ABSTRACT
Wiedemann-Rautenstrauch syndrome (WRS; MIM# 264090) is a rare neonatal progeroid disorder resulting from biallelic pathogenic variants in the POLR3A. It is an autosomal recessive condition characterized by growth retardation, lipoatrophy, a distinctive face, sparse scalp hair, and dental anomalies. Till date, 19 families are reported with WRS due to variants in POLR3A. Here, we describe an 18 months old male child with biallelic c.2005C>T p.(Arg669Ter) and c.1771-7C>G variant in heterozygous state identified by exome sequencing in POLR3A leading to WRS phenotype. The variant c.1771-7C>G was earlier found to be associated with hereditary spastic ataxia. We emphasize on the phenotype in an Indian patient with WRS.
Subject(s)
Fetal Growth Retardation/genetics , Genetic Predisposition to Disease , Progeria/genetics , RNA Polymerase III/genetics , Alleles , Female , Fetal Growth Retardation/mortality , Fetal Growth Retardation/pathology , Humans , Infant , Infant Mortality , Infant, Newborn , Male , Mutation/genetics , Phenotype , Progeria/mortality , Progeria/pathology , Exome SequencingABSTRACT
Mutations in lamin A (LMNA) are responsible for a variety of human dystrophic and metabolic diseases. Here, we created a mouse model in which progerin, the lamin A mutant protein that causes Hutchinson-Gilford progeria syndrome (HGPS), can be inducibly overexpressed. Muscle-specific overexpression of progerin was sufficient to induce muscular dystrophy and alter whole-body energy expenditure, leading to premature death. Intriguingly, sarcolipin (Sln), an endoplasmic reticulum (ER)-associated protein involved in heat production, is upregulated in progerin-expressing and Lmna knockout (Lmna-/- ) skeletal muscle. The depletion of Sln accelerated the early death of Lmna-/- mice. An examination at the molecular level revealed that progerin recruits Sln and Calnexin to the nuclear periphery. Furthermore, progerin-expressing myoblasts presented enhanced store-operated Ca2+ entry, as well as increased co-localization of STIM1 and ORAI1. These findings suggest that progerin dysregulates calcium homeostasis through an interaction with a subset of ER-associated proteins, resulting in thermogenic and metabolic abnormalities.
Subject(s)
Calcium/metabolism , Lamin Type A/metabolism , Muscular Dystrophies/metabolism , Progeria/metabolism , Thermogenesis/genetics , Animals , Calnexin/metabolism , Cell Nucleus/metabolism , Disease Models, Animal , Endoplasmic Reticulum/metabolism , Endoplasmic Reticulum/ultrastructure , Endoplasmic Reticulum Stress/genetics , Lamin Type A/genetics , Mice , Mice, Knockout , Microscopy, Electron, Transmission , Muscle Proteins/metabolism , Muscle, Skeletal/metabolism , Muscle, Skeletal/physiopathology , Muscular Dystrophies/physiopathology , Mutation , Myoblasts/metabolism , Myoblasts/pathology , ORAI1 Protein/metabolism , Progeria/genetics , Progeria/mortality , Progeria/physiopathology , Proteolipids/metabolism , Stromal Interaction Molecule 1/metabolism , Up-RegulationABSTRACT
Hutchinson-Gilford progeria syndrome (HGPS) is a rare genetic disorder caused by progerin, a mutant lamin A variant. HGPS patients display accelerated aging and die prematurely, typically from atherosclerosis complications. Recently, we demonstrated that progerin-driven vascular smooth muscle cell (VSMC) loss accelerates atherosclerosis leading to premature death in apolipoprotein E-deficient mice. However, the molecular mechanism underlying this process remains unknown. Using a transcriptomic approach, we identify here endoplasmic reticulum stress (ER) and the unfolded protein responses as drivers of VSMC death in two mouse models of HGPS exhibiting ubiquitous and VSMC-specific progerin expression. This stress pathway was also activated in HGPS patient-derived cells. Targeting ER stress response with a chemical chaperone delayed medial VSMC loss and inhibited atherosclerosis in both progeria models, and extended lifespan in the VSMC-specific model. Our results identify a mechanism underlying cardiovascular disease in HGPS that could be targeted in patients. Moreover, these findings may help to understand other vascular diseases associated with VSMC death, and provide insight into aging-dependent vascular damage related to accumulation of unprocessed toxic forms of lamin A.
Subject(s)
Endoplasmic Reticulum Stress , Lamin Type A/metabolism , Animals , Aorta/metabolism , Aorta/pathology , Apoptosis/drug effects , Atherosclerosis/etiology , Disease Models, Animal , Endoplasmic Reticulum Stress/drug effects , Gene Expression/drug effects , HSP90 Heat-Shock Proteins/genetics , HSP90 Heat-Shock Proteins/metabolism , Kaplan-Meier Estimate , Longevity/drug effects , Male , Mice , Mice, Inbred C57BL , Mice, Transgenic , Muscle, Smooth, Vascular/cytology , Muscle, Smooth, Vascular/metabolism , Progeria/drug therapy , Progeria/mortality , Progeria/pathology , Protein Disulfide-Isomerases/genetics , Protein Disulfide-Isomerases/metabolism , Taurochenodeoxycholic Acid/pharmacology , Taurochenodeoxycholic Acid/therapeutic use , Unfolded Protein Response/drug effectsABSTRACT
Importance: Hutchinson-Gilford progeria syndrome (HGPS) is an extremely rare fatal premature aging disease. There is no approved treatment. Objective: To evaluate the association of monotherapy using the protein farnesyltransferase inhibitor lonafarnib with mortality rate in children with HGPS. Design, Setting, and Participants: Cohort study comparing contemporaneous (birth date ≥1991) untreated patients with HGPS matched with treated patients by age, sex, and continent of residency using conditional Cox proportional hazards regression. Treatment cohorts included patients from 2 single-group, single-site clinical trials (ProLon1 [n = 27; completed] and ProLon2 [n = 36; ongoing]). Untreated patients originated from a separate natural history study (n = 103). The cutoff date for patient follow-up was January 1, 2018. Exposure: Treated patients received oral lonafarnib (150 mg/m2) twice daily. Untreated patients received no clinical trial medications. Main Outcomes and Measures: The primary outcome was mortality. The primary analysis compared treated patients from the first lonafarnib trial with matched untreated patients. A secondary analysis compared the combined cohorts from both lonafarnib trials with matched untreated patients. Results: Among untreated and treated patients (n = 258) from 6 continents, 123 (47.7%) were female; 141 (54.7%) had a known genotype, of which 125 (88.7%) were classic (c.1824C>T in LMNA). When identified (n = 73), the primary cause of death was heart failure (79.4%). The median treatment duration was 2.2 years. Median age at start of follow-up was 8.4 (interquartile range [IQR], 4.8-9.5) years in the first trial cohort and 6.5 (IQR, 3.7-9.0) years in the combined cohort. There was 1 death (3.7%) among 27 patients in the first trial group and there were 9 deaths (33.3%) among 27 patients in the matched untreated group. Treatment was associated with a lower mortality rate (hazard ratio, 0.12; 95% CI, 0.01-0.93; P = .04). In the combined cohort, there were 4 deaths (6.3%) among 63 patients in the treated group and 17 deaths (27.0%) among 63 patients in the matched untreated group (hazard ratio, 0.23; 95% CI, 0.06-0.90; P = .04). Conclusions and Relevance: Among patients with HGPS, lonafarnib monotherapy, compared with no treatment, was associated with a lower mortality rate after 2.2 years of follow-up. Study interpretation is limited by its observational design.
Subject(s)
Enzyme Inhibitors/therapeutic use , Phosphotransferases (Phosphate Group Acceptor)/antagonists & inhibitors , Piperidines/therapeutic use , Progeria/drug therapy , Pyridines/therapeutic use , Adolescent , Adult , Cause of Death , Child , Cohort Studies , Female , Humans , Kaplan-Meier Estimate , Lamin Type A/biosynthesis , Lamin Type A/metabolism , Male , Progeria/genetics , Progeria/mortality , Protein Processing, Post-Translational , Young AdultABSTRACT
Hutchinson-Gilford Progeria Syndrome (HGPS) is a rare, but devastating genetic disease characterized by segmental premature aging, with cardiovascular disease being the main cause of death. Cells from HGPS patients accumulate progerin, a permanently farnesylated, toxic form of Lamin A, disrupting the nuclear shape and chromatin organization, leading to DNA-damage accumulation and senescence. Therapeutic approaches targeting farnesylation or aiming to reduce progerin levels have provided only partial health improvements. Recently, we identified Remodelin, a small-molecule agent that leads to amelioration of HGPS cellular defects through inhibition of the enzyme N-acetyltransferase 10 (NAT10). Here, we show the preclinical data demonstrating that targeting NAT10 in vivo, either via chemical inhibition or genetic depletion, significantly enhances the healthspan in a Lmna G609G HGPS mouse model. Collectively, the data provided here highlights NAT10 as a potential therapeutic target for HGPS.
Subject(s)
Aging, Premature/drug therapy , Genomic Instability/drug effects , Hydrazones/pharmacology , N-Terminal Acetyltransferase A/antagonists & inhibitors , Progeria/drug therapy , Thiazoles/pharmacology , Aging, Premature/genetics , Aging, Premature/mortality , Aging, Premature/pathology , Animals , DNA Damage/drug effects , DNA Damage/genetics , Disease Models, Animal , Female , Genomic Instability/genetics , Humans , Hydrazones/therapeutic use , Kaplan-Meier Estimate , Lamin Type A/genetics , Male , Mice , Mice, Inbred C57BL , Mice, Knockout , N-Terminal Acetyltransferase A/genetics , N-Terminal Acetyltransferase A/metabolism , N-Terminal Acetyltransferases , Progeria/genetics , Progeria/mortality , Progeria/pathology , Thiazoles/therapeutic useABSTRACT
BACKGROUND: Hutchinson-Gilford progeria syndrome is an ultrarare segmental premature aging disease resulting in early death from heart attack or stroke. There is no approved treatment, but starting in 2007, several recent single-arm clinical trials administered inhibitors of protein farnesylation aimed at reducing toxicity of the disease-producing protein progerin. No study assessed whether treatments influence patient survival. The key elements necessary for this analysis are a robust natural history of survival and comparison with a sufficiently large patient population that has been treated for a sufficient time period with disease-targeting medications. METHODS AND RESULTS: We generated Kaplan-Meier survival analyses for the largest untreated Hutchinson-Gilford progeria syndrome cohort to date. Mean survival was 14.6 years. Comparing survival for treated versus age- and sex-matched untreated cohorts, hazard ratio was 0.13 (95% confidence interval, 0.04-0.37; P<0.001) with median follow-up of 5.3 years from time of treatment initiation. There were 21 of 43 deaths in untreated versus 5 of 43 deaths among treated subjects. Treatment increased mean survival by 1.6 years. CONCLUSIONS: This study provides a robust untreated disease survival profile that can be used for comparisons now and in the future to assess changes in survival with treatments for Hutchinson-Gilford progeria syndrome. The current comparisons estimating increased survival with protein farnesylation inhibitors provide the first evidence of treatments influencing survival for this fatal disease. CLINICAL TRIAL REGISTRATION URL: http://www.clinicaltrials.gov. Unique Indentifiers: NCT00425607, NCT00879034, and NCT00916747.
Subject(s)
Diphosphonates/therapeutic use , Imidazoles/therapeutic use , Nuclear Proteins/metabolism , Piperidines/therapeutic use , Pravastatin/therapeutic use , Progeria/drug therapy , Protein Precursors/metabolism , Protein Prenylation/drug effects , Pyridines/therapeutic use , Adolescent , Adult , Alkyl and Aryl Transferases/antagonists & inhibitors , Atherosclerosis/etiology , Atherosclerosis/genetics , Atherosclerosis/prevention & control , Cause of Death , Child , Child, Preschool , Clinical Trials as Topic/statistics & numerical data , Cohort Studies , Dimethylallyltranstransferase/antagonists & inhibitors , Diphosphonates/administration & dosage , Diphosphonates/pharmacology , Drug Therapy, Combination , Female , Genes, Dominant , Genotype , Humans , Hydroxymethylglutaryl-CoA Reductase Inhibitors/administration & dosage , Hydroxymethylglutaryl-CoA Reductase Inhibitors/pharmacology , Hydroxymethylglutaryl-CoA Reductase Inhibitors/therapeutic use , Imidazoles/administration & dosage , Imidazoles/pharmacology , Kaplan-Meier Estimate , Lamin Type A , Male , Multicenter Studies as Topic/statistics & numerical data , Nuclear Proteins/deficiency , Nuclear Proteins/genetics , Piperidines/administration & dosage , Piperidines/pharmacology , Pravastatin/administration & dosage , Pravastatin/pharmacology , Progeria/complications , Progeria/mortality , Proportional Hazards Models , Protein Precursors/deficiency , Protein Precursors/genetics , Pyridines/administration & dosage , Pyridines/pharmacology , Treatment Outcome , Young Adult , Zoledronic AcidABSTRACT
We report on a Palestinian family with three affected individuals exhibiting progeroid syndrome characterized by intrauterine growth retardation, a progeroid appearance, failure to thrive, short stature, and hypotonia. The progeroid features were evident at birth. All the affected members of this family have survived beyond the neonatal period and one of them is currently a 27-year-old adult. As parental consanguinity suggested an autosomal recessive mode of inheritance, we employed homozygosity mapping using single nucleotide polymorphism arrays followed by next generation whole exome sequencing to identify the disease-causing gene. We were able to identify a single block of homozygosity shared between all the affected members of the studied family spanning 2.3 Mb on chromosome 19p13.3p13.2. However, Sanger sequencing of known genes and whole exome sequencing of the three affected sibs did not reveal a convincing causal mutation. These findings are anticipated to open the way for the identification of the molecular causes underlying this syndrome.
Subject(s)
Chromosomes, Human, Pair 19/genetics , Exome , Family , Fetal Growth Retardation/genetics , Homozygote , Pedigree , Progeria/genetics , Adult , Chromosome Mapping/methods , DNA Mutational Analysis , Female , Fetal Growth Retardation/mortality , Follow-Up Studies , Humans , Male , Progeria/mortality , Survival RateABSTRACT
Hutchinson-Gilford progeria syndrome (HGPS), a rare disease that results in what appears to be premature aging, is caused by the production of a mutant form of prelamin A known as progerin. Progerin retains a farnesyl lipid anchor at its carboxyl terminus, a modification that is thought to be important in disease pathogenesis. Inhibition of protein farnesylation improves the hallmark nuclear shape abnormalities in HGPS cells and ameliorates disease phenotypes in mice harboring a knockin HGPS mutation (LmnaHG/+). The amelioration of disease, however, is incomplete, leading us to hypothesize that nonfarnesylated progerin also might be capable of eliciting disease. To test this hypothesis, we created knockin mice expressing nonfarnesylated progerin (LmnanHG/+). LmnanHG/+ mice developed the same disease phenotypes observed in LmnaHG/+ mice, although the phenotypes were milder, and mouse embryonic fibroblasts (MEFs) derived from these mice contained fewer misshapen nuclei. The steady-state levels of progerin in LmnanHG/+ MEFs and tissues were lower, suggesting a possible explanation for the milder phenotypes. These data support the concept that inhibition of protein farnesylation in progeria could be therapeutically useful but also suggest that this approach may be limited, as progerin elicits disease phenotypes whether or not it is farnesylated.
Subject(s)
Nuclear Proteins/metabolism , Prenylation , Progeria/physiopathology , Protein Precursors/metabolism , Animals , Blotting, Western , Body Weight , Bone and Bones/abnormalities , Cell Nucleus Shape , Disease Models, Animal , Female , Fibroblasts/cytology , Fibroblasts/metabolism , Gene Expression Regulation , Lamin Type A , Liver/metabolism , Male , Mice , Mice, Inbred C57BL , Mice, Transgenic , Nuclear Proteins/genetics , Phenotype , Point Mutation , Progeria/mortality , Protein Precursors/genetics , Survival AnalysisABSTRACT
Schizophrenia is associated with a number of anatomical and physiological abnormalities outside of the brain, as well as with a decrease in average life span estimated at 20% in the United States. Some studies suggest that this increased mortality is not entirely due to associated causes such as suicide and the use of psychotropic medications. In this article, in order to focus greater attention on the increased mortality associated with schizophrenia, we present a special case of the hypothesis that physiological abnormalities associated with schizophrenia make a contribution to the increased mortality of schizophrenia: specifically, the hypothesis that schizophrenia is a syndrome of accelerated aging. Evidence consistent with this hypothesis comes from several areas. The biological plausibility of the hypothesis is supported by the existence of established syndromes of accelerated aging and by the sharing of risk factors between schizophrenia and other age-related conditions. We propose methods for testing the hypothesis.
Subject(s)
Progeria/diagnosis , Schizophrenia/diagnosis , Alzheimer Disease/diagnosis , Alzheimer Disease/mortality , Alzheimer Disease/physiopathology , Atrophy , Blood Pressure/physiology , Brain/pathology , Brain/physiopathology , Cognition Disorders/diagnosis , Cognition Disorders/mortality , Cognition Disorders/physiopathology , Female , Humans , Infant, Low Birth Weight , Infant, Newborn , Life Expectancy , Male , Mental Status Schedule , Paternal Age , Pregnancy , Prenatal Exposure Delayed Effects/physiopathology , Progeria/mortality , Progeria/physiopathology , Risk Factors , Schizophrenia/mortality , Schizophrenia/physiopathologyABSTRACT
Progeria, also known as the Hutchinson-Gilford syndrome, is an extremely rare condition that was initially reported by Johnathan Hutchinson in 1886 and further described by Hastings Gilford in 1904. Transmission is most likely from a sporadic autosomal dominant mutation. Clinical manifestations are evident by the first or second year of life and include the physical characteristics usually associated with the elderly. Mentally, patients are alert and attentive with normal intelligence and emotions. Histopathologic changes occur primarily in the skin, bone, and cardiovascular tissues, while other organs appear to be unaffected. Laboratory findings are unremarkable, with the exception of an increased urinary excretion of hyaluronic acid. The diagnosis rests on the clinical presentation; at present, no treatment has been proved to be effective. Death results from cardiovascular abnormalities in the majority of cases and usually occurs between the ages of 10 and 15 years. Current research suggests an underlying defect of hyaluronic acid that may possibly account for the entire process.
Subject(s)
Progeria , Aging/physiology , Diagnosis, Differential , Female , Humans , Hyaluronic Acid/metabolism , Male , Progeria/diagnosis , Progeria/genetics , Progeria/mortality , Progeria/pathology , Prognosis , ResearchABSTRACT
The author gives an overview on health damages from former prisoners in concentration camps more then 30 years after the deliverance.
