ABSTRACT
Barth syndrome (BTHS) is an X-linked inborn error of metabolism which affects males. The main manifestations are cardiomyopathy, myopathy, hypotonia, growth delay, intermittent neutropenia and 3-methylglutaconic aciduria. Diagnosis is confirmed by mutational analysis of the TAZ gene and biochemical dosage of the monolysocardiolipin/tetralinoleoyl cardiolipin (MLCL:L4-CL) ratio. We report a 6-year-old boy who presented with severe hypoglycemia, lactic acidosis and severe dilated cardiomyopathy soon after birth. The MLCL:L4-CL ratio confirmed BTHS (3.90 on patient's fibroblast, normal: 0-0.3). Subsequent sequencing of the TAZ gene revealed only the new synonymous variant NM_000116.3 (TAZ):c.348C>T p.(Gly116Gly), which did not appear to affect the protein sequence. In silico prediction analysis suggested the new c.348C>T nucleotide change could alter the TAZ mRNA splicing processing. We analyzed TAZ mRNAs in the patient's fibroblasts and found an abnormal skipping of 24 bases (NM_000116.3:c.346_371), with the consequent ablation of 8 amino acid residues in the tafazzin protein (NP_000107.1:p.Lys117_Gly124del). Molecular analysis of at risk female family members identified the patient's sister and mother as heterozygous carriers. Apparently harmless synonymous variants in the TAZ gene can damage gene expression. Such findings widen our knowledge of molecular heterogeneity in BTHS.
Subject(s)
Barth Syndrome/genetics , Cardiomyopathy, Dilated/genetics , Transcription Factors/genetics , Transcription, Genetic , Acidosis, Lactic/genetics , Acidosis, Lactic/physiopathology , Acyltransferases , Barth Syndrome/blood , Barth Syndrome/physiopathology , Cardiolipins/blood , Cardiomyopathy, Dilated/physiopathology , Child , Exons/genetics , Female , Heterozygote , Humans , Hypoglycemia/genetics , Hypoglycemia/physiopathology , Lysophospholipids/blood , Male , MutationABSTRACT
Mutations in the FGD1 gene have been shown to cause Aarskog-Scott syndrome (AAS), or facio-digito-genital dysplasia (OMIM#305400), an X-linked disorder characterized by distinctive genital and skeletal developmental abnormalities with a broad spectrum of clinical phenotypes. To date, 20 distinct mutations have been reported, but little phenotypic data are available on patients with molecularly confirmed AAS. In the present study, we report on our experience of screening for mutations in the FGD1 gene in a cohort of 60 European patients with a clinically suspected diagnosis of AAS. We identified nine novel mutations in 11 patients (detection rate of 18.33%), including three missense mutations (p.R402Q; p.S558W; p.K748E), four truncating mutations (p.Y530X; p.R656X; c.806delC; c.1620delC), one in-frame deletion (c.2020_2022delGAG) and the first reported splice site mutation (c.1935+3A>C). A recurrent mutation (p.R656X) was detected in three independent families. We did not find any evidence for phenotype-genotype correlations between type and position of mutations and clinical features. In addition to the well-established phenotypic features of AAS, other clinical features are also reported and discussed.
Subject(s)
Guanine Nucleotide Exchange Factors/genetics , Intellectual Disability/genetics , Mutation , Syndrome , Abnormalities, Multiple/genetics , Amino Acid Motifs , Bone and Bones/abnormalities , Cohort Studies , DNA Mutational Analysis , Europe , Genitalia, Male/abnormalities , Germ-Line Mutation , Humans , Male , PhenotypeABSTRACT
Glycogen storage disease type Ib (GSD Ib, OMIM 232220) is an inborn disorder of glucose metabolism, caused by mutations in the G6PT gene, encoding a glucose 6-phosphate transporter (G6PT). GSD Ib is mainly associated with fasting hypoglycaemia and hepatomegaly. Most GSD Ib patients also show neutropenia and neutrophil dysfunction and therefore are at risk of developing severe infections and inflammatory bowel disease (IBD). An increased risk for autoimmune disorders, such as thyroid autoimmunity and Crohn-like disease, has also been demonstrated, but no systematic study on the prevalence of autoimmune disorders in GSD Ib patients has ever been performed. We describe a 25-year-old patient affected by GSD Ib who developed 'seronegative' myasthenia gravis (MG), presenting with bilateral eyelid ptosis, diplopia, dysarthria, severe dysphagia, dyspnoea and fatigue. The repetitive stimulation of peripheral nerves test showed signs of exhaustion of neuromuscular transmission, particularly evident in the cranial area. Even in the absence of identifiable anti-acetylcholine receptor antibodies, seronegative MG is considered an autoimmune disorder and may be related to the disturbed immune function observed in GSD Ib patients.
Subject(s)
Autoimmunity , Glycogen Storage Disease Type I/immunology , Myasthenia Gravis/immunology , Adult , Blepharoptosis/immunology , Blepharoptosis/physiopathology , Cholinesterase Inhibitors/therapeutic use , Deglutition Disorders/immunology , Deglutition Disorders/physiopathology , Dyspnea/immunology , Dyspnea/physiopathology , Fatigue/immunology , Fatigue/physiopathology , Female , Glycogen Storage Disease Type I/complications , Glycogen Storage Disease Type I/physiopathology , Glycogen Storage Disease Type I/therapy , Humans , Immunoglobulins, Intravenous/therapeutic use , Myasthenia Gravis/physiopathology , Myasthenia Gravis/therapy , Neurologic Examination , Neuromuscular Junction/physiopathology , Peripheral Nerves/physiopathology , Respiratory Insufficiency/immunology , Respiratory Insufficiency/physiopathology , Risk Assessment , Risk Factors , Steroids/therapeutic use , Treatment OutcomeABSTRACT
We describe three patients with type A Niemann-Pick disease (NPD-A). NPD-A is an autosomal recessive neuronal storage disease classified among the sphingolipidoses, characterized by accumulation of sphingomyelin in various tissues and in the brain. Magnetic Resonance imaging (MRI) of our three patients showed a marked delay of myelination with frontal atrophy. Few descriptions of this MRI pattern of delayed myelination have been published to date.
