RÉSUMÉ
BACKGROUND: The U.K. 100,000 Genomes Project is in the process of investigating the role of genome sequencing in patients with undiagnosed rare diseases after usual care and the alignment of this research with health care implementation in the U.K. National Health Service. Other parts of this project focus on patients with cancer and infection. METHODS: We conducted a pilot study involving 4660 participants from 2183 families, among whom 161 disorders covering a broad spectrum of rare diseases were present. We collected data on clinical features with the use of Human Phenotype Ontology terms, undertook genome sequencing, applied automated variant prioritization on the basis of applied virtual gene panels and phenotypes, and identified novel pathogenic variants through research analysis. RESULTS: Diagnostic yields varied among family structures and were highest in family trios (both parents and a proband) and families with larger pedigrees. Diagnostic yields were much higher for disorders likely to have a monogenic cause (35%) than for disorders likely to have a complex cause (11%). Diagnostic yields for intellectual disability, hearing disorders, and vision disorders ranged from 40 to 55%. We made genetic diagnoses in 25% of the probands. A total of 14% of the diagnoses were made by means of the combination of research and automated approaches, which was critical for cases in which we found etiologic noncoding, structural, and mitochondrial genome variants and coding variants poorly covered by exome sequencing. Cohortwide burden testing across 57,000 genomes enabled the discovery of three new disease genes and 19 new associations. Of the genetic diagnoses that we made, 25% had immediate ramifications for clinical decision making for the patients or their relatives. CONCLUSIONS: Our pilot study of genome sequencing in a national health care system showed an increase in diagnostic yield across a range of rare diseases. (Funded by the National Institute for Health Research and others.).
Sujet(s)
Génome humain , Maladies rares/génétique , Adolescent , Adulte , Enfant , Enfant d'âge préscolaire , Caractéristiques familiales , Femelle , Variation génétique , Humains , Mâle , Adulte d'âge moyen , Projets pilotes , Réaction de polymérisation en chaîne , Maladies rares/diagnostic , Sensibilité et spécificité , Médecine d'État , Royaume-Uni , Séquençage du génome entier , Jeune adulteRÉSUMÉ
PURPOSE: Genome sequencing (GS) for diagnosis of rare genetic disease is being introduced into the clinic, but the complexity of the data poses challenges for developing pipelines with high diagnostic sensitivity. We evaluated the performance of the Genomics England 100,000 Genomes Project (100kGP) panel-based pipelines, using craniosynostosis as a test disease. METHODS: GS data from 114 probands with craniosynostosis and their relatives (314 samples), negative on routine genetic testing, were scrutinized by a specialized research team, and diagnoses compared with those made by 100kGP. RESULTS: Sixteen likely pathogenic/pathogenic variants were identified by 100kGP. Eighteen additional likely pathogenic/pathogenic variants were identified by the research team, indicating that for craniosynostosis, 100kGP panels had a diagnostic sensitivity of only 47%. Measures that could have augmented diagnoses were improved calling of existing panel genes (+18% sensitivity), review of updated panels (+12%), comprehensive analysis of de novo small variants (+29%), and copy-number/structural variants (+9%). Recent NHS England recommendations that partially incorporate these measures should achieve 85% overall sensitivity (+38%). CONCLUSION: GS identified likely pathogenic/pathogenic variants in 29.8% of previously undiagnosed patients with craniosynostosis. This demonstrates the value of research analysis and the importance of continually improving algorithms to maximize the potential of clinical GS.
Sujet(s)
Craniosynostoses , Dépistage génétique , Séquence nucléotidique , Cartographie chromosomique , Craniosynostoses/diagnostic , Craniosynostoses/génétique , Humains , Maladies rares/génétiqueRÉSUMÉ
Broad-based cognitive deficits are an enduring and disabling symptom for many patients with severe mental illness, and these impairments are inadequately addressed by current medications. While novel drug targets for schizophrenia and depression have emerged from recent large-scale genome-wide association studies (GWAS) of these psychiatric disorders, GWAS of general cognitive ability can suggest potential targets for nootropic drug repurposing. Here, we (1) meta-analyze results from two recent cognitive GWAS to further enhance power for locus discovery; (2) employ several complementary transcriptomic methods to identify genes in these loci that are credibly associated with cognition; and (3) further annotate the resulting genes using multiple chemoinformatic databases to identify "druggable" targets. Using our meta-analytic data set (N = 373,617), we identified 241 independent cognition-associated loci (29 novel), and 76 genes were identified by 2 or more methods of gene identification. Actin and chromatin binding gene sets were identified as novel pathways that could be targeted via drug repurposing. Leveraging our transcriptomic and chemoinformatic databases, we identified 16 putative genes targeted by existing drugs potentially available for cognitive repurposing.
Sujet(s)
Nootropiques , Schizophrénie , Cognition , Étude d'association pangénomique , Humains , Schizophrénie/traitement médicamenteux , Schizophrénie/génétique , TranscriptomeRÉSUMÉ
The extracellular matrix comprises a network of macromolecules such as collagens, proteoglycans and glycoproteins. VWA1 (von Willebrand factor A domain containing 1) encodes a component of the extracellular matrix that interacts with perlecan/collagen VI, appears to be involved in stabilizing extracellular matrix structures, and demonstrates high expression levels in tibial nerve. Vwa1-deficient mice manifest with abnormal peripheral nerve structure/function; however, VWA1 variants have not previously been associated with human disease. By interrogating the genome sequences of 74 180 individuals from the 100K Genomes Project in combination with international gene-matching efforts and targeted sequencing, we identified 17 individuals from 15 families with an autosomal-recessive, non-length dependent, hereditary motor neuropathy and rare biallelic variants in VWA1. A single disease-associated allele p.(G25Rfs*74), a 10-bp repeat expansion, was observed in 14/15 families and was homozygous in 10/15. Given an allele frequency in European populations approaching 1/1000, the seven unrelated homozygote individuals ascertained from the 100K Genomes Project represents a substantial enrichment above expected. Haplotype analysis identified a shared 220 kb region suggesting that this founder mutation arose >7000 years ago. A wide age-range of patients (6-83 years) helped delineate the clinical phenotype over time. The commonest disease presentation in the cohort was an early-onset (mean 2.0 ± 1.4 years) non-length-dependent axonal hereditary motor neuropathy, confirmed on electrophysiology, which will have to be differentiated from other predominantly or pure motor neuropathies and neuronopathies. Because of slow disease progression, ambulation was largely preserved. Neurophysiology, muscle histopathology, and muscle MRI findings typically revealed clear neurogenic changes with single isolated cases displaying additional myopathic process. We speculate that a few findings of myopathic changes might be secondary to chronic denervation rather than indicating an additional myopathic disease process. Duplex reverse transcription polymerase chain reaction and immunoblotting using patient fibroblasts revealed that the founder allele results in partial nonsense mediated decay and an absence of detectable protein. CRISPR and morpholino vwa1 modelling in zebrafish demonstrated reductions in motor neuron axonal growth, synaptic formation in the skeletal muscles and locomotive behaviour. In summary, we estimate that biallelic variants in VWA1 may be responsible for up to 1% of unexplained hereditary motor neuropathy cases in Europeans. The detailed clinical characterization provided here will facilitate targeted testing on suitable patient cohorts. This novel disease gene may have previously evaded detection because of high GC content, consequential low coverage and computational difficulties associated with robustly detecting repeat-expansions. Reviewing previously unsolved exomes using lower QC filters may generate further diagnoses.
Sujet(s)
Protéines de la matrice extracellulaire/génétique , Neuropathie héréditaire motrice et sensitive/génétique , Adulte , Sujet âgé , Animaux , Comportement animal/physiologie , Enfant , Femelle , Neuropathie héréditaire motrice et sensitive/anatomopathologie , Humains , Mâle , Adulte d'âge moyen , Muscles squelettiques/anatomopathologie , Mutation , Pedigree , Jeune adulte , Danio zébréRÉSUMÉ
OBJECTIVE: To identify genes underlying childhood onset psychosis. METHODS: Patients with onset of psychosis at age 13 or younger were identified from clinics across England, and they and their parents were exome sequenced and analysed for possible highly penetrant genetic contributors. RESULTS: We report two male childhood onset psychosis patients of different ancestries carrying hemizygous very rare possibly damaging missense variants (p.Arg846His and p.Pro145Ser) in the L1CAM gene. L1CAM is an X-linked Mendelian disease gene in which both missense and loss of function variants are associated with syndromic forms of intellectual disability and developmental disorder. CONCLUSIONS: This is the first study reporting a possible extension of the phenotype of L1CAM variant carriers to childhood onset psychosis. The family history and presence of other significant rare genetic variants in the patients suggest that there may be genetic interactions modulating the presentation.
Sujet(s)
Molécule d'adhérence cellulaire neurale L-1/génétique , Troubles psychotiques/génétique , Adolescent , Adulte , Enfant , Exome/génétique , Femelle , Hémizygote , Humains , Mâle , Mutation/génétique , Mutation faux-sens/génétique , Molécule d'adhérence cellulaire neurale L-1/métabolisme , Phénotype , /méthodesRÉSUMÉ
Susceptibility to schizophrenia is inversely correlated with general cognitive ability at both the phenotypic and the genetic level. Paradoxically, a modest but consistent positive genetic correlation has been reported between schizophrenia and educational attainment, despite the strong positive genetic correlation between cognitive ability and educational attainment. Here we leverage published genome-wide association studies (GWASs) in cognitive ability, education, and schizophrenia to parse biological mechanisms underlying these results. Association analysis based on subsets (ASSET), a pleiotropic meta-analytic technique, allowed jointly associated loci to be identified and characterized. Specifically, we identified subsets of variants associated in the expected ("concordant") direction across all three phenotypes (i.e., greater risk for schizophrenia, lower cognitive ability, and lower educational attainment); these were contrasted with variants that demonstrated the counterintuitive ("discordant") relationship between education and schizophrenia (i.e., greater risk for schizophrenia and higher educational attainment). ASSET analysis revealed 235 independent loci associated with cognitive ability, education, and/or schizophrenia at p < 5 × 10-8. Pleiotropic analysis successfully identified more than 100 loci that were not significant in the input GWASs. Many of these have been validated by larger, more recent single-phenotype GWASs. Leveraging the joint genetic correlations of cognitive ability, education, and schizophrenia, we were able to dissociate two distinct biological mechanisms-early neurodevelopmental pathways that characterize concordant allelic variation and adulthood synaptic pruning pathways-that were linked to the paradoxical positive genetic association between education and schizophrenia. Furthermore, genetic correlation analyses revealed that these mechanisms contribute not only to the etiopathogenesis of schizophrenia but also to the broader biological dimensions implicated in both general health outcomes and psychiatric illness.
Sujet(s)
Troubles de la cognition/physiopathologie , Cognition/physiologie , Niveau d'instruction , Troubles du développement neurologique/étiologie , Polymorphisme de nucléotide simple , Schizophrénie/physiopathologie , Transmission synaptique , Adulte , Prédisposition génétique à une maladie , Étude d'association pangénomique , Humains , Troubles du développement neurologique/anatomopathologieRÉSUMÉ
PURPOSE: Sixty to seventy-five percent of individuals with rare and undiagnosed phenotypes remain undiagnosed after exome sequencing (ES). With standard ES reanalysis resolving 10-15% of the ES negatives, further approaches are necessary to maximize diagnoses in these individuals. METHODS: In 38 ES negative patients an individualized genomic-phenotypic approach was employed utilizing (1) phenotyping; (2) reanalyses of FASTQ files, with innovative bioinformatics; (3) targeted molecular testing; (4) genome sequencing (GS); and (5) conferring of clinical diagnoses when pathognomonic clinical findings occurred. RESULTS: Certain and highly likely diagnoses were made in 18/38 (47%) individuals, including identifying two new developmental disorders. The majority of diagnoses (>70%) were due to our bioinformatics, phenotyping, and targeted testing identifying variants that were undetected or not prioritized on prior ES. GS diagnosed 3/18 individuals with structural variants not amenable to ES. Additionally, tentative diagnoses were made in 3 (8%), and in 5 individuals (13%) candidate genes were identified. Overall, diagnoses/potential leads were identified in 26/38 (68%). CONCLUSIONS: Our comprehensive approach to ES negatives maximizes the ES and clinical data for both diagnoses and candidate gene identification, without GS in the majority. This iterative approach is cost-effective and is pertinent to the current conundrum of ES negatives.
Sujet(s)
Incapacités de développement/diagnostic , Incapacités de développement/génétique , Exome/génétique , Prédisposition génétique à une maladie , Enfant , Incapacités de développement/épidémiologie , Femelle , Génomique , Humains , Mâle , Phénotype , Analyse de séquence d'ADN , /méthodes , Séquençage du génome entierRÉSUMÉ
Hill (Twin Research and Human Genetics, Vol. 21, 2018, 84-88) presented a critique of our recently published paper in Cell Reports entitled 'Large-Scale Cognitive GWAS Meta-Analysis Reveals Tissue-Specific Neural Expression and Potential Nootropic Drug Targets' (Lam et al., Cell Reports, Vol. 21, 2017, 2597-2613). Specifically, Hill offered several interrelated comments suggesting potential problems with our use of a new analytic method called Multi-Trait Analysis of GWAS (MTAG) (Turley et al., Nature Genetics, Vol. 50, 2018, 229-237). In this brief article, we respond to each of these concerns. Using empirical data, we conclude that our MTAG results do not suffer from 'inflation in the FDR [false discovery rate]', as suggested by Hill (Twin Research and Human Genetics, Vol. 21, 2018, 84-88), and are not 'more relevant to the genetic contributions to education than they are to the genetic contributions to intelligence'.
Sujet(s)
Étude d'association pangénomique , Nootropiques , Cognition , Prédisposition génétique à une maladie , Humains , Polymorphisme de nucléotide simpleRÉSUMÉ
The 17 genes of the T-box family are transcriptional regulators that are involved in all stages of embryonic development, including craniofacial, brain, heart, skeleton and immune system. Malformation syndromes have been linked to many of the T-box genes. For example, haploinsufficiency of TBX1 is responsible for many structural malformations in DiGeorge syndrome caused by a chromosome 22q11.2 deletion. We report four individuals with an overlapping spectrum of craniofacial dysmorphisms, cardiac anomalies, skeletal malformations, immune deficiency, endocrine abnormalities and developmental impairments, reminiscent of DiGeorge syndrome, who are heterozygotes for TBX2 variants. The p.R20Q variant is shared by three affected family members in an autosomal dominant manner; the fourth unrelated individual has a de novo p.R305H mutation. Bioinformatics analyses indicate that these variants are rare and predict them to be damaging. In vitro transcriptional assays in cultured cells show that both variants result in reduced transcriptional repressor activity of TBX2. We also show that the variants result in reduced protein levels of TBX2. Heterologous over-expression studies in Drosophila demonstrate that both p.R20Q and p.R305H function as partial loss-of-function alleles. Hence, these and other data suggest that TBX2 is a novel candidate gene for a new multisystem malformation disorder.
Sujet(s)
Incapacités de développement/génétique , Syndrome de DiGeorge/génétique , Prédisposition génétique à une maladie , Protéines à domaine boîte-T/génétique , Adulte , Animaux , Malformations cardiovasculaires/génétique , Malformations cardiovasculaires/physiopathologie , Système cardiovasculaire/physiopathologie , Enfant , Malformations crâniofaciales/génétique , Malformations crâniofaciales/physiopathologie , Incapacités de développement/physiopathologie , Syndrome de DiGeorge/physiopathologie , Modèles animaux de maladie humaine , Drosophila melanogaster , Femelle , Régulation de l'expression des gènes au cours du développement , Haploinsuffisance/génétique , Cardiopathies congénitales/génétique , Cardiopathies congénitales/physiopathologie , Humains , Souris , Pedigree , Grossesse , Jeune adulte , Danio zébréRÉSUMÉ
Here, we present a large (n = 107,207) genome-wide association study (GWAS) of general cognitive ability ("g"), further enhanced by combining results with a large-scale GWAS of educational attainment. We identified 70 independent genomic loci associated with general cognitive ability. Results showed significant enrichment for genes causing Mendelian disorders with an intellectual disability phenotype. Competitive pathway analysis implicated the biological processes of neurogenesis and synaptic regulation, as well as the gene targets of two pharmacologic agents: cinnarizine, a T-type calcium channel blocker, and LY97241, a potassium channel inhibitor. Transcriptome-wide and epigenome-wide analysis revealed that the implicated loci were enriched for genes expressed across all brain regions (most strongly in the cerebellum). Enrichment was exclusive to genes expressed in neurons but not oligodendrocytes or astrocytes. Finally, we report genetic correlations between cognitive ability and disparate phenotypes including psychiatric disorders, several autoimmune disorders, longevity, and maternal age at first birth.
Sujet(s)
Étude d'association pangénomique/méthodes , Nootropiques/pharmacologie , Céfotaxime/analogues et dérivés , Céfotaxime/pharmacologie , Cognition/effets des médicaments et des substances chimiques , Cognition/physiologie , Femelle , Locus génétiques/génétique , Prédisposition génétique à une maladie/génétique , Humains , Mâle , Polymorphisme de nucléotide simple/génétique , Synapses/effets des médicaments et des substances chimiques , Synapses/métabolismeSujet(s)
, Dépistage génétique , Exome , Études d'associations génétiques/méthodes , Études d'associations génétiques/normes , Prédisposition génétique à une maladie , Dépistage génétique/méthodes , Dépistage génétique/normes , Variation génétique , Humains , Reproductibilité des résultats , Sensibilité et spécificité , /méthodes , /normesRÉSUMÉ
Only a few years after its development, next-generation sequencing is rapidly becoming an essential part of clinical care for patients with serious neurological conditions, especially in the diagnosis of early-onset and severe presentations. Beyond this diagnostic role, there has been an explosion in definitive gene discovery in a range of neuropsychiatric diseases. This is providing new pointers to underlying disease biology and is beginning to outline a new framework for genetic stratification of neuropsychiatric disease, with clear relevance to both individual treatment optimization and clinical trial design. Here, we outline these developments and chart the expected impact on the treatment of neurological, neurodevelopmental, and psychiatric disease.
Solo unos pocos años después de su descubrimiento, la secuenciación de nueva generación se está constituyendo rápidamente en una parte esencial del cuidado clínico de los pacientes con patologías neurológicas serias, especialmente en el diagnóstico de cuadros de aparición precoz y grave. Más allá de este papel diagnóstico, ha constituido una explosión en el descubrimiento de genes definitivos en una amplia variedad de enfermedades neuropsiquiátricas. Esto está aportando nuevos indicadores para sustentar la biología de la enfermedad y se está empezando a perfilar un nuevo marco de referencia para la estratificación genética de las enfermedades neuropsiquiátricas, con especial relevancia tanto en la optimización del tratamiento individual como en el diseño de ensayos clínicos. En este artículo se resumen estos desarrollos y se proyecta el impacto esperado en el tratamiento de enfermedades neurológicas, del neurodesarrollo y psiquiátricas.
Quelques années seulement après son développement, la nouvelle génération de séquençage est rapidement devenue une part essentielle des traitements pour les patients atteints de maladies neurologiques graves, surtout dans le diagnostic des tableaux sévères et d'installation précoce. Au-delà de ce rôle diagnostique, de très nombreux gènes ont été formellement impliqués dans plusieurs maladies neuropsychiatriques. L'explosion de ces découvertes a fourni de nouvelles indications sur les mécanismes sous-tendant ces maladies et a permis d'établir une ébauche de leur stratification génétique, ce qui est très utile à la fois pour optimiser les traitements individuels et pour planifier les études cliniques. Dans cet article, nous soulignons ces évolutions et retraçons l'impact attendu sur le traitement de la maladie neurologique, neurodéveloppementale et psychiatrique.
Sujet(s)
Génomique , Neuropsychiatrie , Médecine de précision , Diagnostic , Études d'associations génétiques , Génétique , Humains ,RÉSUMÉ
The ASXL genes (ASXL1, ASXL2, and ASXL3) participate in body patterning during embryogenesis and encode proteins involved in epigenetic regulation and assembly of transcription factors to specific genomic loci. Germline de novo truncating variants in ASXL1 and ASXL3 have been respectively implicated in causing Bohring-Opitz and Bainbridge-Ropers syndromes, which result in overlapping features of severe intellectual disability and dysmorphic features. ASXL2 has not yet been associated with a human Mendelian disorder. In this study, we performed whole-exome sequencing in six unrelated probands with developmental delay, macrocephaly, and dysmorphic features. All six had de novo truncating variants in ASXL2. A careful review enabled the recognition of a specific phenotype consisting of macrocephaly, prominent eyes, arched eyebrows, hypertelorism, a glabellar nevus flammeus, neonatal feeding difficulties, hypotonia, and developmental disabilities. Although overlapping features with Bohring-Opitz and Bainbridge-Ropers syndromes exist, features that distinguish the ASXL2-associated condition from ASXL1- and ASXL3-related disorders are macrocephaly, absence of growth retardation, and more variability in the degree of intellectual disabilities. We were also able to demonstrate with mRNA studies that these variants are likely to exert a dominant-negative effect, given that both alleles are expressed in blood and the mutated ASXL2 transcripts escape nonsense-mediated decay. In conclusion, de novo truncating variants in ASXL2 underlie a neurodevelopmental syndrome with a clinically recognizable phenotype. This report expands the germline disorders that are linked to the ASXL genes.
Sujet(s)
Phénotype , Protéines de répression/génétique , Enfant , Enfant d'âge préscolaire , Incapacités de développement/génétique , Exome/génétique , Sourcils/malformations , Humains , Hypertélorisme/génétique , Nourrisson , Nouveau-né , Mâle , Mégalencéphalie/génétique , Hypotonie musculaire/génétique , ARN messager/métabolisme , SyndromeRÉSUMÉ
PURPOSE: Despite the recognized clinical value of exome-based diagnostics, methods for comprehensive genomic interpretation remain immature. Diagnoses are based on known or presumed pathogenic variants in genes already associated with a similar phenotype. Here, we extend this paradigm by evaluating novel bioinformatics approaches to aid identification of new gene-disease associations. METHODS: We analyzed 119 trios to identify both diagnostic genotypes in known genes and candidate genotypes in novel genes. We considered qualifying genotypes based on their population frequency and in silico predicted effects we also characterized the patterns of genotypes enriched among this collection of patients. RESULTS: We obtained a genetic diagnosis for 29 (24%) of our patients. We showed that patients carried an excess of damaging de novo mutations in intolerant genes, particularly those shown to be essential in mice (P = 3.4 × 10(-8)). This enrichment is only partially explained by mutations found in known disease-causing genes. CONCLUSION: This work indicates that the application of appropriate bioinformatics analyses to clinical sequence data can also help implicate novel disease genes and suggest expanded phenotypes for known disease genes. These analyses further suggest that some cases resolved by whole-exome sequencing will have direct therapeutic implications.
Sujet(s)
Exome , Maladies génétiques congénitales/diagnostic , Maladies génétiques congénitales/génétique , Séquençage nucléotidique à haut débit , Biologie informatique/méthodes , Femelle , Études d'associations génétiques , Génomique/méthodes , Génotype , Humains , Mâle , Mutation , PhénotypeRÉSUMÉ
The new GWAS from the Schizophrenia Working Group of the Psychiatric Genomics Consortium (2014) clearly validates a genetic approach to understanding schizophrenia. The challenge now remains to track down the contributing genes and to develop appropriate models to elucidate the biological effects of the contributing variants.
Sujet(s)
Locus génétiques , Prédisposition génétique à une maladie/génétique , Étude d'association pangénomique , Schizophrénie/génétique , HumainsRÉSUMÉ
Schizophrenia continues to pose a serious challenge to neuroscience and psychiatry as well as to health care systems and to the patients and families who suffer this terrible and disabling illness. Major developments in the past few months in both genetics and drug development oblige us to consider novel drug discovery tactics for future schizophrenia research. Here we review what we consider to be the key issues and some suggested solutions.
Sujet(s)
Neuroleptiques/usage thérapeutique , Recherche biomédicale , Schizophrénie/traitement médicamenteux , Schizophrénie/génétique , Animaux , Recherche biomédicale/tendances , HumainsRÉSUMÉ
Recent human genetic studies have consistently shown that mutations in the same gene or same genomic region can increase the risk of a broad range of complex neuropsychiatric disorders. Despite the steadily increasing number of examples of such nonspecific effects on risk, the underlying biological causes remain mysterious. Here we investigate the phenomenon of such nonspecific risk by identifying Mendelian disease genes that are associated with multiple diseases and explore what is known about the underlying mechanisms in these more 'simple' examples. Our analyses make clear that there are a variety of mechanisms at work, emphasizing how challenging it will be to elucidate the causes of nonspecific risk in complex disease. Ultimately, we conclude that functional approaches will be critical for explaining the causes of nonspecific risk factors discovered by human genetic studies of neuropsychiatric disorders.
Sujet(s)
Prédisposition génétique à une maladie/génétique , Analyse de randomisation mendélienne/méthodes , Troubles mentaux/génétique , Mutation/génétique , Animaux , Humains , Analyse de randomisation mendélienne/tendances , Troubles mentaux/diagnosticRÉSUMÉ
PURPOSE: The endoplasmic reticulum-associated degradation pathway is responsible for the translocation of misfolded proteins across the endoplasmic reticulum membrane into the cytosol for subsequent degradation by the proteasome. To define the phenotype associated with a novel inherited disorder of cytosolic endoplasmic reticulum-associated degradation pathway dysfunction, we studied a series of eight patients with deficiency of N-glycanase 1. METHODS: Whole-genome, whole-exome, or standard Sanger sequencing techniques were employed. Retrospective chart reviews were performed in order to obtain clinical data. RESULTS: All patients had global developmental delay, a movement disorder, and hypotonia. Other common findings included hypolacrima or alacrima (7/8), elevated liver transaminases (6/7), microcephaly (6/8), diminished reflexes (6/8), hepatocyte cytoplasmic storage material or vacuolization (5/6), and seizures (4/8). The nonsense mutation c.1201A>T (p.R401X) was the most common deleterious allele. CONCLUSION: NGLY1 deficiency is a novel autosomal recessive disorder of the endoplasmic reticulum-associated degradation pathway associated with neurological dysfunction, abnormal tear production, and liver disease. The majority of patients detected to date carry a specific nonsense mutation that appears to be associated with severe disease. The phenotypic spectrum is likely to enlarge as cases with a broader range of mutations are detected.
Sujet(s)
Malformations multiples/génétique , Dégradation associée au réticulum endoplasmique/génétique , Mutation , Peptide-N4-(N-acetyl-beta-glucosaminyl) asparagine amidase/génétique , Transduction du signal/génétique , Malformations multiples/enzymologie , Malformations multiples/anatomopathologie , Adolescent , Enfant d'âge préscolaire , Incapacités de développement/anatomopathologie , Exome/génétique , Santé de la famille , Issue fatale , Femelle , Étude d'association pangénomique/méthodes , Humains , Nourrisson , Mâle , Microcéphalie/anatomopathologie , Troubles de la motricité/anatomopathologie , Hypotonie musculaire/anatomopathologie , Pedigree , Peptide-N4-(N-acetyl-beta-glucosaminyl) asparagine amidase/déficit , Études rétrospectives , Crises épileptiques/anatomopathologie , Analyse de séquence d'ADN/méthodes , Jeune adulteRÉSUMÉ
PURPOSE: The purpose of this study was to assess the diagnostic yield of the traditional, comprehensive clinical evaluation and targeted genetic testing, within a general genetics clinic. These data are critically needed to develop clinically and economically grounded diagnostic algorithms that consider presenting phenotype, traditional genetics testing, and the emerging role of next-generation sequencing (whole-exome/genome sequencing). METHODS: We retrospectively analyzed a cohort of 500 unselected consecutive patients who received traditional genetic diagnostic evaluations at a tertiary medical center. We calculated the diagnosis rate, number of visits to diagnosis, genetic tests, and the cost of testing. RESULTS: Thirty-nine patients were determined to not have a genetic disorder; 212 of the remaining 461 (46%) received a genetic diagnosis, and 72% of these were diagnosed on the first visit. The cost per subsequent successful genetic diagnosis was estimated at $25,000. CONCLUSION: Almost half of the patients were diagnosed using the traditional approach, most at the initial visit. For those remaining undiagnosed, next-generation sequencing may be clinically and economically beneficial. Estimating a 50% success rate for next-generation sequencing in undiagnosed genetic disorders, its application after the first clinical visit could result in a higher rate of genetic diagnosis at a considerable cost savings per successful diagnosis.
