Your search keyword '"James C. Mullikin"' showing total 4 results

1. TMEM231Gene Conversion Associated with Joubert and Meckel-Gruber Syndromes in the Same Family

Author

Meral Gunay-Aygun, Joshi Stephen, Daniel Konzman, Jennifer Guo, James C. Mullikin, Roxanne Fischer, Dino Maglic, William A. Gahl, May Christine V. Malicdan, and Thierry Vilboux

Subjects

0301 basic medicine, Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Occipital encephalocele, Polydactyly, Genetic heterogeneity, 030105 genetics & heredity, Biology, medicine.disease, Brother, Ciliopathies, 03 medical and health sciences, Exon, 030104 developmental biology, medicine, Missense mutation, Genetics (clinical), Exome sequencing

Abstract

Joubert and Meckel-Gruber syndromes (JS and MGS) are ciliopathies with overlapping features. JS patients manifest the “molar tooth sign” on brain imaging and variable eye, kidney and liver disease. MGS presents with polycystic kidneys, occipital encephalocele and polydactyly; it is typically perinatally fatal. Both syndromes are genetically heterogeneous; some genes cause either syndrome. Here, we report two brothers married to unrelated women. The first brother had three daughters with JS and a son with polycystic kidneys who died at birth. The second brother's wife had a fetal demise due to MGS. Whole exome sequencing identified TMEM231 NM_001077416.2: c.784G>A; p.(Asp262Asn) in all children and the wife of the first brother; the second brother's wife had a c.406T>G;p.(Trp136Gly) change. In-depth analysis uncovered a rare gene conversion event in TMEM231, leading to loss of exon 4, in all the affected children of first brother. We believe that the combination of this gene conversion with different missense mutations led to a spectrum of phenotypes that span JS and MGS. This article is protected by copyright. All rights reserved

Published

2016

2. Common genetic causes of holoprosencephaly are limited to a small set of evolutionarily conserved driver genes of midline development coordinated by TGF-β, hedgehog, and FGF signaling

Author

Paul Kruszka, Seth I. Berger, Yupeng Wang, Maximilian Muenke, James C. Mullikin, Ping Hu, Rachel A. Hart, Lucilene Arilho Ribeiro-Bicudo, Nisc Comparative Sequencing Program, Antonio Richieri-Costa, Benjamin D. Solomon, Wendy S. W. Wong, James W. Thomas, Erich Roessler, Juliana Marino, Sung-Kook Hong, John E Niederhuber, Ariel F. Martinez, and Yu Abe

Subjects

0301 basic medicine, Proband, congenital, hereditary, and neonatal diseases and abnormalities, Genotype, Inheritance Patterns, Fibroblast growth factor, 03 medical and health sciences, Holoprosencephaly, Gene Frequency, Transforming Growth Factor beta, biology.animal, Genetics, medicine, Humans, Genetic Predisposition to Disease, Hedgehog Proteins, Gene, Hedgehog, Genetics (clinical), Genetic Association Studies, biology, MUTAÇÃO GENÉTICA, Wnt signaling pathway, Vertebrate, Syndrome, medicine.disease, Fibroblast Growth Factors, 030104 developmental biology, Phenotype, Mutation, NODAL, Signal Transduction

Abstract

Here, we applied targeted capture to examine 153 genes representative of all the major vertebrate developmental pathways among 333 probands to rank their relative significance as causes for holoprosencephaly (HPE). We now show that comparisons of variant transmission versus nontransmission among 136 HPE Trios indicates some reported genes now lack confirmation, while novel genes are implicated. Furthermore, we demonstrate that variation of modest intrinsic effect can synergize with these driver mutations as gene modifiers.

Published

2018

3. A comprehensive approach to identification of pathogenic FANCA variants in Fanconi anemia patients and their families

Author

James W. Thomas, Agata Smogorzewska, Alice Young, Danielle C. Kimble, Meghana Vemulapalli, Aparna Kamat, Frank X. Donovan, James C. Mullikin, Francis P. Lach, Elizabeth K. Flynn, Settara C. Chandrasekharappa, Siobhan Q. Gregg, and Arleen D. Auerbach

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Mutant, Mutation, Missense, Fluorescent Antibody Technique, Biology, Article, Cell Line, 03 medical and health sciences, Exon, Fanconi anemia, Complementary DNA, hemic and lymphatic diseases, Genotype, Genetics, medicine, Missense mutation, Humans, Gene, Genetics (clinical), Fanconi Anemia Complementation Group A Protein, medicine.disease, FANCA, 030104 developmental biology, Fanconi Anemia

Abstract

Fanconi anemia (FA) is a rare recessive DNA repair deficiency resulting from mutations in one of at least 22 genes. Two-thirds of FA families harbor mutations in FANCA. To genotype patients in the International Fanconi Anemia Registry (IFAR) we employed multiple methodologies, screening 216 families for FANCA mutations. We describe identification of 57 large deletions and 261 sequence variants, in 159 families. All but seven families harbored distinct combinations of two mutations demonstrating high heterogeneity. Pathogenicity of the 18 novel missense variants was analyzed functionally by determining the ability of the mutant cDNA to improve the survival of a FANCA-null cell line when treated with MMC. Overexpressed pathogenic missense variants were found to reside in the cytoplasm, and nonpathogenic in the nucleus. RNA analysis demonstrated that two variants (c.522G > C and c.1565A > G), predicted to encode missense variants, which were determined to be nonpathogenic by a functional assay, caused skipping of exons 5 and 16 respectively, and are most likely pathogenic. We report 48 novel FANCA sequence variants. Defining both variants in a large patient cohort is a major step towards cataloging all FANCA variants, and permitting studies of genotype-phenotype correlations. This article is protected by copyright. All rights reserved

Published

2017

4. TMEM231 Gene Conversion Associated with Joubert and Meckel-Gruber Syndromes in the Same Family

Author

Dino, Maglic, Joshi, Stephen, May Christine V, Malicdan, Jennifer, Guo, Roxanne, Fischer, Daniel, Konzman, James C, Mullikin, William A, Gahl, Thierry, Vilboux, and Meral, Gunay-Aygun

Subjects

Male, Polycystic Kidney Diseases, Gene Conversion, Mutation, Missense, Membrane Proteins, Sequence Analysis, DNA, Kidney Diseases, Cystic, Retina, Pedigree, Cerebellum, Humans, Abnormalities, Multiple, Exome, Female, Eye Abnormalities, Retinitis Pigmentosa, Ciliary Motility Disorders, Encephalocele

Abstract

Joubert and Meckel-Gruber syndromes (JS and MGS) are ciliopathies with overlapping features. JS patients manifest the "molar tooth sign" on brain imaging and variable eye, kidney, and liver disease. MGS presents with polycystic kidneys, occipital encephalocele, and polydactyly; it is typically perinatally fatal. Both syndromes are genetically heterogeneous; some genes cause either syndrome. Here, we report two brothers married to unrelated women. The first brother had three daughters with JS and a son with polycystic kidneys who died at birth. The second brother's wife had a fetal demise due to MGS. Whole exome sequencing identified TMEM231 NM_001077416.2: c.784GA; p.(Asp262Asn) in all children and the wife of the first brother; the second brother's wife had a c.406TG;p.(Trp136Gly) change. In-depth analysis uncovered a rare gene conversion event in TMEM231, leading to loss of exon 4, in all the affected children of first brother. We believe that the combination of this gene conversion with different missense mutations led to a spectrum of phenotypes that span JS and MGS.

Published

2016