AI Article Synopsis

  • Synaptic plasticity, essential for long-term memory, relies on transcription and translation triggered by various stimuli, leading to mRNA synthesis that regulates synaptic changes.
  • A detailed biochemical model was developed to understand how cells decide which mRNAs to produce in response to different synaptic activities, highlighting distinct signaling pathways that decode stimulus patterns into specific mRNA subtypes.
  • This model includes major regulatory pathways and has been validated against experimental data, suggesting that the mechanisms for selecting mRNA patterns may be applicable across various cell types.

Article Abstract

Synaptic plasticity requires transcription and translation to establish long-term changes that form the basis for long term memory. Diverse stimuli, such as synaptic activity and growth factors, trigger synthesis of mRNA to regulate changes at the synapse. The palette of possible mRNAs is vast, and a key question is how the cell selects which mRNAs to synthesize. To address this molecular decision-making, we have developed a biochemically detailed model of synaptic-activity triggered mRNA synthesis. We find that there are distinct time-courses and amplitudes of different branches of the mRNA regulatory signaling pathways, which carry out pattern-selective combinatorial decoding of stimulus patterns into distinct mRNA subtypes. Distinct, simultaneously arriving input patterns that impinge on the transcriptional control network interact nonlinearly to generate novel mRNA combinations. Our model combines major regulatory pathways and their interactions connecting synaptic input to mRNA synthesis. We parameterized and validated the model by incorporating data from multiple published experiments. The model replicates outcomes of knockout experiments. We suggest that the pattern-selectivity mechanisms analyzed in this model may act in many cell types to confer the capability to decode temporal patterns into combinatorial mRNA expression.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4006808PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0095154PLOS

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