Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system

C-type allatostatins (AST-Cs) are pleiotropic neuropeptides that are broadly conserved within arthropods; the presence of three AST-C isoforms, encoded by paralog genes, is common. However, these peptides are hypothesized to act through a single receptor, thereby exerting similar bioactivities withi...

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Autores principales: Dickinson, Patsy S., Armstrong, Matthew K., Dickinson, Evyn S., Fernandez, Rebecca, Miller, Alexandra, Pong, Sovannarath, Powers, Brian W., Pupo-Wiss, Alixander, Stanhope, Meredith E., Walsh, Patrick J., Wiwatpanit, Teerawat, Christie, Andrew E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Physiological Society 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6008092/
https://www.ncbi.nlm.nih.gov/pubmed/29384453
http://dx.doi.org/10.1152/jn.00850.2017
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author Dickinson, Patsy S.
Armstrong, Matthew K.
Dickinson, Evyn S.
Fernandez, Rebecca
Miller, Alexandra
Pong, Sovannarath
Powers, Brian W.
Pupo-Wiss, Alixander
Stanhope, Meredith E.
Walsh, Patrick J.
Wiwatpanit, Teerawat
Christie, Andrew E.
author_facet Dickinson, Patsy S.
Armstrong, Matthew K.
Dickinson, Evyn S.
Fernandez, Rebecca
Miller, Alexandra
Pong, Sovannarath
Powers, Brian W.
Pupo-Wiss, Alixander
Stanhope, Meredith E.
Walsh, Patrick J.
Wiwatpanit, Teerawat
Christie, Andrew E.
author_sort Dickinson, Patsy S.
collection PubMed
description C-type allatostatins (AST-Cs) are pleiotropic neuropeptides that are broadly conserved within arthropods; the presence of three AST-C isoforms, encoded by paralog genes, is common. However, these peptides are hypothesized to act through a single receptor, thereby exerting similar bioactivities within each species. We investigated this hypothesis in the American lobster, Homarus americanus, mapping the distributions of AST-C isoforms within relevant regions of the nervous system and digestive tract, and comparing their modulatory influences on the cardiac neuromuscular system. Immunohistochemistry showed that in the pericardial organ, a neuroendocrine release site, AST-C I and/or III and AST-C II are contained within distinct populations of release terminals. Moreover, AST-C I/III-like immunoreactivity was seen in midgut epithelial endocrine cells and the cardiac ganglion (CG), whereas AST-C II-like immunoreactivity was not seen in these tissues. These data suggest that AST-C I and/or III can modulate the CG both locally and hormonally; AST-C II likely acts on the CG solely as a hormonal modulator. Physiological studies demonstrated that all three AST-C isoforms can exert differential effects, including both increases and decreases, on contraction amplitude and frequency when perfused through the heart. However, in contrast to many state-dependent modulatory changes, the changes in contraction amplitude and frequency elicited by the AST-Cs were not functions of the baseline parameters. The responses to AST-C I and III, neither of which is COOH-terminally amidated, are more similar to one another than they are to the responses elicited by AST-C II, which is COOH-terminally amidated. These results suggest that the three AST-C isoforms are differentially distributed in the lobster nervous system/midgut and can elicit distinct behaviors from the cardiac neuromuscular system, with particular structural features, e.g., COOH-terminal amidation, likely important in determining the effects of the peptides. NEW & NOTEWORTHY Multiple isoforms of many peptides exert similar effects on neural circuits. In this study we show that each of the three isoforms of C-type allatostatin (AST-C) can exert differential effects, including both increases and decreases in contraction amplitude and frequency, on the lobster cardiac neuromuscular system. The distribution of effects elicited by the nonamidated isoforms AST-C I and III are more similar to one another than to the effects of the amidated AST-C II.
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spelling pubmed-60080922018-06-21 Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system Dickinson, Patsy S. Armstrong, Matthew K. Dickinson, Evyn S. Fernandez, Rebecca Miller, Alexandra Pong, Sovannarath Powers, Brian W. Pupo-Wiss, Alixander Stanhope, Meredith E. Walsh, Patrick J. Wiwatpanit, Teerawat Christie, Andrew E. J Neurophysiol Research Article C-type allatostatins (AST-Cs) are pleiotropic neuropeptides that are broadly conserved within arthropods; the presence of three AST-C isoforms, encoded by paralog genes, is common. However, these peptides are hypothesized to act through a single receptor, thereby exerting similar bioactivities within each species. We investigated this hypothesis in the American lobster, Homarus americanus, mapping the distributions of AST-C isoforms within relevant regions of the nervous system and digestive tract, and comparing their modulatory influences on the cardiac neuromuscular system. Immunohistochemistry showed that in the pericardial organ, a neuroendocrine release site, AST-C I and/or III and AST-C II are contained within distinct populations of release terminals. Moreover, AST-C I/III-like immunoreactivity was seen in midgut epithelial endocrine cells and the cardiac ganglion (CG), whereas AST-C II-like immunoreactivity was not seen in these tissues. These data suggest that AST-C I and/or III can modulate the CG both locally and hormonally; AST-C II likely acts on the CG solely as a hormonal modulator. Physiological studies demonstrated that all three AST-C isoforms can exert differential effects, including both increases and decreases, on contraction amplitude and frequency when perfused through the heart. However, in contrast to many state-dependent modulatory changes, the changes in contraction amplitude and frequency elicited by the AST-Cs were not functions of the baseline parameters. The responses to AST-C I and III, neither of which is COOH-terminally amidated, are more similar to one another than they are to the responses elicited by AST-C II, which is COOH-terminally amidated. These results suggest that the three AST-C isoforms are differentially distributed in the lobster nervous system/midgut and can elicit distinct behaviors from the cardiac neuromuscular system, with particular structural features, e.g., COOH-terminal amidation, likely important in determining the effects of the peptides. NEW & NOTEWORTHY Multiple isoforms of many peptides exert similar effects on neural circuits. In this study we show that each of the three isoforms of C-type allatostatin (AST-C) can exert differential effects, including both increases and decreases in contraction amplitude and frequency, on the lobster cardiac neuromuscular system. The distribution of effects elicited by the nonamidated isoforms AST-C I and III are more similar to one another than to the effects of the amidated AST-C II. American Physiological Society 2018-05-01 2018-01-31 /pmc/articles/PMC6008092/ /pubmed/29384453 http://dx.doi.org/10.1152/jn.00850.2017 Text en Copyright © 2018 the American Physiological Society http://creativecommons.org/licenses/by/4.0/deed.en_US Licensed under Creative Commons Attribution CC-BY 4.0 (http://creativecommons.org/licenses/by/4.0/deed.en_US) : © the American Physiological Society.
spellingShingle Research Article
Dickinson, Patsy S.
Armstrong, Matthew K.
Dickinson, Evyn S.
Fernandez, Rebecca
Miller, Alexandra
Pong, Sovannarath
Powers, Brian W.
Pupo-Wiss, Alixander
Stanhope, Meredith E.
Walsh, Patrick J.
Wiwatpanit, Teerawat
Christie, Andrew E.
Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
title Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
title_full Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
title_fullStr Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
title_full_unstemmed Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
title_short Three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
title_sort three members of a peptide family are differentially distributed and elicit differential state-dependent responses in a pattern generator-effector system
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6008092/
https://www.ncbi.nlm.nih.gov/pubmed/29384453
http://dx.doi.org/10.1152/jn.00850.2017
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