Your search keyword '"Proband"' showing total 179 results

1. Molecular and genetic characterization of a large Brazilian cohort presenting hearing loss

Author

Diego Mariano, Cindy Yukimi Sonoda, Juliana Sampaio-Silva, Osório Abath-Neto, Vinicius Pedroso-Campos, Estefany Uchoa da Silva de Oliveira Longati, Karina Lezirovitz, Ana Carla Batissoco, Ricardo Ferreira Bento, Rafaela Jesus-Santos, Jeanne Oiticica, Ana Cristina Hiromi Hoshino, Gleiciele Alice Vieira-Silva, Robinson Koji Tsuji, and Eliete Pardono

Subjects

Proband, Pediatrics, medicine.medical_specialty, Hearing loss, Auditory neuropathy, Population, Connexins, Cohort Studies, Genetics, medicine, Humans, Genetic Testing, Hearing Loss, education, Genetics (clinical), education.field_of_study, biology, Waardenburg syndrome, Genetic heterogeneity, medicine.disease, Human genetics, Connexin 26, Mutation, biology.protein, medicine.symptom, Brazil, GJB6

Abstract

Hearing loss is one of the most common sensory defects, affecting 5.5% of the worldwide population and significantly impacting health and social life. It is mainly attributed to genetic causes, but their relative contribution reflects the geographical region’s socio-economic development. Extreme genetic heterogeneity with hundreds of deafness genes involved poses challenges for molecular diagnosis. Here we report the investigation of 542 hearing-impaired subjects from all Brazilian regions to search for genetic causes. Biallelic GJB2/GJB6 causative variants were identified in 12.9% (the lowest frequency was found in the Northern region, 7.7%), 0.4% carried GJB2 dominant variants, and 0.6% had the m.1555A > G variant (one aminoglycoside-related). In addition, other genetic screenings, employed in selected probands according to clinical presentation and presumptive inheritance patterns, identified causative variants in 2.4%. Ear malformations and auditory neuropathy were diagnosed in 10.8% and 3.5% of probands, respectively. In 3.8% of prelingual/perilingual cases, Waardenburg syndrome was clinically diagnosed, and in 71.4%, these diagnoses were confirmed with pathogenic variants revealed; seven out of them were novel, including one CNV. All these genetic screening strategies revealed causative variants in 16.2% of the cases. Based on causative variants in the molecular diagnosis and genealogy analyses, a probable genetic etiology was found in ~ 50% of the cases. The present study highlights the relevance of GJB2/GJB6 as a cause of hearing loss in all Brazilian regions and the importance of screening unselected samples for estimating frequencies. Moreover, when a comprehensive screening is not available, molecular diagnosis can be enhanced by selecting probands for specific screenings.

Published

2021

2. IFIH1 loss-of-function variants contribute to very early-onset inflammatory bowel disease

Author

Giorgio Perilongo, Luca Bosa, Mara Cananzi, Alberta Leon, Huie Jing, Joselito Sobreira Filho, Antonio Marzollo, Maria Oliva-Hemker, Howard A. Kader, Claudia Mescoli, Yu Zhang, Jing You, James R. Lupski, Anthony L. Guerrerio, Elizabeth Wohler, Maurizio Dalle Carbonare, Davide Colavito, P. Gaio, David Valle, Nara Sobreira, Sangeeta Bade, Richard Kellermayer, Alessandra Biffi, Helen C. Su, Shalini N. Jhangiani, Wesley Tung, Silvia Bresolin, Jennifer E. Posey, Maria Gabelli, and Renan Paulo Martin

Subjects

Male, Proband, Interferon-Induced Helicase, IFIH1, Biology, Inflammatory bowel disease, Article, Child, Preschool, Female, Humans, Infant, Inflammatory Bowel Diseases, Italy, Whole Genome Sequencing, Loss of Function Mutation, 03 medical and health sciences, Genetics, medicine, Human virome, Enteropathy, Expressivity (genetics), Child, Preschool, Interferon-Induced Helicase, Genetics (clinical), Exome sequencing, Immunodeficiency, IFIH1, 030304 developmental biology, 0303 health sciences, 030305 genetics & heredity, medicine.disease, Penetrance, Immunology

Abstract

BACKGROUND. Genetic defects of innate immunity impairing intestinal bacterial sensing are linked to the development of Inflammatory Bowel Disease (IBD). Although much evidence supports a role of the intestinal virome in gut homeostasis, most studies focus on intestinal viral composition rather than on host intestinal viral sensitivity. AIM. To demonstrate the association between the development of Very Early Onset IBD (VEOIBD) and variants in the IFIH1 gene which encodes MDA5, a key cytosolic sensor for viral nucleic acids. METHODS. Whole exome sequencing (WES) was performed in two independent cohorts of children with VEOIBD enrolled in Italy (n=18) and USA (n=24). Luciferase reporter assays were employed to assess MDA5 activity. An enrichment analysis was performed on IFIH1 comparing 42 VEOIBD probands with 1527 unrelated individuals without gastrointestinal or immunological issues. RESULTS. We identified rare, likely loss-of-function (LoF), IFIH1 variants in eight patients with VEOIBD from a combined cohort of 42 children. One subject, carrying a homozygous truncating variant resulting in complete LoF, experienced neonatal-onset, pan-gastrointestinal, IBD-like enteropathy plus multiple infectious episodes. The remaining seven subjects, affected by VEOIBD without immunodeficiency, were carriers of one LoF variant in IFIH1. Among these, two patients also carried a second hypomorphic variant, with partial function apparent when MDA5 was weakly stimulated. Furthermore, IFIH1 variants were significantly enriched in children with VEOIBD as compared to controls (p=0.007). CONCLUSIONS. Complete and partial MDA5 deficiency is associated with VEOIBD with variable penetrance and expressivity, suggesting a role for impaired intestinal viral sensing in IBD pathogenesis.

Published

2021

3. Unraveling the genetic complexities of combined retinal dystrophy and hearing impairment

Author

Susanne Kohl, Asuman Koparir, Hassan Behboudi, Seungbin Han, Thomas Haaf, Hossein Darvish, Rocio Zamora-Ortiz, Cristina Villanueva-Mendoza, Julia Doll, Daniel Villalobos, Reza Maroofian, Vianney Cortés-González, Laura Kuehlewein, Barbara Vona, Michaela A.H. Hofrichter, Narsis Daftarian, Mehraban Mirrahimi, Paulina Bahena, Aboulfazl Rad, Elham Alehabib, Paola Linares, Maria de la Luz Arenas-Sordo, Fatemeh Suri, Tabea Röder, Hamideh Sabbaghi, and Hamid Ahmadieh

Subjects

Proband, Pediatrics, medicine.medical_specialty, Hearing loss, MYO7A, Usher syndrome, Genetic counseling, Retinal Degeneration, Iran, Biology, medicine.disease, Pedigree, Phenotype, Mutation, otorhinolaryngologic diseases, Genetics, medicine, Humans, ddc:610, medicine.symptom, Scheie syndrome, Usher Syndromes, Genetics (clinical), Exome sequencing, Alström syndrome

Abstract

Usher syndrome, the most prevalent cause of combined hereditary vision and hearing impairment, is clinically and genetically heterogeneous. Moreover, several conditions with phenotypes overlapping Usher syndrome have been described. This makes the molecular diagnosis of hereditary deaf–blindness challenging. Here, we performed exome sequencing and analysis on 7 Mexican and 52 Iranian probands with combined retinal degeneration and hearing impairment (without intellectual disability). Clinical assessment involved ophthalmological examination and hearing loss questionnaire. Usher syndrome, most frequently due to biallelic variants in MYO7A (USH1B in 16 probands), USH2A (17 probands), and ADGRV1 (USH2C in 7 probands), was diagnosed in 44 of 59 (75%) unrelated probands. Almost half of the identified variants were novel. Nine of 59 (15%) probands displayed other genetic entities with dual sensory impairment, including Alström syndrome (3 patients), cone-rod dystrophy and hearing loss 1 (2 probands), and Heimler syndrome (1 patient). Unexpected findings included one proband each with Scheie syndrome, coenzyme Q10 deficiency, and pseudoxanthoma elasticum. In four probands, including three Usher cases, dual sensory impairment was either modified/aggravated or caused by variants in distinct genes associated with retinal degeneration and/or hearing loss. The overall diagnostic yield of whole exome analysis in our deaf–blind cohort was 92%. Two (3%) probands were partially solved and only 3 (5%) remained without any molecular diagnosis. In many cases, the molecular diagnosis is important to guide genetic counseling, to support prognostic outcomes and decisions with currently available and evolving treatment modalities.

Published

2021

4. Novel truncation mutations in MYRF cause autosomal dominant high hyperopia mapped to 11p12–q13.3

Author

Zhiqun Tan, Wenmin Sun, Shiqiang Li, Xiaoyun Jia, Jiamin Ouyang, J. Fielding Hejtmancik, Xueshan Xiao, and Qingjiong Zhang

Subjects

Male, Proband, Eye Diseases, genetic structures, DNA Mutational Analysis, Neurodegenerative, Eye, medicine.disease_cause, Gene Knockout Techniques, Pair 11, Fluorescein Angiography, Zebrafish, Genetics (clinical), Original Investigation, Genes, Dominant, Genetics & Heredity, Genetics, 0303 health sciences, Mutation, 030305 genetics & heredity, Chromosome Mapping, Eye Diseases, Hereditary, Phenotype, Pedigree, Hereditary, Hyperopia, Female, Human, Biotechnology, Biology, Chromosomes, Paediatrics and Reproductive Medicine, 03 medical and health sciences, Complementary and Alternative Medicine, medicine, Animals, Humans, Dominant, Genetic Predisposition to Disease, Gene, Genetic Association Studies, 030304 developmental biology, Chromosomes, Human, Pair 11, Human Genome, Neurosciences, Membrane Proteins, Chromosome, biology.organism_classification, eye diseases, Human genetics, Genes, Genetic Loci, Lod Score, Transcription Factors

Abstract

High hyperopia is a common and severe form of refractive error. Genetic factors play important roles in the development of high hyperopia but the exact gene responsible for this condition is mostly unknown. We identified a large Chinese family with autosomal dominant high hyperopia. A genome-wide linkage scan mapped the high hyperopia to chromosome 11p12–q13.3, with maximum log of the odds scores of 4.68 at theta = 0 for D11S987. Parallel whole-exome sequencing detected a novel c.3377delG (p.Gly1126Valfs*31) heterozygous mutation in the MYRF gene within the linkage interval. Whole-exome sequencing in other 121 probands with high hyperopia identified additional novel mutations in MYRF within two other families: a de novo c.3274_3275delAG (p.Leu1093Profs*22) heterozygous mutation and a c.3194+2T>C heterozygous mutation. All three mutations are located in the C-terminal region of MYRF and are predicted to result in truncation of that portion. Two patients from two of the three families developed angle-closure glaucoma. These three mutations were present in neither the ExAC database nor our in-house whole-exome sequencing data from 3280 individuals. No other truncation mutations in MYRF were detected in the 3280 individuals. Knockdown of myrf resulted in small eye size in zebrafish. These evidence all support that truncation mutations in the C-terminal region of MYRF are responsible for autosomal dominant high hyperopia in these families. Our results may provide useful clues for further understanding the functional role of the C-terminal region of this critical myelin regulatory factor, as well as the molecular pathogenesis of high hyperopia and its associated angle-closure glaucoma. Electronic supplementary material The online version of this article (10.1007/s00439-019-02039-z) contains supplementary material, which is available to authorized users.

Published

2019

5. A genome-wide association study implicates the BMP7 locus as a risk factor for nonsyndromic metopic craniosynostosis

Author

Julie M. Phipps, Jenny Morton, Elizabeth Sweeney, Araceli Cuellar, Jeremy A. Sabourin, Assen Bussarsky, Val C. Sheffield, James L. Mills, Michael L. Cunningham, David W. Johnson, Karen Crawford, Krithi Bala, Mary M. Jenkins, Marta Barba, Louise C. Wilson, Cristina M. Justice, Nadezhda Yaneva, Lawrence C. Brody, Simeon A. Boyadjiev, Paul A. Romitti, Katie E. M. Rees, Andrew O.M. Wilkie, Wanda Lattanzi, Peter H. Langlois, Peter Noons, Yan Zhou, Rachel K. Tittle, Steven A. Wall, Tony Roscioli, Marike Zwienenberg, Denise M. Kay, Deirdre Cilliers, Kiril Georgiev, Jo C. Byren, Robert J. Sicko, Craig W. Senders, Lorenzo D. Botto, Alexander F. Wilson, Radka Kaneva, E Simeonov, Astrid Weber, Gianpiero Tamburrini, Kristin M Conway, James E. Boggan, and Janine M. LaSalle

Subjects

Proband, Linkage disequilibrium, Genotype, Bone Morphogenetic Protein 7, Genome-wide association study, Single-nucleotide polymorphism, Biology, genome‑wide association study, Polymorphism, Single Nucleotide, Linkage Disequilibrium, Article, Craniosynostosis, Paediatrics and Reproductive Medicine, 03 medical and health sciences, single nucleotide polymorphisms, Craniosynostoses, Complementary and Alternative Medicine, non syndromic craniosynostosis, Genes, Reporter, Risk Factors, Genetics, medicine, GWAS, Settore BIO/13 - BIOLOGIA APPLICATA, Humans, Genetic Predisposition to Disease, Promoter Regions, Genetic, Genetics (clinical), Alleles, 030304 developmental biology, PCDH11X, Genetics & Heredity, 0303 health sciences, 030305 genetics & heredity, Genetic Variation, Odds ratio, DNA Methylation, medicine.disease, Introns, craniosynostosis, Imputation (genetics), Genome-Wide Association Study

Abstract

Our previous genome-wide association study (GWAS) for sagittal nonsyndromic craniosynostosis (sNCS) provided important insights into the genetics of midline CS. In this study, we performed a GWAS for a second midline NCS, metopic NCS (mNCS), using 215 non-Hispanic white case-parent triads. We identified six variants with genome-wide significance (P ≤ 5 × 10(−8)): rs781716 (P = 4.71 × 10(−9); odds ratio [OR] = 2.44) intronic to SPRY3; rs6127972 (P = 4.41 × 10(−8); OR = 2.17) intronic to BMP7; rs62590971 (P = 6.22 × 10(−9); OR = 0.34), located ~155 kb upstream from TGIF2LX; and rs2522623, rs2573826, and rs2754857, all intronic to PCDH11X (P = 1.76 × 10(−8), OR = 0.45; P = 3.31 × 10(−8), OR = 0.45; P = 1.09 × 10(−8), OR=0.44, respectively). We performed a replication study of these variants using an independent non-Hispanic white sample of 194 unrelated mNCS cases and 333 unaffected controls; only the association for rs6127972 (P = 0.004, OR = 1.45; meta-analysis P = 1.27 × 10(−8), OR = 1.74) was replicated. Our meta-analysis examining single nucleotide polymorphisms common to both our mNCS and sNCS studies showed the strongest association for rs6127972 (P = 1.16 × 10(−6)). Our imputation analysis identified a linkage disequilibrium block encompassing rs6127972, which contained an enhancer overlapping a CTCF transcription factor binding site (chr20:55,798,821–55,798,917) that was significantly hypomethylated in mesenchymal stem cells derived from fused metopic compared to open sutures from the same probands. This study provides additional insights into genetic factors in midline CS.

Published

2020

6. Rare SLC1A1 variants in hot water epilepsy

Author

Anuranjan Anand, Parthasarthy Satishchandra, Kalpita Rashimi Karan, and Sanjib Sinha

Subjects

Male, 0301 basic medicine, Proband, Hot Temperature, Patch-Clamp Techniques, Genetic Linkage, Excitotoxicity, medicine.disease_cause, 03 medical and health sciences, Genetic linkage, Genetics, medicine, Animals, Humans, Missense mutation, Exome, Amino Acid Sequence, Genetics (clinical), Exome sequencing, Epilepsy, Sequence Homology, Amino Acid, biology, SLC1A1, Glutamate receptor, Water, Pedigree, Excitatory Amino Acid Transporter 3, 030104 developmental biology, biology.protein, Female

Abstract

Hot water epilepsy is sensory epilepsy, wherein seizures are triggered by an unusual stimulus: contact with hot water. Although genetic factors contribute to the etiology of hot water epilepsy, molecular underpinnings of the disorder remain largely unknown. We aimed to identify the molecular genetic basis of the disorder by studying families with two or more of their members affected with hot water epilepsy. Using a combination of genome-wide linkage mapping and whole exome sequencing, a missense variant was identified in SLC1A1 in a three-generation family. Further, we examined SLC1A1in probands of 98 apparently unrelated HWE families with positive histories of seizures provoked by contact with hot water. In doing so, we found three rare variants, p.Asp174Asn, p.Val251Ile and p.Ile304Met in the gene. SLC1A1 is a neuronal glutamate transporter which limits excitotoxicity and its loss-of-function leads to age-dependent neurodegeneration. We examined functional attributes of the variants in cultured mammalian cells. All three non-synonymous variants affected glutamate uptake, exhibited altered glutamate kinetics and anion conductance properties of SLC1A1. These observations provide insights into the molecular basis of hot water epilepsy and show the role of SLC1A1 variants in this intriguing neurobehavioral disorder.

Published

2017

7. Genetic innovations and our understanding of stillbirth

Author

Louise Wilkins-Haug

Subjects

Proband, Long QT syndrome, Aneuploidy, Gestational Age, Disease, Biology, Bioinformatics, 03 medical and health sciences, Pregnancy, Genotype, Exome Sequencing, Genetics, medicine, Humans, Genetics (clinical), Exome sequencing, 030304 developmental biology, Chromosome Aberrations, 0303 health sciences, 030305 genetics & heredity, Infant, Newborn, Sudden infant death syndrome, Stillbirth, medicine.disease, Human genetics, Smith-Lemli-Opitz Syndrome, Channelopathies, Female

Abstract

Stillbirth after 20 weeks gestation happens in 1 in 200 pregnancies and occurs more commonly than neonatal loss and sudden infant death syndrome (SIDs) combined. The stillbirth rate is several times greater in low as opposed to high-resource countries. However, among high-resource countries, although a lower overall stillbirth rate exists, there has been little change for several decades. Molecular genetic technologies are emerging as important contributors to our understanding of stillbirth. Initially, genetic etiologies included alterations in chromosome number or structure such as aneuploidy and microduplications and deletions. More recently, next-generation sequencing analysis in two genetic conditions, Smith Lemli Optiz Syndrome (SLOs) and the channelopathy disorders (such as long QT syndrome (LQTS)) provide examples into the association of pathogenic gene variants with stillbirth. Although these specific conditions individually account for only a small number of stillbirths, investigating these disorders provides a new and innovative approach for further understanding genetic contributors to adverse pregnancy outcomes. Our knowledge of the role of genetic disease as an etiology for stillbirth is elementary. Genomic interrogation of maternal–fetal genotypes, gene–gene, and genotype–environment interaction is lacking in stillbirth research. At the DNA sequence level, further investigation of variants of unknown significance is an opportunity for exploration of biologic pathways of importance to pregnancy loss. This review concentrates on SLO as an example of a single gene disorder with a high carrier but low affected liveborn proband rate. The channelopathy disorders are included as initial examples of genetic conditions with variable presentation including an association with sudden infant death syndrome. Highlighted are the challenges when numerous genes and variants are involved, and the task of assigning pathogenicity. The advantages and limitations of genetic evaluations are presented and avenues for further research considered.

Published

2019

8. Biallelic variants in SMAD6 are associated with a complex cardiovascular phenotype

Author

Kerstin Kutsche, Frederike L. Harms, Katja Kloth, Mark C. Johnson, Jane Juusola, Jessika Johannsen, Tatjana Bierhals, and Dorothy K. Grange

Subjects

Proband, Male, Pathology, medicine.medical_specialty, Genotype, Smad6 Protein, Population, Mutation, Missense, Biology, Compound heterozygosity, Thoracic aortic aneurysm, Craniosynostosis, 03 medical and health sciences, Mice, Exome Sequencing, Genetics, medicine, Missense mutation, Animals, Humans, Genetic Predisposition to Disease, education, Genetics (clinical), Exome sequencing, Alleles, 030304 developmental biology, 0303 health sciences, education.field_of_study, 030305 genetics & heredity, Left pulmonary artery, medicine.disease, Phenotype, Cardiovascular Diseases, Child, Preschool, Female

Abstract

Rare heterozygous variants in SMAD6 have been identified as a significant genetic contributor to bicuspid aortic valve-associated thoracic aortic aneurysm on one hand and non-syndromic midline craniosynostosis on the other. In this study, we report two individuals with biallelic missense variants in SMAD6 and a complex cardiac phenotype. Trio exome sequencing in Proband 1, a male who had aortic isthmus stenosis, revealed the homozygous SMAD6 variant p.(Ile466Thr). He also had mild intellectual disability and radio-ulnar synostosis. Proband 2 is a female who presented with a more severe cardiac phenotype with a dysplastic and stenotic pulmonary valve and dilated cardiomyopathy. In addition, she had vascular anomalies, including a stenotic left main coronary artery requiring a bypass procedure, narrowing of the proximal left pulmonary artery and a venous anomaly in the brain. Proband 2 has compound heterozygous SMAD6 missense variants, p.(Phe357Ile) and p.(Ser483Pro). Absence of these SMAD6 variants in the general population and high pathogenicity prediction scores suggest that these variants caused the probands' phenotypes. This is further corroborated by cardiovascular anomalies and appendicular skeletal defects in Smad6-deficient mice. SMAD6 acts as an inhibitory SMAD and preferentially inhibits bone morphogenetic protein (BMP)-induced signaling. Our data suggest that biallelic variants in SMAD6 may affect the inhibitory activity of SMAD6 and cause enhanced BMP signaling underlying the cardiovascular anomalies and possibly other clinical features in the two probands.

Published

2019

9. Spectrum of DNA variants for non-syndromic deafness in a large cohort from multiple continents

Author

Claudia Carranza, Guney Bademci, Marianna Herrera, Majid Mojarrad, M'hamed Grati, Joseph Foster, Abhiraami Kannan-Sundhari, Yong Feng, Denise Yan, F. Basak Cengiz, Mariem Bensaid, Akeem O. Lasisi, Reza Maroofian, Saber Masmoudi, Alex M. Mawla, Mahdiyeh Behnam, Bing Zou, Duygu Duman, Rahul Mittal, Demet Tekin, Mohan Kameswaran, Waheed A. Adedeji, Xuezhong Liu, Rosemary I. Kabahuma, Alexander Nord, Mustafa Tekin, T.J. Lasisi, Andrew H. Crosby, Susan H. Blanton, Ibis Menéndez, and Shengru Guo

Subjects

Male, 0301 basic medicine, Proband, MYO15A, Usher syndrome, Population, Deafness, Biology, Genetic analysis, Article, Paediatrics and Reproductive Medicine, 03 medical and health sciences, Complementary and Alternative Medicine, Clinical Research, Ethnicity, otorhinolaryngologic diseases, Genetics, medicine, 2.1 Biological and endogenous factors, Humans, Genetic Testing, Aetiology, education, Gene, Genetics (clinical), Genetic testing, Genetics & Heredity, education.field_of_study, medicine.diagnostic_test, medicine.disease, Human genetics, Brain Disorders, Genetics, Population, 030104 developmental biology, Mutation, Female, Usher Syndromes

Abstract

Hearing loss is the most common sensory deficit in humans with causative variants in over 140 genes. With few exceptions, however, the population-specific distribution for many of the identified variants/genes is unclear. Until recently, the extensive genetic and clinical heterogeneity of deafness precluded comprehensive genetic analysis. Here, using a custom capture panel (MiamiOtoGenes), we undertook a targeted sequencing of 180 genes in a multi-ethnic cohort of 342 GJB2 mutation-negative deaf probands from South Africa, Nigeria, Tunisia, Turkey, Iran, India, Guatemala, and the United States (South Florida). We detected causative DNA variants in 25% of multiplex and 7% of simplex families. The detection rate varied between 0 and 57% based on ethnicity, with Guatemala and Iran at the lower and higher end of the spectrum, respectively. We detected causative variants within 27 genes without predominant recurring pathogenic variants. The most commonly implicated genes include MYO15A, SLC26A4, USH2A, MYO7A, MYO6, and TRIOBP. Overall, our study highlights the importance of family history and generation of databases for multiple ethnically discrete populations to improve our ability to detect and accurately interpret genetic variants for pathogenicity.

Published

2016

10. Phenotypic subregions within the split-hand/foot malformation 1 locus

Author

Nanna Dahl Rendtorff, Niels Tommerup, Per Anker Jensen, Malene B. Rasmussen, Sven Kreiborg, Lisbeth Tranebjærg, Yuan Mang, Esben Budtz-Jørgensen, Mads Bak, and Marianne Lodahl

Subjects

Adult, Male, 0301 basic medicine, Proband, Proteasome Endopeptidase Complex, Craniofacial abnormality, Hearing loss, Molecular Sequence Data, Limb Deformities, Congenital, Locus (genetics), Biology, Craniofacial Abnormalities, Young Adult, 03 medical and health sciences, Genetics, medicine, Humans, Amino Acid Sequence, Craniofacial, Hearing Loss, Genetic Association Studies, Genetics (clinical), Chromosomal inversion, Homeodomain Proteins, High-Throughput Nucleotide Sequencing, DLX6, medicine.disease, Penetrance, Pedigree, Logistic Models, Phenotype, 030104 developmental biology, Gene Expression Regulation, Genetic Loci, Chromosome Inversion, Mutation, Female, medicine.symptom, Chromosomes, Human, Pair 7, Transcription Factors

Abstract

Split-hand/foot malformation 1 (SHFM1) is caused by chromosomal aberrations involving the region 7q21.3, DLX5 mutation, and dysregulation of DLX5/DLX6 expression by long-range position effects. SHFM1 can be isolated or syndromic with incomplete penetrance and a highly variable clinical expression, possibly influenced by sex and imprinting. We report on a new family with five affected individuals with syndromic SHFM1 that includes split-hand/foot malformations, hearing loss, and craniofacial anomalies, and an inv(7)(q21.3q35) present both in the proband and her affected son. The proximal inversion breakpoint, identified by next generation mate-pair sequencing, truncates the SHFM1 locus within the regulatory region of DLX5/6 expression. Through genotype-phenotype correlations of 100 patients with molecularly characterized chromosomal aberrations from 32 SHFM1 families, our findings suggest three phenotypic subregions within the SHFM1 locus associated with (1) isolated SHFM, (2) SHFM and hearing loss, and (3) SHFM, hearing loss, and craniofacial anomalies, respectively (ranked for increasing proximity to DLX5/6), and encompassing previously reported tissue-specific enhancers for DLX5/6. This uniquely well-characterized cohort of SHFM1 patients allowed us to systematically analyze the recently suggested hypothesis of skewed transmission and to confirm a higher penetrance in males vs. females in a subgroup of patients with isolated SHFM.

Published

2016

11. Delineation of LZTR1 mutation-positive patients with Noonan syndrome and identification of LZTR1 binding to RAF1-PPP1CB complexes

Author

Taiki Abe, Ikumi Umeki, Seiji Mizuno, Nobuhiko Okamoto, Keisuke Nagasaki, Yoichi Matsubara, Hirofumi Ohashi, Shigeo Kure, Tetsuya Niihori, Ikuma Fujiwara, Yoko Aoki, Shin Ichi Inoue, Makoto Yoshida, Kenji Kurosawa, and Shin Ichiro Kanno

Subjects

MAPK/ERK pathway, Proband, Adult, Male, Adolescent, Biology, Compound heterozygosity, Cardiofaciocutaneous syndrome, 03 medical and health sciences, Young Adult, Costello syndrome, Protein Phosphatase 1, Genetics, medicine, Humans, Exome, Child, Genetics (clinical), Exome sequencing, 030304 developmental biology, 0303 health sciences, 030305 genetics & heredity, Noonan Syndrome, medicine.disease, Prognosis, Proto-Oncogene Proteins c-raf, Phenotype, Child, Preschool, Mutation, Noonan syndrome, Female, Biomarkers, Follow-Up Studies, Protein Binding, Transcription Factors

Abstract

RASopathies are a group of developmental disorders caused by mutations in genes that regulate the RAS/MAPK pathway and include Noonan syndrome (NS), Costello syndrome, cardiofaciocutaneous syndrome and other related disorders. Whole exome sequencing studies recently identified LZTR1, PPP1CB and MRAS as new causative genes in RASopathies. However, information on the phenotypes of LZTR1 mutation-positive patients and functional properties of the mutations are limited. To identify variants of LZTR1, PPP1CB, and MRAS, we performed a targeted next-generation sequencing and reexamined previously analyzed exome data in 166 patients with suspected RASopathies. We identified eight LZTR1 variants, including a de novo variant, in seven probands who were suspicious for NS and one known de novo PPP1CB variant in a patient with NS. One of the seven probands had two compound heterozygous LZTR1 variants, suggesting autosomal recessive inheritance. All probands with LZTR1 variants had cardiac defects, including hypertrophic cardiomyopathy and atrial septal defect. Five of the seven probands had short stature or intellectual disabilities. Immunoprecipitation of endogenous LZTR1 followed by western blotting showed that LZTR1 bound to the RAF1-PPP1CB complex. Cells transfected with a small interfering RNA against LZTR1 exhibited decreased levels of RAF1 phosphorylated at Ser259. These are the first results to demonstrate LZTR1 in association with the RAF1-PPP1CB complex as a component of the RAS/MAPK pathway.

Published

2018

12. Attitudes towards the sharing of genetic information with at-risk relatives: results of a quantitative survey

Author

Timothy J Heaton and Victoria Chico

Subjects

0301 basic medicine, Proband, Adult, Male, Adolescent, media_common.quotation_subject, Population, Disease, 030105 genetics & heredity, Biology, Affect (psychology), 03 medical and health sciences, Surveys and Questionnaires, Genetics, Humans, Genetics(clinical), Confidentiality, Family, Genetic Predisposition to Disease, education, Genetics (clinical), media_common, Original Investigation, education.field_of_study, Information Dissemination, Focus Groups, Middle Aged, Focus group, Test (assessment), Female, Attitude to Health, Seriousness, Demography

Abstract

To investigate public attitudes towards receiving genetic information arising from a test on a relative, 955 University of Sheffield students and staff were surveyed using disease vignettes. Strength of attitude was measured on whether, in the event of relevant information being discovered, they, as an at-risk relative, would want to be informed, whether the at-risk relative’s interest should override proband confidentiality, and, if they had been the proband, willingness to give up confidentiality to inform such relatives. Results indicated considerably more complexity to the decision-making than simple statistical risk. Desire for information only slightly increased with risk of disease manifestation [log odds 0.05 (0.04, 0.06) per percentage point increase in manifestation risk]. Condition preventability was the primary factor increasing desire [modifiable baseline, non-preventable log odds −1.74 (−2.04, −1.44); preventable 0.64 (0.34, 0.95)]. Disease seriousness also increased desire [serious baseline, non-serious log odds −0.89 (−1.19, −0.59); fatal 0.55 (0.25, 0.86)]. Individuals with lower education levels exhibited much greater desire to be informed [GCSE log odds 1.67 (0.64, 2.66)]. Age did not affect desire. Our findings suggest that attitudes were influenced more by disease characteristics than statistical risk. Respondents generally expressed strong attitudes demonstrating that this was not an issue which people felt ambivalent about. We provide estimates of the British population in favour/against disclosure for various disease scenarios. Electronic supplementary material The online version of this article (doi:10.1007/s00439-015-1612-z) contains supplementary material, which is available to authorized users.

Published

2015

13. Oral-facial-digital syndrome type VI: is C5orf42 really the major gene?

Author

Alessia Micalizzi, Maja Steinlin, Patrizia Accorsi, Lorenzo Pinelli, Serdar Ceylaner, Eugen Boltshauser, Renato Borgatti, Franco Stanzial, Ronen Spiegel, Emanuela Avola, P Póo, Enrico Bertini, Tommaso Mazza, Giangennaro Coppola, Mario Lituania, Andrea Poretti, Loreto Martorell, Marta Romani, Nicole I. Wolf, Andreas R. Janecke, Sabrina Signorini, Elide Miccinilli, Kathrin Ludwig, Brahim Tabarki, Romina Romaniello, Sylvie Odent, Alessandro Simonati, Margherita Santucci, Francesca Mancini, Stefano D'Arrigo, Federica Zibordi, Enza Maria Valente, Lucio Giordano, Romani, Marta, Mancini, Francesca, Micalizzi, Alessia, Poretti, Andrea, Miccinilli, Elide, Accorsi, Patrizia, Avola, Emanuela, Bertini, Enrico, Borgatti, Renato, Romaniello, Romina, Ceylaner, Serdar, Coppola, Giangennaro, D’Arrigo, Stefano, Giordano, Lucio, Janecke, Andreas R., Lituania, Mario, Ludwig, Kathrin, Martorell, Loreto, Mazza, Tommaso, Odent, Sylvie, Pinelli, Lorenzo, Poo, Pilar, Santucci, Margherita, Signorini, Sabrina, Simonati, Alessandro, Spiegel, Ronen, Stanzial, Franco, Steinlin, Maja, Tabarki, Brahim, Wolf, Nicole I., Zibordi, Federica, Boltshauser, Eugen, Valente, Enza Maria, Cytogenetics, INGEMM, Institute of Medical and Molecular Genetics, Institut de Génétique et Développement de Rennes (IGDR), Université de Rennes 1 (UR1), Université de Rennes (UNIV-RENNES)-Université de Rennes (UNIV-RENNES)-Centre National de la Recherche Scientifique (CNRS)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Division of Anatomic Pathology, Department of Critical Care Medicine and Surgery, University of Florence Medical School, Università degli Studi di Firenze = University of Florence [Firenze] (UNIFI), Department of Neurological and Visual Sciences, University of Verona (UNIVR), Servizio aziendale di Consulenza Genetica, Ospedale di Bolzano, Pediatric surgery, NCA - Brain mechanisms in health and disease, Université de Rennes (UR)-Centre National de la Recherche Scientifique (CNRS)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Università degli Studi di Firenze = University of Florence (UniFI), and Università degli studi di Verona = University of Verona (UNIVR)

Subjects

Male, Proband, Oral-facial-digital type VI syndrome, [SDV]Life Sciences [q-bio], Joubert syndrome, C5orf42 gene, medicine.disease_cause, Cohort Studies, Cerebellum, Genetics(clinical), Eye Abnormalities, 610 Medicine & health, Orofaciodigital Syndrome, Membrane Protein, ComputingMilieux_MISCELLANEOUS, Genetics (clinical), Genetics, 0303 health sciences, Mutation, Polydactyly, 030305 genetics & heredity, Hypothalamic Disease, Cerebellar Disease, Kidney Diseases, Cystic, Orofaciodigital Syndromes, Major gene, Phenotype, Kidney Diseases, Female, Hypothalamic Diseases, Human, Hamartoma, Short Report, Biology, Retina, Follow-Up Studie, Cystic, 03 medical and health sciences, Genetic, Hypothalamic hamartoma, Cerebellar Diseases, Family, Follow-Up Studies, Humans, Membrane Proteins, medicine, Abnormalities, Multiple, 030304 developmental biology, medicine.disease, Eye Abnormalitie, Cohort Studie

Abstract

Oral-facial-digital type VI syndrome (OFDVI) is a rare phenotype of Joubert syndrome (JS). Recently, C5orf42 was suggested as the major OFDVI gene, being mutated in 9 of 11 families (82 %). We sequenced C5orf42 in 313 JS probands and identified mutations in 28 (8.9 %), most with a phenotype of pure JS. Only 2 out of 17 OFDVI patients (11.7 %) were mutated. A comparison of mutated vs. non-mutated OFDVI patients showed that preaxial and mesoaxial polydactyly, hypothalamic hamartoma and other congenital defects may predict C5orf42 mutations, while tongue hamartomas are more common in negative patients. Electronic supplementary material The online version of this article (doi:10.1007/s00439-014-1508-3) contains supplementary material, which is available to authorized users.

Published

2014

14. Increased prevalence of seizures in boys who were probands with the FMR1 premutation and co-morbid autism spectrum disorder

Author

Flora Tassone, Susan W. Harris, Randi J Hagerman, Yi Mu, Jacky Au, Andrea Schneider, Danh V. Nguyen, Weerasak Chonchaiya, David R Hessl, and Meredith Laird

Subjects

Male, Proband, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Adolescent, Population, Comorbidity, Biology, behavioral disciplines and activities, Article, California, Autism Diagnostic Observation Schedule, Fragile X Mental Retardation Protein, Gene Frequency, Seizures, mental disorders, Prevalence, Genetics, medicine, Humans, Sibling, Child, education, Genetics (clinical), Analysis of Variance, education.field_of_study, medicine.disease, FMR1, Fragile X syndrome, Child Development Disorders, Pervasive, Autism spectrum disorder, Child, Preschool, Trinucleotide Repeat Expansion

Abstract

Seizures are a common co-occurring condition in those with fragile X syndrome (FXS), and in those with idiopathic autism spectrum disorder (ASD). Seizures are also associated with ASD in those with FXS. However, little is known about the rate of seizures and how commonly these problems co-occur with ASD in boys with the FMR1 premutation. We, therefore, determined the prevalence of seizures and ASD in boys with the FMR1 permutation compared with their sibling counterparts and population prevalence estimates. Fifty premutation boys who presented as clinical probands (N = 25), or non-probands (identified by cascade testing after the proband was found) (N = 25), and 32 non-carrier controls were enrolled. History of seizures was documented and ASD was diagnosed by standardized measures followed by a team consensus of ASD diagnosis. Seizures (28%) and ASD (68%) were more prevalent in probands compared with non-probands (0 and 28%), controls (0 and 0%), and population estimates (1 and 1.7%). Seizures occurred more frequently in those with the premutation and co-morbid ASD particularly in probands compared with those with the premutation alone (25 vs. 3.85%, p = 0.045). Although cognitive and adaptive functioning in non-probands were similar to controls, non-probands were more likely to meet the diagnosis of ASD than controls (28 vs. 0%, p < 0.0001). In conclusion, seizures were relatively more common in premutation carriers who presented clinically as probands of the family and seizures were commonly associated with ASD in these boys. Therefore, boys with the premutation, particularly if they are probands should be assessed carefully for both ASD and seizures.

Published

2011

15. Genome-wide study of familial juvenile hyperuricaemic (gouty) nephropathy (FJHN) indicates a new locus, FJHN3, linked to chromosome 2p22.1-p21

Author

William Wong, Rajesh V. Thakker, Sian E. Piret, Olivier Devuyst, Peter Kotanko, Rosa J. Torres, Karl Lhotta, Anita A C Reed, Karena Pryce, Matthew A. Brown, Patrick Danoy, Thomas Müller, Juan G. Puig, and Karin Dahan

Subjects

Male, Proband, Gout, Genetic Linkage, 030232 urology & nephrology, Locus (genetics), Single-nucleotide polymorphism, Genome-wide association study, Hyperuricemia, Biology, Gene mutation, Genetic Heterogeneity, 03 medical and health sciences, 0302 clinical medicine, Genetic linkage, Genetics, Humans, Genetic Predisposition to Disease, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Genome, Human, Genetic heterogeneity, Autosomal dominant trait, Molecular biology, Pedigree, Uric Acid, Genetic Loci, Chromosomes, Human, Pair 2, Kidney Failure, Chronic, Female, Kidney Diseases, Genome-Wide Association Study

Abstract

Familial juvenile hyperuricaemic (gouty) nephropathy (FJHN), is an autosomal dominant disease associated with a reduced fractional excretion of urate, and progressive renal failure. FJHN is genetically heterogeneous and due to mutations of three genes: uromodulin (UMOD), renin (REN) and hepatocyte nuclear factor-1beta (HNF-1β) on chromosomes 16p12, 1q32.1, and 17q12, respectively. However, UMOD, REN or HNF-1β mutations are found in only approximately 45% of FJHN probands, indicating the involvement of other genetic loci in approximately 55% of probands. To identify other FJHN loci, we performed a single nucleotide polymorphism (SNP)-based genome-wide linkage analysis, in six FJHN families in whom UMOD, HNF-1β and REN mutations had been excluded. Parametric linkage analysis using a 'rare dominant' model established linkage in five of the six FJHN families, with a LOD score >+3, at 0% recombination, between FJHN and SNPs at chromosome 2p22.1-p21. Analysis of individual recombinants in two unrelated affected individuals defined a approximately 5.5 Mbp interval, flanked telomerically by SNP RS372139 and centromerically by RS896986 that contained the locus, designated FJHN3. The interval contains 28 genes, and DNA sequence analysis of the most likely candidate, solute carrier family 8 member 1 (SLC8A1), did not identify any abnormalities in the FJHN3 probands. FJHN3 is likely located within a approximately 5.5 Mbp interval on chromosome 2p22.1-p21, and identifying the genetic abnormality will help to further elucidate mechanisms predisposing to gout and renal failure.

Published

2011

16. Outcome of array CGH analysis for 255 subjects with intellectual disability and search for candidate genes using bioinformatics

Author

Xudong Liu, Ying Qiao, Evica Rajcan-Separovic, M. E. S. Lewis, Christine Tyson, Chansonette Harvard, C. Fawcett, Paul Pavlidis, and J. J. A. Holden

Subjects

Genetics, Proband, Comparative Genomic Hybridization, Candidate gene, Computational Biology, Disease, Biology, Bioinformatics, medicine.disease, Human genetics, Developmental disorder, Genes, Intellectual Disability, Intellectual disability, medicine, Humans, Copy-number variation, Gene, Genetics (clinical)

Abstract

Array CGH enables the detection of pathogenic copy number variants (CNVs) in 5-15% of individuals with intellectual disability (ID), making it a promising tool for uncovering ID candidate genes. However, most CNVs encompass multiple genes, making it difficult to identify key disease gene(s) underlying ID etiology. Using array CGH we identified 47 previously unreported unique CNVs in 45/255 probands. We prioritized ID candidate genes using five bioinformatic gene prioritization web tools. Gene priority lists were created by comparing integral genes from each CNV from our ID cohort with sets of training genes specific either to ID or randomly selected. Our findings suggest that different training sets alter gene prioritization only moderately; however, only the ID gene training set resulted in significant enrichment of genes with nervous system function (19%) in prioritized versus non-prioritized genes from the same de novo CNVs (7%, p < 0.05). This enrichment further increased to 31% when the five web tools were used in concert and included genes within mitogen-activated protein kinase (MAPK) and neuroactive ligand-receptor interaction pathways. Gene prioritization web tools enrich for genes with relevant function in ID and more readily facilitate the selection of ID candidate genes for functional studies, particularly for large CNVs.

Published

2010

17. Update on molecular diagnosis of hereditary hemorrhagic telangiectasia

Author

Kathleen Grant, Susan E. Walther, Arupa Ganguly, Jennifer Richards-Yutz, and Elizabeth C. Chao

Subjects

Adult, Male, Proband, Nonsynonymous substitution, Adolescent, Genotype, Activin Receptors, Type II, Receptors, Cell Surface, Single-nucleotide polymorphism, Telangiectases, Biology, medicine.disease_cause, Germline mutation, Antigens, CD, Gene Duplication, Genetics, medicine, Humans, Genetics (clinical), Aged, Aged, 80 and over, Mutation, Haplotype, Endoglin, ACVRL1, Middle Aged, Haplotypes, Molecular Diagnostic Techniques, Female, Telangiectasia, Hereditary Hemorrhagic, Gene Deletion

Abstract

Hereditary hemorrhagic telangiectasia (HHT) is an autosomal dominant, vascular disease hallmarked by the development of arteriovenous malformations (AVMs). Germline mutations in two genes, endoglin (ENG) and activin receptor like kinase 1 (ACVRL1), have been implicated in this disease. This report describes molecular diagnosis in a consecutive series of 600 individuals with clinical features of HHT disease. Each coding exon and flanking intronic regions of ENG and ACVRL1 genes was sequenced. Exonic copy number was quantified in probands without a coding sequence mutation. Novel nonsynonymous variants were further analyzed to predict functional consequences. In addition, common single nucleotide polymorphisms genotypes and haplotypes for the two genes were compared between individuals with and without mutations. The highest mutation detection rate (87% [95% CI 80.2-91.5]) was observed in probands who met all four Curacao criteria (epistaxis, telangiectases, AVMs and family history). More than 30% of identified mutations were novel; however, only 6% were variants of unknown significance. Determining the significance of novel mutations as related to disease presents additional challenges. Detection of multiple alterations in the same proband also requires careful evaluation for disease association. In conclusion, the sensitivity of molecular diagnosis is highest in probands with a clinically confirmed diagnosis of HHT. However, a substantial fraction of probands in this group do not carry an identifiable mutation in the coding exons of these two genes. This suggests alternate mechanisms of gene inactivation or involvement of alternate loci, and it requires further investigation.

Published

2010

18. A novel hypomorphic MECP2 point mutation is associated with a neuropsychiatric phenotype

Author

Abidemi A. Adegbola, Andrew Chess, Michael L. Gonzales, Gerald F. Cox, and Janine M. LaSalle

Subjects

Adult, Male, Proband, congenital, hereditary, and neonatal diseases and abnormalities, BALB 3T3 Cells, Methyl-CpG-Binding Protein 2, Developmental Disabilities, Mutation, Missense, Rett syndrome, Biology, Transfection, Bioinformatics, MECP2, Mice, mental disorders, Rett Syndrome, Genetics, medicine, Animals, Humans, Point Mutation, Missense mutation, Allele, Child, Genetics (clinical), DNA Primers, Chromosomes, Human, X, Base Sequence, Point mutation, medicine.disease, Ghrelin, Recombinant Proteins, nervous system diseases, Phenotype, Mutation (genetic algorithm), Mutation testing, Female

Abstract

The MECP2 gene on Xq28 encodes a transcriptional repressor, which binds to and modulates expression of active genes. Mutations in MECP2 cause classic or preserved speech variant Rett syndrome and intellectual disability in females and early demise or marked neurodevelopmental handicap in males. The consequences of a hypomorphic Mecp2 allele were recently investigated in a mouse model, which developed obesity, motor, social, learning, and behavioral deficits, predicting a human neurobehavioral syndrome. Here, we describe mutation analysis of a nondysmorphic female proband and her father who presented with primarily neuropsychiatric manifestations and obesity with relative sparing of intelligence, language, growth, and gross motor skills. We identified and characterized a novel missense mutation (c.454C>G; p.P152A) in the critical methyl-binding domain of MeCP2 that disrupts MeCP2 functional activity. We show that a gradient of impairment is present when the p.P152A mutation is compared with an allelic p.P152R mutation, which causes classic Rett syndrome and another Rett syndrome-causing mutation, such that protein-heterochromatin binding observed by immunofluorescence and immunoblotting is wild-type > P152A > P152R > T158 M, consistent with the severity of the observed phenotype. Our findings provide evidence for very mild phenotypes in humans associated with partial reduction of MeCP2 function arising from subtle variation in MECP2.

Published

2008

19. Compound heterozygous NOTCH1 mutations underlie impaired cardiogenesis in a patient with hypoplastic left heart syndrome

Author

Sybil C. L. Hrstka, Timothy M. Olson, Megan M. O’Byrne, Timothy J. Nelson, Mariza de Andrade, Patrick W. O'Leary, Jeanne L. Theis, and Jared M. Evans

Subjects

Proband, Male, Candidate gene, Heterozygote, Genetic Linkage, Heart Valve Diseases, Biology, Compound heterozygosity, Hypoplastic left heart syndrome, Bicuspid aortic valve, Bicuspid Aortic Valve Disease, Aortic Valve Atresia, Hypoplastic Left Heart Syndrome, Genetics, medicine, Missense mutation, Humans, Allele, Receptor, Notch1, Genetics (clinical), Computational Biology, Genomics, medicine.disease, Pedigree, Aortic Valve, Mutation, Female, Genome-Wide Association Study

Abstract

Hypoplastic left heart syndrome (HLHS) is a severe congenital heart defect (CHD) that necessitates staged, single ventricle surgical palliation. An increased frequency of bicuspid aortic valve (BAV) has been observed among relatives. We postulated number of mutant alleles as a molecular basis for variable CHD expression in an extended family comprised of an HLHS proband and four family members who underwent echocardiography and whole-genome sequencing (WGS). Dermal fibroblast-derived induced pluripotent stem cells (iPSC) were procured from the proband–parent trio and bioengineered into cardiomyocytes. Cardiac phenotyping revealed aortic valve atresia and a slit-like left ventricular cavity in the HLHS proband, isolated bicuspid pulmonary valve in his mother, BAV in a maternal 4° relative, and no CHD in his father or sister. Filtering of WGS for rare, functional variants that segregated with CHD and were compound heterozygous in the HLHS proband identified NOTCH1 as the sole candidate gene. An unreported missense mutation (P1964L) in the cytoplasmic domain, segregating with semilunar valve malformation, was maternally inherited and a rare missense mutation (P1256L) in the extracellular domain, clinically silent in the heterozygous state, was paternally inherited. Patient-specific iPSCs exhibited diminished transcript levels of NOTCH1 signaling pathway components, impaired myocardiogenesis, and a higher prevalence of heterogeneous myofilament organization. Extended, phenotypically characterized families enable WGS-derived variant filtering for plausible Mendelian modes of inheritance, a powerful strategy to discover molecular underpinnings of CHD. Identification of compound heterozygous NOTCH1 mutations and iPSC-based functional modeling implicate mutant allele burden and impaired myogenic potential as mechanisms for HLHS.

Published

2015

20. High diagnostic yield of clinical exome sequencing in Middle Eastern patients with Mendelian disorders

Author

Mariam Al-Mulla, Laila Mahmoud, Fowzan S. Alkuraya, Tawfeg Ben-Omran, Shenela Lakhani, Tarunashree Yavarna, Zafar Nawaz, Fatma Al-Mesaifri, Noora Shahbeck, Patrik Vitazka, Nader Al-Dewik, Rehab Ali, and Mariam Almureikhi

Subjects

Proband, Adult, Male, Microcephaly, Pediatrics, medicine.medical_specialty, Adolescent, Developmental Disabilities, Population, Consanguinity, Biology, Young Adult, Intellectual Disability, Genetics, medicine, Humans, Exome, Global developmental delay, Genetic Testing, education, Child, Qatar, Genetics (clinical), Exome sequencing, Genetic testing, education.field_of_study, Epilepsy, medicine.diagnostic_test, Infant, Genomics, Sequence Analysis, DNA, Middle Aged, medicine.disease, Arabs, Phenotype, Child, Preschool, Female

Abstract

Clinical exome sequencing (CES) has become an increasingly popular diagnostic tool in patients with heterogeneous genetic disorders, especially in those with neurocognitive phenotypes. Utility of CES in consanguineous populations has not yet been determined on a large scale. A clinical cohort of 149 probands from Qatar with suspected Mendelian, mainly neurocognitive phenotypes, underwent CES from July 2012 to June 2014. Intellectual disability and global developmental delay were the most common clinical presentations but our cohort displayed other phenotypes, such as epilepsy, dysmorphism, microcephaly and other structural brain anomalies and autism. A pathogenic or likely pathogenic mutation, including pathogenic CNVs, was identified in 89 probands for a diagnostic yield of 60%. Consanguinity and positive family history predicted a higher diagnostic yield. In 5% (7/149) of cases, CES implicated novel candidate disease genes (MANF, GJA9, GLG1, COL15A1, SLC35F5, MAGE4, NEUROG1). CES uncovered two coexisting genetic disorders in 4% (6/149) and actionable incidental findings in 2% (3/149) of cases. Average time to diagnosis was reduced from 27 to 5 months. CES, which already has the highest diagnostic yield among all available diagnostic tools in the setting of Mendelian disorders, appears to be particularly helpful diagnostically in the highly consanguineous Middle Eastern population.

Published

2015

21. Familial aggregation in lone atrial fibrillation

Author

Danita M. Yoerger, Jeremy N. Ruskin, Calum A. MacRae, and Patrick T. Ellinor

Subjects

Adult, Male, Proband, medicine.medical_specialty, Adolescent, Quantitative Trait Loci, Population, Biology, Cohort Studies, Risk Factors, Internal medicine, Atrial Fibrillation, Prevalence, Genetics, medicine, Humans, Family, Risk factor, education, Genetics (clinical), Aged, education.field_of_study, Age Factors, Family aggregation, Atrial fibrillation, Middle Aged, medicine.disease, Pedigree, Stroke, Endocrinology, Relative risk, Female, Familial atrial fibrillation, Demography, Cohort study

Abstract

Atrial fibrillation (AF) is the most common clinical arrhythmia and a major risk factor for stroke. To investigate the role of genetic factors in a typical clinical population, we determined the extent of familial aggregation in patients with lone AF. To estimate the relative risk to family members, the prevalence of AF for each class of relative was compared to the prevalence in the comparable age and sex group from the general population. Family members had an increased relative risk of AF compared to the general population (risk ratio; 95% confidence intervals): sons (8.1; 2.0-32), daughters (9.5; 1.3-67), brothers (70; 47-102), sisters (34; 14-80), mothers (4.0; 2.5-6.5) and fathers (2.0; 1.2-3.6). Relatives of probands with lone AF are at a substantially increased risk of developing this arrhythmia suggesting a Mendelian genetic contribution to the etiology of this common trait.

Published

2005

22. Molecular screening of the TGIF gene in holoprosencephaly: identification of two novel mutations

Author

Laurent Pasquier, Véronique David, Martine Blayau, Céline Aguilella, Sylvie Odent, Christèle Dubourg, Leila Lazaro, Jocelyne Attia-Sobol, and Jacqueline Vigneron

Subjects

Adult, Male, musculoskeletal diseases, Proband, congenital, hereditary, and neonatal diseases and abnormalities, DNA Mutational Analysis, Nonsense mutation, Mutation, Missense, Biology, Fetus, Holoprosencephaly, Genetics, medicine, Humans, Missense mutation, Transcription factor, Gene, Cells, Cultured, Genetics (clinical), Homeodomain Proteins, Genes, Homeobox, Infant, DNA, medicine.disease, Hedgehog signaling pathway, Human genetics, Repressor Proteins, Codon, Nonsense, Female

Abstract

Holoprosencephaly (HPE) is the most common severe brain anomaly in humans, which results from incomplete cleavage of the forebrain during early embryogenesis. The aetiology of HPE is very heterogeneous. Among the genetic factors, TGIF ( TG-interacting factor), which codes for a transcription factor modulating the signalling pathway of TGF-beta, was previously implicated. We investigated 127 HPE probands by sequencing their TGIF gene and identified the first nonsense mutation reported so far and also a novel missense mutation, in two families that presented a large range of disease severity. The low number of mutations in TGIF suggests that this gene has no major contribution to the aetiology of HPE and our study confirms the wide clinical heterogeneity of the disease.

Published

2003

23. The prevalence of connexin 26 ( GJB2 ) mutations in the Chinese population

Author

Xiao Mei Ke, Yu He Liu, Xia Juan Xia, Walter E. Nance, Fred F. Telischi, Xiao Mei Ouyang, Thomas J. Balkany, Xue Zhong Liu, Li Lin Du, Simon I. Angeli, and Li Rong Xu

Subjects

Male, Proband, China, Genotype, Hearing loss, Population, Deafness, Connexins, otorhinolaryngologic diseases, Genetics, medicine, Humans, Allele, education, Alleles, Genetics (clinical), education.field_of_study, biology, Haplotype, Connexin 26, Mutation, Mutation (genetic algorithm), biology.protein, Female, medicine.symptom, GJB6

Abstract

Mutations in GJB2, encoding gap junction beta 2 protein (connexin 26), are responsible for the commonest form of non-syndromic recessive deafness in many populations. It has been reported recently that the most common 35delG mutation in GJB2 is exceptionally low in Japanese and Korean populations, but another deletion, 235delC, is relatively frequent. Since the Chinese constitute approximately one fifth of the global population, the frequency of GJB2 mutations in the population has important implications for understanding worldwide causes of genetic deafness. To determine whether GJB2 mutations are an important cause of deafness in Chinese, we conducted mutation screening for GJB2 in 118 deaf Chinese probands, including 60 from simplex and 58 from multiplex families with non-syndromic deafness, and 150 normal hearing Chinese controls. Four mutations, including 235delC, 299–300delAT, V37I, and 35delG, were found in the patients. Thirty-nine percent of the probands had a GJB2 mutation. Of the 118 probands, 19 carried two definitely pathogenic mutations: three among the 58 multiplex cases (5.2%) and 16 among the 60 simplex cases (26.7%). Twenty-seven probands (22.9%) were found to carry only single GJB2 mutations. None of them had mutations in exon 1 of GJB2 and or the 342-kb deletion of GJB6. The 235delC mutation was the most prevalent mutation (20.3% of alleles), accounting for 81% of the pathologic alleles in multiplex cases and 67% in simplex cases. Analysis of the affected haplotypes in the patients with the homozygous 235delC mutation yielded evidence for a single origin of the mutation. The carrier frequency of the 235delC mutation in control subjects with normal hearing was 1.3%. The 35delG mutation was only noted as a heterozygous change in two simplex cases (1.2% of alleles). These results indicated that mutations in GJB2 are a major cause of inherited and sporadic congenital deafness in the Chinese population. The 235delC mutation, rather than 35delG, is the most common mutation found in the Chinese deaf population. Our data support the view that specific combinations of GJB2 mutation exist in different populations.

Published

2002

24. Complex segregation analysis of hypospadias

Author

Göran Läckgren, Arne Stenberg, Andrew Collins, Gunnar Westbacke, Jörgen Pedersen, Lars Lundquist, Einar Hansson, Lennart Iselius, Staffan Holmner, Louise Fredell, and Agneta Nordenskjöld

Subjects

Male, Proband, medicine.medical_specialty, Pediatrics, Biology, Risk Factors, Internal medicine, Genetics, medicine, Humans, Risk factor, Alleles, Genetics (clinical), Sweden, Hypospadias, Likelihood Functions, Family aggregation, Complex segregation analysis, medicine.disease, Pedigree, Low birth weight, medicine.anatomical_structure, Endocrinology, Multifactorial Inheritance, Female, medicine.symptom, Penis

Abstract

Hypospadias, when the urethra opens on the ventral side of the penis, is a common malformation seen in about 3 per 1000 male births. It is considered a complex disorder with both genetic and environmental factors involved in the pathogenesis. Low birth weight is known to be an important risk factor for hypospadias, but several observations speak in favour of genetic factors as well. In order to delineate the relative contribution of the genetic factors behind hypospadias, we performed a complex segregation analysis of 2005 pedigrees in Sweden. The probands were ascertained through the departments of paediatric surgery and departments of plastic surgery and urology in Sweden where boys with hypospadias undergo surgery. In 7% of the ascertained families one or more additional cases of hypospadias were present. The complex segregation analysis showed a heritability of 0.99 and evidence for multifactorial inheritance. The results suggest that hypospadias might be due to monogenic effects in a small proportion of the families, but that there is a multifactorial cause for the majority of the cases.

Published

2002

25. Analysis of short stature homeobox-containing gene ( SHOX ) and auxological phenotype in dyschondrosteosis and isolated Madelung deformity

Author

Lars Hagenäs, Ove Enkvist, Jacqueline Schoumans, Nils Östen Nilsson, Jan P. Dumanski, Giedre Grigelioniene, Ingegerd Fransson, Isabel Tapia-Páez, Maria Elfving, Lo Neumeyer, Ole Eklöf, Ian O. Ellis, Paul Tordai, Inger Fosdal, Anne Grethe Myhre, Sten A. Ivarsson, Britt-Marie Anderlid, Magnus Nordenskjöld, and Otto Westphal

Subjects

Proband, Nonsense mutation, Biology, Osteochondrodysplasias, Polymerase Chain Reaction, Short stature, Short Stature Homeobox Protein, Gene duplication, Genetics, medicine, Humans, Expressivity (genetics), Léri–Weill dyschondrosteosis, In Situ Hybridization, Fluorescence, Genetics (clinical), Homeodomain Proteins, Langer mesomelic dysplasia, Genes, Homeobox, Syndrome, medicine.disease, Body Height, Blotting, Southern, Phenotype, medicine.symptom

Abstract

Dyschondrosteosis (DCO; also called Léri-Weill syndrome) is a skeletal dysplasia characterised by disproportionate short stature because of mesomelic shortening of the limbs. Madelung deformity is a feature of DCO that is distinctive, variable in expressivity and frequently observed. Mutations of the SHOX (short stature homeobox-containing) gene have been previously described as causative in DCO. Isolated Madelung deformity (IMD) without the clinical characteristics of DCO has also been described in sporadic and a few familial cases but the genetic defect underlying IMD is unknown. In this study, we have examined 28 probands with DCO and seven probands with IMD for mutations in the SHOX gene by using polymorphic CA-repeat analysis, fluorescence in situ hybridisation (FISH), Southern blotting, direct sequencing and fibre-FISH analyses. This was combined with auxological examination of the probands and their family members. Evaluation of the auxological data showed a wide intra- and interfamilial phenotype variability in DCO. Out of 28 DCO probands, 22 (79%) were shown to have mutations in the SHOX gene. Sixteen unrelated DCO families had SHOX gene deletions. Four novel DCO-associated mutations were found in different families. In two additional DCO families, the previously described nonsense mutation (Arg195Stop) was detected. We conclude that mutations in the SHOX gene are the major factor in the pathogenesis of DCO. In a female proband with severe IMD and her unaffected sister, we detected an intrachromosomal duplication of the SHOX gene.

Published

2001

26. Respiratory distress syndrome: evaluation of genetic susceptibility and protection by transmission disequilibrium test

Author

Pekka Uimari, Ritva Haataja, Mika Rämet, Johan Löfgren, Riitta Marttila, and Mikko Hallman

Subjects

Male, Proband, Linkage disequilibrium, Candidate gene, Pulmonary Surfactant-Associated Proteins, Offspring, Proteolipids, Biology, Linkage Disequilibrium, Gene Frequency, Genetics, Genetic predisposition, Humans, Genetic Predisposition to Disease, Allele frequency, Alleles, Genetics (clinical), Genetic association, Respiratory Distress Syndrome, Newborn, Polymorphism, Genetic, Pulmonary Surfactant-Associated Protein A, Infant, Newborn, Pulmonary Surfactants, Transmission disequilibrium test, Haplotypes, Immunology, Female, Infant, Premature

Abstract

Based on epidemiological data and genetic association studies, neonatal respiratory distress syndrome (RDS) is a complex disease with a multigenic background. The genes coding for surfactant proteins (SP) A and B have been assigned as the most likely genes in the etiology of RDS. The major factor predisposing to RDS is prematurity, and thus the phenotype of a very premature newborn infant that does not develop the disease can be regarded as hypernormal. Altogether 107 father-mother-offspring trios were divided into two sets according to the proband's phenotype, to evaluate familial segregation of candidate gene polymorphisms by the transmission disequilibrium test. A set of 76 trios were analyzed for transmission disequilibrium from parents to affected offspring. Another set of 31 trios were studied for allele transmission from parents to hypernormal offspring born very prematurely before the gestational age of 32 weeks. SP-A1-A2 haplotype 6A(2)-1A(0) showed significant excess transmission to affected infants and SP-A1 allele 6A(2) decreased transmission to the hypernormals. The present family study provides strong support for a direct or indirect role of the SP-A alleles as genetic predisposers to RDS in premature infants. The inclusion of parent-hypernormal offspring trios in transmission disequilibrium test is a useful approach to test for genetic protection against a disease.

Published

2001

27. Complex segregation analysis of Parkinson's disease in the Finnish population

Author

Jukka S. Moilanen, Autere Jm, Vilho V. Myllylä, and Kari Majamaa

Subjects

Adult, Male, Proband, Population, Penetrance, Locus (genetics), Biology, Genetic Heterogeneity, Gene Frequency, Prevalence, Genetics, Humans, Family, Age of Onset, education, Nuclear family, Finland, Genetics (clinical), Aged, Aged, 80 and over, Family Health, education.field_of_study, Models, Genetic, Parkinson Disease, Complex segregation analysis, Middle Aged, Major gene, Human genetics, Female

Abstract

The risk of Parkinson's disease (PD) is higher among relatives of affected individuals than among other members of the population, and most family studies have suggested autosomal dominant inheritance, although both autosomal dominant and recessive susceptibility genes have recently been identified. We carried out a complex segregation analysis with POINTER to assess the mode of inheritance of PD in the population of northern Finland. Nuclear families (n=265) were identified through a proband with idiopathic PD. The analysis was first carried out for the total data set, and then the heterogeneity between early-onset (proband under 55 years at onset) and late-onset families was examined. Finally, families with more than one affected individual were analyzed separately. The sporadic model was rejected (P

Published

2001

28. Phenotypic effects of balanced X-autosome translocations in females: a retrospective survey of 104 cases reported from UK laboratories

Author

Paul L. Campbell, Jonathan J. Waters, A. J. Crocker, and Carolyn M. Campbell

Subjects

Adult, Proband, medicine.medical_specialty, X Chromosome, Adolescent, Developmental Disabilities, Biology, Translocation, Genetic, Internal medicine, Recurrent miscarriage, Genetics, medicine, Humans, Abnormalities, Multiple, Child, Genetics (clinical), X chromosome, Aged, Retrospective Studies, Aged, 80 and over, Autosome, Gonadal Disorders, Breakpoint, Cytogenetics, Retrospective cohort study, Publication bias, Middle Aged, medicine.disease, United Kingdom, Phenotype, Child, Preschool, Female, Laboratories

Abstract

Females with balanced X-autosome translocations are a clinically heterogeneous group of patients in which X breakpoint position and replication behaviour may influence phenotypic outcome. This study reviewed all cases reported by UK cytogenetics laboratories over a 15-year period (1983-1997). Publication bias was avoided by reviewing all reported cases. One hundred and four female carriers were identified, 62 of who were probands. By reason for referral, these were: multiple congenital abnormalities and/or developmental delay (MCA/DD): 26 (42%); gonadal dysfunction: 22 (35%); phenotypically normal with or without recurrent miscarriage (NRM): 9 (15%); recognized X-linked syndrome: 5 (8%). The information obtained was compared with published data and with data from the authors' own laboratories of female patients with balanced autosome-autosome translocations (n=115). We concluded that: (1) MCA/DD cases were significantly over-represented compared to previous published data (P0.005) and were more common than in female probands with balanced autosome-autosome translocations (P0.05). (2) MCA/DD cases showed random breakpoint distribution along the X chromosome (P0.05). MCA/DD cases with subtelomeric breakpoints at Xp22 or Xq28 were not always associated with deviation from the expected pattern of X-inactivation where this was known. De novo cases were significantly more likely to be assigned as MCA/DD than any other category (P0.005). (3) Gonadal dysfunction (GD) was invariably associated with a 'critical region' breakpoint, Xq13-q26, (20/22 probands). However, 7/44 (16%) of patients surveyed had breakpoints within Xq13-Xq26 and proven fertility. (4) Recognized 'X-linked syndrome' cases were significantly under-represented (P0.001) compared to previous published data.

Published

2001

29. Interchromosomal insertions

Author

Eussen Hj and Van Hemel Jo

Subjects

Proband, Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Microcephaly, medicine.medical_specialty, Psychomotor retardation, Cytogenetics, Chromosomal translocation, Gene rearrangement, Biology, medicine.disease, Gene duplication, medicine, medicine.symptom, Trisomy, Genetics (clinical)

Abstract

In five families with questionable chromosome rearrangements, we identified an interchromosomal insertion by fluorescent in situ hybridization (FISH). In case 1 with a dir ins (5;11)(p14;q14q24) in three generations, the mentally retarded and microcephalic proband showed a 5p14-->pter deletion. In case 2, a duplication (13)(q21.31--> q31.2) combined with a deletion (11)(q14-->q22) segregated from a reciprocal ins(11;13)(q14q122)(q21.32q31.2), causing a mixed phenotype with psychomotor retardation, caput quadratum, choanal atresia, and pes equinovarus. In case 3, a dir ins (18;5)(q21.3;p13.1p14) was associated with spontaneous abortions, in case 4, the proband with mental retardation, microcephaly, and a heart defect showed a pure trisomy of (12)(q13-->q15), which had segregated from a carrier of an ins (18;12)(p11.3;q13q15). In case 5, a duplication of (10)(q26.3-->q25.2) segregated from an inv ins(5;10)(q15;q26.3q25.2), which was passed on directly from a mother to her son,with mental retardation. In all families the elucidation of the insertional translocation (IT) considerably increased the associated genetic risks of carriers. For the review, we collected data from 81 articles on 87 IT probands on ascertainment, origin, familial transmittance, progeny, and genetic risks of IT carriers. We also discussed the recombinant chromosomes and complex rearrangements associated with ITs, and listed chromosome regions occurring solely as deletions, or solely as duplications, or as both to facilitate genotype/phenotype correlations. We conclude that ITs are rare chromosomal rearrangements with an 1:80,000 incidence, of which nearly 80% were referred because of congenital abnormalities and mental retardation. A maternal origin was seen in 59.5%, a paternal origin in 26.6%, and 13.9% were de novo. No notable difference in fertility between male and female IT carriers was noticed. Bias of ascertainment was excluded in 15 familial cases and led to an estimate of the genetic risks for IT carriers of 32.0-36.0%. The mean size of the inserted regions occurring solely as duplications (n=39) measures 0.96% of the haploid autosomal length (HAL), and of regions solely occurring as deletions (n=14) 0.47% HAL. In the families where both aneusomies occurred, the size of the insertions ranged between 0.22 and 1.21% HAL. Overall, the findings fit with the general idea that a surplus of genetic material is tolerated more easily than a deficiency.

Published

2000

30. Neurofibromatosis pseudogene amplification underlies euchromatic cytogenetic duplications and triplications of proximal 15q

Author

John C K Barber, Ian E. Cross, Fiona Douglas, Caroline E. Browne, Kirk J. Moore, and J.C. Nicholson

Subjects

Male, Proband, medicine.medical_specialty, Adolescent, Euchromatin, Pseudogene, Gene Dosage, Biology, Gene mapping, Genes, Neurofibromatosis 1, Gene duplication, Centromere, Genetics, medicine, Humans, Neurofibromatosis, In Situ Hybridization, Fluorescence, Genetics (clinical), Chromosomes, Human, Pair 15, Gene Amplification, Cytogenetics, Infant, medicine.disease, Chromatin, Chromosome Banding, Pedigree, Karyotyping, Pseudogenes

Abstract

Cytogenetically visible interstitial duplications of proximal 15q, which lack the Prader-Willi Angelman critical region (PWACR) frequently segregate in families without phenotypic effect, but the nature of the extra euchromatin has remained unclear. We used comparative genome hybridisation to confirm that the extra material in a cytogenetic triplication originated from proximal 15q. A PAC clone containing sequences specific for the type-1 neurofibromatosis (NF-1) pseudogenes, which map to 15q11.2, hybridised along the length of the enlarged region between the PWACR and the centromere. Computerised measurement of the fluorescent signal from the enlarged and normal chromosomes gave an average ratio of 9.85:1, consistent with amplification. In a second family, an amplified P1–4 signal co-segregated with a cytogenetic duplication and the average ratio between amplified and normal signals in the proband was 8.22:1. Ratios in non-carrier family members and control individuals were close to unity in most cases, but significantly greater than one in at least one instance. Our results provide a novel explanation for cytogenetic variation in 15q11.2. They also suggest that NF-1 pseudogene copy number may be polymorphic in the normal population, and that high copy numbers can produce G bands which do not reflect those of the normal constitutional karyotype.

Published

1998

31. A high risk phenotype of hypertrophic cardiomyopathy associated with a compound genotype of two mutated β-myosin heavy chain genes

Author

Bernd Weist, Kerstin Uhl, Hans-Peter Vosberg, Thomas Meitinger, Brigitte Jeschke, Dirk Schröder, and C. Döhlemann

Subjects

Male, Proband, Heterozygote, DNA Mutational Analysis, Cardiomyopathy, macromolecular substances, Biology, Compound heterozygosity, Genotype, Genetics, medicine, Humans, Point Mutation, Missense mutation, Age of Onset, Allele, Child, Polymorphism, Single-Stranded Conformational, Genetics (clinical), Myosin Heavy Chains, Hypertrophic cardiomyopathy, Cardiomyopathy, Hypertrophic, medicine.disease, Pedigree, Phenotype, Mutation (genetic algorithm), Female

Abstract

Hypertrophic cardiomyopathy (HCM) is a genetically and clinically heterogeneous myocardial disease that is in most cases familial and transmitted in a dominant fashion. The most frequently affected gene codes for the cardiac (ventricular) beta-myosin heavy chain. We have investigated the genetic cause of an isolated case of HCM, which was marked by an extremely severe phenotype and a very early age of onset. HCM is normally not a disease of small children. The proband was a boy who had suffered cardiac arrest at the age of 6.5 years (resuscitation by cardioconversion). Upon screening of the beta-myosin heavy chain gene as a candidate, two missense mutations, one in exon 19 (Arg719Trp) and a second in exon 12 (Met349Thr), were identified. The Arg719Trp mutation was de novo, as it was not found in the parents. In contrast, the Met349Thr mutation was inherited through the maternal grandmother. Six family members were carriers of this mutation but only the proband was clinically affected. Segregation and molecular analysis allowed us to assign the Met349Thr mutation to the maternal and the Arg719Trp de novo mutation to the paternal beta-myosin allele. Thus, the patient has no normal myosin. We interpret these findings in terms of compound heterozygosity of a dominant (Arg719Trp) and a recessive (Met349Thr) mutation. Whereas a single mutated Arg719Trp allele would be sufficient to cause HCM, the concurrent Met349Thr mutation alone does not apparently induce the disease. Nevertheless, it conceivably contributes to the particularly severe phenotype.

Published

1998

32. Breast cancer risk assessment: use of complete pedigree information and the effect of misspecified ages at diagnosis of affected relatives

Author

Silke Schmidt, Jenny Chang-Claude, and Heiko Becher

Subjects

Adult, Proband, Heterozygote, Genetic counseling, Genes, BRCA1, Breast Neoplasms, Disease, Biology, Risk Assessment, Breast cancer, Genetic model, Genetics, medicine, Humans, Genes, Tumor Suppressor, Interpersonal Relations, Risk factor, Genetics (clinical), Aged, Aged, 80 and over, Estimation, Likelihood Functions, Age Factors, Middle Aged, medicine.disease, Penetrance, Pedigree, Female, Demography

Abstract

Reliable risk estimates for hereditary breast cancer are important for the genetic counseling of women who have one or more first- and/or second-degree relatives affected by the disease. If no mutation analysis of known high-penetrance breast cancer genes is performed, risk estimation is often based on published reference tables. These tables express a woman's age-specific risk of breast cancer as a function of the ages at diagnosis of one or two affected relatives with different degrees of relationship to the counselee. However, unaffected relatives are not taken into account when these estimates are derived. We report here the extent to which risk estimation is influenced by the number and ages of any unaffected relatives and by the exact genealogical relationship between the proband and affected relative rather than merely the degree. Additionally, we describe the sensitivity of risk estimates when ages at diagnosis of affected relatives are misspecified because of inaccurate information supplied by the counselee. We determined a proband's probability of being a carrier of a highly penetrant breast cancer susceptibility gene, such as BRCA1 or BRCA2, by likelihood calculations that take into account information from the entire pedigree. This genetic risk was used to estimate a phenotypic lifetime breast cancer risk, which was compared with the risks derived from the published reference tables. We demonstrate numerically that the tabulated values tend to over-estimate the probands risk and that the extent of over-estimation depends greatly on the number and ages of unaffected relatives. The validity of the relatives ages at diagnosis can affect risk predictions considerably in small families with two or three affected relatives. Furthermore, the magnitude of the estimated breast cancer risks depends upon the assumed genetic model and can therefore vary appreciably when different penetrance estimates are used.

Published

1998

33. Homozygosity by descent for a COL1A2 mutation in two sibs with severe osteogenesis imperfecta and mild clinical expression in the heterozygotes

Author

A. De Paepe, Marc Raes, Lieve Nuytinck, and Jean-Pierre Fryns

Subjects

Male, Proband, Heterozygote, Mutant, Biology, Genetics, medicine, Humans, Missense mutation, Child, Genetics (clinical), Transition (genetics), Homozygote, Infant, Heterozygote advantage, Osteogenesis Imperfecta, medicine.disease, Osteochondrodysplasia, Pedigree, Radiography, Osteogenesis imperfecta, Mutation, Mutation (genetic algorithm), Female, Collagen

Abstract

We report two sibs with severe, progressively deforming osteogenesis imperfecta (OI) and homozygosity by descent for a glycine 751 to serine substitution in the alpha2(I) collagen chain due to a G to A transition in the COL1A2 gene. The parents, who were first cousins, and two elder sibs were heterozygous for the mutation and presented mild clinical manifestations of OI. Collagen studies on cultured fibroblasts from one of the probands and from the father showed that cells from the homozygote produced only mutant, unstable collagen I, whereas cells from the heterozygote produced both normal and mutant collagen I. This family represents an exceptional example of autosomal recessive OI, caused by homozygosity for a missense mutation in collagen I.

Published

1997

34. The contribution of de novo and rare inherited copy number changes to congenital heart disease in an unselected sample of children with conotruncal defects or hypoplastic left heart disease

Author

Ismee A. Williams, Jennie Kline, Michael Ronemus, Chih-yu Yu, Yoon-ha Lee, Dorothy Warburton, Nancy Wong, Danielle Awad, Boris Yamrom, Anthony Leotta, Michael Wigler, Wendy K. Chung, Lan Yu, Jude Kendall, Dan Levy, Vaidehi Jobanputra, and Kwame Anyane-Yeboa

Subjects

Proband, Heart Defects, Congenital, Male, Candidate gene, congenital, hereditary, and neonatal diseases and abnormalities, DNA Copy Number Variations, Biology, Article, Hypoplastic left heart syndrome, DiGeorge syndrome, Gene Duplication, Conotruncal defect, mental disorders, Hypoplastic Left Heart Syndrome, Genetics, medicine, Humans, Copy-number variation, Genetics (clinical), Comparative Genomic Hybridization, Genome, Human, Intracellular Signaling Peptides and Proteins, Infant, Membrane Proteins, Reproducibility of Results, medicine.disease, Penetrance, Child, Preschool, dup, Intercellular Signaling Peptides and Proteins, Female, Gene Deletion

Abstract

Congenital heart disease (CHD) is the most common congenital malformation, with evidence of a strong genetic component. We analyzed data from 223 consecutively ascertained families, each consisting of at least one child affected by a conotruncal defect (CNT) or hypoplastic left heart disease (HLHS) and both parents. The NimbleGen HD2-2.1 comparative genomic hybridization platform was used to identify de novo and rare inherited copy number variants (CNVs). Excluding 10 cases with 22q11.2 DiGeorge deletions, we validated de novo CNVs in 8 % of 148 probands with CNTs, 12.7 % of 71 probands with HLHS and none in 4 probands with both. Only 2 % of control families showed a de novo CNV. We also identified a group of ultra-rare inherited CNVs that occurred de novo in our sample, contained a candidate gene for CHD, recurred in our sample or were present in an affected sibling. We confirmed the contribution to CHD of copy number changes in genes such as GATA4 and NODAL and identified several genes in novel recurrent CNVs that may point to novel CHD candidate loci. We also found CNVs previously associated with highly variable pheno-types and reduced penetrance, such as dup 1q21.1, dup 16p13.11, dup 15q11.2-13, dup 22q11.2, and del 2q23.1. We found that the presence of extra-cardiac anomalies was not related to the frequency of CNVs, and that there was no significant difference in CNV frequency or specificity between the probands with CNT and HLHS. In agreement with other series, we identified likely causal CNVs in 5.6 % of our total sample, half of which were de novo.

Published

2013

35. Whole exome sequencing in dominant cataract identifies a new causative factor, CRYBA2, and a variety of novel alleles in known genes

Author

Leonardo Salviati, Hagith Yonath, Víctor Raggio, Sanaa Muheisen, Sarah Hall, Deborah M. Costakos, Patricia Power, Dennis P. Han, Elena V. Semina, Rebecca C. Tyler, and Linda M. Reis

Subjects

Proband, Adult, Male, DNA Mutational Analysis, Mutation, Missense, Biology, Cataract, Article, beta-Crystallin A Chain, Genetics, medicine, Missense mutation, Animals, Humans, Exome, Allele, Genetics (clinical), Exome sequencing, Alleles, Zebrafish, Genes, Dominant, Genetic heterogeneity, Genetic Diseases, Inborn, Gene Expression Regulation, Developmental, Infant, Zebrafish Proteins, medicine.disease, Penetrance, eye diseases, Amino Acid Substitution, Child, Preschool, Congenital cataracts, Female

Abstract

Pediatric cataracts are observed in 1–15 per 10,000 births with 10–25 % of cases attributed to genetic causes; autosomal dominant inheritance is the most commonly observed pattern. Since the specific cataract phenotype is not sufficient to predict which gene is mutated, whole exome sequencing (WES) was utilized to concurrently screen all known cataract genes and to examine novel candidate factors for a disease-causing mutation in probands from 23 pedigrees affected with familial dominant cataract. Review of WES data for 36 known cataract genes identified causative mutations in nine pedigrees (39 %) in CRYAA, CRYBB1, CRYBB3, CRYGC (2), CRYGD, GJA8 (2), and MIP and an additional likely causative mutation in EYA1; the CRYBB3 mutation represents the first dominant allele in this gene and demonstrates incomplete penetrance. Examination of crystallin genes not yet linked to human disease identified a novel cataract gene, CRYBA2, a member of the βγ-crystallin superfamily. The p.(Val50Met) mutation in CRYBA2 cosegregated with disease phenotype in a four-generation pedigree with autosomal dominant congenital cataracts with incomplete penetrance. Expression studies detected cryba2 transcripts during early lens development in zebrafish, supporting its role in congenital disease. Our data highlight the extreme genetic heterogeneity of dominant cataract as the eleven causative/likely causative mutations affected nine different genes, and the majority of mutant alleles were novel. Furthermore, these data suggest that less than half of dominant cataract can be explained by mutations in currently known genes.

Published

2013

36. A jumping Robertsonian translocation: a molecular and cytogenetic study

Author

Lee P. Shulman, Susan J. Gross, Eniko K. Pivnick, Vicki M. Park, Avirachan T. Tharapel, and Owen P. Phillips

Subjects

Adult, Male, Proband, medicine.medical_specialty, Chromosomes, Human, Pair 21, Chromosomes, Human, Pair 22, Isochromosome, Robertsonian translocation, Chromosomal translocation, Biology, medicine.disease_cause, Translocation, Genetic, Dicentric chromosome, Genetics, medicine, Humans, Child, In Situ Hybridization, Fluorescence, Genetics (clinical), Mosaicism, Cytogenetics, Infant, medicine.disease, Molecular biology, Uniparental disomy, Pedigree, Karyotyping, Female, Down Syndrome, Chromosome 21

Abstract

We report a patient with mosaicism for two different Robertsonian translocations, both involving chromosome 21. She carries an unbalanced cell line with an i(21q) and a balanced cell line with a rob(21q22q). She is phenotypically normal but has two children who inherited the i(21q) and have Down syndrome. We demonstrate that both abnormal chromosomes are dicentric and that the proband's 21/21 rearrangement is an isochromosome formed from a maternally derived chromosome 21. We propose a model in which the i(21q) is the progenitor rearrangement in the proband, which subsequently participated in a nonreciprocal rearrangement characteristic of a jumping translocation. In addition, we review other cases of constitutional mosaicism involving jumping translocations.

Published

1996

37. Mutation analysis of the RET proto-oncogene in Dutch families with MEN 2A, MEN 2B and FMTC: two novel mutations and one de novo mutation for MEN 2A

Author

R.M. Landsvater, Hkp vanAmstel, Robert M.W. Hofstra, Rpm Jansen, Cjm Lips, and Chcm Buys

Subjects

Proband, DNA Mutational Analysis, Molecular Sequence Data, Multiple Endocrine Neoplasia Type 2a, Multiple Endocrine Neoplasia Type 2b, RET proto-oncogene, Biology, Polymerase Chain Reaction, Proto-Oncogene Mas, law.invention, Exon, law, Proto-Oncogene Proteins, Proto-Oncogenes, Genetics, medicine, Drosophila Proteins, Humans, Point Mutation, Amino Acid Sequence, Thyroid Neoplasms, Genetics (clinical), Polymerase chain reaction, DNA Primers, Netherlands, Genetic testing, Base Sequence, medicine.diagnostic_test, Proto-Oncogene Proteins c-ret, Receptor Protein-Tyrosine Kinases, Exons, PROTOONCOGENE, Human genetics, Carcinoma, Medullary, Mutation, Mutation (genetic algorithm), Mutation testing

Abstract

Hereditary C-cell carcinoma is encountered in multiple endocrine neoplasia type 2A (MEN 2A), MEN 2B, and familial medullary thyroid carcinoma (FMTC). Mutations of the RET proto-oncogene are associated with all three diseases. To obtain an insight into the molecular heterogeneity of MEN 2 syndromes and FMTC in the Netherlands, probands of 20 MEN 2A families, two FMTC families, and seven MEN 2B families were analyzed by the polymerase chain reaction (PCR), DNA sequencing, and restriction enzyme digestion for abnormalities in the RET proto-oncogene. RET mutations were found in all cases. All MEN 2A families had a mutation involving one of five cysteine codons in exons 10 and 11 of RET. Two novel dinucleotide mutations and a de novo mutation were found. Both FMTC families had a mutation of the Cys at codon 618. All MEN 2B probands carried a Met to Thr mutation in exon 16. All mutations could be confirmed by restriction enzyme digestion of PCR amplicons. Identification of the RET mutation in the Dutch population with hereditary C-cell carcinoma facilitates genetic testing for families or individuals at risk for MEN 2A, FMTC, and MEN 2B.

Published

1996

38. Acceptability of carrier screening for cystic fibrosis during pregnancy in a German population

Author

U. Jung, K. Grade, Charles Coutelle, and U. Urner

Subjects

Male, Proband, medicine.medical_specialty, Cystic Fibrosis, Genetic counseling, Molecular Sequence Data, Genetic Counseling, Pilot Projects, Prenatal diagnosis, Biology, Cystic fibrosis, Pregnancy, Informed consent, Germany, Prenatal Diagnosis, Genetics, medicine, Humans, Genetic Testing, ΔF508, Genetics (clinical), DNA Primers, Base Sequence, Information Dissemination, Genetic Carrier Screening, Patient Acceptance of Health Care, medicine.disease, Family medicine, Mutation, Anxiety, Female, Pregnant Women, medicine.symptom, Comprehension

Abstract

A pilot project offering voluntary heterozygote screening for the delta F508 mutation causing cystic fibrosis (CF) to 638 pregnant women attending two antenatal clinics in the eastern part of Berlin was carried out from 1990-1993. Participation was invited using an information leaflet and inclusion in the study was conditional on written informed consent. Of those invited to participate, only one refused to be tested, on the grounds of non-acceptance of prenatal diagnosis. Eighteen pregnant women were identified as carriers of the delta F508 mutation. All of them and their male partners accepted counselling in which the genetics of CF, its prognosis and treatment were explained, with emphasis on the meaning of heterozygosity, the fact that carriers are healthy, and the risk of an affected fetus when only one parent is identified as a heterozygote. All partners agreed to be tested for the delta F508 R553X and G551D mutations and a second counselling session was carried out after this test result was available. No problems were observed during initial testing but, as in other studies, we found considerable anxiety on being given the result in all couples where the woman tested positive; this was reduced substantially by counselling and when the partner tested negative. All probands found to be carriers stated that they found screening acceptable. In contrast to the cautious statement by the German Berufsverband Medizinische Genetik and the hostile reaction from a representative of the CF self-support organisation towards community-based heterozygote screening for CF, this study shows that CF screening is generally acceptable in this German population and that it is actively taken up by most pregnant women when offered.

Published

1994

39. Topographic pattern of the rearrangement of the dystrophin gene in Japanese Duchenne muscular dystrophy

Author

Natsuki Imoto, Tadao Arinami, Hitoshi Takita, Kenzo Hamano, Hideo Hamaguchi, Kiichiro Matsumura, and Hiroki Yamada

Subjects

Adult, Male, musculoskeletal diseases, Proband, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Duchenne muscular dystrophy, Biology, Muscular Dystrophies, Dystrophin, Gene Frequency, Japan, Gene duplication, Genetics, medicine, Humans, Muscular dystrophy, Child, Gene, Genetics (clinical), Southern blot, Gene Rearrangement, Intron, Chromosome Mapping, medicine.disease, Europe, Blotting, Southern, Child, Preschool, North America, biology.protein, Female, Chromosome Deletion

Abstract

To compare the frequency and distribution of rearrangements in the dystrophin gene in Duchenne muscular dystrophy (DMD) between Japanese DMD patients and those in North America and Europe, Southern blot analyses of the dystrophin gene were carried out in 88 probands classified as DMD. Gene rearrangements were found in 61 (69%) subjects, and they were composed of partial gene deletions in 53 (60%) probands and partial duplications in 7 (8%) probands. A total deletion of the gene was found in 1 (1%) patient. Among 53 patients with deletions, 34 (64%) had breakpoints between introns 44 and 52 and 7 (13%) had breakpoints between introns 2 and 11. Both the frequency and the distribution of gene rearrangements found in this study were similar to those reported in North America and Europe. These data suggest that there are no ethnic or racial differences in the frequency and distribution of rearrangements thought to be caused by similar mechanisms in the dystrophin gene in all human racial groupings.

Published

1993

40. Spondyloepiphyseal dysplasia and precocious osteoarthritis in a family with an Arg75?Cys mutation in the procollagen type II gene (COL2A1)

Author

Guillermo Neumann, Charlene J. Williams, David Harrison, Sergio A. Jimenez, Paul Buxton, Antonio J. Reginato, E. Considine, Robert G. Knowlton, and Darwin J. Prockop

Subjects

Adult, Male, musculoskeletal diseases, Proband, Spondyloepiphyseal dysplasia, Adolescent, Genetic Linkage, DNA Mutational Analysis, Molecular Sequence Data, Biology, Arginine, Osteochondrodysplasias, Polymerase Chain Reaction, Exon, Osteoarthritis, Genetics, medicine, Humans, Point Mutation, Amino Acid Sequence, Cysteine, Age of Onset, Allele, Child, Genetics (clinical), Aged, DNA Primers, Base Sequence, Point mutation, Middle Aged, medicine.disease, Osteochondrodysplasia, Pedigree, Procollagen peptidase, Mutation (genetic algorithm), Female, Procollagen

Abstract

Direct sequencing of polymerase chain reaction (PCR)-amplified genomic DNA from a patient with spondyloepiphyseal dysplasia and precocious osteoarthritis revealed a single-base change in exon 11 of the type II procollagen gene (COL2A1), which produces an Arg--Cys mutation in one allele. The proband is a member of a large Chilean kindred presenting with chondrodysplasia of the hips, knees, shoulders, elbows, and spine associated with severe, early-onset osteoarthritis. All affected individuals exhibit mildly short stature; in addition, five out of seven affected family members display shortened metacarpals or metatarsals. DNA from affected and unaffected family members was PCR-amplified and analysis of restriction digests of the products determined that the mutation segregated with the disease with a lod score of 2.2 at zero recombination. The mutation, which resides in the triple-helical region of type II procollagen at amino acid position 75, is the second example of an Arg--Cys mutation in the COL2A1 gene in heritable cartilaginous disease and is the first example of a point mutation in the amino terminal region of the alpha 1(II) chain, that results in a spondyloepiphyseal dysplastic phenotype.

Published

1993

41. Evidence for inheritance in patients with VACTERL association

Author

Manu S. Raam, Derek A. T. Cummings, Daniel E. Pineda-Alvarez, and Benjamin D. Solomon

Subjects

Proband, Male, Pediatrics, medicine.medical_specialty, Heredity, Population, Biology, medicine.disease_cause, Article, Genetics, medicine, Prevalence, Humans, Abnormalities, Multiple, Family, Genetic Testing, education, Genetics (clinical), Genetic testing, education.field_of_study, medicine.diagnostic_test, Inheritance (genetic algorithm), medicine.disease, VACTERL association, Human genetics, Etiology, Female

Abstract

VACTERL/VATER association is typically a sporadic disorder. We present data on inheritance in 78 probands with VACTERL association, and show that 9% of probands have a primary relative with at least one component feature of VACTERL association. The prevalence of component features in first-degree relatives is significantly higher than expected in the general population, which has implications for counseling of affected families and for research into possible etiologies.

Published

2009

42. Linkage and sequence analysis indicate that CCBE1 is mutated in recessively inherited generalised lymphatic dysplasia

Author

Glen Brice, Sahar Mansour, Fiona Connell, Pia Ostergaard, Peter S. Mortimer, Lesley Roberts, Tessa Homfray, David J. Bunyan, Sally Mitton, Kamini Kalidas, and Steve Jeffery

Subjects

Proband, Male, Genotype, Genetic Linkage, DNA Mutational Analysis, Locus (genetics), Genes, Recessive, Biology, Polymorphism, Single Nucleotide, Fatal Outcome, Chromosome 18, Genetic linkage, Hydrops fetalis, Genetics, medicine, Humans, Genetic Predisposition to Disease, Lymphedema, Fetal Death, Genetics (clinical), Family Health, Base Sequence, Tumor Suppressor Proteins, Calcium-Binding Proteins, Chromosome Mapping, Infant, medicine.disease, Lymphangiogenesis, Pedigree, Dysplasia, Mutation, Female, Chromosomes, Human, Pair 18, SNP array

Abstract

Generalised lymphatic dysplasia (GLD) is characterised by extensive peripheral lymphoedema with visceral involvement. In some cases, it presents in utero with hydrops fetalis. Autosomal dominant and recessive inheritance has been reported. A large, non-consanguineous family with three affected siblings with generalised lymphatic dysplasia is presented. One child died aged 5 months, one spontaneously miscarried at 17 weeks gestation, and the third has survived with extensive lymphoedema. All three presented with hydrops fetalis. There are seven other siblings who are clinically unaffected. Linkage analysis produced two loci on chromosome 18, covering 22 Mb and containing 150 genes, one of which is CCBE1. A homozygous cysteine to serine change in CCBE1 has been identified in the proband, in a residue that is conserved across species. High density SNP analysis revealed homozygosity (a region of 900 kb) around the locus for CCBE1 in all three affected cases. This indicates a likely ancestral mutation that is common to both parents; an example of a homozygous mutation representing Identity by Descent (IBD) in this pedigree. Recent studies in zebrafish have shown this gene to be required for lymphangiogenesis and venous sprouting and are therefore supportive of our findings. In view of the conserved nature of the cysteine, the nature of the amino acid change, the occurrence of a homozygous region around the locus, the segregation within the family, and the evidence from zebrafish, we propose that this mutation is causative for the generalised lymphatic dysplasia in this family, and may be of relevance in cases of non-immune hydrops fetalis.

Published

2009

43. Mutations in the VNTR of the carboxyl-ester lipase gene (CEL) are a rare cause of monogenic diabetes

Author

Torben Hansen, Andrew T. Hattersley, Jayne A. L. Minton, Sian Ellard, Anders Johansen, Pål R. Njølstad, Anders Molven, Oluf Pedersen, Jakob Ek, Janniche Torsvik, Stefan Johansson, and Helge Ræder

Subjects

Proband, Adult, Male, Minisatellite Repeat, Denmark, DNA Mutational Analysis, Minisatellite Repeats, Biology, medicine.disease_cause, Gene Frequency, Genetics, medicine, Humans, Allele, Allele frequency, Gene, Genetics (clinical), Alleles, Aged, Family Health, Mutation, Great Britain, Lipase, Middle Aged, Molecular biology, Human genetics, United Kingdom, Pedigree, Variable number tandem repeat, Diabetes Mellitus, Type 2, Female

Abstract

Udgivelsesdato: 2010-Jan We have previously shown that heterozygous single-base deletions in the carboxyl-ester lipase (CEL) gene cause exocrine and endocrine pancreatic dysfunction in two multigenerational families. These deletions were found in the first and fourth repeats of a variable number of tandem repeats (VNTR), which has proven challenging to sequence due to high GC-content and considerable length variation. We have therefore developed a screening method consisting of a multiplex PCR followed by fragment analysis. The method detected putative disease-causing insertions and deletions in the proximal repeats of the VNTR, and determined the VNTR-length of each allele. When blindly testing 56 members of the two families with known single-base deletions in the CEL VNTR, the method correctly assessed the mutation carriers. Screening of 241 probands from suspected maturity-onset diabetes of the young (MODY) families negative for mutations in known MODY genes (95 individuals from Denmark and 146 individuals from UK) revealed no deletions in the proximal repeats of the CEL VNTR. However, we found one Danish patient with a short, novel CEL allele containing only three VNTR repeats (normal range 7-23 in healthy controls). This allele co-segregated with diabetes or impaired glucose tolerance in the patient's family as six of seven mutation carriers were affected. We also identified individuals who had three copies of a complete CEL VNTR. In conclusion, the CEL gene is highly polymorphic, but mutations in CEL are likely to be a rare cause of monogenic diabetes.

Published

2009

44. The importance of further cytogenetic and molecular investigation of acrocentric variants: justification by presentation of a case [t(8;14)(q24;p11)]

Author

M. Wilson, Elizabeth D. Earle, David M. Danks, Margaret Leversha, Louise Hills, Vida Petrovic, Lucille Voullaire, and Choo Kh

Subjects

Male, Proband, medicine.medical_specialty, Adolescent, Secondary constriction, Chromosomal translocation, Biology, Translocation, Genetic, Intellectual Disability, Centromere, Genetics, medicine, Humans, Genetics (clinical), Chromosomes, Human, Pair 14, Breakpoint, Cytogenetics, Nucleic Acid Hybridization, Chromosome, Karyotype, Chromosome Banding, Phenotype, Karyotyping, DNA Probes, Chromosomes, Human, Pair 8

Abstract

On routine chromosome analysis a moderately retarded 18-year-old man was found to have an unusual short arm on one chromosome 14. With GTL-banding this chromosome showed an enlarged short arm with no evident secondary constriction. Negative CBG-banding of the short arm suggested the possibility of a translocation involving euchromatin. Interpretation of the abnormality as an unbalanced translocation relied on chromosome analysis using GTL-, CBG-, and Ag-NOR-banding of the proband's phenotypically normal mother, who was found to be carrying a balanced translocation involving chromosomes 8 and 14. In situ hybridization of sequences known to map to the short arm of chromosome 14 confirmed the interpretation and established that the breakpoint was within p11. The patient, whose karyotype is 46,XY, -14, +der(14)t(8;14)(q24.1;p11), is trisomic for the terminal end of the long arm of chromosome 8. The patient's clinical features are described and compared with those reported in patients trisomic for this region. This study demonstrates the importance of using a number of different banding techniques in conjunction with in situ hybridization for the investigation of morphologically unusual acrocentric short arm variants seen at routine diagnosis.

Published

1991

45. A novel missense mutation in exon 8 of the ornithine transcarbamylase gene in two unrelated male patients with mild ornithine transcarbamylase deficiency

Author

Akira Hata, T Yokoi, Ichiro Matsuda, Chiaki Setoyama, Kazuniro Shimada, Izumi Akaboshi, and Toshinobu Matsuura

Subjects

Male, Proband, Heterozygote, Genotype, Molecular Sequence Data, Ornithine Carbamoyltransferase Deficiency Disease, Ornithine transcarbamylase, Biology, Arginine, Exon, Ornithine Carbamoyltransferase, Genetics, medicine, Humans, Missense mutation, Amino Acid Sequence, Alleles, Genetics (clinical), Ornithine transcarbamylase deficiency, Orotic Acid, Base Sequence, Point mutation, Tryptophan, Infant, Nucleic Acid Hybridization, Exons, medicine.disease, Molecular biology, Pedigree, Mutation, Oligonucleotide Probes

Abstract

We studied two unrelated male probands with mild ornithine transcarbamylase (OTC) (E.C.2.1.3.3) deficiency presenting a similar clinical course. Previous analyses of their liver OTCs also revealed similar properties. To identify the underlying molecular defects, we first cloned the entire coding region of the OTC gene from one proband and found a single base-substitution (C to T) leading to the substitution of tryptophan for arginine at amino acid position 277. Using a genomic amplification technique followed by allele specific oligonucleotide hybridization, we identified the same point mutation in the OTC gene of the other proband. We observed the presence of the mutation among family members in at least three generations, and in one asymptomatic hemizygous sibling in each family.

Published

1991

46. PHEX analysis in 118 pedigrees reveals new genetic clues in hypophosphatemic rickets

Author

Frédéric Jehan, Odile Walrant-Debray, Thy-Minh Nguyen, Céline Gaucher, Laure Esterle, and Michèle Garabédian

Subjects

Proband, Male, Models, Molecular, Protein Conformation, DNA Mutational Analysis, Mutation, Missense, Biology, medicine.disease_cause, Frameshift mutation, Cohort Studies, Genetics, medicine, Missense mutation, Humans, Frameshift Mutation, Genetics (clinical), DNA Primers, Sequence Deletion, Mutation, Base Sequence, PHEX, Genetic Diseases, X-Linked, DNA, PHEX Phosphate Regulating Neutral Endopeptidase, Human genetics, Introns, Pedigree, Familial Hypophosphatemic Rickets, Hypophosphatemic Rickets, Mutagenesis, Insertional, Codon, Nonsense, Female, RNA Splice Sites, 5' Untranslated Regions

Abstract

Familial hypophosphatemic rickets is a rare disease, which is mostly transmitted as an X-linked dominant trait, and mutations on the phosphate regulating gene with homologies to endopeptidases on the X-chromosome (PHEX) gene are responsible for the disease in most familial cases. In this study we analyzed PHEX in a large cohort of 118 pedigrees representing 56 familial cases and 62 sporadic cases. The high-resolution melting curves technique was tested as a screening method, along with classical sequencing. PHEX mutations have been found in 87% of familial cases but also in 72% of sporadic cases. Missense mutations were found in 16 probands, two of which being associated with other PHEX mutations resulting into truncated proteins. By plotting missense mutations described so far on a 3D model of PHEX we observed that these mutations focus on two regions located in the inner part of the PHEX protein. Family members of 13 sporadic cases were analyzed and a PHEX mutation was detected in one of the apparently healthy mother. These results highlight the major role of PHEX in X-linked dominant hypophosphatemic rickets, and give new clues regarding the genetic analysis of the disease. A screening of the different family members should be mandatory when a PHEX mutation is assessed in a sporadic case and the search for another PHEX mutation should be systematically proceed when facing a missense mutation.

Published

2008

47. Investigation of the origins of human autosomal inversions

Author

N. Simon Thomas, Victoria Bryant, Annette E. Cockwell, Patricia A. Jacobs, and Vivienne Maloney

Subjects

Proband, Genetics, Chromosomes, Human, Pair 14, Recombination, Genetic, Autosome, Chromosomes, Human, Pair 10, Haplotype, Breakpoint, Chromosome Mapping, Chromosome Breakage, Biology, Identity by descent, Chromosomal crossover, Haplotypes, Chromosome Inversion, Cytogenetic Analysis, Chromosomes, Human, Pair 5, Humans, Chromosome breakage, Genetics (clinical), Gene Deletion, Chromosomal inversion

Abstract

A significant proportion of both pericentric and paracentric inversions have recurrent breakpoints and so could either have arisen through multiple independent events or be identical by descent (IBD) with a single common ancestor. Of two common variant inversions previously studied, the inv(2)(p11q13) was genuinely recurrent while the inv(10)(p11.2q21.2) was IBD in all cases tested. Excluding these two variants we have ascertained 257 autosomal inversion probands at the Wessex Regional Genetics Laboratory. There were 104 apparently recurrent inversions, representing 35 different breakpoint combinations and we speculated that at least some of these had arisen on more than one occasion. However, haplotype analysis identified no recurrent cases among eight inversions tested, including the variant inv(5)(p13q13). The cases not IBD were shown to have different breakpoints at the molecular cytogenetic level. No crossing over was detected within any of the inversions and the founder haplotypes extended for variable distances beyond the inversion breakpoints. Defining breakpoint intervals by FISH mapping identified no obvious predisposing elements in the DNA sequence. In summary the vast majority of human inversions arise as unique events. Even apparently recurrent inversions, with the exception of the inv(2)(p12q13), are likely to be either derived from a common ancestor or to have subtly different breakpoints. Presumably the lack of selection against most inversions allows them to accumulate and disperse amongst different populations over time.

Published

2008

48. Apolipoprotein A1 Baltimore (Arg10→Leu), a new ApoA1 variant

Author

Stylianos E. Antonarakis, Hazel H. Smith, John A. A. Ladias, Peter O. Kwiterovich, and Sotirios K. Karathanasis

Subjects

Adult, Male, Proband, Adolescent, TaqI, Molecular Sequence Data, Mutant, Biology, Polymerase Chain Reaction, Exon, chemistry.chemical_compound, Genetics, medicine, Humans, Electrophoresis, Gel, Two-Dimensional, Amino Acid Sequence, Child, Deoxyribonucleases, Type II Site-Specific, Hypoalphalipoproteinemia, Apolipoproteins A, Genetics (clinical), Apolipoprotein A-I, Base Sequence, Middle Aged, medicine.disease, Pedigree, genomic DNA, Restriction site, chemistry, Mutation, Mutation (genetic algorithm), Female, lipids (amino acids, peptides, and proteins)

Abstract

A new apolipoprotein A1 (APOA1) gene variant has been identified in a family ascertained through a proband undergoing coronary angiography. The variant, ApoA1 Baltimore, was due to a mutation at codon 34 of the third exon of the APOA1 gene (CGA to CTA) that resulted in an arginine-to-leucine substitution at the tenth amino acid of the mature ApoA1 and a change in charge of -1. The mutation abolishes a TaqI restriction site and it is easily detectable after polymerase chain reaction amplification of genomic DNA. The proband was heterozygous for the mutation. Eight other members of the pedigree had the same ApoA1 variant. Cosegregation of the variant with hypoalphalipoproteinemia could not be demonstrated and the association of this mutation with hypoalphalipoproteinemia was confined to three affected members of the nuclear family. No effect of the mutant on any lipoprotein phenotype could be established.

Published

1990

49. Inheritance of chronic tension-type headache investigated by complex segregation analysis

Author

Jes Olesen, Lennart Iselius, Steen Østergaard, and MB Russell

Subjects

Male, Proband, Pediatrics, medicine.medical_specialty, Tension headache, Denmark, media_common.quotation_subject, Chronic tension-type headache, Neurological disorder, Biology, Nuclear Family, Sex Factors, Genetics, medicine, Humans, Genetics (clinical), media_common, Models, Genetic, Tension-Type Headache, Age Factors, Complex segregation analysis, medicine.disease, Logistic Models, Chronic disease, Chronic Disease, Multifactorial Inheritance, Female, Inheritance

Abstract

We investigated the mode of inheritance of chronic tension-type headache in 122 families. The probands were from the Copenhagen Headache Clinic, Denmark. The criteria of the International Headache Society were used. The patterns of segregation of chronic tension-type headache were assessed by complex segregation analysis performed with the computer program POINTER. Of the 122 probands with chronic tension-type headache, 56 had 71 first-degree relatives with chronic tension-type headache. The complex segregation analysis indicates that chronic tension-type headache has multifactorial inheritance.

Published

1998

50. Sequence variant in the laminin gamma1 (LAMC1) gene associated with familial pelvic organ prolapse

Author

Stanley F. Nelson, Eric Vilain, Janet Sinsheimer, Ganka Nikolova, Larissa V. Rodriguez, Hane Lee, and Suzanne Berkovitz

Subjects

Proband, Male, Candidate gene, Population, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Cohort Studies, Gene Frequency, Polymorphism (computer science), Uterine Prolapse, Genetics, SNP, Humans, education, Promoter Regions, Genetic, Allele frequency, Genotyping, Genetics (clinical), DNA Primers, Oligonucleotide Array Sequence Analysis, education.field_of_study, Binding Sites, Base Sequence, Chromosome Mapping, Genetic Variation, DNA, Pedigree, Basic-Leucine Zipper Transcription Factors, Female, Laminin

Abstract

Pelvic organ prolapse is a common condition, affecting up to a third of women throughout their lifetime. Genetic factors are believed to account for about 30% of the incidence, and are the least understood component of the disorder. Familial cases, particularly those in which prolapse manifests in young women, are especially valuable in the effort to find the genes involved. We recently reported autosomal dominant transmission as the most likely mode of inheritance, based on a collection of families with high incidence of prolapse. Of greatest interest was a family in which three generations of female relatives suffered from prolapse at a very young age. A genome-wide linkage scan performed using the Affymetrix GeneChip Human mapping 10K array identified ten regions with a LOD score of 1.5, the maximum possible for this family. Candidate genes within those regions were analyzed for expression in vaginal tissue by RT-PCR. Of the genes confirmed to be expressed, LAMC1 was further evaluated by sequencing and select single nucleotide polymorphism (SNP) genotyping for causative sequence variants in affected family members. We identified one such SNP, rs10911193. The rare T variant segregating with the condition is present at a frequency of 4.9% in the general population and 22% among probands from our cohort of families. It affects the binding site for NFIL3, a transcription factor that we verified to be co-expressed in vaginal tissue. Altogether these data suggest that a polymorphism in the promoter of LAMC1 may increase the susceptibility to early-onset pelvic organ prolapse.

Published

2006