Peripherally restricted PICK1 inhibitor mPD5 ameliorates pain behaviors in murine inflammatory and neuropathic pain models
Kathrine Louise Jensen, … , Andreas Toft Sørensen, Kenneth Lindegaard Madsen
Kathrine Louise Jensen, … , Andreas Toft Sørensen, Kenneth Lindegaard Madsen
Published September 17, 2024
Citation Information: JCI Insight. 2024;9(20):e170976. https://doi.org/10.1172/jci.insight.170976.
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Research Article Neuroscience

Peripherally restricted PICK1 inhibitor mPD5 ameliorates pain behaviors in murine inflammatory and neuropathic pain models

Abstract

Chronic pain is a complex, debilitating, and escalating health problem worldwide, impacting 1 in 5 adults. Current treatment is compromised by dose-limiting side effects, including high abuse liability, loss of ability to function socially and professionally, fatigue, drowsiness, and apathy. PICK1 has emerged as a promising target for the treatment of chronic pain conditions. Here, we developed and characterized a cell-permeable fatty acid–conjugated bivalent peptide inhibitor of PICK1 and assessed its effects on acute and chronic pain. The myristoylated PICK1 inhibitor, myr-NPEG4-(HWLKV)2 (mPD5), self-assembled into core-shell micelles that provided favorable pharmacodynamic properties and relieved evoked mechanical and thermal hypersensitivity as well as ongoing hypersensitivity and anxiodepressive symptoms in mouse models of neuropathic and inflammatory pain following subcutaneous administration. No overt side effects were associated with mPD5 administration, and it had no effect on acute nociception. Finally, neuropathic pain was relieved far into the chronic phase (18 weeks after spared nerve injury surgery) and while the effect of a single injection ceased after a few hours, repeated administration provided pain relief lasting up to 20 hours after the last injection.

Authors

Kathrine Louise Jensen, Nikolaj Riis Christensen, Carolyn Marie Goddard, Sara Elgaard Jager, Gith Noes-Holt, Ida Buur Kanneworff, Alexander Jakobsen, Lucía Jiménez-Fernández, Emily G. Peck, Line Sivertsen, Raquel Comaposada Baro, Grace Anne Houser, Felix Paul Mayer, Marta Diaz-delCastillo, Marie Løth Topp, Chelsea Hopkins, Cecilie Dubgaard Thomsen, Ahmed Barakat Ibrahim Soltan, Frederik Grønbæk Tidemand, Lise Arleth, Anne-Marie Heegaard, Andreas Toft Sørensen, Kenneth Lindegaard Madsen

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Figure 5

Efficacy of mPD5 in a model of neuropathic pain in WT and PICK1-KO mice.

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Efficacy of mPD5 in a model of neuropathic pain in WT and PICK1-KO mice....
(A) Timeline for B, C, and E. (B) Paw withdrawal threshold (PWT) before and after induction of neuropathic pain (SNI surgery) and s.c. treatment with mPD5 or PBS. n = 6. (C) Marbles buried after induction of neuropathic pain or naive 1 hour after s.c. treatment with mPD5 or PBS. n = 12 in each group. (D) Time spent in the paired compartment of SNI mice conditioned with 30 μmol/kg mPD5 or saline in the paired compartment. n = 11. (E) Recordings of ultrasonic vocalizations of SNI and naive mice at 37 kHz made for 60 minutes at baseline and 60–120 minutes after s.c. treatment with mPD5 or PBS. n = 6. (F) PWT before and after induction of neuropathic pain and s.c. treatment with mPD5 or PBS in PICK1-WT and -KO mice. Cross-sectional study ending up with n = 6 in each group. adm., administration; BL, baseline; D, day; inj., injection; NS, not significant; s.c., subcutaneous; SNI, spared nerve injury; USV, ultrasonic vocalizations. *P < 0.05; **P < 0.01; ***P < 0.001 by 2-way ANOVA with Dunnett’s post hoc test vs. 0 hours (B and F), 1-way ANOVA with Dunnett’s multiple-comparison test (C), unpaired, 2-tailed t test (D), or 1-way ANOVA with Dunnett’s post hoc test of SNI-PBS vs. the other 2 groups at baseline and after treatment (E). In B and F, the dashed line indicates the contralateral paw.