TY - JOUR
T1 - Glial loss of the metallo β-lactamase domain containing protein, SWIP-10, induces age- and glutamate-signaling dependent, dopamine neuron degeneration
AU - Gibson, Chelsea L.
AU - Balbona, Joseph T.
AU - Niedzwiecki, Ashlin
AU - Rodriguez, Peter
AU - Nguyen, Ken C.Q.
AU - Hall, David H.
AU - Blakely, Randy D.
N1 - Funding Information:
Strainsweremaintainedasdescribedpreviously[142].WethankJ.Rand(OklahomaMedical Research Foundation); the Caenhorha bditis Genetics Center; Shohei Mitani of the National BioresourceProjectatTokyoWomen’sMedicalUniversity;andShaiShaham,NielsRingstad, andOliverHobertforprovidingthestrainsusedinthiswork.N2(Bristol)servedasourwild-typestrain,andunlessspecifiedotherwise,weutilizedtheproposednullallele,TM5915,of swip-10[44]. Strains used inthis study are enumerated per figure appearance in S1 Table.
Funding Information:
We acknowledge that the majority of this work was generously supported the National Institute of Health via the National Institute of Mental Health (https://www.nimh.nih.gov/index.shtmlaward)MH095044 (RDB). Electron microscopy work was supported by the Intellectual and Developmental Disabilities Research Center (Einstein) (https://www.einstein.yu.edu/centers/childrens-evaluation-rehabilitation/research/IDDRC-research.aspx) award 5P030HD071593 to S.U. Walkley. Additional financial support was also generously provided by the Office of the Director, National Institute of Health (https://www.nih.gov/institutes-nih/nih-office-director), award OD010943 (DHH). The funders had no role in study design, data collection and analysis, decision to publish or preparation of the manuscript. We wish to acknowledge J. Andrew Hardaway for his intellectual input and mentorship during the early stages of the project and the outstanding laboratory support provided by Sarah Sturgeon, Christina Svitek, Qiao Hann, Tracy Moore-Jarrett, Angela Steele, Matthew Gross, and Peter Rodriquez. Fig 2G was drawn by Chris Crocker. CLG acknowledges the support of the Vanderbilt University Graduate Neuroscience Program, JTB acknowledges the support of the Vanderbilt University Undergraduate Neuroscience Research program, and JTB and AN acknowledge the support of the Vanderbilt University Summer for Undergraduate Research Program. Work was completed with the assistance of the Vanderbilt Cell Imaging Shared Resource and the FAU Brain Institute Cell Imaging Core.
Publisher Copyright:
© 2018 Gibson et al.
PY - 2018/3
Y1 - 2018/3
N2 - Across phylogeny, glutamate (Glu) signaling plays a critical role in regulating neural excitability, thus supporting many complex behaviors. Perturbed synaptic and extrasynaptic Glu homeostasis in the human brain has been implicated in multiple neuropsychiatric and neurodegenerative disorders including Parkinson’s disease, where theories suggest that excitotoxic insults may accelerate a naturally occurring process of dopamine (DA) neuron degeneration. In C. elegans, mutation of the glial expressed gene, swip-10, results in Glu-dependent DA neuron hyperexcitation that leads to elevated DA release, triggering DA signaling-dependent motor paralysis. Here, we demonstrate that swip-10 mutations induce premature and progressive DA neuron degeneration, with light and electron microscopy studies demonstrating the presence of dystrophic dendritic processes, as well as shrunken and/or missing cell soma. As with paralysis, DA neuron degeneration in swip-10 mutants is rescued by glial-specific, but not DA neuron-specific expression of wildtype swip-10, consistent with a cell non-autonomous mechanism. Genetic studies implicate the vesicular Glu transporter VGLU-3 and the cystine/Glu exchanger homolog AAT-1 as potential sources of Glu signaling supporting DA neuron degeneration. Degeneration can be significantly suppressed by mutations in the Ca2+permeable Glu receptors, nmr-2 and glr-1, in genes that support intracellular Ca2+signaling and Ca2+-dependent proteolysis, as well as genes involved in apoptotic cell death. Our studies suggest that Glu stimulation of nematode DA neurons in early larval stages, without the protective actions of SWIP-10, contributes to insults that ultimately drive DA neuron degeneration. The swip-10 model may provide an efficient platform for the identification of molecular mechanisms that enhance risk for Parkinson’s disease and/or the identification of agents that can limit neurodegenerative disease progression.
AB - Across phylogeny, glutamate (Glu) signaling plays a critical role in regulating neural excitability, thus supporting many complex behaviors. Perturbed synaptic and extrasynaptic Glu homeostasis in the human brain has been implicated in multiple neuropsychiatric and neurodegenerative disorders including Parkinson’s disease, where theories suggest that excitotoxic insults may accelerate a naturally occurring process of dopamine (DA) neuron degeneration. In C. elegans, mutation of the glial expressed gene, swip-10, results in Glu-dependent DA neuron hyperexcitation that leads to elevated DA release, triggering DA signaling-dependent motor paralysis. Here, we demonstrate that swip-10 mutations induce premature and progressive DA neuron degeneration, with light and electron microscopy studies demonstrating the presence of dystrophic dendritic processes, as well as shrunken and/or missing cell soma. As with paralysis, DA neuron degeneration in swip-10 mutants is rescued by glial-specific, but not DA neuron-specific expression of wildtype swip-10, consistent with a cell non-autonomous mechanism. Genetic studies implicate the vesicular Glu transporter VGLU-3 and the cystine/Glu exchanger homolog AAT-1 as potential sources of Glu signaling supporting DA neuron degeneration. Degeneration can be significantly suppressed by mutations in the Ca2+permeable Glu receptors, nmr-2 and glr-1, in genes that support intracellular Ca2+signaling and Ca2+-dependent proteolysis, as well as genes involved in apoptotic cell death. Our studies suggest that Glu stimulation of nematode DA neurons in early larval stages, without the protective actions of SWIP-10, contributes to insults that ultimately drive DA neuron degeneration. The swip-10 model may provide an efficient platform for the identification of molecular mechanisms that enhance risk for Parkinson’s disease and/or the identification of agents that can limit neurodegenerative disease progression.
UR - http://www.scopus.com/inward/record.url?scp=85044827250&partnerID=8YFLogxK
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U2 - 10.1371/journal.pgen.1007269
DO - 10.1371/journal.pgen.1007269
M3 - Article
C2 - 29590100
AN - SCOPUS:85044827250
SN - 1553-7390
VL - 14
JO - PLoS genetics
JF - PLoS genetics
IS - 3
M1 - e1007269
ER -
