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	Provedor de dados BJMBR (16) Autor Krieger,J.E. (16) Oliveira,E.M. (4) Pereira,A.C. (4) Junqueira,M.L. (2) Mady,C. (2) Miyakawa,A.A. (2) Ramires,F.J.A. (2) Alves,M.F. (1) Aneas,I.M.S. (1) Araujo,A.Q. (1) Araujo,M.C. (1) Arteaga,E. (1) Atala,M.M. (1) Barreto-Chaves,M.L.M. (1) Benseñor,I. (1) Benvenuti,L.A. (1) Benício,A.M.D. (1) Brum,P.C. (1) Buck,P.C. (1) Cardoso,L. (1) Mais... Palavra-chave Angiotensin-converting enzyme (3) Hypertension (3) ACE activity (2) 22q11.2 (1) ACE (1) ACE polymorphism (1) APOE (1) Agonist-induced receptor internalization (1) Alcohol (1) Angiotensin II (1) Angiotensin converting enzyme (1) Angiotensin-I converting enzyme (1) Angiotensin-converting enzyme activity (1) Angiotensinogen (1) Association study (1) Autoregressive model (1) Broodstock (1) CAMP (1) Cardiac hypertrophy (1) Cardiac myocytes (1) Mais... Tipo do documento Info:eu-repo/semantics/article (14) Info:eu-repo/semantics/other (2) Ano 2009 (2) 2008 (1) 2006 (1) 2005 (1) 2004 (2) 2003 (3) 2001 (3) 2000 (2) 1999 (1) Mais... País Brazil (16) Idioma Inglês (16)		Registro completo Provedor de dados:  BJMBR País:  Brazil Título:  Control of the rat angiotensin I converting enzyme gene by CRE-like sequences Autores:  Xavier-Neto,J. Pereira,A.C. Oliveira,E.M. Miyakawa,A.A. Junqueira,M.L. Krieger,J.E. Data:  2004-10-01 Ano:  2004 Palavras-chave:  Angiotensin converting enzyme Endothelium CAMP Cyclic AMP responsive element Resumo:  We characterized the role of potential cAMP-responsive elements (CRE) in basal and in induced angiotensin converting enzyme (ACE) gene promoter activity in order to shed light on the regulation of somatic ACE expression. We identified stimulators and repressors of basal expression between 122 and 288 bp and between 415 and 1303 bp upstream from the transcription start site, respectively, using a rabbit endothelial cell (REC) line. These regions also contained elements associated with the response to 8BrcAMP. When screening for CRE motifs we found pCRE, a proximal sequence between 209 and 222 bp. dCRE, a distal tandem of two CRE-like sequences conserved between rats, mice and humans, was detected between 834 and 846 bp. Gel retardation analysis of nuclear extracts of REC indicated that pCRE and dCRE bind to the same protein complexes as bound by a canonical CRE. Mutation of pCRE and dCRE in REC established the former as a positive element and the latter as a negative element. In 293 cells, a renal cell line, pCRE and dCRE are negative regulators. Co-transfection of ATF-2 or ATF-2 plus c-Jun repressed ACE promoter activity, suggesting that the ACE gene is controlled by cellular stress. Although mapping of cAMP responsiveness was consistent with roles for pCRE and dCRE, mutation analysis indicated that they were not required for cAMP responsiveness. We conclude that the basal activity of the somatic ACE promoter is controlled by proximal and distal CREs that can act as enhancers or repressors depending on the cell context. Tipo:  Info:eu-repo/semantics/article Idioma:  Inglês Identificador:  http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0100-879X2004001000002 Editor:  Associação Brasileira de Divulgação Científica Relação:  10.1590/S0100-879X2004001000002 Formato:  text/html Fonte:  Brazilian Journal of Medical and Biological Research v.37 n.10 2004 Direitos:  info:eu-repo/semantics/openAccess Fechar

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