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. 2025 Mar;28(3):470-486.
doi: 10.1038/s41593-025-01875-9. Epub 2025 Mar 3.

CLEC16A in astrocytes promotes mitophagy and limits pathology in a multiple sclerosis mouse model

Atsushi Kadowaki  1   2   3 Michael A Wheeler  1   4 Zhaorong Li  1 Brian M Andersen  1   5 Hong-Gyun Lee  1 Tomer Illouz  1 Joon-Hyuk Lee  1 Alain Ndayisaba  1 Stephanie E J Zandee  6 Himanish Basu  7 Chun-Cheih Chao  1 Joao V Mahler  1 Wendy Klement  6 Dylan Neel  7 Matthew Bergstresser  7 Veit Rothhammer  1 Gabriel Lipof  1 Lena Srun  1 Scott A Soleimanpour  8   9   10 Isaac Chiu  7 Alexandre Prat  6 Vikram Khurana  1   4   11 Francisco J Quintana  12   13
Affiliations

CLEC16A in astrocytes promotes mitophagy and limits pathology in a multiple sclerosis mouse model

Atsushi Kadowaki et al. Nat Neurosci. 2025 Mar.

Abstract

Astrocytes promote neuroinflammation and neurodegeneration in multiple sclerosis (MS) through cell-intrinsic activities and their ability to recruit and activate other cell types. In a genome-wide CRISPR-based forward genetic screen investigating regulators of astrocyte proinflammatory responses, we identified the C-type lectin domain-containing 16A gene (CLEC16A), linked to MS susceptibility, as a suppressor of nuclear factor-κB (NF-κB) signaling. Gene and small-molecule perturbation studies in mouse primary and human embryonic stem cell-derived astrocytes in combination with multiomic analyses established that CLEC16A promotes mitophagy, limiting mitochondrial dysfunction and the accumulation of mitochondrial products that activate NF-κB, the NLRP3 inflammasome and gasdermin D. Astrocyte-specific Clec16a inactivation increased NF-κB, NLRP3 and gasdermin D activation in vivo, worsening experimental autoimmune encephalomyelitis, a mouse model of MS. Moreover, we detected disrupted mitophagic capacity and gasdermin D activation in astrocytes in samples from individuals with MS. These findings identify CLEC16A as a suppressor of astrocyte pathological responses and a candidate therapeutic target in MS.

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Conflict of interest statement

Competing interests: The authors declare no competing interests.

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