| Literature DB >> 32492405 |
Boxing Li1, Benjamin S Suutari2, Simón(e) D. Sun2, Zhengyi Luo3, Chuanchuan Wei4, Nicolas Chenouard5, Nataniel J Mandelberg5, Guoan Zhang6, Brie Wamsley7, Guoling Tian5, Sandrine Sanchez5, Sikun You4, Lianyan Huang4, Thomas A Neubert6, Gordon Fishell7, Richard W Tsien8.
Abstract
Homeostasis of neural firing properties is important in stabilizing neuronal circuitry, but how such plasticity might depend on alternative splicing is not known. Here we report that chronic inactivity homeostatically increases action potential duration by changing alternative splicing of BK channels; this requires nuclear export of the splicing factor Nova-2. Inactivity and Nova-2 relocation were connected by a novel synapto-nuclear signaling pathway that surprisingly invoked mechanisms akin to Hebbian plasticity: Ca2+-permeable AMPA receptor upregulation, L-type Ca2+ channel activation, enhanced spine Ca2+ transients, nuclear translocation of a CaM shuttle, and nuclear CaMKIV activation. These findings not only uncover commonalities between homeostatic and Hebbian plasticity but also connect homeostatic regulation of synaptic transmission and neuronal excitability. The signaling cascade provides a full-loop mechanism for a classic autoregulatory feedback loop proposed ∼25 years ago. Each element of the loop has been implicated previously in neuropsychiatric disease.Entities:
Keywords: Alternative splicing; BK channel; CaM kinase; Nova-2; action potential duration; chronic inactivity; homeostasis; synaptic activity
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Year: 2020 PMID: 32492405 PMCID: PMC9310388 DOI: 10.1016/j.cell.2020.05.013
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 66.850