| Literature DB >> 32991906 |
Laura Trobiani1, Maria Meringolo2, Tamara Diamanti1, Yves Bourne3, Pascale Marchot3, Giuseppina Martella2, Luciana Dini1, Antonio Pisani2, Antonella De Jaco4, Paola Bonsi5.
Abstract
The genetics underlying autism spectrum disorder (ASD) is complex and heterogeneous, and de novo variants are found in genes converging in functional biological processes. Neuronal communication, including trans-synaptic signaling involving two families of cell-adhesion proteins, the presynaptic neurexins and the postsynaptic neuroligins, is one of the most recurrently affected pathways in ASD. Given the role of these proteins in determining synaptic function, abnormal synaptic plasticity and failure to establish proper synaptic contacts might represent mechanisms underlying risk of ASD. More than 30 mutations have been found in the neuroligin genes. Most of the resulting residue substitutions map in the extracellular, cholinesterase-like domain of the protein, and impair protein folding and trafficking. Conversely, the stalk and intracellular domains are less affected. Accordingly, several genetic animal models of ASD have been generated, showing behavioral and synaptic alterations. The aim of this review is to discuss the current knowledge on ASD-linked mutations in the neuroligin proteins and their effect on synaptic function, in various brain areas and circuits.Entities:
Keywords: Animal model; Behaviour; Endoplasmic reticulum; Genetics; Homeostatic mechanisms; Misfolding; Physiology; Synaptic plasticity; Trafficking; Unfolded protein response; excitatory/inhibitory balance
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Year: 2020 PMID: 32991906 DOI: 10.1016/j.neubiorev.2020.09.017
Source DB: PubMed Journal: Neurosci Biobehav Rev ISSN: 0149-7634 Impact factor: 8.989