Monocytes expressing CX3CR1 orchestrate the development of vincristine-induced pain |
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| Authors: | Elizabeth A. Old Suchita Nadkarni John Grist Clive Gentry Stuart Bevan Ki-Wook Kim Adrian J. Mogg Mauro Perretti Marzia Malcangio |
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| Affiliation: | 1.Wolfson Centre for Age-Related Diseases, King’s College London, London, United Kingdom. 2.The William Harvey Research Institute, Barts and The London School of Medicine, London, United Kingdom. 3.Department of Microbial Pathogenesis, Yale University School of Medicine, New Haven, Connecticut, USA. 4.Eli Lilly and Company Ltd., Erl Wood Manor, Windlesham, Surrey, United Kingdom. |
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| Abstract: | ![]()
A major dose-limiting side effect associated with cancer-treating antineoplastic drugs is the development of neuropathic pain, which is not readily relieved by available analgesics. A better understanding of the mechanisms that underlie pain generation has potential to provide targets for prophylactic management of chemotherapy pain. Here, we delineate a pathway for pain that is induced by the chemotherapeutic drug vincristine sulfate (VCR). In a murine model of chemotherapy-induced allodynia, VCR treatment induced upregulation of endothelial cell adhesion properties, resulting in the infiltration of circulating CX3CR1+ monocytes into the sciatic nerve. At the endothelial-nerve interface, CX3CR1+ monocytes were activated by the chemokine CX3CL1 (also known as fractalkine [FKN]), which promoted production of reactive oxygen species that in turn activated the receptor TRPA1 in sensory neurons and evoked the pain response. Furthermore, mice lacking CX3CR1 exhibited a delay in the development of allodynia following VCR administration. Together, our data suggest that CX3CR1 antagonists and inhibition of FKN proteolytic shedding, possibly by targeting ADAM10/17 and/or cathepsin S, have potential as peripheral approaches for the prophylactic treatment of chemotherapy-induced pain. |
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