Characterization of exosome-mediated propagation of systemic inflammatory responses into the Central Nervous System
Mahesh Chandra Kodali, Chinnu Salim, Saifudeen Ismael, Sarah Grace Lebovitz, Geng Lin, Francesca-fang Liao

TL;DR
This study shows how exosomes from the blood can spread inflammation to the brain during systemic inflammation.
Contribution
The study demonstrates a novel role of circulating exosomes in propagating systemic inflammation to the central nervous system.
Findings
Serum-derived exosomes from LPS-treated mice upregulate pro-inflammatory cytokine genes in brain-related cell lines.
Intravenous injection of these exosomes in mice leads to increased cytokine mRNA in the brain.
Proteomic analysis confirms elevated inflammatory cytokines in the exosomes.
Abstract
The mechanisms through which systemic inflammation exerts its effect on the CNS are still not completely understood. Exosomes are small (30 to 100 nanometers) membrane-bound extracellular vesicles released by most of the mammalian cells. Exosomes play a vital role in cell-to-cell communication. This includes regulation of inflammatory responses by shuttling mRNAs, miRNAs, and cytokines both locally and systemically to the neighboring as well as distant cells to further modulate their transcriptional and/or translational states and affect the functional phenotype of those cells that have taken up these exosomes. The role of circulating blood exosomes leading to neuroinflammation during systemic inflammatory conditions was further characterized. Serum-derived exosomes from LPS-challenged mice (SDEL) were freshly isolated from the sera of the mice that were earlier treated with LPS and…
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Taxonomy
TopicsCriminal Justice and Penology · European Criminal Justice and Data Protection · Comparative constitutional jurisprudence studies
