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Publication DateCell Reports, ISSN 2211-1247, 06/2019, Volume 27, Issue 13, pp. 3790 - 3798.e7
The tumor suppressor BRCA2 is essential for homologous recombination (HR), replication fork stability, and DNA interstrand crosslink repair in vertebrates. We...
spermatogenesis | HSF2BP | meiosis | homologous recombination | BRCA2 | REPAIR | PROTEIN | RAD51 | GENE | CHROMOSOME SYNAPSIS | DNA-DAMAGE | GENOME-WIDE | HOMOLOGOUS RECOMBINATION | FANCONI-ANEMIA | CANCER | CELL BIOLOGY
spermatogenesis | HSF2BP | meiosis | homologous recombination | BRCA2 | REPAIR | PROTEIN | RAD51 | GENE | CHROMOSOME SYNAPSIS | DNA-DAMAGE | GENOME-WIDE | HOMOLOGOUS RECOMBINATION | FANCONI-ANEMIA | CANCER | CELL BIOLOGY
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Loading RightsNature Reviews Cancer, ISSN 1474-175X, 2014, Volume 14, Issue 7, pp. 481 - 493
Recent developments and improvements of multimodal imaging methods for use in animal research have substantially strengthened the options of in vivo...
COLON-CANCER | ENGINEERED MOUSE MODELS | CELL-TRACKING | ONCOLOGY | PROSTATE-CANCER | DRUG DISCOVERY | ANIMAL-MODELS | ORTHOTOPIC MODEL | FLUORESCENT PROTEIN | DYNAMICS IN-VIVO | HUMANIZED MICE | Neoplasms - metabolism | Neoplasms - therapy | Animals | Neoplasms - genetics | Molecular Imaging - instrumentation | Humans | Translational Medical Research | Molecular Imaging - methods | Neoplasms - diagnosis | Disease Models, Animal | Usage | Genetic aspects | Diagnostic imaging | Diagnosis | Research | Cancer
COLON-CANCER | ENGINEERED MOUSE MODELS | CELL-TRACKING | ONCOLOGY | PROSTATE-CANCER | DRUG DISCOVERY | ANIMAL-MODELS | ORTHOTOPIC MODEL | FLUORESCENT PROTEIN | DYNAMICS IN-VIVO | HUMANIZED MICE | Neoplasms - metabolism | Neoplasms - therapy | Animals | Neoplasms - genetics | Molecular Imaging - instrumentation | Humans | Translational Medical Research | Molecular Imaging - methods | Neoplasms - diagnosis | Disease Models, Animal | Usage | Genetic aspects | Diagnostic imaging | Diagnosis | Research | Cancer
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Loading RightsThe New England Journal of Medicine, ISSN 0028-4793, 04/2019, Volume 380, Issue 16, pp. 1499 - 1508
Patients presenting within 36 hours after the onset of atrial fibrillation were randomly assigned to undergo early cardioversion or to receive rate-control...
To be checked for WOS id | STROKE | MEDICINE, GENERAL & INTERNAL | DESIGN | MANAGEMENT | SPONTANEOUS CONVERSION | GUIDELINES | ABLATION | ECHOCARDIOGRAPHY | CATHETER | TEMPORAL RELATIONSHIP | ANTICOAGULATION | Heart Rate | Recurrence | Emergency Service, Hospital | Time-to-Treatment | Atrial Fibrillation - drug therapy | Atrial Fibrillation - therapy | Humans | Middle Aged | Calcium Channel Blockers - therapeutic use | Kaplan-Meier Estimate | Male | Treatment Outcome | Anti-Arrhythmia Agents - therapeutic use | Electric Countershock - adverse effects | Anti-Arrhythmia Agents - adverse effects | Quality of Life | Female | Aged | Digoxin - therapeutic use | Adrenergic beta-Antagonists - therapeutic use | Care and treatment | Usage | Safety and security measures | Electric countershock | Atrial fibrillation | Heart failure | Cardiac arrhythmia | Medical research | Stroke | Review boards | Research & development--R&D | Family medical history | Patients | Outpatient care facilities | Sinuses | Hospitals | Fibrillation | Electrocardiography | Full text | Cardiology
To be checked for WOS id | STROKE | MEDICINE, GENERAL & INTERNAL | DESIGN | MANAGEMENT | SPONTANEOUS CONVERSION | GUIDELINES | ABLATION | ECHOCARDIOGRAPHY | CATHETER | TEMPORAL RELATIONSHIP | ANTICOAGULATION | Heart Rate | Recurrence | Emergency Service, Hospital | Time-to-Treatment | Atrial Fibrillation - drug therapy | Atrial Fibrillation - therapy | Humans | Middle Aged | Calcium Channel Blockers - therapeutic use | Kaplan-Meier Estimate | Male | Treatment Outcome | Anti-Arrhythmia Agents - therapeutic use | Electric Countershock - adverse effects | Anti-Arrhythmia Agents - adverse effects | Quality of Life | Female | Aged | Digoxin - therapeutic use | Adrenergic beta-Antagonists - therapeutic use | Care and treatment | Usage | Safety and security measures | Electric countershock | Atrial fibrillation | Heart failure | Cardiac arrhythmia | Medical research | Stroke | Review boards | Research & development--R&D | Family medical history | Patients | Outpatient care facilities | Sinuses | Hospitals | Fibrillation | Electrocardiography | Full text | Cardiology
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Loading RightsIEEE Transactions on Medical Imaging, ISSN 0278-0062, 03/2010, Volume 29, Issue 3, pp. 852 - 867
Cell segmentation and tracking in time-lapse fluorescence microscopy images is a task of fundamental importance in many biological studies on cell migration...
Level set | Biological system modeling | Fluorescence | fluorescence microscopy | multiple object tracking | Image segmentation | level sets | Evolution (biology) | Microscopy | cell tracking | Cells (biology) | Biology computing | Robustness | Labeling | Cell segmentation | Level sets | Cell tracking | Multiple object tracking | Fluorescence microscopy | MIGRATION | MEAN-SHIFT | ENGINEERING, BIOMEDICAL | IMAGING SCIENCE & PHOTOGRAPHIC TECHNOLOGY | ENGINEERING, ELECTRICAL & ELECTRONIC | COMPUTER SCIENCE, INTERDISCIPLINARY APPLICATIONS | NUCLEI | LINEAGE CONSTRUCTION | IMAGE-ANALYSIS | SEGMENTATION | LIGHT-MICROSCOPY | ACTIVE CONTOURS | RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING | CYCLE | MOTILITY | Reproducibility of Results | Humans | Cell Separation - methods | Cell Movement - physiology | Algorithms | Microscopy, Fluorescence - methods | Cell Division | Sensitivity and Specificity | Bayes Theorem | Biomarkers | HeLa Cells | Fluorescent Dyes | Luminescent Proteins | Databases, Factual | CT imaging | Usage | Diagnostic imaging | Analysis | Morphology | Studies | Proteins | Cell division | Cell adhesion & migration
Level set | Biological system modeling | Fluorescence | fluorescence microscopy | multiple object tracking | Image segmentation | level sets | Evolution (biology) | Microscopy | cell tracking | Cells (biology) | Biology computing | Robustness | Labeling | Cell segmentation | Level sets | Cell tracking | Multiple object tracking | Fluorescence microscopy | MIGRATION | MEAN-SHIFT | ENGINEERING, BIOMEDICAL | IMAGING SCIENCE & PHOTOGRAPHIC TECHNOLOGY | ENGINEERING, ELECTRICAL & ELECTRONIC | COMPUTER SCIENCE, INTERDISCIPLINARY APPLICATIONS | NUCLEI | LINEAGE CONSTRUCTION | IMAGE-ANALYSIS | SEGMENTATION | LIGHT-MICROSCOPY | ACTIVE CONTOURS | RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING | CYCLE | MOTILITY | Reproducibility of Results | Humans | Cell Separation - methods | Cell Movement - physiology | Algorithms | Microscopy, Fluorescence - methods | Cell Division | Sensitivity and Specificity | Bayes Theorem | Biomarkers | HeLa Cells | Fluorescent Dyes | Luminescent Proteins | Databases, Factual | CT imaging | Usage | Diagnostic imaging | Analysis | Morphology | Studies | Proteins | Cell division | Cell adhesion & migration
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Loading RightsCardiovascular Research, ISSN 0008-6363, 11/2018, Volume 114, Issue 13, pp. 1776 - 1793
textabstractMethods and results: In Fibulin-4R/R mice, the extracellular matrix protein Fibulin-4 is 4-fold reduced, resulting in progressive ascending...
Mitochondria | Molecular biology | Aneurysm | Organismal metabolism | HOMEOSTASIS | CARDIAC & CARDIOVASCULAR SYSTEMS | ANGIOTENSIN-II | SMOOTH-MUSCLE-CELL | CONNECTIONS | CARDIOVASCULAR MANIFESTATIONS | CUTIS LAXA | MARFAN-SYNDROME | MUTATIONS | EXPRESSION | CONTRIBUTES | Aneurysm • Mitochondria • Molecular biology • Organismal metabolism | Original
Mitochondria | Molecular biology | Aneurysm | Organismal metabolism | HOMEOSTASIS | CARDIAC & CARDIOVASCULAR SYSTEMS | ANGIOTENSIN-II | SMOOTH-MUSCLE-CELL | CONNECTIONS | CARDIOVASCULAR MANIFESTATIONS | CUTIS LAXA | MARFAN-SYNDROME | MUTATIONS | EXPRESSION | CONTRIBUTES | Aneurysm • Mitochondria • Molecular biology • Organismal metabolism | Original
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Loading RightsNature Structural & Molecular Biology, ISSN 1545-9993, 11/2007, Volume 14, Issue 11, pp. 1096 - 1104
Faithful duplication of the genome requires structure-specific endonucleases such as the RuvABC complex in Escherichia coli. These enzymes help to resolve...
CHECKPOINT KINASE CDS1 | BUDDING YEAST | BIOCHEMISTRY & MOLECULAR BIOLOGY | ESCHERICHIA-COLI | MAMMALIAN-CELLS | SACCHAROMYCES-CEREVISIAE | DAMAGE | CELL BIOLOGY | HOLLIDAY JUNCTION RESOLVASE | IN-VITRO | BIOPHYSICS | GENOME INTEGRITY | HOMOLOGOUS RECOMBINATION | Hydroxyurea - pharmacology | Endonucleases - genetics | Embryonic Stem Cells - cytology | Nucleic Acid Synthesis Inhibitors - pharmacology | Chromosomes, Mammalian - genetics | Humans | Endonucleases - metabolism | DNA Breaks, Double-Stranded | DNA-Binding Proteins - metabolism | Aphidicolin - pharmacology | Embryonic Stem Cells - radiation effects | Nuclear Proteins - genetics | Nucleic Acid Conformation | Chromosomal Instability | Radiation, Ionizing | Rad51 Recombinase - metabolism | Rad51 Recombinase - genetics | Cells, Cultured | Enzyme Inhibitors - pharmacology | Chromosomes, Mammalian - chemistry | DNA Replication | Nuclear Proteins - metabolism | DNA-Binding Proteins - genetics | Embryonic Stem Cells - physiology | Mice, Knockout | DNA Helicases | Animals | Embryonic Stem Cells - drug effects | Cell Cycle - physiology | Mice | Chromosomes, Mammalian - metabolism | Chromosome Aberrations - chemically induced | Physiological aspects | Nucleases | DNA replication | Research | DNA damage | Enzymes | Molecular structure | E coli | Molecular biology | Genomics
CHECKPOINT KINASE CDS1 | BUDDING YEAST | BIOCHEMISTRY & MOLECULAR BIOLOGY | ESCHERICHIA-COLI | MAMMALIAN-CELLS | SACCHAROMYCES-CEREVISIAE | DAMAGE | CELL BIOLOGY | HOLLIDAY JUNCTION RESOLVASE | IN-VITRO | BIOPHYSICS | GENOME INTEGRITY | HOMOLOGOUS RECOMBINATION | Hydroxyurea - pharmacology | Endonucleases - genetics | Embryonic Stem Cells - cytology | Nucleic Acid Synthesis Inhibitors - pharmacology | Chromosomes, Mammalian - genetics | Humans | Endonucleases - metabolism | DNA Breaks, Double-Stranded | DNA-Binding Proteins - metabolism | Aphidicolin - pharmacology | Embryonic Stem Cells - radiation effects | Nuclear Proteins - genetics | Nucleic Acid Conformation | Chromosomal Instability | Radiation, Ionizing | Rad51 Recombinase - metabolism | Rad51 Recombinase - genetics | Cells, Cultured | Enzyme Inhibitors - pharmacology | Chromosomes, Mammalian - chemistry | DNA Replication | Nuclear Proteins - metabolism | DNA-Binding Proteins - genetics | Embryonic Stem Cells - physiology | Mice, Knockout | DNA Helicases | Animals | Embryonic Stem Cells - drug effects | Cell Cycle - physiology | Mice | Chromosomes, Mammalian - metabolism | Chromosome Aberrations - chemically induced | Physiological aspects | Nucleases | DNA replication | Research | DNA damage | Enzymes | Molecular structure | E coli | Molecular biology | Genomics
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Loading RightsEMBO Journal, ISSN 0261-4189, 10/2006, Volume 25, Issue 20, pp. 4921 - 4932
textabstractRepair of interstrand crosslinks (ICLs) requires multiple-strand incisions to separate the two covalently attached strands of DNA. It is unclear...
Stalled replication forks | Structure-specific endonucleases | Interstrand crosslink | Rad54 | Homologous recombination | structure‐specific endonucleases | stalled replication forks | homologous recombination | interstrand crosslink | HOLLIDAY JUNCTION RESOLUTION | FISSION YEAST | structure-specific | BIOCHEMISTRY & MOLECULAR BIOLOGY | SACCHAROMYCES-CEREVISIAE | MAMMALIAN-CELLS | NUCLEOTIDE EXCISION-REPAIR | CELL BIOLOGY | RAD51 NUCLEOPROTEIN FILAMENT | REPLICATION FORKS | DAMAGE REPAIR | ERCC1-XPF | endonucleases | Endonucleases - deficiency | Cells, Cultured | Nuclear Proteins - metabolism | Stem Cells - cytology | Endonucleases - metabolism | Stem Cells - metabolism | DNA Breaks, Double-Stranded | S Phase - genetics | DNA-Binding Proteins - deficiency | Embryo, Mammalian - metabolism | Mice, Knockout | DNA-Binding Proteins - metabolism | DNA Helicases | Endodeoxyribonucleases - genetics | Animals | Embryo, Mammalian - cytology | Recombination, Genetic | DNA Repair | Nuclear Proteins - deficiency | Endodeoxyribonucleases - metabolism | DNA Replication - genetics | Mice | Proteins | Enzymes | Deoxyribonucleic acid | DNA | Rodents | Stem cells | Genetics | structure-specific endonucleases
Stalled replication forks | Structure-specific endonucleases | Interstrand crosslink | Rad54 | Homologous recombination | structure‐specific endonucleases | stalled replication forks | homologous recombination | interstrand crosslink | HOLLIDAY JUNCTION RESOLUTION | FISSION YEAST | structure-specific | BIOCHEMISTRY & MOLECULAR BIOLOGY | SACCHAROMYCES-CEREVISIAE | MAMMALIAN-CELLS | NUCLEOTIDE EXCISION-REPAIR | CELL BIOLOGY | RAD51 NUCLEOPROTEIN FILAMENT | REPLICATION FORKS | DAMAGE REPAIR | ERCC1-XPF | endonucleases | Endonucleases - deficiency | Cells, Cultured | Nuclear Proteins - metabolism | Stem Cells - cytology | Endonucleases - metabolism | Stem Cells - metabolism | DNA Breaks, Double-Stranded | S Phase - genetics | DNA-Binding Proteins - deficiency | Embryo, Mammalian - metabolism | Mice, Knockout | DNA-Binding Proteins - metabolism | DNA Helicases | Endodeoxyribonucleases - genetics | Animals | Embryo, Mammalian - cytology | Recombination, Genetic | DNA Repair | Nuclear Proteins - deficiency | Endodeoxyribonucleases - metabolism | DNA Replication - genetics | Mice | Proteins | Enzymes | Deoxyribonucleic acid | DNA | Rodents | Stem cells | Genetics | structure-specific endonucleases
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Loading RightsAnalytical Chemistry, ISSN 0003-2700, 08/2009, Volume 81, Issue 16, pp. 6879 - 6888
In livestock production, illegal use of natural steroids is hard to prove because metabolites are either unknown or not significantly above highly fluctuating...
liquid-chromatography | androgen bioassay | cattle | dehydroepiandrosterone | metabolites | validation | tandem mass-spectrometry | ratio | CHEMISTRY, ANALYTICAL | METABOLITES | LIQUID-CHROMATOGRAPHY | CATTLE | VALIDATION | RATIO | TANDEM MASS-SPECTROMETRY | DEHYDROEPIANDROSTERONE | ANDROGEN BIOASSAY | Metabolomics | Reproducibility of Results | Animals | Anabolic Agents - urine | Cattle | Dehydroepiandrosterone - administration & dosage | Pregnenolone - urine | Chromatography, Liquid - methods | Dehydroepiandrosterone - urine | Mass Spectrometry - methods | Pregnenolone - administration & dosage | Measurement | Urine | Drugs and athletes | Metabonomic analysis | Hormones in animal nutrition | Drug testing | Mandatory drug testing | Analysis | Anabolic steroids | Chemical properties | Identification and classification | Methods
liquid-chromatography | androgen bioassay | cattle | dehydroepiandrosterone | metabolites | validation | tandem mass-spectrometry | ratio | CHEMISTRY, ANALYTICAL | METABOLITES | LIQUID-CHROMATOGRAPHY | CATTLE | VALIDATION | RATIO | TANDEM MASS-SPECTROMETRY | DEHYDROEPIANDROSTERONE | ANDROGEN BIOASSAY | Metabolomics | Reproducibility of Results | Animals | Anabolic Agents - urine | Cattle | Dehydroepiandrosterone - administration & dosage | Pregnenolone - urine | Chromatography, Liquid - methods | Dehydroepiandrosterone - urine | Mass Spectrometry - methods | Pregnenolone - administration & dosage | Measurement | Urine | Drugs and athletes | Metabonomic analysis | Hormones in animal nutrition | Drug testing | Mandatory drug testing | Analysis | Anabolic steroids | Chemical properties | Identification and classification | Methods
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Loading RightsProceedings of the National Academy of Sciences of the United States of America, ISSN 0027-8424, 6/2011, Volume 108, Issue 24, pp. 9851 - 9856
Defective homologous recombination (HR) DNA repair imposed by BRCA1 or BRCA2 deficiency sensitizes cells to poly (ADP-ribose) polymerase (PARP)-1 inhibition...
B lymphocytes | Homologous recombination | Cell lines | HeLa cells | Small interfering RNA | Immunoblotting | CHO cells | Hyperthermia | Cells | Tumors | Double-strand break | Anti-cancer treatment | RAD51 | PATHWAYS | NUDE-MICE | MUTANT | MECHANISM | MULTIDISCIPLINARY SCIENCES | DNA-DAMAGE | COMBINATION | REPAIR | double-strand break | anti-cancer treatment | PHASE-I | SISTER-CHROMATID EXCHANGES | THERMAL RADIOSENSITIZATION | Embryonic Stem Cells - metabolism | Humans | Transplantation, Heterologous | DNA-Binding Proteins - metabolism | Neoplasms, Experimental - pathology | RNA Interference | Embryonic Stem Cells - radiation effects | Neoplasms, Experimental - genetics | Recombination, Genetic - genetics | Female | Cell Line | Cells, Cultured | Rats | Hot Temperature | DNA-Binding Proteins - genetics | Lactams, Macrocyclic - pharmacology | Piperazines - pharmacology | Poly(ADP-ribose) Polymerase Inhibitors | Benzoquinones - pharmacology | Phthalazines - pharmacology | Poly(ADP-ribose) Polymerases - metabolism | Animals | BRCA2 Protein - metabolism | Poly(ADP-ribose) Polymerases - genetics | Embryonic Stem Cells - drug effects | Tumor Burden - drug effects | Mice, Nude | DNA Repair | Cell Line, Tumor | Mice | Recombination, Genetic - radiation effects | HeLa Cells | Neoplasms, Experimental - metabolism | Quinazolines - pharmacology | BRCA2 Protein - genetics | Recombination, Genetic - drug effects | BRCA mutations | Proteolysis | Cancer cells | Genetic aspects | Research | Genetic recombination | Health aspects | Fever | Cancer | Biological Sciences
B lymphocytes | Homologous recombination | Cell lines | HeLa cells | Small interfering RNA | Immunoblotting | CHO cells | Hyperthermia | Cells | Tumors | Double-strand break | Anti-cancer treatment | RAD51 | PATHWAYS | NUDE-MICE | MUTANT | MECHANISM | MULTIDISCIPLINARY SCIENCES | DNA-DAMAGE | COMBINATION | REPAIR | double-strand break | anti-cancer treatment | PHASE-I | SISTER-CHROMATID EXCHANGES | THERMAL RADIOSENSITIZATION | Embryonic Stem Cells - metabolism | Humans | Transplantation, Heterologous | DNA-Binding Proteins - metabolism | Neoplasms, Experimental - pathology | RNA Interference | Embryonic Stem Cells - radiation effects | Neoplasms, Experimental - genetics | Recombination, Genetic - genetics | Female | Cell Line | Cells, Cultured | Rats | Hot Temperature | DNA-Binding Proteins - genetics | Lactams, Macrocyclic - pharmacology | Piperazines - pharmacology | Poly(ADP-ribose) Polymerase Inhibitors | Benzoquinones - pharmacology | Phthalazines - pharmacology | Poly(ADP-ribose) Polymerases - metabolism | Animals | BRCA2 Protein - metabolism | Poly(ADP-ribose) Polymerases - genetics | Embryonic Stem Cells - drug effects | Tumor Burden - drug effects | Mice, Nude | DNA Repair | Cell Line, Tumor | Mice | Recombination, Genetic - radiation effects | HeLa Cells | Neoplasms, Experimental - metabolism | Quinazolines - pharmacology | BRCA2 Protein - genetics | Recombination, Genetic - drug effects | BRCA mutations | Proteolysis | Cancer cells | Genetic aspects | Research | Genetic recombination | Health aspects | Fever | Cancer | Biological Sciences
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Loading RightsMolecular and Cellular Biology, ISSN 0270-7306, 01/2010, Volume 30, Issue 1, pp. 260 - 272
Article Usage Stats Services MCB Citing Articles Google Scholar PubMed Related Content Social Bookmarking CiteULike Delicious Digg Facebook Google+ Mendeley...
N-METHYLTRANSFERASE | TRANSCRIPTIONAL ACTIVATION | SUBSTRATE-SPECIFICITY | BIOCHEMISTRY & MOLECULAR BIOLOGY | ESTROGEN-RECEPTOR-ALPHA | EFFICIENT GENE DELIVERY | IN-VIVO | BINDING PROTEINS | SUBCELLULAR-LOCALIZATION | HISTONE H4 | MAMMALIAN-CELLS | CELL BIOLOGY | Cell Line | Chromatin - metabolism | Biotinylation | Chromosomal Proteins, Non-Histone - metabolism | Humans | Transcriptional Activation | Substrate Specificity | Nuclear Proteins - metabolism | Protein Methyltransferases - metabolism | Chromosomal Proteins, Non-Histone - genetics | Protein Interaction Mapping | Protein-Arginine N-Methyltransferases - metabolism | Animals | Proteomics | Mice | Protein-Arginine N-Methyltransferases - genetics | Transcription Factors | Methylation | Nuclear Proteins - genetics | Arginine - metabolism | Estradiol - pharmacology | Repressor Proteins - metabolism
N-METHYLTRANSFERASE | TRANSCRIPTIONAL ACTIVATION | SUBSTRATE-SPECIFICITY | BIOCHEMISTRY & MOLECULAR BIOLOGY | ESTROGEN-RECEPTOR-ALPHA | EFFICIENT GENE DELIVERY | IN-VIVO | BINDING PROTEINS | SUBCELLULAR-LOCALIZATION | HISTONE H4 | MAMMALIAN-CELLS | CELL BIOLOGY | Cell Line | Chromatin - metabolism | Biotinylation | Chromosomal Proteins, Non-Histone - metabolism | Humans | Transcriptional Activation | Substrate Specificity | Nuclear Proteins - metabolism | Protein Methyltransferases - metabolism | Chromosomal Proteins, Non-Histone - genetics | Protein Interaction Mapping | Protein-Arginine N-Methyltransferases - metabolism | Animals | Proteomics | Mice | Protein-Arginine N-Methyltransferases - genetics | Transcription Factors | Methylation | Nuclear Proteins - genetics | Arginine - metabolism | Estradiol - pharmacology | Repressor Proteins - metabolism
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Loading RightsMolecular and Cellular Biology, ISSN 0270-7306, 11/2005, Volume 25, Issue 21, pp. 9350 - 9359
Article Usage Stats Services MCB Citing Articles Google Scholar PubMed Related Content Social Bookmarking CiteULike Delicious Digg Facebook Google+ Mendeley...
Cricetinae | Cell Nucleus/metabolism | Cricetulus | Humans | Proliferating Cell Nuclear Antigen/genetics/physiology | DNA Replication/genetics | Protein Transport | Animals | Cell Cycle/radiation effects | Ultraviolet Rays | DNA Repair | Green Fluorescent Proteins/genetics | DNA Damage | Mutation | CHO Cells | Photobleaching | PROTEIN DYNAMICS | BIOCHEMISTRY & MOLECULAR BIOLOGY | IN-VIVO | SITES | HUMAN FIBROBLASTS | INTERPHASE | BINDING | CANCER | DAMAGE | NUCLEOTIDE EXCISION-REPAIR | LIVING CELLS | CELL BIOLOGY | Cell Cycle - radiation effects | Green Fluorescent Proteins - genetics | Proliferating Cell Nuclear Antigen - physiology | Cell Nucleus - metabolism | Proliferating Cell Nuclear Antigen - genetics | DNA Replication - genetics | Chromosome Structure and Dynamics
Cricetinae | Cell Nucleus/metabolism | Cricetulus | Humans | Proliferating Cell Nuclear Antigen/genetics/physiology | DNA Replication/genetics | Protein Transport | Animals | Cell Cycle/radiation effects | Ultraviolet Rays | DNA Repair | Green Fluorescent Proteins/genetics | DNA Damage | Mutation | CHO Cells | Photobleaching | PROTEIN DYNAMICS | BIOCHEMISTRY & MOLECULAR BIOLOGY | IN-VIVO | SITES | HUMAN FIBROBLASTS | INTERPHASE | BINDING | CANCER | DAMAGE | NUCLEOTIDE EXCISION-REPAIR | LIVING CELLS | CELL BIOLOGY | Cell Cycle - radiation effects | Green Fluorescent Proteins - genetics | Proliferating Cell Nuclear Antigen - physiology | Cell Nucleus - metabolism | Proliferating Cell Nuclear Antigen - genetics | DNA Replication - genetics | Chromosome Structure and Dynamics
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Dynamics of DNA Double-Strand Breaks Revealed by Clustering of Damaged Chromosome Domains
Science, ISSN 0036-8075, 1/2004, Volume 303, Issue 5654, pp. 92 - 95
Interactions between ends from different DNA double-strand breaks (DSBs) can produce tumorigenic chromosome translocations. Two theories for the juxtaposition...
Chromatin | Interphase | DNA | DNA damage | HeLa cells | Irradiation | Fibroblasts | Reports | Chromosomes | Cells | Chromosome translocation | REPAIR | COMPLEX | CHROMATIN | HUMAN-CELLS | MULTIDISCIPLINARY SCIENCES | PARTICLE TRACKS | ALPHA | ABERRATIONS | RADIATION | CANCER | FOCI | Translocation, Genetic | Phosphorylation | Cricetulus | Humans | DNA - radiation effects | DNA-Binding Proteins - metabolism | MRE11 Homologue Protein | Cell Nucleus - metabolism | Alpha Particles | Cell Nucleus - radiation effects | S Phase | G2 Phase | Chromosome Breakage | CHO Cells | Fibroblasts - metabolism | Cricetinae | Rad51 Recombinase | Ataxia Telangiectasia - metabolism | Chromosomes, Human - metabolism | DNA - metabolism | G1 Phase | Animals | DNA Repair | Ataxia Telangiectasia - genetics | DNA Damage | HeLa Cells | Histones - metabolism | Chromosomes, Mammalian - metabolism | Chemical properties | Insertion elements, DNA | Research | Proteins | Genes | Deoxyribonucleic acid--DNA
Chromatin | Interphase | DNA | DNA damage | HeLa cells | Irradiation | Fibroblasts | Reports | Chromosomes | Cells | Chromosome translocation | REPAIR | COMPLEX | CHROMATIN | HUMAN-CELLS | MULTIDISCIPLINARY SCIENCES | PARTICLE TRACKS | ALPHA | ABERRATIONS | RADIATION | CANCER | FOCI | Translocation, Genetic | Phosphorylation | Cricetulus | Humans | DNA - radiation effects | DNA-Binding Proteins - metabolism | MRE11 Homologue Protein | Cell Nucleus - metabolism | Alpha Particles | Cell Nucleus - radiation effects | S Phase | G2 Phase | Chromosome Breakage | CHO Cells | Fibroblasts - metabolism | Cricetinae | Rad51 Recombinase | Ataxia Telangiectasia - metabolism | Chromosomes, Human - metabolism | DNA - metabolism | G1 Phase | Animals | DNA Repair | Ataxia Telangiectasia - genetics | DNA Damage | HeLa Cells | Histones - metabolism | Chromosomes, Mammalian - metabolism | Chemical properties | Insertion elements, DNA | Research | Proteins | Genes | Deoxyribonucleic acid--DNA
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