Utilize este identificador para referenciar este registo: https://hdl.handle.net/10316/106654
Título: Identification of new targets of S-nitrosylation in neural stem cells by thiol redox proteomics
Autor: Santos, Ana Isabel 
Lourenço, Ana Sofia 
Simão, Sónia
Marques da Silva, Dorinda
Santos, Daniela Filipa
Onofre de Carvalho, Ana Paula
Pereira, Ana Catarina
Izquierdo-Álvarez, Alicia
Ramos, Elena
Morato, Esperanza
Marina, Anabel
Martínez-Ruiz, Antonio
Araújo, Inês Maria 
Palavras-chave: Nitric oxide S-nitrosylation; Neurogenesis; Neural stem cells; Neurogenesis Seizures; Hippocampus
Data: Mai-2020
Editora: Elsevier
Projeto: SFRH/BD/77903/2011 
SFRH/BD/79308/2011 
PTDC/QUI-QFI/29319/2017 
PTDC/NEU-OSD/0473/2012 
UID/BIM/04773/2019 
Título da revista, periódico, livro ou evento: Redox Biology
Volume: 32
Resumo: Nitric oxide (NO) is well established as a regulator of neurogenesis. NO increases the proliferation of neural stem cells (NSC), and is essential for hippocampal injury-induced neurogenesis following an excitotoxic lesion. One of the mechanisms underlying non-classical NO cell signaling is protein S-nitrosylation. This post-translational modification consists in the formation of a nitrosothiol group (R-SNO) in cysteine residues, which can promote formation of other oxidative modifications in those cysteine residues. S-nitrosylation can regulate many physiological processes, including neuronal plasticity and neurogenesis. In this work, we aimed to identify S-nitrosylation targets of NO that could participate in neurogenesis. In NSC, we identified a group of proteins oxidatively modified using complementary techniques of thiol redox proteomics. S-nitrosylation of some of these proteins was confirmed and validated in a seizure mouse model of hippocampal injury and in cultured hippocampal stem cells. The identified S-nitrosylated proteins are involved in the ERK/MAPK pathway and may be important targets of NO to enhance the proliferation of NSC.
URI: https://hdl.handle.net/10316/106654
ISSN: 22132317
DOI: 10.1016/j.redox.2020.101457
Direitos: openAccess
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