Your search keyword '"Indira B. Taylor"' showing total 13 results

1. A biallelic mutation in

Author

Tobias, Schwerd, Stephen R F, Twigg, Dominik, Aschenbrenner, Santiago, Manrique, Kerry A, Miller, Indira B, Taylor, Melania, Capitani, Simon J, McGowan, Elizabeth, Sweeney, Astrid, Weber, Liye, Chen, Paul, Bowness, Andrew, Riordan, Andrew, Cant, Alexandra F, Freeman, Joshua D, Milner, Steven M, Holland, Natalie, Frede, Miryam, Müller, Dirk, Schmidt-Arras, Bodo, Grimbacher, Steven A, Wall, E Yvonne, Jones, Andrew O M, Wilkie, and Holm H, Uhlig

Subjects

Interleukin-6, Interleukins, Immunologic Deficiency Syndromes, Mutation, Missense, Brief Definitive Report, Interleukin-11, Craniosynostoses, Child, Preschool, Cytokine Receptor gp130, Humans, Exome, Female, Research Articles

Abstract

Schwerd et al. report a novel homozygous missense substitution in the cytokine co-receptor GP130 encoded by IL6ST. This is associated with defective IL-6, IL-11, OSM, and IL-27 signaling and causes immunodeficiency and skeletal abnormalities with similarities to STAT3 hyper-IgE syndrome., Multiple cytokines, including interleukin 6 (IL-6), IL-11, IL-27, oncostatin M (OSM), and leukemia inhibitory factor (LIF), signal via the common GP130 cytokine receptor subunit. In this study, we describe a patient with a homozygous mutation of IL6ST (encoding GP130 p.N404Y) who presented with recurrent infections, eczema, bronchiectasis, high IgE, eosinophilia, defective B cell memory, and an impaired acute-phase response, as well as skeletal abnormalities including craniosynostosis. The p.N404Y missense substitution is associated with loss of IL-6, IL-11, IL-27, and OSM signaling but a largely intact LIF response. This study identifies a novel immunodeficiency with phenotypic similarities to STAT3 hyper-IgE syndrome caused by loss of function of GP130.

Published

2016

2. Genetic screening of 202 individuals with congenital limb malformations and requiring reconstructive surgery

Author

Henk Giele, David Johnson, Paul Critchley, Dominic Furniss, Andrew O.M. Wilkie, Shih-hsin Kan, and Indira B. Taylor

Subjects

Original article, Candidate gene, medicine.medical_specialty, Reconstructive surgery, animal structures, DNA Mutational Analysis, Limb Deformities, Congenital, Biology, Denaturing high performance liquid chromatography, Cohort Studies, 03 medical and health sciences, Molecular genetics, Internal medicine, Genetics, medicine, Humans, Genetic Testing, Multiplex ligation-dependent probe amplification, Child, Genetics (clinical), 030304 developmental biology, Genetic testing, 0303 health sciences, medicine.diagnostic_test, 030305 genetics & heredity, Plastic Surgery Procedures, 3. Good health, Karyotyping, Cohort, embryonic structures, Cohort study

Abstract

Background: Congenital limb malformations (CLMs) are common and present to a variety of specialties, notably plastic and orthopaedic surgeons, and clinical geneticists. The authors aimed to characterise causative mutations in an unselected cohort of patients with CLMs requiring reconstructive surgery. Methods: 202 patients presenting with CLM were recruited. The authors obtained G-banded karyotypes and screened EN1 , GLI3 , HAND2 , HOXD13 , ROR2 , SALL1 , SALL4 , ZRS of SHH , SPRY4 , TBX5 , TWIST1 and WNT7A for point mutations using denaturing high performance liquid chromatography (DHPLC) and direct sequencing. Multiplex ligation dependent probe amplification (MLPA) kits were developed and used to measure copy number in GLI3 , HOXD13 , ROR2 , SALL1 , SALL4, TBX5 and the ZRS of SHH . Results: Within the cohort, causative genetic alterations were identified in 23 patients (11%): mutations in GLI3 (n = 5), HOXD13 (n = 5), the ZRS of SHH (n = 4), and chromosome abnormalities (n = 4) were the most common lesions found. Clinical features that predicted the discovery of a genetic cause included a bilateral malformation, positive family history, and having increasing numbers of limbs affected (all p

Published

2016

3. Mutations in CDC45, Encoding an Essential Component of the Pre-initiation Complex, Cause Meier-Gorlin Syndrome and Craniosynostosis

Author

Kerry A. Miller, Gijs W. E. Santen, Anne Goriely, Alice Gardham, Andrew O.M. Wilkie, Clare V. Logan, Maciej Kliszczak, Deepthi De Silva, Ravi Savarirayan, Donna M. McDonald-McGinn, Stephen R.F. Twigg, Olivier Vanakker, Chris P. Ponting, Louise S. Bicknell, Sumita Danda, Wojciech Niedzwiedz, Elaine H. Zackai, Ozge Ozalp Yuregir, Solaf M. Elsayed, Ezzat Elsobky, Jennie E. Murray, Fay Cooper, Mariëtte J.V. Hoffer, Louise C. Wilson, Andrew P. Jackson, Marije Koopmans, Simon J. McGowan, Luis Sanchez-Pulido, Sevcan Tug Bozdogan, Aimee L. Fenwick, Indira B. Taylor, Steven A. Wall, and Joanne Dixon

Subjects

0301 basic medicine, Male, Models, Molecular, Protein Conformation, DNA Mutational Analysis, Eukaryotic DNA replication, Cell Cycle Proteins, 030105 genetics & heredity, medicine.disease_cause, DNA replication factor CDT1, ORC6, Genetics(clinical), Exome, Child, Genetics (clinical), Cells, Cultured, Growth Disorders, Genetics, Mutation, Exons, Patella, Syndrome, Child, Preschool, Female, Adult, DNA Replication, Adolescent, Micrognathism, Biology, Article, Cell Line, 03 medical and health sciences, Craniosynostoses, Young Adult, Minichromosome maintenance, medicine, Humans, Amino Acid Sequence, Amnion, Alleles, Genetic Association Studies, Congenital Microtia, DNA replication, DNA replication origin, Alternative Splicing, 030104 developmental biology, biology.protein, Origin recognition complex

Abstract

DNA replication precisely duplicates the genome to ensure stable inheritance of genetic information. Impaired licensing of origins of replication during the G1 phase of the cell cycle has been implicated in Meier-Gorlin syndrome (MGS), a disorder defined by the triad of short stature, microtia, and a/hypoplastic patellae. Biallelic partial loss-of-function mutations in multiple components of the pre-replication complex (preRC; ORC1, ORC4, ORC6, CDT1, or CDC6) as well as de novo stabilizing mutations in the licensing inhibitor, GMNN, cause MGS. Here we report the identification of mutations in CDC45 in 15 affected individuals from 12 families with MGS and/or craniosynostosis. CDC45 encodes a component of both the pre-initiation (preIC) and CMG helicase complexes, required for initiation of DNA replication origin firing and ongoing DNA synthesis during S-phase itself, respectively, and hence is functionally distinct from previously identified MGS-associated genes. The phenotypes of affected individuals range from syndromic coronal craniosynostosis to severe growth restriction, fulfilling diagnostic criteria for Meier-Gorlin syndrome. All mutations identified were biallelic and included synonymous mutations altering splicing of physiological CDC45 transcripts, as well as amino acid substitutions expected to result in partial loss of function. Functionally, mutations reduce levels of full-length transcripts and protein in subject cells, consistent with partial loss of CDC45 function and a predicted limited rate of DNA replication and cell proliferation. Our findings therefore implicate the preIC as an additional protein complex involved in the etiology of MGS and connect the core cellular machinery of genome replication with growth, chondrogenesis, and cranial suture homeostasis.

Published

2016

4. Activating mutations in FGFR3 and HRAS reveal a shared genetic origin for congenital disorders and testicular tumors

Author

Indira B. Taylor, Ruth M. S. Hansen, Andrew O.M. Wilkie, G K Jacobsen, Anne Goriely, Inge A. Olesen, Simon J. McGowan, Gilean McVean, Susanne P. Pfeifer, and Ewa Rajpert-De Meyts

Subjects

Adult, Male, medicine.risk_factor, Thanatophoric dysplasia, Somatic cell, Biology, medicine.disease_cause, Testicular Diseases, Article, Germline, 03 medical and health sciences, Age Distribution, 0302 clinical medicine, Germline mutation, Testicular Neoplasms, Genetics, medicine, Humans, Receptor, Fibroblast Growth Factor, Type 3, Genetic Predisposition to Disease, HRAS, Paternal age effect, Aged, 030304 developmental biology, Aged, 80 and over, 0303 health sciences, Mutation, Base Sequence, Middle Aged, medicine.disease, Spermatozoa, Phenotype, 3. Good health, Genes, ras, 030220 oncology & carcinogenesis

Abstract

Genes mutated in congenital malformation syndromes are frequently implicated in oncogenesis, but the causative germline and somatic mutations occur in separate cells at different times of an organism's life. Here we unify these processes to a single cellular event for mutations arising in male germ cells that show a paternal age effect. Screening of 30 spermatocytic seminomas for oncogenic mutations in 17 genes identified 2 mutations in FGFR3 (both 1948A>G, encoding K650E, which causes thanatophoric dysplasia in the germline) and 5 mutations in HRAS. Massively parallel sequencing of sperm DNA showed that levels of the FGFR3 mutation increase with paternal age and that the mutation spectrum at the Lys650 codon is similar to that observed in bladder cancer. Most spermatocytic seminomas show increased immunoreactivity for FGFR3 and/or HRAS. We propose that paternal age-effect mutations activate a common 'selfish' pathway supporting proliferation in the testis, leading to diverse phenotypes in the next generation including fetal lethality, congenital syndromes and cancer predisposition.

Published

2009

5. A variant in the sonic hedgehog regulatory sequence (ZRS) is associated with triphalangeal thumb and deregulates expression in the developing limb

Author

Laura A. Lettice, Paul Critchley, Indira B. Taylor, Robert E. Hill, Henk Giele, Dominic Furniss, and Andrew O.M. Wilkie

Subjects

Male, Triphalangeal thumb, Genetic Linkage, Molecular Sequence Data, Locus (genetics), Mice, Transgenic, Cohort Studies, 03 medical and health sciences, Mice, Genetics, medicine, Animals, Humans, Genetics(clinical), Hedgehog Proteins, Sonic hedgehog, Allele, Enhancer, Molecular Biology, Genetics (clinical), 030304 developmental biology, 0303 health sciences, biology, Polydactyly, Base Sequence, 030305 genetics & heredity, Haplotype, Gene Expression Regulation, Developmental, Extremities, General Medicine, Articles, medicine.disease, Penetrance, Pedigree, Enhancer Elements, Genetic, Haplotypes, Mutation, biology.protein, Female, Hand Deformities, Congenital, Sequence Alignment, Chromosomes, Human, Pair 7, Microsatellite Repeats

Abstract

A locus for triphalangeal thumb, variably associated with pre-axial polydactyly, was previously identified in the zone of polarizing activity regulatory sequence (ZRS), a long range limb-specific enhancer of the Sonic Hedgehog (SHH) gene at human chromosome 7q36.3. Here, we demonstrate that a 295T>C variant in the human ZRS, previously thought to represent a neutral polymorphism, acts as a dominant allele with reduced penetrance. We found this variant in three independently ascertained probands from southern England with triphalangeal thumb, demonstrated significant linkage of the phenotype to the variant (LOD = 4.1), and identified a shared microsatellite haplotype around the ZRS, suggesting that the probands share a common ancestor. An individual homozygous for the 295C allele presented with isolated bilateral triphalangeal thumb resembling the heterozygous phenotype, suggesting that the variant is largely dominant to the wild-type allele. As a functional test of the pathogenicity of the 295C allele, we utilized a mutated ZRS construct to demonstrate that it can drive ectopic anterior expression of a reporter gene in the developing mouse forelimb. We conclude that the 295T>C variant is in fact pathogenic and, in southern England, appears to be the most common cause of triphalangeal thumb. Depending on the dispersal of the founding mutation, it may play a wider role in the aetiology of this disorder.

Published

2008

6. Clinical dividends from the molecular genetic diagnosis of craniosynostosis

Author

Jane A. Hurst, Margarida Venâncio, Sahan V. Rannan-Eliya, Tracy Lester, Lina Ramos, A O'Rourke, Elena G. Bochukova, Anneke Seller, Louise J. Williams, Jo C. Byren, Indira B. Taylor, Ruth M. S. Hansen, Andrew O.M. Wilkie, and Steven A. Wall

Subjects

Adult, Male, Mental development, DNA Mutational Analysis, Biology, Bioinformatics, Recurrence risk, Craniosynostosis, Craniosynostoses, Recurrence, Risk Factors, Genetics, medicine, Humans, Genetic Testing, Multiplex ligation-dependent probe amplification, Genetics (clinical), Dysostosis, Middle Aged, Prognosis, medicine.disease, Penetrance, Pedigree, Child, Preschool, Mutation, Mutation (genetic algorithm), Female, Genetic diagnosis

Abstract

A dozen years have passed since the first genetic lesion was identified in a family with craniosynostosis, the premature fusion of the cranial sutures. Subsequently, mutations in the FGFR2, FGFR3, TWIST1, and EFNB1 genes have been shown to account for approximately 25% of craniosynostosis, whilst several additional genes make minor contributions. Using specific examples, we show how these discoveries have enabled refinement of information on diagnosis, recurrence risk, prognosis for mental development, and surgical planning. However, phenotypic variability can present a significant challenge to the clinical interpretation of molecular genetic tests. In particular, the difficulty of analyzing the complex interaction of genetic background and prenatal environment in determining clinical features, limits the value of identifying low penetrance mutations. (c) 2007 Wiley-Liss, Inc.

Published

2006

7. The origin of EFNB1 mutations in craniofrontonasal syndrome: Frequent somatic mosaicism and explanation of the paucity of carrier males

Author

Indira B. Taylor, Anne Goriely, Andrew O.M. Wilkie, Irene M.J. Mathijssen, A. Jeannette M. Hoogeboom, Jenny Morton, Richard B. Fisher, Louise C. Wilson, Elizabeth Sweeney, Alexa Kidd, John B. Mulliken, M. Teresa Lourenço, Steven A. Wall, Kazuya Matsumoto, Stephen R.F. Twigg, Han G. Brunner, Clinical Genetics, and Plastic and Reconstructive Surgery and Hand Surgery

Subjects

Male, Heterozygote, Genetics and epigenetic pathways of disease [NCMLS 6], Genetic counseling, Germline mosaicism, Ephrin-B1, Biology, medicine.disease_cause, Germline, Craniofacial Abnormalities, Genomic disorders and inherited multi-system disorders [IGMD 3], 03 medical and health sciences, Germline mutation, Genetics, medicine, Humans, Genetics(clinical), Hypertelorism, Allele, Frontonasal dysplasia, 10. No inequality, Germ-Line Mutation, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Mutation, Mosaicism, 030305 genetics & heredity, Articles, medicine.disease, Pedigree, Genetic defects of metabolism [UMCN 5.1], Female, medicine.symptom

Abstract

Contains fulltext : 51037.pdf (Publisher’s version ) (Closed access) Craniofrontonasal syndrome (CFNS) is an X-linked disorder that exhibits a paradoxical sex reversal in phenotypic severity: females characteristically have frontonasal dysplasia, craniosynostosis, and additional minor malformations, but males are usually mildly affected with hypertelorism only. Despite this, males appear underrepresented in CFNS pedigrees, with carrier males encountered infrequently compared with affected females. To investigate these unusual genetic features of CFNS, we exploited the recent discovery of causative mutations in the EFNB1 gene, which encodes ephrin-B1, to survey the molecular alterations in 59 families (39 newly investigated and 20 published elsewhere). We identified the first complete deletions of EFNB1, catalogued 27 novel intragenic mutations, and used Pyrosequencing and analysis of nearby polymorphic alleles to quantify mosaic cases and to determine the parental origin of verified germline mutations. Somatic mosaicism was demonstrated in 6 of 53 informative families, and, of 17 germline mutations in individuals for whom the parental origin of mutation could be demonstrated, 15 arose from the father. We conclude that the major factor accounting for the relative scarcity of carrier males is the bias toward mutations in the paternal germline (which present as affected female offspring) combined with reduced reproductive fitness in affected females. Postzygotic mutations also contribute to the female preponderance, whereas true nonpenetrance in males who are hemizygous for an EFNB1 mutation appears unusual. These results highlight the importance of considering possible origins of mutation in the counseling of families with CFNS and provide a generally applicable approach to the combined analysis of mosaic and germline mutations.

Published

2006

8. Enlarged parietal foramina caused by mutations in the homeobox genes ALX4 and MSX2: from genotype to phenotype

Author

Indira B. Taylor, Andrew O.M. Wilkie, Sally J. Davies, José L. Olivares, Feliciano J. Ramos, and Lampros A Mavrogiannis

Subjects

medicine.medical_specialty, DNA Mutational Analysis, Molecular Sequence Data, Locus (genetics), Biology, Article, Craniosynostosis, Genetic linkage, Molecular genetics, Genotype, Genetics, medicine, Enlarged parietal foramina, Humans, Chromatography, High Pressure Liquid, Genetics (clinical), DNA Primers, Homeodomain Proteins, Base Sequence, Chromosomes, Human, Pair 11, Skull, Chromosome Mapping, Sequence Analysis, DNA, medicine.disease, DNA-Binding Proteins, Phenotype, medicine.anatomical_structure, Tandem Repeat Sequences, Mutation, Homeobox, Gene Deletion, Transcription Factors

Abstract

Heterozygous mutations of the homeobox genes ALX4 and MSX2 cause skull defects termed enlarged parietal foramina (PFM) and cranium bifidum (CB); a single MSX2 mutation has been documented in a unique craniosynostosis (CRS) family. However, the relative mutational contribution of these genes to PFM/CB and CRS is not known and information on genotype-phenotype correlations is incomplete. We analysed ALX4 and MSX2 in 11 new unrelated cases or families with PFM/CB, 181 cases of CRS, and a single family segregating a submicroscopic deletion of 11p11.2, including ALX4. We explored the correlations between skull defect size and age, gene, and mutation type, and reviewed additional phenotypic manifestations. Four PFM cases had mutations in either ALX4 or MSX2; including previous families, we have identified six ALX4 and six MSX2 mutations, accounting for 11/13 familial, but only 1/6 sporadic cases. The deletion family confirms the delineation of a mental retardation locus to within 1.1 Mb region of 11p11.2. Overall, no significant size difference was found between ALX4- and MSX2-related skull defects, but the ALX4 mutation p.R218Q tends to result in persistent CB and is associated with anatomical abnormalities of the posterior fossa. We conclude that PFM caused by mutations in ALX4 and MSX2 have a similar prevalence and are usually clinically indistinguishable. Mutation screening has a high pickup rate in PFM, especially in familial cases, but is not indicated in CRS.

Published

2005

9. Contributions of intrinsic mutation rate and selfish selection to levels of de novo HRAS mutations in the paternal germline

Author

Eleni, Giannoulatou, Gilean, McVean, Indira B, Taylor, Simon J, McGowan, Geoffrey J, Maher, Zamin, Iqbal, Susanne P, Pfeifer, Isaac, Turner, Emma M M, Burkitt Wright, Jennifer, Shorto, Aysha, Itani, Karen, Turner, Lorna, Gregory, David, Buck, Ewa, Rajpert-De Meyts, Leendert H J, Looijenga, Bronwyn, Kerr, Andrew O M, Wilkie, and Anne, Goriely

Subjects

Adult, Male, Aging, Models, Statistical, Carcinogenesis, Costello Syndrome, Middle Aged, Biological Sciences, Proto-Oncogene Mas, Proto-Oncogene Proteins p21(ras), Germ Cells, Mutation, Humans, Selection, Genetic, Codon, Aged

Abstract

The RAS proto-oncogene Harvey rat sarcoma viral oncogene homolog (HRAS) encodes a small GTPase that transduces signals from cell surface receptors to intracellular effectors to control cellular behavior. Although somatic HRAS mutations have been described in many cancers, germline mutations cause Costello syndrome (CS), a congenital disorder associated with predisposition to malignancy. Based on the epidemiology of CS and the occurrence of HRAS mutations in spermatocytic seminoma, we proposed that activating HRAS mutations become enriched in sperm through a process akin to tumorigenesis, termed selfish spermatogonial selection. To test this hypothesis, we quantified the levels, in blood and sperm samples, of HRAS mutations at the p.G12 codon and compared the results to changes at the p.A11 codon, at which activating mutations do not occur. The data strongly support the role of selection in determining HRAS mutation levels in sperm, and hence the occurrence of CS, but we also found differences from the mutation pattern in tumorigenesis. First, the relative prevalence of mutations in sperm correlates weakly with their in vitro activating properties and occurrence in cancers. Second, specific tandem base substitutions (predominantly GCTT/AA) occur in sperm but not in cancers; genomewide analysis showed that this same mutation is also overrepresented in constitutional pathogenic and polymorphic variants, suggesting a heightened vulnerability to these mutations in the germline. We developed a statistical model to show how both intrinsic mutation rate and selfish selection contribute to the mutational burden borne by the paternal germline.

Published

2013

10. Rare mutations of FGFR2 causing apert syndrome: identification of the first partial gene deletion, and an Alu element insertion from a new subfamily

Author

David J. David, David Johnson, Dale J. Hedges, Indira B. Taylor, Andrew O.M. Wilkie, Elena G. Bochukova, Tony Roscioli, and Prescott L. Deininger

Subjects

Adult, Male, Subfamily, Adolescent, DNA Mutational Analysis, Molecular Sequence Data, Alu element, Apert syndrome, Biology, medicine.disease_cause, Germline, Genomic disorders and inherited multi-system disorders [IGMD 3], Exon, Fathers, Alu Elements, Genetics, medicine, Humans, Receptor, Fibroblast Growth Factor, Type 2, Base Pairing, Genetics (clinical), Mutation, Base Sequence, Fibroblast growth factor receptor 2, Genome, Human, Intron, Infant, Exons, Acrocephalosyndactylia, medicine.disease, Molecular biology, Mutagenesis, Insertional, Child, Preschool, Gene Deletion

Abstract

Contains fulltext : 81780.pdf (Publisher’s version ) (Closed access) Apert syndrome (AS) is a severe disorder, characterized by craniosynostosis and complex syndactyly of the hands and feet. Two heterozygous gain-of-function substitutions (Ser252Trp and Pro253Arg) in exon IIIa of fibroblast growth factor receptor 2 (FGFR2) are responsible for >98% of cases. Here we describe two novel mutations in FGFR2 in the two patients in whom a mutation had not previously been found in our cohort of 227 AS cases. The first is a 1.93-kb deletion, removing exon IIIc and substantial portions of the flanking introns. This is the first large FGFR2 deletion described in any individual with craniosynostosis. The other mutation is a 5' truncated Alu insertion into exon IIIc. This is the third Alu insertion identified in AS; all have occurred within an interval of only 104 bp, representing an enrichment of over a million-fold compared to the background genomic rate. We show that the inserted Alu element belongs to a small subfamily, not previously known to be mobile, which we term Alu Yk13. Both the deletion and insertion are likely to act by a similar gain-of-function mechanism in which disruption of exon IIIc leads to illegitimate mesenchymal expression of an FGFR2 spliceform containing the alternatively spliced exon IIIb. All the AS-associated Alu insertions have arisen in the paternal germline; we propose that their enrichment in FGFR2 is driven by positive selection of the mutant spermatogonial progenitors, a mechanism analogous to that explaining why the canonical AS nucleotide substitutions also reach exceptionally high levels in sperm.

Published

2009

11. A further mutation of the FGFR2 tyrosine kinase domain in mild Crouzon syndrome

Author

Alex J T Van Oostveldt, Indira B. Taylor, Thomy de Ravel, Andrew O.M. Wilkie, Jean-Pierre Fryns, Clinical sciences, and Medical Genetics

Subjects

Adult, Male, musculoskeletal diseases, Heterozygote, congenital, hereditary, and neonatal diseases and abnormalities, Child, preschool, Acrocephalosyndactylia, Molecular Sequence Data, Mutation, Missense, Biology, medicine.disease_cause, Polymerase Chain Reaction, Receptors, Fibroblast Growth Factor/genetics, Genetics, medicine, Missense mutation, Humans, Acrocephalosyndactylia/diagnosis, Amino Acid Sequence, Receptor, Fibroblast Growth Factor, Type 2, Child, Gene, Peptide sequence, Genetics (clinical), Mutation, Sequence Homology, Amino Acid, Craniofacial Dysostosis, Receptor Protein-Tyrosine Kinases/genetics, Crouzon syndrome, Receptor Protein-Tyrosine Kinases, Heterozygote advantage, Middle Aged, medicine.disease, Receptors, Fibroblast Growth Factor, Pedigree, Amino Acid Substitution, Mutation, Missense/genetics, Female, Craniofacial Dysostosis/diagnosis, Tyrosine kinase

Abstract

We report a family heterozygous for a newly identified mutation in the tyrosine kinase I domain of the FGFR2 gene (1576A > G, encoding the missense substitution Lys526Glu), associated with variable expressivity of Crouzon syndrome, including clinical nonpenetrance. Our observations expand both the clinical and molecular spectrum of this unusual subset of FGFR2 mutations.

Published

2005

12. Paternal origin of FGFR3 mutations in Muenke-type craniosynostosis

Author

Steven A. Wall, Sahan V. Rannan-Eliya, Andrew O.M. Wilkie, I. Marieke. de Heer, Ans M.W. van den Ouweland, Indira B. Taylor, Plastic and Reconstructive Surgery and Hand Surgery, and Clinical Genetics

Subjects

musculoskeletal diseases, Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, DNA Mutational Analysis, Mutation, Missense, Biology, medicine.disease_cause, Polymerase Chain Reaction, Paternal Age, Muenke syndrome, Craniosynostosis, Craniosynostoses, Risk Factors, Internal medicine, Genetics, medicine, Humans, Receptor, Fibroblast Growth Factor, Type 3, Allele, Achondroplasia, Transversion, Child, Gene, Genetics (clinical), Mutation, Age Factors, Syndrome, Protein-Tyrosine Kinases, medicine.disease, Receptors, Fibroblast Growth Factor, Human genetics, Pedigree, stomatognathic diseases, Endocrinology, Amino Acid Substitution, Female

Abstract

Muenke syndrome, also known as FGFR3-associated coronal synostosis, is defined molecularly by the presence of a heterozygous nucleotide transversion, c.749C>G, encoding the amino acid substitution Pro250Arg, in the fibroblast growth factor receptor type 3 gene (FGFR3). This frequently occurs as a new mutation, manifesting one of the highest documented rates for any transversion in the human genome. To understand the biology of this mutation, we have investigated its parental origin, and the ages of the parents, in 19 families with de novo c.749C>G mutations. All ten informative cases originated from the paternal allele (95% confidence interval 74-100% paternal); the average paternal age at birth overall was 34.7 years. An exclusive paternal origin of mutations, and increased paternal age, were previously described for a different mutation (c.1138G>A) of the FGFR3 gene causing achondroplasia, as well as for mutations of the related FGFR2 gene causing Apert, Crouzon and Pfeiffer syndromes. We conclude that similar biological processes are likely to shape the occurrence of this c.749C>G mutation as for other mutations of FGFR3 as well as FGFR2.

Published

2004

13. PATERNAL AGE EFFECT AND SELFISH MUTATIONS

Author

Wilkie Aom., Anne Goriely, Geoffrey J. Maher, Simon J. McGowan, E Rajpert-DeMeyts, J Lim, Susanne P. Pfeifer, Indira B. Taylor, and McVean Gat.

Subjects

Genetics, Psychiatry and Mental health, medicine.risk_factor, medicine, Paternal age effect, Biology, Biological Psychiatry

Published

2012