Neuropathy-associated Tecpr2 mutation knock-in mice reveal endolysosomal loss of function phenotypes in neurons and microglia.

Bhattacharya, Debjani; Behrends, Christian; Werner, Georg; Wurst, Wolfgang; Wefers, Benedikt; Nalbach, Karsten; da Silva-Buttkus, Patricia; Lengger, Christoph; Rodde, Ramona; Garrett, Lillian; Brill, Monika S; Schifferer, Martina; Fuchs, Helmut; Cheng, Lizhen; Hölter, Sabine M; Lichtenthaler, Stefan F; Gailus-Durner, Valerie; Kislinger, Georg; Zimprich, Annemarie; Hrabe de Angelis, Martin; Beckers, Johannes; Irmler, Martin

doi:10.1038/s41419-025-08168-w

TY  - JOUR
AU  - Bhattacharya, Debjani
AU  - da Silva-Buttkus, Patricia
AU  - Nalbach, Karsten
AU  - Cheng, Lizhen
AU  - Garrett, Lillian
AU  - Irmler, Martin
AU  - Kislinger, Georg
AU  - Werner, Georg
AU  - Rodde, Ramona
AU  - Lengger, Christoph
AU  - Beckers, Johannes
AU  - Zimprich, Annemarie
AU  - Hölter, Sabine M
AU  - Gailus-Durner, Valerie
AU  - Fuchs, Helmut
AU  - Hrabe de Angelis, Martin
AU  - Wefers, Benedikt
AU  - Wurst, Wolfgang
AU  - Brill, Monika S
AU  - Schifferer, Martina
AU  - Lichtenthaler, Stefan F
AU  - Behrends, Christian
TI  - Neuropathy-associated Tecpr2 mutation knock-in mice reveal endolysosomal loss of function phenotypes in neurons and microglia.
JO  - Cell death & disease
VL  - 16
IS  - 1
SN  - 2041-4889
CY  - London [u.a.]
PB  - Nature Publishing Group
M1  - DZNE-2025-01222
SP  - 775
PY  - 2025
AB  - Mutations in the gene encoding Tectonic β-propeller repeat-containing repeat protein 2 (TECPR2) cause hereditary sensory and autonomic neuropathy subtype 9 (HSAN9) which is a fatal neurodevelopmental and neurodegenerative disorder involving the sensory and peripheral nervous system. TECPR2 is ubiquitously expressed and linked to trafficking and sorting within the cell, however, its functional role remains poorly defined. Moreover, molecular insights into pathogenic mechanisms underlying HSAN9 are lacking. Here, we report a novel mouse model which harbors a HSAN9-associated nonsense mutation that causes loss of TECPR2 expression. Mice show altered gait, highly region-specific axonal dystrophy, and extensive local gliosis. The affected medulla area prominently features swollen axons filled with amorphous protein aggregates, glycogen granules, single and double membrane vesicles as well as aberrant organelles including ER and mitochondria whose proteome is distinctly altered. Despite the locally restricted pathology the neuronal demise is detectable in the cerebrospinal fluid and responded to by damage-associated microglia. However, their capacity to clear neuronal debris seems attenuated. Overall, neuronal and microglia phenotypes point to a dysfunctional endolysosomal system when TECPR2 is missing. This was confirmed in TECPR2 knockout cells and linked to TECPR2's interaction with the homotypic fusion and protein sorting (HOPS)-tethering complex. Collectively, we uncovered a role of TECPR2 in endolysosome maintenance which seems relevant for healthy neurons in a particular brain region.
KW  - Animals
KW  - Microglia: metabolism
KW  - Microglia: pathology
KW  - Neurons: metabolism
KW  - Neurons: pathology
KW  - Mice
KW  - Phenotype
KW  - Lysosomes: metabolism
KW  - Gene Knock-In Techniques
KW  - Endosomes: metabolism
KW  - Nerve Tissue Proteins: genetics
KW  - Nerve Tissue Proteins: metabolism
KW  - Disease Models, Animal
KW  - Mutation: genetics
KW  - Nerve Tissue Proteins (NLM Chemicals)
LB  - PUB:(DE-HGF)16
C6  - pmid:41173829
C2  - pmc:PMC12578842
DO  - DOI:10.1038/s41419-025-08168-w
UR  - https://pub.dzne.de/record/281843
ER  -

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