[No authors listed]
Forkhead box P2 (Foxp2) is a transcription factor involved in vocal learning. However, the number of previous studies that have investigated the role of Foxp2 in early vascular dementia (VD) is limited. The aim of the present study was to determine whether microRNA (miR)â134â5p/Foxp2 contributes to cognitive impairment in a chronic ischemiaâinduced early VD model. miRâ134â5p was found to be significantly increased in the cortex in a rat VD model. Intracerebroventricular injection of miRâ134â5p antagomir into VD rats prevented the loss of synaptic proteins and the development of cognitive impairment phenotypes. Histopathological analysis revealed that miRâ134â5p aggravated cognitive impairment in VD rats through damage to cortical neurons and loss of synaptic proteins. Bioinformatics analysis predicted that miRâ134â5p targets Foxp2 mRNA. Dual luciferase analysis and western blotting supported the prediction that miRâ134â5p targets Foxp2. Furthermore, the silencing of Foxp2 significantly inhibited the effect of miRâ134â5p on synaptic protein loss. Chromatin immunoprecipitationâquantitative polymerase chain reaction analysis indicated that Foxp2 binds to the synapsin I (Syn1) promoter at â400/â600Â bp upstream of the transcription start site. In conclusion, the miRâ134â5p/Foxp2/Syn1 axis was found to contribute to cognitive impairment in a chronic ischemiaâinduced early VD model, which may enable the development of new therapeutic strategies for the prevention and treatment of VD.
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