Spinophilin modulates pain through suppressing dendritic spine morphogenesis via negative control of Rac1-ERK signaling in rat spinal dorsal horn

• Published in: Neurobiology of disease Vol. 152; p. 105302
• Main Authors: Wang, Jiang-Lin, Wang, Yan, Sun, Wei, Yu, Yang, Wei, Na, Du, Rui, Yang, Yan, Liang, Ting, Wang, Xiao-Liang, Ou, Ce-Hua, Chen, Jun
• Format: Journal Article
• Language: English
• Published: United States Elsevier Inc 01.05.2021; Elsevier
• Subjects: Animals; Dendritic spine; Dendritic Spines; ERK; Male; MAP Kinase Signaling System - physiology; Microfilament Proteins - metabolism; Nerve Tissue Proteins - metabolism; Pain; Pain - metabolism; Rac1; rac1 GTP-Binding Protein - metabolism; Rats; Rats, Sprague-Dawley; Spinal Cord Dorsal Horn - metabolism; Spinal dorsal horn; Spinophilin; Dendritic spine; Spinal dorsal horn; Spinophilin; Pain; Rac1; ERK
• ISSN: 0969-9961; 1095-953X
• DOI: 10.1016/j.nbd.2021.105302

Both spinophilin (SPN, also known as neurabin 2) and Rac1 (a member of Rho GTPase family) are believed to play key roles in dendritic spine (DS) remodeling and spinal nociception. However, how SPN interacts with Rac1 in the above process is unknown. Here, we first demonstrated natural existence of SPN-protein phosphatase 1-Rac1 complex in the spinal dorsal horn (DH) neurons by both double immunofluorescent labeling and co-immunoprecipitation, then the effects of SPN over-expression and down-regulation on mechanical and thermal pain sensitivity, GTP-bound Rac1-ERK signaling activity, and spinal DS density were studied. Over-expression of SPN in spinal neurons by intra-DH pAAV-CMV-SPN-3FLAG could block both mechanical and thermal pain hypersensitivity induced by intraplantar bee venom injection, however it had no effect on the basal pain sensitivity. Over-expression of SPN also resulted in a significant decrease in GTP-Rac1-ERK activities, relative to naive and irrelevant control (pAAV-MCS). In sharp contrast, knockdown of SPN in spinal neurons by intra-DH pAAV-CAG-eGFP-U6-shRNA[SPN] produced both pain hypersensitivity and dramatic elevation of GTP-Rac1-ERK activities, relative to naive and irrelevant control (pAAV-shRNA [NC]). Moreover, knockdown of SPN resulted in increase in DS density while over-expression of it had no such effect. Collectively, SPN is likely to serve as a regulator of Rac1 signaling to suppress DS morphogenesis via negative control of GTP-bound Rac1-ERK activities at postsynaptic component in rat DH neurons wherein both mechanical and thermal pain sensitivity are controlled. •Spinophilin binds Rac1 with protein phosphatase 1 in spinal dorsal horn neurons.•Spinophilin negatively controls GTP-bound Rac1-ERK activities at dendritic spines.•Spinophilin suppresses spinal dendritic spine morphogenesis and pain.