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

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

doi:10.1172/jci.insight.170976

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

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 ArlethAnne Marie Heegaard, Andreas Toft Sørensen, Kenneth Lindegaard Madsen

^*Corresponding author for this work

Research output: Contribution to journal › Journal article › Research › peer-review

31 Downloads (Pure)

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.

Original language	English
Article number	e170976
Journal	JCI insight
Volume	9
Issue number	20
Number of pages	19
ISSN	2379-3708
DOIs	https://doi.org/10.1172/jci.insight.170976
Publication status	Published - 2024

Bibliographical note

Publisher Copyright:
: © 2024, Jensen et al.

Access to Document

10.1172/jci.insight.170976Licence: CC BY

FulltextFinal published version, 27.1 MBLicence: CC BY

Cite this

Jensen, K. L., Riis Christensen, N., Goddard, C. M., Jager, S. E., Noes-Holt, G., Kanneworff, I. B., Jakobsen, A., Jiménez-Fernández, L., Peck, E. G., Sivertsen, L., Baro, R. C., Houser, G. A., Mayer, F. P., Diaz-DelCastillo, M., Topp, M. L., Hopkins, C., Thomsen, C. D., Soltan, A. B. I., Tidemand, F. G., ... Madsen, K. L. (2024). Peripherally restricted PICK1 inhibitor mPD5 ameliorates pain behaviors in murine inflammatory and neuropathic pain models. JCI insight, 9(20), Article e170976. https://doi.org/10.1172/jci.insight.170976

Jensen, KL, Riis Christensen, N, Goddard, CM , Jager, SE , Noes-Holt, G , Kanneworff, IB, Jakobsen, A, Jiménez-Fernández, L, Peck, EG, Sivertsen, L, Baro, RC , Houser, GA, Mayer, FP, Diaz-DelCastillo, M, Topp, ML, Hopkins, C, Thomsen, CD, Soltan, ABI, Tidemand, FG , Arleth, L , Heegaard, AM , Sørensen, AT & Madsen, KL 2024, 'Peripherally restricted PICK1 inhibitor mPD5 ameliorates pain behaviors in murine inflammatory and neuropathic pain models', JCI insight, vol. 9, no. 20, e170976. https://doi.org/10.1172/jci.insight.170976

@article{284e6788c3a6498f8ba37199c3bc8a41,

title = "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.",

author = "Jensen, {Kathrine Louise} and {Riis Christensen}, Nikolaj and Goddard, {Carolyn Marie} and Jager, {Sara Elgaard} and Gith Noes-Holt and Kanneworff, {Ida Buur} and Alexander Jakobsen and Luc{\'i}a Jim{\'e}nez-Fern{\'a}ndez and Peck, {Emily G.} and Line Sivertsen and Baro, {Raquel Comaposada} and Houser, {Grace Anne} and Mayer, {Felix Paul} and Marta Diaz-DelCastillo and Topp, {Marie L{\o}th} and Chelsea Hopkins and Thomsen, {Cecilie Dubgaard} and Soltan, {Ahmed Barakat Ibrahim} and Tidemand, {Frederik Gr{\o}nb{\ae}k} and Lise Arleth and Heegaard, {Anne Marie} and S{\o}rensen, {Andreas Toft} and Madsen, {Kenneth Lindegaard}",

note = "Publisher Copyright: : {\textcopyright} 2024, Jensen et al.",

year = "2024",

doi = "10.1172/jci.insight.170976",

language = "English",

volume = "9",

journal = "JCI insight",

issn = "2379-3708",

publisher = "American Society for Clinical Investigation",

number = "20",

}

TY - JOUR

T1 - Peripherally restricted PICK1 inhibitor mPD5 ameliorates pain behaviors in murine inflammatory and neuropathic pain models

AU - Jensen, Kathrine Louise

AU - Riis Christensen, Nikolaj

AU - Goddard, Carolyn Marie

AU - Jager, Sara Elgaard

AU - Noes-Holt, Gith

AU - Kanneworff, Ida Buur

AU - Jakobsen, Alexander

AU - Jiménez-Fernández, Lucía

AU - Peck, Emily G.

AU - Sivertsen, Line

AU - Baro, Raquel Comaposada

AU - Houser, Grace Anne

AU - Mayer, Felix Paul

AU - Diaz-DelCastillo, Marta

AU - Topp, Marie Løth

AU - Hopkins, Chelsea

AU - Thomsen, Cecilie Dubgaard

AU - Soltan, Ahmed Barakat Ibrahim

AU - Tidemand, Frederik Grønbæk

AU - Arleth, Lise

AU - Heegaard, Anne Marie

AU - Sørensen, Andreas Toft

AU - Madsen, Kenneth Lindegaard

PY - 2024

Y1 - 2024

N2 - 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.

AB - 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.

U2 - 10.1172/jci.insight.170976

DO - 10.1172/jci.insight.170976

M3 - Journal article

C2 - 39287978

AN - SCOPUS:85207254369

SN - 2379-3708

VL - 9

JO - JCI insight

JF - JCI insight

IS - 20

M1 - e170976

ER -