Your search keyword '"Flávia Martinez de Carvalho"' showing total 5 results

1. New SHH and Known SIX3 Variants in a Series of Latin American Patients with Holoprosencephaly

Author

Ana Maria Bolognese, Milagros M. Duenas-Roque, Viviane Freitas de Castro, Maria Teresa Vieira Sanseverino, Viviana Cosentino, Rachel Sayuri Honjo, Larissa Souza Mario Bueno, Juan C. Llerena, Luiz Carlos Santana da Silva, Júlio César Loguercio Leite, Daniel Mattos, Márcia Pereira Alves de Souza, Denise P. Cavalcanti, Pablo Barbero, Pricila Bernardi, Flávia Martinez de Carvalho, Patrícia Santana Correia, Clarice Pagani Savastano, and Iêda M. Orioli

Subjects

Sanger sequencing, Genetics, Genetic counseling, Biology, medicine.disease, ZIC2, Phenotype, Penetrance, symbols.namesake, Holoprosencephaly, RNA splicing, medicine, symbols, Gene, Genetics (clinical)

Abstract

Holoprosencephaly (HPE) is the failure of the embryonic forebrain to develop into 2 hemispheres promoting midline cerebral and facial defects. The wide phenotypic variability and causal heterogeneity make genetic counseling difficult. Heterozygous variants with incomplete penetrance and variable expressivity in the SHH, SIX3, ZIC2, and TGIF1 genes explain ∼25% of the known causes of nonchromosomal HPE. We studied these 4 genes and clinically described 27 Latin American families presenting with nonchromosomal HPE. Three new SHH variants and a third known SIX3 likely pathogenic variant found by Sanger sequencing explained 15% of our cases. Genotype-phenotype correlation in these 4 families and published families with identical or similar driver gene, mutated domain, conservation of residue in other species, and the type of variant explain the pathogenicity but not the phenotypic variability. Nine patients, including 2 with SHH pathogenic variants, presented benign variants of the SHH, SIX3, ZIC2, and TGIF1 genes with potential alteration of splicing, a causal proposition in need of further studies. Finding more families with the same SIX3 variant may allow further identification of genetic or environmental modifiers explaining its variable phenotypic expression.

Published

2021

2. Differential expression of the IRF6 gene in the signs of Van der Woude Syndrome: Are distinct genetic modifiers operating?

Author

Luiz Carlos Santana-da-Silva, Iêda M. Orioli, Maria Elisabete Silva Santos, Danilo Leôncio Aguiar Pereira, Alexandre R. Vieira, João Farias Guerreiro, Flávia Martinez de Carvalho, Cláudia Maria da Rocha Martins, and Rosany de Oliveira Lisboa

Subjects

Genetics, Sequence analysis, Mutant, RK1-715, van der woude syndrome, Biology, irf6 gene, medicine.disease, Exon, orofacial clefts, Dentistry, medicine, SNP, Van der Woude syndrome, IRF6, Family history, General Dentistry, Gene

Abstract

Objective: The purpose of this study was to report a new variant in the Interferon Regulatory Factor 6 gene (IRF6) and to determine phenotype-genotype correlations in a family segregating Van der Woude syndrome.Methods: A five-generation family of 80 individuals segregating VWS was investigated using a tabulated pedigree but considering that three individuals registered in the pedigree died shortly after birth, the final sample size was 77 individuals. Five individuals had a complete dental clinical examination and molecular analysis performed using direct sequencing of the exon 4 and an adjacent region with 23 base pairs of the IRF6 gene.Results: Features of VWS reported in family history were present in 36.4% (28/77) of all family members; of these 57% (16/28) had pits in the lower lip, 36% (10/28) had both pits and orofacial clefts and 7 % (2/28) had only orofacial clefts. Developmental dental anomalies were observed in three individuals. The sequence analysis of exon 4 of the IRF6 gene carried out for 4 family members revealed the presence of the SNP rs7552506 (c.175-5C> G) located in five base pairs before the start of exon. The analysis of exon 4 of the IRF6 gene also revealed a new variant c.269G>C (p.Ser90Thr) which causes exchange of the Serine amino acid residue for the Threonine residue. Conclusions: The c.269G>C(p.Ser90Thr) can interfere with multimeric interactions and with protein conformation that will be slightly destabilized, because the mutant residue is bigger than the wild-type residue. The phenotypic variations in the cases studied, despite carrying the same genetic mutation, suggest that distinct genetic modifiers operate on the formation of clefts and dental development.

Published

2021

3. Analysis of the genetic ancestry of patients with oral clefts from South American admixed populations

Author

Fernando A. Poletta, Sidney Emanuel Batista dos Santos, Camilla Dutra Vieira-Machado, Alexandre R. Vieira, Luiz Carlos Santana da Silva, Juan C. Mereb, Iêda M. Orioli, Eduardo E. Castilla, Cláudia Maria da Rocha Martins, and Flávia Martinez de Carvalho

Subjects

0301 basic medicine, Genetics, medicine.medical_specialty, Genotype, Cleft Lip, Genetic genealogy, Ethnic group, 030206 dentistry, 030105 genetics & heredity, Biology, White People, Cleft Palate, 03 medical and health sciences, 0302 clinical medicine, South american, Statistical significance, Epidemiology, medicine, Humans, In patient, Indel, General Dentistry, Genotyping, Brazil

Abstract

Increased susceptibility to cleft lip, with or without cleft palate (CL±P) has been observed in South America, as related to Amerindian ancestry, using epidemiological data, uniparental markers, and blood groups. In this study, it was evaluated whether this increased risk remains when Amerindian ancestry is estimated using autosomal markers and considered in the predictive model. Ancestry was estimated through genotyping 62 insertion and deletion (INDEL) markers in sample sets of patients with CL±P, patients with cleft palate (CP), and controls, from Patagonia in southern Argentina and Belém in northern Brazil. The Amerindian ancestry in patients from Patagonia with CL±P was greater than in controls although it did not reach statistical significance. The European ancestry in patients with CL±P from Belém and in patients with CP from Belém and Patagonia was higher than in controls and statistically significant for patients with CP who were from Belém. This high contribution of European genetic ancestry among patients with CP who were from Belém has not been previously observed in American populations. Our results do not corroborate the currently accepted risks for CL±P and CP estimated by epidemiological studies in the North American populations and probably reflect the higher admixture found in South American ethnic groups when compared with the same ethnic groups from the North American populations.

Published

2016

4. A Genome-wide Association Study of Nonsyndromic Cleft Palate Identifies an Etiologic Missense Variant in GRHL3

Author

Carmen J. Buxó, Katherine Neiswanger, Ana Maria Lopez-Palacio, Lian Ma, Mauricio Arcos-Burgos, Luz Consuelo Valencia-Ramirez, Seth M. Weinberg, Jacqueline T. Hecht, Dora Rivera Valencia, Eva Maria Cutiongco-de la Paz, Eduardo E. Castilla, Robert A. Cornell, Toby Goldstein McHenry, Babatunde S. Aregbesola, Mary L. Marazita, Elizabeth J. Leslie, Flávia Martinez de Carvalho, Lina M. Moreno, Andrew E. Czeizel, Mekonen Eshete, Cecelia A. Laurie, John R. Shaffer, Carmencita Padilla, Rolv T. Lie, Carla A. Sanchez, Ramat Oyebunmi Braimah, Jennifer Standley, Peter A. Mossey, Susan H. Blanton, Iêda M. Orioli, Kaare Christensen, Olutayo James, Frederic W.-B. Deleyiannis, Javier Enríquez de Salamanca, Alexandre R. Vieira, Wasiu Lanre Adeyemo, Huan Liu, Allen J. Wilcox, Jenna C. Carlson, George L. Wehby, Paul A. Romitti, Ronald G. Munger, Fernando A. Poletta, L. Leigh Field, Judith M. Resick, Cathy C. Laurie, Figen Seymen, Mine Koruyucu, Azeez Butali, Andrew C. Lidral, Kimberly F. Doheny, Milliard Deribew, Deepti Jain, Eleanor Feingold, Juan C. Mereb, Jeffrey C. Murray, Beth Emanuele, and Jennifer Jacobs

Subjects

0301 basic medicine, Genotyping Techniques, Mutation, Missense, Genome-wide association study, Ethnic Groups, medicine.disease_cause, Bioinformatics, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, Transactivation, 0302 clinical medicine, Risk Factors, Ethnicity, Genetics, medicine, Missense mutation, Animals, Humans, Genetics(clinical), Craniofacial, Gene, Zebrafish, Genetics (clinical), Mutation, biology, Case-control study, 030206 dentistry, biology.organism_classification, Cleft Palate, DNA-Binding Proteins, Disease Models, Animal, 030104 developmental biology, Genetic Loci, Case-Control Studies, Genome-Wide Association Study, Transcription Factors

Abstract

Cleft palate (CP) is a common birth defect occurring in 1 in 2,500 live births. Approximately half of infants with CP have a syndromic form, exhibiting other physical and cognitive disabilities. The other half have nonsyndromic CP, and to date, few genes associated with risk for nonsyndromic CP have been characterized. To identify such risk factors, we performed a genome-wide association study of this disorder. We discovered a genome-wide significant association with a missense variant in GRHL3 (p.Thr454Met [c.1361C>T]; rs41268753; p = 4.08 × 10(-9)) and replicated the result in an independent sample of case and control subjects. In both the discovery and replication samples, rs41268753 conferred increased risk for CP (OR = 8.3, 95% CI 4.1-16.8; OR = 2.16, 95% CI 1.43-3.27, respectively). In luciferase transactivation assays, p.Thr454Met had about one-third of the activity of wild-type GRHL3, and in zebrafish embryos, perturbed periderm development. We conclude that this mutation is an etiologic variant for nonsyndromic CP and is one of few functional variants identified to date for nonsyndromic orofacial clefting. This finding advances our understanding of the genetic basis of craniofacial development and might ultimately lead to improvements in recurrence risk prediction, treatment, and prognosis. Cleft palate (CP) is a common birth defect occurring in 1 in 2,500 live births. Approximately half of infants with CP have a syndromic form, exhibiting other physical and cognitive disabilities. The other half have nonsyndromic CP, and to date, few genes associated with risk for nonsyndromic CP have been characterized. To identify such risk factors, we performed a genome-wide association study of this disorder. We discovered a genome-wide significant association with a missense variant in GRHL3 (p.Thr454Met [c.1361C>T]; rs41268753; p = 4.08 × 10(-9)) and replicated the result in an independent sample of case and control subjects. In both the discovery and replication samples, rs41268753 conferred increased risk for CP (OR = 8.3, 95% CI 4.1-16.8; OR = 2.16, 95% CI 1.43-3.27, respectively). In luciferase transactivation assays, p.Thr454Met had about one-third of the activity of wild-type GRHL3, and in zebrafish embryos, perturbed periderm development. We conclude that this mutation is an etiologic variant for nonsyndromic CP and is one of few functional variants identified to date for nonsyndromic orofacial clefting. This finding advances our understanding of the genetic basis of craniofacial development and might ultimately lead to improvements in recurrence risk prediction, treatment, and prognosis.

Published

2016

5. A multi-ethnic genome-wide association study identifies novel loci for non-syndromic cleft lip with or without cleft palate on 2p24.2, 17q23 and 19q13

Author

Deepti Jain, Azeez Butali, Dora Rivera Valencia, Jacqueline T. Hecht, Carmencita Padilla, Rolv T. Lie, Kaare Christensen, Ramat Oyebunmi Braimah, Toby Goldstein McHenry, Jenna C. Carlson, John R. Shaffer, Elizabeth J. Leslie, Luz Consuelo Valencia-Ramirez, Iêda M. Orioli, Peter A. Mossey, Lina M. Moreno, Mine Koruyucu, Wasiu Lanre Adeyemo, Fernando A. Poletta, Cecelia A. Laurie, Judith M. Resick, Eleanor Feingold, Allen J. Wilcox, Paul A. Romitti, L. Leigh Field, Babatunde S. Aregbesola, Alexandre R. Vieira, Susan H. Blanton, Juan C. Mereb, Fikre Abate, Cathy C. Laurie, Seth M. Weinberg, George L. Wehby, Eduardo E. Castilla, Flávia Martinez de Carvalho, Katherine Neiswanger, Ana Maria Lopez-Palacio, Lian Ma, Figen Seymen, Andrew C. Lidral, Andrew E. Czeizel, Jeffrey C. Murray, Beth Emanuele, Kimberly F. Doheny, Mekonen Eshete, Carla A. Sanchez, Jennifer Jacobs, Mary L. Marazita, Olutayo James, Frederic W.-B. Deleyiannis, Javier Enríquez de Salamanca, Carmen J. Buxó, Mauricio Arcos-Burgos, Eva Maria Cutiongco-de la Paz, and Ronald G. Munger

Subjects

Asian Continental Ancestry Group, Male, 0301 basic medicine, Cleft Lip, European Continental Ancestry Group, Black People, Ethnic Groups, Single-nucleotide polymorphism, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, White People, 03 medical and health sciences, 0302 clinical medicine, Asian People, Risk Factors, Polymorphism (computer science), Genetic variation, Ethnicity, Genetics, Humans, Genetic Predisposition to Disease, Craniofacial, Molecular Biology, Genetics (clinical), African Continental Ancestry Group, Genetic association, Association Studies Articles, 030206 dentistry, General Medicine, Actin cytoskeleton, Cleft Palate, 030104 developmental biology, Genetic Loci, Chromosomes, Human, Pair 2, Female, IRF6, Chromosomes, Human, Pair 19, Chromosomes, Human, Pair 17, Genome-Wide Association Study

Abstract

Orofacial clefts (OFCs), which include non-syndromic cleft lip with or without cleft palate (CL/P), are among the most common birth defects in humans, affecting approximately 1 in 700 newborns. CL/P is phenotypically heterogeneous and has a complex etiology caused by genetic and environmental factors. Previous genome-wide association studies (GWASs) have identified at least 15 risk loci for CL/P. As these loci do not account for all of the genetic variance of CL/P, we hypothesized the existence of additional risk loci. We conducted a multiethnic GWAS in 6480 participants (823 unrelated cases, 1700 unrelated controls and 1319 case-parent trios) with European, Asian, African and Central and South American ancestry. Our GWAS revealed novel associations on 2p24 near FAM49A, a gene of unknown function (P = 4.22 × 10-8), and 19q13 near RHPN2, a gene involved in organizing the actin cytoskeleton (P = 4.17 × 10-8). Other regions reaching genome-wide significance were 1p36 (PAX7), 1p22 (ARHGAP29), 1q32 (IRF6), 8q24 and 17p13 (NTN1), all reported in previous GWASs. Stratification by ancestry group revealed a novel association with a region on 17q23 (P = 2.92 × 10-8) among individuals with European ancestry. This region included several promising candidates including TANC2, an oncogene required for development, and DCAF7, a scaffolding protein required for craniofacial development. In the Central and South American ancestry group, significant associations with loci previously identified in Asian or European ancestry groups reflected their admixed ancestry. In summary, we have identified novel CL/P risk loci and suggest new genes involved in craniofacial development, confirming the highly heterogeneous etiology of OFCs. Orofacial clefts (OFCs), which include non-syndromic cleft lip with or without cleft palate (CL/P), are among the most common birth defects in humans, affecting approximately 1 in 700 newborns. CL/P is phenotypically heterogeneous and has a complex etiology caused by genetic and environmental factors. Previous genome-wide association studies (GWASs) have identified at least 15 risk loci for CL/P. As these loci do not account for all of the genetic variance of CL/P, we hypothesized the existence of additional risk loci. We conducted a multiethnic GWAS in 6480 participants (823 unrelated cases, 1700 unrelated controls and 1319 case-parent trios) with European, Asian, African and Central and South American ancestry. Our GWAS revealed novel associations on 2p24 near FAM49A, a gene of unknown function (P = 4.22 × 10(-8)), and 19q13 near RHPN2, a gene involved in organizing the actin cytoskeleton (P = 4.17 × 10(-8)). Other regions reaching genome-wide significance were 1p36 (PAX7), 1p22 (ARHGAP29), 1q32 (IRF6), 8q24 and 17p13 (NTN1), all reported in previous GWASs. Stratification by ancestry group revealed a novel association with a region on 17q23 (P = 2.92 × 10(-8)) among individuals with European ancestry. This region included several promising candidates including TANC2, an oncogene required for development, and DCAF7, a scaffolding protein required for craniofacial development. In the Central and South American ancestry group, significant associations with loci previously identified in Asian or European ancestry groups reflected their admixed ancestry. In summary, we have identified novel CL/P risk loci and suggest new genes involved in craniofacial development, confirming the highly heterogeneous etiology of OFCs.

Published

2016