AI Article Synopsis

  • The study examined the impact of the DRD2 gene variation on thermal pain sensitivity and the effectiveness of rTMS treatment in both healthy individuals and neuropathic pain patients.
  • The DRD2 957C>T variant was found to affect pain detection thresholds and rTMS analgesic effects, with 957TT homozygotes experiencing the lowest thresholds and highest response to rTMS.
  • In patients, the 957TT genotype was linked to more severe pain and a higher prevalence compared to a healthy population, highlighting the significant role of the dopamine system in pain management and potential personalized treatment options.

Article Abstract

We tested whether variation of the dopamine D2 receptor (DRD2) gene contributes to individual differences in thermal pain sensitivity and analgesic efficacy of repetitive transcranial magnetic stimulation (rTMS) in healthy subjects (n=29) or susceptibility to neuropathic pain in patients with neurophysiologically confirmed diagnosis (n=16). Thermal sensitivity of healthy subjects was assessed before and after navigated rTMS provided to the S1/M1 cortex. All subjects were genotyped for the DRD2 gene 957C>T and catechol-O-methyltransferase (COMT) protein Val158Met polymorphisms. In healthy subjects, 957C>T influenced both innocuous and noxious thermal detection thresholds that were lowest in 957TT homozygotes (P values from .0277 to .0462). rTMS to S1 cortex had analgesic effect only in 957TT homozygote genotype (P=.0086). In patients, prevalence of 957TT homozygote genotype was higher than in a healthy Finnish population (50% vs 27%; P=.0191). Patients with 957TT genotype reported more severe pain than patients with other genotypes (P=.0351). COMT Val158Met polymorphism was not independently associated with the studied variables. Genetic regulation of DRD2 function by 957C>T polymorphism thus seems to influence thermal and pain sensitivity, its modulation by rTMS, and susceptibility to neuropathic pain. This indicates a central role for the dopamine system and DRD2 in pain and analgesia. This may have clinical implications regarding individualized selection of patients for rTMS treatment and assessment of risks for neuropathic pain.

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Source
http://dx.doi.org/10.1016/j.pain.2014.08.029DOI Listing

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