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1. Novel hemizygous single‐nucleotide duplication in RPGR in a patient with retinal dystrophy and sensorineural hearing loss

Author

Ryan J. German, Blake Vuocolo, Liesbeth Vossaert, Nichole Owen, Richard A. Lewis, Lisa Saba, The Texome Project, Michael F. Wangler, and Sandesh Nagamani

Subjects
exome sequencing, retinal dystrophy, retinitis pigmentosa, RPGR, Genetics, QH426-470
Abstract

Abstract Background The RPGR gene has been associated with X‐linked cone‐rod dystrophy. This report describes a variant in RPGR detected with exome sequencing (ES). Genes like RPGR have not always been included in panel‐based testing and thus genome‐wide tests such as ES may be required for accurate diagnosis. Methods The Texome Project is studying the impact of ES in medically underserved patients who are in need of genomic testing to guide diagnosis and medical management. The hypothesis is that ES could uncover diagnoses not made by standard medical care. Results A 58‐year‐old male presented with retinitis pigmentosa, sensorineural hearing loss, and a family history of retinal diseases. A previous targeted gene panel for retinal disorders had not identified a molecular cause. ES through the Texome Project identified a novel, hemizygous variant in RPGR (NM_000328.3: c.1302dup, p.L435Sfs*18) that explained the ocular phenotype. Conclusions Continued genetics evaluation can help to end diagnostic odysseys of patients. Careful consideration of genes represented when utilizing gene panels is crucial to ensure an accurate diagnosis. Medically underserved populations are less likely to receive comprehensive genetic testing in their diagnostic workup. Our report is an example of the medical impact of genomic medicine implementation.

Published
2024
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5. P495: Improving access to exome sequencing in medically underserved populations through the Texome Project: A summary of the first 74 cases

Author

Blake Vuocolo, Ryan German, Carlos Bacino, Chaya Murali, Seema Lalani, Stephanie Baskin, Elizabeth Roeder, Carrie Schmid, Scott McLean, Rebecca Littlejohn, Olivia Juarez, Melissa Stuebben, Liesbeth Vossaert, Nichole Owen, Christine Eng, Pengfei Liu, Zhandong Liu, Dongxue Mao, Seon Young Kim, Sasidhar Pasupuleti, Shinya Yamamoto, Hugo Bellen, and Michael Wangler

Subjects
Genetics, QH426-470, Medicine
Published
2024
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12. Precision therapy for a medically actionable ATP1A3 variant from a genomic medicine program in an underserved population

Author

Cara P. Ford, Rebecca O. Littlejohn, Ryan German, Blake Vuocolo, Jose Aceves, Liesbeth Vossaert, Nichole Owen, Michael Wangler, Carrie A. Schmid, and The Texome Project

Subjects
alternating hemiplegia of childhood, ATP1A3, genomics, health care equity, underserved population, Genetics, QH426-470
Abstract

Abstract Background Genomic medicine is revolutionizing the diagnosis of rare diseases, but the implementation has not benefited underrepresented populations to the same degree. Here, we report the case of a 7‐year‐old boy with hypotonia, global developmental delay, strabismus, seizures, and previously suspected mitochondrial myopathy. This proband comes from an underrepresented minority and was denied exome sequencing by his public insurance. Methods After informed consent was obtained, buccal cells from the proband were collected and whole exome sequencing was performed. Illumina Dragen and Emedgene software was used to analyze the data at Baylor Genetics. The variants were further intepreted according to ACMG guidelines and the patient's phenotype. Results Through whole‐exome sequencing (WES) under the Community Texome project, he was found to have a heterozygous de novo pathogenic variant in the ATP1A3 gene located on chromosome 19q13. Conclusion In retrospect, his symptomatology matches the known medical conditions associated with the ATP1A3 gene namely Alternating Hemiplegia of Childhood 2 (AHC), a rare autosomal dominant disorder with an incidence of 1 in one million. His single nucleotide variant, (c.2401G>A, p.D801N), is predicted to be damaging. The specific amino acid change p.D801N has been previously reported in ClinVar along with the allelic variant p.D801Y and both are considered pathogenic. The identification of this variant altered medical management for this patient as he was started on a calcium antagonist and has reported no further hemiplegic episodes. This case illustrates the value of implementing genomic medicine for precision therapy in underserved populations.

Published
2023
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15. Altered cohesin gene dosage affects Mammalian meiotic chromosome structure and behavior.

Author

Brenda Murdoch, Nichole Owen, Michelle Stevense, Helen Smith, So Nagaoka, Terry Hassold, Michael McKay, Huiling Xu, Jun Fu, Ekaterina Revenkova, Rolf Jessberger, and Patricia Hunt

Subjects
Genetics, QH426-470
Abstract

Based on studies in mice and humans, cohesin loss from chromosomes during the period of protracted meiotic arrest appears to play a major role in chromosome segregation errors during female meiosis. In mice, mutations in meiosis-specific cohesin genes cause meiotic disturbances and infertility. However, the more clinically relevant situation, heterozygosity for mutations in these genes, has not been evaluated. We report here evidence from the mouse that partial loss of gene function for either Smc1b or Rec8 causes perturbations in the formation of the synaptonemal complex (SC) and affects both synapsis and recombination between homologs during meiotic prophase. Importantly, these defects increase the frequency of chromosomally abnormal eggs in the adult female. These findings have important implications for humans: they suggest that women who carry mutations or variants that affect cohesin function have an elevated risk of aneuploid pregnancies and may even be at increased risk of transmitting structural chromosome abnormalities.

Published
2013
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16. Expansion of the clinical phenotype of <scp>GALE</scp> deficiency

Author

Lisa Forbes Satter, Rebecca Markovitz, Donald H. Mahoney, Nichole Owen, Fernando Scaglia, Alison A. Bertuch, and Susan E Kirk

Subjects
chemistry.chemical_classification, Galactose epimerase deficiency, Glycosylation, business.industry, Galactosemia, Disease, Immune dysregulation, medicine.disease_cause, medicine.disease, Pancytopenia, carbohydrates (lipids), chemistry.chemical_compound, Immune system, chemistry, Immunology, Genetics, Medicine, business, Glycoprotein, Genetics (clinical)
Abstract

Congenital disorders of glycosylation are a group of rare monogenic inborn errors of metabolism caused by defective glycoprotein and glycolipid glycan synthesis and attachment. Here, we present a patient with galactose epimerase deficiency, also known as GALE deficiency, accompanied by pancytopenia and immune dysregulation. She was first identified by an abnormal newborn screen for galactosemia with subsequent genetic evaluation due to pancytopenia and immune dysregulation. The evaluation ultimately revealed that her known diagnosis of GALE deficiency was the cause of her hematologic and immune abnormalities. These findings further expand the clinical spectrum of disease of congenital disorders of glycosylation.

Published
2021

17. Detection of acquired uniparental disomy in clinical exome sequencing of pediatric patients with leukemia predisposition syndromes and its clinical significance

Author

Weimin Bi, Rachel Rau, Hongzheng Dai, Nichole Owen, Jie Dong, William J. Craigen, and Xiaonan Zhao

Subjects
Oncology, medicine.medical_specialty, business.industry, Endocrinology, Diabetes and Metabolism, medicine.disease, Biochemistry, Uniparental disomy, Leukemia, Endocrinology, Internal medicine, Genetics, Medicine, Clinical significance, business, Molecular Biology, Exome sequencing
Published
2021

18. Enhanced cytarabine-induced killing in OGG1-deficient acute myeloid leukemia cells

Author

Amanda K. McCullough, Samantha A. Moellmer, Sydney K. Cammann, Nichole Owen, Irina G. Minko, and R. Stephen Lloyd

Subjects
0301 basic medicine, Antimetabolites, Antineoplastic, DNA Repair, DNA damage, DNA polymerase, DNA repair, DNA polymerase delta, DNA Glycosylases, 03 medical and health sciences, 0302 clinical medicine, PARP1, Cell Line, Tumor, medicine, Humans, RNA, Messenger, Multidisciplinary, biology, Chemistry, Cytarabine, Myeloid leukemia, Biological Sciences, Leukemia, Myeloid, Acute, 030104 developmental biology, Cell killing, 8-Hydroxy-2'-Deoxyguanosine, 030220 oncology & carcinogenesis, Core Binding Factor Alpha 2 Subunit, biology.protein, Cancer research, medicine.drug
Abstract

Human clinical trials suggest that inhibition of enzymes in the DNA base excision repair (BER) pathway, such as PARP1 and APE1, can be useful in anticancer strategies when combined with certain DNA-damaging agents or tumor-specific genetic deficiencies. There is also evidence suggesting that inhibition of the BER enzyme 8-oxoguanine DNA glycosylase-1 (OGG1), which initiates repair of 8-oxo-7,8-dihydro-2'-deoxyguanosine (8-oxo-dG) and 2,6-diamino-4-hydroxy-5-formamidopyrimidine (Fapy-dG), could be useful in treating certain cancers. Specifically, in acute myeloid leukemia (AML), both the RUNX1-RUNX1T1 fusion and the CBFB-MYH11 subtypes have lower levels of OGG1 expression, which correlate with increased therapeutic-induced cell cytotoxicity and good prognosis for improved, relapse-free survival compared with other AML patients. Here we present data demonstrating that AML cell lines deficient in OGG1 have enhanced sensitivity to cytarabine (cytosine arabinoside [Ara-C]) relative to OGG1-proficient cells. This enhanced cytotoxicity correlated with endogenous oxidatively-induced DNA damage and Ara-C-induced DNA strand breaks, with a large proportion of these breaks occurring at common fragile sites. This lethality was highly specific for Ara-C treatment of AML cells deficient in OGG1, with no other replication stress-inducing agents showing a correlation between cell killing and low OGG1 levels. The mechanism for this preferential toxicity was addressed using in vitro replication assays in which DNA polymerase δ was shown to insert Ara-C opposite 8-oxo-dG, resulting in termination of DNA synthesis. Overall, these data suggest that incorporation of Ara-C opposite unrepaired 8-oxo-dG may be the fundamental mechanism conferring selective toxicity and therapeutic effectiveness in OGG1-deficient AML cells.

Published
2021

20. Alpha-synuclein is a DNA binding protein that modulates DNA repair with implications for Lewy body disorders

Author

Amanda K. McCullough, Sydney Weber Boutros, Tamily A. Weissman, Randall L. Woltjer, Colin M. Wakeham, Sydney E. Dent, Valerie R. Osterberg, Jacob Raber, Esteban Luna, Nichole Owen, Leah J. Weston, Kelvin C. Luk, Vivek K. Unni, Allison J. Schaser, and Teresa L. Stackhouse

Subjects
Lewy Body Disease, 0301 basic medicine, Programmed cell death, DNA End-Joining Repair, DNA damage, DNA repair, Parkinson's disease, animal diseases, Transgene, lcsh:Medicine, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Animals, Humans, DNA Breaks, Double-Stranded, lcsh:Science, Cells, Cultured, Mice, Knockout, Neurons, Alpha-synuclein, Multidisciplinary, Lewy body, Chemistry, lcsh:R, Brain, Parkinson Disease, medicine.disease, nervous system diseases, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, nervous system, alpha-Synuclein, lcsh:Q, Lewy Bodies, Dementia, 030217 neurology & neurosurgery, DNA
Abstract

Alpha-synuclein is a presynaptic protein that forms abnormal cytoplasmic aggregates in Lewy body disorders. Although nuclear alpha-synuclein localization has been described, its function in the nucleus is not well understood. We demonstrate that alpha-synuclein modulates DNA repair. First, alpha-synuclein colocalizes with DNA damage response components within discrete foci in human cells and mouse brain. Removal of alpha-synuclein in human cells leads to increased DNA double-strand break (DSB) levels after bleomycin treatment and a reduced ability to repair these DSBs. Similarly, alpha-synuclein knock-out mice show increased neuronal DSBs that can be rescued by transgenic reintroduction of human alpha-synuclein. Alpha-synuclein binds double-stranded DNA and helps to facilitate the non-homologous end-joining reaction. Using a new, in vivo imaging approach that we developed, we find that serine-129-phosphorylated alpha-synuclein is rapidly recruited to DNA damage sites in living mouse cortex. We find that Lewy inclusion-containing neurons in both mouse model and human-derived patient tissue demonstrate increased DSB levels. Based on these data, we propose a model whereby cytoplasmic aggregation of alpha-synuclein reduces its nuclear levels, increases DSBs, and may contribute to programmed cell death via nuclear loss-of-function. This model could inform development of new treatments for Lewy body disorders by targeting alpha-synuclein-mediated DNA repair mechanisms.

Published
2019

21. DNA polymerase ζ limits chromosomal damage and promotes cell survival following aflatoxin exposure

Author

Ying-Chih Lin, Nichole Owen, Irina G. Minko, Sabine S. Lange, Junya Tomida, Liang Li, Michael P. Stone, Richard D. Wood, Amanda K. McCullough, and R. Stephen Lloyd

Subjects
0301 basic medicine, Mutation, Multidisciplinary, biology, DNA polymerase, Mutagenesis, technology, industry, and agriculture, food and beverages, Biological Sciences, medicine.disease_cause, Molecular biology, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, REV3L, chemistry, 030220 oncology & carcinogenesis, biology.protein, medicine, Depurination, heterocyclic compounds, Chromatid, Polymerase, DNA
Abstract

Routine dietary consumption of foods that contain aflatoxins is the second leading cause of environmental carcinogenesis worldwide. Aflatoxin-driven mutagenesis is initiated through metabolic activation of aflatoxin B1 (AFB1) to its epoxide form that reacts with N7 guanine in DNA. The resulting AFB1-N7-dG adduct undergoes either spontaneous depurination or imidazole-ring opening yielding formamidopyrimidine AFB1 (AFB1-Fapy-dG). Because this latter adduct is known to persist in human tissues and contributes to the high frequency G-to-T mutation signature associated with many hepatocellular carcinomas, we sought to establish the identity of the polymerase(s) involved in processing this lesion. Although our previous biochemical analyses demonstrated the ability of polymerase ζ (pol ζ) to incorporate an A opposite AFB1-Fapy-dG and extend from this mismatch, biological evidence supporting a unique role for this polymerase in cellular tolerance following aflatoxin exposure has not been established. Following challenge with AFB1, survival of mouse cells deficient in pol ζ (Rev3L-/-) was significantly reduced relative to Rev3L+/- cells or Rev3L-/- cells complemented through expression of the wild-type human REV3L. Furthermore, cell-cycle progression of Rev3L-/- mouse embryo fibroblasts was arrested in late S/G2 following AFB1 exposure. These Rev3L-/- cells showed an increase in replication-dependent formation of γ-H2AX foci, micronuclei, and chromosomal aberrations (chromatid breaks and radials) relative to Rev3L+/- cells. These data suggest that pol ζ is essential for processing AFB1-induced DNA adducts and that, in its absence, cells do not have an efficient backup polymerase or a repair/tolerance mechanism facilitating survival.

Published
2016

22. An RNAi screen in human cell lines reveals conserved DNA damage repair pathways that mitigate formaldehyde sensitivity

Author

Nichole Owen, Asia D. Mitchell, Anuradha Kumari, Raymond J. Monnat, Amanda K. McCullough, Eleonora Juarez, Nyasha Chambwe, and Weiliang Tang

Subjects
0301 basic medicine, DNA Repair, DNA repair, DNA damage, Cell, Biology, medicine.disease_cause, Biochemistry, Article, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Formaldehyde, medicine, Humans, Molecular Biology, Gene, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Cell growth, DNA replication, Genomics, Cell Biology, 3. Good health, Cell biology, 030104 developmental biology, medicine.anatomical_structure, chemistry, Cell culture, 030220 oncology & carcinogenesis, RNA Interference, Homologous recombination, Genotoxicity, DNA, DNA Damage
Abstract

Formaldehyde is a ubiquitous DNA damaging agent, with human exposures occurring from both exogenous and endogenous sources. Formaldehyde exposure can result in multiple types of DNA damage, including DNA-protein crosslinks and thus, is representative of other exposures that induce DNA-protein crosslinks such as cigarette smoke, automobile exhaust, wood smoke, metals, ionizing radiation, and certain chemotherapeutics. Our objective in this study was to identify the genes necessary to mitigate formaldehyde toxicity following chronic exposure in human cells. We used siRNAs that targeted 320 genes representing all major human DNA repair and damage response pathways, in order to assess cell proliferation following siRNA depletion and subsequent formaldehyde treatment. Three unrelated human cell lines frequently used in genotoxicity studies (SW480, U-2 OS and GM00639) were used to identify common pathways involved in mitigating formaldehyde sensitivity. Although there were gene-specific differences among the cell lines, four inter-related cellular pathways were determined to mitigate formaldehyde toxicity: homologous recombination, DNA double-strand break repair, ionizing radiation response and DNA replication. Additional insight into cell line-specific response patterns was obtained by using a combination of exome sequencing and Cancer Cell Line Encyclopedia genomic data. The results of this DNA damage repair pathway-focused siRNA screen for formaldehyde toxicity in human cells provide a foundation for detailed mechanistic analyses of pathway-specific involvement in the response to environmentally-induced DNA-protein crosslinks and, more broadly, genotoxicity studies using human and other mammalian cell lines.

Published
2018

23. Modulation of UVB-induced Carcinogenesis by Activation of Alternative DNA Repair Pathways

Author

Yan Sha, R. Stephen Lloyd, Marcus J. Calkins, Nichole Owen, Amanda K. McCullough, Lisa E. Goldsmith, Jeong Y. Lim, Andy Kaempf, Vladimir Vartanian, Paul W. Doetsch, Zahra Mirafzali, Stephanie Mengden Koon, Sara Mir, Courtney S. Thompson, Chun Luo, Huaping He, and S. Brown

Subjects
0301 basic medicine, Genome instability, Skin Neoplasms, DNA Repair, DNA repair, DNA damage, Carcinogenesis, Ultraviolet Rays, viruses, lcsh:Medicine, Pyrimidine dimer, medicine.disease_cause, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Animals, lcsh:Science, Mice, Hairless, Multidisciplinary, lcsh:R, Molecular biology, Recombinant Proteins, 3. Good health, 030104 developmental biology, DNA Repair Enzymes, chemistry, DNA glycosylase, 030220 oncology & carcinogenesis, lcsh:Q, DNA, Nuclear localization sequence
Abstract

The molecular basis for ultraviolet (UV) light-induced nonmelanoma and melanoma skin cancers centers on cumulative genomic instability caused by inefficient DNA repair of dipyrimidine photoproducts. Inefficient DNA repair and subsequent translesion replication past these DNA lesions generate distinct molecular signatures of tandem CC to TT and C to T transitions at dipyrimidine sites. Since previous efforts to develop experimental strategies to enhance the repair capacity of basal keratinocytes have been limited, we have engineered the N-terminally truncated form (Δ228) UV endonuclease (UVDE) from Schizosaccharomyces pombe to include a TAT cell-penetrating peptide sequence with or without a nuclear localization signal (NLS): UVDE-TAT and UVDE-NLS-TAT. Further, a NLS was engineered onto a pyrimidine dimer glycosylase from Paramecium bursaria chlorella virus-1 (cv-pdg-NLS). Purified enzymes were encapsulated into liposomes and topically delivered to the dorsal surface of SKH1 hairless mice in a UVB-induced carcinogenesis study. Total tumor burden was significantly reduced in mice receiving either UVDE-TAT or UVDE-NLS-TAT versus control empty liposomes and time to death was significantly reduced with the UVDE-NLS-TAT. These data suggest that efficient delivery of exogenous enzymes for the initiation of repair of UVB-induced DNA damage may protect from UVB induction of squamous and basal cell carcinomas.

Published
2018

24. Bloom Syndrome Radials Are Predominantly Non-Homologous and Are Suppressed by Phosphorylated BLM

Author

Robb E. Moses, Susan B. Olson, Navid Ziaie, Scott Rennie, Nichole Owen, Amy E. Hanlon Newell, Asia D. Mitchell, and James Hejna

Subjects
Genome instability, 0303 health sciences, Mutation, Cell cycle checkpoint, Sister chromatid exchange, Biology, medicine.disease, medicine.disease_cause, Molecular biology, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Chromosome instability, Genetics, medicine, Homologous chromosome, Sister chromatids, Bloom syndrome, Molecular Biology, Genetics (clinical), 030304 developmental biology
Abstract

Biallelic mutations in BLM cause Bloom syndrome (BS), a genome instability disorder characterized by growth retardation, sun sensitivity and a predisposition to cancer. As evidence of decreased genome stability, BS cells demonstrate not only elevated levels of spontaneous sister chromatid exchanges (SCEs), but also exhibit chromosomal radial formation. The molecular nature and mechanism of radial formation is not known, but radials have been thought to be DNA recombination intermediates between homologs that failed to resolve. However, we find that radials in BS cells occur over 95% between non-homologous chromosomes, and occur non-randomly throughout the genome. BLM must be phosphorylated at T99 and T122 for certain cell cycle checkpoints, but it is not known whether these modifications are necessary to suppress radial formation. We find that exogenous BLM constructs preventing phosphorylation at T99 and T122 are not able to suppress radial formation in BS cells, but are able to inhibit SCE formation. These findings indicate that BLM functions in 2 distinct pathways requiring different modifications. In one pathway, for which the phosphorylation marks appear dispensable, BLM functions to suppress SCE formation. In a second pathway, T99 and T122 phosphorylations are essential for suppression of chromosomal radial formation, both those formed spontaneously and those formed following interstrand crosslink damage.

Published
2014

25. Enhanced Sensitivity of Neil1−/− Mice to Chronic UVB Exposure

Author

Güldal Kirkali, Amanda K. McCullough, Vladimir Vartanian, Pawel Jaruga, Miral Dizdaroglu, R. Stephen Lloyd, Marcus J. Calkins, and Nichole Owen

Subjects
0301 basic medicine, Guanine, DNA Repair, Ultraviolet Rays, medicine.medical_treatment, NEIL1, Biology, medicine.disease_cause, Biochemistry, Article, DNA Glycosylases, 030207 dermatology & venereal diseases, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, medicine, Animals, Uracil, Molecular Biology, Skin, chemistry.chemical_classification, Inflammation, Mice, Knockout, Reactive oxygen species, Gene Expression Profiling, Cell Biology, Base excision repair, Molecular biology, Oxidative Stress, 030104 developmental biology, Cytokine, Pyrimidines, chemistry, Gene Expression Regulation, Neutrophil Infiltration, DNA glycosylase, Cytokines, Carcinogenesis, Reactive Oxygen Species, DNA, Oxidative stress, Thymine, DNA Damage
Abstract

Oxidative stress and reactive oxygen species (ROS)-induced DNA base damage are thought to be central mediators of UV-induced carcinogenesis and skin aging. However, increased steady-state levels of ROS-induced DNA base damage have not been reported after chronic UV exposure. Accumulation of ROS-induced DNA base damage is governed by rates of lesion formation and repair. Repair is generally performed by Base Excision Repair (BER), which is initiated by DNA glycosylases, such as 8-oxoguanine glycosylase and Nei-Endonuclease VIII-Like 1 (NEIL1). In the current study, UV light (UVB) was used to elicit protracted low-level ROS challenge in wild-type (WT) and Neil1 −/− mouse skin. Relative to WT controls, Neil1 −/− mice showed an increased sensitivity to tissue destruction from the chronic UVB exposure, and corresponding enhanced chronic inflammatory responses as measured by cytokine message levels and profiling, as well as neutrophil infiltration. Additionally, levels of several ROS-induced DNA lesions were measured including 4,6-diamino-5-formamidopyrimidine (FapyGua), 2,6-diamino-4-hydroxy-5-formamidopyrimidine (FapyAde), 8-hydroxyguanine (8-OH-Gua), 5,6-dihydroxyuracil (5,6-diOH-Ura) and thymine glycol (ThyGly). In WT mice, chronic UVB exposure led to increased steady-state levels of FapyGua, FapyAde, and ThyGly with no significant increases in 8-OH-Gua or 5,6-diOH-Ura. Interestingly, the lesions that accumulated were all substrates of NEIL1. Collectively, these data suggest that NEIL1-initiated repair of a subset of ROS-induced DNA base lesions may be insufficient to prevent the initiation of inflammatory pathways during chronic UV exposure in mouse skin.

Published
2016

26. FANCD2 facilitates replication through common fragile sites

Author

Susan B. Olson, María L. García-Rubio, Emilia Herrera-Moyano, Zi Yan, Carl L. Schildkraut, Nichole Owen, Jeannine Gerhardt, Elizabeth A Vuono, Niall G. Howlett, Advaitha Madireddy, Andrés Aguilera, Rebecca A. Boisvert, Settapong T. Kosiyatrakul, Universidad de Sevilla. Departamento de Genética, National Institute of General Medical Sciences (US), New York State, Starr Cancer Consortium, American Lung Association, Ministerio de Economía y Competitividad (España), and European Research Council

Subjects
0301 basic medicine, DNA re-replication, DNA Replication, Genomic instability, musculoskeletal diseases, Herpesvirus 4, Human, congenital, hereditary, and neonatal diseases and abnormalities, Common fragile sites, Gene Expression, DNA replication, Pre-replication complex, Article, DNA replication factor CDT1, 03 medical and health sciences, Control of chromosome duplication, SeqA protein domain, hemic and lymphatic diseases, cancer, Humans, Lymphocytes, Molecular Biology, Cell Line, Transformed, Genetics, BRCA2 Protein, biology, Fanconi Anemia Complementation Group A Protein, DNA:RNA hybrids, Chromosome Fragile Sites, Fanconi Anemia Complementation Group D2 Protein, nutritional and metabolic diseases, RNA hybrids [DNA], Cell Biology, DNA, Fibroblasts, genomic instability, Fanconi Anemia Complementation Group Proteins, 3. Good health, 030104 developmental biology, Licensing factor, Fanconi Anemia, Fanconi anemia, biology.protein, Origin recognition complex, RNA, common fragile sites
Abstract

Madireddy, Advaitha et al., Common fragile sites (CFSs) are genomic regions that are unstable under conditions of replicative stress. Although the characteristics of CFSs that render them vulnerable to stress are associated mainly with replication, the cellular pathways that protect CFSs during replication remain unclear. Here, we identify and describe a role for FANCD2 as a trans-acting facilitator of CFS replication, in the absence of exogenous replicative stress. In the absence of FANCD2, replication forks stall within the AT-rich fragility core of CFS, leading to dormant origin activation. Furthermore, FANCD2 deficiency is associated with DNA:RNA hybrid formation at CFS-FRA16D, and inhibition of DNA:RNA hybrid formation suppresses replication perturbation. In addition, we also found that FANCD2 reduces the number of potential sites of replication initiation. Our data demonstrate that FANCD2 protein is required to ensure efficient CFS replication and provide mechanistic insight into how FANCD2 regulates CFS stability., This work was supported by National Institute of General Medical Sciences grant 5R01-GM045751 and Empire State Stem Cell Fund through New York State contract C024348 and the Tri-Institutional Stem Cell Initiative, funded by the Starr Foundation to C.L.S.; National Heart, Lung, and Blood Institute grant R01HL101977 to N.G.H.; and Spanish Ministry of Economy and Competitiveness BFU2013-15687 and European ERC-2014-ADG 669898 TARLOOP grants to A.A.

Published
2016

27. Multiple loci contribute to genome-wide recombination levels in male mice

Author

Terry J. Hassold, Nichole Owen, Brenda M. Murdoch, Sofia Shirley, Sara Crumb, and Karl W. Broman

Subjects
Male, Genotype, Quantitative Trait Loci, Biology, Quantitative trait locus, MLH1, Genetic recombination, Genome, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Meiosis, Spermatocytes, Genetics, Animals, Allele, Alleles, Crosses, Genetic, Genetic Association Studies, Adaptor Proteins, Signal Transducing, 030304 developmental biology, Recombination, Genetic, 0303 health sciences, Nuclear Proteins, Chromosomes, Mammalian, Mice, Inbred C57BL, Expression quantitative trait loci, Female, MutL Protein Homolog 1, 030217 neurology & neurosurgery, Recombination
Abstract

Recent linkage-based studies in humans suggest the presence of loci that affect either genome-wide recombination rates, utilization of recombination hotspots, or both. We have been interested in utilizing cytological methodology to directly assess recombination in mammalian meiocytes and to identify recombination-associated loci. In the present report we summarize studies in which we combined a cytological assay of recombination in mouse pachytene spermatocytes with QTL analyses to identify loci that contribute to genome-wide levels of recombination in male meiosis. Specifically, we analyzed MLH1 foci, a marker of crossovers, in 194 F2 male mice derived from a subspecific cross between CAST/EiJ and C57BL/6J parental strains. We then used these data to uncover loci associated with individual variation in mean MLH1 values. We identified seven recombination-associated loci across the genome (on chromosomes 2, 3, 4, 14, 15, 17, and X), indicating that there are multiple recombination "setting" loci in mammalian male meiosis.

Published
2010

28. Contents Vol. 144, 2014

Author

Stephen R. Braddock, Francisco Galán, Petra Musilova, Doralice M. Cella, Jiri Rubes, Hidekazu Saito, Alberto Plaja, Mara Cristina de Almeida, Yingjun Xie, Kaline Ziemniczak, Paulo Augusto de Lima-Filho, Kazuki Saito, Marcelo de Bello Cioffi, Yoichi Matsubara, Xiaoman Wang, Roberto Ferreira Artoni, Kazuhiko Nakabayashi, Yoko Tanaka, Hiroshi Okada, Sonia Mayo, Min Chen, James Hejna, Weiqiang Liu, Wagner Franco Molina, Hiromichi Ishikawa, Wenyin He, Miguel del Campo, Viviane Nogaroto, Wei Jian, Yoshitomo Kobori, Viviane F. Mattos, Pruthvi Pota, Tsutomu Ogata, Mami Miyado, Luis A. Alcaraz, Marielle Cristina Schneider, Josiane B. Traldi, Maki Fukami, Marcelo Ricardo Vicari, Neus Castells, Jacqueline R. Batanian, Teresa Vendrell, Orlando Moreira-Filho, Vasiliki Grammatopoulou, Cristina Hernando, Ana Cueto, Jiri Vahala, Hana Sebestova, Nichole Owen, Vanessa Penacho, Jitka Drbalova, Luiz Antonio Carlos Bertollo, Asia D. Mitchell, Erin Torti, Xiaofang Sun, Ding Wang, Robb E. Moses, Susan B. Olson, Tina-A. Martín-Bayón, Scott Rennie, Asunción Fernández, Francisco Martínez-Castellano, Irene Manchón, Olaya Villa, Jun Wei, Karlla Danielle Jorge Amorim, Elisabet Lloveras, Svatava Kubickova, Satz Mengensatzproduktion, Momori Katsumi, Alfonso Carrasco, Navid Ziaie, Druckerei Stückle, Amy E. Hanlon Newell, and Leonardo S. Carvalho

Subjects
Botany, Genetics, Biology, Molecular Biology, Genetics (clinical)
Published
2015

29. Altered Cohesin Gene Dosage Affects Mammalian Meiotic Chromosome Structure and Behavior

Author

Huiling Xu, So I. Nagaoka, Rolf Jessberger, Nichole Owen, Patricia A. Hunt, Terry J. Hassold, Ekaterina Revenkova, Brenda M. Murdoch, Helen Smith, Michelle Stevense, Michael J. McKay, and Jun Fu

Subjects
Cancer Research, lcsh:QH426-470, Chromosomal Proteins, Non-Histone, Gene Dosage, Cell Cycle Proteins, Biology, Chromosomes, Chromosome segregation, 03 medical and health sciences, Mice, 0302 clinical medicine, Prophase, Meiosis, Chromosome Segregation, Genetics, Homologous chromosome, Animals, Humans, Molecular Biology, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Recombination, Genetic, 0303 health sciences, Cohesin, Chromosome Biology, Synaptonemal Complex, Synapsis, Nuclear Proteins, Genomics, Phosphoproteins, lcsh:Genetics, Synaptonemal complex, Chromosome Pairing, Mutation, Chromatid, Female, 030217 neurology & neurosurgery, Research Article
Abstract

Based on studies in mice and humans, cohesin loss from chromosomes during the period of protracted meiotic arrest appears to play a major role in chromosome segregation errors during female meiosis. In mice, mutations in meiosis-specific cohesin genes cause meiotic disturbances and infertility. However, the more clinically relevant situation, heterozygosity for mutations in these genes, has not been evaluated. We report here evidence from the mouse that partial loss of gene function for either Smc1b or Rec8 causes perturbations in the formation of the synaptonemal complex (SC) and affects both synapsis and recombination between homologs during meiotic prophase. Importantly, these defects increase the frequency of chromosomally abnormal eggs in the adult female. These findings have important implications for humans: they suggest that women who carry mutations or variants that affect cohesin function have an elevated risk of aneuploid pregnancies and may even be at increased risk of transmitting structural chromosome abnormalities., Author Summary Chromosome segregation errors during meiosis are the leading cause of birth defects and miscarriages in humans. While the basis for these errors is unknown, recent studies suggest that defective sister chromatid cohesion may be an important contributor. Accordingly, we tested the hypothesis that partial loss of gene function for either of two meiosis-specific cohesins, Smc1b or Rec8, might adversely affect synapsis or recombination between homologs during meiotic prophase. Our analyses of different mouse models demonstrate cohesin dosage effects on meiosis in both males and females. Importantly, reduced gene function led to an increase the frequency of chromosomally abnormal eggs in the adult female, suggesting that, in humans, women carrying cohesin mutations may be at an increased risk of chromosomally abnormal pregnancies.

Published
2013

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