| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2047437 | FEBS Letters | 2015 | 7 Pages |
Abstract
JNK/stress-activated protein kinase-associated protein 1 (JSAP1) and JNK-associated leucine zipper protein (JLP) are structurally related scaffolding proteins that are highly expressed in the brain. Here, we found that JSAP1 and JLP play functionally redundant and essential roles in mouse cerebellar Purkinje cell (PC) survival. Mice containing PCs with deletions in both JSAP1 and JLP exhibited PC axonal dystrophy, followed by gradual, progressive neuronal loss. Kinesin-1 cargoes accumulated selectively in the swollen axons of Jsap1/Jlp-deficient PCs. In addition, autophagy inactivation in these mice markedly accelerated PC degeneration. These findings suggest that JSAP1 and JLP play critical roles in kinesin-1-dependent axonal transport, which prevents brain neuronal degeneration.
Keywords
KLCCyt CcKOKHCc-Jun NH2-terminal kinaseSYPfloxedSynaptotagmin 1APPDAPIJLPHRPSyt1GFAPDCNJnkJIPAxonal swellingJNK-interacting protein4,6-diamidino-2-phenylindoleMAPKAutophagyImmunohistochemistryIHCNeurodegenerationKinesin light chainkinesin heavy chainPurkinje cellcytochrome cSynaptophysinphosphorylated phosphoknockoutdeep cerebellar nucleiHorseradish peroxidaseGlial fibrillary acidic proteinamyloid precursor proteinmitogen-activated protein kinaseKinesin-1Ubiquitin
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Authors
Tokiharu Sato, Momoe Ishikawa, Toru Yoshihara, Ryota Nakazato, Haruhiro Higashida, Masahide Asano, Katsuji Yoshioka,