Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density

Gespeichert in:

Bibliographische Detailangaben
Zeitschriftentitel:	Stroke
Personen und Körperschaften:	Kahl, Anja, Poon, Carrie, Rodney-Sandy, Reunet, Blanco, Ismary, Iadecola, Costantino, Hochrainer, Karin
In:	Stroke, 49, 2018, Suppl_1
Format:	E-Article
Sprache:	Englisch
veröffentlicht:	Ovid Technologies (Wolters Kluwer Health)
Schlagwörter:	Advanced and Specialized Nursing Cardiology and Cardiovascular Medicine Neurology (clinical)

author_facet	Kahl, Anja Poon, Carrie Rodney-Sandy, Reunet Blanco, Ismary Iadecola, Costantino Hochrainer, Karin Kahl, Anja Poon, Carrie Rodney-Sandy, Reunet Blanco, Ismary Iadecola, Costantino Hochrainer, Karin
author	Kahl, Anja Poon, Carrie Rodney-Sandy, Reunet Blanco, Ismary Iadecola, Costantino Hochrainer, Karin
spellingShingle	Kahl, Anja Poon, Carrie Rodney-Sandy, Reunet Blanco, Ismary Iadecola, Costantino Hochrainer, Karin Stroke Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density Advanced and Specialized Nursing Cardiology and Cardiovascular Medicine Neurology (clinical)
author_sort	kahl, anja
spelling	Kahl, Anja Poon, Carrie Rodney-Sandy, Reunet Blanco, Ismary Iadecola, Costantino Hochrainer, Karin 0039-2499 1524-4628 Ovid Technologies (Wolters Kluwer Health) Advanced and Specialized Nursing Cardiology and Cardiovascular Medicine Neurology (clinical) http://dx.doi.org/10.1161/str.49.suppl_1.31 <jats:p> <jats:bold>Background:</jats:bold> Brain calcium-calmodulin-dependent protein kinase II (CaMKII) is exclusively expressed in neurons, where it localizes to the post-synaptic density (PSD) to link calcium signals to changes in synaptic activity. Independent studies suggest that deregulation of CaMKII contributes to neuronal death associated with cerebral ischemia and could be a target for stroke therapy. However, the molecular events underlying CaMKII activity modification after ischemia are not understood. Cerebral ischemia induces ubiquitination of PSD proteins, raising the possibility that post-ischemic CaMKII function is modulated by ubiquitination. Here we investigate a novel link between CaMKIIα subunit ubiquitination and post-ischemic CaMKII regulation. </jats:p> <jats:p> <jats:bold>Methods:</jats:bold> Cerebral ischemia was induced in male C57BL6 mice by middle cerebral artery occlusion (MCAO) for 35 min. Whole tissue extracts as well as cytosolic, membrane and PSD fractions were prepared at different times after ischemia to assess CaMKIIα ubiquitination, protein levels and activity. Ubiquitination was reverted with recombinant USP2cc de-ubiquitinase. </jats:p> <jats:p> <jats:bold>Results:</jats:bold> MCAO induces CaMKIIα ubiquitination specifically in the neocortical PSD fraction peaking at 1-hour reperfusion. The ubiquitination is accompanied by translocation of CaMKIIα from cytosol/membrane to PSD (cytosol/membrane: 61±4%; PSD: 190±6% of sham, P<0.001, n=9/group), while total CaMKIIα protein levels are not affected (98±1% of sham, P=0.767, n=3/group). In the cytosol CaMKII activity normalized to protein content is not changed post-stroke (91±19% of sham; P<0.001, n=9/group), however at the PSD it is severely suppressed (31±6% of sham, P<0.001, n=9/group). De-ubiquitination leads to restoration of PSD-associated CaMKII activity (347±59% of untreated, P<0.001, n=6/group), identifying ubiquitination as reversible repressor of CaMKII activity at the PSD. </jats:p> <jats:p> <jats:bold>Conclusions:</jats:bold> CaMKIIα ubiquitination induced by cerebral ischemia-reperfusion constitutes a previously unappreciated mechanism of post-ischemic CaMKII regulation that may be important for modulating the ischemic outcome. Better understanding of how post-ischemic CaMKIIα ubiquitination is controlled may help to identify a new therapeutic stroke target. </jats:p> Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density Stroke
doi_str_mv	10.1161/str.49.suppl_1.31
facet_avail	Online Free
finc_class_facet	Medizin
format	ElectronicArticle
fullrecord	blob:ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTE2MS9zdHIuNDkuc3VwcGxfMS4zMQ
id	ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTE2MS9zdHIuNDkuc3VwcGxfMS4zMQ
institution	DE-Gla1 DE-Zi4 DE-15 DE-Pl11 DE-Rs1 DE-105 DE-14 DE-Ch1 DE-L229 DE-D275 DE-Bn3 DE-Brt1 DE-Zwi2 DE-D161
imprint	Ovid Technologies (Wolters Kluwer Health), 2018
imprint_str_mv	Ovid Technologies (Wolters Kluwer Health), 2018
issn	0039-2499 1524-4628
issn_str_mv	0039-2499 1524-4628
language	English
mega_collection	Ovid Technologies (Wolters Kluwer Health) (CrossRef)
match_str	kahl2018abstract31camkiialphaubiquitinationinducedbycerebralischemiareperfusioninjuryreversiblyinhibitspostischemiccamkiiactivityatthepostsynapticdensity
publishDateSort	2018
publisher	Ovid Technologies (Wolters Kluwer Health)
recordtype	ai
record_format	ai
series	Stroke
source_id	49
title	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_unstemmed	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_full	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_fullStr	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_full_unstemmed	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_short	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_sort	abstract 31: camkii-alpha ubiquitination induced by cerebral ischemia-reperfusion injury reversibly inhibits post-ischemic camkii activity at the post-synaptic density
topic	Advanced and Specialized Nursing Cardiology and Cardiovascular Medicine Neurology (clinical)
url	http://dx.doi.org/10.1161/str.49.suppl_1.31
publishDate	2018
physical
description	<jats:p> <jats:bold>Background:</jats:bold> Brain calcium-calmodulin-dependent protein kinase II (CaMKII) is exclusively expressed in neurons, where it localizes to the post-synaptic density (PSD) to link calcium signals to changes in synaptic activity. Independent studies suggest that deregulation of CaMKII contributes to neuronal death associated with cerebral ischemia and could be a target for stroke therapy. However, the molecular events underlying CaMKII activity modification after ischemia are not understood. Cerebral ischemia induces ubiquitination of PSD proteins, raising the possibility that post-ischemic CaMKII function is modulated by ubiquitination. Here we investigate a novel link between CaMKIIα subunit ubiquitination and post-ischemic CaMKII regulation. </jats:p> <jats:p> <jats:bold>Methods:</jats:bold> Cerebral ischemia was induced in male C57BL6 mice by middle cerebral artery occlusion (MCAO) for 35 min. Whole tissue extracts as well as cytosolic, membrane and PSD fractions were prepared at different times after ischemia to assess CaMKIIα ubiquitination, protein levels and activity. Ubiquitination was reverted with recombinant USP2cc de-ubiquitinase. </jats:p> <jats:p> <jats:bold>Results:</jats:bold> MCAO induces CaMKIIα ubiquitination specifically in the neocortical PSD fraction peaking at 1-hour reperfusion. The ubiquitination is accompanied by translocation of CaMKIIα from cytosol/membrane to PSD (cytosol/membrane: 61±4%; PSD: 190±6% of sham, P<0.001, n=9/group), while total CaMKIIα protein levels are not affected (98±1% of sham, P=0.767, n=3/group). In the cytosol CaMKII activity normalized to protein content is not changed post-stroke (91±19% of sham; P<0.001, n=9/group), however at the PSD it is severely suppressed (31±6% of sham, P<0.001, n=9/group). De-ubiquitination leads to restoration of PSD-associated CaMKII activity (347±59% of untreated, P<0.001, n=6/group), identifying ubiquitination as reversible repressor of CaMKII activity at the PSD. </jats:p> <jats:p> <jats:bold>Conclusions:</jats:bold> CaMKIIα ubiquitination induced by cerebral ischemia-reperfusion constitutes a previously unappreciated mechanism of post-ischemic CaMKII regulation that may be important for modulating the ischemic outcome. Better understanding of how post-ischemic CaMKIIα ubiquitination is controlled may help to identify a new therapeutic stroke target. </jats:p>
container_issue	Suppl_1
container_start_page	0
container_title	Stroke
container_volume	49
format_de105	Article, E-Article
format_de14	Article, E-Article
format_de15	Article, E-Article
format_de520	Article, E-Article
format_de540	Article, E-Article
format_dech1	Article, E-Article
format_ded117	Article, E-Article
format_degla1	E-Article
format_del152	Buch
format_del189	Article, E-Article
format_dezi4	Article
format_dezwi2	Article, E-Article
format_finc	Article, E-Article
format_nrw	Article, E-Article
_version_	1792323795019628553
geogr_code	not assigned
last_indexed	2024-03-01T11:39:28.496Z
geogr_code_person	not assigned
openURL	url_ver=Z39.88-2004&ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fvufind.svn.sourceforge.net%3Agenerator&rft.title=Abstract+31%3A+CaMKII-alpha+Ubiquitination+Induced+by+Cerebral+Ischemia-Reperfusion+Injury+Reversibly+Inhibits+Post-Ischemic+CaMKII+Activity+at+the+Post-Synaptic+Density&rft.date=2018-01-22&genre=article&issn=1524-4628&volume=49&issue=Suppl_1&jtitle=Stroke&atitle=Abstract+31%3A+CaMKII-alpha+Ubiquitination+Induced+by+Cerebral+Ischemia-Reperfusion+Injury+Reversibly+Inhibits+Post-Ischemic+CaMKII+Activity+at+the+Post-Synaptic+Density&aulast=Hochrainer&aufirst=Karin&rft_id=info%3Adoi%2F10.1161%2Fstr.49.suppl_1.31&rft.language%5B0%5D=eng
SOLR
_version_	1792323795019628553
author	Kahl, Anja, Poon, Carrie, Rodney-Sandy, Reunet, Blanco, Ismary, Iadecola, Costantino, Hochrainer, Karin
author_facet	Kahl, Anja, Poon, Carrie, Rodney-Sandy, Reunet, Blanco, Ismary, Iadecola, Costantino, Hochrainer, Karin, Kahl, Anja, Poon, Carrie, Rodney-Sandy, Reunet, Blanco, Ismary, Iadecola, Costantino, Hochrainer, Karin
author_sort	kahl, anja
container_issue	Suppl_1
container_start_page	0
container_title	Stroke
container_volume	49
description	<jats:p> <jats:bold>Background:</jats:bold> Brain calcium-calmodulin-dependent protein kinase II (CaMKII) is exclusively expressed in neurons, where it localizes to the post-synaptic density (PSD) to link calcium signals to changes in synaptic activity. Independent studies suggest that deregulation of CaMKII contributes to neuronal death associated with cerebral ischemia and could be a target for stroke therapy. However, the molecular events underlying CaMKII activity modification after ischemia are not understood. Cerebral ischemia induces ubiquitination of PSD proteins, raising the possibility that post-ischemic CaMKII function is modulated by ubiquitination. Here we investigate a novel link between CaMKIIα subunit ubiquitination and post-ischemic CaMKII regulation. </jats:p> <jats:p> <jats:bold>Methods:</jats:bold> Cerebral ischemia was induced in male C57BL6 mice by middle cerebral artery occlusion (MCAO) for 35 min. Whole tissue extracts as well as cytosolic, membrane and PSD fractions were prepared at different times after ischemia to assess CaMKIIα ubiquitination, protein levels and activity. Ubiquitination was reverted with recombinant USP2cc de-ubiquitinase. </jats:p> <jats:p> <jats:bold>Results:</jats:bold> MCAO induces CaMKIIα ubiquitination specifically in the neocortical PSD fraction peaking at 1-hour reperfusion. The ubiquitination is accompanied by translocation of CaMKIIα from cytosol/membrane to PSD (cytosol/membrane: 61±4%; PSD: 190±6% of sham, P<0.001, n=9/group), while total CaMKIIα protein levels are not affected (98±1% of sham, P=0.767, n=3/group). In the cytosol CaMKII activity normalized to protein content is not changed post-stroke (91±19% of sham; P<0.001, n=9/group), however at the PSD it is severely suppressed (31±6% of sham, P<0.001, n=9/group). De-ubiquitination leads to restoration of PSD-associated CaMKII activity (347±59% of untreated, P<0.001, n=6/group), identifying ubiquitination as reversible repressor of CaMKII activity at the PSD. </jats:p> <jats:p> <jats:bold>Conclusions:</jats:bold> CaMKIIα ubiquitination induced by cerebral ischemia-reperfusion constitutes a previously unappreciated mechanism of post-ischemic CaMKII regulation that may be important for modulating the ischemic outcome. Better understanding of how post-ischemic CaMKIIα ubiquitination is controlled may help to identify a new therapeutic stroke target. </jats:p>
doi_str_mv	10.1161/str.49.suppl_1.31
facet_avail	Online, Free
finc_class_facet	Medizin
format	ElectronicArticle
format_de105	Article, E-Article
format_de14	Article, E-Article
format_de15	Article, E-Article
format_de520	Article, E-Article
format_de540	Article, E-Article
format_dech1	Article, E-Article
format_ded117	Article, E-Article
format_degla1	E-Article
format_del152	Buch
format_del189	Article, E-Article
format_dezi4	Article
format_dezwi2	Article, E-Article
format_finc	Article, E-Article
format_nrw	Article, E-Article
geogr_code	not assigned
geogr_code_person	not assigned
id	ai-49-aHR0cDovL2R4LmRvaS5vcmcvMTAuMTE2MS9zdHIuNDkuc3VwcGxfMS4zMQ
imprint	Ovid Technologies (Wolters Kluwer Health), 2018
imprint_str_mv	Ovid Technologies (Wolters Kluwer Health), 2018
institution	DE-Gla1, DE-Zi4, DE-15, DE-Pl11, DE-Rs1, DE-105, DE-14, DE-Ch1, DE-L229, DE-D275, DE-Bn3, DE-Brt1, DE-Zwi2, DE-D161
issn	0039-2499, 1524-4628
issn_str_mv	0039-2499, 1524-4628
language	English
last_indexed	2024-03-01T11:39:28.496Z
match_str	kahl2018abstract31camkiialphaubiquitinationinducedbycerebralischemiareperfusioninjuryreversiblyinhibitspostischemiccamkiiactivityatthepostsynapticdensity
mega_collection	Ovid Technologies (Wolters Kluwer Health) (CrossRef)
physical
publishDate	2018
publishDateSort	2018
publisher	Ovid Technologies (Wolters Kluwer Health)
record_format	ai
recordtype	ai
series	Stroke
source_id	49
spelling	Kahl, Anja Poon, Carrie Rodney-Sandy, Reunet Blanco, Ismary Iadecola, Costantino Hochrainer, Karin 0039-2499 1524-4628 Ovid Technologies (Wolters Kluwer Health) Advanced and Specialized Nursing Cardiology and Cardiovascular Medicine Neurology (clinical) http://dx.doi.org/10.1161/str.49.suppl_1.31 <jats:p> <jats:bold>Background:</jats:bold> Brain calcium-calmodulin-dependent protein kinase II (CaMKII) is exclusively expressed in neurons, where it localizes to the post-synaptic density (PSD) to link calcium signals to changes in synaptic activity. Independent studies suggest that deregulation of CaMKII contributes to neuronal death associated with cerebral ischemia and could be a target for stroke therapy. However, the molecular events underlying CaMKII activity modification after ischemia are not understood. Cerebral ischemia induces ubiquitination of PSD proteins, raising the possibility that post-ischemic CaMKII function is modulated by ubiquitination. Here we investigate a novel link between CaMKIIα subunit ubiquitination and post-ischemic CaMKII regulation. </jats:p> <jats:p> <jats:bold>Methods:</jats:bold> Cerebral ischemia was induced in male C57BL6 mice by middle cerebral artery occlusion (MCAO) for 35 min. Whole tissue extracts as well as cytosolic, membrane and PSD fractions were prepared at different times after ischemia to assess CaMKIIα ubiquitination, protein levels and activity. Ubiquitination was reverted with recombinant USP2cc de-ubiquitinase. </jats:p> <jats:p> <jats:bold>Results:</jats:bold> MCAO induces CaMKIIα ubiquitination specifically in the neocortical PSD fraction peaking at 1-hour reperfusion. The ubiquitination is accompanied by translocation of CaMKIIα from cytosol/membrane to PSD (cytosol/membrane: 61±4%; PSD: 190±6% of sham, P<0.001, n=9/group), while total CaMKIIα protein levels are not affected (98±1% of sham, P=0.767, n=3/group). In the cytosol CaMKII activity normalized to protein content is not changed post-stroke (91±19% of sham; P<0.001, n=9/group), however at the PSD it is severely suppressed (31±6% of sham, P<0.001, n=9/group). De-ubiquitination leads to restoration of PSD-associated CaMKII activity (347±59% of untreated, P<0.001, n=6/group), identifying ubiquitination as reversible repressor of CaMKII activity at the PSD. </jats:p> <jats:p> <jats:bold>Conclusions:</jats:bold> CaMKIIα ubiquitination induced by cerebral ischemia-reperfusion constitutes a previously unappreciated mechanism of post-ischemic CaMKII regulation that may be important for modulating the ischemic outcome. Better understanding of how post-ischemic CaMKIIα ubiquitination is controlled may help to identify a new therapeutic stroke target. </jats:p> Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density Stroke
spellingShingle	Kahl, Anja, Poon, Carrie, Rodney-Sandy, Reunet, Blanco, Ismary, Iadecola, Costantino, Hochrainer, Karin, Stroke, Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density, Advanced and Specialized Nursing, Cardiology and Cardiovascular Medicine, Neurology (clinical)
title	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_full	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_fullStr	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_full_unstemmed	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_short	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
title_sort	abstract 31: camkii-alpha ubiquitination induced by cerebral ischemia-reperfusion injury reversibly inhibits post-ischemic camkii activity at the post-synaptic density
title_unstemmed	Abstract 31: CaMKII-alpha Ubiquitination Induced by Cerebral Ischemia-Reperfusion Injury Reversibly Inhibits Post-Ischemic CaMKII Activity at the Post-Synaptic Density
topic	Advanced and Specialized Nursing, Cardiology and Cardiovascular Medicine, Neurology (clinical)
url	http://dx.doi.org/10.1161/str.49.suppl_1.31