Pain sensitivity and vasopressin analgesia are mediated by a gene-sex-environment interaction

Mogil, Jeffrey S.; Sorge, Robert E.; LaCroix-Fralish, Michael L.; Smith, Shad B.; Fortin, Anny; Sotocinal, Susana G.; Ritchie, Judith A.; Austin, Jean-Sébastien; Schorscher-Petcu, Ara; Melmed, Kara; Czerminski, Jan T.; Bittong, Rosalie A.; Mokris, J. Brad; Neubert, John K.; Campbell, Claudia M.; Edwards, Robert R.; Campbell, James N.; Crawley, Jacqueline N.; Lariviere, William R.; Wallace, Margaret R.; Sternberg, Wendy F.; Balaban, Carey D.; Belfer, Inna; Fillingim, Roger B.

doi:10.1038/nn.2941

Cited by 111 publications

(109 citation statements)

References 39 publications

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“…As might be expected given this interaction, genes (quantitative trait loci) with sex-dependent effects on pain trait variability have been uncovered [38][39][40][41][42] . A recent study uncovered a three-way interaction in both mice and humans between sex, genetics (AVPR1A genotype (AVPR1A encodes the vasopressin 1A receptor)) and acute stress 43 . Recent mouse studies have revealed another surprising factor that interacts with sex to modulate pain: social interaction.…”

Section: Male Onlymentioning

confidence: 99%

“…The distinction between the latter two types can be considered the difference between 'quantitative' and 'qualitative' sex differences. Although attention has mostly been paid to documenting quantitative sex differences in pain, a growing number of examples of qualitative differences in pain have been reported 31,39,43,[53][54][55][56][57][58][59][60][61][62][63][64] , and these promise to be far more important in the long run. As a practical matter, analgesics are routinely titrated according to their effect, which will effectively mitigate any sex differences along with other sources of inter-individual variability.…”

Section: Male Onlymentioning

confidence: 99%

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Sex differences in pain and pain inhibition: multiple explanations of a controversial phenomenon

2012

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| A clear majority of patients with chronic pain are women; however, it has been surprisingly difficult to determine whether this sex bias corresponds to actual sex differences in pain sensitivity. A survey of the currently available epidemiological and laboratory data indicates that the evidence for clinical and experimental sex differences in pain is overwhelming. Various explanations for this phenomenon have been given, ranging from experiential and sociocultural differences in pain experience between men and women to hormonally and genetically driven sex differences in brain neurochemistry. PERSPECTIVES NATURE REVIEWS | NEUROSCIENCE VOLUME 13 | DECEMBER 2012 | 859

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Section: Male Onlymentioning

confidence: 99%

Section: Male Onlymentioning

confidence: 99%

Sex differences in pain and pain inhibition: multiple explanations of a controversial phenomenon

2012

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“…This same phenomenon was thereafter demonstrated in high-and low-autotomy mouse strains 126 . In one of our studies, a particularly robust strain difference in pain sensitivity 127 was found eventually to exist only because of SIA-resulting simply from being placed in the testing room itself-in one strain but not the other; if mice were habituated to the room on several days before testing no strain difference was observed 36 . These sorts of findings have led to a discussion as to whether reproducibility in animal experiments would be enhanced by standardization of husbandry and experimental parameters across laboratories 128 .…”

Section: The Impact Of Laboratory Environmental Factorsmentioning

confidence: 55%

“…Also unappreciated is the fact that stress associated with pain testing can be surprisingly high (and hugely variable) in human participants as well. In a study of capsaicin pain, self-reported stress levels ranged from 0 to 8 on a 0-to-10-point scale, and this stress interacted with both sex and a genetic variant within the AVPR1A gene to significantly affect pain ratings 36 . Some laboratory stressors (or non-stressful modulatory factors) are related to husbandry, and have long been known.…”

Section: Jeffrey S Mogilmentioning

confidence: 99%

Laboratory environmental factors and pain behavior: the relevance of unknown unknowns to reproducibility and translation

Mogil

2017

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“…The vasopressin receptor has been linked to strain-dependent pain sensitivity to formalin and capsaicin 266 and oxytocin activation ameliorates visceral pain in particular 267 .…”

Section: Functional Vasopressin Receptors Were Absent From All Cell Lmentioning

confidence: 99%

A pharmacological and transcriptomic approach to exploring novel pain targets

Yin¹

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Ever since the discovery that mutations in the voltage-gated sodium channel 1.7 protein are responsible for human congenital insensitivity to pain, the voltage-gated sodium channel (Na V ) family of ion channels has been the subject of intense research with the hope of discovering novel analgesics. We now know that Na V 1.7 deletion in select neuronal populations yield different phenotypes, with the deletion of Na V 1.7 in all sensory neurons being successful at abolishing mechanical and heat-induced pain. However, it is rapidly becoming apparent that a number of pain syndromes are not modulated by Na V 1.7 at all, such as oxaliplatin-mediated neuropathy. It is particularly interesting to note that the loss of Na V 1.7 function is also associated with the selective inhibition of pain mediated by specific stimuli, such as that observed in burn-induced pain where Na V 1.7 gene knockout abolished thermal allodynia but did not affect mechanical allodynia. Accordingly, significant interests exist in delineating the contribution of other Na V isoforms in modality-specific pain pathways. Two other isoforms, Na V 1.6 and Na V 1.8, are now specifically implicated in some Na V 1.7-independent conditions such as oxaliplatin-induced cold allodynia. Such selective contributions of specific ion channel isoforms to pain highlight the need to discover other putative protein targets involved in mediating nociception.The aim of my work is therefore to discover selective molecular inhibitors of Na V 1.6 and Na V 1.8, to find useful cell models for peripheral nociceptors, to investigate the roles of Na V 1.6 and Na V 1.8 in an animal model of burn-induced pain, and to screen for putative new targets for analgesia in burn-related pain.Chapter 2 of this thesis describes activity-guided discovery of novel Na V 1.6 and Na V 1.8-modulting peptides from crude spider venoms. Crude venom from Poecilotheria metallica successfully reduced Na V 1.8-mediated voltage changes in HEK293-expressing cells. A new Na V 1.8-inhibitory peptide was sequenced from the venom and named Pme1a. However, Pme1a exhibited TRPV1 agonist activity and induced nocifensive behaviours, such as paw licking, after injection into the hind paws of mice, indicating the peptide was not a selective Na V 1.8 modulator and was unsuitable as a tool for Na V 1.8 investigation.iii With the unsuccessful exploration of spider venoms for new specific inhibitors, I then investigated in vitro cell models as tools to research specific nociceptor subtypes that express Na V 1.6 or Na V 1.8. In Chapter 3, I provide the first complete transcriptome of three common in vitro neuronal cell lines (SH-SY5Y, F-11, and ND7/23) to examine whether they were appropriate for investigating the functions of Na V 1.6 and Na V 1.8, and to identify if the cell lines resemble in vivo dorsal root ganglion (DRG) neuronal subclasses. The three cell lines examined all expressed proteins belonging to similar pathways and of similar proportions to native DRG neurons. However, they did not express any ce...

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Pain sensitivity and vasopressin analgesia are mediated by a gene-sex-environment interaction

Cited by 111 publications

References 39 publications

Sex differences in pain and pain inhibition: multiple explanations of a controversial phenomenon

Sex differences in pain and pain inhibition: multiple explanations of a controversial phenomenon

Laboratory environmental factors and pain behavior: the relevance of unknown unknowns to reproducibility and translation

A pharmacological and transcriptomic approach to exploring novel pain targets

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