PSD-95 and PSD-93 Play Critical But Distinct Roles in Synaptic Scaling Up and Down

Abstract: Synaptic scaling stabilizes neuronal firing through the homeostatic regulation of postsynaptic strength, but the mechanisms by which chronic changes in activity lead to bidirectional adjustments in synaptic AMPAR abundance are incompletely understood. Further, it remains unclear to what extent scaling up and scaling down utilize distinct molecular machinery. PSD-95 is a scaffold protein proposed to serve as a binding “slot” that determines synaptic AMPAR content, and synaptic PSD-95 abundance is regulated by a… Show more

“…This is consistent with our previous finding that PSD-95 knockdown reduces metabotropic excitatory postsynaptic current frequency in old but not young neurons [29]. Between DIV 7 and DIV 14 the levels of synaptic PSD-95 increase substantially [28,29], and it has been shown that postsynaptic densities share and compete for PSD-95 [5,7]. As the acquisition of PSD-95 is probably regulated by changes in activity and experience [5, 45,46] when PSD-95 levels are low early in development, competition for PSD-95 could help determine which synapses are maintained and which are lost.…”

“…This is consistent with our previous finding that PSD-95 knockdown reduces metabotropic excitatory postsynaptic current frequency in old but not young neurons [29]. Between DIV 7 and DIV 14 the levels of synaptic PSD-95 increase substantially [28,29], and it has been shown that postsynaptic densities share and compete for PSD-95 [5,7].…”

“…Interestingly, PDS-95 overexpression did not affect the ratio of contact gain to loss, as this ratio remained close to unity across ages and PSD-95 expression levels (figure 5b). These data show that PSD-95 overexpression in young neurons enhances the stability of putative synaptic contacts, while having little impact on older synapses that express more endogenous PSD-95 [29].…”

“…PSD-95 binds indirectly to a-amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptor (AMPAR), regulates synaptic strength, and has been proposed to serve as a 'slot' protein that directly determines synaptic AMPAR content [36][37][38][39]. Manipulations of PSD-95 can dramatically alter evoked synaptic transmission [23,25,37,[40][41][42][43]], but we found previously that PSD-95 overexpression or knockdown in this same culture system did not significantly increase AMPA quantal amplitude [29], in keeping with other reports of only modest effects [5,23,37,40,41,44]. The modest impact of PSD-95 on quantal amplitude, coupled with the substantial impact on synapse stability shown here and suggested previously [31], suggest that the effects of PSD-95 overexpression on evoked transmission are primarily due to an enhancement of the number of stable, functional synapses.…”

“…We have shown so far that stable AD contacts have a higher ratio of active to inactive CaMKII and an enhanced accumulation of PSD-95. The synaptic localization of PSD-95 increases developmentally and with time in vitro [28,29], and there is ample evidence that PSD-95 overexpression can enhance the number of synapses in immature neurons [20,21,23,35], suggesting an important role for PSD-95 in some aspect of excitatory synapse formation. However, it is not known whether PSD-95 exerts its effects by enhancing the rate of synapse formation, or by enhancing the stability of newly formed contacts.…”

PSD-95 promotes the stabilization of young synaptic contacts

“…This is consistent with our previous finding that PSD-95 knockdown reduces metabotropic excitatory postsynaptic current frequency in old but not young neurons [29]. Between DIV 7 and DIV 14 the levels of synaptic PSD-95 increase substantially [28,29], and it has been shown that postsynaptic densities share and compete for PSD-95 [5,7]. As the acquisition of PSD-95 is probably regulated by changes in activity and experience [5, 45,46] when PSD-95 levels are low early in development, competition for PSD-95 could help determine which synapses are maintained and which are lost.…”

“…This is consistent with our previous finding that PSD-95 knockdown reduces metabotropic excitatory postsynaptic current frequency in old but not young neurons [29]. Between DIV 7 and DIV 14 the levels of synaptic PSD-95 increase substantially [28,29], and it has been shown that postsynaptic densities share and compete for PSD-95 [5,7].…”

“…Interestingly, PDS-95 overexpression did not affect the ratio of contact gain to loss, as this ratio remained close to unity across ages and PSD-95 expression levels (figure 5b). These data show that PSD-95 overexpression in young neurons enhances the stability of putative synaptic contacts, while having little impact on older synapses that express more endogenous PSD-95 [29].…”

“…PSD-95 binds indirectly to a-amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptor (AMPAR), regulates synaptic strength, and has been proposed to serve as a 'slot' protein that directly determines synaptic AMPAR content [36][37][38][39]. Manipulations of PSD-95 can dramatically alter evoked synaptic transmission [23,25,37,[40][41][42][43]], but we found previously that PSD-95 overexpression or knockdown in this same culture system did not significantly increase AMPA quantal amplitude [29], in keeping with other reports of only modest effects [5,23,37,40,41,44]. The modest impact of PSD-95 on quantal amplitude, coupled with the substantial impact on synapse stability shown here and suggested previously [31], suggest that the effects of PSD-95 overexpression on evoked transmission are primarily due to an enhancement of the number of stable, functional synapses.…”

“…We have shown so far that stable AD contacts have a higher ratio of active to inactive CaMKII and an enhanced accumulation of PSD-95. The synaptic localization of PSD-95 increases developmentally and with time in vitro [28,29], and there is ample evidence that PSD-95 overexpression can enhance the number of synapses in immature neurons [20,21,23,35], suggesting an important role for PSD-95 in some aspect of excitatory synapse formation. However, it is not known whether PSD-95 exerts its effects by enhancing the rate of synapse formation, or by enhancing the stability of newly formed contacts.…”

PSD-95 promotes the stabilization of young synaptic contacts

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