Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation

Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation

A family of endogenous lipids, structurally analogous to the endogenous cannabinoid, N-arachidonoyl ethanolamine (Anandamide), and called N-acyl amides have emerged as a family of biologically active compounds at TRP receptors. N-acyl amides are constructed from an acyl group and an amine via an ami...

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Main Authors: Siham eRaboune, Jordyn M Stuart, Emma eLeishman, Sara M Takacs, Brandon eRhodes, Arjun eBasnet, Evan eJameyfield, Douglas eMcHugh, Theodore eWidlanski, Heather Bryte Bradshaw
Format: Article
Language:English
Published: Frontiers Media S.A. 2014-08-01
Series:Frontiers in Cellular Neuroscience
Subjects:
Endocannabinoids
Microglia
lipid signaling
N-acyl amides
TRP receptors
Online Access:http://journal.frontiersin.org/Journal/10.3389/fncel.2014.00195/full
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spelling doaj-59b4fb14171f4c08910612f7cfd52ef32020-11-24T22:54:28ZengFrontiers Media S.A.Frontiers in Cellular Neuroscience1662-51022014-08-01810.3389/fncel.2014.0019592532Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammationSiham eRaboune0Jordyn M Stuart1Emma eLeishman2Sara M Takacs3Brandon eRhodes4Arjun eBasnet5Evan eJameyfield6Douglas eMcHugh7Douglas eMcHugh8Theodore eWidlanski9Heather Bryte Bradshaw10Indiana UniversityIndiana UniversityIndiana UniversityIndiana UniversityIndiana UniversityIndiana UniversityIndiana UniversityIndiana UniversityQuinnipiac UniversityIndiana UniversityIndiana UniversityA family of endogenous lipids, structurally analogous to the endogenous cannabinoid, N-arachidonoyl ethanolamine (Anandamide), and called N-acyl amides have emerged as a family of biologically active compounds at TRP receptors. N-acyl amides are constructed from an acyl group and an amine via an amide bond. This same structure can be modified by changing either the fatty acid or the amide to form potentially hundreds of lipids. More than 70 N-acyl amides have been identified in nature. We have ongoing studies aimed at isolating and characterizing additional members of the family of N-acyl amides in both central and peripheral tissues in mammalian systems. Here, using a unique in-house library of over 70 N-acyl amides we tested the following three hypotheses: 1) Additional N-acyl amides will have activity at TRPV1-4, 2) Acute peripheral injury will drive changes in CNS levels of N-acyl amides, and 3) N-acyl amides will regulate calcium in CNS-derived microglia. Through these studies, we have identified 20 novel N-acyl amides that collectively activate (stimulating or inhibiting) TRPV1-4. Using lipid extraction and HPLC coupled to tandem mass spectrometry we showed that levels of at least 10 of these N-acyl amides that activate TRPVs are regulated in brain after intraplantar carrageenan injection. We then screened the BV2 microglial cell line for activity with this N-acyl amide library and found overlap with TRPV receptor activity as well as additional activators of calcium mobilization from these lipids. Together these data provide new insight into the family of N-acyl amides and their roles as signaling molecules at ion channels, in microglia, and in the brain in the context of inflammation.http://journal.frontiersin.org/Journal/10.3389/fncel.2014.00195/fullEndocannabinoidsMicroglialipid signalingN-acyl amidesTRP receptors
collection DOAJ
language English
format Article
sources DOAJ
author Siham eRaboune
Jordyn M Stuart
Emma eLeishman
Sara M Takacs
Brandon eRhodes
Arjun eBasnet
Evan eJameyfield
Douglas eMcHugh
Douglas eMcHugh
Theodore eWidlanski
Heather Bryte Bradshaw
spellingShingle Siham eRaboune
Jordyn M Stuart
Emma eLeishman
Sara M Takacs
Brandon eRhodes
Arjun eBasnet
Evan eJameyfield
Douglas eMcHugh
Douglas eMcHugh
Theodore eWidlanski
Heather Bryte Bradshaw
Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation
Frontiers in Cellular Neuroscience
Endocannabinoids
Microglia
lipid signaling
N-acyl amides
TRP receptors
author_facet Siham eRaboune
Jordyn M Stuart
Emma eLeishman
Sara M Takacs
Brandon eRhodes
Arjun eBasnet
Evan eJameyfield
Douglas eMcHugh
Douglas eMcHugh
Theodore eWidlanski
Heather Bryte Bradshaw
author_sort Siham eRaboune
title Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation
title_short Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation
title_full Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation
title_fullStr Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation
title_full_unstemmed Novel endogenous N-acyl amides activate TRPV1-4 receptors, BV-2 microglia, and are regulated in brain in an acute model of inflammation
title_sort novel endogenous n-acyl amides activate trpv1-4 receptors, bv-2 microglia, and are regulated in brain in an acute model of inflammation
publisher Frontiers Media S.A.
series Frontiers in Cellular Neuroscience
issn 1662-5102
publishDate 2014-08-01
description A family of endogenous lipids, structurally analogous to the endogenous cannabinoid, N-arachidonoyl ethanolamine (Anandamide), and called N-acyl amides have emerged as a family of biologically active compounds at TRP receptors. N-acyl amides are constructed from an acyl group and an amine via an amide bond. This same structure can be modified by changing either the fatty acid or the amide to form potentially hundreds of lipids. More than 70 N-acyl amides have been identified in nature. We have ongoing studies aimed at isolating and characterizing additional members of the family of N-acyl amides in both central and peripheral tissues in mammalian systems. Here, using a unique in-house library of over 70 N-acyl amides we tested the following three hypotheses: 1) Additional N-acyl amides will have activity at TRPV1-4, 2) Acute peripheral injury will drive changes in CNS levels of N-acyl amides, and 3) N-acyl amides will regulate calcium in CNS-derived microglia. Through these studies, we have identified 20 novel N-acyl amides that collectively activate (stimulating or inhibiting) TRPV1-4. Using lipid extraction and HPLC coupled to tandem mass spectrometry we showed that levels of at least 10 of these N-acyl amides that activate TRPVs are regulated in brain after intraplantar carrageenan injection. We then screened the BV2 microglial cell line for activity with this N-acyl amide library and found overlap with TRPV receptor activity as well as additional activators of calcium mobilization from these lipids. Together these data provide new insight into the family of N-acyl amides and their roles as signaling molecules at ion channels, in microglia, and in the brain in the context of inflammation.
topic Endocannabinoids
Microglia
lipid signaling
N-acyl amides
TRP receptors
url http://journal.frontiersin.org/Journal/10.3389/fncel.2014.00195/full
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