2011
DOI: 10.1074/jbc.m111.271593
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Molecular Characterization of Disrupted in Schizophrenia-1 Risk Variant S704C Reveals the Formation of Altered Oligomeric Assembly

Abstract: Background: A schizophrenia risk DISC1 polymorphism (S704C) shows phenotypic variations in hippocampus structure and associated memory defects. Results: DISC1 forms octamers via dimers as building blocks. S704C forms higher-order oligomers, without affecting its affinity with NDEL1. Conclusion: Schizophrenia risk DISC1-S704C polymorphism has altered oligomeric assembly. Significance: The improper oligomeric assembly of DISC1-S704C provides a clue in understanding the molecular basis of the known phenotype.

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Cited by 27 publications
(43 citation statements)
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“…Of particular interest in this respect, a C-terminal DISC1 (640-854) fragment expressed in Escherichia coli was shown to interact with NDEL1 when the fragment was in an octameric form in a cell free assay (Leliveld et al, 2008), a finding that was later corroborated with full-length DISC1 (Narayanan et al, 2011). These findings suggest that the multimerization state of DISC1 may critically influence its protein interactions (Brandon et al, 2009).…”
Section: Does Disc1 Fit With These Criteria For a Classical Scaffold supporting
confidence: 51%
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“…Of particular interest in this respect, a C-terminal DISC1 (640-854) fragment expressed in Escherichia coli was shown to interact with NDEL1 when the fragment was in an octameric form in a cell free assay (Leliveld et al, 2008), a finding that was later corroborated with full-length DISC1 (Narayanan et al, 2011). These findings suggest that the multimerization state of DISC1 may critically influence its protein interactions (Brandon et al, 2009).…”
Section: Does Disc1 Fit With These Criteria For a Classical Scaffold supporting
confidence: 51%
“…NDEL1 has been shown to interact with octameric, and depending on the assay used potentially dimeric, forms of DISC1, but not with higher-order oligomers (Leliveld et al, 2008;Narayanan et al, 2011), indicating that the interactions exhibit conformational specificity along with domain specificity. This also raises the obvious possibility of oligomer-specific interactions making DISC1 a multi-potent scaffold protein.…”
Section: Discussionmentioning
confidence: 99%
“…We chose to include common variants C704 and F607 as they are frequent in the normal population 43 and have been demonstrated to increase the risk to mental illness 4 and, in biophysical studies, DISC1 misassembly. 6, 7 The PrP promoter was utilized for two reasons: first, it provides pan-cellular expression in the brain that has previously been demonstrated for DISC1 44 and, second, it leads to sufficient expression levels for inducing misassembly as successfully demonstrated in non-prion animal models of protein conformational disease. 45, 46 The PrP promoter is broadly active at embryonic day E13.5 in the mouse brain 47 and continues to be expressed into adulthood, while the Disc1 gene has two expression peaks at E13.5 and around postnatal day P35.…”
Section: Resultsmentioning
confidence: 99%
“…6, 7 Both polymorphisms are common alleles that do not predict mental illness as opposed to mutations. Therefore, when evaluating the potential contribution of these polymorphisms on the observed phenotypes, genetic and protein aggregation effects cannot be separated because both phenomena are linked.…”
Section: Discussionmentioning
confidence: 99%
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