Association between human opioid receptor genes polymorphisms and pressure pain sensitivity in females*

Huang, Chia-Yu; Liu, Hsin‐Fu; Su, Ning; Hsu, Yu Wen; Yang, Chen-Cheng; Chen, C.-C.; Tsai, Pei-Chien

doi:10.1111/j.1365-2044.2008.05760.x

Cited by 48 publications

(40 citation statements)

References 27 publications

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“…Hardy's little letter [4] offers insight into the data presented by Huang et al [1]. Such studies will soon -properlybecome commonplace in our clinical anaesthetic literature.…”

Section: Resultsmentioning

confidence: 99%

“…The human population is assumed both relatively large and stable, but allele frequencies may differ across ethnic groups (a point made by Huang et al [1]) [7]. Hardy's Law also assumes near-random mating of roughly equal males and females within a population, so enforced mating of animals or selectively altering the male:female ratio will cause allele proportions to deviate from those predicted by Hardy's Law.…”

mentioning

confidence: 99%

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‘Hardy’s Law’ and genomics in Anaesthesia

Pandit

2008

Anaesthesia

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“…Hardy's little letter [4] offers insight into the data presented by Huang et al [1]. Such studies will soon -properlybecome commonplace in our clinical anaesthetic literature.…”

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

‘Hardy’s Law’ and genomics in Anaesthesia

Pandit

2008

Anaesthesia

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“…24 In our study there was no association between either experimental heat or cold pain sensitivity and the 118A>G polymorphism in agreement with Huang and co-workers. 12 It is not surprising that the fairly low intensity stimulation with 48°C for 5 s did not show any association with the polymorphism. However, one would have expected an association in the cold pain test, which is very unpleasant and could activate stress-induced analgesia which is at least partly mediated by the endogenous opioid system.…”

Section: Experimental Painmentioning

confidence: 97%

How Much Oxycodone Is Needed for Adequate Analgesia After Breast Cancer Surgery: Effect of the OPRM1 118A>G Polymorphism

Cajanus

Kaunisto

Tallgren

et al. 2014

The Journal of Pain

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“…Opioid gene signaling is a critical link in a number of human behavioral responses [reviewed in Sonetti et al, 2005;Bodnar, 2009;Stein and Zollner, 2009], as well as in many human disease susceptibilities [Kreek, 1996a;Ogden et al, 2004;Kreek et al, 2005;Drakenberg et al, 2006;Kennedy et al, 2006;Xuei et al, 2006Xuei et al, , 2007Huang et al, 2008;Nikoshkov et al, 2008;Bodnar, 2009]. Several studies have presented evidence of functional changes that have occurred in the coding sequences of these genes, both across vertebrate evolution [Dores et al, 2002;Stevens et al, 2007;Dreborg et al, 2008] and within human populations (e.g.…”

Section: Discussionmentioning

confidence: 99%

“…The primary and secondary binding affinities of these ligands and receptors are illustrated in figure 1 [Chen et al, 1993a;Meng et al, 1996;Gong et al, 1998;Zaveri et al, 2001;Snook et al, 2008;Liu et al, 2009]. Most investigations surrounding this gene family have focused on the role its members play in pain and nocicep-155 tion [reviewed in Stein and Zollner, 2009], stress response [Sonetti et al, 2005], behavior [reviewed in Bodnar, 2009], substance abuse [Kreek, 1996;Kreek et al, 2005;Drakenberg et al, 2006;Xuei et al, 2006Xuei et al, , 2007Huang et al, 2008;Nikoshkov et al, 2008], and some psychiatric affective disorders [reviewed in Ogden et al, 2004;Kennedy et al, 2006;Bodnar, 2009].…”

Section: Introductionmentioning

confidence: 99%

Extensive Changes in the Expression of the Opioid Genes between Humans and Chimpanzees

Cruz‐Gordillo

Fédrigo²,

Wray³

et al. 2010

Brain Behav Evol

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The various means by which the body perceives, transmits, and resolves the experiences of pain and nociception are mediated by a host of molecules, including neuropeptides within the opioid gene signaling pathway. The peptide ligands and receptors encoded by this group of genes have been linked to behavioral disorders as well as a number of psychiatric affective disorders. Our aim was to explore the recent evolutionary history of these two gene families by taking a comparative genomics approach, specifically through a comparison between humans and chimpanzees. Our analyses indicate differential expression of these genes between the two species, more than expected based on genome-wide comparisons, indicating that differential expression is pervasive among the opioid genes. Of the 8 family members, three genes showed significant expression differences (PENK, PNOC, and OPRL1), with two others marginally significant (OPRM1 and OPRD1). Accelerated substitution rates along human and chimpanzee lineages within the putative regulatory regions of OPRM1, POMC, and PDYN between the human and chimpanzee branches are consistent with positive selection. Collectively, these results suggest that there may have been a selective advantage to modulating the expression of the opioid genes in humans compared with our closest living relatives. Information about the cognitive roles mediated by these genes in humans may help to elucidate the trait consequences of these putatively adaptive expression changes.

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Association between human opioid receptor genes polymorphisms and pressure pain sensitivity in females*

Cited by 48 publications

References 27 publications

‘Hardy’s Law’ and genomics in Anaesthesia

‘Hardy’s Law’ and genomics in Anaesthesia

How Much Oxycodone Is Needed for Adequate Analgesia After Breast Cancer Surgery: Effect of the OPRM1 118A>G Polymorphism

Extensive Changes in the Expression of the Opioid Genes between Humans and Chimpanzees

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