Senolytic treatment for low back pain

Matthew Mannarino; Hosni Cherif; Saber Ghazizadeh; Oliver Wu Martinez; Kai Sheng; Elsa Cousineau; Seunghwan Lee; Magali Millecamps; Chan Gao; Alice Gilbert; Cedric Peirs; Reza Sharif Naeini; Jean A. Ouellet; Laura S. Stone; Lisbet Haglund

doi:10.1126/sciadv.adr1719

Senolytic treatment for low back pain

Matthew Mannarino
, Hosni Cherif
, Saber Ghazizadeh
, Oliver Wu Martinez
, Kai Sheng
, Elsa Cousineau
, Seunghwan Lee
, Magali Millecamps
, Chan Gao
, Alice Gilbert
, Cedric Peirs
, Reza Sharif Naeini
, Jean A. Ouellet
, Laura S. Stone
, Lisbet Haglund

Anesthesiology

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Senescent cells (SnCs) accumulate because of aging and external cellular stress throughout the body. They adopt a senescence-associated secretory phenotype (SASP) and release inflammatory and degenerative factors that actively contribute to age-related diseases, such as low back pain (LBP). The senolytics, o-vanillin and RG-7112, remove SnCs in human intervertebral discs (IVDs) and reduce SASP release, but it is unknown whether they can treat LBP. sparc^−/− mice, with LBP, were treated orally with o-vanillin and RG-7112 as single or combination treatments. Treatment reduced LBP and SASP factor release and removed SnCs from the IVD and spinal cord. Treatment also lowered degeneration scores in the IVDs, improved vertebral bone quality, and reduced the expression of pain markers in the spinal cord. Together, our data suggest RG-7112 and o-vanillin as potential disease-modifying drugs for LBP and other painful disorders linked to cell senescence.

Original language	English (US)
Article number	eadr1719
Journal	Science Advances
Volume	11
Issue number	11
DOIs	https://doi.org/10.1126/sciadv.adr1719
State	Published - Mar 14 2025

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Copyright © 2025 The Authors, some rights reserved

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title = "Senolytic treatment for low back pain",

abstract = "Senescent cells (SnCs) accumulate because of aging and external cellular stress throughout the body. They adopt a senescence-associated secretory phenotype (SASP) and release inflammatory and degenerative factors that actively contribute to age-related diseases, such as low back pain (LBP). The senolytics, o-vanillin and RG-7112, remove SnCs in human intervertebral discs (IVDs) and reduce SASP release, but it is unknown whether they can treat LBP. sparc−/− mice, with LBP, were treated orally with o-vanillin and RG-7112 as single or combination treatments. Treatment reduced LBP and SASP factor release and removed SnCs from the IVD and spinal cord. Treatment also lowered degeneration scores in the IVDs, improved vertebral bone quality, and reduced the expression of pain markers in the spinal cord. Together, our data suggest RG-7112 and o-vanillin as potential disease-modifying drugs for LBP and other painful disorders linked to cell senescence.",

author = "Matthew Mannarino and Hosni Cherif and Saber Ghazizadeh and Martinez, \{Oliver Wu\} and Kai Sheng and Elsa Cousineau and Seunghwan Lee and Magali Millecamps and Chan Gao and Alice Gilbert and Cedric Peirs and Naeini, \{Reza Sharif\} and Ouellet, \{Jean A.\} and Stone, \{Laura S.\} and Lisbet Haglund",

note = "Publisher Copyright: Copyright {\textcopyright} 2025 The Authors, some rights reserved",

year = "2025",

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doi = "10.1126/sciadv.adr1719",

language = "English (US)",

volume = "11",

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AU - Mannarino, Matthew

AU - Cherif, Hosni

AU - Ghazizadeh, Saber

AU - Martinez, Oliver Wu

AU - Sheng, Kai

AU - Cousineau, Elsa

AU - Lee, Seunghwan

AU - Millecamps, Magali

AU - Gao, Chan

AU - Gilbert, Alice

AU - Peirs, Cedric

AU - Naeini, Reza Sharif

AU - Ouellet, Jean A.

AU - Stone, Laura S.

AU - Haglund, Lisbet

PY - 2025/3/14

Y1 - 2025/3/14

N2 - Senescent cells (SnCs) accumulate because of aging and external cellular stress throughout the body. They adopt a senescence-associated secretory phenotype (SASP) and release inflammatory and degenerative factors that actively contribute to age-related diseases, such as low back pain (LBP). The senolytics, o-vanillin and RG-7112, remove SnCs in human intervertebral discs (IVDs) and reduce SASP release, but it is unknown whether they can treat LBP. sparc−/− mice, with LBP, were treated orally with o-vanillin and RG-7112 as single or combination treatments. Treatment reduced LBP and SASP factor release and removed SnCs from the IVD and spinal cord. Treatment also lowered degeneration scores in the IVDs, improved vertebral bone quality, and reduced the expression of pain markers in the spinal cord. Together, our data suggest RG-7112 and o-vanillin as potential disease-modifying drugs for LBP and other painful disorders linked to cell senescence.

AB - Senescent cells (SnCs) accumulate because of aging and external cellular stress throughout the body. They adopt a senescence-associated secretory phenotype (SASP) and release inflammatory and degenerative factors that actively contribute to age-related diseases, such as low back pain (LBP). The senolytics, o-vanillin and RG-7112, remove SnCs in human intervertebral discs (IVDs) and reduce SASP release, but it is unknown whether they can treat LBP. sparc−/− mice, with LBP, were treated orally with o-vanillin and RG-7112 as single or combination treatments. Treatment reduced LBP and SASP factor release and removed SnCs from the IVD and spinal cord. Treatment also lowered degeneration scores in the IVDs, improved vertebral bone quality, and reduced the expression of pain markers in the spinal cord. Together, our data suggest RG-7112 and o-vanillin as potential disease-modifying drugs for LBP and other painful disorders linked to cell senescence.

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DO - 10.1126/sciadv.adr1719

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AN - SCOPUS:105000237431

SN - 2375-2548

VL - 11

JO - Science Advances

JF - Science Advances

IS - 11

M1 - eadr1719

ER -

Senolytic treatment for low back pain

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