The nonreceptor protein tyrosine kinase Src participates in every step of cancer-induced bone pain - 03/09/21
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Abstract |
Cancer-induced bone pain (CIBP) is a refractory form of pain that has a high incidence in advanced tumors. Src protein tyrosine kinase is mainly composed of six domains, with two states of automatic inhibition and activation. The modular domain allows Src to conveniently regulate by and communicate with a variety of proteins, directly or indirectly participate in each step of the CIBP process. Src is beneficial to the growth and proliferation of tumor cells, and it can promote the metastases of primary tumors to bone. In the microenvironment of bone metastasis, it mainly mediates bone resorption, activates related peripheral receptors to participate in the formation of pain signals, and may promote the generation of pathological sensory nerve fibers. In the process of pain signal transmission, it mainly mediates NMDAR and central glial cells to regulate pain signal intensity and central sensitization, but it is not limited to these two aspects. Both basic experimentation and clinical research have shown encouraging potential, providing new ideas and inspiration for the prevention and treatment of CIBP.
Le texte complet de cet article est disponible en PDF.Graphical Abstract |
Highlights |
• | Src is mainly composed of six domains, with two states of automatic inhibition and activation. |
• | Src directly or indirectly participates in each step of the CIBP process. |
• | Src can promote the metastases of primary tumors to bone. |
• | Src mediates bone resorption and activates related peripheral receptors and may promote the pathological nerve fibers. |
• | Src mainly mediates NMDAR and central glial cells to regulate pain signal intensity and central sensitization. |
Keywords : Src, Cancer-induced bone pain, Bone metastasis
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Vol 141
Article 111822- septembre 2021 Retour au numéroBienvenue sur EM-consulte, la référence des professionnels de santé.
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