Cranial irradiation leads to acute and persistent neuroinflammation with delayed increases in T-cell infiltration and CD11c expression in C57BL/6 mouse brain

MJ Moravan, JA Olschowka, JP Williams… - Radiation …, 2011 - meridian.allenpress.com
MJ Moravan, JA Olschowka, JP Williams, MK O'Banion
Radiation research, 2011meridian.allenpress.com
Radiotherapy is commonly employed to treat cancers of the head and neck and is
increasingly used to treat other central nervous system (CNS) disorders. Exceeding the
radiation tolerance of normal CNS tissues can result in sequelae contributing to patient
morbidity and mortality. Animal studies and clinical experience suggest that
neuroinflammation plays a role in the etiology of these effects; however, detailed
characterization of this response has been lacking. Therefore, a dose–time investigation of …
Radiotherapy is commonly employed to treat cancers of the head and neck and is increasingly used to treat other central nervous system (CNS) disorders. Exceeding the radiation tolerance of normal CNS tissues can result in sequelae contributing to patient morbidity and mortality. Animal studies and clinical experience suggest that neuroinflammation plays a role in the etiology of these effects; however, detailed characterization of this response has been lacking. Therefore, a dose–time investigation of the neuroinflammatory response after single-dose cranial irradiation was performed using C57BL/6 mice. Consistent with previous reports, cranial irradiation resulted in multiphasic inflammatory changes exemplified by increased transcript levels of inflammatory cytokines, along with glial and endothelial cell activation. Cranial irradiation also resulted in acute infiltration of neutrophils and a delayed increase in T cells, MHC II-positive cells, and CD11c-positive cells seen first at 1 month with doses ≥15 Gy. CD11c-positive cells were found almost exclusively in white matter and expressed MHC II, suggesting a “mature” dendritic cell phenotype that remained elevated out to 1 year postirradiation. Our results indicate that cranial irradiation leads to persistent neuroinflammatory changes in the C57BL/6 mouse brain that includes unique immunomodulatory cell populations.
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