ABSTRACT
As a result of exome-based sequencing work performed by the DDD study, de novo variants in CNOT3 have emerged as a newly recognised cause of a developmental disorder. This paper describes molecular and clinical details of 16 probands with developmental disorders and de novo CNOT3 variants. It is the first such description of the developmental phenotype associated with CNOT3 variants. Eight of these cases were discovered as part of the DDD study, while the other eight were found as a result of large-scale sequencing work performed by other groups. A highly specific phenotype was not recognised in these 16 cases. The most consistent phenotypic features seen in subjects with de novo variants in CNOT3 were hypotonia, relatively small stature, developmental delay, behavioural problems and intellectual disability. There is no easily recognisable facial phenotype, but some common dysmorphic features such as anteverted nares, thin upper lip and low set eyebrows were shared among some of the probands. Haploinsufficiency appears to be the most likely mechanism of action, with eight cases found to have protein-truncating variants. Of the other eight cases (all missense variants), three share an amino acid substitution at the same position which may therefore represent an important functional domain.
Subject(s)
Genetic Predisposition to Disease/genetics , Genetic Variation , Neurodevelopmental Disorders/genetics , Transcription Factors/genetics , Amino Acid Sequence , Behavior , Developmental Disabilities/genetics , Exome , Female , Genetic Association Studies , Humans , Intellectual Disability/genetics , Ireland , Learning , Male , Muscle Hypotonia/genetics , Musculoskeletal Abnormalities/genetics , Mutation, Missense , Neurodevelopmental Disorders/physiopathology , Phenotype , Sequence Alignment , United Kingdom , Exome SequencingABSTRACT
Perrault syndrome is a rare autosomal recessive disorder characterized by sensorineural hearing loss (SNHL) in both sexes and primary ovarian insufficiency in 46, XX karyotype females. Biallelic variants in five genes are reported to be causative: HSD17B4, HARS2, LARS2, CLPP and C10orf2. Here we present eight families affected by Perrault syndrome. In five families we identified novel or previously reported variants in HSD17B4, LARS2, CLPP and C10orf2. The proband from each family was whole exome sequenced and variants confirmed by Sanger sequencing. A female was compound heterozygous for a known, p.(Gly16Ser) and novel, p.(Val82Phe) variant in D-bifunctional protein (HSD17B4). A family was homozygous for mitochondrial leucyl aminocyl tRNA synthetase (mtLeuRS) (LARS2) p.(Thr522Asn), previously associated with Perrault syndrome. A further family was compound heterozygous for mtLeuRS, p.(Thr522Asn) and a novel variant, p.(Met117Ile). Affected individuals with LARS2 variants had low frequency SNHL, a feature previously described in Perrault syndrome. A female with significant neurological disability was compound heterozygous for p.(Arg323Gln) and p.(Asn399Ser) variants in Twinkle (C10orf2). A male was homozygous for a novel variant in CLPP, p.(Cys144Arg). In three families there were no putative pathogenic variants in these genes confirming additional disease-causing genes remain unidentified. We have expanded the spectrum of disease-causing variants associated with Perrault syndrome.
Subject(s)
Amino Acyl-tRNA Synthetases/genetics , DNA Helicases/genetics , Endopeptidase Clp/genetics , Gonadal Dysgenesis, 46,XX/genetics , Hearing Loss, Sensorineural/genetics , Mitochondrial Proteins/genetics , Peroxisomal Multifunctional Protein-2/genetics , Exome/genetics , Female , Genotype , Gonadal Dysgenesis, 46,XX/pathology , Hearing Loss, Sensorineural/pathology , Homozygote , Humans , Male , Mutation , Pedigree , Phenotype , Primary Ovarian Insufficiency/genetics , Primary Ovarian Insufficiency/physiopathologyABSTRACT
OBJECTIVE: Barth Syndrome (BTHS) is an X-linked multisystem disorder (OMIM 302060) usually diagnosed in infancy and characterized by cardiac problems [dilated cardiomyopathy (DCM) ± endocardial fibroelastosis (EFE) ± left ventricular non-compaction (LVNC)], proximal myopathy, feeding problems, growth retardation, neutropenia, organic aciduria and variable respiratory chain abnormalities. We wished to determine whether BTHS had a significant impact on fetal and perinatal health in a large cohort of family groups originating from a defined region. METHOD: Case note review on 19 families originating from the UK and known to the Barth Syndrome Service of the Bristol Royal Hospital for Children. RESULTS: Details are presented on six kindreds (32%) with genetically and biochemically proven BTHS that demonstrate a wider phenotype including male fetal loss, stillbirth and severe neonatal illness or death. In these families, 9 males were stillborn and 14 died as neonates or infants but there were no losses of females. BTHS was definitively proven in five males with fetal onset of DCM ± hydrops/EFE/LVNC. CONCLUSION: These findings stress the importance of considering BTHS in the differential diagnosis of unexplained male hydrops, DCM, EFE, LVNC or pregnancy loss, as well as in neonates with hypoglycemia, lactic acidosis and idiopathic mitochondrial disease.
Subject(s)
Barth Syndrome/genetics , Cardiomyopathy, Dilated/genetics , Chromosomes, Human, X/genetics , Fetal Death/genetics , Fetal Diseases/genetics , Stillbirth/genetics , Acyltransferases , Barth Syndrome/epidemiology , Barth Syndrome/pathology , Biomarkers/blood , Cardiolipins/blood , Cardiomyopathy, Dilated/epidemiology , Cardiomyopathy, Dilated/pathology , Cohort Studies , Endocardial Fibroelastosis/epidemiology , Endocardial Fibroelastosis/genetics , Endocardial Fibroelastosis/pathology , Female , Fetal Death/epidemiology , Fetal Diseases/epidemiology , Fetal Diseases/pathology , Humans , Isolated Noncompaction of the Ventricular Myocardium/epidemiology , Isolated Noncompaction of the Ventricular Myocardium/genetics , Isolated Noncompaction of the Ventricular Myocardium/pathology , Lysophospholipids/blood , Male , Pedigree , Sequence Analysis, DNA , Sex Factors , Stillbirth/epidemiology , Transcription Factors/genetics , United Kingdom/epidemiologyABSTRACT
OBJECTIVE: To determine the frequency of mutations in CDKL5 in both male and female patients with infantile spasms or early onset epilepsy of unknown cause, and to consider whether the breadth of the reported phenotype would be extended by studying a different patient group. METHODS: Two groups of patients were investigated for CDKL5 mutations. Group 1 comprised 73 patients (57 female, 16 male) referred to Cardiff for CDKL5 analysis, of whom 49 (42 female, 7 male) had epileptic seizure onset in the first six months of life. Group 2 comprised 26 patients (11 female, 15 male) with infantile spasms previously recruited to a clinical trial, the UK Infantile Spasms Study. Where a likely pathogenic mutation was identified, further clinical data were reviewed. RESULTS: Seven likely pathogenic mutations were found among female patients from group 1 with epileptic seizure onset in the first six months of life, accounting for seven of the 42 in this group (17%). No mutations other than the already published mutation were found in female patients from group 2, or in any male patient from either study group. All patients with mutations had early signs of developmental delay and most had made little developmental progress. Further clinical information was available for six patients: autistic features and tactile hypersensitivity were common but only one had suggestive Rett-like features. All had a severe epileptic seizure disorder, all but one of whom had myoclonic jerks. The EEG showed focal or generalised changes and in those with infantile spasms, hypsarrhythmia. Slow frequencies were seen frequently with a frontal or fronto-temporal predominance and high amplitudes. CONCLUSIONS: The spectrum of the epileptic seizure disorder, and associated EEG changes, in those with CDKL5 mutations is broader than previously reported. CDKL5 mutations are a significant cause of infantile spasms and early epileptic seizures in female patients, and of a later intractable seizure disorder, irrespective of whether they have suspected Rett syndrome. Analysis should be considered in these patients in the clinical setting.
Subject(s)
Intellectual Disability/genetics , Mutation/genetics , Protein Serine-Threonine Kinases/genetics , Seizures/epidemiology , Seizures/genetics , Spasms, Infantile/genetics , Adolescent , Adult , Age of Onset , Child , Child, Preschool , Female , Humans , Infant , Infant, Newborn , MaleABSTRACT
We report two brothers with hypogonadotropic hypogonadism (HH), obesity and short stature associated with a maternally inherited pericentric inversion (X)(p11.4q11.2). On the basis that either breakpoint might disrupt a gene whose function is critical to normal sexual development we mapped the chromosomal breakpoints using two-colour fluorescent in situ hybridisation (FISH). The position of both the Xp11.4 and Xq11.2 breakpoints was refined using a panel of ordered BAC clones. No known genes were shown to map to the breakpoint regions. While we cannot entirely exclude the possibility that association between the clinical and cytogenetic phenotypes in the family is coincidental, it is possible that the inversion is responsible for HH through alternative molecular mechanisms such as position effects.
Subject(s)
Centromere/genetics , Chromosome Inversion/genetics , Obesity/congenital , Puberty, Delayed/genetics , Adolescent , Chromosomes, Human, X , Humans , Male , Pedigree , SiblingsSubject(s)
Cardiomyopathy, Dilated/diagnosis , Cardiomyopathy, Dilated/genetics , Mutation , Proteins/genetics , Adolescent , Adult , Cell Cycle Proteins , Child , Child, Preschool , DNA Mutational Analysis , Female , Humans , Male , PedigreeABSTRACT
We have recently shown that Okihiro syndrome results from mutation in the putative zinc finger transcription factor gene SALL4 on chromosome 20q13.13-13.2. There is considerable overlap of clinical features of Okihiro syndrome with other conditions, most notably Holt-Oram syndrome, a condition in part resulting from mutation of the TBX5 locus, as well as acro-renal-ocular syndrome. We analysed further families/patients with the clinical diagnosis of Holt-Oram syndrome and acro-renal-ocular syndrome for SALL4 mutations. We identified a novel SALL4 mutation in one family where the father was originally thought to have thalidomide embryopathy and had a daughter with a similar phenotype. We also found two novel mutations in two German families originally diagnosed as Holt-Oram syndrome and a further mutation in one out of two families carrying the diagnosis acro-renal-ocular syndrome. Our results show that some cases of "thalidomide embryopathy" might be the result of SALL4 mutations, resulting in an increased risk for similarly affected offspring. Furthermore we confirm the overlap of acro-renal-ocular syndrome with Okihiro syndrome at the molecular level and expand the phenotype of SALL4 mutations.
Subject(s)
Abnormalities, Multiple/genetics , Chromosomes, Human, Pair 20/genetics , Duane Retraction Syndrome/genetics , Transcription Factors/genetics , Abnormalities, Multiple/pathology , Base Sequence , DNA/chemistry , DNA/genetics , DNA Mutational Analysis , Duane Retraction Syndrome/pathology , Family Health , Female , Fetal Diseases/chemically induced , Fetal Diseases/genetics , Hand Deformities, Congenital/pathology , Heart Septal Defects, Atrial/pathology , Humans , Kidney/abnormalities , Male , Mutation , Pedigree , Phenotype , Thalidomide/adverse effects , Thumb/abnormalitiesABSTRACT
We describe a brother and sister with Bohring-Opitz syndrome and suggest that autosomal recessive inheritance may occur in this condition.
Subject(s)
Abnormalities, Multiple/genetics , Developmental Disabilities/genetics , Microcephaly/genetics , Abnormalities, Multiple/pathology , Agenesis of Corpus Callosum , Brain Stem/abnormalities , Child, Preschool , Developmental Disabilities/pathology , Female , Genes, Recessive , Humans , Magnetic Resonance Imaging , Microcephaly/pathology , SiblingsABSTRACT
The thrombocytopenia-absent radius (TAR) syndrome is a congenital malformation syndrome characterised by bilateral absence of the radii and a thrombocytopenia. The lower limbs, gastrointestinal, cardiovascular, and other systems may also be involved. Shaw and Oliver in 1959 were the first to describe this condition, but it was Hall et al in 1969 who reported the first major series of patients. Since then most reports have been based on single or small numbers of cases. We report the results of a clinical study looking at the phenotype of 34 patients with TAR syndrome. All cases had a documented thrombocytopenia and bilateral radial aplasia, 47% had lower limb anomalies, 47% cow's milk intolerance, 23% renal anomalies, and 15% cardiac anomalies. Congenital anomalies not previously described in association with TAR syndrome included facial capillary haemangiomata, intracranial vascular malformation, sensorineural hearing loss, and scoliosis. Karyotype analysis, chromosome breakage studies including premature centromeric separation and fluorescence in situ hybridisation studies looking for a deletion of chromosome 22q11 were undertaken. Two abnormal karyotypes were identified.
Subject(s)
Abnormalities, Multiple/genetics , Abnormalities, Multiple/physiopathology , Arm/abnormalities , Radius/abnormalities , Thrombocytopenia/genetics , Thrombocytopenia/physiopathology , Child , Chromosome Aberrations , Chromosomes, Human, Pair 22/genetics , Digestive System Abnormalities , Female , Humans , In Situ Hybridization, Fluorescence , Infant, Newborn , Karyotyping , Leg/abnormalities , Male , Syndrome , Urogenital Abnormalities/geneticsABSTRACT
Dominant optic atrophy (DOA) is the commonest form of inherited optic neuropathy. Although heterogeneous, a major locus has been mapped to chromosome 3q28 and the gene responsible, OPA1, was recently identified. We therefore screened a panel of 35 DOA patients for mutations in OPA1. This revealed 14 novel mutations and a further three known mutations, which together accounted for 20 of the 35 families (57%) included in this study. This more than doubles the number of OPA1 mutations reported in the literature, bringing the total to 25. These are predominantly null mutations generating truncated proteins, strongly suggesting that the mechanism underlying DOA is haploinsufficiency. The mutations are largely family-specific, although a common 4 bp deletion in exon 27 (eight different families) and missense mutations in exons 8 (two families) and 9 (two families) have been identified. Haplotype analysis of individuals with the exon 27 2708del(TTAG) mutation suggests that this is a mutation hotspot and not an ancient mutation, thus excluding a major founder effect at the OPA1 locus. The mutation screening in this study also identified a number of asymptomatic individuals with OPA1 mutations. A re-calculation of the penetrance of this disorder within two of our families indicates figures as low as 43 and 62% associated with the 2708del(TTAG) mutation. If haploinsufficiency is the mechanism underlying DOA it is unlikely that this figure will be mutation-specific, indicating that the penetrance in DOA is much lower than the 98% reported previously. To investigate whether Leber's hereditary optic neuropathy (LHON) could be caused by mutations in OPA1 we also screened a panel of 28 LHON patients who tested negatively for the three major LHON mutations. No mutations were identified in any LHON patients, indicating that DOA and LHON are genetically distinct.
Subject(s)
GTP Phosphohydrolases/genetics , Optic Atrophies, Hereditary/genetics , Alternative Splicing/genetics , Amino Acid Sequence , Codon, Nonsense , DNA/chemistry , DNA/genetics , DNA Mutational Analysis , Family Health , Female , Gene Frequency , Genetic Testing , Haplotypes , Humans , Male , Microsatellite Repeats , Molecular Sequence Data , Mutation , Mutation, Missense , Optic Atrophies, Hereditary/diagnosis , Pedigree , Penetrance , Polymorphism, Single-Stranded Conformational , Sequence Deletion , Sequence Homology, Amino AcidABSTRACT
3-Hydroxyisobutyric aciduria is a rare biochemical finding associated with a variable clinical phenotype in the literature. We report two siblings excreting abnormal levels of this metabolite from a consanguineous family who manifested distinct phenotypic variation. We speculate as to whether this biochemical anomaly may simply be an incidental finding and suggest that pre-natal counselling on the basis of metabolite identification may be unwarranted.
Subject(s)
Hydroxybutyrates/urine , Metabolism, Inborn Errors/genetics , Metabolism, Inborn Errors/urine , Microcephaly/genetics , Microcephaly/urine , Child , Family Health , Female , Genetic Heterogeneity , Humans , Male , PhenotypeABSTRACT
p63 mutations have been associated with EEC syndrome (ectrodactyly, ectodermal dysplasia, and cleft lip/palate), as well as with nonsyndromic split hand-split foot malformation (SHFM). We performed p63 mutation analysis in a sample of 43 individuals and families affected with EEC syndrome, in 35 individuals affected with SHFM, and in three families with the EEC-like condition limb-mammary syndrome (LMS), which is characterized by ectrodactyly, cleft palate, and mammary-gland abnormalities. The results differed for these three conditions. p63 gene mutations were detected in almost all (40/43) individuals affected with EEC syndrome. Apart from a frameshift mutation in exon 13, all other EEC mutations were missense, predominantly involving codons 204, 227, 279, 280, and 304. In contrast, p63 mutations were detected in only a small proportion (4/35) of patients with isolated SHFM. p63 mutations in SHFM included three novel mutations: a missense mutation (K193E), a nonsense mutation (Q634X), and a mutation in the 3' splice site for exon 5. The fourth SHFM mutation (R280H) in this series was also found in a patient with classical EEC syndrome, suggesting partial overlap between the EEC and SHFM mutational spectra. The original family with LMS (van Bokhoven et al. 1999) had no detectable p63 mutation, although it clearly localizes to the p63 locus in 3q27. In two other small kindreds affected with LMS, frameshift mutations were detected in exons 13 and 14, respectively. The combined data show that p63 is the major gene for EEC syndrome, and that it makes a modest contribution to SHFM. There appears to be a genotype-phenotype correlation, in that there is a specific pattern of missense mutations in EEC syndrome that are not generally found in SHFM or LMS.
Subject(s)
Ectodermal Dysplasia/genetics , Limb Deformities, Congenital/genetics , Membrane Proteins , Mutation , Phosphoproteins/genetics , Trans-Activators/genetics , Alternative Splicing , Amino Acid Substitution , Base Sequence , DNA Mutational Analysis , DNA-Binding Proteins , Gene Deletion , Genes, Tumor Suppressor , Genotype , Humans , Karyotyping , Molecular Sequence Data , Phenotype , Statistics as Topic , Transcription Factors , Tumor Suppressor ProteinsABSTRACT
The aims of this study were to assess the feasibility of using comparative genomic hybridisation instead of conventional cytogenetics in prenatal diagnosis and to determine the size of DNA loss that can be detected. Using comparative genomic hybridisation, six cases with standard aneuploidies were diagnosed correctly. This technique clearly identified a partial duplication of the long arm of chromosome 1 but was not capable of detecting the associated inversion. A small interstitial deletion on short arm of chromosome 10 also was detected precisely. Although the current comparative genomic hybridisation resolution is similar to the sensitivity of the highest resolution G banding, the latter is not a routine strategy in prenatal diagnosis. Comparative genomic hybridisation can allow full chromosome assessment equal to the highest resolution cytogenetic studies without the need for cell culture.
Subject(s)
Monosomy/diagnosis , Nucleic Acid Hybridization/methods , Prenatal Diagnosis/methods , Trisomy/diagnosis , Cytogenetic Analysis/standards , DNA/analysis , Feasibility Studies , Female , Humans , Pregnancy , Prenatal Diagnosis/standards , Sensitivity and SpecificityABSTRACT
AIMS: To investigate pancreatic function in children attending an obesity clinic. METHODS: Thirty six children (of which 34 were white) with severe obesity of prepubertal onset (body mass index more than +2 SDS) were reviewed clinically and dysmorphologically, with assessment of pancreatic function. RESULTS: Eight had dysmorphic features and 13 had learning difficulties. Four of 17 prepubertal children had hyperinsulinaemia and seven had hyperproinsulinaemia. All 19 pubertal children had hyperinsulinaemia, 14 had hyperproinsulinaemia, and one had type II diabetes. CONCLUSIONS: Metabolic abnormalities predictive of type II diabetes occur in severely obese white children.
Subject(s)
Obesity, Morbid/metabolism , Pancreas/metabolism , Adolescent , Body Mass Index , Child , Child, Preschool , Diabetes Mellitus/etiology , Diabetes Mellitus/metabolism , Diabetes Mellitus, Type 2/etiology , Female , Humans , Hyperinsulinism/etiology , Male , Obesity , Obesity, Morbid/complications , Pancreatic Function Tests , Predictive Value of Tests , Puberty, Precocious/etiology , Puberty, Precocious/metabolism , Risk FactorsABSTRACT
A child with macrocephaly-cutis marmorata developed severe abdominal pain thought to represent mesenteric angina. There were abnormalities of the aortic and mesenteric vasculature not previously reported in this condition. Angina therapy afforded amelioration of his symptoms. Mesenteric angina should be considered as a cause for abdominal pain in children with mesodermal anomalies.
Subject(s)
Abnormalities, Multiple/diagnosis , Infarction/diagnosis , Mesenteric Arteries/abnormalities , Mesoderm/pathology , Abdominal Pain/etiology , Abnormalities, Multiple/diagnostic imaging , Adolescent , Angiography , Anorexia/etiology , Brain/blood supply , Brain/pathology , Humans , Infant, Newborn , Infarction/diagnostic imaging , Infarction/therapy , Kidney/diagnostic imaging , Kidney/pathology , Male , Mesenteric Arteries/pathology , Spleen/diagnostic imaging , Spleen/pathology , Venous Thrombosis/diagnosis , Venous Thrombosis/drug therapy , Warfarin/therapeutic useABSTRACT
EEC syndrome is an autosomal dominant disorder characterized by ectrodactyly, ectodermal dysplasia, and facial clefts. We have mapped the genetic defect in several EEC syndrome families to a region of chromosome 3q27 previously implicated in the EEC-like disorder, limb mammary syndrome (LMS). Analysis of the p63 gene, a homolog of p53 located in the critical LMS/EEC interval, revealed heterozygous mutations in nine unrelated EEC families. Eight mutations result in amino acid substitutions that are predicted to abolish the DNA binding capacity of p63. The ninth is a frameshift mutation that affects the p63alpha, but not p63beta and p63gamma isotypes. Transactivation studies with these mutant p63 isotypes provide a molecular explanation for the dominant character of p63 mutations in EEC syndrome.
Subject(s)
Abnormalities, Multiple/genetics , Chromosomes, Human, Pair 3 , Genes, Tumor Suppressor , Genes, p53 , Germ-Line Mutation , Membrane Proteins , Mutation, Missense , Phosphoproteins/genetics , Trans-Activators , Amino Acid Sequence , Amino Acid Substitution , Chromosome Mapping , DNA-Binding Proteins , Ectodermal Dysplasia/genetics , Face/abnormalities , Female , Foot Deformities, Congenital/genetics , Genetic Markers , Hand Deformities, Congenital/genetics , Humans , Male , Models, Molecular , Molecular Sequence Data , Pedigree , Phosphoproteins/chemistry , Protein Structure, Secondary , Sequence Alignment , Sequence Homology, Amino Acid , Syndrome , Transcription Factors , Tumor Suppressor ProteinsABSTRACT
Mutations have recently been identified in the G4.5 gene (Xq28), encoding the tafazzin protein, in patients with Barth syndrome. We performed mutational analysis in 5 families with suspected Barth syndrome. In 4 families a male child had all the cardinal features of this syndrome, and mutations of G4.5 were found in each case. A mutation was also found in a fifth family with an extensive history of early infant death from heart disease. The recognition of 5 unrelated families in 1 hospital during a 7-year period suggests that this disease may be underdiagnosed.
Subject(s)
Cardiomyopathy, Dilated/diagnosis , Cardiomyopathy, Dilated/genetics , DNA Mutational Analysis , Failure to Thrive/diagnosis , Failure to Thrive/genetics , Genetic Linkage/genetics , Glutarates/urine , Mutagenesis, Insertional/genetics , Mutation, Missense/genetics , Neutropenia/diagnosis , Neutropenia/genetics , X Chromosome/genetics , Cardiomyopathy, Dilated/metabolism , Failure to Thrive/metabolism , Humans , Infant , Infant, Newborn , Male , Mitochondrial Myopathies/diagnosis , Mitochondrial Myopathies/genetics , Mitochondrial Myopathies/metabolism , Neutropenia/metabolism , Pedigree , SyndromeABSTRACT
Atelosteogenesis type 2 (AO2) (MIM 256050) is a neonatally lethal chondrodysplasia characterised by severe limb shortening and deficient ossification of parts of the skeleton. Other features include facial dysmorphism, cleft palate, talipes, and abducted thumbs and toes. Phenotypic overlap with non-lethal diastrophic dysplasia (DTD) suggested a common aetiology and it has recently been confirmed that both syndromes result from mutations in the DTDST (diastrophic dysplasia sulphate transporter) gene.
Subject(s)
Abnormalities, Multiple , Osteochondrodysplasias , Abnormalities, Multiple/diagnosis , Abnormalities, Multiple/genetics , Abnormalities, Multiple/pathology , Anion Transport Proteins , Carrier Proteins/genetics , Diagnosis, Differential , Female , Humans , Infant, Newborn , Male , Membrane Transport Proteins , Osteochondrodysplasias/diagnosis , Osteochondrodysplasias/genetics , Osteochondrodysplasias/pathology , Sulfate Transporters , SyndromeABSTRACT
Holt-Oram syndrome is a developmental disorder affecting the heart and upper limb, the gene for which was mapped to chromosome 12 two years ago. We have now identified a gene for this disorder (HOS1). The gene (TBX5) is a member of the Brachyury (T) family corresponding to the mouse Tbx5 gene. We have identified six mutations, three in HOS families and three in sporadic HOS cases. Each of the mutations introduces a premature stop codon in the TBX5 gene product. Tissue in situ hybridization studies on human embryos from days 26 to 52 of gestation reveal expression of TBX5 in heart and limb, consistent with a role in human embryonic development.
