Attenuation of thermal nociception and hyperalgesia by VR1 blockers

doi:10.1073/pnas.022285899

Attenuation of thermal nociception and hyperalgesia by VR1 blockers

^*Centro de Biología Molecular y Celular, Universidad Miguel Hernández, Alicante, Spain; ^†Institut d'Investigacions Químiques i Ambientals de Barcelona, Consejo Superior de Investigaciones Científicas, Barcelona, Spain; ^§Departamento de Bioquímica y Biología Molecular, Universidad de Valencia, Valencia, Spain; and ^‡Instituto de Neurociencias, Universidad Miguel Hernández–Consejo Superior de Investigaciones Científicas, Alicante, Spain

Edited by Ramon Latorre, Center for Scientific Studies, Valdivia, Chile, and approved November 20, 2001 (received for review June 7, 2001)

Abstract

Vanilloid receptor subunit 1 (VR1) appears to play a critical role in the transduction of noxious chemical and thermal stimuli by sensory nerve endings in peripheral tissues. Thus, VR1 antagonists are useful compounds to unravel the contribution of this receptor to pain perception, as well as to induce analgesia. We have used a combinatorial approach to identify new, nonpeptidic channel blockers of VR1. Screening of a library of trimers of N-alkylglycines resulted in the identification of two molecules referred to as DD161515 {N-[2-(2-(N-methylpyrrolidinyl)ethyl]glycyl]-[N-[2,4-dichlorophenethyl]glycyl]-N-(2,4-dichlorophenethyl)glycinamide} and DD191515 {[N-[3-(N,N-diethylamino)propyl]glycyl]-[N-[2,4-dichlorophenethyl]glycyl]-N-(2,4-dichlorophenethyl)glycinamide} that selectively block VR1 channel activity with micromolar efficacy, rivaling that characteristic of vanilloid-related inhibitors. These compounds appear to be noncompetitive VR1 antagonists that recognize a receptor site distinct from that of capsaicin. Intraperitoneal administration of both trialkylglycines into mice significantly attenuated thermal nociception as measured in the hot plate test. It is noteworthy that these compounds eliminated pain and neurogenic inflammation evoked by intradermal injection of capsaicin into the animal hindpaw, as well as the thermal hyperalgesia induced by tissue irritation with nitrogen mustard. In contrast, responses to mechanical stimuli were not modified by either compound. Modulation of sensory nerve fibers excitability appears to underlie the peptoid analgesic activity. Collectively, these results indicate that blockade of VR1 activity attenuates chemical and thermal nociception and hyperalgesia, supporting the tenet that this ionotropic receptor contributes to chemical and thermal sensitivity and pain perception in vivo. These trialkylglycine-based, noncompetitive VR1 antagonists may likely be developed into analgesics to treat inflammatory pain.

Footnotes

↵ ¶ To whom reprint requests should be addressed at: Centro de Biología Molecular y Celular, Universidad Miguel Hernández, Edificio Torregaitán, Avenida Ferrocarril s/n, 03202 Elche (Alicante), Spain. E-mail: aferrer{at}umh.es.
This paper was submitted directly (Track II) to the PNAS office.
Abbreviations:

VR1,

vanilloid receptor subunit 1;

DD161515,

[N-[2-(2-(N-methylpyrrolidinyl)ethyl]glycyl]-[N-[2,4-dichlorophenethyl]glycyl]-N-(2,4-dichlorophenethyl)glycinamide;

DD191515,

[N-[3-(N,N-diethylamino)propyl]glycyl]-[N-[2,4-dichlorophenethyl]glycyl]-N-(2,4-dichlorophenethyl)glycinamide;

[Ca2+]i,

intracellular Ca2+