COMMENTS
Client Education
LC‐MS may be useful in legal cases.
Prevention/Avoidance
Prevent exposure to illegal drugs.
Keep animals away from illegal drugs.
Educate trainers/riders/grooms of the risk of low‐level contamination.
Avoid access to illegal drugs.
Expected Course and Prognosis
Acute fatal toxicity has not been reported. Toxic effects would likely reside within hours.
Abbreviations
See Appendix 1 for a complete list.
Suggested Reading
1 Kollias‐Baker C, Maxwell L, Stanley S, Boone T. Detection and quantification of cocaine metabolites in urine samples from horses administered cocaine. J Vet Pharmacol Ther. 2003; 26(6):429–434.
2 Richards JR, Hollander JE, Ramoska EA, et al. β‐Blockers, cocaine, and the unopposed α‐stimulation phenomenon. J Cardiovasc Pharmacol Ther 2017; 22(3):239–249.
3 Zimmerman JL. Cocaine intoxication. Crit Care Clin 2012; 28(4):517–526.
Author: Cynthia Cole, DVM, PhD, DACVCP
Consulting Editor: Dionne Benson, DVM, JD
Chapter 8 Dermorphin
DEFINITION/OVERVIEW
Dermorphin (“derm” = skin, and “morphin” = morphine) is just one compound in a family of peptides secreted by the skin of South American hylid frogs, genus Phyllomedusa.
Most commonly found as a synthesized series of amino acids.
Dermorphin is a hepta‐peptide known to have exceptionally long‐lasting and potent opioid activity.
Potency is about 30–40 times greater than that of morphine, and less likely to cause a drug tolerance effect and addiction in humans.
In humans it has been shown to block pain effectively.
First detected in post‐race testing in Quarter Horse racing in the southwestern United States in 30 horses in 2011–2012.
Dermorphin stimulates locomotor activity and purportedly improves focus and determination in equines.
The D‐isomer is biologically active, but the L‐isomer is not.
Prohibited under ARCI and AQHA rules.
ETIOLOGY/PATHOPHYSIOLOGY
Mechanism of Action
Dermorphin is a mu‐opioid receptor‐binding peptide that causes central and peripheral effects after intravenous administration to rats, dogs, and humans.
In addition to dermorphin, the family of mu‐opioid agonists include seven naturally occurring dermorphin analogs, and at least 30 known synthetic analogs. The inactive L‐isomer of dermorphin is also known as “pseudomorphin”. Another close relative is HYP6‐dermorphin, which contains hydroxyproline instead of proline in the otherwise same amino acid sequence.
Some members of the dermorphin peptide family can cross the blood–brain barrier (BBB) and produce central antinociception after peripheral administration, but dermorphin itself is not able to cross the BBB.
Toxicokinetics
Onset of action is rapid with clinical signs appearing in minutes.
Duration of action is short, with most clinical signs subsiding within hours.
Hepatic and renal metabolism was observed in rats.
Urinary excretion primarily.
Toxicity
Toxicity observed in horses in doses of 5 mg.
Compounded versions may have variable toxicity.
Dermorphin is unstable at room temp, with some studies showing > 50% degradation after 4 hours at room temperature which may contribute to toxicity. The L‐isomer (inactive stereoisomer) is more labile than the D‐isomer (active form).
Systems Affected
Neurological – head shaking, sedation, sweating, increased locomotion, catalepsy.
Gastrointestinal – colic, decreased borborygmi.
Cardiovascular – tachypnea.
Musculoskeletal – antinociception.
SIGNALMENT
Risk Factors
Iatrogenic.
Historical Findings
Owners and trainers may be reluctant to admit possession or use.
Location and Circumstances of Poisoning
Likely in competitive equine sports environment (e.g., racing, barrel racing, etc.).
CLINICAL FEATURES
Clinical signs begin less than a minute after administration.
Common signs include head shaking, sedation, sweating, trance‐like state, colic, tachypnea, and antinociception.
DIFFERENTIAL DIAGNOSIS
CNS depressants (benzodiazepine, opioids).
Hallucinogenic plants and mushrooms.
Ethanol.
Rabies.
Colic of other etiology.
DIAGNOSTICS
CBC/Serum Chemistry/Urinalysis
Routine bloodwork:Hyponatremia/hypokalemia reported in humans but may be attributable to other causes.