Genetic risk shared across 24 chronic pain conditions: identification and characterization with genomic structural equation modeling

Zorina-Lichtenwalter, Katerina; Bango, Carmen I.; Oudenhove, Lukas Van; Čeko, Marta; Lindquist, Martin A.; Grotzinger, Andrew D.; Keller, Matthew C.; Friedman, Naomi P.; Wager, Tor D.

doi:10.1097/j.pain.0000000000002922

Cited by 12 publications

(5 citation statements)

References 116 publications

(177 reference statements)

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“…A longitudinal, psychometric analysis has supported the validity of a common component underlying pain across body sites (Battaglia et al, 2022). Consistent with this psychometric evidence for a general pain factor, twin and genome-wide association studies have identified a common genetic factor that contributes to many chronic pain conditions (Vehof et al, 2014;Zorina-Lichtenwalter et al, 2023). Of the people who reported pain in our sample, 97.2% reported pain lasting more than 3 months, characterizing the measure as chronic.…”

Section: Brief Pain History Questionnairesupporting

confidence: 78%

Familial effects account for association between chronic pain and past month smoking

Rader,

Reineberg,

Petre

et al. 2024

European Journal of Pain

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BackgroundSmoking is associated with chronic pain, but it is not established whether smoking causes pain or if the link is due to familial effects. One proposed mechanism is that smoking strengthens maladaptive cortico‐striatal connectivity, which contributes to pain chronification. We leveraged a twin design to assess direct effects of smoking on pain controlling for familial confounds, and whether cortico‐striatal connectivity mediates this association.MethodsIn a population‐based sample of 692 twins (age = 28.83 years), we assessed past‐month smoking frequency (n = 132 used in the past month), presence and severity of a current pain episode (n = 179 yes), and resting‐state functional connectivity of the nucleus accumbens and medial prefrontal cortex (NAc‐mPFC).ResultsSmoking was significantly associated with pain, but the association was not significantly mediated by NAc‐mPFC connectivity. In a co‐twin control model, smoking predicted which families had more pain but could not distinguish pain between family members. Pain risk was 43% due to additive genetic (A) and 57% due to non‐shared environmental (E) influences. Past‐month smoking frequency was 71% genetic and 29% non‐shared environmental. Smoking and pain significantly correlated phenotypically (r = 0.21, p = 0.001) and genetically (rg = 0.51, p < 0.001), but not environmentally (re = −0.18, p = 0.339).ConclusionsPain and smoking are associated; however, the association appears to reflect shared familial risk factors, such as genetic risk, rather than being causal in nature. The connectivity strength of the reward pathway was not related to concurrent pain and smoking in this sample.SignificanceSmoking does not appear to directly cause chronic pain; rather, there may be shared biopsychosocial risk factors, including genetic influences, that explain their association. These findings can be integrated into future research to identify shared biological pathways of both chronic pain and smoking behaviours as a way to conceptualize pain chronification.

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Section: Brief Pain History Questionnairesupporting

confidence: 78%

Familial effects account for association between chronic pain and past month smoking

Rader,

Reineberg,

Petre

et al. 2024

European Journal of Pain

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“…Variants associated with drinks per week, schizophrenia, smoking initiation, and bipolar disorder were mapped to synaptosome associated protein 91 (SNAP91). The chromosome 17 Pehlq1 interval maps to regions on human chromosomes 5 (109.5-110.7Mb) and 18 (2.57-8.83; 9.10-9.96Mb), and it features variants associated with opioid analgesic sensitivity (DLGAP1)[41], schizophrenia (MAN2A1)[42], chronic pain (TMEM200C)[43], and post-traumatic stress disorder symptomatology (DLGAP1)[44].…”

Section: Resultsmentioning

confidence: 99%

Identification of ethanol analgesia quantitative trait loci and candidate genes in BXD recombinant inbred mouse lines

Rogers,

White,

Damaj

et al. 2024

Preprint

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Alcohol consumption produces acute analgesic effects, and people experiencing pain conditions may drink alcohol to alleviate discomfort. However, tolerance to the analgesic properties of alcohol could prompt escalating consumption and dependence. Both nociception and alcohol-induced analgesia are under significant genetic control. Understanding the genetic architecture of these processes could inform better treatment options for people with pain conditions. This study aims to identify quantitative trait loci (QTL) driving variation in ethanol-induced analgesia across BXD recombinant inbred mouse lines. Male and female mice from 62 BXD strains received ethanol or saline oral gavage for five days and were tested for hot plate (HP) latency at baseline, Day 1, and Day 5. QTL mapping of HP phenotypes identified a significant provisional QTL on chromosome 17 for Day 1 HP latency in mice receiving ethanol. An additional highly suggestive QTL was present on chromosome 9 for the difference in pre- and post-ethanol thermal nociception. Candidate genes within QTL support intervals were provisionally identified using HP phenotypic correlations to transcriptomic database, expression QTL analysis, and other bioinformatics inquiries. The combined behavioral and bioinformatic analyses yielded strong ethanol analgesia candidate genes, specificallyMyo6. Thus, the results of this genetic study of ethanol-induced analgesia in BXD mouse strains may contribute significantly to our understanding of the molecular basis for individual variation in the analgesic response to acute ethanol.

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“…Our study demonstrates an interplay of genetic determinants in the manifestation of pain, corroborating previous research. Specifically, a prior network analysis has identified a substantial cluster of conditions and pinpointed arthropathic, back, and neck pain as potential hubs for cross-condition chronic pain (Zorina-Lichtenwalter et al 2023).…”

Section: Discussionmentioning

confidence: 99%

A genome-wide association study identifies genetic variants associated with hip pain in the UK Biobank cohort (N=221,127)

Pan,

Cai,

Veluchamy

et al. 2023

Preprint

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Hip pain is a common musculoskeletal complaint that leads many people to seek medical attention. Approximately 14.3% of the population aged 60 and above have reported substantial hip pain persisting for the majority of days within a six-week duration. Our research aimed to identify the genetic variants associated with hip pain by conducting a genome-wide association study (GWAS) on the hip pain phenotype, utilizing data from 221,127 participants from the UK Biobank cohort. We found 7 different loci associated with hip pain, with the most significant SNP being rs77641763, which is situated within theEXD3gene (p value = 2.20 x 10^-13). We utilized publicly available summary statistics from a previous GWAS meta-analysis on hip osteoarthritis as a replication cohort. Two loci (rs12042579 and rs9597759) were suggestively replicated. Further analysis of tissue expression revealed significant associations between brain tissues and hip pain. Additionally, we found strong genetic correlations between hip pain and other pain phenotypes. This research has therefore identified multiple genetic loci associated with hip pain, which may potentially pave the way for medical interventions that can alleviate the burden of hip pain.

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Genetic risk shared across 24 chronic pain conditions: identification and characterization with genomic structural equation modeling

Cited by 12 publications

References 116 publications

Familial effects account for association between chronic pain and past month smoking

Familial effects account for association between chronic pain and past month smoking

Identification of ethanol analgesia quantitative trait loci and candidate genes in BXD recombinant inbred mouse lines

A genome-wide association study identifies genetic variants associated with hip pain in the UK Biobank cohort (N=221,127)

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