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	Provedor de dados Biol. Res. (992) Autor Valenzuela,Carlos Y (11) Ercisli,Sezai (9) Santos,Manuel J (8) HIDALGO,CECILIA (7) ROSEMBLATT,MARIO (7) GÜNTHER,BRUNO (6) KRAUSKOPF,MANUEL (6) MORGADO,ENRIQUE (6) ARREDONDO,MIGUEL (5) GARCÍA,CARLOS (5) JAIMOVICH,ENRIQUE (5) LAGOS,NÉSTOR (5) Moreno,Ricardo D (5) NÚÑEZ,MARCO T (5) SERANI-MERLO,ALEJANDRO (5) Sadiq,Abdul (5) Ullah,Farhat (5) VIDELA,LUIS A (5) Ahmad,Sajjad (4) Ayaz,Muhammad (4) Mais... Palavra-chave Apoptosis (29) Oxidative stress (27) Antioxidant (18) Antioxidants (12) Lipid peroxidation (12) Nitric oxide (11) Gene expression (10) Angiogenesis (9) Free radicals (9) Polymorphism (9) Proliferation (9) Trypanosoma cruzi (9) Calcium (8) Mitochondria (8) Morphology (8) Rat (8) Ryanodine receptors (8) Chile (7) Iron (7) Obesity (7) Mais... Tipo do documento Journal article (992) Ano 2017 (39) 2016 (44) 2015 (69) 2014 (76) 2013 (57) 2012 (50) 2011 (50) 2010 (57) 2009 (53) 2008 (50) 2007 (58) 2006 (73) 2005 (43) 2004 (81) 2003 (44) 2002 (53) 2001 (48) 2000 (38) 1999 (9) Mais... País Chile (992) Idioma Inglês (914) Espanhol (78)		Registro completo Provedor de dados:  Biol. Res. País:  Chile Título:  S100A8 inhibits PDGF-induced proliferation of airway smooth muscle cells dependent on the receptor for advanced glycation end-products Autores:  Xu,Yu‑Dong Wang,Yu Yin,Lei‑Miao Peng,Ling‑Ling Park,Gyoung‑Hee Yang,Yong‑Qing Data:  2017-01-01 Ano:  2017 Palavras-chave:  S100A8 Airway smooth muscle cells Cell proliferation The receptor for advanced glycation end&#8209 Products Platelet&#8209 Derived growth factor Resumo:  Abstract Background Airway remodeling is a key feature of asthma, characterized by increased proliferation of airway smooth muscle cells (ASMCs). S100A8 is a calcium‑binding protein with a potential to regulate cell proliferation. Here, the effect of exogenous S100A8 protein on the proliferation of ASMCs induced by platelet‑derived growth factor (PDGF) and the underlying molecular mechanism was investigated. Methods Rat ASMCs were cultured with or without a neutralizing antibody to the receptor for advanced glycation end‑products (RAGE), a potential receptor for S100A8 protein. Purified recombinant rat S100A8 protein was then added into the cultured cells, and the proliferation of ASMCs induced by PDGF was detected by colorimetric‑based WST‑8 assay and ampedance‑based xCELLigence proliferation assay. The expression levels of RAGE in ASMCs were analyzed using western blotting assay. Results Results showed that exogenous S100A8 inhibited the PDGF‑induced proliferation of rat ASMCs in a dose‑ dependent manner with the maximal effect at 1 μg/ml in vitro. Furthermore, when ASMCs was pre‑treated with anti‑RAGE neutralizing antibody, the inhibitory effect of S100A8 on PDGF‑induced proliferation was significantly sup‑ pressed. In addition, neither the treatment with S100A8 or PDGF alone nor the pre‑treatment with rS100A8 followed by PDGF stimulation affected the expression levels of RAGE. Conclusions Our study demonstrated that S100A8 inhibits PDGF‑induced ASMCs proliferation in a manner depend‑ ent on membrane receptor RAGE. Tipo:  Journal article Idioma:  Inglês Identificador:  http://www.scielo.cl/scielo.php?script=sci_arttext&pid=S0716-97602017000100216 Editor:  Sociedad de Biología de Chile Formato:  text/html Fonte:  Biological Research v.50 2017 Fechar

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