AI Article Synopsis
- * Researchers found that early-life viral infections led to changes in the brain's immune environment, specifically the buildup of memory T cells that produce a signaling molecule called CCL5.
- * Blocking CCL5 signaling in mice prevented brain damage related to autoimmune diseases, suggesting that early viral infections could create long-lasting changes in the immune system, making it more prone to autoimmune reactions.
Article Abstract
Epidemiological studies associate viral infections during childhood with the risk of developing autoimmune disease during adulthood. However, the mechanistic link between these events remains elusive. We report that transient viral infection of the brain in early life, but not at a later age, precipitates brain autoimmune disease elicited by adoptive transfer of myelin-specific CD4 T cells at sites of previous infection in adult mice. Early-life infection of mouse brains imprinted a chronic inflammatory signature that consisted of brain-resident memory T cells expressing the chemokine (C-C motif) ligand 5 (CCL5). Blockade of CCL5 signaling via C-C chemokine receptor type 5 prevented the formation of brain lesions in a mouse model of autoimmune disease. In mouse and human brain, CCL5 T were located predominantly to sites of microglial activation. This study uncovers how transient brain viral infections in a critical window in life might leave persisting chemotactic cues and create a long-lived permissive environment for autoimmunity.
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| http://dx.doi.org/10.1126/scitranslmed.aav5519 | DOI Listing |
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