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Publication : A novel knockout mouse model of the noncoding antisense <i>Brain-Derived Neurotrophic Factor</i> (<i>Bdnf</i>) gene displays increased endogenous Bdnf protein and improved memory function following exercise.

First Author  Modarresi F Year  2021
Journal  Heliyon Volume  7
Issue  7 Pages  e07570
PubMed ID  34377851 Mgi Jnum  J:310099
Mgi Id  MGI:6756238 Doi  10.1016/j.heliyon.2021.e07570
Citation  Modarresi F, et al. (2021) A novel knockout mouse model of the noncoding antisense Brain-Derived Neurotrophic Factor (Bdnf) gene displays increased endogenous Bdnf protein and improved memory function following exercise. Heliyon 7(7):e07570
abstractText  Brain-derived neurotrophic factor (Bdnf) expression is tightly controlled at the transcriptional and post-transcriptional levels. Previously, we showed that inhibition of noncoding Bdnf antisense (Bdnf-AS) RNA upregulates Bdnf protein. Here, we generated a Bdnf-antisense knockout (Bdnf-AS KO) mouse model by deleting 6 kilobases upstream of Bdnf-AS. After verifying suppression of Bdnf-AS, baseline behavioral tests indicated no significant difference in knockout and wild type mice, except for enhanced cognitive function in the knockout mice in the Y-maze. Following acute involuntary exercise, Bdnf-AS KO mice were re-assessed and a significant increase in Bdnf mRNA and protein were observed. Following long-term involuntary exercise, we observed a significant increase in nonspatial and spatial memory in novel object recognition and Barnes maze tests in young and aged Bdnf-AS KO mice. Our data provides evidence for the beneficial effects of endogenous Bdnf upregulation and the synergistic effect of Bdnf-AS knockout on exercise and memory retention.
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