PT  - JOURNAL ARTICLE
AU  - Todd W. Vanderah
AU  - Claudio D. Schteingart
AU  - Jerzy Trojnar
AU  - Jean-Louis Junien
AU  - Josephine Lai
AU  - Pierre J.-M. Riviere
TI  - FE200041 (&lt;span class=&quot;sc&quot;&gt;d&lt;/span&gt;-Phe-&lt;span class=&quot;sc&quot;&gt;d&lt;/span&gt;-Phe-&lt;span class=&quot;sc&quot;&gt;d&lt;/span&gt;-Nle-&lt;span class=&quot;sc&quot;&gt;d&lt;/span&gt;-Arg-NH&lt;sub&gt;2&lt;/sub&gt;): A Peripheral Efficacious κ Opioid Agonist with Unprecedented Selectivity
AID  - 10.1124/jpet.104.065391
DP  - 2004 Jul 01
TA  - Journal of Pharmacology and Experimental Therapeutics
PG  - 326--333
VI  - 310
IP  - 1
4099  - http://jpet.aspetjournals.org/content/310/1/326.short
4100  - http://jpet.aspetjournals.org/content/310/1/326.full
SO  - J Pharmacol Exp Ther2004 Jul 01; 310
AB  - The side effects typically associated with the clinical profiles of opioid μ-receptor agonists have driven continuing efforts to identify novel efficacious analgesics, including agonists acting at opioid κ receptors. Unfortunately, the therapeutic potential of κ agonists seems limited by significant central nervous system side effects. κ Opioid agonists, however, exhibit potent peripherally mediated antihyperalgesic and antinociceptive effects, suggesting that a peripherally acting κ agonist may be efficacious in pain control with a more desirable safety profile than that associated with currently available opioids. Here, we report an all d-amino acid tetrapeptide characterized as a novel, highly selective κ opioid receptor agonist. FE200041 (d-Phe-d-Phe-d-Nle-d-Arg-NH2) showed selectivity for the human κ opioid receptor of greater than 30,000- and 68,000-fold versus human μ opioid receptor and human δ-opioid receptor receptors, respectively, and efficacious agonist activity using in vitro tissue assays. FE200041 produced local, peripheral antinociception in the hindpaw ipsilateral, but not contralateral, to injection. Antinociceptive effects of FE200041 in the mouse acetic acid writhing assay lasted over 60 min and were antagonized by naloxone and by selective κ, but not μ, opioid receptor antagonists. FE200041 significantly inhibited acetic acid writhing and inhibited formalin-induced flinching in rats. FE200041 did not elicit sedation or motor impairment after systemic administration at a dose 10-fold higher than that needed to achieve antinociception. FE200041 is thus a potent peripherally restricted opioid κ agonist with no demonstrable side effects typical of κ agonists with central nervous system activity and with unprecedented selectivity for the opioid κ receptor. The pharmacology of this compound suggests the possibility of therapeutic application. The American Society for Pharmacology and Experimental Therapeutics