PT  - JOURNAL ARTICLE
AU  - R. Gill
AU  - A. Alanine
AU  - A. Bourson
AU  - B. Buttelmann
AU  - G. Fischer
AU  - M.-P. Heitz
AU  - J. N. C. Kew
AU  - B. Levet-Trafit
AU  - H.-P. Lorez
AU  - P. Malherbe
AU  - M.-T. Miss
AU  - V. Mutel
AU  - E. Pinard
AU  - S. Roever
AU  - M. Schmitt
AU  - G. Trube
AU  - R. Wybrecht
AU  - R. Wyler
AU  - J. A. Kemp
TI  - Pharmacological Characterization of Ro 63-1908 (1-[2-(4-Hydroxy-phenoxy)-ethyl]-4-(4-methyl-benzyl)-piperidin-4-ol), a Novel Subtype-Selective&lt;em&gt;N&lt;/em&gt;-Methyl-&lt;span class=&quot;sc&quot;&gt;d&lt;/span&gt;-Aspartate Antagonist
AID  - 10.1124/jpet.102.034322
DP  - 2002 Sep 01
TA  - Journal of Pharmacology and Experimental Therapeutics
PG  - 940--948
VI  - 302
IP  - 3
4099  - http://jpet.aspetjournals.org/content/302/3/940.short
4100  - http://jpet.aspetjournals.org/content/302/3/940.full
SO  - J Pharmacol Exp Ther2002 Sep 01; 302
AB  - Ro 63-1908, 1-[2-(4-hydroxy-phenoxy)-ethyl]-4-(4-methyl-benzyl)-piperidin-4-ol, is a novel subtype-selectiveN-methyl-d-aspartate (NMDA) antagonist that has been characterized in vitro and in vivo. Ro 63-1908 inhibited [3H]dizocilpine (3H-MK-801) binding in a biphasic manner with IC50 values of 0.002 and 97 μM for the high- and low-affinity sites, respectively. Ro 63-1908 selectively blocked recombinant receptors expressed in Xenopusoocytes containing NR1C + NR2B subunits with an IC50 of 0.003 μM and those containing NR1C + NR2A subunits with an IC50 of &amp;gt;100 μM, thus demonstrating greater than 20,000-fold selectivity for the recombinant receptors expressing NR1C + NR2B. Ro 63-1908 blocked these NMDA NR2B-subtype receptors in an activity-dependent manner. Ro 63-1908 was neuroprotective against glutamate-induced toxicity and against oxygen/glucose deprivation-induced toxicity in vitro with IC50 values of 0.68 and 0.06 μM, respectively. Thus, the in vitro pharmacological characterization demonstrated that Ro 63-1908 was a potent and highly selective antagonist of the NR2B subtype of NMDA receptors. Ro 63-1908 was active against sound-induced seizures (ED50 = 4.5 mg/kg i.p. when administered 30 min beforehand) in DBA/2 mice. The dose required to give a full anticonvulsant effect did not produce a deficit in the Rotarod test. NMDA-induced seizures were also inhibited by Ro 63-1908 with an ED50 of 2.31 mg/kg i.v. when administered 15 min before testing. Ro 63-1908 gave a dose-related neuroprotective effect against cortical damage in a model of permanent focal ischemia. Maximum protection of 39% was seen at a plasma concentration of 450 ng/ml. There were, however, no adverse cardiovascular or CNS side-effects seen at this dosing level. The American Society for Pharmacology and Experimental Therapeutics