AI Article Synopsis
- Multiple sclerosis (MS) is an autoimmune disease affecting the central nervous system (CNS), characterized by inflammation that leads to damage of neurons and loss of myelin.
- Recent findings indicate that granzyme B (GrB), a serine protease from cytotoxic T cells, selectively causes neuronal death and contributes to disability progression in MS.
- The study reveals that GrB enters neurons, accumulates in the cell body, activates cell death pathways, and highlights the potential of mannose-6-phosphate in preventing GrB-induced neurotoxicity, opening doors for new treatment approaches.
Article Abstract
Multiple sclerosis (MS) is considered an autoimmune disease of the CNS and is characterized by inflammatory cells infiltrating the CNS and inducing demyelination, axonal loss, and neuronal death. Recent evidence strongly suggests that axonal and neuronal degeneration underlie the progression of permanent disability in MS. In this study, we report that human neurons are selectively susceptible to the serine-protease granzyme B (GrB) isolated from cytotoxic T cell granules. In vitro, purified human GrB induced neuronal death to the same extent as the whole activated T cell population. On the contrary, activated T cells isolated from GrB knockout mice failed to induce neuronal injury. We found that following internalization through various parts of neurons, GrB accumulated in the neuronal soma. Within the cell body, GrB diffused out of endosomes possibly through a perforin-independent mechanism and induced subsequent activation of caspases and cleavage of α-tubulin. Inhibition of caspase-3, a well-known substrate for GrB, significantly reduced GrB-mediated neurotoxicity. We demonstrated that treatment of neurons with mannose-6-phosphate prevented GrB entry and inhibited GrB-mediated neuronal death, suggesting mannose-6-phosphate receptor-dependent endocytosis. Together, our data unveil a novel mechanism by which GrB induces selective neuronal injury and suggest potential new targets for the treatment of inflammatory-mediated neurodegeneration in diseases such as MS.
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| http://dx.doi.org/10.4049/jimmunol.1100943 | DOI Listing |
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