Your search keyword '"Robert M. Brosh"' showing total 46 results

1. Replication stress as a driver of cellular senescence and aging

Author

Lauren M. Herr, Ethan D. Schaffer, Kathleen F. Fuchs, Arindam Datta, and Robert M. Brosh

Subjects

Biology (General), QH301-705.5

Abstract

Abstract Replication stress refers to slowing or stalling of replication fork progression during DNA synthesis that disrupts faithful copying of the genome. While long considered a nexus for DNA damage, the role of replication stress in aging is under-appreciated. The consequential role of replication stress in promotion of organismal aging phenotypes is evidenced by an extensive list of hereditary accelerated aging disorders marked by molecular defects in factors that promote replication fork progression and operate uniquely in the replication stress response. Additionally, recent studies have revealed cellular pathways and phenotypes elicited by replication stress that align with designated hallmarks of aging. Here we review recent advances demonstrating the role of replication stress as an ultimate driver of cellular senescence and aging. We discuss clinical implications of the intriguing links between cellular senescence and aging including application of senotherapeutic approaches in the context of replication stress.

Published

2024

2. Editorial: DNA repair and interventions in aging

Author

Robert M. Brosh, Alexey Moskalev, and Vera Gorbunova

Subjects

DNA repair, aging, epigenetic, oxidative stress, cockayne syndrome, NAD+, Geriatrics, RC952-954.6

Published

2023

3. Frontiers in aging special issue: DNA repair and interventions in aging perspective on 'loss of epigenetic information as a cause of mammalian aging'

Author

Ethan D. Schaffer, Isabel Beerman, Rafael de Cabo, and Robert M. Brosh

Subjects

aging, epigenetic, healthspan, mouse, genetic, double-strand break, Geriatrics, RC952-954.6

Abstract

The recently published article in Cell by the Sinclair lab and collaborators entitled “Loss of Epigenetic Information as a Cause of Mammalian Aging” [1] implicates heritable changes in gene expression as the basis for aging, a postulate consistent with the emerging information theory of aging. Sinclair’s group and colleagues induced epigenetic changes, i.e., DNA and histone modifications, via double-strand breaks (DSBs) catalyzed by the I-Pol endonuclease at specific genomic loci. The genomic DNA breaks, introduced without inducing insertion or deletion mutations (indels) in a mouse model, were targeted to 19 non-coding regions and one region in ribosomal DNA (rDNA), the latter shown to not have a significant effect on the function or transcription of rDNA [1]. With that experimental model in place, the authors present experimental evidence supporting a model that epigenetic changes drive aging via this inducible DNA break mechanism. After demonstrating the phenotypic alterations of this accelerated aging, they attempt to reverse selective phenotypes by resetting the altered epigenetic landscape. Establishing a causal relationship between epigenetic changes and aging, and how this connection might be manipulated to overturn cellular features of aging, is provocative and merits further study.

Published

2023

4. WRN helicase safeguards deprotected replication forks in BRCA2-mutated cancer cells

Author

Arindam Datta, Kajal Biswas, Joshua A. Sommers, Haley Thompson, Sanket Awate, Claudia M. Nicolae, Tanay Thakar, George-Lucian Moldovan, Robert H. Shoemaker, Shyam K. Sharan, and Robert M. Brosh

Subjects

Science

Abstract

The tumor suppressor BRCA2 protects stalled DNA replication forks from unrestrained degradation; however the mechanism whereby unprotected stalled forks are preserved and restarted has remained elusive. Here the authors show that the WRN helicase promotes stalled fork recovery and limits fork hyper-degradation in the absence of BRCA2 protection.

Published

2021

5. RECON syndrome is a genome instability disorder caused by mutations in the DNA helicase RECQL1

Author

Bassam Abu-Libdeh, Satpal S. Jhujh, Srijita Dhar, Joshua A. Sommers, Arindam Datta, Gabriel M.C. Longo, Laura J. Grange, John J. Reynolds, Sophie L. Cooke, Gavin S. McNee, Robert Hollingworth, Beth L. Woodward, Anil N. Ganesh, Stephen J. Smerdon, Claudia M. Nicolae, Karina Durlacher-Betzer, Vered Molho-Pessach, Abdulsalam Abu-Libdeh, Vardiella Meiner, George-Lucian Moldovan, Vassilis Roukos, Tamar Harel, Robert M. Brosh Jr., and Grant S. Stewart

Subjects

Cell biology, Genetics, Medicine

Abstract

Despite being the first homolog of the bacterial RecQ helicase to be identified in humans, the function of RECQL1 remains poorly characterized. Furthermore, unlike other members of the human RECQ family of helicases, mutations in RECQL1 have not been associated with a genetic disease. Here, we identify 2 families with a genome instability disorder that we have named RECON (RECql ONe) syndrome, caused by biallelic mutations in the RECQL gene. The affected individuals had short stature, progeroid facial features, a hypoplastic nose, xeroderma, and skin photosensitivity and were homozygous for the same missense mutation in RECQL1 (p.Ala459Ser), located within its zinc binding domain. Biochemical analysis of the mutant RECQL1 protein revealed that the p.A459S missense mutation compromised its ATPase, helicase, and fork restoration activity, while its capacity to promote single-strand DNA annealing was largely unaffected. At the cellular level, this mutation in RECQL1 gave rise to a defect in the ability to repair DNA damage induced by exposure to topoisomerase poisons and a failure of DNA replication to progress efficiently in the presence of abortive topoisomerase lesions. Taken together, RECQL1 is the fourth member of the RecQ family of helicases to be associated with a human genome instability disorder.

Published

2022

6. Special Issue: DNA Helicases: Mechanisms, Biological Pathways, and Disease Relevance

Author

Robert M. Brosh

Subjects

helicase, replication, DNA repair, recombination, transcription, DNA structure, Genetics, QH426-470

Abstract

DNA helicases have emerged as a prominent class of nucleic acid-metabolizing enzymes that play important roles in genome maintenance and cellular homeostasis [...]

Published

2021

7. CDK1 phosphorylates WRN at collapsed replication forks

Author

Valentina Palermo, Sara Rinalducci, Massimo Sanchez, Francesca Grillini, Joshua A. Sommers, Robert M. Brosh, Lello Zolla, Annapaola Franchitto, and Pietro Pichierri

Subjects

Science

Abstract

End-resection of double strand DNA breaks is essential for pathway choice between non-homologous end-joining and homologous recombination. Here the authors show that phosphorylation of WRN helicase by CDK1 is essential for resection at replication-related breaks.

Published

2016

8. History of DNA Helicases

Author

Robert M. Brosh and Steven W. Matson

Subjects

helicase, dna replication, dna repair, recombination, transcription, nucleic acid metabolism, molecular biology, human disease, genomic instability, science education, Genetics, QH426-470

Abstract

Since the discovery of the DNA double helix, there has been a fascination in understanding the molecular mechanisms and cellular processes that account for: (i) the transmission of genetic information from one generation to the next and (ii) the remarkable stability of the genome. Nucleic acid biologists have endeavored to unravel the mysteries of DNA not only to understand the processes of DNA replication, repair, recombination, and transcription but to also characterize the underlying basis of genetic diseases characterized by chromosomal instability. Perhaps unexpectedly at first, DNA helicases have arisen as a key class of enzymes to study in this latter capacity. From the first discovery of ATP-dependent DNA unwinding enzymes in the mid 1970’s to the burgeoning of helicase-dependent pathways found to be prevalent in all kingdoms of life, the story of scientific discovery in helicase research is rich and informative. Over four decades after their discovery, we take this opportunity to provide a history of DNA helicases. No doubt, many chapters are left to be written. Nonetheless, at this juncture we are privileged to share our perspective on the DNA helicase field − where it has been, its current state, and where it is headed.

Published

2020

9. New Insights Into DNA Helicases as Druggable Targets for Cancer Therapy

Author

Arindam Datta and Robert M. Brosh

Subjects

helicase, DNA repair, replication, genomic instability, small molecule, therapy, Biology (General), QH301-705.5

Abstract

Small molecules that deter the functions of DNA damage response machinery are postulated to be useful for enhancing the DNA damaging effects of chemotherapy or ionizing radiation treatments to combat cancer by impairing the proliferative capacity of rapidly dividing cells that accumulate replicative lesions. Chemically induced or genetic synthetic lethality is a promising area in personalized medicine, but it remains to be optimized. A new target in cancer therapy is DNA unwinding enzymes known as helicases. Helicases play critical roles in all aspects of nucleic acid metabolism. We and others have investigated small molecule targeted inhibition of helicase function by compound screens using biochemical and cell-based approaches. Small molecule-induced trapping of DNA helicases may represent a generalized mechanism exemplified by certain topoisomerase and PARP inhibitors that exert poisonous consequences, especially in rapidly dividing cancer cells. Taking the lead from the broader field of DNA repair inhibitors and new information gleaned from structural and biochemical studies of DNA helicases, we predict that an emerging strategy to identify useful helicase-interacting compounds will be structure-based molecular docking interfaced with a computational approach. Potency, specificity, drug resistance, and bioavailability of helicase inhibitor drugs and targeting such compounds to subcellular compartments where the respective helicases operate must be addressed. Beyond cancer therapy, continued and new developments in this area may lead to the discovery of helicase-interacting compounds that chemically rescue clinically relevant helicase missense mutant proteins or activate the catalytic function of wild-type DNA helicases, which may have novel therapeutic application.

Published

2018

10. Protein Degradation Pathways Regulate the Functions of Helicases in the DNA Damage Response and Maintenance of Genomic Stability

Author

Joshua A. Sommers, Avvaru N. Suhasini, and Robert M. Brosh

Subjects

helicase, DNA damage response, proteasome, ubiquitin, phosphorylation, acetylation, post-translational modification, Bloom’s syndrome, Fanconi Anemia, Cockayne syndrome, Werner syndrome, Microbiology, QR1-502

Abstract

Degradation of helicases or helicase-like proteins, often mediated by ubiquitin-proteasomal pathways, plays important regulatory roles in cellular mechanisms that respond to DNA damage or replication stress. The Bloom’s syndrome helicase (BLM) provides an example of how helicase degradation pathways, regulated by post-translational modifications and protein interactions with components of the Fanconi Anemia (FA) interstrand cross-link (ICL) repair pathway, influence cell cycle checkpoints, DNA repair, and replication restart. The FANCM DNA translocase can be targeted by checkpoint kinases that exert dramatic effects on FANCM stability and chromosomal integrity. Other work provides evidence that degradation of the F-box DNA helicase (FBH1) helps to balance translesion synthesis (TLS) and homologous recombination (HR) repair at blocked replication forks. Degradation of the helicase-like transcription factor (HLTF), a DNA translocase and ubiquitylating enzyme, influences the choice of post replication repair (PRR) pathway. Stability of the Werner syndrome helicase-nuclease (WRN) involved in the replication stress response is regulated by its acetylation. Turning to transcription, stability of the Cockayne Syndrome Group B DNA translocase (CSB) implicated in transcription-coupled repair (TCR) is regulated by a CSA ubiquitin ligase complex enabling recovery of RNA synthesis. Collectively, these studies demonstrate that helicases can be targeted for degradation to maintain genome homeostasis.

Published

2015

11. Special Issue on DNA Replication Stress: Summary of Topics Covered

Author

Robert M. Brosh

Subjects

n/a, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

A Special Issue of International Journal of Molecular Sciences (IJMS) is dedicated to mechanisms mediated at the molecular and cellular levels to respond to adverse genomic perturbations and DNA replication stress (https://www [...]

Published

2019

12. Holding All the Cards—How Fanconi Anemia Proteins Deal with Replication Stress and Preserve Genomic Stability

Author

Arindam Datta and Robert M. Brosh

Subjects

Fanconi anemia, genomic instability, DNA repair, DNA replication, genetic diseases, cancer, chromosome, helicase, Genetics, QH426-470

Abstract

Fanconi anemia (FA) is a hereditary chromosomal instability disorder often displaying congenital abnormalities and characterized by a predisposition to progressive bone marrow failure (BMF) and cancer. Over the last 25 years since the discovery of the first linkage of genetic mutations to FA, its molecular genetic landscape has expanded tremendously as it became apparent that FA is a disease characterized by a defect in a specific DNA repair pathway responsible for the correction of covalent cross-links between the two complementary strands of the DNA double helix. This pathway has become increasingly complex, with the discovery of now over 20 FA-linked genes implicated in interstrand cross-link (ICL) repair. Moreover, gene products known to be involved in double-strand break (DSB) repair, mismatch repair (MMR), and nucleotide excision repair (NER) play roles in the ICL response and repair of associated DNA damage. While ICL repair is predominantly coupled with DNA replication, it also can occur in non-replicating cells. DNA damage accumulation and hematopoietic stem cell failure are thought to contribute to the increased inflammation and oxidative stress prevalent in FA. Adding to its confounding nature, certain FA gene products are also engaged in the response to replication stress, caused endogenously or by agents other than ICL-inducing drugs. In this review, we discuss the mechanistic aspects of the FA pathway and the molecular defects leading to elevated replication stress believed to underlie the cellular phenotypes and clinical features of FA.

Published

2019

13. Molecular and cellular functions of the FANCJ DNA helicase defective in cancer and in Fanconi Anemia

Author

Robert M. Brosh and Sharon B. Cantor

Subjects

DNA Repair, Fanconi Anemia, Cancer, replication, genomic stability, tumor suppressor, Genetics, QH426-470

Abstract

The FANCJ DNA helicase is mutated in hereditary breast and ovarian cancer as well as the progressive bone marrow failure disorder Fanconi anemia (FA). FANCJ is linked to cancer suppression and DNA double strand break (DSB) repair through its direct interaction with the hereditary breast cancer associated gene product, BRCA1. FANCJ also operates in the FA pathway of interstrand cross-link (ICL) repair and contributes to homologous recombination (HR). FANCJ collaborates with a number of DNA metabolizing proteins implicated in DNA damage detection and repair, and plays an important role in cell cycle checkpoint control. In addition to its role in the classical FA pathway, FANCJ is believed to have other functions that are centered on alleviating replication stress. FANCJ resolves G-quadruplex (G4) DNA structures that are known to affect cellular replication and transcription, and potentially plays a role in the preservation and functionality of chromosomal structures such as telomeres. Recent studies suggest that FANCJ helps to maintain chromatin structure and preserve epigenetic stability by facilitating smooth progression of the replication fork when it encounters DNA damage or an alternate DNA structure such as a G4. Ongoing studies suggest a prominent but still not well-understood role of FANCJ in transcriptional regulation, chromosomal structure and function, and DNA damage repair to maintain genomic stability. This review will synthesize our current understanding of the molecular and cellular functions of FANCJ that are critical for chromosomal integrity.

Published

2014

14. Getting Ready for the Dance: FANCJ Irons Out DNA Wrinkles

Author

Sanjay Kumar Bharti, Sanket Awate, Taraswi Banerjee, and Robert M. Brosh

Subjects

G-quadruplex, secondary DNA structure, helicase, replication, genetic diseases, FANCJ, genomic instability, Fanconi Anemia, cancer, Genetics, QH426-470

Abstract

Mounting evidence indicates that alternate DNA structures, which deviate from normal double helical DNA, form in vivo and influence cellular processes such as replication and transcription. However, our understanding of how the cellular machinery deals with unusual DNA structures such as G-quadruplexes (G4), triplexes, or hairpins is only beginning to emerge. New advances in the field implicate a direct role of the Fanconi Anemia Group J (FANCJ) helicase, which is linked to a hereditary chromosomal instability disorder and important for cancer suppression, in replication past unusual DNA obstacles. This work sets the stage for significant progress in dissecting the molecular mechanisms whereby replication perturbation by abnormal DNA structures leads to genomic instability. In this review, we focus on FANCJ and its role to enable efficient DNA replication when the fork encounters vastly abundant naturally occurring DNA obstacles, which may have implications for targeting rapidly dividing cancer cells.

Published

2016

15. WRN helicase safeguards deprotected replication forks in BRCA2-mutated cancer cells

Author

Sanket Awate, Kajal Biswas, Joshua A. Sommers, Shyam K. Sharan, Tanay Thakar, Claudia M. Nicolae, Robert M. Brosh, Arindam Datta, Robert H. Shoemaker, Haley Thompson, and George Lucian Moldovan

Subjects

DNA Replication, congenital, hereditary, and neonatal diseases and abnormalities, Werner Syndrome Helicase, DNA damage, Science, Poly ADP ribose polymerase, Poly (ADP-Ribose) Polymerase-1, Mice, Nude, General Physics and Astronomy, Poly(ADP-ribose) Polymerase Inhibitors, Genomic Instability, General Biochemistry, Genetics and Molecular Biology, Article, Mice, Cell Line, Tumor, Neoplasms, Chromosome instability, Animals, Cancer genetics, Polymerase, BRCA2 Protein, MRE11 Homologue Protein, Nuclease, Multidisciplinary, biology, Chemistry, DNA Helicases, Helicase, nutritional and metabolic diseases, General Chemistry, Stalled forks, Cell biology, Chromatin, enzymes and coenzymes (carbohydrates), Cancer cell, biology.protein, Heterografts, Female, DNA Damage

Abstract

The tumor suppressor BRCA2 protects stalled forks from degradation to maintain genome stability. However, the molecular mechanism(s) whereby unprotected forks are stabilized remains to be fully characterized. Here, we demonstrate that WRN helicase ensures efficient restart and limits excessive degradation of stalled forks in BRCA2-deficient cancer cells. In vitro, WRN ATPase/helicase catalyzes fork restoration and curtails MRE11 nuclease activity on regressed forks. We show that WRN helicase inhibitor traps WRN on chromatin leading to rapid fork stalling and nucleolytic degradation of unprotected forks by MRE11, resulting in MUS81-dependent double-strand breaks, elevated non-homologous end-joining and chromosomal instability. WRN helicase inhibition reduces viability of BRCA2-deficient cells and potentiates cytotoxicity of a poly (ADP)ribose polymerase (PARP) inhibitor. Furthermore, BRCA2-deficient xenograft tumors in mice exhibited increased DNA damage and growth inhibition when treated with WRN helicase inhibitor. This work provides mechanistic insight into stalled fork stabilization by WRN helicase when BRCA2 is deficient., The tumor suppressor BRCA2 protects stalled DNA replication forks from unrestrained degradation; however the mechanism whereby unprotected stalled forks are preserved and restarted has remained elusive. Here the authors show that the WRN helicase promotes stalled fork recovery and limits fork hyper-degradation in the absence of BRCA2 protection.

Published

2021

16. G-Quadruplex Assembly by Ribosomal DNA: Emerging Roles in Disease Pathogenesis and Cancer Biology

Author

Robert M. Brosh, Arindam Datta, Karen A. Kormuth, and Kevin J. Pollock

Subjects

Genetics, Genome instability, DNA Replication, DNA damage, Genome, Human, DNA Helicases, Helicase, Biology, G-quadruplex, Ribosome, Genome, DNA, Ribosomal, Article, Genomic Instability, G-Quadruplexes, Gene Expression Regulation, Neoplastic, Transcription (biology), Neoplasms, biology.protein, Humans, Molecular Biology, Ribosomal DNA, Genetics (clinical), Repetitive Sequences, Nucleic Acid

Abstract

Unique repetitive elements of the eukaryotic genome can be problematic for cellular DNA replication and transcription and pose a source of genomic instability. Human ribosomal DNA (rDNA) exists as repeating units clustered together on several chromosomes. Understanding the molecular mechanisms whereby rDNA interferes with normal genome homeostasis is the subject of this review. We discuss the instability of rDNA as a driver of senescence and the important roles of helicases to suppress its deleterious effects. The propensity of rDNA that is rich in guanine bases to form G-quadruplexes (G4) is discussed and evaluated in disease pathogenesis. Targeting G4 in the ribosomes and other chromosomal loci may represent a useful synthetic lethal approach to combating cancer.

Published

2021

17. A minimal threshold of FANCJ helicase activity is required for its response to replication stress or double-strand break repair

Author

Sanjay Kumar Bharti, Lynda Bradley, Robert M. Brosh, Joshua A. Sommers, Keir C. Neuman, Irfan Khan, Sanket Awate, Marina A. Bellani, Kazuo Shin-ya, Graeme A. King, Koji Kobayashi, Yuliang Wu, Dana Branzei, Marc S. Wold, Takuye Abe, Yeonee Seol, Hiroyuki Kitao, and Venkatasubramanian Vidhyasagar

Subjects

0301 basic medicine, Aphidicolin, DNA Replication, DNA Repair, DNA damage, DNA repair, Mutation, Missense, DNA, Single-Stranded, Cell Line, Recombinases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Stress, Physiological, Replication Protein A, Genetics, Animals, DNA Breaks, Double-Stranded, Replication protein A, Oxazoles, Adenosine Triphosphatases, biology, Nucleic Acid Enzymes, DNA replication, DNA Helicases, Helicase, Processivity, Fanconi Anemia Complementation Group Proteins, Cell biology, G-Quadruplexes, 030104 developmental biology, Fanconi Anemia, chemistry, 030220 oncology & carcinogenesis, Checkpoint Kinase 1, biology.protein, DNA Polymerase Inhibitor, Rad51 Recombinase, Cisplatin, Chickens, RNA Helicases

Abstract

Fanconi Anemia (FA) is characterized by bone marrow failure, congenital abnormalities, and cancer. Of over 20 FA-linked genes, FANCJ uniquely encodes a DNA helicase and mutations are also associated with breast and ovarian cancer. fancj−/− cells are sensitive to DNA interstrand cross-linking (ICL) and replication fork stalling drugs. We delineated the molecular defects of two FA patient-derived FANCJ helicase domain mutations. FANCJ-R707C was compromised in dimerization and helicase processivity, whereas DNA unwinding by FANCJ-H396D was barely detectable. DNA binding and ATP hydrolysis was defective for both FANCJ-R707C and FANCJ-H396D, the latter showing greater reduction. Expression of FANCJ-R707C or FANCJ-H396D in fancj−/− cells failed to rescue cisplatin or mitomycin sensitivity. Live-cell imaging demonstrated a significantly compromised recruitment of FANCJ-R707C to laser-induced DNA damage. However, FANCJ-R707C expressed in fancj-/- cells conferred resistance to the DNA polymerase inhibitor aphidicolin, G-quadruplex ligand telomestatin, or DNA strand-breaker bleomycin, whereas FANCJ-H396D failed. Thus, a minimal threshold of FANCJ catalytic activity is required to overcome replication stress induced by aphidicolin or telomestatin, or to repair bleomycin-induced DNA breakage. These findings have implications for therapeutic strategies relying on DNA cross-link sensitivity or heightened replication stress characteristic of cancer cells.

Published

2018

18. A high-throughput screen to identify novel small molecule inhibitors of the Werner Syndrome Helicase-Nuclease (WRN)

Author

Robert M. Brosh, Vilhelm A. Bohr, Thomas S. Dexheimer, Tomasz Kulikowicz, Joshua A. Sommers, Dorjbal Dorjsuren, Deborah L. Croteau, Anton Simeonov, David J. Maloney, and Ajit Jadhav

Subjects

0301 basic medicine, Werner Syndrome Helicase, DNA repair, Science, Synthetic lethality, Small Molecule Libraries, Inhibitory Concentration 50, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, medicine, Humans, Fluorometry, Enzyme Inhibitors, education, Cell Proliferation, Enzyme Assays, Werner syndrome, education.field_of_study, Multidisciplinary, biology, Chemistry, DNA replication, Reproducibility of Results, Helicase, DNA, medicine.disease, High-Throughput Screening Assays, Cell biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, Biocatalysis, biology.protein, Medicine

Abstract

Werner syndrome (WS), an autosomal recessive genetic disorder, displays accelerated clinical symptoms of aging leading to a mean lifespan less than 50 years. The WS helicase-nuclease (WRN) is involved in many important pathways including DNA replication, recombination and repair. Replicating cells are dependent on helicase activity, leading to the pursuit of human helicases as potential therapeutic targets for cancer treatment. Small molecule inhibitors of DNA helicases can be used to induce synthetic lethality, which attempts to target helicase-dependent compensatory DNA repair pathways in tumor cells that are already genetically deficient in a specific pathway of DNA repair. Alternatively, helicase inhibitors may be useful as tools to study the specialized roles of helicases in replication and DNA repair. In this study, approximately 350,000 small molecules were screened based on their ability to inhibit duplex DNA unwinding by a catalytically active WRN helicase domain fragment in a high-throughput fluorometric assay to discover new non-covalent small molecule inhibitors of the WRN helicase. Select compounds were screened to exclude ones that inhibited DNA unwinding by other helicases in the screen, bound non-specifically to DNA, acted as irreversible inhibitors, or possessed unfavorable chemical properties. Several compounds were tested for their ability to impair proliferation of cultured tumor cells. We observed that two of the newly identified WRN helicase inhibitors inhibited proliferation of cancer cells in a lineage-dependent manner. These studies represent the first high-throughput screen for WRN helicase inhibitors and the results have implications for anti-cancer strategies targeting WRN in different cancer cells and genetic backgrounds.

Published

2019

19. Replication checkpoint-mediated symmetric DNA synthesis: beginning to understand mechanism

Author

Robert M. Brosh and Steven W. Matson

Subjects

0301 basic medicine, DNA Replication, Saccharomyces cerevisiae Proteins, DNA polymerase, Replication Origin, Cell Cycle Proteins, Computational biology, Saccharomyces cerevisiae, Editorials: Cell Cycle Features, Article, 03 medical and health sciences, DNA, Fungal, Molecular Biology, DNA Polymerase III, Genetics, DNA synthesis, biology, Mechanism (biology), Cell Biology, DNA, DNA Polymerase II, Replication (computing), Checkpoint Kinase 2, 030104 developmental biology, Checkpoint Kinase 1, biology.protein, Developmental Biology

Abstract

The checkpoint kinase Rad53 is activated during replication stress to prevent fork collapse, an essential but poorly understood process. Here we show that Rad53 couples leading- and lagging-strand synthesis under replication stress. In rad53-1 cells stressed by dNTP depletion, the replicative DNA helicase, MCM, and the leading-strand DNA polymerase, Pol ε, move beyond the site of DNA synthesis, likely unwinding template DNA. Remarkably, DNA synthesis progresses further along the lagging strand than the leading strand, resulting in the exposure of long stretches of single-stranded leading-strand template. The asymmetric DNA synthesis in rad53-1 cells is suppressed by elevated levels of dNTPs in vivo, and the activity of Pol ε is compromised more than lagging-strand polymerase Pol δ at low dNTP concentrations in vitro. Therefore, we propose that Rad53 prevents the generation of excessive ssDNA under replication stress by coordinating DNA unwinding with synthesis of both strands.

Published

2018

20. RecQ and Fe–S helicases have unique roles in DNA metabolism dictated by their unwinding directionality, substrate specificity, and protein interactions

Author

Robert M. Brosh and Katrina N Estep

Subjects

0301 basic medicine, Iron-Sulfur Proteins, DNA repair, Biochemistry, Article, Nucleic acid metabolism, Protein–protein interaction, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, Neoplasms, Molecular motor, Humans, Gene, Regulation of gene expression, Genetics, Chromosome Aberrations, biology, RecQ Helicases, DNA Helicases, Helicase, DNA, 030104 developmental biology, chemistry, Mutation, biology.protein, Protein Binding

Abstract

Helicases are molecular motors that play central roles in nucleic acid metabolism. Mutations in genes encoding DNA helicases of the RecQ and iron–sulfur (Fe–S) helicase families are linked to hereditary disorders characterized by chromosomal instabilities, highlighting the importance of these enzymes. Moreover, mono-allelic RecQ and Fe–S helicase mutations are associated with a broad spectrum of cancers. This review will discuss and contrast the specialized molecular functions and biological roles of RecQ and Fe–S helicases in DNA repair, the replication stress response, and the regulation of gene expression, laying a foundation for continued research in these important areas of study.

Published

2017

21. Fanconi Anemia: a DNA Repair Disorder Characterized by Accelerated Decline of the Hematopoietic Stem Cell Compartment and Other Features of Aging

Author

Michael M. Seidman, Robert M. Brosh, Marina A. Bellani, and Yie Liu

Subjects

0301 basic medicine, Aging, DNA Repair, DNA repair, DNA damage, Biology, Biochemistry, Article, Epigenesis, Genetic, 03 medical and health sciences, Fanconi anemia, medicine, Humans, Epigenetics, Molecular Biology, Bone marrow failure, Genetic disorder, Hematopoietic stem cell, Telomere, medicine.disease, Hematopoietic Stem Cells, Fanconi Anemia Complementation Group Proteins, 030104 developmental biology, medicine.anatomical_structure, Fanconi Anemia, Neurology, Immunology, Biotechnology, DNA Damage

Abstract

Fanconi Anemia (FA) is a rare autosomal genetic disorder characterized by progressive bone marrow failure (BMF), endocrine dysfunction, cancer, and other clinical features commonly associated with normal aging. The anemia stems directly from an accelerated decline of the hematopoietic stem cell compartment. Although FA is a complex heterogeneous disease linked to mutations in 19 currently identified genes, there has been much progress in understanding the molecular pathology involved. FA is broadly considered a DNA repair disorder and the FA gene products, together with other DNA repair factors, have been implicated in interstrand cross-link (ICL) repair. However, in addition to the defective DNA damage response, altered epigenetic regulation, and telomere defects, FA is also marked by elevated levels of inflammatory mediators in circulation, a hallmark of faster decline in not only other hereditary aging disorders but also normal aging. In this review, we offer a perspective of FA as a monogenic accelerated aging disorder, citing the latest evidence for its multi-factorial deficiencies underlying its unique clinical and cellular features.

Published

2016

22. Biochemical and Cell Biological Assays to Identify and Characterize DNA Helicase Inhibitors

Author

Taraswi Banerjee, Monika Aggarwal, Joshua A. Sommers, and Robert M. Brosh

Subjects

0301 basic medicine, Premature aging, DNA Replication, DNA Repair, DNA repair, Cellular homeostasis, Computational biology, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, Transcription (biology), medicine, Humans, Enzyme Inhibitors, Molecular Biology, Werner syndrome, Genetics, DNA replication, DNA Helicases, Helicase, medicine.disease, 030104 developmental biology, chemistry, biology.protein, Biological Assay, DNA

Abstract

The growing number of DNA helicases implicated in hereditary disorders and cancer indicates that this particular class of enzymes plays key roles in genomic stability and cellular homeostasis. Indeed, a large body of work has provided molecular and cellular evidence that helicases act upon a variety of nucleic acid substrates and interact with numerous proteins to enact their functions in replication, DNA repair, recombination, and transcription. Understanding how helicases operate in unique and overlapping pathways is a great challenge to researchers. In this review, we describe a series of experimental approaches and methodologies to identify and characterize DNA helicase inhibitors which collectively provide an alternative and useful strategy to explore their biological significance in cell-based systems. These procedures were used in the discovery of biologically active compounds that inhibited the DNA unwinding function catalyzed by the human WRN helicase-nuclease defective in the premature aging disorder Werner syndrome. We describe in vitro and in vivo experimental approaches to characterize helicase inhibitors with WRN as the model, anticipating that these approaches may be extrapolated to other DNA helicases, particularly those implicated in DNA repair and/or the replication stress response.

Published

2016

23. Tim/Timeless, a member of the fork-protection complex, operates with the Warsaw breakage syndrome DNA helicase DDX11 in the same fork recovery pathway

Author

Robert M. Brosh, Francesca M. Pisani, Sanjay Kumar Bharti, Roberta Di Perna, and Federica Calì

Subjects

0301 basic medicine, Molecular Sequence Data, Cell Cycle Proteins, DNA helicase, Genome Integrity, Repair and Replication, DNA replication, DEAD-box RNA Helicases, 03 medical and health sciences, chemistry.chemical_compound, Replication fork protection complex, Control of chromosome duplication, Genome stability, Genetics, Humans, Hydroxyurea, biology, Base Sequence, DNA Helicases, Intracellular Signaling Peptides and Proteins, Helicase, DNA, DNA Replication Fork, Molecular biology, Chromatin, Cell biology, G-Quadruplexes, 030104 developmental biology, chemistry, biology.protein, Nucleic acid, Nucleic Acid Conformation, HeLa Cells

Abstract

We present evidence that Tim establishes a physi- cal and functional interaction with DDX11, a super- family 2 iron-sulfur cluster DNA helicase genetically linked to the chromosomal instability disorder War- saw breakage syndrome. Tim stimulates DDX11 un- winding activity on forked DNA substrates up to 10- fold and on bimolecular anti-parallel G-quadruplex DNA structures and three-stranded D-loop approx- imately 4-5-fold. Electrophoretic mobility shift as- says revealed that Tim enhances DDX11 binding to DNA, suggesting that the observed stimulation de- rives from an improved ability of DDX11 to interact with the nucleic acid substrate. Surface plasmon res- onance measurements indicate that DDX11 directly interacts with Tim. DNA fiber track assays with HeLa cells exposed to hydroxyurea demonstrated that Tim or DDX11 depletion significantly reduced replication fork progression compared to control cells; whereas no additive effect was observed by co-depletion of both proteins. Moreover, Tim and DDX11 are epistatic in promoting efficient resumption of stalled DNA replication forks in hydroxyurea-treated cells. This is consistent with the finding that association of the two endogenous proteins in the cell extract chro- matin fraction is considerably increased following hydroxyurea exposure. Overall, our studies provide evidence that Tim and DDX11 physically and func- tionally interact and act in concert to preserve repli- cation fork progression in perturbed conditions.

Published

2016

24. Human premature aging, DNA repair and RecQ helicases

Author

Robert M. Brosh and Vilhelm A. Bohr

Subjects

Genome instability, Premature aging, DNA Replication, Werner Syndrome Helicase, DNA Repair, DNA repair, RecQ helicase, Cellular homeostasis, Chromosomal Instability, Neoplasms, Replication Protein A, Genetics, Humans, Survey and Summary, education, Replication protein A, education.field_of_study, biology, RecQ Helicases, Helicase, Aging, Premature, Telomere, Exodeoxyribonucleases, Mutation, biology.protein, Sister Chromatid Exchange

Abstract

Genomic instability leads to mutations, cellular dysfunction and aberrant phenotypes at the tissue and organism levels. A number of mechanisms have evolved to cope with endogenous or exogenous stress to prevent chromosomal instability and maintain cellular homeostasis. DNA helicases play important roles in the DNA damage response. The RecQ family of DNA helicases is of particular interest since several human RecQ helicases are defective in diseases associated with premature aging and cancer. In this review, we will provide an update on our understanding of the specific roles of human RecQ helicases in the maintenance of genomic stability through their catalytic activities and protein interactions in various pathways of cellular nucleic acid metabolism with an emphasis on DNA replication and repair. We will also discuss the clinical features of the premature aging disorders associated with RecQ helicase deficiencies and how they relate to the molecular defects.

Published

2007

25. Impact of age-associated cyclopurine lesions on DNA repair helicases

Author

Joshua A. Sommers, Taraswi Banerjee, Jochen Kuper, Avvaru N. Suhasini, Daniel L. Kaplan, Irfan Khan, Robert M. Brosh, and Caroline Kisker

Subjects

DNA Repair, DNA repair, DNA damage, Archaeal Proteins, lcsh:Medicine, DNA replication, Biochemistry, chemistry.chemical_compound, DDX11, ddc:570, DNA metabolism, Humans, lcsh:Science, Molecular Biology, dnaB helicase, Multidisciplinary, Deoxyadenosines, Biology and life sciences, biology, lcsh:R, DNA Helicases, Deoxyguanosine, Helicase, DNA, Archaea, Biochemical Activity, Molecular biology, Recombinant Proteins, chemistry, Molecular Machines, biology.protein, lcsh:Q, Research Article, Nucleotide excision repair

Abstract

8,5′ cyclopurine deoxynucleosides (cPu) are locally distorting DNA base lesions corrected by nucleotide excision repair (NER) and proposed to play a role in neurodegeneration prevalent in genetically defined Xeroderma pigmentosum (XP) patients. In the current study, purified recombinant helicases from different classifications based on sequence homology were examined for their ability to unwind partial duplex DNA substrates harboring a single site-specific cPu adduct. Superfamily (SF) 2 RecQ helicases (RECQ1, BLM, WRN, RecQ) were inhibited by cPu in the helicase translocating strand, whereas helicases from SF1 (UvrD) and SF4 (DnaB) tolerated cPu in either strand. SF2 Fe-S helicases (FANCJ, DDX11 (ChlR1), DinG, XPD) displayed marked differences in their ability to unwind the cPu DNA substrates. Archaeal Thermoplasma acidophilum XPD (taXPD), homologue to the human XPD helicase involved in NER DNA damage verification, was impeded by cPu in the non-translocating strand, while FANCJ was uniquely inhibited by the cPu in the translocating strand. Sequestration experiments demonstrated that FANCJ became trapped by the translocating strand cPu whereas RECQ1 was not, suggesting the two SF2 helicases interact with the cPu lesion by distinct mechanisms despite strand-specific inhibition for both. Using a protein trap to simulate single-turnover conditions, the rate of FANCJ or RECQ1 helicase activity was reduced 10-fold and 4.5-fold, respectively, by cPu in the translocating strand. In contrast, single-turnover rates of DNA unwinding by DDX11 and UvrD helicases were only modestly affected by the cPu lesion in the translocating strand. The marked difference in effect of the translocating strand cPu on rate of DNA unwinding between DDX11 and FANCJ helicase suggests the two Fe-S cluster helicases unwind damaged DNA by distinct mechanisms. The apparent complexity of helicase encounters with an unusual form of oxidative damage is likely to have important consequences in the cellular response to DNA damage and DNA repair.

Published

2014

26. Targeting an Achilles’ heel of cancer with a WRN helicase inhibitor

Author

Joshua A. Sommers, Taraswi Banerjee, Robert M. Brosh, and Monika Aggarwal

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, DNA End-Joining Repair, DNA repair, DNA damage, Mitomycin, Synthetic lethality, Biology, Models, Biological, Werner Syndrome Helicase, Cell Line, Maleimides, Stress, Physiological, Report, Neoplasms, FANCD2, medicine, Humans, Enzyme Inhibitors, education, Molecular Biology, Werner syndrome, education.field_of_study, RecQ Helicases, Helicase, nutritional and metabolic diseases, Cell Biology, medicine.disease, Molecular biology, Fanconi Anemia, Cancer research, biology.protein, Developmental Biology, Signal Transduction

Abstract

Our recently published work suggests that DNA helicases such as the Werner syndrome helicase (WRN) represent a novel class of proteins to target for anticancer therapy. Specifically, pharmacological inhibition of WRN helicase activity in human cells defective in the Fanconi anemia (FA) pathway of interstrand cross-link (ICL) repair are sensitized to the DNA cross-linking agent and chemotherapy drug mitomycin C (MMC) by the WRN helicase inhibitor NSC 617145. (1) The mechanistic basis for the synergistic interaction between NSC 617145 and MMC is discussed in this paper and extrapolated to potential implications for genetic or chemically induced synthetic lethality provoked by cellular exposure to the WRN helicase inhibitor under the context of relevant DNA repair deficiencies associated with cancers or induced by small-molecule inhibitors. Experimental data are presented showing that small-molecule inhibition of WRN helicase elevates sensitivity to MMC-induced stress in human cells that are deficient in both FANCD2 and DNA protein kinase catalytic subunit (DNA-PKcs). These findings suggest a model in which drug-mediated inhibition of WRN helicase activity exacerbates the deleterious effects of MMC-induced DNA damage when both the FA and NHEJ pathways are defective. We conclude with a perspective for the FA pathway and synthetic lethality and implications for DNA repair helicase inhibitors that can be developed for anticancer strategies.

Published

2013

27. Specialization among Iron-Sulfur Cluster Helicases to Resolve G-quadruplex DNA Structures That Threaten Genomic Stability*

Author

Kazuo Shin-ya, Caroline Kisker, Fourbears George, Marie-Paule Teulade-Fichou, Robert M. Brosh, Sanjay Kumar Bharti, Joshua A. Sommers, Jochen Kuper, and Florian Hamon

Subjects

Genome instability, DNA Replication, Iron-Sulfur Proteins, congenital, hereditary, and neonatal diseases and abnormalities, Guanine, DNA Repair, DNA repair, DNA damage, Thermoplasma, DNA and Chromosomes, G-quadruplex, Ligands, Biochemistry, Genomic Instability, chemistry.chemical_compound, Inhibitory Concentration 50, hemic and lymphatic diseases, Escherichia coli, Humans, Molecular Biology, Genetics, biology, DNA replication, DNA Helicases, Helicase, nutritional and metabolic diseases, Cell Biology, DNA, Fanconi Anemia Complementation Group Proteins, Recombinant Proteins, G-Quadruplexes, Basic-Leucine Zipper Transcription Factors, chemistry, Gene Expression Regulation, biology.protein, RNA Interference, Nucleotide excision repair

Abstract

G-quadruplex (G4) DNA, an alternate structure formed by Hoogsteen hydrogen bonds between guanines in G-rich sequences, threatens genomic stability by perturbing normal DNA transactions including replication, repair, and transcription. A variety of G4 topologies (intra- and intermolecular) can form in vitro, but the molecular architecture and cellular factors influencing G4 landscape in vivo are not clear. Helicases that unwind structured DNA molecules are emerging as an important class of G4-resolving enzymes. The BRCA1-associated FANCJ helicase is among those helicases able to unwind G4 DNA in vitro, and FANCJ mutations are associated with breast cancer and linked to Fanconi anemia. FANCJ belongs to a conserved iron-sulfur (Fe S) cluster family of helicases important for genomic stability including XPD (nucleotide excision repair), DDX11 (sister chromatid cohesion), and RTEL (telomere metabolism), genetically linked to xeroderma pigmentosum/Cockayne syndrome, Warsaw breakage syndrome, and dyskeratosis congenita, respectively. To elucidate the role of FANCJ in genomic stability, its molecular functions in G4 metabolism were examined. FANCJ efficiently unwound in a kinetic and ATPase-dependent manner entropically favored unimolecular G4 DNA, whereas other Fe-S helicases tested did not. The G4-specific ligands Phen-DC3 or Phen-DC6 inhibited FANCJ helicase on unimolecular G4 ∼1000-fold better than bi- or tetramolecular G4 DNA. The G4 ligand telomestatin induced DNA damage in human cells deficient in FANCJ but not DDX11 or XPD. These findings suggest FANCJ is a specialized Fe-S cluster helicase that preserves chromosomal stability by unwinding unimolecular G4 DNA likely to form in transiently unwound single-stranded genomic regions. Background: The Fe-S helicase FANCJ implicated in Fanconi anemia plays important roles in DNA replication and repair. Results: FANCJ, but not the Fe-S XPD or DDX11 helicases, unwinds unimolecular G4 DNA. Conclusion: FANCJ is a specialized Fe-S helicase, preventing G4-induced DNA damage. Significance: FANCJ has a unique role in DNA metabolism to prevent G4 accumulation that causes genomic instability.

Published

2013

28. Human RECQ1 interacts with Ku70/80 and modulates DNA end-joining of double-strand breaks

Author

Sudha Sharma, Alexei Stortchevoi, Robert M. Brosh, Joshua A. Sommers, and Swetha Parvathaneni

Subjects

Genome instability, DNA End-Joining Repair, RecQ helicase, Oligonucleotides, lcsh:Medicine, Electrophoretic Mobility Shift Assay, Toxicology, Biochemistry, Molecular cell biology, 0302 clinical medicine, DNA Breaks, Double-Stranded, Bloom syndrome, Protein Interaction Maps, lcsh:Science, 0303 health sciences, Multidisciplinary, RecQ Helicases, Chromosome Biology, Antigens, Nuclear, Enzymes, Nucleic acids, 030220 oncology & carcinogenesis, Protein Binding, Research Article, Premature aging, congenital, hereditary, and neonatal diseases and abnormalities, Genetic Toxicology, DNA repair, DNA damage, Biology, 03 medical and health sciences, DNA-binding proteins, medicine, Humans, Ku Autoantigen, 030304 developmental biology, lcsh:R, Proteins, Helicase, nutritional and metabolic diseases, DNA, medicine.disease, Molecular biology, biology.protein, Nucleic Acid Conformation, lcsh:Q, HeLa Cells

Abstract

Genomic instability is a known precursor to cancer and aging. The RecQ helicases are a highly conserved family of DNA-unwinding enzymes that play key roles in maintaining genome stability in all living organisms. Human RecQ homologs include RECQ1, BLM, WRN, RECQ4, and RECQ5β, three of which have been linked to diseases with elevated risk of cancer and growth defects (Bloom Syndrome and Rothmund-Thomson Syndrome) or premature aging (Werner Syndrome). RECQ1, the first RecQ helicase discovered and the most abundant in human cells, is the least well understood of the five human RecQ homologs. We have previously described that knockout of RECQ1 in mice or knockdown of its expression in human cells results in elevated frequency of spontaneous sister chromatid exchanges, chromosomal instability, increased load of DNA damage and heightened sensitivity to ionizing radiation. We have now obtained evidence implicating RECQ1 in the nonhomologous end-joining pathway of DNA double-strand break repair. We show that RECQ1 interacts directly with the Ku70/80 subunit of the DNA-PK complex, and depletion of RECQ1 results in reduced end-joining in cell free extracts. In vitro, RECQ1 binds and unwinds the Ku70/80-bound partial duplex DNA substrate efficiently. Linear DNA is co-bound by RECQ1 and Ku70/80, and DNA binding by Ku70/80 is modulated by RECQ1. Collectively, these results provide the first evidence for an interaction of RECQ1 with Ku70/80 and a role of the human RecQ helicase in double-strand break repair through nonhomologous end-joining.

Published

2013

29. Identification and Biochemical Characterization of a Novel Mutation in DDX11 Causing Warsaw Breakage Syndrome

Author

Mark E. Samuels, Robert M. Brosh, Jacques L. Michaud, Eliane Chouery, Sanjay Kumar Bharti, Guy A. Rouleau, Zoha Kibar, Fadi F. Hamdan, Joshua A. Sommers, Tony Yammine, André Mégarbané, Lysanne Patry, and Jose-Mario Capo-Chichi

Subjects

Male, Microcephaly, Mutation, Missense, Biology, medicine.disease_cause, Article, DEAD-box RNA Helicases, Consanguinity, DDX11, Intellectual Disability, Genetics, medicine, Missense mutation, Humans, Abnormalities, Multiple, Exome, Genetic Predisposition to Disease, Amino Acid Sequence, Genetics (clinical), Exome sequencing, Family Health, Mutation, Base Sequence, DNA Helicases, Chromosome Breakage, Sequence Analysis, DNA, Syndrome, medicine.disease, Disease gene identification, Molecular biology, Pedigree, Female, Chromosome breakage

Abstract

Mutations in the gene encoding the iron–sulfur-containing DNA helicase DDX11 (ChlR1) were recently identified as a cause of a new recessive cohesinopathy, Warsaw breakage syndrome (WABS), in a single patient with severe microcephaly, pre- and postnatal growth retardation, and abnormal skin pigmentation. Here, using homozygosity mapping in a Lebanese consanguineous family followed by exome sequencing, we identified a novel homozygous mutation (c.788G>A [p.R263Q]) in DDX11 in three affected siblings with severe intellectual disability and many of the congenital abnormalities reported in the WABS original case. Cultured lymphocytes from the patients showed increased mitomycin C-induced chromosomal breakage, as found in WABS. Biochemical studies of purified recombinant DDX11 indicated that the p.R263Q mutation impaired DDX11 helicase activity by perturbing its DNA binding and DNA-dependent ATP hydrolysis. Our findings thus confirm the involvement of DDX11 in WABS, describe its phenotypical spectrum, and provide novel insight into the structural requirement for DDX11 activity. Hum Mutat 34:103-107, 2013.

Published

2012

30. MECHANISTIC AND BIOLOGICAL ASPECTS OF HELICASE ACTION ON DAMAGED DNA

Author

Robert M. Brosh and Avvaru N. Suhasini

Subjects

Genetics, DNA Replication, DNA clamp, biology, DNA Repair, DNA Helicases, Helicase, DNA, Single-Stranded, Eukaryotic DNA replication, Cell Biology, DNA, RNA Helicase A, Article, Cell biology, Control of chromosome duplication, biology.protein, Replisome, Humans, Primase, Molecular Biology, Replication protein A, Developmental Biology, DNA Damage

Abstract

Helicases catalytically unwind structured nucleic acids in a nucleoside-triphosphate-dependent and directionally specific manner, and are essential for virtually all aspects of nucleic acid metabolism. ATPase-driven helicases which translocate along nucleic acids play a role in damage recognition or unwinding of a DNA tract containing the lesion. Although classical biochemical experiments provided evidence that bulky covalent adducts inhibit DNA unwinding catalyzed by certain DNA helicases in a strand-specific manner (i.e. , block to DNA unwinding restricted to adduct residence in the strand the helicase translocates), recent studies suggest more complex arrangements that may depend on the helicase under study, its assembly in a protein complex, and the type of structural DNA perturbation. Moreover, base and sugar phosphate backbone modifications exert effects on DNA helicases that suggest specialized tracking mechanisms. As a component of the replication stress response, the single-stranded DNA binding protein Replication Protein A (RPA) may serve to enable eukaryotic DNA helicases to overcome certain base lesions. Helicases play important roles in DNA damage signaling which also involve their partnership with RPA. In this review, we will discuss our current understanding of mechanistic and biological aspects of helicase action on damaged DNA.

Published

2010

31. FANCJ Helicase Uniquely Senses Oxidative Base Damage in Either Strand of Duplex DNA and Is Stimulated by Replication Protein A to Unwind the Damaged DNA Substrate in a Strand-specific Manner*

Author

Aaron C. Mason, Robert M. Brosh, Marc S. Wold, R. Daniel Camerini-Otero, Joshua A. Sommers, Avvaru N. Suhasini, and Oleg N. Voloshin

Subjects

Guanine, Breast Neoplasms, Oxidative phosphorylation, medicine.disease_cause, Biochemistry, Substrate Specificity, chemistry.chemical_compound, DNA Adducts, Fanconi anemia, Replication Protein A, medicine, Humans, Molecular Biology, Replication protein A, Escherichia coli, dnaB helicase, biology, DNA Helicases, Helicase, Cell Biology, DNA, medicine.disease, Fanconi Anemia Complementation Group Proteins, Enzyme Activation, Oxidative Stress, Basic-Leucine Zipper Transcription Factors, Fanconi Anemia, chemistry, DNA: Replication, Repair, Recombination, and Chromosome Dynamics, biology.protein, Female, Carcinogenesis, Thymine, DNA Damage

Abstract

FANCJ mutations are genetically linked to the Fanconi anemia complementation group J and predispose individuals to breast cancer. Understanding the role of FANCJ in DNA metabolism and how FANCJ dysfunction leads to tumorigenesis requires mechanistic studies of FANCJ helicase and its protein partners. In this work, we have examined the ability of FANCJ to unwind DNA molecules with specific base damage that can be mutagenic or lethal. FANCJ was inhibited by a single thymine glycol, but not 8-oxoguanine, in either the translocating or nontranslocating strands of the helicase substrate. In contrast, the human RecQ helicases (BLM, RECQ1, and WRN) display strand-specific inhibition of unwinding by the thymine glycol damage, whereas other DNA helicases (DinG, DnaB, and UvrD) are not significantly inhibited by thymine glycol in either strand. In the presence of replication protein A (RPA), but not Escherichia coli single-stranded DNA-binding protein, FANCJ efficiently unwound the DNA substrate harboring the thymine glycol damage in the nontranslocating strand; however, inhibition of FANCJ helicase activity by the translocating strand thymine glycol was not relieved. Strand-specific stimulation of human RECQ1 helicase activity was also observed, and RPA bound with high affinity to single-stranded DNA containing a single thymine glycol. Based on the biochemical studies, we propose a model for the specific functional interaction between RPA and FANCJ on the thymine glycol substrates. These studies are relevant to the roles of RPA, FANCJ, and other DNA helicases in the metabolism of damaged DNA that can interfere with basic cellular processes of DNA metabolism.

Published

2009

32. FANCJ Uses Its Motor ATPase to Destabilize Protein-DNA Complexes, Unwind Triplexes, and Inhibit RAD51 Strand Exchange*

Author

Alexander V. Mazin, Dmitry V. Bugreev, Sharon B. Cantor, Rigu Gupta, Robert M. Brosh, Joshua A. Sommers, and Nina A Rawtani

Subjects

DNA Replication, DNA Repair, DNA repair, RAD51, Biochemistry, chemistry.chemical_compound, Adenosine Triphosphate, Humans, DNA Breaks, Double-Stranded, Molecular Biology, Adenosine Triphosphatases, Recombination, Genetic, biology, Hydrolysis, DNA replication, Helicase, Cell Biology, DNA, Double Strand Break Repair, Fanconi Anemia Complementation Group Proteins, Homologous Recombination Pathway, Basic-Leucine Zipper Transcription Factors, chemistry, DNA: Replication, Repair, Recombination, and Chromosome Dynamics, biology.protein, Female, Rad51 Recombinase, Homologous recombination

Abstract

Mutations in the FANCJ helicase predispose individuals to breast cancer and are genetically linked to the Fanconi anemia (FA) complementation group J. FA is a chromosomal instability disorder characterized by multiple congenital anomalies, progressive bone marrow failure, and high cancer risk. FANCJ has been proposed to function downstream of FANCD2 monoubiquitination, a critical event in the FA pathway. Evidence supports a role for FANCJ in a homologous recombination pathway of double strand break repair. In an effort to understand the molecular functions of FANCJ, we have investigated the ability of purified FANCJ recombinant protein to use its motor ATPase function for activities in addition to unwinding of conventional duplex DNA substrates. These efforts have led to the discovery that FANCJ ATP hydrolysis can be used to destabilize protein-DNA complexes and unwind triple helix alternate DNA structures. These novel catalytic functions of FANCJ may be important for its role in cellular DNA repair, recombination, or resolving DNA structural obstacles to replication. Consistent with this, we show that FANCJ can inhibit RAD51 strand exchange, an activity that is likely to be important for its role in controlling DNA repair through homologous recombination.

Published

2009

33. Human RECQ1 is a DNA damage responsive protein required for genotoxic stress resistance and suppression of sister chromatid exchanges

Author

Sudha Sharma and Robert M. Brosh

Subjects

DNA damage, DNA repair, RecQ helicase, Cell Biology/Cell Growth and Division, lcsh:Medicine, Eukaryotic DNA replication, medicine, Humans, Bloom syndrome, Molecular Biology/Chromatin Structure, RNA, Small Interfering, lcsh:Science, Replication protein A, Molecular Biology/DNA Replication, Genetics, Molecular Biology/Recombination, Biochemistry/Replication and Repair, Multidisciplinary, Molecular Biology/DNA Repair, biology, Base Sequence, RecQ Helicases, lcsh:R, Helicase, Cell Biology/Cellular Death and Stress Responses, medicine.disease, Oxidative Stress, biology.protein, DNA mismatch repair, lcsh:Q, Sister Chromatid Exchange, Research Article, DNA Damage, HeLa Cells, Mutagens

Abstract

Background. DNA helicases are ubiquitous enzymes that unwind DNA in an ATP-dependent and directionally specific manner. Unwinding of double-stranded DNA is essential for the processes of DNA repair, recombination, transcription, and DNA replication. Five human DNA helicases sharing sequence similarity with the E. coli RecQ helicase have been identified. Three of the human RecQ helicases are implicated in hereditary diseases (Bloom syndrome, Werner syndrome, and Rothmund-Thomson syndrome) which display clinical symptoms of premature aging and cancer. RECQ1 helicase is the most highly expressed of the human RecQ helicases; however, a genetic disease has yet not been linked to mutations in the RECQ1 gene, and the biological functions of human RECQ1 in cellular DNA metabolism are not known. Methodology/Principal Findings. In this study, we report that RECQ1 becomes phosphorylated upon DNA damage and forms irradiation-induced nuclear foci that associate with chromatin in human cells. Depletion of RECQ1 renders human cells sensitive to DNA damage induced by ionizing radiation or the topoisomerase inhibitor camptothecin, and results in spontaneous c-H2AX foci and elevated sister chromatid exchanges, indicating aberrant repair of DNA breaks. Consistent with a role in homologous recombinational repair, endogenous RECQ1 is associated with the strand exchange protein Rad51 and the two proteins directly interact with high affinity. Conclusion/ Significance. Collectively, these results provide the first evidence for a role of human RECQ1 in the response to DNA damage and chromosomal stability maintenance and point to the vital importance of RECQ1 in genome homeostasis.

Published

2007

34. FANCJ (BACH1) helicase forms DNA damage inducible foci with replication protein A and interacts physically and functionally with the single-stranded DNA-binding protein

Author

Rigu Gupta, Sharon B. Cantor, Joshua A. Sommers, Mark K. Kenny, Robert M. Brosh, and Sudha Sharma

Subjects

DNA repair, DNA damage, Immunology, medicine.disease_cause, Biochemistry, DNA-binding protein, complex mixtures, Cell Line, chemistry.chemical_compound, Replication Protein A, medicine, Humans, RNA, Small Interfering, Replication protein A, Genetics, Mutation, biology, DNA replication, DNA Helicases, Helicase, Cell Biology, Hematology, Fanconi Anemia Complementation Group Proteins, Hematopoiesis, DNA-Binding Proteins, enzymes and coenzymes (carbohydrates), Kinetics, Basic-Leucine Zipper Transcription Factors, Fanconi Anemia, chemistry, biology.protein, DNA, DNA Damage, Protein Binding

Abstract

The BRCA1 associated C-terminal helicase (BACH1, designated FANCJ) is implicated in the chromosomal instability genetic disorder Fanconi anemia (FA) and hereditary breast cancer. A critical role of FANCJ helicase may be to restart replication as a component of downstream events that occur during the repair of DNA cross-links or double-strand breaks. We investigated the potential interaction of FANCJ with replication protein A (RPA), a single-stranded DNA-binding protein implicated in both DNA replication and repair. FANCJ and RPA were shown to coimmunoprecipitate most likely through a direct interaction of FANCJ and the RPA70 subunit. Moreover, dependent on the presence of BRCA1, FANCJ colocalizes with RPA in nuclear foci after DNA damage. Our data are consistent with a model in which FANCJ associates with RPA in a DNA damage-inducible manner and through the protein interaction RPA stimulates FANCJ helicase to better unwind duplex DNA substrates. These findings identify RPA as the first regulatory partner of FANCJ. The FANCJ-RPA interaction is likely to be important for the role of the helicase to more efficiently unwind DNA repair intermediates to maintain genomic stability.

Published

2007

35. Mechanisms of RecQ helicases in pathways of DNA metabolism and maintenance of genomic stability

Author

Robert M. Brosh, Kevin M. Doherty, and Sudha Sharma

Subjects

Genetics, Genome instability, Premature aging, Adenosine Triphosphatases, biology, RecQ Helicases, DNA repair, DNA replication, DNA Helicases, Helicase, Cell Biology, Review Article, DNA, Biochemistry, Genomic Instability, chemistry.chemical_compound, chemistry, Chromosome instability, biology.protein, Humans, Molecular Biology, Gene

Abstract

Helicases are molecular motor proteins that couple the hydrolysis of NTP to nucleic acid unwinding. The growing number of DNA helicases implicated in human disease suggests that their vital specialized roles in cellular pathways are important for the maintenance of genome stability. In particular, mutations in genes of the RecQ family of DNA helicases result in chromosomal instability diseases of premature aging and/or cancer predisposition. We will discuss the mechanisms of RecQ helicases in pathways of DNA metabolism. A review of RecQ helicases from bacteria to human reveals their importance in genomic stability by their participation with other proteins to resolve DNA replication and recombination intermediates. In the light of their known catalytic activities and protein interactions, proposed models for RecQ function will be summarized with an emphasis on how this distinct class of enzymes functions in chromosomal stability maintenance and prevention of human disease and cancer.

Published

2006

36. WRN helicase and FEN-1 form a complex upon replication arrest and together process branchmigrating DNA structures associated with the replication fork

Author

Sudha Sharma, Hui-I Kao, Henry C. Driscoll, Robert M. Brosh, Marit Otterlei, Robert A. Bambara, Grigory L. Dianov, and Joshua A. Sommers

Subjects

DNA Replication, congenital, hereditary, and neonatal diseases and abnormalities, Werner Syndrome Helicase, Flap Endonucleases, Electrophoretic Mobility Shift Assay, Biology, Pre-replication complex, DNA replication factor CDT1, Replication factor C, Control of chromosome duplication, Minichromosome maintenance, Fluorescence Resonance Energy Transfer, Humans, education, Molecular Biology, S phase, Genetics, education.field_of_study, RecQ Helicases, DNA Helicases, nutritional and metabolic diseases, Articles, Cell Biology, Recombinant Proteins, Cell biology, Exodeoxyribonucleases, biology.protein, Origin recognition complex, HeLa Cells, Protein Binding

Abstract

Werner Syndrome is a premature aging disorder characterized by genomic instability, elevated recombination, and replication defects. It has been hypothesized that defective processing of certain replication fork structures by WRN may contribute to genomic instability. Fluorescence resonance energy transfer (FRET) analyses show that WRN and Flap Endonuclease-1 (FEN-1) form a complex in vivo that colocalizes in foci associated with arrested replication forks. WRN effectively stimulates FEN-1 cleavage of branch-migrating double-flap structures that are the physiological substrates of FEN-1 during replication. Biochemical analyses demonstrate that WRN helicase unwinds the chicken-foot HJ intermediate associated with a regressed replication fork and stimulates FEN-1 to cleave the unwound product in a structure-dependent manner. These results provide evidence for an interaction between WRN and FEN-1 in vivo and suggest that these proteins function together to process DNA structures associated with the replication fork.

Published

2004

37. Analysis of the unwinding activity of the dimeric RECQ1 helicase in the presence of human replication protein A

Author

Alessandro Vindigni, Robert M. Brosh, Daniele Arosio, Kevin M. Doherty, Arturo Falaschi, and Sheng Cui

Subjects

Protein subunit, Size-exclusion chromatography, DNA, Single-Stranded, Enzyme-Linked Immunosorbent Assay, medicine.disease_cause, Blotting, Far-Western, law.invention, chemistry.chemical_compound, Adenosine Triphosphate, law, Replication Protein A, Genetics, medicine, Humans, Scattering, Radiation, Protein Structure, Quaternary, Replication protein A, Escherichia coli, Adenosine Triphosphatases, Molecular mass, biology, RecQ Helicases, DNA Helicases, Helicase, Articles, DNA, Precipitin Tests, DNA-Binding Proteins, Biochemistry, chemistry, biology.protein, Recombinant DNA, Chromatography, Gel, Dimerization, HeLa Cells, Protein Binding

Abstract

RecQ helicases are required for the maintenance of genome stability. Characterization of the substrate specificity and identification of the binding partners of the five human RecQ helicases are essential for understanding their function. In the present study, we have developed an efficient baculovirus expression system that allows us to obtain milligram quantities of recombinant RECQ1. Our gel filtration and dynamic light scattering experiments show that RECQ1 has an apparent molecular mass of 158 kDa and a hydrodynamic radius of 5.4 +/- 0.6 nm, suggesting that RECQ1 forms dimers in solution. The oligomeric state of RECQ1 remains unchanged upon binding to a single-stranded (ss)DNA fragment of 50 nt. We show that RECQ1 alone is able to unwind short DNA duplexes (

Published

2004

38. Differential requirement for the ATPase domain of the Cockayne syndrome group B gene in the processing of UV-induced DNA damage and 8-oxoguanine lesions in human cells

Author

Jingsheng Tuo, Rebecca R. Selzer, Elisabetta Citterio, Mette Christiansen, Simon G. Nyaga, Meltem Muftuoglu, Robert M. Brosh, Vilhelm A. Bohr, and Alfred May

Subjects

Premature aging, Cell Extracts, Guanine, DNA Repair, DNA repair, DNA damage, Cell Survival, Ultraviolet Rays, Mutant, Amino Acid Motifs, Apoptosis, Biology, Radiation Tolerance, Cockayne syndrome, Article, Cell Line, Cytosine, Genetics, medicine, Humans, Amino Acid Sequence, Cockayne Syndrome, Poly-ADP-Ribose Binding Proteins, Gene, Oligonucleotide Array Sequence Analysis, Adenosine Triphosphatases, Point mutation, Gene Expression Profiling, Genetic Complementation Test, DNA Helicases, Transfection, Hydrogen Peroxide, Fibroblasts, medicine.disease, Molecular biology, Protein Structure, Tertiary, DNA Repair Enzymes, Mutation, RNA, Thymine, DNA Damage

Abstract

Cockayne syndrome (CS) is a rare inherited human genetic disorder characterized by UV sensitivity, developmental abnormalities and premature aging. The cellular and molecular phenotypes of CS include increased sensitivity to oxidative and UV-induced DNA lesions. The CSB protein is thought to play a pivotal role in transcription-coupled repair and CS-B cells are defective in the repair of the transcribed strand of active genes, both after exposure to UV and in the presence of oxidative DNA lesions. A previous study has indicated that a conserved helicase ATPase motif II residue is essential for the function of the CSB protein in responding to UV-induced DNA damage in a hamster cell line. Due to the limitations in studying a complex human disorder in another species, this study introduced the site-directed mutation of the ATPase motif II in the human CSB gene in an isogenic human cell line. The CSB mutant allele was tested for genetic complementation of UV-sensitive phenotypes in the human CS-B cell line CS1AN.S3.G2. In addition, the incision of an 8-oxoguanine lesion by extracts of the CS-B cell lines stably transfected with the wild-type or ATPase mutant CSB gene has been investigated. The ATPase motif II point mutation (E646Q) abolished the function of the CSB protein to complement the UV-sensitive phenotypes of survival, RNA synthesis recovery and apoptosis. Interestingly, whole-cell extract prepared from these mutant cells retained wild-type incision activity on an oligonucleotide containing a single 8-oxoguanine lesion, whereas the absence of the CSB gene altogether resulted in reduced incision activity relative to wild-type. These results suggest damage-specific functional requirements for CSB in the repair of UV-induced and oxidative lesions in human cells. The transfection of the mutant or wild-type CSB gene into the CS1AN.S3.G2 cells did not alter the expression of the subset of genes examined by cDNA array analysis.

Published

2002

39. Werner's syndrome protein (WRN) migrates Holliday junctions and co-localizes with RPA upon replication arrest

Author

Robert M. Brosh, Madalena Tarsounas, Julia K. Karow, Angelos Constantinou, Stephen C. West, Vilhelm A. Bohr, and Ian D. Hickson

Subjects

DNA Replication, congenital, hereditary, and neonatal diseases and abnormalities, Werner Syndrome Helicase, RecQ helicase, Biochemistry, Adenosine Triphosphate, Bacterial Proteins, Genetics, Holliday junction, medicine, Humans, education, Molecular Biology, Gene, Werner syndrome, Adenosine Triphosphatases, Cell Nucleus, Recombination, Genetic, education.field_of_study, biology, RecQ Helicases, Scientific Reports, DNA replication, DNA Helicases, Helicase, nutritional and metabolic diseases, DNA, medicine.disease, Molecular biology, Recombinant Proteins, Exodeoxyribonucleases, Microscopy, Fluorescence, biology.protein, Werner Syndrome, Homologous recombination, HeLa Cells

Abstract

Individuals affected by the autosomal recessive disorder Werner's syndrome (WS) develop many of the symptoms characteristic of premature ageing. Primary fibroblasts cultured from WS patients exhibit karyotypic abnormalities and a reduced replicative life span. The WRN gene encodes a 3'-5' DNA helicase, and is a member of the RecQ family, which also includes the product of the Bloom's syndrome gene (BLM). In this work, we show that WRN promotes the ATP-dependent translocation of Holliday junctions, an activity that is also exhibited by BLM. In cells arrested in S-phase with hydroxyurea, WRN localizes to discrete nuclear foci that coincide with those formed by the single-stranded DNA binding protein replication protein A. These results are consistent with a model in which WRN prevents aberrant recombination events at sites of stalled replication forks by dissociating recombination intermediates.

Published

2000

40. The Werner Syndrome Protein Is Involved in RNA Polymerase II Transcription

Author

Jan O. Nehlin, Alfred May, Robert M. Brosh, David K. Orren, George M. Martin, Vilhelm A. Bohr, Matthew D. Gray, Junko Oshima, Amrita Machwe, and Adayabalam S. Balajee

Subjects

Cell Extracts, Repetitive Sequences, Amino Acid, Cell Membrane Permeability, Werner Syndrome Helicase, Transcription, Genetic, Molecular Sequence Data, Fluorescent Antibody Technique, RNA polymerase II, Article, Cell Line, Humans, Amino Acid Sequence, Molecular Biology, RNA polymerase II holoenzyme, Cell Nucleus, biology, General transcription factor, RecQ Helicases, Genetic Complementation Test, DNA Helicases, Promoter, Cell Biology, Molecular biology, Chromatin, Exodeoxyribonucleases, Mutation, biology.protein, Transcription factor II H, RNA, Transcription factor II F, RNA Polymerase II, Werner Syndrome, Transcription factor II D, Transcription factor II B, Plasmids

Abstract

Werner syndrome (WS) is a human progeroid syndrome characterized by the early onset of a large number of clinical features associated with the normal aging process. The complex molecular and cellular phenotypes of WS involve characteristic features of genomic instability and accelerated replicative senescence. The gene involved (WRN) was recently cloned, and its gene product (WRNp) was biochemically characterized as a helicase. Helicases play important roles in a variety of DNA transactions, including DNA replication, transcription, repair, and recombination. We have assessed the role of the WRN gene in transcription by analyzing the efficiency of basal transcription in WS lymphoblastoid cell lines that carry homozygous WRN mutations. Transcription was measured in permeabilized cells by [3H]UTP incorporation and in vitro by using a plasmid template containing the RNA polymerase II (RNA pol II)–dependent adenovirus major late promoter. With both of these approaches, we find that the transcription efficiency in different WS cell lines is reduced to 40–60% of the transcription in cells from normal individuals. This defect can be complemented by the addition of normal cell extracts to the chromatin of WS cells. Addition of purified wild-type WRNp but not mutated WRNp to the in vitro transcription assay markedly stimulates RNA pol II–dependent transcription carried out by nuclear extracts. A nonhelicase domain (a direct repeat of 27 amino acids) also appears to have a role in transcription enhancement, as revealed by a yeast hybrid–protein reporter assay. This is further supported by the lack of stimulation of transcription when mutant WRNp lacking this domain was added to the in vitro assay. We have thus used several approaches to show a role for WRNp in RNA pol II transcription, possibly as a transcriptional activator. A deficit in either global or regional transcription in WS cells may be a primary molecular defect responsible for the WS clinical phenotype.

Published

1999

41. Molecular characterization of an acidic region deletion mutant of Cockayne syndrome group B protein.

Author

Sunesen, Morten, Selzer, Rebecca R., Jr, Robert M. Brosh, Balajee, Adayabalam S., Stevnsner, Tinna, and Bohr, Vilhelm A.

Published

2000

42. Impact papers on aging in 2009

Author

Blagosklonny, Mikhail V., Campisi, Judy, Bartke, Andrzej, Blasco, Maria A., Bonner, William M., Bohr, Vilhelm A., Jr, Robert M. Brosh, Brunet, Anne, Donehower, Lawrence A., Finch, Caleb E., Finkel, Toren, Gorospe, Myriam, Gudkov, Andrei V., Hall, Michael N., Hekimi, Siegfried, Helfand, Stephen L., Karlseder, Jan, Kenyon, Cynthia, Kroemer, Guido, Longo, Valter, Nussenzweig, Andre, Osiewacz, Heinz D., Peeper, Daniel S., Rando, Thomas A., Rudolph, K Lenhard, Sassone-Corsi, Paolo, Serrano, Manuel, Sharpless, Norman E., Skulachev, Vladimir P., Tower, John, Verdin, Eric, Vijg, Jan, Sinclair, David Andrew, DePinho, Ronald A., and Tilly, Jonathan Lee

Subjects

aging, senescence, signal transduction, genes for longevity

Abstract

The editorial board of Aging reviews research papers published in 2009, which they believe have or will have a significant impact on aging research. Among many others, the topics include genes that accelerate aging or in contrast promote longevity in model organisms, DNA damage responses and telomeres, molecular mechanisms of life span extension by calorie restriction and pharmacologic interventions into aging. The emerging message in 2009 is that aging is not random but determined by a genetically-regulated longevity network and can be decelerated both genetically and pharmacologically.

Published

2010

43. A high-throughput screen to identify novel small molecule inhibitors of the Werner Syndrome Helicase-Nuclease (WRN).

Author

Joshua A Sommers, Tomasz Kulikowicz, Deborah L Croteau, Thomas Dexheimer, Dorjbal Dorjsuren, Ajit Jadhav, David J Maloney, Anton Simeonov, Vilhelm A Bohr, and Robert M Brosh

Subjects

Medicine, Science

Abstract

Werner syndrome (WS), an autosomal recessive genetic disorder, displays accelerated clinical symptoms of aging leading to a mean lifespan less than 50 years. The WS helicase-nuclease (WRN) is involved in many important pathways including DNA replication, recombination and repair. Replicating cells are dependent on helicase activity, leading to the pursuit of human helicases as potential therapeutic targets for cancer treatment. Small molecule inhibitors of DNA helicases can be used to induce synthetic lethality, which attempts to target helicase-dependent compensatory DNA repair pathways in tumor cells that are already genetically deficient in a specific pathway of DNA repair. Alternatively, helicase inhibitors may be useful as tools to study the specialized roles of helicases in replication and DNA repair. In this study, approximately 350,000 small molecules were screened based on their ability to inhibit duplex DNA unwinding by a catalytically active WRN helicase domain fragment in a high-throughput fluorometric assay to discover new non-covalent small molecule inhibitors of the WRN helicase. Select compounds were screened to exclude ones that inhibited DNA unwinding by other helicases in the screen, bound non-specifically to DNA, acted as irreversible inhibitors, or possessed unfavorable chemical properties. Several compounds were tested for their ability to impair proliferation of cultured tumor cells. We observed that two of the newly identified WRN helicase inhibitors inhibited proliferation of cancer cells in a lineage-dependent manner. These studies represent the first high-throughput screen for WRN helicase inhibitors and the results have implications for anti-cancer strategies targeting WRN in different cancer cells and genetic backgrounds.

Published

2019

44. Impact of age-associated cyclopurine lesions on DNA repair helicases.

Author

Irfan Khan, Avvaru N Suhasini, Taraswi Banerjee, Joshua A Sommers, Daniel L Kaplan, Jochen Kuper, Caroline Kisker, and Robert M Brosh

Subjects

Medicine, Science

Abstract

8,5' cyclopurine deoxynucleosides (cPu) are locally distorting DNA base lesions corrected by nucleotide excision repair (NER) and proposed to play a role in neurodegeneration prevalent in genetically defined Xeroderma pigmentosum (XP) patients. In the current study, purified recombinant helicases from different classifications based on sequence homology were examined for their ability to unwind partial duplex DNA substrates harboring a single site-specific cPu adduct. Superfamily (SF) 2 RecQ helicases (RECQ1, BLM, WRN, RecQ) were inhibited by cPu in the helicase translocating strand, whereas helicases from SF1 (UvrD) and SF4 (DnaB) tolerated cPu in either strand. SF2 Fe-S helicases (FANCJ, DDX11 (ChlR1), DinG, XPD) displayed marked differences in their ability to unwind the cPu DNA substrates. Archaeal Thermoplasma acidophilum XPD (taXPD), homologue to the human XPD helicase involved in NER DNA damage verification, was impeded by cPu in the non-translocating strand, while FANCJ was uniquely inhibited by the cPu in the translocating strand. Sequestration experiments demonstrated that FANCJ became trapped by the translocating strand cPu whereas RECQ1 was not, suggesting the two SF2 helicases interact with the cPu lesion by distinct mechanisms despite strand-specific inhibition for both. Using a protein trap to simulate single-turnover conditions, the rate of FANCJ or RECQ1 helicase activity was reduced 10-fold and 4.5-fold, respectively, by cPu in the translocating strand. In contrast, single-turnover rates of DNA unwinding by DDX11 and UvrD helicases were only modestly affected by the cPu lesion in the translocating strand. The marked difference in effect of the translocating strand cPu on rate of DNA unwinding between DDX11 and FANCJ helicase suggests the two Fe-S cluster helicases unwind damaged DNA by distinct mechanisms. The apparent complexity of helicase encounters with an unusual form of oxidative damage is likely to have important consequences in the cellular response to DNA damage and DNA repair.

Published

2014

45. Human RECQ1 interacts with Ku70/80 and modulates DNA end-joining of double-strand breaks.

Author

Swetha Parvathaneni, Alexei Stortchevoi, Joshua A Sommers, Robert M Brosh, and Sudha Sharma

Subjects

Medicine, Science

Abstract

Genomic instability is a known precursor to cancer and aging. The RecQ helicases are a highly conserved family of DNA-unwinding enzymes that play key roles in maintaining genome stability in all living organisms. Human RecQ homologs include RECQ1, BLM, WRN, RECQ4, and RECQ5β, three of which have been linked to diseases with elevated risk of cancer and growth defects (Bloom Syndrome and Rothmund-Thomson Syndrome) or premature aging (Werner Syndrome). RECQ1, the first RecQ helicase discovered and the most abundant in human cells, is the least well understood of the five human RecQ homologs. We have previously described that knockout of RECQ1 in mice or knockdown of its expression in human cells results in elevated frequency of spontaneous sister chromatid exchanges, chromosomal instability, increased load of DNA damage and heightened sensitivity to ionizing radiation. We have now obtained evidence implicating RECQ1 in the nonhomologous end-joining pathway of DNA double-strand break repair. We show that RECQ1 interacts directly with the Ku70/80 subunit of the DNA-PK complex, and depletion of RECQ1 results in reduced end-joining in cell free extracts. In vitro, RECQ1 binds and unwinds the Ku70/80-bound partial duplex DNA substrate efficiently. Linear DNA is co-bound by RECQ1 and Ku70/80, and DNA binding by Ku70/80 is modulated by RECQ1. Collectively, these results provide the first evidence for an interaction of RECQ1 with Ku70/80 and a role of the human RecQ helicase in double-strand break repair through nonhomologous end-joining.

Published

2013

46. FANCJ/BACH1 acetylation at lysine 1249 regulates the DNA damage response.

Author

Jenny Xie, Min Peng, Shawna Guillemette, Steven Quan, Stephanie Maniatis, Yuliang Wu, Aditya Venkatesh, Scott A Shaffer, Robert M Brosh, and Sharon B Cantor

Subjects

Genetics, QH426-470

Abstract

BRCA1 promotes DNA repair through interactions with multiple proteins, including CtIP and FANCJ (also known as BRIP1/BACH1). While CtIP facilitates DNA end resection when de-acetylated, the function of FANCJ in repair processing is less well defined. Here, we report that FANCJ is also acetylated. Preventing FANCJ acetylation at lysine 1249 does not interfere with the ability of cells to survive DNA interstrand crosslinks (ICLs). However, resistance is achieved with reduced reliance on recombination. Mechanistically, FANCJ acetylation facilitates DNA end processing required for repair and checkpoint signaling. This conclusion was based on the finding that FANCJ and its acetylation were required for robust RPA foci formation, RPA phosphorylation, and Rad51 foci formation in response to camptothecin (CPT). Furthermore, both preventing and mimicking FANCJ acetylation at lysine 1249 disrupts FANCJ function in checkpoint maintenance. Thus, we propose that the dynamic regulation of FANCJ acetylation is critical for robust DNA damage response, recombination-based processing, and ultimately checkpoint maintenance.

Published

2012