| Literature DB >> 35146426 |
Michael J Rigby1,2,3, Nicola Salvatore Orefice1,2, Alexis J Lawton4, Min Ma5, Samantha L Shapiro1,2, Sue Y Yi3, Inca A Dieterich1,2,3, Alyssa Frelka6, Hannah N Miles5, Robert A Pearce6, John Paul J Yu7, Lingjun Li5, John M Denu4, Luigi Puglielli1,2,8.
Abstract
Endoplasmic reticulum-based N ɛ-lysine acetylation serves as an important protein quality control system for the secretory pathway. Dysfunctional endoplasmic reticulum-based acetylation, as caused by overexpression of the acetyl coenzyme A transporter AT-1 in the mouse, results in altered glycoprotein flux through the secretory pathway and an autistic-like phenotype. AT-1 works in concert with SLC25A1, the citrate/malate antiporter in the mitochondria, SLC13A5, the plasma membrane sodium/citrate symporter and ATP citrate lyase, the cytosolic enzyme that converts citrate into acetyl coenzyme A. Here, we report that mice with neuron-specific overexpression of SLC13A5 exhibit autistic-like behaviours with a jumping stereotypy. The mice displayed disrupted white matter integrity and altered synaptic structure and function. Analysis of both the proteome and acetyl-proteome revealed unique adaptations in the hippocampus and cortex, highlighting a metabolic response that likely plays an important role in the SLC13A5 neuron transgenic phenotype. Overall, our results support a mechanistic link between aberrant intracellular citrate/acetyl coenzyme A flux and the development of an autistic-like phenotype. Published by Oxford University Press on behalf of the Guarantors of Brain 2022. This work is written by (a) US Government employee(s) and is in the public domain in the US.Entities:
Keywords: AT-1; SLC13A5; acetyl-CoA; citrate; lysine acetylation
Year: 2022 PMID: 35146426 PMCID: PMC8823335 DOI: 10.1093/braincomms/fcac002
Source DB: PubMed Journal: Brain Commun ISSN: 2632-1297