Hematopoietic pannexin 1 function is critical for neuropathic pain

Janelle L. Weaver; Sanja Arandjelovic; Gregory Brown; Suresh K. Mendu; Michael S. Schappe; Monica W. Buckley; Yu Hsin Chiu; Shaofang Shu; Jin K. Kim; Joyce Chung; Julia Krupa; Vesna Jevtovic-Todorovic; Bimal N. Desai; Kodi S. Ravichandran; Douglas A. Bayliss

doi:10.1038/srep42550

Hematopoietic pannexin 1 function is critical for neuropathic pain

Janelle L. Weaver, Sanja Arandjelovic, Gregory Brown, Suresh K. Mendu, Michael S. Schappe, Monica W. Buckley, Yu Hsin Chiu, Shaofang Shu, Jin K. Kim, Joyce Chung, Julia Krupa, Vesna Jevtovic-Todorovic, Bimal N. Desai, Kodi S. Ravichandran, Douglas A. Bayliss

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48 Scopus citations

Abstract

Neuropathic pain symptoms respond poorly to available therapeutics, with most treated patients reporting unrelieved pain and significant impairment in daily life. Here, we show that Pannexin 1 (Panx1) in hematopoietic cells is required for pain-like responses following nerve injury in mice, and a potential therapeutic target. Panx1 knockout mice (Panx1^-/-) were protected from hypersensitivity in two sciatic nerve injury models. Bone marrow transplantation studies show that expression of functional Panx1 in hematopoietic cells is necessary for mechanical hypersensitivity following nerve injury. Reconstitution of irradiated Panx1 knockout mice with hematopoietic Panx1^-/- cells engineered to re-express Panx1 was sufficient to recover hypersensitivity after nerve injury; this rescue required expression of a Panx1 variant that can be activated by G protein-coupled receptors (GPCRs). Finally, chemically distinct Panx1 inhibitors blocked development of nerve injury-induced hypersensitivity and partially relieved this hypersensitivity after it was established. These studies indicate that Panx1 expressed in immune cells is critical for pain-like effects following nerve injury in mice, perhaps via a GPCR-mediated activation mechanism, and suggest that inhibition of Panx1 may be useful in treating neuropathic pain.

Original language	English
Article number	42550
Journal	Scientific reports
Volume	7
DOIs	https://doi.org/10.1038/srep42550
State	Published - Feb 14 2017

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title = "Hematopoietic pannexin 1 function is critical for neuropathic pain",

abstract = "Neuropathic pain symptoms respond poorly to available therapeutics, with most treated patients reporting unrelieved pain and significant impairment in daily life. Here, we show that Pannexin 1 (Panx1) in hematopoietic cells is required for pain-like responses following nerve injury in mice, and a potential therapeutic target. Panx1 knockout mice (Panx1-/-) were protected from hypersensitivity in two sciatic nerve injury models. Bone marrow transplantation studies show that expression of functional Panx1 in hematopoietic cells is necessary for mechanical hypersensitivity following nerve injury. Reconstitution of irradiated Panx1 knockout mice with hematopoietic Panx1-/- cells engineered to re-express Panx1 was sufficient to recover hypersensitivity after nerve injury; this rescue required expression of a Panx1 variant that can be activated by G protein-coupled receptors (GPCRs). Finally, chemically distinct Panx1 inhibitors blocked development of nerve injury-induced hypersensitivity and partially relieved this hypersensitivity after it was established. These studies indicate that Panx1 expressed in immune cells is critical for pain-like effects following nerve injury in mice, perhaps via a GPCR-mediated activation mechanism, and suggest that inhibition of Panx1 may be useful in treating neuropathic pain.",

author = "Weaver, {Janelle L.} and Sanja Arandjelovic and Gregory Brown and Mendu, {Suresh K.} and Schappe, {Michael S.} and Buckley, {Monica W.} and Chiu, {Yu Hsin} and Shaofang Shu and Kim, {Jin K.} and Joyce Chung and Julia Krupa and Vesna Jevtovic-Todorovic and Desai, {Bimal N.} and Ravichandran, {Kodi S.} and Bayliss, {Douglas A.}",

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year = "2017",

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doi = "10.1038/srep42550",

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AU - Weaver, Janelle L.

AU - Arandjelovic, Sanja

AU - Brown, Gregory

AU - Mendu, Suresh K.

AU - Schappe, Michael S.

AU - Buckley, Monica W.

AU - Chiu, Yu Hsin

AU - Shu, Shaofang

AU - Kim, Jin K.

AU - Chung, Joyce

AU - Krupa, Julia

AU - Jevtovic-Todorovic, Vesna

AU - Desai, Bimal N.

AU - Ravichandran, Kodi S.

AU - Bayliss, Douglas A.

PY - 2017/2/14

Y1 - 2017/2/14

N2 - Neuropathic pain symptoms respond poorly to available therapeutics, with most treated patients reporting unrelieved pain and significant impairment in daily life. Here, we show that Pannexin 1 (Panx1) in hematopoietic cells is required for pain-like responses following nerve injury in mice, and a potential therapeutic target. Panx1 knockout mice (Panx1-/-) were protected from hypersensitivity in two sciatic nerve injury models. Bone marrow transplantation studies show that expression of functional Panx1 in hematopoietic cells is necessary for mechanical hypersensitivity following nerve injury. Reconstitution of irradiated Panx1 knockout mice with hematopoietic Panx1-/- cells engineered to re-express Panx1 was sufficient to recover hypersensitivity after nerve injury; this rescue required expression of a Panx1 variant that can be activated by G protein-coupled receptors (GPCRs). Finally, chemically distinct Panx1 inhibitors blocked development of nerve injury-induced hypersensitivity and partially relieved this hypersensitivity after it was established. These studies indicate that Panx1 expressed in immune cells is critical for pain-like effects following nerve injury in mice, perhaps via a GPCR-mediated activation mechanism, and suggest that inhibition of Panx1 may be useful in treating neuropathic pain.

AB - Neuropathic pain symptoms respond poorly to available therapeutics, with most treated patients reporting unrelieved pain and significant impairment in daily life. Here, we show that Pannexin 1 (Panx1) in hematopoietic cells is required for pain-like responses following nerve injury in mice, and a potential therapeutic target. Panx1 knockout mice (Panx1-/-) were protected from hypersensitivity in two sciatic nerve injury models. Bone marrow transplantation studies show that expression of functional Panx1 in hematopoietic cells is necessary for mechanical hypersensitivity following nerve injury. Reconstitution of irradiated Panx1 knockout mice with hematopoietic Panx1-/- cells engineered to re-express Panx1 was sufficient to recover hypersensitivity after nerve injury; this rescue required expression of a Panx1 variant that can be activated by G protein-coupled receptors (GPCRs). Finally, chemically distinct Panx1 inhibitors blocked development of nerve injury-induced hypersensitivity and partially relieved this hypersensitivity after it was established. These studies indicate that Panx1 expressed in immune cells is critical for pain-like effects following nerve injury in mice, perhaps via a GPCR-mediated activation mechanism, and suggest that inhibition of Panx1 may be useful in treating neuropathic pain.

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Hematopoietic pannexin 1 function is critical for neuropathic pain

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