BACKGROUND: Phospholemman regulates the plasmalemmal sodium pump in excitable tissues. RESULTS: In cardiac muscle, a subpopulation of phospholemman with a unique phosphorylation signature associates with other phospholemman molecules but not with the pump. CONCLUSION: Phospholemman oligomers exist in cardiac muscle. SIGNIFICANCE: Much like phospholamban regulation of SERCA, phospholemman exists as both a sodium pump inhibiting monomer and an unassociated oligomer. Phospholemman (PLM), the principal quantitative sarcolemmal substrate for protein kinases A and C in the heart, regulates the cardiac sodium pump. Much like phospholamban, which regulates the related ATPase SERCA, PLM is reported to oligomerize. We investigated subpopulations of PLM in adult rat ventricular myocytes based on phosphorylation status. Co-immunoprecipitation identified two pools of PLM: one not associated with the sodium pump phosphorylated at Ser(63) and one associated with the pump, both phosphorylated at Ser(68) and unphosphorylated. Phosphorylation of PLM at Ser(63) following activation of PKC did not abrogate association of PLM with the pump, so its failure to associate with the pump was not due to phosphorylation at this site. All pools of PLM co-localized to cell surface caveolin-enriched microdomains with sodium pump α subunits, despite the lack of caveolin-binding motif in PLM. Mass spectrometry analysis of phosphospecific immunoprecipitation reactions revealed no unique protein interactions for Ser(63)-phosphorylated PLM, and cross-linking reagents also failed to identify any partner proteins for this pool. In lysates from hearts of heterozygous transgenic animals expressing wild type and unphosphorylatable PLM, Ser(63)-phosphorylated PLM co-immunoprecipitated unphosphorylatable PLM, confirming the existence of PLM multimers. Dephosphorylation of the PLM multimer does not change sodium pump activity. Hence like phospholamban, PLM exists as a pump-inhibiting monomer and an unassociated oligomer. The distribution of different PLM phosphorylation states to different pools may be explained by their differential proximity to protein phosphatases rather than a direct effect of phosphorylation on PLM association with the pump.
BACKGROUND: Phospholemman regulates the plasmalemmal sodium pump in excitable tissues. RESULTS: In cardiac muscle, a subpopulation of phospholemman with a unique phosphorylation signature associates with other phospholemman molecules but not with the pump. CONCLUSION: Phospholemman oligomers exist in cardiac muscle. SIGNIFICANCE: Much like phospholamban regulation of SERCA, phospholemman exists as both a sodium pump inhibiting monomer and an unassociated oligomer. Phospholemman (PLM), the principal quantitative sarcolemmal substrate for protein kinases A and C in the heart, regulates the cardiac sodium pump. Much like phospholamban, which regulates the related ATPase SERCA, PLM is reported to oligomerize. We investigated subpopulations of PLM in adult rat ventricular myocytes based on phosphorylation status. Co-immunoprecipitation identified two pools of PLM: one not associated with the sodium pump phosphorylated at Ser(63) and one associated with the pump, both phosphorylated at Ser(68) and unphosphorylated. Phosphorylation of PLM at Ser(63) following activation of PKC did not abrogate association of PLM with the pump, so its failure to associate with the pump was not due to phosphorylation at this site. All pools of PLM co-localized to cell surface caveolin-enriched microdomains with sodium pump α subunits, despite the lack of caveolin-binding motif in PLM. Mass spectrometry analysis of phosphospecific immunoprecipitation reactions revealed no unique protein interactions for Ser(63)-phosphorylated PLM, and cross-linking reagents also failed to identify any partner proteins for this pool. In lysates from hearts of heterozygous transgenic animals expressing wild type and unphosphorylatable PLM, Ser(63)-phosphorylated PLM co-immunoprecipitated unphosphorylatable PLM, confirming the existence of PLM multimers. Dephosphorylation of the PLM multimer does not change sodium pump activity. Hence like phospholamban, PLM exists as a pump-inhibiting monomer and an unassociated oligomer. The distribution of different PLM phosphorylation states to different pools may be explained by their differential proximity to protein phosphatases rather than a direct effect of phosphorylation on PLM association with the pump.
Entities:
Keywords:
Caveolae; FXYD Proteins; Heart; Na,K-ATPase; PP2A; Phospholemman; Protein Palmitoylation; Protein Phosphatase; Protein Phosphorylation; Serine-Threonine Protein Phosphatase
Authors: Miyoun Hong; Eirini Kefaloyianni; Li Bao; Brian Malester; Diane Delaroche; Thomas A Neubert; William A Coetzee Journal: FASEB J Date: 2011-04-11 Impact factor: 5.191
Authors: Gilles Crambert; Maria Fuzesi; Haim Garty; Steven Karlish; Kathi Geering Journal: Proc Natl Acad Sci U S A Date: 2002-08-08 Impact factor: 11.205
Authors: J R Moorman; S J Ackerman; G C Kowdley; M P Griffin; J P Mounsey; Z Chen; S E Cala; J J O'Brian; G Szabo; L R Jones Journal: Nature Date: 1995-10-26 Impact factor: 49.962
Authors: Palanikumar Manoharan; Tatiana L Radzyukevich; Hesamedin Hakim Javadi; Cory A Stiner; Julio A Landero Figueroa; Jerry B Lingrel; Judith A Heiny Journal: Am J Physiol Cell Physiol Date: 2015-10-14 Impact factor: 4.249
Authors: Ryan D Himes; Nikolai Smolin; Andreas Kukol; Julie Bossuyt; Donald M Bers; Seth L Robia Journal: Biochemistry Date: 2016-10-25 Impact factor: 3.162
Authors: Arthur M Feldman; Jennifer Gordon; JuFang Wang; Jianliang Song; Xue-Qian Zhang; Valerie D Myers; Douglas G Tilley; Erhe Gao; Nicholas E Hoffman; Dhanendra Tomar; Muniswamy Madesh; Joseph Rabinowitz; Walter J Koch; Feifei Su; Kamel Khalili; Joseph Y Cheung Journal: J Mol Cell Cardiol Date: 2016-01-19 Impact factor: 5.000
Authors: Zeynep Bastug-Özel; Peter T Wright; Axel E Kraft; Davor Pavlovic; Jacqueline Howie; Alexander Froese; William Fuller; Julia Gorelik; Michael J Shattock; Viacheslav O Nikolaev Journal: Cardiovasc Res Date: 2019-03-01 Impact factor: 10.787
Authors: Krzysztof J Wypijewski; Michele Tinti; Wenzhang Chen; Douglas Lamont; Michael L J Ashford; Sarah C Calaghan; William Fuller Journal: Mol Cell Proteomics Date: 2015-01-05 Impact factor: 5.911
Authors: Louise Reilly; Jacqueline Howie; Krzysztof Wypijewski; Michael L J Ashford; Donald W Hilgemann; William Fuller Journal: FASEB J Date: 2015-07-14 Impact factor: 5.191
Authors: Tandekile Lubelwana Hafver; Kjetil Hodne; Pimthanya Wanichawan; Jan Magnus Aronsen; Bjørn Dalhus; Per Kristian Lunde; Marianne Lunde; Marita Martinsen; Ulla Helene Enger; William Fuller; Ivar Sjaastad; William Edward Louch; Ole Mathias Sejersted; Cathrine Rein Carlson Journal: J Biol Chem Date: 2015-12-14 Impact factor: 5.157
Authors: Jacqueline Howie; Louise Reilly; Niall J Fraser; Julia M Vlachaki Walker; Krzysztof J Wypijewski; Michael L J Ashford; Sarah C Calaghan; Heather McClafferty; Lijun Tian; Michael J Shipston; Andrii Boguslavskyi; Michael J Shattock; William Fuller Journal: Proc Natl Acad Sci U S A Date: 2014-11-24 Impact factor: 11.205