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Monocytes expressing CX3CR1 orchestrate the development of vincristine-induced pain.


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.

SUBMITTER: Old EA 

PROVIDER: S-EPMC4001538 | biostudies-literature | 2014 May

REPOSITORIES: biostudies-literature

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Monocytes expressing CX3CR1 orchestrate the development of vincristine-induced pain.

Old Elizabeth A EA   Nadkarni Suchita S   Grist John J   Gentry Clive C   Bevan Stuart S   Kim Ki-Wook KW   Mogg Adrian J AJ   Perretti Mauro M   Malcangio Marzia M  

The Journal of clinical investigation 20140417 5


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, V  ...[more]

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