Long-term male-specific chronic pain via telomere- and p53‑mediated spinal cord cellular senescence
Arjun Muralidharan, … , Alfredo Ribeiro-da-Silva, Jeffrey S. Mogil
Arjun Muralidharan, … , Alfredo Ribeiro-da-Silva, Jeffrey S. Mogil
Published April 15, 2022
Citation Information: J Clin Invest. 2022;132(8):e151817. https://doi.org/10.1172/JCI151817.
View: Text | PDF
Research Article Neuroscience

Long-term male-specific chronic pain via telomere- and p53‑mediated spinal cord cellular senescence

Abstract

Mice with experimental nerve damage can display long‑lasting neuropathic pain behavior. We show here that 4 months and later after nerve injury, male but not female mice displayed telomere length (TL) reduction and p53‑mediated cellular senescence in the spinal cord, resulting in maintenance of pain and associated with decreased lifespan. Nerve injury increased the number of p53‑positive spinal cord neurons, astrocytes, and microglia, but only in microglia was the increase male‑specific, matching a robust sex specificity of TL reduction in this cell type, which has been previously implicated in male‑specific pain processing. Pain hypersensitivity was reversed by repeated intrathecal administration of a p53‑specific senolytic peptide, only in male mice and only many months after injury. Analysis of UK Biobank data revealed sex-specific relevance of this pathway in humans, featuring male‑specific genetic association of the human p53 locus (TP53) with chronic pain and a male-specific effect of chronic pain on mortality. Our findings demonstrate the existence of a biological mechanism maintaining pain behavior, at least in males, occurring much later than the time span of virtually all extant preclinical studies.

Authors

Arjun Muralidharan, Susana G. Sotocinal, Noosha Yousefpour, Nur Akkurt, Lucas V. Lima, Shannon Tansley, Marc Parisien, Chengyang Wang, Jean-Sebastien Austin, Boram Ham, Gabrielle M.G.S. Dutra, Philippe Rousseau, Sioui Maldonado-Bouchard, Teleri Clark, Sarah F. Rosen, Mariam R. Majeed, Olivia Silva, Rachel Nejade, Xinyu Li, Stephania Donayre Pimentel, Christopher S. Nielsen, G. Gregory Neely, Chantal Autexier, Luda Diatchenko, Alfredo Ribeiro-da-Silva, Jeffrey S. Mogil

×

Figure 2

Pain and mortality phenotype of Terc-null mutant mice.

Options: View larger image (or click on image) Download as PowerPoint
Pain and mortality phenotype of Terc-null mutant mice. (A) Confirmation ...
(A) Confirmation of reduced PBMC TL in mice lacking 1 or 2 copies of the Terc gene. Bars represent mean ± SEM TL measured in kb/diploid genome; n = 8–10 mice per genotype. (B) Increased mechanical allodynia in the ipsilateral hind paw after SNI in Terc–/– mice. Symbols represent mean ± SEM change (Δ) in withdrawal thresholds (g) of the ipsilateral hind paw at each time point compared with baseline thresholds; n = 8–11 mice per genotype. (CE) Kaplan-Meier survival curves of +/+ (C), +/– (D), and –/– (E) mice given sham or SNI surgeries at 2 months of age and left undisturbed (except for behavioral testing at time points shown in B) in their same-sex, same‑genotype home cages until death. *P < 0.05, **P < 0.01, ***P < 0.001 compared with corresponding sham group, +/+ genotype (within surgical condition), or as indicated, via 1-way ANOVA or log-rank test.