MicroRNA-132 Potentiates Cholinergic Anti-Inflammatory Signaling by Targeting Acetylcholinesterase

MicroRNAs (miRNAs) contribute to both neuronal and immune cell fate, but their involvement in intertissue communication remained unexplored. The brain, via vagal secretion of acetylcholine (ACh), suppresses peripheral inflammation by intercepting cytokine production; therefore, we predicted that mic...

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Bibliographic Details
Published in:Immunity (Cambridge, Mass.) Mass.), 2009-12, Vol.31 (6), p.965-973
Main Authors: Shaked, Iftach, Meerson, Ari, Wolf, Yochai, Avni, Ran, Greenberg, David, Gilboa-Geffen, Adi, Soreq, Hermona
Format: Article
Language:English
Subjects:
Acetylcholine - metabolism
Acetylcholinesterase - genetics
Animals
Base Sequence
Binding sites
Bone marrow
Bone Marrow Cells - drug effects
Bone Marrow Cells - immunology
Cell Line
Cytokines
Down-Regulation
Female
Gene expression
Humans
Inflammation - enzymology
Inflammation - immunology
Intestine, Small - drug effects
Intestine, Small - immunology
Kinases
Lentivirus
Ligands
Lipopolysaccharides - immunology
Macrophages - drug effects
Macrophages - immunology
Mice
Mice, Transgenic
MicroRNAs
MicroRNAs - agonists
MicroRNAs - genetics
MicroRNAs - metabolism
Molecular Sequence Data
MOLIMMUNO
Oligonucleotides - pharmacology
Rodents
Sequence Deletion
Signal Transduction
Up-Regulation
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Summary:MicroRNAs (miRNAs) contribute to both neuronal and immune cell fate, but their involvement in intertissue communication remained unexplored. The brain, via vagal secretion of acetylcholine (ACh), suppresses peripheral inflammation by intercepting cytokine production; therefore, we predicted that microRNAs targeting acetylcholinesterase (AChE) can attenuate inflammation. Here, we report that inflammatory stimuli induced leukocyte overexpression of the AChE-targeting miR-132. Injected locked nucleic acid (LNA)-modified anti-miR-132 oligonucleotide depleted miR-132 amounts while elevating AChE in mouse circulation and tissues. In transfected cells, a mutated 3′UTR miR-132 binding site increased AChE mRNA expression, whereas cells infected with a lentivirus expressing pre-miR-132 showed suppressed AChE. Transgenic mice overexpressing 3′UTR null AChE showed excessive inflammatory mediators and impaired cholinergic anti-inflammatory regulation, in spite of substantial miR-132 upregulation in brain and bone marrow. Our findings identify the AChE mRNA-targeting miR-132 as a functional regulator of the brain-to-body resolution of inflammation, opening avenues for study and therapeutic manipulations of the neuro-immune dialog.
ISSN:1074-7613
1097-4180
DOI:10.1016/j.immuni.2009.09.019