Selective Disruption of Metabotropic Glutamate Receptor 5-Homer Interactions Mimics Phenotypes of Fragile X Syndrome in Mice

Guo, Weirui; Molinaro, Gemma; Collins, Katie A.; Hays, Seth A.; Paylor, Richard; Worley, Paul F.; Szumlinski, Karen K.; Huber, Kimberly M.

doi:10.1523/jneurosci.2921-15.2016

Cited by 54 publications

(62 citation statements)

References 93 publications

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“…Alternatively, widespread dissociation of scaffold proteins may allow for the competitive capture of dendritic proteins, expansion of the synapse, and an increase in synaptic strength (22). Decreased association of Homer_mGluR5 itself has been crucially implicated in both normal mGluR5 signaling and the pathophysiology of Fragile X syndrome (19,29,44), further supporting the physiological relevance of our findings in NP-40 and Triton conditions. Collectively, our data support a model in which strong synaptic stimulation elicits widespread dissociation of multiprotein complexes localized to the PSD.…”

Section: Discussionsupporting

confidence: 79%

“…We initially examined the effect of lysis buffer reagents on Homer_mGluR5, a well characterized synaptic protein interaction known to play an important role in glutamatergic signaling (19,26,29,35). Significantly more Homer_mGluR5 co-association was detected in NP-40 and Triton compared to DOC ( Figure 3B, C).…”

Section: Resultsmentioning

confidence: 99%

“…We find this unlikely for three reasons: first, we confirmed by SEC fractionation that both NP-40 and Triton solubilize high MW complexes that contain 4 well known PSD associated proteins: Homer, mGluR5, PSD-95, and SynGAP. Second, we recapitulated two well-known activity dependent interactions that have been localized to within the PSD, dissociation of Homer_mGluR5 (29) and SynGAP_PSD95 (22). We find it unlikely that the high MW multiprotein complexes observed by SEC-western in NP-40 or Triton conditions are both composed of PSD-associated proteins, and exhibit activity-dependent dynamics similar to the PSD, but are not actually part of the PSD.…”

Section: Discussionmentioning

confidence: 99%

“…However, because the PSD, as it is traditionally defined, is not soluble in NP40, it is unclear if these dissociations represent proteins localized to the PSD, or a group of peri-synaptic proteins. The Huber group showed that levels of mGluR5 found in a PSD fraction are also reduced following activity, suggesting direct relevance of the mGluR-Homer dissociation (29). Similarly, Frank et al (11) reported that PSDassociated protein super-complexes were consistent across five different detergents.…”

Section: Introductionmentioning

confidence: 97%

“…While many large protein complexes do survive DOC solubilization and have been extensively characterized by mass spectrometry and other approaches (7,11,26,27), interactions that might be present at the native PSD but that do not survive DOC solubilization may remain biochemically uncharacterized. Recently, we and others have reported activitydependent changes in protein co-associations involving presumably synaptic proteins using the relatively gentle, non-ionic detergent NP-40 (18,19,28,29). For example, Ronesi et.…”

Section: Introductionmentioning

confidence: 99%

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Activity-dependent changes in synaptic protein complex composition are consistent in different detergents despite differential solubility

Lautz¹,

Gniffke²,

Brown

et al. 2019

Preprint

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At the post-synaptic density (PSD), large protein complexes dynamically form and dissociate in response to synaptic activity, comprising the biophysical basis for learning and memory. The use of detergents to both isolate the PSD fraction and release its membrane-associated proteins complicates studies of these activity-dependent protein interaction networks, because detergents can simultaneously disrupt the very interactions under study. Despite widespread recognition that different detergents yield different experimental results, the effect of detergent on activity-dependent synaptic protein complexes has not been rigorously examined. Here, we characterize the effect of three detergents commonly used to study synaptic proteins on activitydependent protein interactions. We first demonstrate that SynGAP-containing interactions are more abundant in 1% Deoxycholate (DOC), while Shank-, Homer-and mGluR5-containing interactions are more abundant in 1% NP-40 or Triton. All interactions were detected preferentially in high molecular weight (HMW) complexes generated by size exclusion chromatography, although the detergent-specific abundance of proteins in HMW fractions did not correlate with the abundance of detected interactions. Activity-dependent changes in protein complexes were consistent across detergent types, suggesting that detergents do not isolate distinct protein pools with unique behaviors. However, detection of activity-dependent changes is more or less feasible in different detergents due to baseline solubility. Collectively, our results demonstrate that detergents affect the solubility of individual proteins, but activity-dependent changes in protein interactions, when detectable, are consistent across detergent types.

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Section: Discussionsupporting

confidence: 79%