N-ETHYL-2-[(6-METHOXYPYRIDIN-3-YL)-(2-METHYLPHENYL)SULFONYLAMINO]-N-(PYRIDIN-3-YLMETHYL)ACETAMIDE

EMPA competitively antagonizes orexin-A-and orexin-B-evoked accumulation of [ ³ H]inositol phosphates (IP) at hOX ₂ receptors with pA ₂ values of 8.6 and 8.8 respectively.
EMPA displaces the [ ³ H]EMPA binding from cell membranes containing human and rat OX ₂ receptors, with K _i values of 1.10±0.24 nM and 1.45±0.13 nM, respectively.
EMPA shows an IC ₅₀ =5.75 µM, K _i =2.63 µM, and IC ₅₀ =12.8 µM, K _i =5.8 µM in the binding assay at human and mouse V _1a receptors, respectively.
In CHO(dHFr ^- ) cells stably expressing hOX ₂ receptors, EMPA inhibits orexin-A-or orexin-B-evoked [Ca ²⁺ ] _i response with IC ₅₀ s of 8.8±1.7 nM and 7.9±1.7 nM, respectively.

EMPA (1-300 mg/kg; i.p.) dose-dependently reverses this [Ala ¹¹ ,D-Leu ¹⁵ ]orexin-B-induced hyperlocomotion without itself significantly affecting locomotor activity (LMA) in male NMRI mice.
EMPA (3-30 mg/kg; i.p.) induces a significant and dose-dependent reduction in the baseline LMA in france and male Wistar rats. EMPA (3-30 mg/kg; i.p.) demonstrates a clear dose-dependent inhibition of spontaneous activity as compared with vehicle-treated animals.