Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis

Lipolysis in adipocytes is regulated by phosphorylation of lipid droplet-associated proteins, including perilipin 1A and hormone-sensitive lipase (HSL). Perilipin 1A is potentially phosphorylated by cAMP(adenosine 3′,5′-cyclic monophosphate)-dependent protein kinase (PKA) on several sites, including...

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Autores principales: McDonough, Patrick M., Maciejewski-Lenoir, Dominique, Hartig, Sean M., Hanna, Rita A., Whittaker, Ross, Heisel, Andrew, Nicoll, James B., Buehrer, Benjamin M., Christensen, Kurt, Mancini, Maureen G., Mancini, Michael A., Edwards, Dean P., Price, Jeffrey H.
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/PMC3566132/
https://www.ncbi.nlm.nih.gov/pubmed/23405163
http://dx.doi.org/10.1371/journal.pone.0055511
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author McDonough, Patrick M.
Maciejewski-Lenoir, Dominique
Hartig, Sean M.
Hanna, Rita A.
Whittaker, Ross
Heisel, Andrew
Nicoll, James B.
Buehrer, Benjamin M.
Christensen, Kurt
Mancini, Maureen G.
Mancini, Michael A.
Edwards, Dean P.
Price, Jeffrey H.
author_facet McDonough, Patrick M.
Maciejewski-Lenoir, Dominique
Hartig, Sean M.
Hanna, Rita A.
Whittaker, Ross
Heisel, Andrew
Nicoll, James B.
Buehrer, Benjamin M.
Christensen, Kurt
Mancini, Maureen G.
Mancini, Michael A.
Edwards, Dean P.
Price, Jeffrey H.
author_sort McDonough, Patrick M.
collection PubMed
description Lipolysis in adipocytes is regulated by phosphorylation of lipid droplet-associated proteins, including perilipin 1A and hormone-sensitive lipase (HSL). Perilipin 1A is potentially phosphorylated by cAMP(adenosine 3′,5′-cyclic monophosphate)-dependent protein kinase (PKA) on several sites, including conserved C-terminal residues, serine 497 (PKA-site 5) and serine 522 (PKA-site 6). To characterize perilipin 1A phosphorylation, novel monoclonal antibodies were developed, which selectively recognize perilipin 1A phosphorylation at PKA-site 5 and PKA-site 6. Utilizing these novel antibodies, as well as antibodies selectively recognizing HSL phosphorylation at serine 563 or serine 660, we used high content analysis to examine the phosphorylation of perilipin 1A and HSL in adipocytes exposed to lipolytic agents. We found that perilipin PKA-site 5 and HSL-serine 660 were phosphorylated to a similar extent in response to forskolin (FSK) and L-γ-melanocyte stimulating hormone (L-γ-MSH). In contrast, perilipin PKA-site 6 and HSL-serine 563 were phosphorylated more slowly and L-γ-MSH was a stronger agonist for these sites compared to FSK. When a panel of lipolytic agents was tested, including multiple concentrations of isoproterenol, FSK, and L-γ-MSH, the pattern of results was virtually identical for perilipin PKA-site 5 and HSL-serine 660, whereas a distinct pattern was observed for perilipin PKA-site 6 and HSL-serine 563. Notably, perilipin PKA-site 5 and HSL-serine 660 feature two arginine residues upstream from the phospho-acceptor site, which confers high affinity for PKA, whereas perilipin PKA-site 6 and HSL-serine 563 feature only a single arginine. Thus, we suggest perilipin 1A and HSL are differentially phosphorylated in a similar manner at the initiation of lipolysis and arginine residues near the target serines may influence this process.
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spelling pubmed-35661322013-02-12 Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis McDonough, Patrick M. Maciejewski-Lenoir, Dominique Hartig, Sean M. Hanna, Rita A. Whittaker, Ross Heisel, Andrew Nicoll, James B. Buehrer, Benjamin M. Christensen, Kurt Mancini, Maureen G. Mancini, Michael A. Edwards, Dean P. Price, Jeffrey H. PLoS One Research Article Lipolysis in adipocytes is regulated by phosphorylation of lipid droplet-associated proteins, including perilipin 1A and hormone-sensitive lipase (HSL). Perilipin 1A is potentially phosphorylated by cAMP(adenosine 3′,5′-cyclic monophosphate)-dependent protein kinase (PKA) on several sites, including conserved C-terminal residues, serine 497 (PKA-site 5) and serine 522 (PKA-site 6). To characterize perilipin 1A phosphorylation, novel monoclonal antibodies were developed, which selectively recognize perilipin 1A phosphorylation at PKA-site 5 and PKA-site 6. Utilizing these novel antibodies, as well as antibodies selectively recognizing HSL phosphorylation at serine 563 or serine 660, we used high content analysis to examine the phosphorylation of perilipin 1A and HSL in adipocytes exposed to lipolytic agents. We found that perilipin PKA-site 5 and HSL-serine 660 were phosphorylated to a similar extent in response to forskolin (FSK) and L-γ-melanocyte stimulating hormone (L-γ-MSH). In contrast, perilipin PKA-site 6 and HSL-serine 563 were phosphorylated more slowly and L-γ-MSH was a stronger agonist for these sites compared to FSK. When a panel of lipolytic agents was tested, including multiple concentrations of isoproterenol, FSK, and L-γ-MSH, the pattern of results was virtually identical for perilipin PKA-site 5 and HSL-serine 660, whereas a distinct pattern was observed for perilipin PKA-site 6 and HSL-serine 563. Notably, perilipin PKA-site 5 and HSL-serine 660 feature two arginine residues upstream from the phospho-acceptor site, which confers high affinity for PKA, whereas perilipin PKA-site 6 and HSL-serine 563 feature only a single arginine. Thus, we suggest perilipin 1A and HSL are differentially phosphorylated in a similar manner at the initiation of lipolysis and arginine residues near the target serines may influence this process. Public Library of Science 2013-02-06 /pmc/articles/PMC3566132/ /pubmed/23405163 http://dx.doi.org/10.1371/journal.pone.0055511 Text en © 2013 McDonough 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
McDonough, Patrick M.
Maciejewski-Lenoir, Dominique
Hartig, Sean M.
Hanna, Rita A.
Whittaker, Ross
Heisel, Andrew
Nicoll, James B.
Buehrer, Benjamin M.
Christensen, Kurt
Mancini, Maureen G.
Mancini, Michael A.
Edwards, Dean P.
Price, Jeffrey H.
Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis
title Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis
title_full Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis
title_fullStr Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis
title_full_unstemmed Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis
title_short Differential Phosphorylation of Perilipin 1A at the Initiation of Lipolysis Revealed by Novel Monoclonal Antibodies and High Content Analysis
title_sort differential phosphorylation of perilipin 1a at the initiation of lipolysis revealed by novel monoclonal antibodies and high content analysis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3566132/
https://www.ncbi.nlm.nih.gov/pubmed/23405163
http://dx.doi.org/10.1371/journal.pone.0055511
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