4.7 Article

AP-1 Transcription Factors Mediate BDNF-Positive Feedback Loop in Cortical Neurons

Journal

JOURNAL OF NEUROSCIENCE
Volume 36, Issue 4, Pages 1290-1305

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.3360-15.2016

Keywords

AP-1; BDNF autoregulation; BDNF-positive feedback loop; Fos; Jun; TrkB

Categories

Funding

  1. Estonian Research Council [IUT19-18, ETF8844]
  2. National R&D program Biotechnology [AR12030]
  3. Estonian Enterprise [EU27553]
  4. Norwegian Financial Mechanism [EMP128]
  5. Estonian Academy of Sciences

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Brain-derived neurotrophic factor (BDNF), a member of the neurotrophin family, regulates both survival and differentiation of several neuronal populations in the nervous system during development, as well as synaptic plasticity in the adult brain. BDNF exerts its biological functions through its receptor TrkB. Although the regulation of BDNF transcription by neuronal activity has been widely studied, little is known about TrkB signaling-dependent expression of BDNF. Using rat primary cortical neuron cultures, we show that the BDNF gene is a subject to an extensive autoregulatory loop, where TrkB signaling upregulates the expression of all major BDNF transcripts, mainly through activating MAPK pathways. Investigating the mechanisms behind this autoregulation, we found that AP-1 transcription factors, comprising Jun and Fos family members, participate in the induction of BDNF exon I, III, and VI transcripts. AP-1 transcription factors directly upregulate the expression of exon I transcripts by binding two novel AP-1 cis-elements in promoter I. Moreover, our results show that the effect of AP-1 proteins on the activity of rat BDNF promoters III and VI is indirect, because AP-1 proteins were not detected to bind the respective promoter regions by chromatin immunoprecipitation (ChIP). Collectively, we describe an extensive positive feedback system in BDNF regulation, adding a new layer to the elaborate control of BDNF gene expression.

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