What is Post-Herpetic Neuralgia?

Posted On: 18 February 2025
Posted By: Hermina Tangerang
8 min read
Reviewed By: dr. Irsyah Dwi Rohmayanti, Sp.N

What is Post-Herpetic Neuralgia?

What is Post-Herpetic Neuralgia?

Herpes zoster (HZ) results from reactivation of latent varicella-zoster virus in dorsal root ganglion neurons. The most common complication of HZ is post-herpetic neuralgia (PHN), which is characterized by persistent neuropathic pain in the affected dermatome after the rash resolves. PHN is characterized by a unilateral, stabbing/burning pain in a dermatomal pattern that persists for three months or more after the onset of the herpes zoster (HZ) outbreak. Two universally accepted risk factors for HZ are increasing age and immunosuppression, and HZ is a major risk factor for the development of PHN. Currently, multimodal management is essential, with some researchers/clinicians focusing on prevention in high-risk populations rather than cure due to the debilitating and often refractory nature of PHN. Treatment modalities for PHN primarily include drug therapy and physical therapy. Post-herpetic neuralgia is defined as neuropathic pain that occurs after the eruptive phase of herpes zoster as the most common clinical sequelae. Post-herpetic neuralgia (PHN) is a chronic neuropathic pain syndrome characterized by chronic, persistent, and often severe pain following reactivation of the varicella-zoster virus (VZV) (herpes zoster) in the sensory ganglia of the cranial nerves or dorsal root ganglia of the spinal cord. To date, the definition of PHN has been inconsistent across studies, with incidence ranging from ≥1 to ≥6 months after the rash. Compared with acute HZ-related pain (pain preceding or accompanying visible skin manifestations), which resolves within a month, PHN can persist for months or even years.

Who is at risk for Post-Herpetic Neuralgia (PHN)?

Several risk factors for PHN have been reported, including advanced age, female sex, severe immunosuppression, severe rash, and acute pain from zoster episodes. Physical comorbidities, such as autoimmune conditions and diabetes, may also be associated with an increased risk of PHN.

How is Post-Herpetic Neuralgia (PHN) diagnosed?

The diagnosis of neuropathic pain is based on the typical symptoms and findings of neuropathic pain, particularly the combination of minus symptoms (sensory deficits such as hypaesthesia, hypalgesia) and plus symptoms (burning pain, especially at rest, throbbing pain, allodynia, hyperalgesia). The history of HZ and the nature of the pain are critical parameters in the diagnosis of PHN. The medical history serves to differentiate the pain syndrome (nociceptive or nociceptive vs neuropathic). It should provide information about relevant lesions or diseases of the peripheral or central somatosensory system. Information about disorders, previous medications, and pain-related comorbidities such as anxiety, depression, or sleep disorders is also important. The patient's history may reveal conditions that may help differentiate the diagnosis of PHN, including a recent history or presence of herpes simplex virus, impetigo, candidiasis, contact dermatitis, insect bites, autoimmune blistering disease, dermatitis herpetiformis and drug-related eruptions. In about 50% of patients with PHN, dynamic mechanical allodynia occurs in the pain-producing area in response to normally painless stimuli, such as light touch. Thermal hyperalgesia occurs in about one-third of patients. However, in some cases, decreased sensation or numbness may be experienced by patients. Complementary quantitative sensory testing may provide additional information about the functional status of the somatosensory system. The intensity and quality of pain should be assessed using an appropriate pain scale, based on the patient's ability to communicate such as a numeric rating scale (usually an 11-point scale: from 0, no pain, to 10, severe pain), a visual analog scale, or a verbal descriptor scale (eg, McGill Pain Questionnaire). The fact that pain affects quality of life should be evaluated, usually by interview, but structured questionnaires can also be used. In children, a Likert scale consisting of 4-5 verbal descriptors or Icons can be used.

Special Inspection

Postherpetic neuralgia is almost universally diagnosed based on patient history and physical examination. However, laboratory tests and some targeted imaging may provide a degree of utility. These diagnostic techniques are of greater value in atypical presentations of PHN, such as zoster sine herpete or herpes zoster laryngeus. Serologic tests for VZV IgG and IgM titers are available, although their sensitivity and specificity are less than ideal. A fourfold rise has been used to diagnose subclinical HZ (zoster sine herpete). However, this elevated titer may or may not be secondary to exposure or reactivation of the virus. Comparatively, immunofluorescence vesicle scrapings detect VZV antigen in a highly specific and sensitive manner. Similarly, PCR is highly sensitive for detecting VZV DNA. Cerebrospinal fluid (CSF) analysis results are abnormal in 61% of patients. Pleocytosis, elevated protein, and varicella-zoster virus (VZV) DNA are commonly seen. Viral culture or immunofluorescent staining helps differentiate herpes simplex from herpes zoster.

Supporting investigation

Small-scale studies suggest that magnetic resonance imaging (MRI) may be promising for diagnosing challenging cases of PHN and differentiating between PHN and HZ. A study by Haanpaa et al. reported that MRI revealed HZ-related lesions in the spinal cord and brainstem in 9 patients (56%). Three months after HZ onset, PHN developed in 5 patients (56%) who had abnormal MRI. On MRI, the seven patients without HZ lesions had no residual pain.

What is the prognosis for Post-Herpetic Neuralgia (PHN)?

Postherpetic neuralgia is difficult to treat. Symptoms can persist for years, sometimes lifelong. With the advent of adult vaccination and newly developed non-live vaccine formulations, prevention appears to be a realistic goal for a large portion of the susceptible American population. When prevention of HZ is not possible, timely treatment is recommended, as duration and severity of pain are considered risk factors for PHN. Unfortunately, once PHN is established, first-line conservative treatment rarely results in resolution of symptoms and does not offer long-term relief. Therefore, a multimodal therapeutic approach recommended by expert consensus should be considered. Limited but compelling evidence suggests that certain unconventional techniques, both invasive and noninvasive, are promising and merit further investigation.

Conclusion

Post-herpetic neuralgia (PHN) represents a potentially debilitating and often underestimated form of neuropathic pain that disproportionately affects vulnerable populations, including the elderly and immunocompromised. Varicella zoster infection is nearly universally prevalent, making prevention of acute herpes zoster (AHZ) infection and prompt diagnosis and aggressive management of PHN critical. Despite the recent development of a herpes zoster vaccine, prevention of AHZ is not yet widespread or addressed in PHN treatment guidelines. The diagnosis of PHN requires consideration of the recognizable signs of PHN and known risk factors, including advancing age, severe prodromal pain, severe rash, and location of AHZ in the trigeminal dermatome or brachial plexus.

PHN is a painful and burdensome condition that can interfere with a patient’s function and quality of life. Health care professionals play a key role in helping to improve pain caused by PHN through routine assessment and early recognition of problems, recommending evidence-based pharmacological modalities for managing long-term PHN pain and monitoring patient side effects, treatment adherence, expectations and response to treatment in the elderly population most at risk.

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What is Post-Herpetic Neuralgia?

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