| Literature DB >> 35394425 |
Murat Kilinc1,2, Vineet Arora2, Thomas K Creson2, Camilo Rojas2, Aliza A Le3, Julie Lauterborn3, Brent Wilkinson4, Nicolas Hartel5, Nicholas Graham5, Adrian Reich6, Gemma Gou7,8, Yoichi Araki9, Àlex Bayés7, Marcelo Coba4, Gary Lynch3, Courtney A Miller1,2, Gavin Rumbaugh1,2.
Abstract
Loss-of-function variants in SYNGAP1 cause a developmental encephalopathy defined by cognitive impairment, autistic features, and epilepsy. SYNGAP1 splicing leads to expression of distinct functional protein isoforms. Splicing imparts multiple cellular functions of SynGAP proteins through coding of distinct C-terminal motifs. However, it remains unknown how these different splice sequences function in vivo to regulate neuronal function and behavior. Reduced expression of SynGAP-α1/2 C-terminal splice variants in mice caused severe phenotypes, including reduced survival, impaired learning, and reduced seizure latency. In contrast, upregulation of α1/2 expression improved learning and increased seizure latency. Mice expressing α1-specific mutations, which disrupted SynGAP cellular functions without altering protein expression, promoted seizure, disrupted synapse plasticity, and impaired learning. These findings demonstrate that endogenous SynGAP isoforms with α1/2 spliced sequences promote cognitive function and impart seizure protection. Regulation of SynGAP-αexpression or function may be a viable therapeutic strategy to broadly improve cognitive function and mitigate seizure.Entities:
Keywords: Syngap1; behavior; cognition; isoforms; mouse; neuroscience; seizure; splicing
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Year: 2022 PMID: 35394425 PMCID: PMC9064290 DOI: 10.7554/eLife.75707
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.713