Genetic polymorphism of Streptococcus mutans in Brazilian family members

Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)

A single nucleotide deletion at the C1 inhibitor gene as the cause of hereditary angioedema: insights from a Brazilian family

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

HB D Los Angeles in a Brazilian family

Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)

MODY 2: Mutation identification and molecular ancestry in a Brazilian family

Maturity Onset Diabetes of the Young (MODY) is a heterogeneous group of genetic diseases characterized by a primary defect in insulin secretion and hyperglycemia, non-ketotic disease, monogenic autosomal dominant mode of inheritance, age at onset less than 25. years, and lack of auto-antibodies. It accounts for 2-5% of all cases of non-type 1 diabetes. MODY subtype 2 is caused by mutations in the glucokinase (GCK) gene. In this study, we sequenced the GCK gene of two volunteers with clinical diagnosis for MODY2 and we were able to identify four mutations including one for a premature stop codon (c.76C>T). Based on these results, we have developed a specific PCR-RFLP assay to detect this mutation and tested 122 related volunteers from the same family. This mutation in the GCK gene was detected in 21 additional subjects who also had the clinical features of this genetic disease. In conclusion, we identified new GCK gene mutations in a Brazilian family of Italian descendance, with one due to a premature stop codon located in the second exon of the gene. We also developed a specific assay that is fast, cheap and reliable to detect this mutation. Finally, we built a molecular ancestry model based on our results for the migration of individuals carrying this genetic mutation from Northern Italy to Brazil. © 2012 Elsevier B.V.

Aberrant transcript produced by a splice donor site deletion in the TECTA gene is associated with autosomal dominant deafness in a Brazilian family

We ascertained a Brazilian family with nine individuals affected by autosomal dominant nonsyndromic sensorineural hearing loss. The bilateral hearing loss affected mainly mid-high frequencies, was apparently stable with an early onset. Microsatellites close to the DFNA8/DFNA12 locus, which harbors the TECTA gene, showed significant multipoint lod scores (32) close to marker D11S4107. Sequencing of the exons and exon-intron boundaries of the TECTA gene in one affected subject revealed the deletion c.5383 + 5delGTGA in the 5' end of intron 16, that includes the last two bases of the donor splice site consensus sequence. This mutation segregates with deafness within the family. To date, 33 different TECTA mutations associated with autossomal dominant hearing loss have been described. Among them is the mutation reported herein, first described by Hildebrand et al. (2011) in a UK family. The audioprofiles from the UK and Brazilian families were similar. In order to investigate the transcripts produced by the mutated allele, we performed cDNA analysis of a lymphoblastoid cell line from an affected heterozygote with the c.5383 + 5delGTGA and a noncarrier from the same family. The analysis allowed us to identify an aberrant transcript with skipping of exon 16, without affecting the reading frame. One of the dominant TECTA mutations already described, a synonymous substitution in exon 16 (c.5331 G<A), was also shown to affect splicing resulting in an aberrant transcript lacking exon 16. Despite the difference in the DNA level, both the synonymous substitution in exon 16 (c.5331 G<A) and the mutation described herein affect splicing of exon 16, leading to its skipping. At the protein level they would have the same effect, an in-frame deletion of 37 amino-acids (p.S1758Y/G1759_N1795del) probably leading to an impaired function of the ZP domain. Thus, like the TECTA missense mutations associated with dominant hearing loss, the c5383 + 5delGTGA mutation does not have an inactivating effect on the protein. (C) 2012 Elsevier B.V. All rights reserved.

Variable expressivity of osteogenesis imperfecta in a Brazilian family due to p.G1079S mutation in the COL1A1 gene

Osteogenesis imperfecta (OI) is a Mendelian disease with genetic heterogeneity characterized by bone fragility, recurrent fractures, blue sclerae, and short stature, caused mostly by mutations in COL1A1 or COL1A2 genes, which encode the pro-alpha 1(I) and pro-alpha 2(I) chains of type I collagen, respectively. A Brazilian family that showed variable expression of autosomal dominant OI was identified and characterized. Scanning for mutations was carried out using SSCP and DNA sequence analysis. The missense mutation c.3235G>A was identified within exon 45 of the COL1A1 gene in a 16-year-old girl diagnosed as having OI type I; it resulted in substitution of a glycine residue (G) by a serine (S) at codon 1079 (p.G1079S). The proband's mother had the disease signs, but without bone fractures, as did five of nine uncles and aunts of the patient. All of them carried the mutation, which was excluded in four healthy brothers of the patient's mother. This is the first description in a Brazilian family with OI showing variable expression; only one among seven carriers for the c.3235G>A mutation developed bone fractures, the most striking clinical feature of this disease. This finding has a significant implication for prenatal diagnosis in OI disease.

Analysis of MLL2 gene in the first Brazilian family with Kabuki syndrome

Most patients with Kabuki syndrome (KS) are the only person in their family with the condition. However, familial cases of KS have been described showing evidence that this syndrome can be inherited as a dominant trait with variable expressivity. We report on two related individuals with facial findings characteristic of KS. The proposita had arched eyebrows, long and upward slanting palpebral fissures, cleft lip and palate, retromicrognathia, brachydactyly of hands and feet, stubby fingers, nail hypoplasia, and prominent finger pads. Her mother had eyebrows with dispersed lateral half, long and upward slanting palpebral fissures, retrognathia, abnormal and posteriorly rotated ears, prominent finger pads, brachydactyly of feet, learning difficulties, and psychomotor development delay. DNA sequencing revealed a novel missense mutation in the MLL2 gene in both the proposita and her mother. The mutation (p.R5432Q) was found in the exon 51, within the SET domain of the gene, which confers methyltransferase activity on the protein. Therefore, the epigenetic and transcriptional regulatory properties of this protein may be altered and this suggests that the mutation is the cause of phenotype observed in both the patient and her mother. The clinical signs and the molecular evidence in this family further support the notion that KS is an autosomal dominant condition with variable expressivity. To our knowledge this is the first report of a Brazilian family with recurrence of this syndrome. (C) 2012 Wiley Periodicals, Inc.

Genetic aspects of adolescent idiopathic scoliosis in a family with multiple affected members: a research article

Abstract Background The etiology of idiopathic scoliosis remains unknown and different factors have been suggested as causal. Hereditary factors can also determine the etiology of the disease; however, the pattern of inheritance remains unknown. Autosomal dominant, X-linked and multifactorial patterns of inheritances have been reported. Other studies have suggested possible chromosome regions related to the etiology of idiopathic scoliosis. We report the genetic aspects of and investigate chromosome regions for adolescent idiopathic scoliosis in a Brazilian family. Methods Evaluation of 57 family members, distributed over 4 generations of a Brazilian family, with 9 carriers of adolescent idiopathic scoliosis. The proband presented a scoliotic curve of 75 degrees, as determined by the Cobb method. Genomic DNA from family members was genotyped. Results Locating a chromosome region linked to adolescent idiopathic scoliosis was not possible in the family studied. Conclusion While it was not possible to determine a chromosome region responsible for adolescent idiopathic scoliosis by investigation of genetic linkage using microsatellites markers during analysis of four generations of a Brazilian family with multiple affected members, analysis including other types of genomic variations, like single nucleotide polymorphisms (SNPs) could contribute to the continuity of this study.

O sistema dos Anjos: memorabilia de uma família brasileira

A internação hospitalar da irmã obriga a narradora de O sistema dos Anjos a realizar uma viagem às pressas do Rio de Janeiro para uma cidade ao sul do Brasil. A partir deste deslocamento, histórias da infância, da adolescência e do início da vida adulta vão surgindo na memória da viajante. A dissertação, em forma de romance, foi estruturada a partir de duas narrativas, ambas escritas em primeira pessoa, que formam um sistema único e colocam em dúvida a identidade daquela que está narrando. Quem o eu, quem o outro é o fio invisível que atravessa essa ficção composta de capítulos que ambientam diferentes fases, desde a gênese da família dos Anjos até a sua dissolução

O princípio da paternidade responsável: de suas diretrizes conceituais à influência sobre os efeitos decorrentes da filiação

A paternidade responsável se destaca no contexto da Constituição de 1988, refletindo seus efeitos para todo o sistema. Os pais, ao assumirem esse status, passam a ser titulares de diversas obrigações sendo verdadeiro afirmar que deles, de alguma forma, sempre se exigiu certo tipo de responsabilidade. Seu conteúdo, todavia, é que variou no histórico da construção da família brasileira. A proteção aos filhos, anteriormente mais formalista e restrita à aplicação de medidas de suspensão ou destituição do poder familiar (pátrio poder), cedeu espaço para outros valores. Atualmente, cabe aos pais, em essência, a formação e a emancipação da pessoa do filho. Assistir, educar e criar são as ações básicas que informam a sua responsabilidade, sendo ainda titulares do dever de inserir o menor no contexto da família e da sociedade. A igualdade, a solidariedade e a autonomia se mesclam ao encargo parental, a bem da formação física e psíquica da prole. Mas, é necessário observar que o dever de cuidado, imposto constitucionalmente aos pais, é transferido para os filhos após a maioridade, por meio de uma lógica de reciprocidade e vulnerabilidade. Assim, passam estes a ser responsáveis pela assistência e pelo cuidado dos ascendentes doentes ou, por qualquer outro motivo, necessitados. Considerado o fato de que a verdadeira parentalidade é aquela que cria o estado concreto de pai-filho, reflexo do cumprimento da responsabilidade, é forçoso concluir pela inexistência de seus efeitos jurídicos nos casos em que o vínculo restou fixado pela simples formalidade do registro. Defende-se, então, para o fim de eximir os filhos de seus deveres, a desconstituição do vínculo registral ou a inocuidade de seus efeitos, sempre que os pais não tenham cumprido responsavelmente as suas funções em benefício da prole. As normas jurídicas constitucionais e infraconstitucionais legitimam tal prerrogativa, afastando as obrigações dos filhos cujos direitos fundamentais não foram respeitados pela incúria daqueles que tinham contrariamente o encargo de assistir e cuidar.

Avaliação da efetividade de intervenção de base comunitária voltada para a promoção do consumo de frutas e hortaliças em territórios de baixa renda da cidade do Rio de Janeiro

Evidências cada vez mais consistentes têm subsidiado a definição de recomendações acerca do consumo de frutas e hortaliças (F&H) como um fator de proteção contra o desenvolvimento de doenças crônicas não-transmissíveis. Essas recomendações têm sido transformadas em iniciativas de promoção do consumo de F&H. A escassez de estudos sobre a efetividade de intervenções voltadas para mudanças no consumo de F&H motivou a concepção desta tese, que teve por objetivo avaliar a efetividade de uma estratégia que integra diversas ações de promoção do consumo de frutas e hortaliças em múltiplos cenários, desenvolvidas junto a famílias que vivem em comunidades de baixa renda no Rio de Janeiro, RJ, Brasil. O estudo foi realizado em três comunidades cobertas pela Estratégia Saúde da Família na Zona Oeste do município do Rio de Janeiro, no período de 2007 a 2010. Trata-se de um estudo de intervenção comunitária tipo antes-e-depois. A coleta de dados incluiu duas avaliações pré-intervenção e uma avaliação pós-intervenção sobre a disponibilidade intradomiciliar e consumo de F&H e outras práticas alimentares. A intervenção mostrou-se efetiva para aumentar a disponibilidade intra-domiciliar de frutas e hortaliças nas três comunidades. Famílias mais expostas ao conjunto de elementos da intervenção apresentaram um maior aumento na aquisição de F&H entre o período pré e pós-intervenção. Mesmo em cenários sócio-demográficos menos favoráveis, quando as famílias foram mais expostas à intervenção, houve aumento pontual na disponibilidade intra-domiciliar de frutas e/ou hortaliças, apesar de não estatisticamente significativo. Por outro lado, também foi demonstrado que aumentos na aquisição de refrigerantes e biscoitos atenuaram o efeito da intervenção.

Craniometaphyseal Dysplasia With Severe Craniofacial Involvement Shows Homozygosity at 6q21-22.1 Locus

Craniotubular dysplasias (CTD) are a heterogeneous group of genetic disorders of skeletal development, whose clinical and etiological classification is still much debated. One of the most common form is the autosomal dominant craniometaphyseal dysplasia (CMD) which is associated with mutation in the ANKH gene. In the literature a few families are reported with CMD phenotype that suggest an autosomal recessive (AR) pattern of inheritance. A candidate locus at 6q21-22 has been mapped in a large inbred Brazilian family, but the gene of the recessive form is still unknown. Our data on a female patient with CMD phenotype, born from healthy first degree cousins and displaying homozygosity for polymorphic markers at the 6q21-22 locus, further support the existence of an AR CMD, expanding its clinical spectrum to a more severe phenotype. (C) 2011 Wiley-Liss, Inc.

Spastic Paraplegia, Optic Atrophy, and Neuropathy: New Observations, Locus Refinement, and Exclusion of Candidate Genes

SPOAN is an autosomal recessive neurodegenerative disorder which was recently characterized by our group in a large inbred Brazilian family with 25 affected individuals. This condition is clinically defined by: 1. congenital optic atrophy; 2. progressive spastic paraplegia with onset in infancy; and 3. progressive motor and sensory axonal neuropathy. Overall, we are now aware of 68 SPOAN patients (45 females and 23 males, with age ranging from 5 to 72 years), 44 of which are presented here for the first time. They were all born in the same geographic micro region. Those 68 patients belong to 43 sibships, 40 of which exhibit parental consanguinity. Sixty-one patients were fully clinically evaluated and 64 were included in the genetic investigation. All molecularly studied patients are homozygotes for D11S1889 at 11q13. This enabled us to reduce the critical region for the SPOAN gene from 4.8 to 2.3 Mb, with a maximum two point lod score of 33.2 (with marker D11S987) and of 27.0 (with marker D11S1889). Three genes located in this newly defined critical region were sequenced, but no pathogenic mutation was detected. The gene responsible for SPOAN remains elusive.

Skipping of exon 30 in C5 gene results in complete human C5 deficiency and demonstrates the importance of C5d and CUB domains for stability

The deficiency of complement C5 is rare and frequently associated with severe and recurrent infections, especially caused by Neisseria spp. We observed the absence of component C5 in the serum of 3 siblings from a Brazilian family with history of consanguinity. The patients had suffered from recurrent episodes of meningitis and other less severe infections. Sera from these patients were unable to mediate hemolytic activity either by the classical or alternative pathways and presented extremely low levels of C5 protein (13, 0.9 and 1.0 mu g/ml-normal range: 45-190 mu g/ml). Hemolytic activity could be restored by the addition of purified C5 to deficient serum. Sequencing of sibling C5 cDNA revealed a homozygous 153 bp deletion that corresponds precisely to exon 30. The parents carried the same deletion but only in one allele. Sequencing of the corresponding region in the genomic DNA revealed a C to C substitution within intron 30 and, most significantly, the substitution of GAG(4028) for GAA(4028) at the 3` end of exon 30 which is most likely responsible for skipping of exon 30. The resulting in-frame deletion in the C5 mRNA codes for a mutant C5 protein lacking residues 1289-1339. These residues map to the CUB and C5d domains of the C5 alpha chain. This deletion is expected to produce a non-functional and unstable C5 protein which is more susceptible to degradation. (C) 2009 Published by Elsevier Ltd.

História social de uma empresa brasileira: a cerâmica Porto Ferreira

O objetivo da pesquisa é construir a história social de uma empresa familiar brasileira fundada nos anos trinta no estado de São Paulo. A investigação acompanhou o desenvolvimento da organização até os dias atuais e pretendeu abranger diferentes dimensões desse processo: econômico-financeiros, políticos, gerenciais e tecnológicos.