AI Article Synopsis

  • Neural stem cells (NSCs) in adult vertebrate brains, particularly in zebrafish, can generate neurons throughout life by making balanced decisions about their fate, including direct conversions without dividing.
  • Researchers reanalyzed imaging data and found that both NSCs and neuronal progenitors share similar delamination dynamics, indicating a direct connection in how these cells transition to neurons.
  • They discovered that non-apoptotic caspase activation (Caspase3/7) in NSCs, influenced by the transcription factor Atf3, plays a significant role in determining the fate of these stem cells, especially during injury, leading to increased neuron formation and maintaining NSC population stability.

Article Abstract

Neural stem cells (NSCs) generate neurons over a lifetime in adult vertebrate brains. In the adult zebrafish pallium, NSCs persist long term through balanced fate decisions. These decisions include direct neuronal conversions, i.e. delamination and neurogenesis without a division. To characterize this process, we reanalyze intravital imaging data of adult pallial NSCs, and observe shared delamination dynamics between NSCs and committed neuronal progenitors. Searching for mechanisms predicting direct NSC conversions, we build an NSC-specific genetic tracer of Caspase3/7 activation (Cas3*/Cas7*) in vivo. We show that non-apoptotic Cas3*/7* events occur in adult NSCs and are biased towards lineage termination under physiological conditions, with a predominant generation of single neurons. We further identify the transcription factor Atf3 as necessary for this bias. Finally, we show that the Cas3*/7* pathway is engaged by NSCs upon parenchymal lesion and correlates with NSCs more prone to lineage termination and neuron formation. These results provide evidence for non-apoptotic caspase events occurring in vertebrate adult NSCs and link these events with the NSC fate decision of direct conversion, which is important for long-term NSC population homeostasis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11607687PMC
http://dx.doi.org/10.1242/dev.204381DOI Listing

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