Transcriptomic evidence of a para-inflammatory state in the middle aged lumbar spinal cord.

Immun Ageing

Department of Anesthesiology, School of Medicine, Health Sciences Center L4, Stony Brook University, Stony Brook, New York, 11794-8480 USA.

Published: April 2017

Background: We have previously reported elevated expression of multiple pro-inflammatory markers in the lumbar spinal cord (LSC) of middle-aged male rats compared to young adults suggesting a para-inflammatory state develops in the LSC by middle age, a time that in humans is associated with the greatest pain prevalence and persistence. The goal of the current study was to examine the transcriptome-wide gene expression differences between young and middle aged LSC.

Methods: Young (3 month) and middle-aged (17 month) naïve Fisher 344 rats ( = 5 per group) were euthanized, perfused with heparinized saline, and the LSC were removed.

Results: ~70% of 31,000 coding sequences were detected. After normalization, ~ 1100 showed statistically significant differential expression. Of these genes, 353 middle-aged annotated genes differed by > 1.5 fold compared to the young group. Nearly 10% of these genes belonged to the microglial sensome. Analysis of this subset revealed that the principal age-related differential pathways populated are complement, pattern recognition receptors, OX40, and various T cell regulatory pathways consistent with microglial priming and T cell invasion and modulation. Many of these pathways substantially overlap those previously identified in studies of LSC of young animals with chronic inflammatory or neuropathic pain.

Conclusions: Up-modulation of complement pathway, microglial priming and activation, and T cell/antigen-presenting cell communication in healthy middle-aged LSC was found. Taken together with our previous work, the results support our conclusion that an incipient or para-inflammatory state develops in the LSC in healthy middle-aged adults.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5390443PMC
http://dx.doi.org/10.1186/s12979-017-0091-6DOI Listing

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