Sex differences underlying orofacial varicella zoster associated pain in rats

Varicella zoster virus (VZV) is a human herpesvirus that infects a majority of the unvaccinated population worldwide. While recovery from varicella “chickenpox” occurs with lifelong immunity the virus persists in a latent state in the nuclei of neurons within sensory and autonomic ganglia across the entire neuro-axis. VZV chromatin remains in the infected cells (extrachromosomal) but viral protein expression and virus production remain repressed [1‐4]. However, reactivation from latency occurs in about one third of VZV positive individuals to cause herpes zoster (HZ), with the incidence of HZ increasing with age and declining immune status. The skin rash of HZ is often large but geographically restricted to a dermatome infiltrated by one or two specific ganglia. Reactivation is accompanied by extensive intra-ganglionic spread, infection of multiple neurons and numerous inflammatory and physiological processes that contribute to the development of pain. Almost all HZ is associated with acute pain, with up to 90% of HZ patients seeking prescription level pain relief [5]. However, some 30% of HZ patients report a chronic pain state termed post herpetic neuralgia (PHN), defined as pain lasting more than 3 months after the resolution of the skin lesions [6‐8]. A fraction of PHN patients may suffer pain more than one year after other disease symptoms dissipate [9]. PHN is debilitating, difficult to treat, and can have secondary long term consequences that can greatly affect quality of life. In the absence of the current HZ vaccine approximately 1 million people annually in the US and about 5% of the total population will suffer from PHN [9‐11]. The majority of HZ sufferers are age 60 years or older [12, 13]. Given that the number of people 60 years of age or older is one of the fastest growing and is expected to double in the next 50 years [9], HZ and the associated pain will be an ever increasing problem in the future. While the HZ vaccine reduces the incidence of HZ by 51% and PHN by 68%, the vaccine remains to be widely used largely due to cost/reimbursement issues, reluctance to vaccination, and ignorance of both the target population and their physicians. [11]. Even if every candidate receives the vaccine (which is far from being achieved) the US would still have some half million HZ cases each year with many suffering from PHN. As such, better prevention and therapy for both zoster and PHN are an unmet need.

It has been difficult to model HZ and PHN because no animal model shows reactivation of latent VZV. In general, VZV is considered human specific, for reasons not yet clear. However it has been shown that VZV injected into the footpad of either Wistar or Sprague Dawley rats results in measurable hypersensitivity that is similar to that in humans with PHN [14‐20]. The footpad animal model has been developed as a platform for one, mechanistic studies of chronic pain after VZV infection of dorsal root ganglia and two, for drug evaluation focused on HZ associated pain relief [20, 21]. Treatment of these animals with antivirals, opioids or NSAIDS mirrors HZ patients treated with these same drugs, in that, zoster associated pain does not respond to antivirals, but does respond to treatment with gabapentin or sodium channel blockers [16, 17, 20, 21].

Given that the rat footpad model has been used to study the mechanism by which VZV associated pain develops and can be used for pre-clinical screening of analgesic drugs [17, 21] we considered whether the model can be extended to orofacial pain that follows VZV reactivation in the trigeminal ganglia. Extension of the model to the orofacial region would be significant because the trigeminal ganglia of human cadavers have the highest latent VZV load, and up to 1 in 5 HZ cases occurs in the orofacial or naso-ocular region [22, 23]. Importantly, females report HZ associated pain 3.75 times more often than men, and HZ associated pain has been reported to be 36% higher in females [24, 25]. The basis for this disparity is not understood. Currently, neither the orofacial effects nor the sex differences have been determined in any zoster associated pain model. In this report, an animal model for zoster associated orofacial pain was characterized that could be utilized first, to study the mechanisms of HZ associated pain in the orofacial region and second, to study the mechanisms resulting in women reporting HZ pain more often than men.

Mechanical allodynia is the most common, most debilitating and the most difficult to treat component seen in PHN patents. Persistent mechanical allodynia and thermal hyperalgesia are present after VZV inoculation of the footpad [14‐20]. The study here expands the footpad model to the orofacial region by demonstrating that VZV induces a significant behavioral response after stimulating the facial region [20, 21, 44]. These responses included thermal and mechanical hypersensitivity, as well as, an aversive response. Interestingly the aversive response, as measured by the PEAP assay [31], lasted several weeks longer than the hypersensitivity measured by Ugo Basile chambers. The longer PEAP response suggests that either the PEAP assay was more sensitive than the Ugo Basile chambers in measuring responses or that the affective component is present longer than the sensory component. In contrast to our results, previous studies injecting compete Freund’s adjuvant into the paw showed that sensory responses (von Frey) and affective responses (PEAP test) lasted for similar times [31]. One explanation for this inconsistency would be that adjuvant induces pain through a different mechanism than VZV. Behavioral tests, such as the PEAP test, require supraspinal pain processing and would be useful in the drug development for patients [36, 37]. In one example of preclinical drug testing, gabapentin reduced the affective PEAP response in this rat model consistent with gabapentin being efficacious in treating patients with HZ associated pain [45]. It is interesting to note that anxiety-like behaviors were not reversed by gabapentin treatment in previous studies [20], but gabapentin does effect the PEAP measurement (reverse the aversive behavior), consistent with the idea that anxiety does not bias the PEAP measurement [36, 46].

Pain is reported 3.75 times more often in women than in men after HZ infection [25] but no model currently exists to study this sex difference. We show here that VZV induced pain was influenced by sex. VZV inoculated female rats experienced the same level of aversive behavior as the VZV injected males post-injection week 1, but by week 2 females clearly experienced a higher level of pain behavior, consistent with females experiencing more orofacial pain-related sensations [47‐49]. One reason for the sex difference could be related to sex steroids. Of note is the fact that the males had a greater percentage of IE62 positive neurons but showed less aversive behavior suggesting that viral infection rates do not explain the sex difference. Moreover, our data support a role for sex steroids because during the estrous cycle there was a significantly greater PEAP response in diestrus rats (when estradiol is low) in comparison to proestrus/estrus rats (when estradiol is higher). This data is consistent with the nociceptive response in an inflammatory TMJ model where rats given a diestrus level of estradiol (low) had a greater nociceptive response in comparison to rats given a proestrus dose of estradiol (high) [50]. Mechanistically estradiol has been shown to alter the pain response through G-protein signaling [51]. Moreover, estradiol utilizes G-protein signaling to alter the nociceptive response by changing the responsiveness of N-methyl-D-aspartic acid (NMDA) receptors and by enhancing dendritic spine growth [52]. Although the mechanism is unclear as to why the nociceptive response was higher in females this animal model can be used to explore the mechanisms contributing to the observed sex difference.

Humans with HZ associated pain do not require continued replication of VZV because administration of the antiviral acyclovir (blocks viral replication) does not reduce the pain response [53]. Similarly, VZV induced pain was not ameliorated by antiviral agents in the rat footpad model [54]. As in humans, VZV induced hypersensitivity in rodents can be present without detectable viral replication [44, 55, 56]. Recent work has indicated that VZV goes through a partial replication cycle in animals resulting in translation of viral proteins that can induce pain [53]. Together the data suggests continued production of lytic virus and necrosis of neurons is not a mechanism for induction or maintenance of the pain response [57]. To date, no animal has supported VZV ganglionic reactivation [58], so PHN after reactivation cannot be studied. Interestingly, Dr. Kinchington’s group has recently reported the first reliable experimental VZV reactivation in vitro using human neuron cultures [59] and proposed that both human PHN and pain in rats are the result of VZV gene expression without viral replication. Our studies add to this previous work by extending the pain response to the orofacial region which contributes to pain in up to 28% of herpes zoster patients [22, 23]. Using this novel model of VZV these pain mechanisms can be determined in the orofacial region.

Zoster-associated pain may last 30–90 days during the acute phase however, about 20–30% of individuals develop chronic pain (>90 days) termed post-herpetic neuralgia (PHN), which may last months to years [6‐8, 60, 61]. In males a VZV dose of 65,000 pfu/whisker pad resulted in a significant response for one week and a dose of 190,000 pfu/whisker pad resulted in a 7 week response. Assuming a linear relationship between dosage and response an injection of 300,000 pfu/whisker pad would result in a 12 week response. A 12 week or 90 day pain response is one of the diagnostic criteria for PHN [60]. Future studies investigating higher dosages could indicate that this model is applicable for studying the mechanisms resulting in the development of PHN.

VZV infection of the whisker pad resulted in IE62 staining within the V1/V2 and V3 regions of the trigeminal ganglia. Because the V1/V2 branch innervates the whisker pad it was not clear why some IE62 staining was present within the V3 region. This is the first evidence for VZV infection of the trigeminal ganglia after injection into the rodent whisker pad but VZV is a human herpes virus, one of eight types of herpes viruses. Whisker pad injection of herpes simplex virus type 1 (one of the eight types of herpes viruses) resulted in a small amount of infection of the V3 region with a majority of the infection being present in the V1/V2 region [62], consistent with our results. Studies of the somatotopic organization of the trigeminal ganglia indicated that there was overlap in the ganglionic regions that contribute to the V1/V2 and V3 branches [63]. The results could be explained by this overlap; if some of the IE62 positive neurons in the V3 region actually project to the whisker pad then it would be expected that these neurons would become infected by VZV.

Our study uses behavioral testing to assess zoster associated orofacial pain in the rat model. For the first time a sex difference is shown after VZV injection, consistent with epidemiological evidence that women report PHN more than men [24, 25]. This model can be utilized to study one, the mechanisms of zoster-associated orofacial pain, two, test drug therapies to treat humans effectively and three, study the mechanisms contributing to the sex differences underlying zoster associated pain.