Registro completo |
Provedor de dados: |
BJMBR
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País: |
Brazil
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Título: |
MicroRNA-455 suppresses the oncogenic function of HDAC2 in human colorectal cancer
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Autores: |
Mao,Q.D.
Zhang,W.
Zhao,K.
Cao,B.
Yuan,H.
Wei,L.Z.
Song,M.Q.
Liu,X.S.
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Data: |
2017-01-01
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Ano: |
2017
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Palavras-chave: |
Colorectal cancer
Histone deacetylase 2
MiR-455
Proliferation
Apoptosis
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Resumo: |
Colorectal cancer (CRC) is the fourth leading cause of cancer-induced mortality. Histone deacetylase 2 (HDAC2) is involved in prognosis and therapy of CRC. This study aimed to explore novel therapeutic targets for CRC. The alteration of HDAC2 expression in CRC tissues was estimated by qRT-PCR. After lentivirus transfection, HDAC2 knockdown was confirmed by western blot analysis. The effect of HDAC2 knockdown on cell proliferation was then assessed by 3-(4,5-dimethylthiazol-2-yl)-2, 5-diphenyltetrazolium bromide (MTT) assay. Screened by TargetScan, microRNA (miR)-455 was predicted to bind to 3′UTR of HDAC2 and the prediction was verified by luciferase assay. Finally, cells were transfected, respectively, with miR-455 mimics or miR-455 negative control (miR-NC) and the expression of HDAC2, cell proliferation and apoptosis of transfected cells were respectively evaluated by western blot analysis, MTT assay and flow cytometry. Results showed that the HDAC2 expression was up-regulated in CRC tissues (P<0.05). HDAC2 knockdown significantly decreased cell viability at day 3 (P<0.05), day 4 (P<0.01), and day 5 (P<0.001) after infection. Then, miR-455 was verified to directly target HDAC2, resulting in a significant difference in luciferase activity (P<0.01). Moreover, miR-455 decreased the expression of HDAC2 (P<0.01). miR-455 remarkably decreased cell viability at day 3 (P<0.05), day 4 (P<0.01), and day 5 (P<0.001) after transfection while inducing cell apoptosis (P<0.001). In conclusion, miR-455 inhibited cell proliferation while inducing cell apoptosis by targeting HDAC2 in CRC cells.
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Tipo: |
Info:eu-repo/semantics/article
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Idioma: |
Inglês
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Identificador: |
http://www.scielo.br/scielo.php?script=sci_arttext&pid=S0100-879X2017000600608
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Editor: |
Associação Brasileira de Divulgação Científica
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Relação: |
10.1590/1414-431x20176103
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Formato: |
text/html
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Fonte: |
Brazilian Journal of Medical and Biological Research v.50 n.6 2017
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Direitos: |
info:eu-repo/semantics/openAccess
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