Your search keyword '"Exonuclease 1"' showing total 222 results

1. Aicardi-Goutières Syndrome Type 1: A Novel Missense Variant and Review of the Mutational Spectrum.

Author

Tasharrofi, Behnoosh, Karimzadeh, Parvaneh, Asadollahi, Mostafa, Hasani, Sepideh, Heidari, Morteza, and Keramatipour, Mohammad

Subjects

POLYMERASE chain reaction, BRAIN, COMPUTED tomography, GENES, AICARDI-Goutieres syndrome, GENETIC mutation, GENETIC testing, PHENOTYPES, SEQUENCE analysis, SYMPTOMS

Abstract

Objectives Mutations in the TREX1 gene cause Aicardi-Goutières syndrome (AGS) 1, associated with a spectrum of autoimmune and neurodegenerative manifestations. AGS 1, the most severe neonatal type of AGS, is characterized by abnormal neurologic findings, visual inattention, hepatosplenomegaly, thrombocytopenia, skin rash, restlessness, and fever. Materials & Methods The present study described two affected siblings from an Iranian family whose phenotypes overlap with intrauterine infections. They had almost similar presentations, including developmental delay, microcephaly, no fix and follow epileptic seizures and the same pattern of brain CT scan involvements. Following clinical and paraclinical assessments, whole-exome sequencing was employed to determine the disease-causing variant, and subsequently, PCR-Sanger sequencing was performed to indicate the segregation pattern of the candidate variant in family members. Results Genetic analysis revealed a novel homozygous missense variant (c.461A>C; p.D154A) in the TREX1 gene in affected family members. Sanger sequencing of other family members showed the expected zygosities. Conclusion This study identifies a novel mutation in the TREX1 gene in this family and highlights the efficiency of next-generation sequencing-based techniques for obtaining a definite diagnosis in patients with early-onset encephalopathy. [ABSTRACT FROM AUTHOR]

Published

2024

2. The properties of Msh2–Msh6 ATP binding mutants suggest a signal amplification mechanism in DNA mismatch repair

Author

Graham, William J, Putnam, Christopher D, and Kolodner, Richard D

Subjects

Biochemistry and Cell Biology, Biological Sciences, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Adenosine Triphosphate, Crystallography, X-Ray, DNA Mismatch Repair, DNA-Binding Proteins, MutL Protein Homolog 1, MutS Homolog 2 Protein, Protein Binding, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, DNA repair, DNA replication, DNA mismatch repair, DNA endonuclease, DNA binding protein, mutagenesis, exonuclease 1, Mlh1-Pms1, Msh2-Msh6, MutS, S, cerevisiae, S. cerevisiae, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

DNA mismatch repair (MMR) corrects mispaired DNA bases and small insertion/deletion loops generated by DNA replication errors. After binding a mispair, the eukaryotic mispair recognition complex Msh2-Msh6 binds ATP in both of its nucleotide-binding sites, which induces a conformational change resulting in the formation of an Msh2-Msh6 sliding clamp that releases from the mispair and slides freely along the DNA. However, the roles that Msh2-Msh6 sliding clamps play in MMR remain poorly understood. Here, using Saccharomyces cerevisiae, we created Msh2 and Msh6 Walker A nucleotide-binding site mutants that have defects in ATP binding in one or both nucleotide-binding sites of the Msh2-Msh6 heterodimer. We found that these mutations cause a complete MMR defect in vivo The mutant Msh2-Msh6 complexes exhibited normal mispair recognition and were proficient at recruiting the MMR endonuclease Mlh1-Pms1 to mispaired DNA. At physiological (2.5 mm) ATP concentration, the mutant complexes displayed modest partial defects in supporting MMR in reconstituted Mlh1-Pms1-independent and Mlh1-Pms1-dependent MMR reactions in vitro and in activation of the Mlh1-Pms1 endonuclease and showed a more severe defect at low (0.1 mm) ATP concentration. In contrast, five of the mutants were completely defective and one was mostly defective for sliding clamp formation at high and low ATP concentrations. These findings suggest that mispair-dependent sliding clamp formation triggers binding of additional Msh2-Msh6 complexes and that further recruitment of additional downstream MMR proteins is required for signal amplification of mispair binding during MMR.

Published

2018

3. A Comprehensive Analysis of Northern versus Liquid Hybridization Assays for mRNAs, Small RNAs, and miRNAs Using a Non-Radiolabeled Approach

Author

Waqar Ahmad, Bushra Gull, Jasmin Baby, and Farah Mustafa

Subjects

northern blotting, liquid hybridization assay, exonuclease 1, non-radioactive, biotinylation, mRNA, Biology (General), QH301-705.5

Abstract

Northern blotting (NB), a gold standard for RNA detection, has lost its charm due to its hands-on nature, need for good quality RNA, and radioactivity. With the emergence of the field of microRNAs (miRNAs), the necessity for sensitive and quantitative NBs has again emerged. Here, we developed highly sensitive yet non-radiolabeled, fast, economical NB, and liquid hybridization (LH) assays without radioactivity or specialized reagents like locked nucleic acid (LNA)- or digoxigenin-labeled probes for mRNAs/small RNAs, especially miRNAs using biotinylated probes. An improvised means of hybridizing oligo probes along with efficient transfer, cross-linking, and signal enhancement techniques was employed. Important caveats of each assay were elaborated upon, especially issues related to probe biotinylation, use of exonuclease, and bioimagers not reported earlier. We demonstrate that, while the NBs were sensitive for mRNAs and small RNAs, our LH protocol could efficiently detect these and miRNAs using less than 10–100 times the total amount of RNA, a sensitivity comparable to radiolabeled probes. Compared to NBs, LH was a faster, more sensitive, and specific approach for mRNA/small RNA/miRNA detection. A comparison of present work with six seminal studies is presented along with detailed protocols for easy reproducibility. Overall, our study provides effective platforms to study large and small RNAs in a sensitive, efficient, and cost-effective manner.

Published

2021

4. Specific Human ATR and ATM Inhibitors Modulate Single Strand DNA Formation in Leishmania major Exposed to Oxidative Agent.

Author

da Silva, Raíssa Bernardes, Bertoldo, Willian dos Reis, Naves, Lucila Langoni, de Vito, Fernanda Bernadelli, Damasceno, Jeziel Dener, Tosi, Luiz Ricardo Orsini, Machado, Carlos Renato, and Pedrosa, André Luiz

Subjects

LEISHMANIA major, ATAXIA telangiectasia, SINGLE-stranded DNA, EXONUCLEASES, AUTOMATED teller machines, NEGLECTED diseases

Abstract

Leishmania parasites are the causative agents of a group of neglected tropical diseases known as leishmaniasis. The molecular mechanisms employed by these parasites to adapt to the adverse conditions found in their hosts are not yet completely understood. DNA repair pathways can be used by Leishmania to enable survival in the interior of macrophages, where the parasite is constantly exposed to oxygen reactive species. In higher eukaryotes, DNA repair pathways are coordinated by the central protein kinases ataxia telangiectasia mutated (ATM) and ataxia telangiectasia and Rad3 related (ATR). The enzyme Exonuclease-1 (EXO1) plays important roles in DNA replication, repair, and recombination, and it can be regulated by ATM- and ATR-mediated signaling pathways. In this study, the DNA damage response pathways in promastigote forms of L. major were investigated using bioinformatics tools, exposure of lineages to oxidizing agents and radiation damage, treatment of cells with ATM and ATR inhibitors, and flow cytometry analysis. We demonstrated high structural and important residue conservation for the catalytic activity of the putative Lmj EXO1. The overexpression of putative Lmj EXO1 made L. major cells more susceptible to genotoxic damage, most likely due to the nuclease activity of this enzyme and the occurrence of hyper-resection of DNA strands. These cells could be rescued by the addition of caffeine or a selective ATM inhibitor. In contrast, ATR-specific inhibition made the control cells more susceptible to oxidative damage in an Lmj EXO1 overexpression-like manner. We demonstrated that ATR-specific inhibition results in the formation of extended single-stranded DNA, most likely due to EXO1 nucleasic activity. Antagonistically, ATM inhibition prevented single-strand DNA formation, which could explain the survival phenotype of lineages overexpressing Lmj EXO1. These results suggest that an ATM homolog in Leishmania could act to promote end resection by putative Lmj EXO1, and an ATR homologue could prevent hyper-resection, ensuring adequate repair of the parasite DNA. [ABSTRACT FROM AUTHOR]

Published

2022

5. Specific Human ATR and ATM Inhibitors Modulate Single Strand DNA Formation in Leishmania major Exposed to Oxidative Agent

Author

Raíssa Bernardes da Silva, Willian dos Reis Bertoldo, Lucila Langoni Naves, Fernanda Bernadelli de Vito, Jeziel Dener Damasceno, Luiz Ricardo Orsini Tosi, Carlos Renato Machado, and André Luiz Pedrosa

Subjects

Leishmania major (L. major), DNA repair, exonuclease 1, ataxia telangiectasia mutated (ATM), ataxia telangiectasia and Rad3 related kinase (ATR), Microbiology, QR1-502

Abstract

Leishmania parasites are the causative agents of a group of neglected tropical diseases known as leishmaniasis. The molecular mechanisms employed by these parasites to adapt to the adverse conditions found in their hosts are not yet completely understood. DNA repair pathways can be used by Leishmania to enable survival in the interior of macrophages, where the parasite is constantly exposed to oxygen reactive species. In higher eukaryotes, DNA repair pathways are coordinated by the central protein kinases ataxia telangiectasia mutated (ATM) and ataxia telangiectasia and Rad3 related (ATR). The enzyme Exonuclease-1 (EXO1) plays important roles in DNA replication, repair, and recombination, and it can be regulated by ATM- and ATR-mediated signaling pathways. In this study, the DNA damage response pathways in promastigote forms of L. major were investigated using bioinformatics tools, exposure of lineages to oxidizing agents and radiation damage, treatment of cells with ATM and ATR inhibitors, and flow cytometry analysis. We demonstrated high structural and important residue conservation for the catalytic activity of the putative LmjEXO1. The overexpression of putative LmjEXO1 made L. major cells more susceptible to genotoxic damage, most likely due to the nuclease activity of this enzyme and the occurrence of hyper-resection of DNA strands. These cells could be rescued by the addition of caffeine or a selective ATM inhibitor. In contrast, ATR-specific inhibition made the control cells more susceptible to oxidative damage in an LmjEXO1 overexpression-like manner. We demonstrated that ATR-specific inhibition results in the formation of extended single-stranded DNA, most likely due to EXO1 nucleasic activity. Antagonistically, ATM inhibition prevented single-strand DNA formation, which could explain the survival phenotype of lineages overexpressing LmjEXO1. These results suggest that an ATM homolog in Leishmania could act to promote end resection by putative LmjEXO1, and an ATR homologue could prevent hyper-resection, ensuring adequate repair of the parasite DNA.

Published

2022

6. Activation of Saccharomyces cerevisiae Mlh1-Pms1 Endonuclease in a Reconstituted Mismatch Repair System*

Author

Smith, Catherine E, Bowen, Nikki, Graham, William J, Goellner, Eva M, Srivatsan, Anjana, and Kolodner, Richard D

Subjects

Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, Generic health relevance, Adaptor Proteins, Signal Transducing, Biocatalysis, Carrier Proteins, Cations, Divalent, DNA Mismatch Repair, Enzyme Activation, Genes, Dominant, MutL Protein Homolog 1, MutL Proteins, Mutant Proteins, Mutation, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, DNA recombination, DNA repair, DNA replication, mutagenesis, proliferating cell nuclear antigen, replication factor C, yeast genetics, exonuclease 1, genome instability, Msh2-Msh6, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences

Abstract

Previous studies reported the reconstitution of an Mlh1-Pms1-independent 5' nick-directed mismatch repair (MMR) reaction using Saccharomyces cerevisiae proteins. Here we describe the reconstitution of a mispair-dependent Mlh1-Pms1 endonuclease activation reaction requiring Msh2-Msh6 (or Msh2-Msh3), proliferating cell nuclear antigen (PCNA), and replication factor C (RFC) and a reconstituted Mlh1-Pms1-dependent 3' nick-directed MMR reaction requiring Msh2-Msh6 (or Msh2-Msh3), exonuclease 1 (Exo1), replication protein A (RPA), RFC, PCNA, and DNA polymerase δ. Both reactions required Mg(2+) and Mn(2+) for optimal activity. The MMR reaction also required two reaction stages in which the first stage required incubation of Mlh1-Pms1 with substrate DNA, with or without Msh2-Msh6 (or Msh2-Msh3), PCNA, and RFC but did not require nicking of the substrate, followed by a second stage in which other proteins were added. Analysis of different mutant proteins demonstrated that both reactions required a functional Mlh1-Pms1 endonuclease active site, as well as mispair recognition and Mlh1-Pms1 recruitment by Msh2-Msh6 but not sliding clamp formation. Mutant Mlh1-Pms1 and PCNA proteins that were defective for Exo1-independent but not Exo1-dependent MMR in vivo were partially defective in the Mlh1-Pms1 endonuclease and MMR reactions, suggesting that both reactions reflect the activation of Mlh1-Pms1 seen in Exo1-independent MMR in vivo. The availability of this reconstituted MMR reaction should now make it possible to better study both Exo1-independent and Exo1-dependent MMR.

Published

2015

7. Perturbation of base excision repair sensitizes breast cancer cells to APOBEC3 deaminase-mediated mutations

Author

Birong Shen, Joseph H Chapman, Michael F Custance, Gianna M Tricola, Charles E Jones, and Anthony V Furano

Subjects

base excision repair, nei-like glycosylase, APOBEC3 deaminase, breast cancer, exonuclease 1, Medicine, Science, Biology (General), QH301-705.5

Abstract

Abundant APOBEC3 (A3) deaminase-mediated mutations can dominate the mutational landscape (‘mutator phenotype’) of some cancers, however, the basis of this sporadic vulnerability is unknown. We show here that elevated expression of the bifunctional DNA glycosylase, NEIL2, sensitizes breast cancer cells to A3B-mediated mutations and double-strand breaks (DSBs) by perturbing canonical base excision repair (BER). NEIL2 usurps the canonical lyase, APE1, at abasic sites in a purified BER system, rendering them poor substrates for polymerase β. However, the nicked NEIL2 product can serve as an entry site for Exo1 in vitro to generate single-stranded DNA, which would be susceptible to both A3B and DSBs. As NEIL2 or Exo1 depletion mitigates the DNA damage caused by A3B expression, we suggest that aberrant NEIL2 expression can explain certain instances of A3B-mediated mutations.

Published

2020

8. Multi-functions of exonuclease 1 in DNA damage response and cancer susceptibility

Author

Ping-Kun Zhou, Shanshan Gao, and Shuang Yan

Subjects

DNA double-strand break (DSB), Exonuclease, DNA end resection, DNA recombination, DNA damage, DNA repair, Strategy and Management, R895-920, medicine.disease_cause, Industrial and Manufacturing Engineering, Exonuclease 1(EXO1), Medical physics. Medical radiology. Nuclear medicine, Exonuclease 1, chemistry.chemical_compound, medicine, Mutation, Radiotherapy, biology, Chemistry, Mechanical Engineering, Metals and Alloys, DNA replication, Cancer susceptibility, Cell biology, biology.protein, Homologous recombination, DNA

Abstract

Exonuclease 1 (EXO1) can catalyze nucleotide chain excision with its conserved N-terminal domain of 5′ to 3′ exonuclease activity, enabling it to influence diverse biological processes facing the challenges of genotoxic environmental factors such as ionizing radiation. This nuclease activity enables EXO1 to maintain replication forks and telomeres length, to facilitate post-replication DNA repair and to process the end resection step of homologous recombination of DNA double-strand breaks-induced by ionizing radiation. When DNA replication is disrupted or blocked, EXO1 can cleave the broken DNA ends to form 3’ ssDNA, leading to repair pathways activation. Excess EXO1-mediated nucleotide excision, however, can introduce an abundance of single-stranded DNA that can cause mutation and recombination via micro-homology-mediated end joining or single-strand annealing mechanisms, contributing to a loss of genetic information. EXO1 activity must therefore be carefully regulated within healthy cells. The mutations and dysregulations of EXO1 can increase the sensitivity of cells to radiation injury and risk of oncogenic transformation, limit the adoption of specific treatments in a range of human diseases. As such, EXO1 represents a promising target for the treatment and prevention of cancer. In the present review, we delineate the structural properties and functional characteristics of EXO1, discuss the relationship between this exonuclease and cancer susceptibility as well as the second cancers related to radiotherapy.

Published

2021

9. Exonuclease 1

Author

Choi, Sangdun, editor

Published

2018

10. Human Exonuclease 1 (EXO1) Regulatory Functions in DNA Replication with Putative Roles in Cancer

Author

Guido Keijzers, Daniela Bakula, Michael Angelo Petr, Nils Gedsig Kirkelund Madsen, Amanuel Teklu, Garik Mkrtchyan, Brenna Osborne, and Morten Scheibye-Knudsen

Subjects

DNA repair, double strand break repair, exonuclease 1, EXO1, mismatch repair, MMR, NER, nucleotide excision repair, strand displacements, TLS, translesion DNA synthesis, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Human exonuclease 1 (EXO1), a 5′→3′ exonuclease, contributes to the regulation of the cell cycle checkpoints, replication fork maintenance, and post replicative DNA repair pathways. These processes are required for the resolution of stalled or blocked DNA replication that can lead to replication stress and potential collapse of the replication fork. Failure to restart the DNA replication process can result in double-strand breaks, cell-cycle arrest, cell death, or cellular transformation. In this review, we summarize the involvement of EXO1 in the replication, DNA repair pathways, cell cycle checkpoints, and the link between EXO1 and cancer.

Published

2018

11. C. elegans electrotaxis behavior is modulated by heat shock response and unfolded protein response signaling pathways

Author

P. Ravi Selvaganapathy, Shane K. B. Taylor, Muhammad H. Minhas, Bhagwati P. Gupta, Ram K. Mishra, and Justin Tong

Subjects

Paraquat, Hot Temperature, Science, Gene Expression, Biology, Article, Behavioural methods, 03 medical and health sciences, Exonuclease 1, chemistry.chemical_compound, Electromagnetic Fields, 0302 clinical medicine, Electricity, Stress, Physiological, Lab-On-A-Chip Devices, Animals, Taxis Response, Chronic stress, Heat shock, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Biological models, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Gene Expression Profiling, Tunicamycin, Endoplasmic reticulum, Endoplasmic Reticulum Stress, Cell biology, Cytosol, chemistry, Exoribonucleases, Behavioural genetics, Unfolded Protein Response, Unfolded protein response, Medicine, Signal transduction, Stress and resilience, Heat-Shock Response, Locomotion, 030217 neurology & neurosurgery, Signal Transduction

Abstract

The nematode C. elegans is a leading model to investigate the mechanisms of stress-induced behavioral changes coupled with biochemical mechanisms. Our group has previously characterized C. elegans behavior using a microfluidic-based electrotaxis device, and showed that worms display directional motion in the presence of a mild electric field. In this study, we describe the effects of various forms of genetic and environmental stress on the electrotactic movement of animals. Using exposure to chemicals, such as paraquat and tunicamycin, as well as mitochondrial and endoplasmic reticulum (ER) unfolded protein response (UPR) mutants, we demonstrate that chronic stress causes abnormal movement. Additionally, we report that pqe-1 (human RNA exonuclease 1 homolog) is necessary for the maintenance of multiple stress response signaling and electrotaxis behavior of animals. Further, exposure of C. elegans to several environmental stress-inducing conditions revealed that while chronic heat and dietary restriction caused electrotaxis speed deficits due to prolonged stress, daily exercise had a beneficial effect on the animals, likely due to improved muscle health and transient activation of UPR. Overall, these data demonstrate that the electrotaxis behavior of worms is susceptible to cytosolic, mitochondrial, and ER stress, and that multiple stress response pathways contribute to its preservation in the face of stressful stimuli.

Published

2021

12. Mispair-bound human MutS–MutL complex triggers DNA incisions and activates mismatch repair

Author

Guo Min Li, Wei Yang, Grace Sanghee Lee, Liya Gu, and Janice Ortega

Subjects

Adenosine Triphosphatases, congenital, hereditary, and neonatal diseases and abnormalities, Nuclease, DNA Repair, biology, Base Pair Mismatch, DNA, Cell Biology, DNA Mismatch Repair, MutS DNA Mismatch-Binding Protein, Article, Cell biology, DNA-Binding Proteins, Exonuclease 1, chemistry.chemical_compound, chemistry, biology.protein, Humans, DNA mismatch repair, Molecular Biology

Abstract

DNA mismatch repair (MMR) relies on MutS and MutL ATPases for mismatch recognition and strand-specific nuclease recruitment to remove mispaired bases in daughter strands. However, whether the MutS–MutL complex coordinates MMR by ATP-dependent sliding on DNA or protein–protein interactions between the mismatch and strand discrimination signal is ambiguous. Using functional MMR assays and systems preventing proteins from sliding, we show that sliding of human MutSα is required not for MMR initiation, but for final mismatch removal. MutSα recruits MutLα to form a mismatch-bound complex, which initiates MMR by nicking the daughter strand 5′ to the mismatch. Exonuclease 1 (Exo1) is then recruited to the nick and conducts 5′ → 3′ excision. ATP-dependent MutSα dissociation from the mismatch is necessary for Exo1 to remove the mispaired base when the excision reaches the mismatch. Therefore, our study has resolved a long-standing puzzle, and provided new insights into the mechanism of MMR initiation and mispair removal.

Published

2021

13. EXO1 Plays a Carcinogenic Role in Hepatocellular Carcinoma and is related to the regulation of FOXP3

Author

Er-lei Zhang, Bin-yong Liang, Keshuai Dong, Zun-yi Zhang, Xiaoping Chen, Zhiyong Huang, and Guang Yang

Subjects

Gene knockdown, Nuclease, biology, Oncogene, FOXP3, Hepatocellular carcinoma, Chemistry, Cell growth, EXO1, Metastasis, Exonuclease 1, Transcriptional regulation, Oncology, Cancer research, biology.protein, Transcription factor, Research Paper

Abstract

Exonuclease 1 (EXO1), a member of the RAD2 nuclease family, was first described as possessing 5' to 3' nuclease activity and 5' structure-specific endonuclease activity. Here, we show that EXO1 is significantly upregulated in HCC tumor tissues and that high EXO1 expression is significantly correlated with liver cirrhosis. We further demonstrate that EXO1 knockdown decreases proliferation and colony forming abilities of HCC cells in vitro and tumorigenicity in vivo, as well as decreases migration and invasive capabilities of HCC cells. Alternatively, EXO1 overexpression significantly increases the proliferation, colony forming ability, and migration and invasive capabilities of HCC cells in vitro. Additionally, we truncated a region upstream of the transcription start site (TSS) of EXO1 and used the region with the strongest transcriptional activity to predict that the transcription factor FOXP3 can bind to the EXO1 promoter. Bioinformatics analysis found that FOXP3 was positively correlated with EXO1 and luciferase reporter assays and RT-PCR confirmed that FOXP3 could enhance the transcriptional activity of EXO1. CCK-8 assays showed that depletion of FOXP3 further reduces cell proliferation ability after knocking down of EXO1 in vitro. Taken together, our findings indicate that EXO1 acts as an oncogene in HCC and its expression level is related to FOXP3 activity.

Published

2020

14. Association of C>T p757l Polymorphism in EXO1 Gene and Risk of Sporadic Colorectal Cancer in an Iranian Population

Author

Mahdi Montazer Haghighi, Mohammad Yaghoob Yaghoub Taleghani, Atena Irani Shemirani, Zahra Akbari, Mohsen Vahedi, Seyyed Reza Mohebi, Seyyed Reza Fatemi, Arash Jenabian, and Mohammadreza Zali

Subjects

colorectal neoplasms, gene, exonuclease 1, polymorphism, single nucleotide, Medicine

Abstract

Introduction & Objective: One candidate gene for colorectal cancer susceptibility is exonuclease1 (EXO1) .It is a member of RAD2 nuclease family. It plays a main role in mismatch repair. EXO1 acts also in DNA replication and recombination. Single nucleotide polymorphisms (SNPs) are shown to be related with cancer incidence. The aim of the present study was to examine the association between P757L polymorphism at exon 13 of the EXO1 gene and the risk of colorectal cancer in an Iranian population. Materials & Methods: In this case-control study, 81cases and 86 healthy controls were selected from among individuals who were referred toTehran Taleghani hospital during 2008-2009. The individuals were divided into two groups, case and control, based on their colonoscopy and pathology results. Genotype analysis was performed using polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) method and MNII restriction enzyme. Totally 167 samples were analyzed. Results: Based on our findings when Pro/Pro genotype was reference for the Leu/Leu (TT) genotype (OR=0.168, 95%CI 0.034-0.816), it showed a reverse association with colorectal cancer. While Pro/Leu (CT) genotype did not revealed a significant association with colorectal cancer at the same status. (OR=0.663, 95%CI 0.340-1.294). Conclusion: The results of this study were compatible with other investigations which convey Leu/Leu (TT) genotype of EXO1 has reverse association with colorectal cancer. Therefore TT genotype has a protective effect against colorectal cancer.

Published

2011

15. Specific Human ATR and ATM Inhibitors Modulate Single Strand DNA Formation in

Author

Raíssa Bernardes, da Silva, Willian Dos Reis, Bertoldo, Lucila Langoni, Naves, Fernanda Bernadelli, de Vito, Jeziel Dener, Damasceno, Luiz Ricardo Orsini, Tosi, Carlos Renato, Machado, and André Luiz, Pedrosa

Subjects

ataxia telangiectasia and Rad3 related kinase (ATR), Leishmania major (L. major), DNA, Single-Stranded, DNA repair, Ataxia Telangiectasia Mutated Proteins, DNA, Protozoan, exonuclease 1, Oxidative Stress, Cellular and Infection Microbiology, ataxia telangiectasia mutated (ATM), Humans, Phosphorylation, Leishmania major, Original Research

Abstract

Leishmania parasites are the causative agents of a group of neglected tropical diseases known as leishmaniasis. The molecular mechanisms employed by these parasites to adapt to the adverse conditions found in their hosts are not yet completely understood. DNA repair pathways can be used by Leishmania to enable survival in the interior of macrophages, where the parasite is constantly exposed to oxygen reactive species. In higher eukaryotes, DNA repair pathways are coordinated by the central protein kinases ataxia telangiectasia mutated (ATM) and ataxia telangiectasia and Rad3 related (ATR). The enzyme Exonuclease-1 (EXO1) plays important roles in DNA replication, repair, and recombination, and it can be regulated by ATM- and ATR-mediated signaling pathways. In this study, the DNA damage response pathways in promastigote forms of L. major were investigated using bioinformatics tools, exposure of lineages to oxidizing agents and radiation damage, treatment of cells with ATM and ATR inhibitors, and flow cytometry analysis. We demonstrated high structural and important residue conservation for the catalytic activity of the putative LmjEXO1. The overexpression of putative LmjEXO1 made L. major cells more susceptible to genotoxic damage, most likely due to the nuclease activity of this enzyme and the occurrence of hyper-resection of DNA strands. These cells could be rescued by the addition of caffeine or a selective ATM inhibitor. In contrast, ATR-specific inhibition made the control cells more susceptible to oxidative damage in an LmjEXO1 overexpression-like manner. We demonstrated that ATR-specific inhibition results in the formation of extended single-stranded DNA, most likely due to EXO1 nucleasic activity. Antagonistically, ATM inhibition prevented single-strand DNA formation, which could explain the survival phenotype of lineages overexpressing LmjEXO1. These results suggest that an ATM homolog in Leishmania could act to promote end resection by putative LmjEXO1, and an ATR homologue could prevent hyper-resection, ensuring adequate repair of the parasite DNA.

Published

2021

16. Role of EXO1 nuclease activity in genome maintenance, the immune response and tumor suppression in Exo1D173A mice

Author

Richard Chahwan, Stephen Gray, Sergio Roa, Shanzhi Wang, Thomas MacCarthy, Matthew D. Scharff, Winfried Edelmann, Yongwei Zhang, Rikke Morrish, Catherine Tangcatherin, Kyeryoung Lee, Elena Tosti, Johanna van Oers, and Paula E. Cohen

Subjects

Nuclease, chemistry.chemical_compound, Exonuclease 1, biology, Chemistry, DNA repair, DNA damage, Mutant, biology.protein, Somatic hypermutation, DNA Exonuclease, DNA, Cell biology

Abstract

DNA damage response pathways rely extensively on nuclease activity to process DNA intermediates. Exonuclease 1 (EXO1) is a pleiotropic evolutionary conserved DNA exonuclease involved in various DNA repair pathways, replication, antibody diversification, and meiosis. But, whether EXO1 facilitates these DNA metabolic processes through its enzymatic or scaffolding functions remains unclear. Here we dissect the contribution of EXO1 enzymatic versus scaffolding activity by comparing Exo1DA/DA mice expressing a proven nuclease-dead mutant form of EXO1 to entirely EXO1-deficient Exo1−/− and EXO1 wild type Exo1+/+ mice. We show that Exo1DA/DA and Exo1−/− mice are compromised in canonical DNA repair processing, suggesting that the EXO1 enzymatic role is important for error-free DNA mismatch and double-strand break repair pathways. However, in non-canonical repair pathways, EXO1 appears to have a more nuanced function. Next-generation sequencing of heavy chain V region in B cells showed the mutation spectra of Exo1DA/DA mice to be intermediate between Exo1+/+ and Exo1−/− mice, suggesting that both catalytic and scaffolding roles of EXO1 are important for somatic hypermutation. Similarly, while overall class switch recombination in Exo1DA/DA and Exo1−/− mice was comparably defective, switch-switch junction analysis suggests that EXO1 might fulfill an additional scaffolding function downstream of class switching. In contrast to Exo1−/− mice that are infertile, meiosis progressed normally in Exo1DA/DA and Exo1+/+ cohorts, indicating that a structural but not the nuclease function of EXO1 is critical for meiosis. However, both Exo1DA/DA and Exo1−/− mice displayed similar mortality and cancer predisposition profiles. Taken together, these data demonstrate that EXO1 has both scaffolding and enzymatic functions in distinct DNA repair processes and suggest a more composite and intricate role for EXO1 in DNA metabolic processes and disease.

Published

2021

17. Rad27 and Exo1 function in different excision pathways for mismatch repair in Saccharomyces cerevisiae

Author

Bin-Zhong Li, Richard D. Kolodner, Kendall A Torres, Christopher D. Putnam, Felipe A. Calil, Nikki Bowen, and Katarina Nguyen

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Saccharomyces cerevisiae Proteins, DNA Ligases, Flap Endonucleases, Science, 1.1 Normal biological development and functioning, Saccharomyces cerevisiae, General Physics and Astronomy, Eukaryotic DNA replication, medicine.disease_cause, MLH1, complex mixtures, DNA Mismatch Repair, General Biochemistry, Genetics and Molecular Biology, Article, Exonuclease 1, chemistry.chemical_compound, Underpinning research, Proliferating Cell Nuclear Antigen, Genetics, medicine, DNA, Fungal, Mutation, Multidisciplinary, biology, General Chemistry, DNA, biology.organism_classification, digestive system diseases, Fungal, Exodeoxyribonucleases, MutL Proteins, chemistry, MSH2, Microsatellite instability, DNA mismatch repair, Generic health relevance

Abstract

Eukaryotic DNA Mismatch Repair (MMR) involves redundant exonuclease 1 (Exo1)-dependent and Exo1-independent pathways, of which the Exo1-independent pathway(s) is not well understood. The exo1Δ440-702 mutation, which deletes the MutS Homolog 2 (Msh2) and MutL Homolog 1 (Mlh1) interacting peptides (SHIP and MIP boxes, respectively), eliminates the Exo1 MMR functions but is not lethal in combination with rad27Δ mutations. Analyzing the effect of different combinations of the exo1Δ440-702 mutation, a rad27Δ mutation and the pms1-A99V mutation, which inactivates an Exo1-independent MMR pathway, demonstrated that each of these mutations inactivates a different MMR pathway. Furthermore, it was possible to reconstitute a Rad27- and Msh2-Msh6-dependent MMR reaction in vitro using a mispaired DNA substrate and other MMR proteins. Our results demonstrate Rad27 defines an Exo1-independent eukaryotic MMR pathway that is redundant with at least two other MMR pathways., Defects in DNA mismatch repair (MMR) have been linked to inherited and sporadic cancers. Here the authors demonstrate that the DNA repair protein Rad27 (human FEN1) functions in one of three redundant mispair excision pathways, where its flap endonuclease activity catalyzes mispair excision.

Published

2021

18. ZGRF1 promotes end resection of DNA homologous recombination via forming complex with BRCA1/EXO1

Author

Hua Guan, Chenjun Bai, Da-Fei Xie, Ping-Kun Zhou, Shuang Yan, Xiao-yu Cao, Man Song, Jie Ping, Shu-ting Lai, and Shanshan Gao

Subjects

Cancer Research, Cell cycle checkpoint, QH573-671, DNA damage, Chemistry, DNA repair, Immunology, Regulator, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell Biology, DNA, Article, Cell biology, Cellular and Molecular Neuroscience, Exonuclease 1, chemistry.chemical_compound, Targeted therapies, Null cell, Cytology, Homologous recombination, RC254-282

Abstract

To maintain genomic stability, the mammalian cells has evolved a coordinated response to DNA damage, including activation of DNA repair and cell cycle checkpoint processes. Exonuclease 1 (EXO1)-dependent excision of DNA ends is important for the initiation of homologous recombination (HR) repair of DNA breaks, which is thought to play a key role in activating the ATR-CHK1 pathway to induce G2/M cell cycle arrest. But the mechanism is still not fully understood. Here, we report that ZGRF1 forms complexes with EXO1 as well as other repair proteins and promotes DNA repair through HR. ZGRF1 is recruited to DNA damage sites in a MDC1-RNF8-BRCA1 dependent manner. Furthermore, ZGRF1 is important for the recruitment of RPA2 to DNA damage sites and the following ATR-CHK1 mediated G2/M checkpoint in response to irradiation. ZGRF1 null cells show increased sensitivity to many DNA-damaging agents, especially PARPi and irradiation. Collectively,our findings identify ZGRF1 as a novel regulator of DNA end resection and G2/M checkpoint. ZGRF1 is a potential target of radiation and PARPi cancer therapy.

Published

2021

19. Association of DNA repair gene polymorphisms with response to cisplatin-based concurrent chemoradiotherapy in patients with cervical carcinoma.

Author

Liu, Jin-hui, Xi, Pei, Chai, Yan-lan, Wang, Juan, Wang, Tao, Liu, Zi, and Dai, Peng-gao

Subjects

*DNA repair, *CISPLATIN, *SINGLE nucleotide polymorphisms, *CHEMORADIOTHERAPY, *CERVICAL cancer treatment, *CERVICAL cancer, *GENETICS

Abstract

Purpose The aim of this study was to investigate polymorphisms in DNA repair genes as potential predictive factors among Chinese cervical cancer patients. Methods A total of 72 patients with cervical carcinoma, who received cisplatin-based chemoradiotherapy and whose responses were evaluated by Response Evaluation Criteria in Solid Tumors, were included. The association between response to chemoradiotherapy and the genotypes for 29 single-nucleotide polymorphisms (SNPs) in 25 DNA repair genes were analyzed. Results A minor allele of SNP rs9350 in the exonuclease 1 gene was associated with a better response rate, regardless of age and tumor stage (odds ratio, 8.316; p = 0.002). Conclusion SNP rs9350 in the exonuclease 1 gene is involved in inter-individual differences in the response to cisplatin-based chemoradiotherapy, in patients with cervical carcinoma. [ABSTRACT FROM AUTHOR]

Published

2016

20. Association between three exonuclease 1 polymorphisms and cancer risks: a meta-analysis.

Author

Zi-Yu Chen, Si-Rong Zheng, Jie-Hui Zhong, Xiao-Duan Zhuang, and Jue-Yu Zhou

Subjects

*EXONUCLEASES, *META-analysis, *GENETIC polymorphisms, *CANCER risk factors, *CIGARETTE smokers, *DISEASES

Abstract

To date, the results of studies exploring the relation between exonuclease 1 (Exo1) polymorphisms and cancer risks have differed. In this study, we performed a meta-analysis to investigate the effect of the three most extensively studied Exo1 polymorphisms (Pro757Leu, Glu589Lys, and Glu670Gly) on cancer susceptibility. The related studies published before August 5, 2015, were collected by searching the PubMed and EMBASE databases. We found 16 publications containing studies that were eligible for our study, including 10 studies for Pro757Leu polymorphism (4,093 cases and 3,834 controls), 12 studies for Glu589Lys polymorphism (6,479 cases and 6,550 controls), and 7 studies for Glu670Gly polymorphism (3,700 cases and 3,496 controls). Pooled odds ratios and 95% confidence intervals were used to assess the strength of the associations, and all the statistical analyses were calculated using the software program STATA version 12.0. Our results revealed that the Pro757Leu polymorphism was significantly associated with a reduced cancer risk, whereas an inverse association was found for the Glu589Lys polymorphism. Furthermore, subgroup analysis of smoking status indicated that the Glu589Lys polymorphism was significantly associated with an increased cancer risk in smokers, but not in nonsmokers. However, no evidence was found for an association between the Glu670Gly polymorphism and cancer risk. In conclusion, this meta-analysis suggests that the Pro757Leu polymorphism may provide protective effects against cancer, while the Glu589Lys polymorphism may be a risk factor for cancer. Moreover, the Glu670Gly polymorphism may have no influence on cancer susceptibility. In the future, large-scaled and well-designed studies are needed to achieve a more precise and comprehensive result. [ABSTRACT FROM AUTHOR]

Published

2016

21. FANCD2-associated nuclease 1 partially compensates for the lack of Exonuclease 1 in mismatch repair

Author

Gene Koh, Josef Jiricny, Serena Nik-Zainal, Hiroyuki Sasanuma, Alessandro A. Sartori, Saho Kobayashi-Era, Goncalo Oliveira, Katja Kratz, Andreia Oliveira, Julia Richter, Shunichi Takeda, Shunsuke Kobayashi, Masataka Tsuda, Mariela Artola-Borán, Joanna I. Loizou, Xueqing Zou, and University of Zurich

Subjects

Exonuclease, Methylnitronitrosoguanidine, congenital, hereditary, and neonatal diseases and abnormalities, exonuclease, DNA repair, 610 Medicine & health, EXO1, DNA Mismatch Repair, Cell Line, Avian Proteins, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, Germline mutation, FAN1, PMS2, Animals, Humans, Amino Acid Sequence, Molecular Biology, 030304 developmental biology, 0303 health sciences, Endodeoxyribonucleases, Thionucleosides, biology, Base Sequence, Guanosine, 10061 Institute of Molecular Cancer Research, MLH1, Cell Biology, mutational signature, MSH6, Multifunctional Enzymes, digestive system diseases, Cell biology, mismatch repair, Exodeoxyribonucleases, HEK293 Cells, MSH2, 030220 oncology & carcinogenesis, Mutation, biology.protein, 570 Life sciences, DNA mismatch repair, Chickens, Research Article

Abstract

Germline mutations in the mismatch repair (MMR) genes MSH2, MSH6, MLH1, and PMS2 are linked to cancer of the colon and other organs, characterized by microsatellite instability and a large increase in mutation frequency. Unexpectedly, mutations in EXO1, encoding the only exonuclease genetically implicated in MMR, are not linked to familial cancer and cause a substantially weaker mutator phenotype. This difference could be explained if eukaryotic cells possessed additional exonucleases redundant with EXO1. Analysis of the MLH1 interactome identified FANCD2-associated nuclease 1 (FAN1), a novel enzyme with biochemical properties resembling EXO1. We now show that FAN1 efficiently substitutes for EXO1 in MMR assays and that this functional complementation is modulated by its interaction with MLH1. FAN1 also contributes to MMR in vivo; cells lacking both EXO1 and FAN1 have an MMR defect and display resistance to N-methyl-N-nitrosourea (MNU) and 6-thioguanine (TG). Moreover, FAN1 loss amplifies the mutational profile of EXO1-deficient cells, suggesting that the two nucleases act redundantly in the same antimutagenic pathway. However, the increased drug resistance and mutator phenotype of FAN1/EXO1-deficient cells are less prominent than those seen in cells lacking MSH6 or MLH1. Eukaryotic cells thus apparently possess additional mechanisms that compensate for the loss of EXO1., Cellular and Molecular Biology, 41 (9), ISSN:0145-5680, ISSN:1165-158X

Published

2021

22. TREX1 As a Potential Therapeutic Target for Autoimmune and Inflammatory Diseases

Author

Tian-Ping Zhang, Rui-Xue Leng, Qin Zhang, Sha-Sha Tao, Guo-Cui Wu, Dong-Qing Ye, and Hai-Feng Pan

Subjects

Programmed cell death, Systemic inflammation, medicine.disease_cause, Autoimmune Diseases, Autoimmunity, law.invention, Pathogenesis, Mice, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, law, Drug Discovery, medicine, Animals, Humans, Gene, 030304 developmental biology, Inflammation, Pharmacology, Autoimmune disease, 0303 health sciences, business.industry, Phosphoproteins, medicine.disease, Exodeoxyribonucleases, Mutation, Immunology, Suppressor, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Background and Objectives: The 3’ repair exonuclease 1 (TREX1) gene is the major DNA-specific 3’–5 ’exonuclease of mammalian cells which reduces single- and double-stranded DNA (ssDNA and dsDNA) to prevent undue immune activation mediated by the nucleic acid. TREX1 is also a crucial suppressor of selfrecognition that protects the host from inappropriate autoimmune activations. It has been revealed that TREX1 function is necessary to prevent host DNA accumulating after cell death which could actuate an autoimmune response. In the manuscript, we will discuss in detail the latest advancement to study the role of TREX1 in autoimmune disease. Methods: As a pivotal cytoprotective, antioxidant, anti-apoptotic, immunosuppressive, as well as an antiinflammatory molecule, the functional mechanisms of TREX1 were multifactorial. In this review, we will briefly summarize the latest advancement in studying the role of TREX1 in autoimmune disease, and discuss its potential as a therapeutic target for these diseases. Results: Deficiency of TREX1 in human patients and murine models is characterized by systemic inflammation and the disorder of TREX1 functions drives inflammatory responses leading to autoimmune disease. Moreover, much more studies revealed that mutations in TREX1 have been associated with a range of autoimmune disorders. But it is also unclear whether the mutations of TREX1 play a causal role in the disease progression, and whether manipulation of TREX1 has a beneficial effect in the treatment of autoimmune diseases. Conclusion: Integration of functional TREX1 biology into autoimmune diseases may further deepen our understanding of the development and pathogenesis of autoimmune diseases and provide new clues and evidence for the treatment of autoimmune diseases.

Published

2019

23. RBX1 prompts degradation of EXO1 to limit the homologous recombination pathway of DNA double-strand break repair in G1 phase

Author

Ying Xie, Zong-Pei Guo, Ping-Kun Zhou, Hua Guan, Yiguo Jiang, Yike Liu, Xiao-Dan Liu, Da-Fei Xie, and Teng Ma

Subjects

DNA Repair, Cell Survival, DNA repair, RAD51, DNA-Activated Protein Kinase, Models, Biological, Article, chemistry.chemical_compound, Exonuclease 1, Cell Line, Tumor, Humans, DNA Breaks, Double-Stranded, Homologous Recombination, Molecular Biology, G1 Phase, Ubiquitination, DNA, Cell Biology, Cullin Proteins, Double Strand Break Repair, Protein quality control, Homologous Recombination Pathway, Cell biology, enzymes and coenzymes (carbohydrates), DNA Repair Enzymes, Exodeoxyribonucleases, chemistry, Gamma Rays, Proteolysis, Rad51 Recombinase, Neddylation, Carrier Proteins, Homologous recombination

Abstract

End resection of DNA double-strand breaks (DSBs) to form 3′ single-strand DNA (ssDNA) is critical to initiate the homologous recombination (HR) pathway of DSB repair. HR pathway is strictly limited in the G1-phase cells because of lack of homologous DNA as the templates. Exonuclease 1 (EXO1) is the key molecule responsible for 3′ ssDNA formation of DSB end resection. We revealed that EXO1 is inactivated in G1-phase cells via ubiquitination-mediated degradation, resulting from an elevated expression level of RING-box protein 1 (RBX1) in G1 phase. The increased RBX1 significantly prompted the neddylation of Cullin1 and contributed to the G1 phase-specific degradation of EXO1. Knockdown of RBX1 remarkedly attenuated the degradation of EXO1 and increased the end resection and HR activity in γ-irradiated G1-phase cells, as demonstrated by the increased formation of RPA32, BrdU, and RAD51 foci. And EXO1 depletion mitigated DNA repair defects due to RBX1 reduction. Moreover, increased autophosphorylation of DNA-PKcs at S2056 was found to be responsible for the higher expression level of the RBX1 in the G1 phase. Inactivation of DNA-PKcs decreased RBX1 expression, and simultaneously increased EXO1 expression and DSB end resection in G1-phase cells. This study demonstrates a new mechanism for restraining the HR pathway of DNA DSB repair in G1 phase via RBX1-prompted inactivation of EXO1.

Published

2019

24. The human Exonuclease-1 interactome and phosphorylation sites

Author

Christiane König, Christian Gentili, Stefano Ferrari, Wassim Eid, and Daniel Hess

Subjects

0301 basic medicine, DNA damage, DNA repair, Biophysics, Biochemistry, Interactome, Minor Histocompatibility Antigens, 03 medical and health sciences, Exonuclease 1, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Protein Interaction Mapping, Humans, Gene Regulatory Networks, Phosphorylation, Molecular Biology, Gene, Chemistry, Nuclear Proteins, RNA-Binding Proteins, Reproducibility of Results, Cell Biology, Cell biology, DNA Repair Enzymes, Exodeoxyribonucleases, 030104 developmental biology, Apoptosis, 030220 oncology & carcinogenesis, Homologous recombination, DNA, DNA Damage, Protein Binding

Abstract

Error-free repair of DNA double-strand break is orchestrated by homologous recombination (HR) pathways and requires the concerted action of several factors. Among these, EXO1 and DNA2/BLM execute extensive resection of DNA ends to produce 3’-overhangs, which are key intermediates for downstream steps of HR. To help shedding light on regulatory aspects of DNA repair pathways in which EXO1 participates, we set out to identify proteins interacting with EXO1. Affinity purification of EXO1 followed by Orbitrap mass spectrometry led to the identification of novel partners that are involved in RNA processing or that are the causative agents of rare X-linked disorders. Depletion of a selected subset of EXO1 interacting proteins led to reduction of the DNA damage response. Among those, we examined the RRP5-homologue and NFκB-interacting protein PDCD11/ALG-4, which has roles in apoptosis and is a putative driver gene in cutaneous T-cell lymphoma. We provide evidence that depletion of PDCD11 decreased the formation of γH2AX foci and the phosphorylation of DNA damage response signaling intermediates in response to camptothecin or bleomycin, resulting in increased cellular resistance to DNA damage. Furthermore, extensive coverage of EXO1 sequence (>85%) by mass spectrometry allowed conducting an in-depth analysis of its phosphorylation sites, with the identification of 26 residues that are differentially modified in untreated conditions or upon induction of DNA damage.As a whole, these results provide the basis for future in-depth studies on novel roles of EXO1 in genome stability and indicate targets for pharmacological inhibition of pathways of cancer development.HIGHLIGHTSProteome-wide analysis of Exonuclease-1 (EXO1) interacting proteins revealed novel partners involved in RNA processing or that are the causative agents of rare X-linked disorders.We provide evidence for a role of PDCD11 in the DNA Damage Response.We conducted a comprehensive identification of EXO1 phosphorylation sites.

Published

2019

25. Exonuclease 1 expression is associated with clinical progression, metastasis, and survival prognosis of prostate cancer

Author

Yuzhuo Wang, Dong Lin, Fei Luo, Kuo Yang, and Jian Li

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, business.industry, Cell Biology, medicine.disease, Malignancy, Biochemistry, Metastasis, 03 medical and health sciences, Exonuclease 1, Prostate cancer, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Internal medicine, Cohort, medicine, business, Prospective cohort study, Molecular Biology, Lymph node, Clinical progression

Abstract

Prostate cancer (PCa) is the most prevalent malignancy and the second leading cause of cancer-related deaths in the male population in western countries, and we explored the association between exonuclease 1 (EXO1) expression and clinical progression, metastasis (Met), and survival prognosis of PCa. EXO1 expression of high/low-metastatic patient-derived xenografts model was investigated and clinical correlation and prognosis outcomes were validated. EXO1 in high-metastatic models was significantly increased compared with low-metastatic lines. In memorial sloan-kettering cancer center (MSKCC) cohort, EXO1 expression positively correlated with PCa Met, and patients with high EXO1 had poor biochemical recurrence-free survival in primary PCa cohort. Validation in The Cancer Genome Atlas primary cohort indicated EXO1 expression was significantly associated with lymph node Met and disease-free survival. The overexpression of EXO1 is significantly associated with PCa poor survival outcome, and is a promising biomarker for PCa, especially for primary PCa. A prospective study is clearly needed to validate these findings.

Published

2019

26. Replication stress-induced Exo1 phosphorylation is mediated by Rad53/Pph3 and Exo1 nuclear localization is controlled by 14-3-3 proteins

Author

Nagaraja Chappidi, Stefano Ferrari, and Giuseppe De Gregorio

Subjects

DNA repair, Short Report, Biology, DNA replication, Pph3, Biochemistry, lcsh:RC254-282, Dephosphorylation, 03 medical and health sciences, Exonuclease 1, chemistry.chemical_compound, 0302 clinical medicine, Budding yeast, Phosphorylation, lcsh:QH573-671, Molecular Biology, 14-3-3, 030304 developmental biology, 0303 health sciences, Sub-cellular localization, Kinase, lcsh:Cytology, Cell Biology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell biology, chemistry, 030220 oncology & carcinogenesis, Rad53, Exonuclease-1, DNA, Nuclear localization sequence

Abstract

Background Mechanisms controlling DNA resection at sites of damage and affecting genome stability have been the subject of deep investigation, though their complexity is not yet fully understood. Specifically, the regulatory role of post-translational modifications in the localization, stability and function of DNA repair proteins is an important aspect of such complexity. Results Here, we took advantage of the superior resolution of phosphorylated proteins provided by Phos-Tag technology to study pathways controlling the reversible phosphorylation of yeast Exo1, an exonuclease involved in a number of DNA repair pathways. We report that Rad53, a checkpoint kinase downstream of Mec1, is responsible for Exo1 phosphorylation in response to DNA replication stress and we demonstrate a role for the type-2A protein phosphatase Pph3 in the dephosphorylation of both Rad53 and Exo1 during checkpoint recovery. Fluorescence microscopy studies showed that Rad53-dependent phosphorylation is not required for the recruitment or the release of Exo1 from the nucleus, whereas 14-3-3 proteins are necessary for Exo1 nuclear translocation. Conclusions By shedding light on the mechanism of Exo1 control, these data underscore the importance of post-translational modifications and protein interactions in the regulation of DNA end resection. Electronic supplementary material The online version of this article (10.1186/s13008-018-0044-2) contains supplementary material, which is available to authorized users.

Published

2019

27. Phosphorylation meets DNA mismatch repair

Author

Angela Brieger and Isabel M. Weßbecher

Subjects

0301 basic medicine, chemistry.chemical_classification, DNA ligase, Mutation rate, biology, DNA polymerase, DNA damage, Cell Cycle, Cell Biology, DNA Mismatch Repair, Biochemistry, Cell biology, 03 medical and health sciences, Exonuclease 1, 030104 developmental biology, chemistry, Proteolysis, biology.protein, Animals, Humans, Phosphorylation, Nucleotide, DNA mismatch repair, Molecular Biology

Abstract

DNA mismatch repair (MMR) is a highly conserved process and ensures the removal of mispaired DNA bases and insertion-deletion loops right after replication. For this, a MutSα or MutSβ protein complex recognizes the DNA damage, MutLα nicks the erroneous strand, exonuclease 1 removes the wrong nucleotides, DNA polymerase δ refills the gap and DNA ligase I joins the fragments to seal the nicks and complete the repair process. The failure to accomplish these functions is associated with higher mutation rates and may lead to cancer, which highlights the importance of MMR by the maintenance of genomic stability. The post-replicative MMR implies that involved proteins are regulated at several levels, including posttranslational modifications (PTMs). Phosphorylation is one of the most common and major PTMs. Suitable with its regulatory force phosphorylation was shown to influence MMR factors thereby adjusting eukaryotic MMR activity. In this review, we summarized the current knowledge of the role of phosphorylation of MMR process involved proteins and their functional relevance.

Published

2018

28. A Comprehensive Analysis of Northern versus Liquid Hybridization Assays for mRNAs, Small RNAs, and miRNAs Using a Non-Radiolabeled Approach

Author

Bushra Gull, Jasmin Baby, Farah Mustafa, and Waqar Ahmad

Subjects

0301 basic medicine, Microbiology (medical), Exonuclease, Small RNA, QH301-705.5, mRNA, Biotin, Microbiology, 03 medical and health sciences, 0302 clinical medicine, microRNA, small RNA, Northern blot, biotinylation, RNA, Messenger, Locked nucleic acid, Biology (General), Molecular Biology, miRNA, Messenger RNA, biology, Typhoon & Sapphire biomolecular imaging, Chemistry, northern blotting, RNA, Nucleic Acid Hybridization, General Medicine, Blotting, Northern, exonuclease 1, MicroRNAs, 030104 developmental biology, Biochemistry, 030220 oncology & carcinogenesis, Biotinylation, non-radioactive, biology.protein, DNA Probes, Digoxigenin, liquid hybridization assay

Abstract

Northern blotting (NB), a gold standard for RNA detection, has lost its charm due to its hands-on nature, need for good quality RNA, and radioactivity. With the emergence of the field of microRNAs (miRNAs), the necessity for sensitive and quantitative NBs has again emerged. Here, we developed highly sensitive yet non-radiolabeled, fast, economical NB, and liquid hybridization (LH) assays without radioactivity or specialized reagents like locked nucleic acid (LNA)- or digoxigenin-labeled probes for mRNAs/small RNAs, especially miRNAs using biotinylated probes. An improvised means of hybridizing oligo probes along with efficient transfer, cross-linking, and signal enhancement techniques was employed. Important caveats of each assay were elaborated upon, especially issues related to probe biotinylation, use of exonuclease, and bioimagers not reported earlier. We demonstrate that, while the NBs were sensitive for mRNAs and small RNAs, our LH protocol could efficiently detect these and miRNAs using less than 10–100 times the total amount of RNA, a sensitivity comparable to radiolabeled probes. Compared to NBs, LH was a faster, more sensitive, and specific approach for mRNA/small RNA/miRNA detection. A comparison of present work with six seminal studies is presented along with detailed protocols for easy reproducibility. Overall, our study provides effective platforms to study large and small RNAs in a sensitive, efficient, and cost-effective manner.

Published

2021

29. New insights from Whole Genome Sequencing: BCLAF1 deletion as a structural variant that predisposes cells towards cellular transformation

Author

Hendrina Shipanga, Vimbaishe Chibanga, M. Iqbal Parker, and Lamech M Mwapagha

Subjects

Adult, Male, Cancer Research, Esophageal Neoplasms, Biology, Malignant transformation, Exonuclease 1, Cell Line, Tumor, Gene expression, Gene silencing, Humans, Gene, Transcription factor, Aged, Genetics, Whole genome sequencing, Aged, 80 and over, Gene knockdown, Whole Genome Sequencing, Tumor Suppressor Proteins, General Medicine, Middle Aged, Repressor Proteins, Cell Transformation, Neoplastic, Oncology, Mutation, Female, Esophageal Squamous Cell Carcinoma

Abstract

Cancer arises from a multi‑step cellular transformation process where some mutations may be inherited, while others are acquired during the process of malignant transformation. Aberrations in the BCL2 associated transcription factor 1 (BCLAF1) gene have previously been identified in patients with cancer and the aim of the present study was to identify structural variants (SVs) and the effects of BCLAF1 gene silencing on cell transformation. Whole‑genome sequencing was performed on DNA isolated from tumour biopsies with a histologically confirmed diagnosis of oesophageal squamous cell carcinoma (OSCC). Paired‑end sequencing was performed on the Illumina HiSeq2000, with 300 bp reads. Reads were aligned to the Homo sapiens reference genome (NCBI37) using ELAND and CASAVA software. SVs reported from the alignment were collated with gene loci, using the variant effect predictor of Ensembl. The affected genes were subsequently cross‑checked against the Genetic Association Database for disease and cancer associations. BCLAF1 deletion was identified as a noteworthy SV that could be associated with OSCC. Transient small interfering RNA‑mediated knockdown of BCLAF1 resulted in the altered expression of several downstream genes, including downregulation of the proapoptotic genes Caspase‑3 and BAX and the DNA damage repair genes exonuclease 1, ATR‑interacting protein and transcription regulator protein BACH1. BCLAF1 deficiency also attenuated P53 gene expression. Inhibition of BCLAF1 expression also resulted in increased colony formation. These results provide evidence that the abrogation of BCLAF1 expression results in the dysregulation of several cancer signalling pathways and abnormal cell proliferation.

Published

2021

30. Systemic lupus erythematosus overlapping dermatomyositis owing to a heterozygous TREX1 Asp130Asn missense mutation

Author

Tomohiro Koga, Yushiro Endo, Hiroki Otaki, Atsushi Kawakami, and Kaori Furukawa

Subjects

0301 basic medicine, Exonuclease, Adult, Male, Myxovirus Resistance Proteins, Heterozygote, Immunology, Mutant, Mutation, Missense, medicine.disease_cause, GPI-Linked Proteins, Dermatomyositis, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, medicine, Immunology and Allergy, Missense mutation, Humans, Lupus Erythematosus, Systemic, skin and connective tissue diseases, Gene, Mutation, biology, business.industry, TREX1 Gene, Tumor Suppressor Proteins, Interferon-alpha, DNA, medicine.disease, Phosphoproteins, Molecular Docking Simulation, 030104 developmental biology, Exodeoxyribonucleases, Antigens, Surface, Interferon Type I, biology.protein, business, Transcriptome, 030215 immunology

Abstract

The 3' repair exonuclease 1 (TREX1) gene encodes a nuclear protein with 3' exonuclease activity, and the mutations have been associated with autoimmune diseases. Herein, we performed genetic analysis for the TREX1 gene in 55 patients with systemic lupus erythematosus (SLE). We identified one SLE patient with overlapping dermatomyositis having a heterozygous p.Asp130Asn mutation in the TREX1 gene. The patient had a high level of serum interferon (IFN)-α compared with that in healthy controls and other patients with SLE. In addition, the patient expressed elevated IFN signature genes compared with healthy controls. Our molecular dynamics simulation of the TREX1 protein in a complex with double-stranded DNA revealed that the D130N mutant causes significant changes in the active site's interaction network. One of our cases exhibited a heterozygous TREX1 p.Asp130Asn mutation that contributed to the type I IFN pathway, which may lead to the development of a severe SLE phenotype.

Published

2021

31. Functional analysis of the nasopharyngeal carcinoma primary tumor-associated gene interaction network.

Author

FENGWEI AN, ZHIQIANG ZHANG, and MING XIA

Subjects

*NASOPHARYNX cancer, *FUNCTIONAL analysis, *BIOINFORMATICS, *GENE expression, *PROTEIN-protein interactions, *CENTROMERE

Abstract

The aim of the present study was to investigate the molecular mechanism of nasopharyngeal carcinoma (NPC) primary tumor development through the identification of key genes using bioinformatics approaches. Using the GSE53819 microarray dataset, acquired from the Gene Expression Omnibus database, differentially expressed genes (DEGs) were screened out between NPC primary tumor and control samples, followed by hierarchical clustering analysis. The Search Tool for the Retrieval of Interacting Genes database was utilized to build a protein-protein interaction network to identify key node proteins. In total, 1,067 DEGs, including 326 upregulated genes and 741 downregulated genes, were identified between the NPC and control samples. The results of the hierarchical clustering analysis demonstrated that 95% of the DEGs were sample-specific. Furthermore, PDZ binding kinase (PBK), centromere protein F (CENPF), actin-binding protein anillin (ANLN), exonuclease 1 (EXO1) and chromosome 15 open reading frame 42 (C15ORF42) were included in the obtained network module, which was closely associated with the cell cycle and nucleic acid metabolic process GO functions. The results of the present study revealed that EXO1, CENPF, ANLN, PBK and C15ORF42 may be involved in the mechanism of NPC via modulating the cell cycle and nucleic acid metabolic processes, and may serve as molecular biomarkers for the diagnosis of this disease. [ABSTRACT FROM AUTHOR]

Published

2015

32. BKM120 sensitizes BRCA-proficient triple negative breast cancer cells to olaparib through regulating FOXM1 and Exo1 expression

Author

Xinchen Wang, Wanpeng Zhang, Lu Chen, Shuping Wang, Yuantao Wang, and Yu Li

Subjects

DNA damage, Morpholines, Science, Poly ADP ribose polymerase, RAD51, Aminopyridines, Antineoplastic Agents, Triple Negative Breast Neoplasms, Piperazines, Article, Olaparib, Exonuclease 1, chemistry.chemical_compound, Breast cancer, PARP1, Cell Line, Tumor, Humans, PI3K/AKT/mTOR pathway, Triple-negative breast cancer, Phosphoinositide-3 Kinase Inhibitors, Cancer, BRCA2 Protein, Multidisciplinary, BRCA1 Protein, Chemistry, Forkhead Box Protein M1, Gene Expression Regulation, Neoplastic, DNA Repair Enzymes, Exodeoxyribonucleases, Cancer research, Phthalazines, Medicine, Female

Abstract

Poly (ADP-ribose) polymerase (PARP) inhibitors offer a significant clinical benefit for triple-negative breast cancers (TNBCs) with BRCA1/2 mutation. However, the narrow clinical indication limits the development of PARP inhibitors. Phosphoinositide 3-kinase (PI3K) inhibition sensitizes BRCA-proficient TNBC to PARP inhibition, which broadens the indication of PARP inhibitors. Previously researches have reported that PI3K inhibition induced the defect of homologous recombination (HR) mediated repair by downregulating the expression of BRCA1/2 and Rad51. However, the mechanism for their synergistic effects in the treatment of TNBC is still unclear. Herein, we focused on DNA damage, DNA single-strand breaks (SSBs) repair and DNA double-strand breaks (DSBs) repair three aspects to investigate the mechanism of dual PI3K and PARP inhibition in DNA damage response. We found that dual PI3K and PARP inhibition with BKM120 and olaparib significantly reduced the proliferation of BRCA-proficient TNBC cell lines MDA-MB-231 and MDA231-LM2. BKM120 increased cellular ROS to cause DNA oxidative damage. Olaparib resulted in concomitant gain of PARP1, forkhead box M1 (FOXM1) and Exonuclease 1 (Exo1) while inhibited the activity of PARP. BKM120 downregulated the expression of PARP1 and PARP2 to assist olaparib in blocking PARP mediated repair of DNA SSBs. Meanwhile, BKM120 inhibited the expression of BRAC1/2 and Rad51/52 to block HR mediated repair through the PI3K/Akt/NFκB/c-Myc signaling pathway and PI3K/Akt/ FOXM1/Exo1 signaling pathway. BKM120 induced HR deficiency expanded the application of olaparib to HR proficient TNBCs. Our findings proved that PI3K inhibition impaired the repair of both DNA SSBs and DNA DSBs. FOXM1 and Exo1 are novel therapeutic targets that serves important roles in DNA damage response.

Published

2021

33. Exonuclease 1 (EXO1) is a Potential Prognostic Biomarker and Correlates with Immune Infiltrates in Lung Adenocarcinoma

Author

Liangdong Li, Yiqun Cao, Mingtao Feng, Changshuai Zhou, Xin Chen, Yang Gao, Lei Chen, and Deheng Li

Subjects

0301 basic medicine, EXO1, OncoTargets and Therapy, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, Immune system, medicine, Pharmacology (medical), Lung cancer, Survival analysis, Original Research, Tumor microenvironment, immune infiltration, business.industry, Cell cycle, lung adenocarcinoma, medicine.disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biomarker, Biomarker (medicine), Adenocarcinoma, prognosis, business

Abstract

Chang-shuai Zhou,1,2,* Ming-tao Feng,1,2,* Xin Chen,1,2 Yang Gao,1,2 Lei Chen,1,2 Liang-dong Li,1,2 De-heng Li,1,2 Yi-qun Cao1,2 1Department of Neurosurgery, Fudan University Shanghai Cancer Center, Shanghai, People’s Republic of China; 2Department of Oncology, Shanghai Medical College, Fudan University, Shanghai, People’s Republic of China*These authors contributed equally to this workCorrespondence: Yi-qun Cao Email yiqun_fduscc@163.comBackground: Exonuclease 1 (EXO1) has been identified to be highly expressed in different human malignancies, but its expression and prognostic role in lung adenocarcinoma (LUAD) remain unknown.Materials and Methods: Two independent cohorts extracted from public databases and one cohort from our center were analyzed in this study. Expression levels of EXO1 in LUAD tissues and paired para-cancer tissues were detected. The prognostic value of EXO1 in LUAD patients was evaluated in the three cohorts. Enrichment analyses were performed to explore the possible underlying biological pathways. Moreover, we also explored the correlations between EXO1 and tumor-infiltrating immune cells and evaluated the impact of EXO1 knock-down on the migration of lung cancer cells.Results: In this study, we found that EXO1 was highly expressed in LUAD tissues compared with para-cancerous tissues in public databases (p < 0.01), which was consistent with our data (p < 0.01). Survival analysis indicated that high expression of EXO1 was associated with poor prognosis in LUAD (p < 0.01). Enrichment analyses indicated that biological pathways like cell cycle regulation, DNA damage and repair, immune response, neuroactive ligand-receptor interaction, may be associated with EXO1 aberrant expression. Moreover, high expression of EXO1 was correlated with decreased infiltrating B cells (p < 0.01) and CD4+ T cells (p < 0.01) levels, and low infiltrating levels of B cells (p < 0.01) and dendritic cells (DCs) (p < 0.05) indicated poor overall survival (OS) in LUAD. Additionally, in vitro experiments suggested that knockdown of EXO1 may inhibit the migratory ability of lung cancer cells.Conclusion: In conclusion, EXO1 is a potential prognostic biomarker in LUAD, and correlates with infiltrating levels of immune cells in the tumor microenvironment. Further prospective validation of EXO1 in lung cancer is warranted.Keywords: EXO1, lung adenocarcinoma, prognosis, biomarker, immune infiltration

Published

2021

34. Identification of MLH2/hPMS1 dominant mutations that prevent DNA mismatch repair function

Author

Hans Hombauer, Matthias Kloor, Kerstin Gries, Gloria X Reyes, Boyu Zhao, and Tobias T. Schmidt

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Saccharomyces cerevisiae Proteins, QH301-705.5, DNA mismatch repair, Mutant, Medicine (miscellaneous), Saccharomyces cerevisiae, Biology, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Frameshift mutation, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, Two-Hybrid System Techniques, medicine, Humans, Missense mutation, Biology (General), Cancer genetics, Gene, 030304 developmental biology, Genetics, 0303 health sciences, Mutation, Microsatellite instability, medicine.disease, digestive system diseases, Neoplasm Proteins, MutL Proteins, General Agricultural and Biological Sciences, Gene Deletion, 030217 neurology & neurosurgery, DNA Damage

Abstract

Inactivating mutations affecting key mismatch repair (MMR) components lead to microsatellite instability (MSI) and cancer. However, a number of patients with MSI-tumors do not present alterations in classical MMR genes. Here we discovered that specific missense mutations in the MutL homolog MLH2, which is dispensable for MMR, confer a dominant mutator phenotype in S. cerevisiae. MLH2 mutations elevated frameshift mutation rates, and caused accumulation of long-lasting nuclear MMR foci. Both aspects of this phenotype were suppressed by mutations predicted to prevent the binding of Mlh2 to DNA. Genetic analysis revealed that mlh2 dominant mutations interfere with both Exonuclease 1 (Exo1)-dependent and Exo1-independent MMR. Lastly, we demonstrate that a homolog mutation in human hPMS1 results in a dominant mutator phenotype. Our data support a model in which yeast Mlh1-Mlh2 or hMLH1-hPMS1 mutant complexes act as roadblocks on DNA preventing MMR, unraveling a novel mechanism that can account for MSI in human cancer., Reyes et al. identified and characterized dominant mutations in the MutL homolog MLH2 (in S. cerevisiae) and PMS1 (in humans) causing an increased mutator phenotype. Based on their findings, they propose that Mlh2/hPMS1-Mlh1 mutant complexes can act as roadblocks on DNA preventing mismatch repair function.

Published

2020

35. Exo1 independent DNA mismatch repair involves multiple compensatory nucleases.

Author

Desai, Amar and Gerson, Stanton

Subjects

*DNA repair, *NUCLEASES, *DNA replication, *HEREDITARY nonpolyposis colorectal cancer, *HEMATOPOIETIC stem cells, *IN vitro studies

Abstract

Functional DNA mismatch repair (MMR) is essential for maintaining the fidelity of DNA replication and genetic stability. In hematopoiesis, loss of MMR results in methylating agent resistance and a hematopoietic stem cell (HSC) repopulation defect. Additionally MMR failure is associated with a variety of human malignancies, notably Lynch syndrome. We focus on the 5' → 3' exonuclease Exo1, the primary enzyme excising the nicked strand during MMR, preceding polymerase synthesis. We found that nuclease dead Exo1 mutant cells are sensitive to the O6-methylguanine alkylating agent temozolomide when given with the MGMT inactivator, O6benzylguanine (BG). Additionally we used an MMR reporter plasmid to verify that Exo1mut MEFs were able to repair G:T base mismatches in vitro. We showed that unlike other MMR deficient mouse models, Exo1mut mouse HSC did not gain a competitive survival advantage post temozolomide/BG treatment in vivo. To determine potential nucleases implicated in MMR in the absence of Exo1 nuclease activity, but in the presence of the inactive protein, we performed gene expression analyses of several mammalian nucleases in WT and Exo1mut MEFs before and after temozolomide treatment and identified upregulation of Artemis, Fan1, and Mre11. Partial shRNA mediated silencing of each of these in Exo1mut cells resulted in decreased MMR capacity and increased resistance to temozolomide/BG. We propose that nuclease function is required for fully functional MMR, but a portfolio of nucleases is able to compensate for loss of Exo1 nuclease activity to maintain proficiency. [ABSTRACT FROM AUTHOR]

Published

2014

36. EXO1: A tightly regulated nuclease

Author

Federico Lazzaro, Roberto Quadri, Marco Muzi-Falconi, and Sarah Sertic

Subjects

Genome instability, Exonuclease, DNA Repair, DNA damage, Biology, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Exonuclease 1, 0302 clinical medicine, Animals, Humans, Molecular Biology, 030304 developmental biology, 0303 health sciences, Cell Biology, DNA, Double Strand Break Repair, Cell biology, DNA Repair Enzymes, Exodeoxyribonucleases, chemistry, 030220 oncology & carcinogenesis, biology.protein, DNA mismatch repair, Protein Processing, Post-Translational, Nucleotide excision repair, DNA Damage

Abstract

Exonuclease 1 (EXO1) is an evolutionarily well conserved exonuclease. Its ability to resect DNA in the 5'-3' direction has been extensively characterized and shown to be implicated in several genomic DNA metabolic processes such as replication stress response, double strand break repair, mismatch repair, nucleotide excision repair and telomere maintenance. While the processing of DNA is critical for its repair, an excessive nucleolytic activity can lead to secondary lesions, increased genome instability and alterations in cellular functions. It is thus clear that different regulatory layers must be in effect to keep DNA degradation under control. Regulatory events that modulate EXO1 activity have been reported to act at different levels. Here we summarize the different post-translational modifications (PTMs) that affect EXO1 and discuss the implications of PTMs for EXO1 activities and how this regulation may be associated to cancer development.

Published

2020

37. EXO1 resection at G-quadruplex structures facilitates resolution and replication

Author

Kevin Kurtz, Sergey Karachenets, Kevin Lin, Eric A. Hendrickson, Susanna Stroik, Chad L. Myers, and Anja Katrin Bielinsky

Subjects

Genome instability, DNA Replication, DNA End-Joining Repair, DNA Repair, DNA repair, AcademicSubjects/SCI00010, Biology, G-quadruplex, Cell Line, 03 medical and health sciences, Exonuclease 1, chemistry.chemical_compound, Gene Knockout Techniques, 0302 clinical medicine, Neoplasms, Genetics, Humans, heterocyclic compounds, Picolinic Acids, Molecular Biology, 030304 developmental biology, 0303 health sciences, DNA replication, Telomere, Prognosis, Cell biology, G-Quadruplexes, DNA Repair Enzymes, Exodeoxyribonucleases, chemistry, 030220 oncology & carcinogenesis, Aminoquinolines, DNA, HeLa Cells

Abstract

G-quadruplexes represent unique roadblocks to DNA replication, which tends to stall at these secondary structures. Although G-quadruplexes can be found throughout the genome, telomeres, due to their G-richness, are particularly predisposed to forming these structures and thus represent difficult-to-replicate regions. Here, we demonstrate that exonuclease 1 (EXO1) plays a key role in the resolution of, and replication through, telomeric G-quadruplexes. When replication forks encounter G-quadruplexes, EXO1 resects the nascent DNA proximal to these structures to facilitate fork progression and faithful replication. In the absence of EXO1, forks accumulate at stabilized G-quadruplexes and ultimately collapse. These collapsed forks are preferentially repaired via error-prone end joining as depletion of EXO1 diverts repair away from error-free homology-dependent repair. Such aberrant repair leads to increased genomic instability, which is exacerbated at chromosome termini in the form of dysfunction and telomere loss.

Published

2020

38. Exonuclease 1 (Exo1) Participates in Mammalian Non-Homologous End Joining and Contributes to Drug Resistance in Ovarian Cancer

Author

Ben Yang, Dongyun He, Minjia Sheng, and Tao Li

Subjects

Exonucleases, DNA End-Joining Repair, Cell Survival, Antineoplastic Agents, 030204 cardiovascular system & hematology, Gene Knockout Techniques, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, Lab/In Vitro Research, Cell Line, Tumor, Radiation, Ionizing, medicine, Humans, Viability assay, Ku Autoantigen, Ovarian Neoplasms, Cisplatin, Ku70, Chemistry, General Medicine, Molecular biology, Non-homologous end joining, DNA Repair Enzymes, Exodeoxyribonucleases, Doxorubicin, Drug Resistance, Neoplasm, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Female, DNA mismatch repair, Homologous recombination, DNA Damage, Nucleotide excision repair, medicine.drug

Abstract

BACKGROUND Exonuclease 1 (Exo1) participates in a variety of DNA damage repair, including mismatch repair, nucleotide excision repair, and homologous recombination. Genetic study in yeast indicates a role of Exo1 in non-homologous end joining (NHEJ), acting as a regulator for accuracy repairing DNA. This study aimed to investigate the effects of human Exo1 in NHEJ and drug resistance in ovarian cells. MATERIAL AND METHODS Ectopic expression of Exo1 was carried out using pcDNA3.1-EXO1 plasmid in SKOV3 cells. GST-tagged human Exo1 was purified using pTXB1-gst-EXO1 and the his-tagged-Ku was collected using pET15b.his.Ku. Exo1 and Ku70 proteins expressed in bacteria were harvested and purified. DNA-protein binding was examined using affinity capture assay. The cells were treated using drugs for 72 hours. Then, the viabilities of cells were evaluated with sulforhodamine B cell viability analysis. The protein expression was evaluated using western blot assay. RESULTS As expected, human cells that deficient of Exo1 were sensitive to ionizing radiation and DNA damaging drugs (cisplatin and doxorubicin). Cisplatin resistant ovarian cancer cell line and Exo1 deficient cell lines were successfully generated. Exo1 interacts with NHEJ required factor Ku70 and affects NHEJ efficiency. We observed that Exo1 expression level was upregulated in drug resistant cell line and knockdown of Exo1 in drug resistant cells sensitized cells to cisplatin and doxorubicin. CONCLUSIONS Exo1 participated in mammalian non-homologous end joining and contributed to drug resistance in ovarian cancer.

Published

2020

39. The properties of Msh2–Msh6 ATP binding mutants suggest a signal amplification mechanism in DNA mismatch repair

Author

Christopher D. Putnam, Richard D. Kolodner, and William J. Graham

Subjects

0301 basic medicine, DNA mismatch repair, MutS, DNA endonuclease, S. cerevisiae, Crystallography, X-Ray, Medical and Health Sciences, Biochemistry, chemistry.chemical_compound, Endonuclease, 0302 clinical medicine, Adenosine Triphosphate, Crystallography, DNA clamp, biology, Biological Sciences, exonuclease 1, Cell biology, DNA-Binding Proteins, MutS Homolog 2 Protein, Mlh1-Pms1, MutL Protein Homolog 1, mutagenesis, Protein Binding, Biochemistry & Molecular Biology, congenital, hereditary, and neonatal diseases and abnormalities, Saccharomyces cerevisiae Proteins, DNA repair, 1.1 Normal biological development and functioning, Saccharomyces cerevisiae, DNA and Chromosomes, DNA replication, 03 medical and health sciences, Underpinning research, cerevisiae, Molecular Biology, neoplasms, Msh2-Msh6, Mutagenesis, nutritional and metabolic diseases, Cell Biology, digestive system diseases, DNA binding protein, 030104 developmental biology, chemistry, MSH2, Chemical Sciences, X-Ray, biology.protein, Generic health relevance, 030217 neurology & neurosurgery, DNA

Abstract

DNA mismatch repair (MMR) corrects mispaired DNA bases and small insertion/deletion loops generated by DNA replication errors. After binding a mispair, the eukaryotic mispair recognition complex Msh2–Msh6 binds ATP in both of its nucleotide-binding sites, which induces a conformational change resulting in the formation of an Msh2–Msh6 sliding clamp that releases from the mispair and slides freely along the DNA. However, the roles that Msh2–Msh6 sliding clamps play in MMR remain poorly understood. Here, using Saccharomyces cerevisiae, we created Msh2 and Msh6 Walker A nucleotide–binding site mutants that have defects in ATP binding in one or both nucleotide-binding sites of the Msh2–Msh6 heterodimer. We found that these mutations cause a complete MMR defect in vivo. The mutant Msh2–Msh6 complexes exhibited normal mispair recognition and were proficient at recruiting the MMR endonuclease Mlh1–Pms1 to mispaired DNA. At physiological (2.5 mm) ATP concentration, the mutant complexes displayed modest partial defects in supporting MMR in reconstituted Mlh1–Pms1-independent and Mlh1–Pms1-dependent MMR reactions in vitro and in activation of the Mlh1–Pms1 endonuclease and showed a more severe defect at low (0.1 mm) ATP concentration. In contrast, five of the mutants were completely defective and one was mostly defective for sliding clamp formation at high and low ATP concentrations. These findings suggest that mispair-dependent sliding clamp formation triggers binding of additional Msh2–Msh6 complexes and that further recruitment of additional downstream MMR proteins is required for signal amplification of mispair binding during MMR.

Published

2018

40. Calcium Influx Guards Replication Forks against Exonuclease 1

Author

Lee Zou and Antoine Simoneau

Subjects

0303 health sciences, Nuclease, Cell Biology, Biology, Replication (computing), Cell biology, Genomic Stability, enzymes and coenzymes (carbohydrates), 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, biology.protein, Phosphorylation, Molecular Biology, Calcium influx, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

In this issue, Li et al. (2019) report a previously unknown Ca2+-CaMKK2-AMPK signaling cascade that protects stalled forks from degradation by phosphorylating and inhibiting the EXO1 nuclease, revealing a surprising role for Ca2+ influx in the maintenance of genomic stability.

Published

2019

41. Human exonuclease 1 (EXO1) regulatory functions in DNA replication with putative roles in cancer

Author

Keijzers, Guido, Bakula, Daniela, Petr, Michael Angelo, Madsen, Nils Gedsig Kirkelund, Teklu, Amanuel, Mkrtchyan, Garik, Osborne, Brenna, Scheibye-Knudsen, Morten, Keijzers, Guido, Bakula, Daniela, Petr, Michael Angelo, Madsen, Nils Gedsig Kirkelund, Teklu, Amanuel, Mkrtchyan, Garik, Osborne, Brenna, and Scheibye-Knudsen, Morten

Abstract

Human exonuclease 1 (EXO1), a 5′→3′ exonuclease, contributes to the regulation of the cell cycle checkpoints, replication fork maintenance, and post replicative DNA repair pathways. These processes are required for the resolution of stalled or blocked DNA replication that can lead to replication stress and potential collapse of the replication fork. Failure to restart the DNA replication process can result in double-strand breaks, cell-cycle arrest, cell death, or cellular transformation. In this review, we summarize the involvement of EXO1 in the replication, DNA repair pathways, cell cycle checkpoints, and the link between EXO1 and cancer.

Published

2019

42. The significance of Exonuclease 1 K589E polymorphism on hepatocellular carcinoma susceptibility in the Turkish population: a case-control study.

Author

Bayram, Süleyman, Akkız, Hikmet, Bekar, Aynur, Akgöllü, Ersin, and Yıldırım, Selçuk

Abstract

Exonuclease 1 (Exo 1) is an important nuclease involved in mismatch repair system that contributes to maintain genomic stability, to modulate DNA recombination, and to mediate cell cycle arrest. A guanine (G)/adenine (A) common single nucleotide polymorphism at first position of codon 589 in Exo 1 gene determines a glutamic acid (Glu, E) to lysine (Lys, K) (K589E) aminoacidic substitution which may alter cancer risk by influencing the activity of Exo 1 protein. Exo 1 K589E polymorphism has been studied in various cancers, but its association with hepatocellular carcinoma (HCC) has yet to be investigated. To determine the association of the Exo 1 K589E polymorphism with the risk of HCC development in a Turkish population, a hospital-based case-control study was designed consisting of 224 subjects with HCC and 224 cancer-free control subjects matched for age, gender, smoking and alcohol status. The genotype frequency of the Exo 1 K589E polymorphism was determined by using a polymerase chain reaction-restriction fragment length polymorphism assay. Our data shows that the Lys/Lys genotype of the Exo 1 K589E polymorphism is associated with increased risk of HCC development in this Turkish population [odds ratio (OR) = 2.15, 95% confidence interval (CI): 1.13-4.09, P = 0.02]. Furthermore, according to stratified analysis, a significant association was observed between the homozygote Lys/Lys genotype and HCC risk in the subgroups of male gender (OR = 2.67, 95% CI: 1.27-5.61, P = 0.009) and patients with non-viral-related HCC (OR = 3.14, 95% CI: 1.09-8.99, P = 0.03). Because our results suggest for the first time that the Lys/Lys homozygote genotype of Exo 1 K589E polymorphism may be a genetic susceptibility factor for HCC in the Turkish population, further independent studies are required to validate our findings in a larger series, as well as in patients of different ethnic origins. [ABSTRACT FROM AUTHOR]

Published

2012

43. Chromosome integrity at a double-strand break requires exonuclease 1 and MRX

Author

Nakai, Wataru, Westmoreland, Jim, Yeh, Elaine, Bloom, Kerry, and Resnick, Michael A.

Subjects

*DNA repair, *CHROMOSOMES, *EXONUCLEASES, *ATP-binding cassette transporters, *GENETIC mutation, *YEAST, *MOLECULAR biology, *FLUORESCENCE microscopy

Abstract

Abstract: The continuity of duplex DNA is generally considered a prerequisite for chromosome continuity. However, as previously shown in yeast as well as human cells, the introduction of a double-strand break (DSB) does not generate a chromosome break (CRB) in yeast or human cells. The transition from DSB to CRB was found to be under limited control by the tethering function of the RAD50/MRE11/XRS2 (MRX) complex. Using a system for differential fluorescent marking of both sides of an endonuclease-induced DSB in single cells, we found that nearly all DSBs are converted to CRBs in cells lacking both exonuclease 1 (EXO1) activity and MRX complex. Thus, it appears that some feature of exonuclease processing or resection at a DSB is critical for maintaining broken chromosome ends in close proximity. In addition, we discovered a thermal sensitive (cold) component to CRB formation in an MRX mutant that has implications for chromosome end mobility and/or end-processing. [ABSTRACT FROM AUTHOR]

Published

2011

44. DNA helicases Sgs1 and BLM promote DNA double-strand break resection.

Author

Gravel, Serge, Chapman, J. Ross, Magill, Christine, and Jackson, Stephen P.

Subjects

*DNA damage, *DNA helicases, *SACCHAROMYCES cerevisiae, *GENETIC mutation, *DNA repair, *BIOCHEMICAL genetics

Abstract

A key cellular response to DNA double-strand breaks (DSBs) is 5'-to-3' DSB resection by nucleases to generate regions of ssDNA that then trigger cell cycle checkpoint signaling and DSB repair by homologous recombination (HR). Here, we reveal that in the absence of exonuclease Exo1 activity, deletion or mutation of the Saccharomyces cerevisiae RecQ-family helicase, Sgs1, causes pronounced hypersensitivity to DSB-inducing agents. Moreover, we establish that this reflects severely compromised DSB resection, deficient DNA damage signaling, and strongly impaired HR-mediated repair. Furthermore, we show that the mammalian Sgs1 ortholog, BLM-whose deficiency causes cancer predisposition and infertility in people-also functions in parallel with Exo1 to promote DSB resection, DSB signaling and resistance to DSB-generating agents. Collectively, these data establish evolutionarily conserved roles for the BLM and Sgs1 helicases in DSB processing, signaling, and repair. [ABSTRACT FROM AUTHOR]

Published

2008

45. Inhibition of the 5′ to 3′ Exonuclease Activity of hEXO1 by 8-Oxoguanine.

Author

McDowell, Heather D., Carney, James P., and Wilson, Teresa M.

Subjects

EXONUCLEASES, GENOMICS, MOLECULAR genetics, ALKYLATION, REACTIVE oxygen species, DNA damage, BIOCHEMICAL genetics, NUCLEOTIDES, NUCLEIC acids

Abstract

The article offers information on the inhibition of the 5' to 3' exonuclease activity of hEXO1 by 8-Oxoguanine. It is discussed that the mismatch repair pathway is responsible for maintaining genomic stability by correcting mismatches and insertion and deletion loops that arise mainly via replication errors. Furthermore, the mismatch repair pathway performs a central role in the cellular response to both alkylation and reactive oxygen species induced DNA damage. It is tested whether hEXO1 can degrade double-stranded DNA substrates containing alkylated or oxidized nucleotides.

Published

2008

46. Significant association of the EXO1 rs851797 polymorphism with clinical outcome of ovarian cancer

Author

Yuan Xu, Xi Cheng, Rong Jiang, Sheng Yin, Tingyan Shi, Rongyu Zang, and Pan Wang

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, EXO1, OncoTargets and Therapy, polymorphism, 03 medical and health sciences, Exonuclease 1, 0302 clinical medicine, Internal medicine, Genetic variation, Genotype, medicine, TaqMan, Pharmacology (medical), Epithelial ovarian cancer, Original Research, business.industry, medicine.disease, 030104 developmental biology, ovarian cancer, Tumor progression, 030220 oncology & carcinogenesis, prognosis, Ovarian cancer, business, Cohort study

Abstract

Tingyan Shi,1,2 Rong Jiang,1 Pan Wang,1 Yuan Xu,2 Sheng Yin,1 Xi Cheng,3 Rongyu Zang1,3 1Division of Gynecologic Oncology, Department of Obstetrics and Gynecology, Zhongshan Hospital, Fudan University, 2Cancer Institute, 3Gynecologic Oncology, Fudan University Shanghai Cancer Center, Shanghai, China Background: Exonuclease 1 (EXO1), one of DNA mismatch repair pathway genes, functions in maintaining genomic stability and affects tumor progression. We hypothesized that genetic variations in EXO1 may predict clinical outcomes in epithelial ovarian cancer (EOC). Methods: In this cohort study with 1,030 consecutive EOC patients, we genotyped four potentially functional polymorphisms in EXO1 by the Taqman assay and evaluated their associations with patients’ survival. Results: Using multivariate Cox proportional hazards regression models, we found that rs851797AG/GG genotypes were significantly associated with recurrence and cancer death (HR =1.30 and 1.38, 95% CI =1.11–1.52 and 1.02–1.88, respectively). Kaplan–Meier survival estimates showed that patients who carried rs851797AG/GG genotypes had poorer progression-free survival and poorer overall survival, compared with rs851797AA genotype carriers (log-rank test, P=0.002 and 0.025, respectively). Moreover, patients with older age at menophania, advanced stage tumor, or being received incomplete cytoreduction were more likely to be recurrent and dead. Conclusion: EXO1 rs851797 polymorphism can predict the clinical outcomes in EOC patients. In addition, age at menophania, FIGO stage, and complete cytoreduction might be independently prognostic factors of ovarian cancer. Large studies with functional experiments are warranted to validate these findings. Keywords: EXO1, ovarian cancer, polymorphism, prognosis

Published

2017

47. Aicardi–Goutières syndrome protein TREX1 suppresses L1 and maintains genome integrity through exonuclease-independent ORF1p depletion

Author

Jingwei Hou, Peng Li, Jian Kang, Xiao-Fang Yu, Juan Du, Ke Zhao, Haig H. Kazazian, and John L. Goodier

Subjects

0301 basic medicine, Exonuclease, Genome instability, Retroelements, DNA damage, Autoimmunity, DNA Exonuclease, Nervous System Malformations, Transfection, medicine.disease_cause, Genomic Instability, 03 medical and health sciences, Exonuclease 1, Autoimmune Diseases of the Nervous System, 0302 clinical medicine, Genetics, medicine, Humans, DNA Breaks, Double-Stranded, Phosphorylation, RNA, Small Interfering, Molecular Biology, Mutation, biology, Genome, Human, Proteins, DNA, Phosphoproteins, medicine.disease, Molecular biology, Recombinant Proteins, 3. Good health, Exodeoxyribonucleases, HEK293 Cells, 030104 developmental biology, Gene Expression Regulation, Protein destabilization, 030220 oncology & carcinogenesis, biology.protein, Aicardi–Goutières syndrome, HeLa Cells, Plasmids

Abstract

Maintaining genome integrity is important for cells and damaged DNA triggers autoimmunity. Previous studies have reported that Three-prime repair exonuclease 1(TREX1), an endogenous DNA exonuclease, prevents immune activation by depleting damaged DNA, thus preventing the development of certain autoimmune diseases. Consistently, mutations in TREX1 are linked with autoimmune diseases such as systemic lupus erythematosus, Aicardi–Goutières syndrome (AGS) and familial chilblain lupus. However, TREX1 mutants competent for DNA exonuclease activity are also linked to AGS. Here, we report a nuclease-independent involvement of TREX1 in preventing the L1 retrotransposon-induced DNA damage response. TREX1 interacted with ORF1p and altered its intracellular localization. Furthermore, TREX1 triggered ORF1p depletion and reduced the L1-mediated nicking of genomic DNA. TREX1 mutants related to AGS were deficient in inducing ORF1p depletion and could not prevent L1-mediated DNA damage. Therefore, our findings not only reveal a new mechanism for TREX1-mediated L1 suppression and uncover a new function for TREX1 in protein destabilization, but they also suggest a novel mechanism for TREX1-mediated suppression of innate immune activation through maintaining genome integrity.

Published

2017

48. A novel role of the Dna2 translocase function in DNA break resection

Author

Adam S. Miller, Xiaoyu Xue, Patrick Sung, Nhung Pham, Grzegorz Ira, James M. Daley, and Hengyao Niu

Subjects

0301 basic medicine, DNA End-Joining Repair, Saccharomyces cerevisiae Proteins, DNA Repair, 5' Flanking Region, DNA repair, Saccharomyces cerevisiae, Biology, 03 medical and health sciences, Exonuclease 1, Adenosine Triphosphate, 0302 clinical medicine, Genetics, Translocase, DNA Breaks, Double-Stranded, Flap endonuclease, Okazaki fragments, DNA Helicases, DNA replication, Helicase, Cell biology, 030104 developmental biology, Mutation, biology.protein, Homologous recombination, 030217 neurology & neurosurgery, Research Paper, Developmental Biology

Abstract

DNA double-strand break repair by homologous recombination entails nucleolytic resection of the 5′ strand at break ends. Dna2, a flap endonuclease with 5′–3′ helicase activity, is involved in the resection process. The Dna2 helicase activity has been implicated in Okazaki fragment processing during DNA replication but is thought to be dispensable for DNA end resection. Unexpectedly, we found a requirement for the helicase function of Dna2 in end resection in budding yeast cells lacking exonuclease 1. Biochemical analysis reveals that ATP hydrolysis-fueled translocation of Dna2 on ssDNA facilitates 5′ flap cleavage near a single-strand–double strand junction while attenuating 3′ flap incision. Accordingly, the ATP hydrolysis-defective dna2-K1080E mutant is less able to generate long products in a reconstituted resection system. Our study thus reveals a previously unrecognized role of the Dna2 translocase activity in DNA break end resection and in the imposition of the 5′ strand specificity of end resection.

Published

2017

49. Morphogenetic investigation of metaphase-specific cell death in meiotic spermatocytes in mice.

Author

Yasuhiro Kon

Subjects

*MORPHOGENESIS, *APOPTOSIS, *CELL death, *SPERMATOZOA, *COLLAGEN diseases

Abstract

An MRL/MpJ strain of mice, including lpr mutants, reveals the complex pathological manifestations of collagen disease, such as systemic vasculitis, glomerulonephritis, arthritis and sialoadenitis, in association with several autoimmune factors. Studies involving this mouse strain have shown that it exhibits a much-enhanced healing response compared with other mouse strains, together with reduced scarring in the periphery. Recently, unique characteristics were found in the testis of the MRL/MpJ mouse: metaphase-specific apoptosis (MSA) of meiotic spermatocytes, heat stress resistance in spermatocytes and the appearance of oocyte-like cells. The present review describes the morphological and genetic analysis of MSA, culminating in the conclusion that inherent mutation of exonuclease 1 induces checkpoint activity during meiotic division in MRL mice. [ABSTRACT FROM AUTHOR]

Published

2005

50. Complementary functions of the Saccharomyces cerevisiae Rad2 family nucleases in Okazaki fragment maturation, mutation avoidance, and chromosome stability

Author

Sun, Xuemin, Thrower, Douglas, Qiu, Junzhuan, Wu, Phillis, Zheng, Li, Zhou, Mian, Bachant, Jeff, Wilson III, David M., and Shen, Binghui

Subjects

*DNA, *SACCHAROMYCES cerevisiae, *GENES, *EXONUCLEASES, *ENDONUCLEASES

Abstract

Rad2 family nucleases, identified by sequence similarity within their catalytic domains, function in multiple pathways of DNA metabolism. Three members of the Saccharomyces cerevisiae Rad2 family, Rad2, Rad27, and exonuclease 1 (Exo1), exhibit both 5′ exonuclease and flap endonuclease activities. Deletion of RAD27 results in defective Okazaki fragment maturation, DNA repair, and subsequent defects in mutation avoidance and chromosomal stability. However, strains lacking Rad27 are viable. The expression profile of EXO1 during the cell cycle is similar to that of RAD27 and other genes encoding proteins that function in DNA replication and repair, suggesting Exo1 may function as a back up nuclease for Rad27 in DNA replication. We show that overexpression of EXO1 suppresses multiple rad27 null mutation-associated phenotypes derived from DNA replication defects, including temperature sensitivity, Okazaki fragment accumulation, the rate of minichromosome loss, and an elevated mutation frequency. While generally similar findings were observed with RAD2, overexpression of RAD2, but not EXO1, suppressed the MMS sensitivity of the rad27 null mutant cells. This suggests that Rad2 can uniquely complement Rad27 in base excision repair (BER). Furthermore, Rad2 and Exo1 complemented the mutator phenotypes and cell cycle defects of rad27 mutant strains to differing extents, suggesting distinct in vivo nucleic acid substrates. [Copyright &y& Elsevier]

Published

2003