ABSTRACT
Cockayne syndrome (CS) is an inherited disorder that involves photosensitivity, developmental defects, progressive degeneration and characteristics of premature aging. Evidence indicates primarily nuclear roles for the major CS proteins, CSA and CSB, specifically in DNA repair and RNA transcription. We reveal herein a complex regulation of CSB targeting that involves three major consensus signals: NLS1 (aa467-481), which directs nuclear and nucleolar localization in cooperation with NoLS1 (aa302-341), and NLS2 (aa1038-1055), which seemingly optimizes nuclear enrichment. CSB localization to the nucleolus was also found to be important for full UVC resistance. CSA, which does not contain any obvious targeting sequences, was adversely affected (i.e. presumably destabilized) by any form of truncation. No inter-coordination between the subnuclear localization of CSA and CSB was observed, implying that this aspect does not underlie the clinical features of CS. The E3 ubiquitin ligase binding partner of CSA, DDB1, played an important role in CSA stability (as well as DDB2), and facilitated CSA association with chromatin following UV irradiation; yet did not affect CSB chromatin binding. We also observed that initial recruitment of CSB to DNA interstrand crosslinks is similar in the nucleoplasm and nucleolus, although final accumulation is greater in the former. Whereas assembly of CSB at sites of DNA damage in the nucleolus was not affected by RNA polymerase I inhibition, stable retention at these sites of presumed repair was abrogated. Our studies reveal a multi-faceted regulation of the intranuclear dynamics of CSA and CSB that plays a role in mediating their cellular functions.
Subject(s)
Biomarkers , Cell Nucleus/metabolism , Cockayne Syndrome/metabolism , Amino Acid Sequence , Cockayne Syndrome/etiology , DNA Repair Enzymes/chemistry , DNA Repair Enzymes/genetics , DNA Repair Enzymes/metabolism , Fluorescent Antibody Technique , Genes, Reporter , Humans , Intracellular Space , Mutation , Protein Sorting Signals , Protein Transport , Transcription Factors/chemistry , Transcription Factors/genetics , Transcription Factors/metabolismABSTRACT
DNA is constantly being damaged, either by endogenous or exogenous genotoxins. In that regard, DNA repair activities are essential for maintaining genomic stability and to life itself. Mutations in genes encoding DNA repair proteins cause severe human syndromes, but DNA repair defects have also been linked to several other diseases, notably to cancer and normal aging. Recently, new evidence has emerged indicating that some DNA repair diseases display mitochondrial and metabolic dysfunction through mechanisms that are yet being uncovered. These results suggest that mitochondria play an import role in the DNA damage response pathways and that damage accumulation may lead to mitochondrial dysfunction via metabolic imbalance and mitophagy impairment. Here we review the recent findings linking mitochondrial impairment and cell death to DNA damage accumulation in the context of DNA repair defects. In addition, the general involvement of DNA damage in cellular dysfunction suggests that these phenomena may be also involved in other human pathologies in which mitochondrial dysfunction and metabolic disruption play causative roles.
Subject(s)
Congenital Abnormalities/etiology , DNA Repair , Mitochondria/metabolism , Animals , Ataxia Telangiectasia/etiology , Ataxia Telangiectasia/genetics , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , Congenital Abnormalities/genetics , DNA Damage , Humans , Mitophagy , Xeroderma Pigmentosum/etiology , Xeroderma Pigmentosum/geneticsABSTRACT
Ultraviolet (UV) radiation from sunlight is a major etiologic factor for skin cancer, the most prevalent cancer in the United States, as well as premature skin aging. In particular, UVB radiation causes formation of specific DNA damage photoproducts between pyrimidine bases. These DNA damage photoproducts are repaired by a process called nucleotide excision repair, also known as UV-induced DNA repair. When left unrepaired, UVB-induced DNA damage leads to accumulation of mutations, predisposing people to carcinogenesis as well as to premature aging. Genetic loss of nucleotide excision repair leads to severe disorders, namely, xeroderma pigmentosum (XP), trichothiodystrophy (TTD) and Cockayne syndrome (CS), which are associated with predisposition to skin carcinogenesis at a young age as well as developmental and neurological conditions. Regulation of nucleotide excision repair is an attractive avenue to preventing or reversing these detrimental consequences of impaired nucleotide excision repair. Here, we review recent studies on molecular mechanisms regulating nucleotide excision repair by extracellular cues and intracellular signaling pathways, with a special focus on the molecular regulation of individual repair factors.
Subject(s)
Aging/radiation effects , Cockayne Syndrome/metabolism , DNA Repair , Skin Neoplasms/metabolism , Trichothiodystrophy Syndromes/metabolism , Ultraviolet Rays/adverse effects , Xeroderma Pigmentosum/metabolism , Aging/genetics , Aging/metabolism , Carcinogenesis/genetics , Carcinogenesis/metabolism , Carcinogenesis/pathology , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , Cockayne Syndrome/pathology , DNA Repair Enzymes/genetics , DNA Repair Enzymes/metabolism , DNA-Binding Proteins/genetics , DNA-Binding Proteins/metabolism , Gene Expression Regulation , Humans , RNA Polymerase II/genetics , RNA Polymerase II/metabolism , Signal Transduction , Skin Neoplasms/etiology , Skin Neoplasms/genetics , Skin Neoplasms/pathology , Trichothiodystrophy Syndromes/etiology , Trichothiodystrophy Syndromes/genetics , Trichothiodystrophy Syndromes/pathology , Xeroderma Pigmentosum/etiology , Xeroderma Pigmentosum/genetics , Xeroderma Pigmentosum/pathologyABSTRACT
Aberrant mitochondrial structure and function influence tissue homeostasis and thereby contribute to multiple human disorders and ageing. Ten per cent of patients with primary mitochondrial disorders present skin manifestations that can be categorized into hair abnormalities, rashes, pigmentation abnormalities and acrocyanosis. Less attention has been paid to the fact that several disorders of the skin are linked to alterations of mitochondrial energy metabolism. This review article summarizes the contribution of mitochondrial pathology to both common and rare skin diseases. We explore the intriguing observation that a wide array of skin disorders presents with primary or secondary mitochondrial pathology and that a variety of molecular defects can cause dysfunctional mitochondria. Among them are mutations in mitochondrial- and nuclear DNA-encoded subunits and assembly factors of oxidative phosphorylation (OXPHOS) complexes; mutations in intermediate filament proteins involved in linking, moving and shaping of mitochondria; and disorders of mitochondrial DNA metabolism, fatty acid metabolism and heme synthesis. Thus, we assume that mitochondrial involvement is the rule rather than the exception in skin diseases. We conclude the article by discussing how improving mitochondrial function can be beneficial for aged skin and can be used as an adjunct therapy for certain skin disorders. Consideration of mitochondrial energy metabolism in the skin creates a new perspective for both dermatologists and experts in metabolic disease.
Subject(s)
Mitochondria/metabolism , Mitochondrial Diseases/complications , Mitochondrial Diseases/metabolism , Skin Diseases/etiology , Skin Diseases/metabolism , Autoimmune Diseases/etiology , Autoimmune Diseases/genetics , Autoimmune Diseases/metabolism , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , Cockayne Syndrome/metabolism , DNA Repair , DNA, Mitochondrial/genetics , DNA, Mitochondrial/metabolism , Deoxyribonucleotides/metabolism , Energy Metabolism , Fatty Acids/metabolism , Genes, Mitochondrial , Heme/biosynthesis , Humans , Intermediate Filaments/genetics , Intermediate Filaments/metabolism , Intermediate Filaments/pathology , Iron-Sulfur Proteins/biosynthesis , MAP Kinase Signaling System , Mitochondria/genetics , Mitochondria/pathology , Mitochondrial Diseases/genetics , Mitochondrial Proteins/genetics , Mutation , Oxidative Phosphorylation , Skin Aging/genetics , Skin Aging/physiology , Skin Diseases/genetics , Skin Neoplasms/etiology , Skin Neoplasms/genetics , Skin Neoplasms/metabolismABSTRACT
OBJECTIVE: Xeroderma pigmentosum (XP) is a rare autosomal recessive disease caused by mutations in DNA repair genes. Clinical manifestations of XP include mild to extreme sensitivity to ultraviolet radiation resulting in inflammation and neoplasia in sun-exposed areas of the skin, mucous membranes, and ocular surfaces. This report describes the ocular manifestations of XP in patients systematically evaluated in the Clinical Center at the National Institutes of Health. DESIGN: Retrospective observational case series. PARTICIPANTS: Eighty-seven participants, aged 1.3 to 63.4 years, referred to the National Eye Institute (NEI) for examination from 1964 to 2011. Eighty-three patients had XP, 3 patients had XP/Cockayne syndrome complex, and 1 patient had XP/trichothiodystrophy complex. METHODS: Complete age- and developmental stage-appropriate ophthalmic examination. MAIN OUTCOME MEASURES: Visual acuity; eyelid, ocular surface, and lens pathology; tear film and tear production measures; and cytologic analysis of conjunctival surface swabs. RESULTS: Of the 87 patients, 91% had at least 1 ocular abnormality. The most common abnormalities were conjunctivitis (51%), corneal neovascularization (44%), dry eye (38%), corneal scarring (26%), ectropion (25%), blepharitis (23%), conjunctival melanosis (20%), and cataracts (14%). Thirteen percent of patients had some degree of visual axis impingement, and 5% of patients had no light perception in 1 or both eyes. Ocular surface cancer or a history of ocular surface cancer was present in 10% of patients. Patients with an acute sunburning skin phenotype were less likely to develop conjunctival melanosis and ectropion but more likely to develop neoplastic ocular surface lesions than nonburning patients. Some patients also showed signs of limbal stem cell deficiency. CONCLUSIONS: Our longitudinal study reports the ocular status of the largest group of patients with XP systematically examined at 1 facility over an extended period of time. Structural eyelid abnormalities, neoplasms of the ocular surface and eyelids, tear film and tear production abnormalities, ocular surface disease and inflammation, and corneal abnormalities were present in this population. Burning and nonburning patients with XP exhibit different rates of important ophthalmologic findings, including neoplasia. In addition, ophthalmic characteristics can help refine diagnoses in the case of XP complex phenotypes. DNA repair plays a major role in protection of the eye from sunlight-induced damage.
Subject(s)
DNA Repair/physiology , DNA/radiation effects , Eye Diseases/diagnosis , Radiation Injuries/diagnosis , Sunlight/adverse effects , Xeroderma Pigmentosum/diagnosis , Adolescent , Adult , Child , Child, Preschool , Cockayne Syndrome/diagnosis , Cockayne Syndrome/etiology , Cockayne Syndrome/prevention & control , Eye Diseases/etiology , Eye Diseases/prevention & control , Female , Follow-Up Studies , Humans , Infant , Male , Middle Aged , Radiation Injuries/etiology , Radiation Injuries/prevention & control , Retrospective Studies , Trichothiodystrophy Syndromes/diagnosis , Trichothiodystrophy Syndromes/etiology , Trichothiodystrophy Syndromes/prevention & control , Ultraviolet Rays/adverse effects , Visual Acuity/physiology , Xeroderma Pigmentosum/etiology , Xeroderma Pigmentosum/prevention & control , Young AdultABSTRACT
Progeroid syndromes are a group of diseases characterized by signs of premature aging. These syndromes comprise diseases such as Werner syndrome, Bloom syndrome, Rothmund-Thomson syndrome, Hutchinson-Gilford syndrome, Fanconi anemia, and ataxia-telangiectasia, as well as xeroderma pigmentosum, trichothiodystrophy, and Cockayne syndrome. Clinical symptoms of premature aging are skin atrophy with loss of cutaneous elasticity, dysfunction of cutaneous appendices, degeneration of the central nervous system and an increased susceptibility for malignant tumors. Genetic defects in the repair of DNA damage can lead to progeroid syndromes, and it is becoming increasingly evident that direct DNA damage and indirect damage by highly reactive oxygen species play central roles in aging. The clinical signs of progeroid syndromes and the molecular aspects of UV (ultraviolet radiation)-induced oxidative stress in aging are discussed.Journal of Investigative Dermatology Symposium Proceedings (2009) 14, 8-14; doi:10.1038/jidsymp.2009.6.
Subject(s)
Cockayne Syndrome/etiology , DNA Damage , Ultraviolet Rays/adverse effects , Ataxia Telangiectasia/etiology , Bloom Syndrome/etiology , Cockayne Syndrome/genetics , Cockayne Syndrome/metabolism , DNA Repair , Fanconi Anemia/etiology , Female , Humans , Male , Models, Biological , Oxidative Stress/radiation effects , Progeria/etiology , Rothmund-Thomson Syndrome/etiology , Trichothiodystrophy Syndromes/etiology , Werner Syndrome/etiology , Xeroderma Pigmentosum/etiologyABSTRACT
Cockayne syndrome (CS) is a photosensitive, DNA repair disorder associated with progeria that is caused by a defect in the transcription-coupled repair subpathway of nucleotide excision repair (NER). Here, complete inactivation of NER in Csb(m/m)/Xpa(-/-) mutants causes a phenotype that reliably mimics the human progeroid CS syndrome. Newborn Csb(m/m)/Xpa(-/-) mice display attenuated growth, progressive neurological dysfunction, retinal degeneration, cachexia, kyphosis, and die before weaning. Mouse liver transcriptome analysis and several physiological endpoints revealed systemic suppression of the growth hormone/insulin-like growth factor 1 (GH/IGF1) somatotroph axis and oxidative metabolism, increased antioxidant responses, and hypoglycemia together with hepatic glycogen and fat accumulation. Broad genome-wide parallels between Csb(m/m)/Xpa(-/-) and naturally aged mouse liver transcriptomes suggested that these changes are intrinsic to natural ageing and the DNA repair-deficient mice. Importantly, wild-type mice exposed to a low dose of chronic genotoxic stress recapitulated this response, thereby pointing to a novel link between genome instability and the age-related decline of the somatotroph axis.
Subject(s)
Cockayne Syndrome/genetics , DNA Repair , Genome/genetics , Growth Hormone/genetics , Insulin-Like Growth Factor I/metabolism , Aging , Animals , Antioxidants/pharmacology , Cockayne Syndrome/etiology , DNA Repair Enzymes/genetics , DNA-Binding Proteins/genetics , Diethylhexyl Phthalate/pharmacology , Fatty Acids/biosynthesis , Glucose/metabolism , Insulin-Like Growth Factor I/genetics , Liver/metabolism , Male , Mice , Mice, Inbred C57BL , Mice, Knockout , Poly-ADP-Ribose Binding Proteins , Radiation, Ionizing , Somatotrophs/metabolism , Xeroderma Pigmentosum Group A Protein/geneticsABSTRACT
Researchers and clinicians interested in human diseases of DNA repair deficiency and premature aging gathered at the National Conference Center in Lansdowne, Virginia on 5-8 September 2006 to attend a workshop co-organized by Vilhelm Bohr (National Institute of Aging) and Kenneth Kraemer (National Cancer Institute). An important feature of this workshop was the participation of representatives from xeroderma pigmentosum (XP), Cockayne Syndrome (CS) and trichothiodystrophy (TTD) family support groups. Studies presented at the workshop described important new insights into the phenotypic complexity of XP, CS and TTD, renewed focus on the neurological manifestations of each of these diseases, as well as keen interest in the role of oxidative stress and mitochondrial dysfunction in neurodegenerative processes and normal and/or premature aging. This workshop report summarizes some of the presentations and outcomes of the workshop.
Subject(s)
Aging, Premature/etiology , DNA Repair-Deficiency Disorders/etiology , Aging , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , DNA Repair-Deficiency Disorders/epidemiology , DNA Repair-Deficiency Disorders/genetics , Hair Diseases/etiology , Hair Diseases/genetics , Humans , Oxidative Stress , Prevalence , Xeroderma Pigmentosum/etiology , Xeroderma Pigmentosum/geneticsABSTRACT
Progeroid syndromes (PSs) constitute a group of disorders characterized by clinical features mimicking physiological aging at an early age. In some of these syndromes, biological hallmarks of aging are also present, whereas in others, a link with physiological aging, if any, remains to be elucidated. These syndromes are clinically and genetically heterogeneous and most of them, including Werner syndrome and Hutchinson-Gilford progeria, are known as 'segmental aging syndromes', as they do not feature all aspects usually associated to physiological aging. However, all the characterized PSs enter in the field of rare monogenic disorders and several causative genes have been identified. These can be separated in subcategories corresponding to (i) genes encoding DNA repair factors, in particular, DNA helicases, and (ii) genes affecting the structure or post-translational maturation of lamin A, a major nuclear component. In addition, several animal models featuring premature aging have abnormal mitochondrial function or signal transduction between membrane receptors, nuclear regulatory proteins and mitochondria: no human pathological counterpart of these alterations has been found to date. In recent years, identification of mutations and their functional characterization have helped to unravel the cellular processes associated to segmental PSs. Recently, several studies allowed to establish a functional link between DNA repair and A-type lamins-associated syndromes, evidencing a relation between these syndromes, physiological aging and cancer. Here, we review recent data on molecular and cellular bases of PSs and discuss the mechanisms involved, with a special emphasis on lamin A-associated progeria and related disorders, for which therapeutic approaches have started to be developed.
Subject(s)
Progeria/genetics , Adult , Child , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , Cockayne Syndrome/physiopathology , DNA Repair/genetics , Humans , Lamin Type A/genetics , Liver X Receptors , Mitochondria/metabolism , Models, Biological , Models, Genetic , Orphan Nuclear Receptors , Progeria/etiology , Progeria/physiopathology , RecQ Helicases/genetics , Receptors, Cytoplasmic and Nuclear/genetics , Syndrome , Werner Syndrome/etiology , Werner Syndrome/genetics , Werner Syndrome/physiopathologyABSTRACT
The molecular mechanisms leading to human senescence are still not known mostly because of the complexity of the process. Different research approaches are used to study ageing including studies of monogenic segmental progeroid syndromes. None of the known progerias represents true precocious ageing. Some of them, including Werner (WS), Bloom (BS), and Rothmund-Thomson syndromes (RTS) as well as combined xeroderma pigmentosa-Cockayne syndrome (XP-CS) are characterised by features resembling precocious ageing and the increased risk of malignant disease. Such phenotypes result from the mutations of the genes encoding proteins involved in the maintenance of genomic integrity, in most cases DNA helicases. Defective functioning of these proteins affects DNA repair, recombination, replication and transcription. Other segmental progeroid syndromes, such as Hutchinson-Gilford progeria (HGPS) and Cockayne syndrome are not associated with an increased risk of cancer. In this paper we present the clinical and molecular features of selected progeroid syndromes and describe the potential implications of these data for studies of ageing and cancer development.
Subject(s)
Aging, Premature/genetics , Aging/genetics , Bloom Syndrome/etiology , Bloom Syndrome/genetics , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , Humans , Progeria/etiology , Progeria/genetics , Rothmund-Thomson Syndrome/etiology , Rothmund-Thomson Syndrome/genetics , Werner Syndrome/etiology , Werner Syndrome/geneticsABSTRACT
UV-sensitive syndrome (UVsS) is a rare autosomal recessive disorder characterized by photosensitivity and mild freckling but without neurological abnormalities or skin tumors. UVsS cells show UV hypersensitivity and defective transcription-coupled DNA repair of UV damage. It was suggested that UVsS does not belong to any complementation groups of known photosensitive disorders such as xeroderma pigmentosum and Cockayne syndrome (CS). To identify the gene responsible for UVsS, we performed a microcell-mediated chromosome transfer based on the functional complementation of UV hypersensitivity. We found that one of the UVsS cell lines, UVs1KO, acquired UV resistance when human chromosome 10 was transferred. Because the gene responsible for CS group B (CSB), which involves neurological abnormalities and photosensitivity as well as a defect in transcription-coupled DNA repair of UV damage, is located on chromosome 10, we sequenced the CSB gene from UVs1KO and detected a homozygous null mutation. Our results indicate that previous complementation analysis of UVs1KO was erroneous. This finding was surprising because a null mutation of the CSB gene would be expected to result in CS features such as severe developmental and neurological abnormalities. On the other hand, no mutation in the CSB cDNA and a normal amount of CSB protein was detected in Kps3, a UVsS cell line obtained from an unrelated patient, indicating genetic heterogeneity in UVsS. Possible explanations for the discrepancy in the genotype-phenotype relationship in UVs1KO are presented.
Subject(s)
Cockayne Syndrome/etiology , DNA Helicases/physiology , Base Sequence , Chromosomes, Human, Pair 10 , Cockayne Syndrome/genetics , DNA Helicases/genetics , DNA Primers , DNA Repair , DNA Repair Enzymes , Fluorescent Antibody Technique , Genetic Complementation Test , Humans , Poly-ADP-Ribose Binding Proteins , Reverse Transcriptase Polymerase Chain ReactionABSTRACT
Senile or age-related/dependent osteoporosis is caused by reduced bone formation, rather than increased bone resorption as in postmenopausal osteoporosis. Here we review genetically engineered mouse models with defects in osteoblastic proliferation or differentiation with focus on IGF signaling and stem cells. Model mice for human progeroid syndromes may provide useful tools for studying the pathogenesis of senile osteoporosis.
Subject(s)
Cockayne Syndrome/physiopathology , Osteoblasts/pathology , Osteogenesis/physiology , Osteoporosis/physiopathology , Aging/physiology , Aging, Premature/etiology , Animals , Cell Differentiation/physiology , Cockayne Syndrome/etiology , Disease Models, Animal , Female , Humans , Mice , Mice, Knockout , Osteoblasts/cytology , Osteoporosis/etiology , Signal Transduction , Somatomedins/metabolismABSTRACT
Cockayne syndrome (CS) is an inherited photosensitive neurodevelopmental disorder caused by a specific defect in the transcription-coupled repair (TCR) sub-pathway of NER. Remarkably, despite their DNA repair deficiency, CS patients do not develop skin cancer. Here, we present a mouse model for CS complementation group A. Like cells from CS-A patients, Csa-/- mouse embryonic fibroblasts (MEFs): (i) are ultraviolet (UV)-sensitive; (ii) show normal unscheduled DNA synthesis (indicating that the global genome repair sub-pathway is unaffected); (iii) fail to resume RNA synthesis after UV-exposure and (iv) are unable to remove cyclobutane pyrimidine dimers (CPD) photolesions from the transcribed strand of active genes. CS-A mice exhibit UV-sensitivity and pronounced age-dependent loss of retinal photoreceptor cells but otherwise fail to show the severe developmental and neurological abnormalities of the human syndrome. In contrast to human CS, Csa-/- animals develop skin tumors after chronic exposure to UV light, indicating that TCR in mice protects from UV-induced skin cancer development. Strikingly, inactivation of one Xpc allele (encoding a component of the damage recognition complex involved in the global genome repair sub-pathway) in Csa-/- mice resulted in a strongly enhanced UV-mediated skin cancer sensitivity, indicating that in a TC repair defective background, the Xpc gene product may be a rate-limiting factor in the removal of UV-induced DNA lesions.
Subject(s)
Cockayne Syndrome/genetics , DNA Repair/physiology , Neoplasms, Radiation-Induced/genetics , Proteins/genetics , Amino Acid Sequence , Animals , Cockayne Syndrome/etiology , Cockayne Syndrome/pathology , DNA Damage , DNA Repair/radiation effects , DNA Repair Enzymes , DNA-Binding Proteins , Disease Models, Animal , Female , Fibroblasts/radiation effects , Genetic Complementation Test , Genetic Predisposition to Disease , Humans , Male , Mice , Mice, Inbred C57BL , Mice, Knockout , Molecular Sequence Data , Neoplasms, Radiation-Induced/etiology , Neoplasms, Radiation-Induced/pathology , Proteins/metabolism , RNA/genetics , RNA/metabolism , Sequence Homology, Amino Acid , Skin/radiation effects , Skin Neoplasms/etiology , Transcription Factors , Ultraviolet RaysABSTRACT
Infection by adenovirus 12, transfection with the Ad12 E1B 55 kDa gene, or activation of p53 cause metaphase fragility of four loci (RNU1, PSU1, RNU2, and RN5S) each containing tandemly repeated genes for an abundant small RNA (U1, U2, and 5S RNA). We now show that loss of the Cockayne syndrome group B protein (CSB) or overexpression of the p53 carboxy-terminal domain induces fragility of the same loci; moreover, p53 interacts with CSB in vivo and in vitro. We propose that CSB functions as an elongation factor for transcription of structured RNAs, including some mRNAs. Activation of p53 would inhibit CSB, stalling transcription complexes and locally blocking chromatin condensation. Impaired transcription elongation may also explain the diverse clinical features of Cockayne syndrome.
Subject(s)
Chromosome Fragility , Cockayne Syndrome/genetics , DNA Helicases/genetics , RNA, Small Nuclear/genetics , Tumor Suppressor Protein p53/genetics , Acetylation , Adenoviridae/genetics , Cockayne Syndrome/etiology , DNA Helicases/metabolism , DNA Repair , DNA Repair Enzymes , Humans , Metaphase , Models, Genetic , Peptide Fragments/genetics , Phosphorylation , Poly-ADP-Ribose Binding Proteins , Protein Binding , Protein Processing, Post-Translational , Transcription, Genetic , Tumor Suppressor Protein p53/metabolismSubject(s)
Aging, Premature/physiopathology , Cellular Senescence/physiology , Progeria/physiopathology , Werner Syndrome/physiopathology , Adult , Aged , Aging, Premature/etiology , Aging, Premature/genetics , Ataxia Telangiectasia/etiology , Ataxia Telangiectasia/genetics , Ataxia Telangiectasia/physiopathology , Bloom Syndrome/etiology , Bloom Syndrome/genetics , Bloom Syndrome/physiopathology , Cellular Senescence/genetics , Child , Child, Preschool , Cockayne Syndrome/etiology , Cockayne Syndrome/genetics , Cockayne Syndrome/physiopathology , Female , Gene Expression/physiology , Humans , Infant , Male , Progeria/etiology , Progeria/genetics , Werner Syndrome/etiology , Werner Syndrome/geneticsABSTRACT
CAMFAK syndrome is an inherited disease characterized by congenital cataracts, microcephaly, failure to thrive, and kyphoscoliosis with onset in early infancy. Its pathogenesis has not been clearly defined. We report on a patient with this syndrome and present evidence that it is a neurologic disease characterized by peripheral and central demyelination similar to that seen in Cockayne syndrome.
