Home Itens selecionados Provedores de dados OAI Créditos Sobre Ajuda

			Busca avançada
	Provedor de dados Rev. Bras. Ciênc. Avic. (9) Autor Gonzales,E (9) Leandro,NSM (4) Brito,AB (2) Cruz,CP (2) Pezzato,AC (2) Sartori,JR (2) Stringhini,JH (2) Aoyagi,MM (1) Araújo,ICS (1) Barbosa,Lima R (1) Bruno,LDG (1) Café,MB (1) Carvalho,FB (1) Cunha,WCP (1) Dahlke,F (1) Dalke,F (1) Fascina,VB (1) Figueiredo-Lima,DF (1) Furlan,RL (1) Givisiez,PEN (1) Mais... Palavra-chave Embryo (2) Fasting (2) Strain (2) Yolk sac (2) Acidifier (1) Antibiotics (1) Blood (1) Body weight (1) Broiler (1) Broiler breeder age (1) Cardiac (1) Chick (1) Chicks (1) Cholecalciferol (1) Deutectomy (1) Essential oil (1) Estresse (1) Frangos de corte (1) Hatch window (1) Immunity (1) Mais... Tipo do documento Info:eu-repo/semantics/article (9) Ano 2017 (1) 2016 (1) 2013 (1) 2012 (1) 2010 (1) 2008 (2) 2004 (1) 2000 (1) Mais... País Brazil (9) Idioma Inglês (8) Português (1)		Registro completo Provedor de dados:  Genet. Mol. Biol. País:  Brazil Título:  Determining mutations in G6PC and SLC37A4 genes in a sample of Brazilian patients with glycogen storage disease types Ia and Ib Autores:  Carlin,Marcelo Paschoalete Scherrer,Daniel Zanetti Tommaso,Adriana Maria Alves De Bertuzzo,Carmen Silvia Steiner,Carlos Eduardo Data:  2013-01-01 Ano:  2013 Palavras-chave:  DNA-based diagnosis Glycogen storage disease G6PC SLC37A4 Mutation Resumo:  Glycogen storage disease (GSD) comprises a group of autosomal recessive disorders characterized by deficiency of the enzymes that regulate the synthesis or degradation of glycogen. Types Ia and Ib are the most prevalent; while the former is caused by deficiency of glucose-6-phosphatase (G6Pase), the latter is associated with impaired glucose-6-phosphate transporter, where the catalytic unit of G6Pase is located. Over 85 mutations have been reported since the cloning of G6PC and SLC37A4 genes. In this study, twelve unrelated patients with clinical symptoms suggestive of GSDIa and Ib were investigated by using genetic sequencing of G6PC and SLC37A4 genes, being three confirmed as having GSD Ia, and two with GSD Ib. In seven of these patients no mutations were detected in any of the genes. Five changes were detected in G6PC, including three known point mutations (p.G68R, p.R83C and p.Q347X) and two neutral mutations (c.432G > A and c.1176T > C). Four changes were found in SLC37A4: a known point mutation (p.G149E), a novel frameshift insertion (c.1338_1339insT), and two neutral mutations (c.1287G > A and c.1076-28C > T). The frequency of mutations in our population was similar to that observed in the literature, in which the mutation p.R83C is also the most frequent one. Analysis of both genes should be considered in the investigation of this condition. An alternative explanation to the negative results in this molecular study is the possibility of a misdiagnosis. Even with a careful evaluation based on laboratory and clinical findings, overlap with other types of GSD is possible, and further molecular studies should be indicated. Tipo:  Info:eu-repo/semantics/other Idioma:  Inglês Identificador:  http://www.scielo.br/scielo.php?script=sci_arttext&pid=S1415-47572013000400007 Editor:  Sociedade Brasileira de Genética Relação:  10.1590/S1415-47572013000400007 Formato:  text/html Fonte:  Genetics and Molecular Biology v.36 n.4 2013 Direitos:  info:eu-repo/semantics/openAccess Fechar

Empresa Brasileira de Pesquisa Agropecuária - Embrapa Todos os direitos reservados, conforme Lei n° 9.610 Política de Privacidade Área restrita		Embrapa Parque Estação Biológica - PqEB s/n° Brasília, DF - Brasil - CEP 70770-901 Fone: (61) 3448-4433 - Fax: (61) 3448-4890 / 3448-4891 SAC: https://www.embrapa.br/fale-conosco