The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation

BACKGROUND: The P2X(7) receptor binds extracellular ATP to mediate numerous inflammatory responses and is considered a potential biomarker and therapeutic target for diverse inflammatory and neurological diseases. P2X(7) contains many single nucleotide polymorphisms, including several mutations loca...

Descripción completa

Detalles Bibliográficos
Autores principales: Wickert, Lisa E., Blanchette, Joshua B., Waldschmidt, Noelle V., Bertics, Paul J., Denu, John M., Denlinger, Loren C., Lenertz, Lisa Y.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3653848/
https://www.ncbi.nlm.nih.gov/pubmed/23691096
http://dx.doi.org/10.1371/journal.pone.0063789
_version_ 1782269459459735552
author Wickert, Lisa E.
Blanchette, Joshua B.
Waldschmidt, Noelle V.
Bertics, Paul J.
Denu, John M.
Denlinger, Loren C.
Lenertz, Lisa Y.
author_facet Wickert, Lisa E.
Blanchette, Joshua B.
Waldschmidt, Noelle V.
Bertics, Paul J.
Denu, John M.
Denlinger, Loren C.
Lenertz, Lisa Y.
author_sort Wickert, Lisa E.
collection PubMed
description BACKGROUND: The P2X(7) receptor binds extracellular ATP to mediate numerous inflammatory responses and is considered a potential biomarker and therapeutic target for diverse inflammatory and neurological diseases. P2X(7) contains many single nucleotide polymorphisms, including several mutations located within its intracellular C-terminal trafficking domain. Mutations within the trafficking domain result in attenuated receptor activity and cell surface presentation, but the mechanisms by which amino acid changes within this region promote altered P2X(7) function have not been elucidated. METHODS AND RESULTS: We analyzed the amino acid sequence of P2X(7) for any potential trafficking signals and found that P2X(7) contains putative Arg-X-Arg ER retention sequences. Alanine substitutions near or within these sequences were constructed, and we determined that single mutation of R574 and R578 but not R576 or K579 attenuates P2X(7)-stimulated activation of ERK1/2 and induction of the transcription factors FosB and ΔFosB. We found that mutation of R578 within the trafficking domain to the naturally occurring Gln substitution disrupts P2X(7) localization at the plasma membrane and results in R578Q displaying a higher apparent molecular weight in comparison to wild-type receptor. We used the glycosidase endoglycosidase H to determine that this difference in mass is due in part to the R578Q mutant possessing a larger mass of oligosaccharides, indicative of improper N-linked glycosylation addition and/or trimming. Chemical cross-linking experiments were also performed and suggest that the R578Q variant also does not form trimers as well as wild-type receptor, a function required for its full activity. CONCLUSIONS: These data demonstrate the distal C-terminus of P2X(7) is important for oligomerization and post-translational modification of the receptor, providing a mechanism by which mutations in the trafficking domain disrupt P2X(7) activity and localization at the plasma membrane.
format Online
Article
Text
id pubmed-3653848
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-36538482013-05-20 The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation Wickert, Lisa E. Blanchette, Joshua B. Waldschmidt, Noelle V. Bertics, Paul J. Denu, John M. Denlinger, Loren C. Lenertz, Lisa Y. PLoS One Research Article BACKGROUND: The P2X(7) receptor binds extracellular ATP to mediate numerous inflammatory responses and is considered a potential biomarker and therapeutic target for diverse inflammatory and neurological diseases. P2X(7) contains many single nucleotide polymorphisms, including several mutations located within its intracellular C-terminal trafficking domain. Mutations within the trafficking domain result in attenuated receptor activity and cell surface presentation, but the mechanisms by which amino acid changes within this region promote altered P2X(7) function have not been elucidated. METHODS AND RESULTS: We analyzed the amino acid sequence of P2X(7) for any potential trafficking signals and found that P2X(7) contains putative Arg-X-Arg ER retention sequences. Alanine substitutions near or within these sequences were constructed, and we determined that single mutation of R574 and R578 but not R576 or K579 attenuates P2X(7)-stimulated activation of ERK1/2 and induction of the transcription factors FosB and ΔFosB. We found that mutation of R578 within the trafficking domain to the naturally occurring Gln substitution disrupts P2X(7) localization at the plasma membrane and results in R578Q displaying a higher apparent molecular weight in comparison to wild-type receptor. We used the glycosidase endoglycosidase H to determine that this difference in mass is due in part to the R578Q mutant possessing a larger mass of oligosaccharides, indicative of improper N-linked glycosylation addition and/or trimming. Chemical cross-linking experiments were also performed and suggest that the R578Q variant also does not form trimers as well as wild-type receptor, a function required for its full activity. CONCLUSIONS: These data demonstrate the distal C-terminus of P2X(7) is important for oligomerization and post-translational modification of the receptor, providing a mechanism by which mutations in the trafficking domain disrupt P2X(7) activity and localization at the plasma membrane. Public Library of Science 2013-05-14 /pmc/articles/PMC3653848/ /pubmed/23691096 http://dx.doi.org/10.1371/journal.pone.0063789 Text en © 2013 Wickert et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Wickert, Lisa E.
Blanchette, Joshua B.
Waldschmidt, Noelle V.
Bertics, Paul J.
Denu, John M.
Denlinger, Loren C.
Lenertz, Lisa Y.
The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation
title The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation
title_full The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation
title_fullStr The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation
title_full_unstemmed The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation
title_short The C-Terminus of Human Nucleotide Receptor P2X7 Is Critical for Receptor Oligomerization and N-Linked Glycosylation
title_sort c-terminus of human nucleotide receptor p2x7 is critical for receptor oligomerization and n-linked glycosylation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3653848/
https://www.ncbi.nlm.nih.gov/pubmed/23691096
http://dx.doi.org/10.1371/journal.pone.0063789
work_keys_str_mv AT wickertlisae thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT blanchettejoshuab thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT waldschmidtnoellev thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT berticspaulj thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT denujohnm thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT denlingerlorenc thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT lenertzlisay thecterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT wickertlisae cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT blanchettejoshuab cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT waldschmidtnoellev cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT berticspaulj cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT denujohnm cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT denlingerlorenc cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation
AT lenertzlisay cterminusofhumannucleotidereceptorp2x7iscriticalforreceptoroligomerizationandnlinkedglycosylation

Ejemplares similares