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Publication : Macrophage memories of early-life injury drive neonatal nociceptive priming.

First Author  Dourson AJ Year  2024
Journal  Cell Rep Volume  43
Issue  5 Pages  114129
PubMed ID  38640063 Mgi Jnum  J:350952
Mgi Id  MGI:7658783 Doi  10.1016/j.celrep.2024.114129
Citation  Dourson AJ, et al. (2024) Macrophage memories of early-life injury drive neonatal nociceptive priming. Cell Rep 43(5):114129
abstractText  The developing peripheral nervous and immune systems are functionally distinct from those of adults. These systems are vulnerable to early-life injury, which influences outcomes related to nociception following subsequent injury later in life (i.e., "neonatal nociceptive priming"). The underpinnings of this phenomenon are unclear, although previous work indicates that macrophages are trained by inflammation and injury. Our findings show that macrophages are both necessary and partially sufficient to drive neonatal nociceptive priming, possibly due to a long-lasting remodeling in chromatin structure. The p75 neurotrophic factor receptor is an important effector in regulating neonatal nociceptive priming through modulation of the inflammatory profile of rodent and human macrophages. This "pain memory" is long lasting in females and can be transferred to a naive host to alter sex-specific pain-related behaviors. This study reveals a mechanism by which acute, neonatal post-surgical pain drives a peripheral immune-related predisposition to persistent pain following a subsequent injury.
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