| Literature DB >> 33945465 |
Michael Bucher1,2,3, Stephan Niebling4, Yuhao Han2,5, Dmitry Molodenskiy6, Fatemeh Hassani Nia7, Hans-Jürgen Kreienkamp7, Dmitri Svergun6, Eunjoon Kim8, Alla S Kostyukova2,9, Michael R Kreutz3,10,11,12, Marina Mikhaylova1,2.
Abstract
Members of the SH3- and ankyrin repeat (SHANK) protein family are considered as master scaffolds of the postsynaptic density of glutamatergic synapses. Several missense mutations within the canonical SHANK3 isoform have been proposed as causative for the development of autism spectrum disorders (ASDs). However, there is a surprising paucity of data linking missense mutation-induced changes in protein structure and dynamics to the occurrence of ASD-related synaptic phenotypes. In this proof-of-principle study, we focus on two ASD-associated point mutations, both located within the same domain of SHANK3 and demonstrate that both mutant proteins indeed show distinct changes in secondary and tertiary structure as well as higher conformational fluctuations. Local and distal structural disturbances result in altered synaptic targeting and changes of protein turnover at synaptic sites in rat primary hippocampal neurons.Entities:
Keywords: SHANK3; autism; conformational dynamics; neuroscience; postsynaptic density; protein folding; rat; synaptic protein turnover
Year: 2021 PMID: 33945465 PMCID: PMC8169116 DOI: 10.7554/eLife.66165
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140