A Role for Protease Activated Receptor Type 3 (PAR3) in Nociception Demonstrated Through Development of a Novel Peptide Agonist.

Mwirigi, Juliet; Kume, Moeno; Hassler, Shayne N; Ahmad, Ayesha; Ray, Pradipta R; Jiang, Changyu; Chamessian, Alexander; Mseeh, Nakleh; Ludwig, Breya P; Rivera, Benjamin D; Nieman, Marvin T; Van de Ven, Thomas; Ji, Ru-Rong; Dussor, Gregory; Boitano, Scott; Vagner, Josef; Price, Theodore J

Mwirigi, Juliet; Kume, Moeno; Hassler, Shayne N; Ahmad, Ayesha; Ray, Pradipta R; Jiang, Changyu; Chamessian, Alexander; Mseeh, Nakleh; Ludwig, Breya P; Rivera, Benjamin D; Nieman, Marvin T; Van de Ven, Thomas; Ji, Ru-Rong; Dussor, Gregory; Boitano, Scott; Vagner, Josef; Price, Theodore J.

Afiliación

Mwirigi J; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Kume M; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Hassler SN; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Ahmad A; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Ray PR; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Jiang C; Duke University School of Medicine, Department of Anesthesiology, Pharmacology, and Cancer Biology, Durham, North Carolina.
Chamessian A; Duke University School of Medicine, Department of Anesthesiology, Pharmacology, and Cancer Biology, Durham, North Carolina.
Mseeh N; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Ludwig BP; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Rivera BD; Department of Physiology, University of Arizona, Asthma and Airway Disease Research Center, Tucson, Arizona.
Nieman MT; Case Western Reserve University School of Medicine, Department of Pharmacology, Cleveland, Ohio.
Van de Ven T; Duke University School of Medicine, Department of Anesthesiology, Pharmacology, and Cancer Biology, Durham, North Carolina.
Ji RR; Duke University School of Medicine, Department of Anesthesiology, Pharmacology, and Cancer Biology, Durham, North Carolina.
Dussor G; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas.
Boitano S; Department of Physiology, University of Arizona, Asthma and Airway Disease Research Center, Tucson, Arizona.
Vagner J; University of Arizona, Bio5 Research Institute, Tucson, Arizona.
Price TJ; University of Texas at Dallas, School of Behavioral and Brain Sciences and Center for Advanced Pain Studies, Richardson, Texas. Electronic address: Theodore.price@utdallas.edu.

J Pain ; 22(6): 692-706, 2021 06.

Article en En | MEDLINE | ID: mdl-33429107

RESUMEN

The protease activated receptor (PAR) family is a group of G-protein coupled receptors (GPCRs) activated by proteolytic cleavage of the extracellular domain. PARs are expressed in a variety of cell types with crucial roles in homeostasis, immune responses, inflammation, and pain. PAR3 is the least researched of the four PARs, with little known about its expression and function. We sought to better understand its potential function in the peripheral sensory nervous system. Mouse single-cell RNA sequencing data demonstrates that PAR3 is widely expressed in dorsal root ganglion (DRG) neurons. Co-expression of PAR3 mRNA with other PARs was identified in various DRG neuron subpopulations, consistent with its proposed role as a coreceptor of other PARs. We developed a lipid tethered PAR3 agonist, C660, that selectively activates PAR3 by eliciting a Ca2+ response in DRG and trigeminal neurons. In vivo, C660 induces mechanical hypersensitivity and facial grimacing in WT but not PAR3-/- mice. We characterized other nociceptive phenotypes in PAR3-/- mice and found a loss of hyperalgesic priming in response to IL-6, carrageenan, and a PAR2 agonist, suggesting that PAR3 contributes to long-lasting nociceptor plasticity in some contexts. To examine the potential role of PAR3 in regulating the activity of other PARs in sensory neurons, we administered PAR1, PAR2, and PAR4 agonists and assessed mechanical and affective pain behaviors in WT and PAR3-/- mice. We observed that the nociceptive effects of PAR1 agonists were potentiated in the absence of PAR3. Our findings suggest a complex role of PAR3 in the physiology and plasticity of nociceptors. PERSPECTIVE: We evaluated the role of PAR3, a G-protein coupled receptor, in nociception by developing a selective peptide agonist. Our findings suggest that PAR3 contributes to nociception in various contexts and plays a role in modulating the activity of other PARs.

Asunto(s)

Proteínas Adaptadoras Transductoras de Señales/agonistas; Proteínas Adaptadoras Transductoras de Señales/fisiología; Proteínas de Ciclo Celular/agonistas; Proteínas de Ciclo Celular/fisiología; Ganglios Espinales/metabolismo; Nocicepción/fisiología; Animales; Masculino; Ratones; Ratones Endogámicos C57BL; Ratones Endogámicos ICR; Ratones Noqueados; Nocicepción/efectos de los fármacos

Palabras clave

PAR3; hyperalgesic priming; nociceptor; pain; protease activated receptor

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Proteínas de Ciclo Celular / Proteínas Adaptadoras Transductoras de Señales / Nocicepción / Ganglios Espinales Tipo de estudio: Prognostic_studies Límite: Animals Idioma: En Revista: J Pain Asunto de la revista: NEUROLOGIA / PSICOFISIOLOGIA Año: 2021 Tipo del documento: Article

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