Pharmacology, pharmacokinetics, and metabolism of the DNA-decoy AYX1 for the prevention of acute and chronic post-surgical pain

Julien Mamet; Scott Harris; Michael Klukinov; David C Yeomans; Renee R Donahue; Brad K Taylor; Kelly Eddinger; Tony Yaksh; Donald C Manning

doi:10.1177/1744806917703112

Pharmacology, pharmacokinetics, and metabolism of the DNA-decoy AYX1 for the prevention of acute and chronic post-surgical pain

Mol Pain. 2017 Jan:13:1744806917703112. doi: 10.1177/1744806917703112.

Authors

Julien Mamet¹, Scott Harris¹, Michael Klukinov², David C Yeomans², Renee R Donahue³, Brad K Taylor³, Kelly Eddinger⁴, Tony Yaksh⁴, Donald C Manning¹

Affiliations

¹ 1 Adynxx, Inc., CA, USA.
² 2 Department of Anesthesia, Stanford University, CA, USA.
³ 3 Department of Physiology, University of Kentucky, KY, USA.
⁴ 4 Department of Anesthesiology and Pharmacology, University of California, San Diego, CA, USA.

Abstract

Background AYX1 is an unmodified DNA-decoy designed to reduce acute post-surgical pain and its chronification with a single intrathecal dose at the time of surgery. AYX1 inhibits the transcription factor early growth response protein 1, which is transiently induced at the time of injury and triggers gene regulation in the dorsal root ganglia and spinal cord that leads to long-term sensitization and pain. This work characterizes the AYX1 dose-response profile in rats and the link to AYX1 pharmacokinetics and metabolism in the cerebrospinal fluid, dorsal root ganglia, and spinal cord. Results The effects of ascending dose-levels of AYX1 on mechanical hypersensitivity were measured in the spared nerve injury model of chronic pain and in a plantar incision model of acute post-surgical pain. AYX1 dose-response profile shows that efficacy rapidly increases from a minimum effective dose of ∼ 0.5 mg to a peak maximum effective dose of ∼ 1 mg. With further dose escalation, the efficacy paradoxically appears to decrease by ∼ 30% and then returns to full efficacy at the maximum feasible dose of ∼ 4 mg. The reduction of efficacy is associated to doses triggering a near-saturation of AYX1 metabolism by nucleases in the cerebrospinal fluid and a paradoxical reduction of AYX1 exposure during the period of early growth response protein 1 induction. This effect is overcome at higher doses that compensate for the effect of metabolism. Discussion AYX1 is a competitive antagonist of early growth response protein 1, which is consistent with the overall increased efficacy observed as dose-levels initially escalate. Chemically, AYX1 is unprotected against degradation by nucleases. The sensitivity to nucleases is reflected in a paradoxical reduction of efficacy in the dose-response curve. Conclusions These findings point to the importance of the nuclease environment of the cerebrospinal fluid to the research and development of AYX1 and other intrathecal nucleotide-based therapeutics.

Keywords: Chronic pain; cerebrospinal fluid; early growth response protein 1; nucleases; oligonucleotide.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Acute Pain / etiology
Acute Pain / prevention & control*
Analgesics* / administration & dosage
Analgesics* / metabolism
Analgesics* / pharmacology
Animals
Chronic Pain / etiology
Chronic Pain / prevention & control*
DNA* / administration & dosage
DNA* / metabolism
DNA* / pharmacology
Disease Models, Animal
Dose-Response Relationship, Drug
Early Growth Response Protein 1 / metabolism
Ganglia, Spinal / drug effects
Oligonucleotides* / metabolism
Oligonucleotides* / pharmacology
Oligonucleotides* / therapeutic use
Pain Measurement
Pain, Postoperative / complications
Pain, Postoperative / prevention & control
Rats
Rats, Sprague-Dawley
Spinal Cord / drug effects

Substances

Analgesics
Early Growth Response Protein 1
Egr1 protein, rat
Oligonucleotides
DNA

Grants and funding

R01 DA037621/DA/NIDA NIH HHS/United States