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Publication : The EGF-LIKE domain of thrombospondin-4 is a key determinant in the development of pain states due to increased excitatory synaptogenesis.

First Author  Park JF Year  2018
Journal  J Biol Chem Volume  293
Issue  42 Pages  16453-16463
PubMed ID  30194282 Mgi Jnum  J:277220
Mgi Id  MGI:6268519 Doi  10.1074/jbc.RA118.003591
Citation  Park JF, et al. (2018) The EGF-LIKE domain of thrombospondin-4 is a key determinant in the development of pain states due to increased excitatory synaptogenesis. J Biol Chem 293(42):16453-16463
abstractText  Up-regulation of thrombospondin-4 (TSP4) or voltage-gated calcium channel subunit alpha2delta1 (Cavalpha2delta1) proteins in the spinal cord contributes to neuropathic pain development through an unidentified mechanism. We have previously shown that TSP4 interacts with Cavalpha2delta1 to promote excitatory synaptogenesis and the development of chronic pain states. However, the TSP4 determinants responsible for these changes are not known. Here, we tested the hypothesis that the Cavalpha2delta1-binding domains of TSP4 are synaptogenic and pronociceptive. We mapped the major Cavalpha2delta1-binding domains of TSP4 within the coiled-coil and epidermal growth factor (EGF)-like domains in vitro Intrathecal injection of TSP4 fragment proteins containing the EGF-like domain (EGF-LIKE) into naive rodents was sufficient for inducing behavioral hypersensitivity similar to that produced by an equal molar dose of full-length TSP4. Gabapentin, a drug that binds to Cavalpha2delta1, blocked EGF-LIKE-induced behavioral hypersensitivity in a dose-dependent manner, supporting the notion that EGF-LIKE interacts with Cavalpha2delta1 and thereby mediates behavioral hypersensitivity. This notion was further supported by our findings that a peptide within EGF-LIKE (EGFD355-369) could block TSP4- or Cavalpha2delta1-induced behavioral hypersensitivity after intrathecal injections. Furthermore, only TSP4 proteins that contained EGF-LIKE could promote excitatory synaptogenesis between sensory and spinal cord neurons, which could be blocked by peptide EGFD355-369. Together, these findings indicate that EGF-LIKE is the molecular determinant that mediates aberrant excitatory synaptogenesis and chronic pain development. Blocking interactions between EGF-LIKE and Cavalpha2delta1 could be an alternative approach in designing target-specific pain medications.
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