Abstract
The presynaptic proteins MUNC18-1, syntaxin-1, and SNAP25 drive SNARE-mediated synaptic vesicle fusion and are also required for neuronal viability. Their absence triggers rapid, cell-autonomous, neuron-specific degeneration, unrelated to synaptic vesicle deficits. The underlying cell death pathways remain poorly understood. Here, we show that hippocampi of munc18-1 null mice (unknown sex) express apoptosis hallmarks cleaved caspase 3 (CC-3) and phosphorylated p53, and have condensed nuclei. However, side-by-side in vitro comparison with classical apoptosis induced by camptothecin uncovered striking differences to syntaxin-1 and MUNC18-1 depleted neurons. First, live-cell imaging revealed consecutive neurite retraction hours before cell death in MUNC18-1 or syntaxin-1 depleted neurons, whereas all neurites retracted at once, directly before cell death in classical apoptosis. Second, CC-3 activation was observed only after loss of all neurites and cellular breakdown, whereas CC-3 is activated before any neurite loss in classical apoptosis. Third, a pan-caspase inhibitor and a p53 inhibitor both arrested classical apoptosis, as expected, but not cell death in MUNC18-1 or syntaxin-1 depleted neurons. Neuron-specific cell death, consecutive neurite retraction, and late CC-3 activation were conserved in syntaxin-1 depleted human neurons. Finally, no indications were observed for involvement of other established cell death pathways, including necroptosis, Wallerian degeneration, autophagic cell death, and pyroptosis. Together, these data show that depletion of presynaptic proteins MUNC18-1 or syntaxin-1 triggers an atypical, staged cell death pathway characterized by consecutive neurite retraction, ultimately leading to, but not driven by, apoptosis.SIGNIFICANCE STATEMENT Neuronal cell death can occur via a multitude of pathways and plays an important role in the developing nervous system as well as neurodegenerative diseases. One poorly understood pathway to neuronal cell death takes place on depletion of presynaptic SNARE proteins syntaxin-1, SNAP25, or MUNC18-1. The current study demonstrates that MUNC18-1 or syntaxin-1 depleted neurons show a new, atypical, staged cell death that does not resemble any of the established cell death pathways in neurons. Cell death on MUNC18-1 or syntaxin-1 depletion is characterized by consecutive neurite retraction, ultimately involving, but not driven by, classical apoptosis.
| Original language | English |
|---|---|
| Pages (from-to) | 347-358 |
| Number of pages | 12 |
| Journal | The Journal of neuroscience : the official journal of the Society for Neuroscience |
| Volume | 43 |
| Issue number | 3 |
| DOIs | |
| Publication status | Published - 18 Jan 2023 |
Bibliographical note
Publisher Copyright:Copyright © 2023 Feringa, van Berkel et al.
Funding
This work was supported by European Union European Research Council Advanced Grant 322966 to M.V. and Lundbeck Foundation Grant R277-2018-802. We thank Desiree Schut and Lisa Laan for culturing neurons, Joke Wortel for breeding mutant mice, Robbert Zalm for cloning, and the René Medema laboratory (The Netherlands Cancer Institute, Amsterdam) for sharing p-p53ser15 and p53 antibodies. Received Mar. 28, 2022; revised Sep. 9, 2022; accepted Sep. 21, 2022. Author contributions: F.M.F., A.A.V., and M.V. designed research; F.M.F., A.A.V., and A.N. performed research; F.M.F., A.A.V., and A.N. analyzed data; F.M.F. and A.A.V. wrote the paper. This work was supported by European Union European Research Council Advanced Grant 322966 to M.V. and Lundbeck Foundation Grant R277-2018-802. We thank Desiree Schut and Lisa Laan for culturing neurons, Joke Wortel for breeding mutant mice, Robbert Zalm for cloning, and the René Medema laboratory (The Netherlands Cancer Institute, Amsterdam) for sharing p-p53ser15 and p53 antibodies. *F.M.F. and A.A.V. contributed equally to this work. The authors declare no competing financial interests. Correspondence should be addressed to Matthijs Verhage to [email protected]. https://doi.org/10.1523/JNEUROSCI.0611-22.2022 Copyright © 2023 Feringa, van Berkel et al. This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license, which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
| Funders | Funder number |
|---|---|
| European Union European Research Council | 322966 |
| Netherlands Cancer Institute | |
| René Medema laboratory | |
| Lundbeckfonden | R277-2018-802 |
Keywords
- cell death
- Munc-18
- SNARE
- syntaxin
