ABSTRACT
BACKGROUND: Genodermatoses represent genetic anomalies of skin tissues including hair follicles, sebaceous glands, eccrine glands, nails, and teeth. Ten consanguineous families segregating various genodermatosis phenotypes were investigated in the present study. METHODS: Homozygosity mapping, exome, and Sanger sequencing were employed to search for the disease-causing variants in the 10 families. RESULTS: Exome sequencing identified seven homozygous sequence variants in different families, including: c.27delT in FERMT1; c.836delA in ABHD5; c.2453C>T in ERCC5; c.5314C>T in COL7A1; c.1630C>T in ALOXE3; c.502C>T in PPOX; and c.10G>T in ALDH3A2. Sanger sequencing revealed three homozygous variants: c.1718 + 2A>G in FERMT1; c.10459A>T in FLG; and c.92delT in the KRT14 genes as the underlying genetic cause of skin phenotypes. CONCLUSION: This study supports the use of exome sequencing as a powerful, efficient tool for identifying genes that underlie rare monogenic skin disorders.
Subject(s)
Rare Diseases/genetics , Skin Diseases, Genetic/genetics , 1-Acylglycerol-3-Phosphate O-Acyltransferase/genetics , Aldehyde Oxidoreductases/genetics , Blister/genetics , Collagen Type VII/genetics , Consanguinity , DNA Mutational Analysis , DNA-Binding Proteins/genetics , Endonucleases/genetics , Epidermolysis Bullosa/genetics , Epidermolysis Bullosa Dystrophica/genetics , Epidermolysis Bullosa Simplex/genetics , Exome , Female , Filaggrin Proteins , Flavoproteins/genetics , Homozygote , Humans , INDEL Mutation , Ichthyosiform Erythroderma, Congenital/genetics , Ichthyosis Vulgaris/genetics , Ichthyosis, Lamellar/genetics , Intermediate Filament Proteins/genetics , Keratin-14/genetics , Lipid Metabolism, Inborn Errors/genetics , Lipoxygenase/genetics , Male , Membrane Proteins/genetics , Mitochondrial Proteins/genetics , Muscular Diseases/genetics , Neoplasm Proteins/genetics , Nuclear Proteins/genetics , Pedigree , Periodontal Diseases/genetics , Phenotype , Photosensitivity Disorders/genetics , Porphyria, Variegate/genetics , Protoporphyrinogen Oxidase/genetics , Sjogren-Larsson Syndrome/genetics , Transcription Factors/genetics , Xeroderma Pigmentosum/geneticsABSTRACT
The ascending thoracic aorta is designed to withstand biomechanical forces from pulsatile blood. Thoracic aortic aneurysms and acute aortic dissections (TAADs) occur as a result of genetically triggered defects in aortic structure and a dysfunctional response to these forces. Here, we describe mutations in the forkhead transcription factor FOXE3 that predispose mutation-bearing individuals to TAAD. We performed exome sequencing of a large family with multiple members with TAADs and identified a rare variant in FOXE3 with an altered amino acid in the DNA-binding domain (p.Asp153His) that segregated with disease in this family. Additional pathogenic FOXE3 variants were identified in unrelated TAAD families. In mice, Foxe3 deficiency reduced smooth muscle cell (SMC) density and impaired SMC differentiation in the ascending aorta. Foxe3 expression was induced in aortic SMCs after transverse aortic constriction, and Foxe3 deficiency increased SMC apoptosis and ascending aortic rupture with increased aortic pressure. These phenotypes were rescued by inhibiting p53 activity, either by administration of a p53 inhibitor (pifithrin-α), or by crossing Foxe3-/- mice with p53-/- mice. Our data demonstrate that FOXE3 mutations lead to a reduced number of aortic SMCs during development and increased SMC apoptosis in the ascending aorta in response to increased biomechanical forces, thus defining an additional molecular pathway that leads to familial thoracic aortic disease.
Subject(s)
Aortic Aneurysm, Thoracic/genetics , Aortic Dissection/genetics , Forkhead Transcription Factors/genetics , Adult , Aortic Dissection/metabolism , Aortic Dissection/pathology , Animals , Aorta/metabolism , Aorta/pathology , Aortic Aneurysm, Thoracic/metabolism , Aortic Aneurysm, Thoracic/pathology , Apoptosis , Cells, Cultured , Cyclin-Dependent Kinase Inhibitor p21/metabolism , Female , Gene Expression , Genetic Association Studies , Genetic Predisposition to Disease , Humans , Male , Mice, Inbred C57BL , Mice, Knockout , Middle Aged , Muscle, Smooth, Vascular/pathology , Mutation, Missense , Myocytes, Smooth Muscle/physiology , Pedigree , Tumor Suppressor Protein p53/genetics , Vascular Remodeling , ZebrafishABSTRACT
Unbiased genetic studies have uncovered surprising molecular mechanisms in human cellular immunity and autoimmunity. We performed whole-exome sequencing and targeted sequencing in five families with an apparent mendelian syndrome of autoimmunity characterized by high-titer autoantibodies, inflammatory arthritis and interstitial lung disease. We identified four unique deleterious variants in the COPA gene (encoding coatomer subunit α) affecting the same functional domain. Hypothesizing that mutant COPA leads to defective intracellular transport via coat protein complex I (COPI), we show that COPA variants impair binding to proteins targeted for retrograde Golgi-to-ER transport. Additionally, expression of mutant COPA results in ER stress and the upregulation of cytokines priming for a T helper type 17 (TH17) response. Patient-derived CD4(+) T cells also demonstrate significant skewing toward a TH17 phenotype that is implicated in autoimmunity. Our findings uncover an unexpected molecular link between a vesicular transport protein and a syndrome of autoimmunity manifested by lung and joint disease.
Subject(s)
Arthritis/genetics , Autoimmune Diseases/genetics , Coatomer Protein/genetics , Golgi Apparatus/metabolism , Lung Diseases, Interstitial/genetics , Amino Acid Sequence , Child, Preschool , Endoplasmic Reticulum/metabolism , Endoplasmic Reticulum Stress , Female , Genetic Association Studies , Genetic Predisposition to Disease , HEK293 Cells , Humans , Infant , Lod Score , Male , Molecular Sequence Data , Pedigree , Protein TransportABSTRACT
Up to 20% of individuals who have thoracic aortic aneurysms or acute aortic dissections but who do not have syndromic features have a family history of thoracic aortic disease. Significant genetic heterogeneity is established for this familial condition. Whole-genome linkage analysis and exome sequencing of distant relatives from a large family with autosomal-dominant inheritance of thoracic aortic aneurysms variably associated with the bicuspid aortic valve was used for identification of additional genes predisposing individuals to this condition. A rare variant, c.1031A>C (p.Glu344Ala), was identified in MAT2A, which encodes methionine adenosyltransferase II alpha (MAT IIα). This variant segregated with disease in the family, and Sanger sequencing of DNA from affected probands from unrelated families with thoracic aortic disease identified another MAT2A rare variant, c.1067G>A (p.Arg356His). Evidence that these variants predispose individuals to thoracic aortic aneurysms and dissections includes the following: there is a paucity of rare variants in MAT2A in the population; amino acids Glu344 and Arg356 are conserved from humans to zebrafish; and substitutions of these amino acids in MAT Iα are found in individuals with hypermethioninemia. Structural analysis suggested that p.Glu344Ala and p.Arg356His disrupt MAT IIα enzyme function. Knockdown of mat2aa in zebrafish via morpholino oligomers disrupted cardiovascular development. Co-transfected wild-type human MAT2A mRNA rescued defects of zebrafish cardiovascular development at significantly higher levels than mRNA edited to express either the Glu344 or Arg356 mutants, providing further evidence that the p.Glu344Ala and p.Arg356His substitutions impair MAT IIα function. The data presented here support the conclusion that rare genetic variants in MAT2A predispose individuals to thoracic aortic disease.
Subject(s)
Aortic Aneurysm, Thoracic/genetics , Methionine Adenosyltransferase/genetics , Adolescent , Adult , Amino Acid Sequence , Aortic Dissection/genetics , Animals , Aortic Valve/abnormalities , Bicuspid Aortic Valve Disease , Exome , Female , Genetic Linkage , Genetic Predisposition to Disease , Genetic Variation , Genotype , Heart Valve Diseases/genetics , Humans , Male , Methionine Adenosyltransferase/metabolism , Middle Aged , Mutation , Pedigree , Protein Conformation , RNA, Messenger/genetics , RNA, Messenger/metabolism , Young Adult , Zebrafish/geneticsABSTRACT
Gene mutations that lead to decreased contraction of vascular smooth-muscle cells (SMCs) can cause inherited thoracic aortic aneurysms and dissections. Exome sequencing of distant relatives affected by thoracic aortic disease and subsequent Sanger sequencing of additional probands with familial thoracic aortic disease identified the same rare variant, PRKG1 c.530G>A (p.Arg177Gln), in four families. This mutation segregated with aortic disease in these families with a combined two-point LOD score of 7.88. The majority of affected individuals presented with acute aortic dissections (63%) at relatively young ages (mean 31 years, range 17-51 years). PRKG1 encodes type I cGMP-dependent protein kinase (PKG-1), which is activated upon binding of cGMP and controls SMC relaxation. Although the p.Arg177Gln alteration disrupts binding to the high-affinity cGMP binding site within the regulatory domain, the altered PKG-1 is constitutively active even in the absence of cGMP. The increased PKG-1 activity leads to decreased phosphorylation of the myosin regulatory light chain in fibroblasts and is predicted to cause decreased contraction of vascular SMCs. Thus, identification of a gain-of-function mutation in PRKG1 as a cause of thoracic aortic disease provides further evidence that proper SMC contractile function is critical for maintaining the integrity of the thoracic aorta throughout a lifetime.
Subject(s)
Aorta, Thoracic/enzymology , Aortic Aneurysm, Thoracic/genetics , Aortic Dissection/genetics , Cyclic GMP-Dependent Protein Kinase Type I/genetics , Muscle, Smooth, Vascular/enzymology , Mutation , Acute Disease , Adolescent , Adult , Amino Acid Sequence , Aortic Dissection/enzymology , Aortic Dissection/physiopathology , Aorta, Thoracic/physiopathology , Aortic Aneurysm, Thoracic/enzymology , Aortic Aneurysm, Thoracic/physiopathology , Cyclic GMP/metabolism , Cyclic GMP-Dependent Protein Kinase Type I/metabolism , Exome , Female , Fibroblasts/enzymology , Fibroblasts/pathology , High-Throughput Nucleotide Sequencing , Humans , Male , Middle Aged , Molecular Sequence Data , Muscle Contraction , Muscle, Smooth, Vascular/physiopathology , Myosin Light Chains/genetics , Myosin Light Chains/metabolism , PedigreeABSTRACT
White matter hyperintensities (WMHs) of the brain are important markers of aging and small-vessel disease. WMHs are rare in healthy children and, when observed, often occur with comorbid neuroinflammatory or vasculitic processes. Here, we describe a complex 4 kb deletion in 2q36.3 that segregates with early childhood communication disorders and WMH in 15 unrelated families predominantly from Southeast Asia. The premature brain aging phenotype with punctate and multifocal WMHs was observed in ~70% of young carrier parents who underwent brain MRI. The complex deletion removes the penultimate exon 3 of TM4SF20, a gene encoding a transmembrane protein of unknown function. Minigene analysis showed that the resultant net loss of an exon introduces a premature stop codon, which, in turn, leads to the generation of a stable protein that fails to target to the plasma membrane and accumulates in the cytoplasm. Finally, we report this deletion to be enriched in individuals of Vietnamese Kinh descent, with an allele frequency of about 1%, embedded in an ancestral haplotype. Our data point to a constellation of early language delay and WMH phenotypes, driven by a likely toxic mechanism of TM4SF20 truncation, and highlight the importance of understanding and managing population-specific low-frequency pathogenic alleles.
Subject(s)
Aging, Premature/genetics , Base Sequence , Genetic Predisposition to Disease , Language Development Disorders/genetics , Leukoencephalopathies/genetics , Sequence Deletion , Tetraspanins/genetics , Age of Onset , Aging, Premature/complications , Aging, Premature/ethnology , Aging, Premature/pathology , Asian People , Brain/metabolism , Brain/pathology , Child , Child, Preschool , Chromosomes, Human, Pair 2 , Exons , Female , Humans , Language Development Disorders/complications , Language Development Disorders/ethnology , Language Development Disorders/pathology , Leukoencephalopathies/complications , Leukoencephalopathies/ethnology , Leukoencephalopathies/pathology , Magnetic Resonance Imaging , Male , Molecular Sequence Data , Pedigree , Sequence Analysis, DNAABSTRACT
RATIONALE: Thoracic aortic aneurysms leading to acute aortic dissections (TAAD) can be inherited in families in an autosomal dominant manner. As part of the spectrum of clinical heterogeneity of familial TAAD, we recently described families with multiple members that had TAAD and intracranial aneurysms or TAAD and intracranial and abdominal aortic aneurysms inherited in an autosomal dominant manner. OBJECTIVE: To identify the causative mutation in a large family with autosomal dominant inheritance of TAAD with intracranial and abdominal aortic aneurysms by performing exome sequencing of 2 distantly related individuals with TAAD and identifying shared rare variants. METHODS AND RESULTS: A novel frame shift mutation, p. N218fs (c.652delA), was identified in the SMAD3 gene and segregated with the vascular diseases in this family with a logarithm of odds score of 2.52. Sequencing of 181 probands with familial TAAD identified 3 additional SMAD3 mutations in 4 families, p.R279K (c.836G>A), p.E239K (c.715G>A), and p.A112V (c.235C>T), resulting in a combined logarithm of odds score of 5.21. These 4 mutations were notably absent in 2300 control exomes. SMAD3 mutations were recently described in patients with aneurysms osteoarthritis syndrome and some of the features of this syndrome were identified in individuals in our cohort, but these features were notably absent in many SMAD3 mutation carriers. CONCLUSIONS: SMAD3 mutations are responsible for 2% of familial TAAD. Mutations are found in families with TAAD alone, along with families with TAAD, intracranial aneurysms, abdominal aortic and bilateral iliac aneurysms segregating in an autosomal dominant manner.
