Abstract
Background: Chronic neuropathic pain (CNP) is a debilitating condition, often refractory to currently available drugs. Understanding biochemical alterations in peripheral tissues such as blood will be useful for understanding underlying pathophysiological processes relating to CNP. Methods: We collected blood from two independent cohorts of CNP and pain-free controls (CNP n = 129/Controls n = 127) in the UK and Ireland to investigate the relationship between CNP-associated molecular/biochemical alterations and a range of clinical and pain metric parameters. Multiple statistical comparisons were conducted on the data, with selected variables included in one or more of the intended inferential analyses (six models). Results: Gene expression analysis showed that choline phosphotransferase (CHPT1) was increased (p
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Bourke, S. L., Suarez, E. G., Islam, B., Stephenson, J., Finn, D. P., & McHugh, P. C. (2025). Clinical measures in chronic neuropathic pain are related to the Kennedy and endocannabinoid pathways. European Journal of Clinical Investigation, 55(2). https://doi.org/10.1111/eci.14351
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