The Pace of Biological Aging Predicts Nonspecific Chronic Low Back Pain Severity

Edwin N Aroke; Vinodh Srinivasasainagendra; Pooja Kottae; Tammie L Quinn; Asia M Wiggins; Joanna Hobson; Kiari Kinnie; Tonya Stoudmire; Hemant K Tiwari; Burel R Goodin

doi:10.1016/j.jpain.2023.10.018

The Pace of Biological Aging Predicts Nonspecific Chronic Low Back Pain Severity

J Pain. 2024 Apr;25(4):974-983. doi: 10.1016/j.jpain.2023.10.018. Epub 2023 Oct 30.

Authors

Affiliations

¹ School of Nursing, University of Alabama at Birmingham, Birmingham, Alabama.
² Department of Biostatistics, School of Public Health, University of Alabama at Birmingham, Birmingham, Alabama.
³ Department of Computer Science, College of Arts and Sciences, University of Alabama at Birmingham, Birmingham, Alabama.
⁴ Department of Psychology, College of Arts and Sciences, University of Alabama at Birmingham, Birmingham, Alabama.
⁵ Department of Anesthesiology, School of Medicine, Washington University, St Louis, Missouri.

PMID: 37907115
PMCID: PMC10960701 (available on 2025-04-01)
DOI: 10.1016/j.jpain.2023.10.018

Abstract

This study aimed to determine if and how the pace of biological aging was associated with nonspecific chronic low back pain (cLBP) and compare what measure of epigenetic age acceleration most strongly predicts cLBP outcomes. We used the Dunedin Pace of Aging from the Epigenome (DunedinPACE), Horvath's, Hannum's, and PhenoAge clocks to determine the pace of biological aging in 69 cLBP, and 49 pain-free controls (PFCs) adults, ages 18 to 85 years. On average, participants with cLBP had higher DunedinPACE (P < .001) but lower Horvath (P = .04) and Hannum (P = .02) accelerated epigenetic age than PFCs. There was no significant difference in PhenoAge acceleration between the cLBP and PFC groups (P = .97). DunedinPACE had the largest effect size (Cohen's d = .78) on group differences. In univariate regressions, a unit increase in DunedinPACE score was associated with 265.98 times higher odds of cLBP than the PFC group (P < .001). After controlling for sex, race, and body mass index (BMI), the odds ratio of cLBP to PFC group was 149.62 (P < .001). Furthermore, among participants with cLBP, DunedinPACE scores positively correlated with pain severity (r_s = .385, P = .001) and interference (r_s = .338, P = .005). Epigenetic age acceleration from Horvath, Hannum, and PhenoAge clocks were not significant predictors of cLBP. The odds of a faster pace of biological aging are higher among adults with cLBP, and this was associated with greater pain severity and disability. Future interventions to slow the pace of biological aging may improve cLBP outcomes. PERSPECTIVE: Accelerated epigenetic aging is common among adults with nonspecific cLBP. Higher DunedinPACE scores positively correlate with pain severity and interference, and better predict cLBP than other DNA methylation clocks. Interventions to slow the pace of biological aging may be viable targets for improving pain outcomes.

Keywords: Dunedin Pace of Aging from the Epigenome (DunedinPACE); epigenetic age acceleration; epigenetic clocks; nonspecific chronic low back pain; pace of biological aging.

MeSH terms

Adult
Aging
DNA Methylation
Epigenesis, Genetic
Epigenome
Humans
Low Back Pain*
Odds Ratio

Abstract

MeSH terms

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