conserved protein factors that mediate the nucleolytic processing of DNA ends in preparation for homologous recombination-mediated chromosome damage repair., Competing Interests: The authors declare no conflict of interest.

Published

2019

47. Glial ensheathment of the somatodendritic compartment regulates sensory neuron structure and activity.

Author

Yadav S, Younger SH, Zhang L, Thompson-Peer KL, Li T, Jan LY, and Jan YN

Subjects

Animals, Axons metabolism, Axons radiation effects, Caspases metabolism, DNA Helicases metabolism, Dendrites radiation effects, Drosophila Proteins metabolism, Enzyme Activation radiation effects, Light, Neuroglia radiation effects, Sensory Receptor Cells radiation effects, Dendrites metabolism, Drosophila melanogaster metabolism, Neuroglia metabolism, Sensory Receptor Cells cytology, Sensory Receptor Cells metabolism

Abstract

Sensory neurons perceive environmental cues and are important of organismal survival. Peripheral sensory neurons interact intimately with glial cells. While the function of axonal ensheathment by glia is well studied, less is known about the functional significance of glial interaction with the somatodendritic compartment of neurons. Herein, we show that three distinct glia cell types differentially wrap around the axonal and somatodendritic surface of the polymodal dendritic arborization (da) neuron of the Drosophila peripheral nervous system for detection of thermal, mechanical, and light stimuli. We find that glial cell-specific loss of the chromatin modifier gene dATRX in the subperineurial glial layer leads to selective elimination of somatodendritic glial ensheathment, thus allowing us to investigate the function of such ensheathment. We find that somatodendritic glial ensheathment regulates the morphology of the dendritic arbor, as well as the activity of the sensory neuron, in response to sensory stimuli. Additionally, glial ensheathment of the neuronal soma influences dendritic regeneration after injury., Competing Interests: The authors declare no conflict of interest.

Published

2019

48. Dual inhibition of MDM2 and MDM4 in virus-positive Merkel cell carcinoma enhances the p53 response.

Author

Park DE, Cheng J, Berrios C, Montero J, Cortés-Cros M, Ferretti S, Arora R, Tillgren ML, Gokhale PC, and DeCaprio JA

Subjects

Carcinoma, Merkel Cell genetics, Carcinoma, Merkel Cell pathology, Carcinoma, Merkel Cell virology, Cell Cycle Proteins, DNA Helicases genetics, DNA Helicases metabolism, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Humans, Merkel cell polyomavirus genetics, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins genetics, Polyomavirus Infections genetics, Polyomavirus Infections pathology, Proto-Oncogene Proteins antagonists & inhibitors, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-mdm2 antagonists & inhibitors, Proto-Oncogene Proteins c-mdm2 genetics, Retinoblastoma Binding Proteins genetics, Retinoblastoma Binding Proteins metabolism, Tumor Suppressor Protein p53 genetics, Tumor Virus Infections genetics, Tumor Virus Infections pathology, Ubiquitin-Protein Ligases genetics, Ubiquitin-Protein Ligases metabolism, Carcinoma, Merkel Cell metabolism, Merkel cell polyomavirus metabolism, Nuclear Proteins metabolism, Polyomavirus Infections metabolism, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-mdm2 metabolism, Tumor Suppressor Protein p53 metabolism, Tumor Virus Infections metabolism

Abstract

Merkel cell polyomavirus (MCV) contributes to approximately 80% of all Merkel cell carcinomas (MCCs), a highly aggressive neuroendocrine carcinoma of the skin. MCV-positive MCC expresses small T antigen (ST) and a truncated form of large T antigen (LT) and usually contains wild-type p53 (TP53) and RB (RB1). In contrast, virus-negative MCC contains inactivating mutations in TP53 and RB1. While the MCV-truncated LT can bind and inhibit RB, it does not bind p53. We report here that MCV LT binds to RB, leading to increased levels of ARF, an inhibitor of MDM2, and activation of p53. However, coexpression of ST reduced p53 activation. MCV ST recruits the MYC homologue MYCL (L-Myc) to the EP400 chromatin remodeler complex and transactivates specific target genes. We observed that depletion of EP400 in MCV-positive MCC cell lines led to increased p53 target gene expression. We suspected that the MCV ST-MYCL-EP400 complex could functionally inactivate p53, but the underlying mechanism was not known. Integrated ChIP and RNA-sequencing analysis following EP400 depletion identified MDM2 as well as CK1α, an activator of MDM4, as target genes of the ST-MYCL-EP400 complex. In addition, MCV-positive MCC cells expressed high levels of MDM4. Combining MDM2 inhibitors with lenalidomide targeting CK1α or an MDM4 inhibitor caused synergistic activation of p53, leading to an apoptotic response in MCV-positive MCC cells and MCC-derived xenografts in mice. These results support dual targeting of MDM2 and MDM4 in virus-positive MCC and other p53 wild-type tumors., Competing Interests: Conflict of interest statement: M.C.-C. and S.F. are employed by Novartis Institute for Biomedical Research. R.A. was supported by Wellcome Trust DBT India Alliance Early Career Fellowship IA/E/14/1/501773. A patent was filed with the related work.

Published

2019

49. Mcm10 has potent strand-annealing activity and limits translocase-mediated fork regression.

Author

Mayle R, Langston L, Molloy KR, Zhang D, Chait BT, and O'Donnell ME

Subjects

Humans, Mass Spectrometry, Replication Protein A metabolism, DNA metabolism, DNA Helicases metabolism, DNA Replication, Minichromosome Maintenance Proteins metabolism, Saccharomyces cerevisiae Proteins metabolism

Abstract

The 11-subunit eukaryotic replicative helicase CMG (Cdc45, Mcm2-7, GINS) tightly binds Mcm10, an essential replication protein in all eukaryotes. Here we show that Mcm10 has a potent strand-annealing activity both alone and in complex with CMG. CMG-Mcm10 unwinds and then reanneals single strands soon after they have been unwound in vitro. Given the DNA damage and replisome instability associated with loss of Mcm10 function, we examined the effect of Mcm10 on fork regression. Fork regression requires the unwinding and pairing of newly synthesized strands, performed by a specialized class of ATP-dependent DNA translocases. We show here that Mcm10 inhibits fork regression by the well-known fork reversal enzyme SMARCAL1. We propose that Mcm10 inhibits the unwinding of nascent strands to prevent fork regression at normal unperturbed replication forks, either by binding the fork junction to form a block to SMARCAL1 or by reannealing unwound nascent strands to their parental template. Analysis of the CMG-Mcm10 complex by cross-linking mass spectrometry reveals Mcm10 interacts with six CMG subunits, with the DNA-binding region of Mcm10 on the N-face of CMG. This position on CMG places Mcm10 at the fork junction, consistent with a role in regulating fork regression., Competing Interests: The authors declare no conflict of interest., (Copyright © 2019 the Author(s). Published by PNAS.)

Published

2019

50. Meiosis-specific recombinase Dmc1 is a potent inhibitor of the Srs2 antirecombinase.

Author

Crickard JB, Kaniecki K, Kwon Y, Sung P, and Greene EC

Subjects

Adenosine Triphosphate metabolism, Chromosome Segregation drug effects, Homologous Recombination drug effects, Cell Cycle Proteins metabolism, DNA Helicases metabolism, DNA-Binding Proteins metabolism, Meiosis drug effects, Recombinases metabolism, Saccharomyces cerevisiae metabolism, Saccharomyces cerevisiae Proteins metabolism

Abstract

Cross-over recombination products are a hallmark of meiosis because they are necessary for accurate chromosome segregation and they also allow for increased genetic diversity during sexual reproduction. However, cross-overs can also cause gross chromosomal rearrangements and are therefore normally down-regulated during mitotic growth. The mechanisms that enhance cross-over product formation upon entry into meiosis remain poorly understood. In Saccharomyces cerevisiae , the Superfamily 1 (Sf1) helicase Srs2, which is an ATP hydrolysis-dependent motor protein that actively dismantles recombination intermediates, promotes synthesis-dependent strand annealing, the result of which is a reduction in cross-over recombination products. Here, we show that the meiosis-specific recombinase Dmc1 is a potent inhibitor of Srs2. Biochemical and single-molecule assays demonstrate that Dmc1 acts by inhibiting Srs2 ATP hydrolysis activity, which prevents the motor protein from undergoing ATP hydrolysis-dependent translocation on Dmc1-bound recombination intermediates. We propose a model in which Dmc1 helps contribute to cross-over formation during meiosis by antagonizing the antirecombinase activity of Srs2., Competing Interests: The authors declare no conflict of interest.

Published

2018