Home > Publications database > Disruption of ClC-3-mediated 2Cl−/H+ exchange leads to behavioural deficits and thalamic atrophy
 
Journal Article FZJ-2025-04252
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Disruption of ClC-3-mediated 2Cl−/H+ exchange leads to behavioural deficits and thalamic atrophy

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2025
Springer Nature [London]

Scientific reports 15(1), 33326 () [10.1038/s41598-025-19757-2]

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Abstract: CLCN3 encodes ClC-3, an endosomal 2Cl⁻/H⁺ exchanger, with pathogenic variants causing aneurodevelopmental condition marked by developmental delays, intellectual disability, seizures,hyperactivity, anxiety, and brain and retinal abnormalities. Clcn3−/− mice show hippocampal and retinaldegeneration, recapitulating key symptoms observed in humans. ClC-3 forms homodimers (ClC-3/ClC-3) and heterodimers with ClC-4 (ClC-3/ClC-4), with overlapping brain expression. This suggestsdistinct functional roles for homo- and heterodimeric assemblies and raises the question of which brainregions specifically depend on ClC-3/ClC-3 rather than ClC-3/ClC-4 complexes. Using ex vivo PET traceranalyses, Clcn3−/− and Clcn3td/td mice, we found neurodegeneration in the hippocampus and thalamusof Clcn3−/−, while Clcn3td/td mice showed thalamic degeneration and altered neuronal excitability,including changes in action potential threshold and after hyperpolarization. Clcn3td/td mice carryinga transport-deficient p.E281Q ClC-3 variant that still associates with ClC-4, thereby allowing ClC-4 tobe sorted to endosomes as ClC-4/ClC-3 heterodimers, unlike in the Clcn3−/− model. Clcn3td/td mice alsoexhibited reduced weight, hyperactivity, and motor deficits, reflecting clinical features. Lower ClC-4levels in thalamus predict a predominant thalamic expression of ClC-3/ClC-3 homodimers. Overall,our findings indicate a region-specific function of ClC-3/ClC-3 homodimeric complexes and highlightthe importance of ClC-3 transport activity in thalamic neuron survival, with electrophysiologicaldysfunction likely contributing to neurodegeneration.

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Note: Open Access funding enabled and organized by Projekt DEAL.
Contributing Institute(s):
  1. Molekular- und Zellphysiologie (IBI-1)
  2. Projektträger Energie, Technologie, Nachhaltigkeit (ETN)
  3. Jara-Institut Brain structure-function relationships (INM-10)
  4. Physik der Medizinischen Bildgebung (INM-4)
  5. Strukturbiochemie (IBI-7)
  6. Nuklearchemie (INM-5)
Research Program(s):
  1. 5241 - Molecular Information Processing in Cellular Systems (POF4-524) (POF4-524)
  2. 5253 - Neuroimaging (POF4-525) (POF4-525)

Appears in the scientific report 2025
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Document types > Articles > Journal Article
Institute Collections > INM > INM-10
Institute Collections > IBI > IBI-7
Institute Collections > IBI > IBI-1
Institute Collections > INM > INM-4
Institute Collections > INM > INM-5
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 Record created 2025-10-23, last modified 2025-10-30
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