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Shingles

Shingles, also known as herpes zoster, is a viral infection caused by the reactivation of the varicella-zoster virus (VZV), the same virus that causes chickenpox, leading to a painful rash typically appearing as a stripe of blisters on one side of the body. The condition often begins with pain, tingling, or burning sensations in the affected area, followed by a red rash that develops into fluid-filled blisters, which can itch or become infected; additional symptoms may include fever, headache, chills, or fatigue. The rash usually lasts 2 to 4 weeks, but the associated nerve pain can persist longer in some cases. Anyone who has previously had chickenpox is at risk for shingles, as the virus remains dormant in the body's nerve tissues after the initial infection; the risk increases significantly with age, particularly after 50, and in individuals with weakened immune systems due to conditions like HIV, cancer, or immunosuppressive medications. Shingles itself is not directly contagious, but the virus can spread through direct contact with blister fluid to cause chickenpox in people who have never had it or been vaccinated against it. Common complications include postherpetic neuralgia, a chronic nerve pain that affects up to 20% of cases and is more frequent in older adults, as well as potential vision loss if the rash occurs near the eyes, bacterial skin infections, or rare neurological issues. Prevention is possible through vaccination with the recombinant Shingrix vaccine, recommended for adults aged 50 and older or those 19 and older with compromised immunity, administered in two doses 2 to 6 months apart, which is over 90% effective in preventing shingles and its complications. Treatment typically involves antiviral medications like acyclovir, valacyclovir, or famciclovir, started within 72 hours of rash onset to reduce severity and duration, alongside pain management strategies such as over-the-counter analgesics or prescription options.

Introduction

Definition

Shingles, also known as herpes zoster, is a viral infection resulting from the reactivation of the varicella-zoster virus (VZV), the same virus that causes chickenpox (varicella). After an initial episode of chickenpox, VZV establishes latency in the sensory dorsal root ganglia of the nervous system, where it can remain dormant for decades before reactivating under certain conditions. The typical presentation of shingles involves a unilateral rash confined to one or more adjacent dermatomes, often accompanied by pain and the formation of fluid-filled blisters (vesicles). This dermatomal distribution reflects the virus's reactivation along specific sensory nerves, most commonly affecting the trunk in a thoracic dermatome. Shingles differs from primary VZV infection, or chickenpox, which produces a widespread, pruritic vesicular rash across the body rather than a localized dermatomal pattern. It is also distinct from infections caused by other herpesviruses, such as herpes simplex virus types 1 and 2 (HSV-1 and HSV-2), which typically cause recurrent oral or genital lesions in clustered groups without the characteristic unilateral dermatomal involvement of shingles.

Overview

Shingles, medically known as herpes zoster, results from the reactivation of the varicella-zoster virus (VZV), the same virus responsible for chickenpox, within the body of individuals who previously contracted that infection. This condition predominantly impacts adults aged 50 years and older, as well as those who are immunocompromised due to factors such as HIV, cancer treatments, or organ transplants. Unlike chickenpox, shingles is not transmitted directly from person to person; however, the active rash can spread VZV to susceptible contacts who lack immunity to chickenpox, potentially causing varicella in them via direct contact with blister fluid or airborne particles from the lesions. The typical course of shingles includes a prodromal phase of 1 to 5 days marked by localized pain or tingling, followed by rash eruption that scabs over in 7 to 10 days and generally resolves within 2 to 4 weeks, although postherpetic neuralgia—a chronic pain condition—may develop and persist for months or longer in some cases. The rash itself is often intensely painful, following a dermatomal pattern on one side of the body. In the United States, an estimated 1 million cases of shingles occur each year, underscoring its significant public health burden and the critical role of vaccination in reducing incidence and complications among at-risk populations.

Clinical Presentation

Signs and Symptoms

Shingles typically begins with a prodromal phase lasting 2 to 3 days, characterized by flu-like symptoms such as fever and malaise, along with localized pain, itching, or tingling in the affected dermatome. This early warning often precedes the rash and can mimic other conditions due to its nonspecific nature. The hallmark rash of shingles appears unilaterally in a band-like distribution along a sensory nerve dermatome, most commonly thoracic or lumbar. It starts as red macules or papules that rapidly evolve into clusters of fluid-filled vesicles within 1 to 5 days, progressing to pustules and then crusting over 7 to 10 days as the lesions heal. The rash is typically confined to one or a few adjacent dermatomes and does not cross the midline. Pain is a prominent feature, presenting as acute neuropathic discomfort described as burning, stabbing, or electric-shock-like, with intensity ranging from mild to severe and often intensifying with the rash's onset. This pain arises from inflammation of the affected nerve and sensory ganglia. The trunk is the most frequent site, accounting for 50-60% of cases, followed by the face or cranium in about 20%, while limbs are less commonly involved. In immunocompromised individuals, the rash may disseminate to multiple dermatomes or distant sites.

Complications

One of the most common complications of shingles is postherpetic neuralgia (PHN), defined as persistent neuropathic pain lasting more than three months after the rash has resolved, often characterized by burning or lancinating sensations in the affected dermatome. PHN affects 10-18% of shingles patients overall, with incidence rising significantly in older adults—reaching approximately 60% in those aged 60 years and 75% in those aged 70 years—due to age-related declines in immune function and slower viral clearance. The underlying mechanisms involve varicella-zoster virus-induced neuroinflammation leading to peripheral nerve damage, including myelin and axon deficiencies, dorsal root ganglion atrophy, and central sensitization in the spinal cord, which perpetuate ectopic nerve firing even after viral replication ceases. In immunocompromised individuals, shingles can progress to disseminated zoster, characterized by widespread cutaneous lesions exceeding 20 outside the primary dermatome, occurring in up to 37% of untreated cases and 10-30% overall in this population, such as those with malignancies or transplants. This dissemination heightens the risk of visceral organ involvement, including pneumonia (incidence 2.5% in immunocompromised patients) and hepatitis (0.8%), potentially leading to severe systemic illness like acute respiratory distress syndrome if untreated. Zoster ophthalmicus arises when the virus reactivates in the ophthalmic division of the trigeminal nerve, accounting for 10-25% of all shingles cases, particularly in older or immunocompromised patients. Ocular complications are frequent, with keratitis affecting up to 65% of cases through epithelial, stromal, or neurotrophic forms that cause corneal inflammation, scarring, or ulceration; untreated progression can result in uveitis, retinal necrosis, optic neuritis, or permanent vision loss in severe instances. Other complications include bacterial superinfection of skin lesions, which can occur due to disrupted epidermal barriers and lead to cellulitis or impetigo requiring antibiotic intervention. Ramsay Hunt syndrome, a rare cranial neuropathy variant, involves varicella-zoster virus spread to the geniculate ganglion, manifesting as ipsilateral facial palsy, ear pain, vesicles in the auditory canal, hearing loss, vertigo, and tinnitus, with incomplete recovery in many patients. Neurological sequelae such as transverse myelitis, encephalitis, or aseptic meningitis are uncommon but can arise from direct central nervous system invasion or immune-mediated damage, potentially causing motor deficits, sensory loss, or autonomic dysfunction.

Pathophysiology

Viral Mechanism

Varicella-zoster virus (VZV), a member of the alphaherpesvirus family, establishes infection through primary exposure, typically manifesting as chickenpox (varicella), during which the virus disseminates via the bloodstream to sensory ganglia. Following acute replication in epithelial cells and T lymphocytes, VZV enters sensory neurons and travels retrogradely along axons to dorsal root ganglia and cranial nerve ganglia, where it establishes lifelong latency. In this latent state, the virus persists as episomal DNA in neuronal nuclei with minimal viral gene expression, primarily limited to immediate-early genes such as open reading frame 63 (ORF63), which helps maintain dormancy without producing infectious virions. This latency can endure for decades, evading host immune surveillance. Reactivation of latent VZV, leading to shingles (herpes zoster), is primarily triggered by waning cell-mediated immunity, often associated with advancing age or immunosuppressive conditions. Upon reactivation, viral gene expression shifts from restricted latency-associated transcripts to a full lytic cycle: immediate-early genes (e.g., ORF4 and ORF62) initiate transcription, followed by early genes involved in DNA replication (e.g., ORF28 and ORF29), and culminating in late genes for structural proteins and virion assembly (e.g., glycoprotein genes). This cascade enables viral replication within neuronal cell bodies, followed by anterograde axonal transport of newly formed virions to the skin, where they infect keratinocytes and produce the characteristic dermatomal rash. The pathological effects of VZV reactivation center on sensory neurons and ganglia, inducing acute inflammation through mononuclear cell infiltration and cytokine release, which contributes to severe pain. This inflammatory response can lead to demyelination in affected nerve segments, neuronal fibrosis, and loss of sensory neurons, exacerbating nerve damage and potentially resulting in prolonged hypersensitivity. T-cell immunity, particularly CD4+ and CD8+ T cells specific to VZV antigens, plays a crucial role in suppressing latency and preventing reactivation by surveilling infected neurons and limiting viral spread; decline in these responses, as seen in aging, permits the virus to overcome immune control.

Risk Factors

The primary risk factor for developing shingles, or herpes zoster, is a prior infection with the varicella-zoster virus (VZV) that causes chickenpox, as the virus establishes lifelong latency in sensory ganglia following primary infection. In populations born before widespread chickenpox vaccination, such as those in the United States prior to 1980, nearly all adults (approximately 99.5%) have had chickenpox, making them susceptible to reactivation. Age is the most significant non-modifiable risk factor, with incidence rising sharply after age 50 due to immunosenescence, or age-related decline in cell-mediated immunity. The annual incidence increases from about 4 cases per 1,000 persons overall to approximately 10 per 1,000 (1%) in those over age 80. By age 85, the cumulative lifetime risk approaches 50%. Immunosuppression substantially elevates risk, often by 10- to 100-fold depending on the underlying condition or treatment. Conditions such as HIV/AIDS (relative risk [RR] 3.22), malignancies like leukemia or lymphoma (RR 2.17), organ transplantation, and therapies including chemotherapy or prolonged corticosteroid use impair VZV-specific T-cell immunity, facilitating viral reactivation. For instance, solid organ transplant recipients experience a 2- to 10-fold increase in risk compared to immunocompetent individuals. Other factors include a slight increase in risk among females (pooled adjusted RR 1.31). Psychological stress has been associated with elevated risk (RR approximately 2.0), potentially through suppression of cellular immunity, while physical trauma to the affected dermatome may trigger reactivation (RR 2.01). Genetic factors, including family history (RR 2.48), increase susceptibility, though specific genes remain to be firmly identified. Individuals with a history of chickenpox vaccination have a reduced risk of shingles compared to those who experienced natural infection, though the risk is not entirely eliminated due to possible vaccine-strain latency. Widespread varicella vaccination since 1995 has contributed to lower overall HZ incidence in vaccinated cohorts as of 2025. For example, vaccinated children show a 78% lower incidence of herpes zoster than unvaccinated children who had breakthrough chickenpox.

Diagnosis

Clinical Diagnosis

The clinical diagnosis of shingles, or herpes zoster, is primarily based on a patient's medical history and physical examination, as the condition often presents with characteristic features that allow for recognition without laboratory testing in typical cases. During history taking, clinicians focus on prodromal symptoms such as localized pain, tingling, or itching in a specific area, which may precede the rash by several days and often follows a unilateral dermatomal distribution; a history of recent chickenpox exposure is unnecessary, as shingles results from reactivation of latent varicella-zoster virus rather than new infection. Additional prodromal features can include headache, malaise, or photophobia, helping to distinguish the condition from other causes of unilateral pain. On physical examination, the key finding is a unilateral vesicular rash confined to one or two adjacent dermatomes, most commonly on the trunk (thoracic dermatomes) or face, without crossing the midline. The rash typically evolves from erythematous macules to grouped vesicles on an erythematous base over 3 to 5 days, eventually crusting and healing within 2 to 4 weeks, sometimes leaving scars. A notable sign during examination is Hutchinson's sign, characterized by herpetic lesions on the nasal tip or side, indicating involvement of the nasociliary branch of the trigeminal nerve and raising concern for ocular complications such as herpes zoster ophthalmicus. The standard clinical criteria for diagnosing shingles include the presence of a unilateral vesicular rash accompanied by pain or sensory changes in one or more contiguous dermatomes. This presentation is highly suggestive in immunocompetent individuals, though zoster sine herpete—a rare variant involving dermatomal pain without rash—may occur and complicates bedside diagnosis. In atypical cases, particularly among immunocompromised patients, the rash may appear multifocal, disseminated (involving more than 20 lesions outside the primary dermatome), or even absent, potentially leading to visceral involvement such as pneumonitis or hepatitis; in these scenarios, a thorough history of immunosuppression is crucial for suspicion.

Laboratory Confirmation

Laboratory confirmation of herpes zoster (shingles) is typically pursued when the clinical presentation is atypical or uncertain, such as in immunocompromised individuals or cases lacking a classic dermatomal rash, to verify varicella-zoster virus (VZV) infection through objective testing. These tests are adjunctive to clinical evaluation and are not routinely required for straightforward diagnoses, as the characteristic unilateral vesicular eruption often suffices. Common specimen sources include vesicular fluid, lesion swabs, scabs, or cerebrospinal fluid (CSF) in cases of neurological involvement. Polymerase chain reaction (PCR) testing represents the gold standard for laboratory confirmation, detecting VZV DNA with high sensitivity exceeding 95% and specificity approaching 100% in vesicular fluid, lesion swabs, or CSF. The procedure involves collecting a sample from an unroofed vesicle or swabbed lesion base, followed by amplification and detection of viral genetic material, often using real-time PCR for rapid results within hours to one day. This method is particularly valuable for early diagnosis before vesicle formation or in disseminated disease. Viral culture, once a historical mainstay, isolates live VZV from lesion specimens but has lower sensitivity (typically under 70%) and requires 1-2 weeks for growth, rendering it less practical today. The Tzanck smear, performed by scraping a fresh vesicle and staining for microscopic examination, reveals multinucleated giant cells indicative of herpetic infection but lacks specificity, as it cannot differentiate VZV from herpes simplex virus, and its sensitivity is limited to around 60%. Serologic testing measures VZV-specific IgM (for acute infection) or IgG (for immunity) antibodies in serum, but it is unreliable for acute shingles diagnosis due to widespread prior varicella exposure conferring baseline IgG in most adults; a four-fold IgG rise in paired acute-convalescent samples may confirm recent reactivation, though sensitivity remains low compared to PCR. Indications for laboratory confirmation include atypical rashes, immunocompromised patients at risk for dissemination, and zoster sine herpete—a rashless form presenting with dermatomal pain—where PCR from CSF or plasma is especially useful for early detection. Additionally, in suspected neurological complications like encephalitis or myelitis, magnetic resonance imaging (MRI) of the brain or spine may be employed alongside CSF PCR to assess involvement and exclude mimics, though MRI findings are supportive rather than confirmatory of VZV.

Prevention

Vaccination

Vaccination against shingles, caused by reactivation of the varicella-zoster virus, primarily involves two vaccines: the live attenuated Zostavax and the recombinant Shingrix. Zostavax, approved in 2006, demonstrated approximately 51% efficacy in preventing shingles in adults aged 60 years and older, but its protection waned over time and it is no longer preferred or available in many regions, having been discontinued in the United States in 2020 and in other countries by 2023-2025. Shingrix, a recombinant zoster vaccine approved in 2017, has become the standard for prevention due to its superior efficacy and safety profile. It consists of recombinant varicella-zoster virus glycoprotein E (gE) antigen combined with the AS01B adjuvant system, which enhances T-cell mediated immunity by stimulating strong CD4+ T-cell responses essential for controlling viral reactivation. The vaccine is administered as a two-dose intramuscular series, with doses spaced 2 to 6 months apart. The Centers for Disease Control and Prevention (CDC) recommends Shingrix for all adults aged 50 years and older, regardless of prior shingles history or vaccination, and for immunocompromised adults aged 19 years and older who are at increased risk. In clinical trials, Shingrix showed 97% efficacy against shingles in adults over 50 years and 90% efficacy in those over 70 years, with effectiveness ranging from 68% to 91% in immunocompromised individuals depending on the underlying condition. Shingrix also reduces the risk of postherpetic neuralgia (PHN), a common complication, by approximately 90% in adults aged 50 years and older. Recent studies in 2025 have further indicated that vaccination is associated with a 20-25% lower risk of dementia and cardiovascular events, such as heart attacks and strokes, potentially due to reduced viral-induced inflammation. Contraindications include a history of severe allergic reaction to any vaccine component or active shingles infection at the time of vaccination. Shingrix is generally safe for most immunocompromised individuals, though consultation with a healthcare provider is advised for those with severe immunosuppression.

Lifestyle and Risk Reduction

Maintaining a healthy immune system through lifestyle practices is essential for reducing the risk of shingles, as the varicella-zoster virus (VZV) reactivation depends on robust T-cell mediated immunity. A balanced diet rich in vitamins C and E, zinc, and antioxidants supports overall immune function, including T-cell responses that help keep VZV latent. Regular physical activity, such as moderate aerobic exercise or practices like tai chi, has been shown to enhance varicella-zoster virus-specific immunity in older adults by improving cellular immune responses. Adequate sleep, aiming for 7-9 hours per night, is crucial for immune regulation, as sleep deprivation can impair T-cell proliferation and increase susceptibility to viral reactivations like shingles. Chronic stress can suppress cellular immunity, potentially triggering VZV reactivation by reducing the activity of virus-specific T-cells. Stress management techniques, such as mindfulness meditation, yoga, or cognitive behavioral therapy, help mitigate this by lowering cortisol levels and preserving immune competence. Individuals with high perceived stress levels may face up to a twofold increased risk of herpes zoster compared to those with low stress. To avoid unnecessary immunosuppression, healthcare providers should use corticosteroids judiciously, as systemic use increases shingles risk by approximately 59%, with higher doses correlating to greater hazard. Smoking cessation is recommended, as former smokers exhibit a 17% higher risk of herpes zoster compared to never smokers, likely due to lingering inflammatory effects on immunity. Receiving the chickenpox vaccine in childhood prevents primary VZV infection, thereby eliminating the possibility of latent virus establishment and subsequent shingles in adulthood. For those with active shingles, practicing good hygiene and isolating from susceptible contacts—such as unvaccinated children or immunocompromised individuals—prevents transmission of VZV, which can cause chickenpox in non-immune people and indirectly contribute to future shingles risk in the population. Covering the rash and avoiding direct contact until lesions crust over is key to this strategy.

Treatment

Antiviral Medications

Antiviral medications are the cornerstone of treatment for acute shingles (herpes zoster), aiming to inhibit varicella-zoster virus (VZV) replication, thereby shortening the duration and severity of the illness. These drugs are most effective when initiated promptly, ideally within 72 hours of rash onset, as this window allows for maximal reduction in viral shedding and lesion formation. The primary agents include acyclovir, valacyclovir, and famciclovir, all of which are nucleoside analogs that selectively inhibit viral DNA polymerase without significantly affecting host cell replication. Valacyclovir is often preferred as a first-line oral therapy due to its superior bioavailability compared to acyclovir, requiring less frequent dosing. Standard regimens for immunocompetent adults include valacyclovir at 1 g three times daily for 7 days, famciclovir at 500 mg three times daily for 7 days, or acyclovir at 800 mg five times daily for 7 to 10 days. For severe or disseminated cases, particularly in immunocompromised patients, intravenous acyclovir is recommended at 10 mg/kg every 8 hours, with subsequent transition to oral therapy once clinically stable. Renal function monitoring is essential during high-dose therapy to prevent potential nephrotoxicity, especially in older adults. Clinical trials have demonstrated that these antivirals reduce the duration of rash healing and acute pain by approximately 1 to 2 days and can lower the risk of postherpetic neuralgia (PHN) by 20% to 50% when started early, with greater benefits observed in patients over 50 years old. The benefit diminishes significantly if treatment begins after 72 hours, though it may still be considered for select cases with ongoing lesion formation. Common side effects are mild and include nausea, headache, and diarrhea, occurring in less than 10% of patients; these agents are generally well-tolerated. As of 2025, no major new antivirals have emerged for standard acute shingles treatment, but evidence from the Zoster Eye Disease Study (ZEDS) supports long-term low-dose valacyclovir (1 g daily for 1 year) to prevent ocular complications in high-risk patients with herpes zoster ophthalmicus, reducing recurrence risk by 26% at 18 months compared to placebo. This approach targets persistent viral activity in the ophthalmic division of the trigeminal nerve.

Pain Management

Pain management in acute shingles (herpes zoster) focuses on alleviating the characteristic neuropathic and nociceptive pain, which can range from mild discomfort to severe, burning sensations along the affected dermatome. Effective strategies combine pharmacological interventions with supportive measures to improve patient comfort and daily functioning during the typical 2-4 week rash duration. Early pain control is crucial, as uncontrolled acute pain may increase the risk of transitioning to postherpetic neuralgia (PHN). For mild to moderate acute pain, nonsteroidal anti-inflammatory drugs (NSAIDs) such as ibuprofen (400 mg every 4-6 hours, maximum 2,400 mg/day) or acetaminophen (325-1,000 mg every 4-6 hours, maximum 4,000 mg/day) are first-line options, providing relief for nociceptive components without significant side effects in most patients. In cases of severe pain, short-term use of opioids like oxycodone or morphine is recommended, titrated to efficacy while monitoring for constipation and sedation; these should follow the principles of the WHO analgesic ladder, adapted for the neuropathic elements of shingles pain. Neuropathic pain, often described as burning or shooting, responds to agents like gabapentin (starting at 100-300 mg daily, titrated up to 1,800-3,600 mg/day in divided doses) or pregabalin (150-300 mg/day initially, up to 600 mg/day), which modulate nerve excitability and are effective for acute zoster pain when initiated early. Tricyclic antidepressants such as amitriptyline (10-25 mg at bedtime, titrated to 75 mg/day) or nortriptyline are also useful for burning-type pain, offering dual benefits through serotonin and norepinephrine reuptake inhibition, though they require caution in elderly patients due to anticholinergic effects. Topical therapies provide localized relief with minimal systemic absorption. Lidocaine patches (5% applied up to 12 hours daily) numb the affected area and are suitable for intact skin over the rash, reducing hypersensitivity. Capsaicin cream (0.025-0.075%) or high-dose patches (8% applied under supervision) can deplete substance P in sensory nerves, offering relief after initial burning, applied at least 3-5 times daily. Supportive non-pharmacological approaches include cool, wet compresses or baths to soothe itching and inflammation, applied several times daily for 10-15 minutes. Calamine lotion serves as an astringent to dry weeping blisters and reduce pruritus, while wet dressings with 5% aluminum acetate (Burow's solution) for 30-60 minutes, 4-6 times daily, help manage oozing lesions. For intractable pain unresponsive to standard measures, a multidisciplinary approach involving nerve blocks or referral to pain specialists is advised, aligning with adapted WHO ladder escalation for combined nociceptive and neuropathic pain.

Management of Complications

Postherpetic neuralgia (PHN), defined as pain persisting beyond three months after the shingles rash resolves, requires multimodal management tailored to severity. First-line pharmacological options include high-dose gabapentinoids such as gabapentin (up to 3600 mg/day) or pregabalin (up to 600 mg/day), which target neuropathic pain through calcium channel modulation, alongside serotonin-norepinephrine reuptake inhibitors like duloxetine (60-120 mg/day). For refractory PHN unresponsive to oral therapies, intravenous lidocaine infusions (1-5 mg/kg over 30-60 minutes) provide short-term relief by blocking sodium channels in nociceptive fibers. In severe, intractable cases, interventional procedures such as peripheral nerve blocks or epidural injections offer targeted analgesia, while spinal cord stimulation via implanted devices modulates pain signals for long-term control, with success rates exceeding 50% in selected patients. Herpes zoster ophthalmicus (HZO), involving the ophthalmic division of the trigeminal nerve, demands prompt ophthalmologic evaluation to mitigate risks of uveitis, keratitis, or secondary glaucoma. Standard treatment combines oral antivirals—such as valacyclovir (1000 mg three times daily for 7-10 days)—with topical corticosteroids (e.g., prednisolone acetate 1% eyedrops tapered over weeks) to reduce inflammation and prevent corneal scarring. Immediate referral to an ophthalmologist is essential for slit-lamp examination and intraocular pressure monitoring, as untreated uveitis can lead to vision loss in up to 10% of cases. Disseminated zoster, characterized by more than 20 lesions beyond the primary dermatome, particularly in immunocompromised individuals, necessitates hospitalization for intravenous acyclovir (10-15 mg/kg every 8 hours for 7-14 days) to halt viral dissemination and prevent visceral involvement. Close monitoring for organ failure, including hepatic or pulmonary complications, involves serial imaging and laboratory assessments, with dose adjustments for renal impairment to avoid toxicity. Secondary bacterial superinfections of skin lesions require empiric antibiotics such as cephalexin or clindamycin, guided by culture results. Ramsay Hunt syndrome, resulting from varicella-zoster virus reactivation affecting the geniculate ganglion, is managed with combined antiviral and corticosteroid therapy to improve facial nerve recovery. Oral or intravenous acyclovir (800 mg five times daily) or valacyclovir (1000 mg three times daily) for 7-10 days, paired with high-dose prednisone (1 mg/kg/day tapered over 2-3 weeks), enhances viral suppression and reduces nerve edema, potentially improving outcomes if initiated within 72 hours. For associated facial weakness, physical therapy including facial muscle exercises and neuromuscular re-education is recommended to prevent synkinesis and promote symmetry, with evidence showing better recovery rates when started early. A 2025 advancement from the Zoster Eye Disease Study demonstrates that long-term valacyclovir (1000 mg daily for 12 months) reduces the risk of new or worsening ocular disease in HZO by approximately 26% at 18 months compared to placebo, with 32% affected in the treated group versus 40% in placebo (recurrence-free rates of 68% versus 60%), alongside shorter pain duration and reduced need for neuropathic pain medications.

Prognosis

Short-Term Outcomes

In uncomplicated cases of shingles (herpes zoster), the rash typically progresses from red patches to fluid-filled blisters that begin to crust over within 7 to 10 days of onset. Full resolution of the rash, including scab shedding and skin healing, generally occurs within 2 to 4 weeks, though mild scarring or discoloration may persist temporarily. This timeline applies to most immunocompetent individuals without dissemination, allowing return to normal activities as the lesions dry and heal. Acute pain associated with shingles, often described as burning or stabbing, typically subsides as the rash resolves, particularly in younger patients. Initiation of antiviral therapy within 72 hours of rash appearance accelerates pain relief and reduces its duration by promoting faster viral clearance and inflammation control. Without treatment, pain may linger longer during the acute phase, but early intervention improves overall short-term comfort and recovery speed. Hospitalization is required in fewer than 5% of shingles cases, primarily among immunocompromised patients or elderly individuals experiencing disseminated infection or severe complications such as bacterial superinfection. Younger age and prompt antiviral treatment are key factors favoring favorable short-term outcomes, with reduced risk of prolonged acute symptoms and quicker return to baseline function.

Long-Term Effects

The most significant long-term complication of shingles is postherpetic neuralgia (PHN), a chronic neuropathic pain syndrome that persists or emerges after the rash has resolved, affecting 10% to 18% of patients overall. The prevalence increases with age, occurring in 10% to 20% of individuals over 50 years and reaching up to 21% in those aged 80 to 84 years. PHN can substantially impair quality of life, leading to depression, sleep disturbances, reduced mobility, chronic fatigue, and social isolation, with pain often described as burning, stabbing, or electric-shock-like and persisting for months or years. Recurrence of shingles, though uncommon, carries a lifetime risk of 1% to 6% in the general population, rising significantly to 0% to 18% in immunocompromised individuals due to factors such as organ transplantation or HIV. Recurrent episodes typically involve the same dermatome as the initial infection or an adjacent one, driven by persistent varicella-zoster virus latency and waning immunity. Scarring from shingles is generally minimal and resolves without intervention in most cases, though hyperpigmentation or minor discoloration may linger, particularly in individuals with darker skin tones. In ophthalmic shingles (herpes zoster ophthalmicus), which affects about 10% to 20% of cases, there is a 5% to 10% risk of permanent vision impairment, often due to corneal scarring, uveitis, or secondary glaucoma, with higher rates linked to older age and immunosuppression. Recent 2025 research has established a link between shingles and increased dementia risk, with unvaccinated individuals facing approximately 20% higher odds of developing dementia compared to those vaccinated, an effect attributed to varicella-zoster virus reactivation contributing to neuroinflammation; vaccination mitigates this by reducing both shingles incidence and subsequent cognitive decline.

Epidemiology

Incidence and Prevalence

In the United States, an estimated 1 million cases of shingles (herpes zoster) occur annually, with a lifetime risk of approximately 30% for the general population. The annual incidence rate overall ranges from 2 to 9 cases per 1,000 person-years, increasing significantly with age. Shingles is rare in individuals under 20 years of age, with incidence rates of approximately 0.6 to 0.7 cases per 1,000 person-years in this group. In contrast, rates rise sharply in older adults; for those over 50 years, the annual incidence is approximately 8 to 10 cases per 1,000 person-years, escalating to about 12 cases per 1,000 person-years among those over 80. Following the rollout of the Shingrix vaccine in 2017, incidence rates have shown a decline in vaccinated cohorts, with effectiveness estimates of 70% to 90% against shingles in adults aged 50 and older by 2025, depending on immune status and follow-up duration. Population-level trends indicate a modest overall reduction of around 16% in herpes zoster incidence among older adults through 2023, attributed to increasing vaccine uptake, with continued declines observed into 2025 due to higher vaccination rates. Postherpetic neuralgia (PHN), a common complication, affects approximately 12% of shingles cases overall, with rates rising to 20% or higher in those over 60 and decreasing with prompt antiviral treatment initiation within 72 hours of rash onset.

Global Distribution

Shingles, or herpes zoster, exhibits significant geographical variations in incidence and burden, largely influenced by population demographics, healthcare infrastructure, and underlying health conditions. In regions with aging populations such as Europe and Japan, the disease imposes a higher burden, with incidence rates among individuals over 60 years old ranging from 5 to 10 per 1,000 person-years. These elevated rates reflect the increased risk of varicella-zoster virus reactivation in older adults, exacerbated by longer life expectancies and better diagnostic reporting in high-income settings. In contrast, regions like sub-Saharan Africa and parts of Asia report lower overall incidence due to younger demographic profiles, where fewer individuals reach the age groups most susceptible to shingles; however, substantial underreporting occurs owing to limited surveillance systems and prioritization of other infectious diseases. Socioeconomic factors further accentuate disparities, particularly in low-resource settings where access to varicella vaccination remains limited, leading to higher primary chickenpox exposure and a potential future surge in shingles cases as populations age. In areas with high HIV prevalence, such as sub-Saharan Africa, immunosuppression drives notably higher rates, with incidence among untreated HIV patients estimated at 35 to 54 per 1,000 person-years, compared to general populations. This elevated burden underscores the interplay between infectious comorbidities and shingles distribution in resource-constrained environments. Vaccination programs are expanding in low- and middle-income countries (LMICs) to mitigate this, with initiatives focusing on integrating shingles vaccines into national immunization schedules to address inequities in access and reduce future incidence.

History

Historical Recognition

The earliest descriptions of what is now known as shingles date back to ancient times. Hippocrates in the 5th century BCE used the term "herpes" (Greek: "to creep") to describe ulcerative skin lesions that appeared to crawl along the skin, thus encompassing conditions including herpes simplex and herpes zoster. These observations captured the characteristic unilateral, girdle-like eruption and associated neuralgia, distinguishing it from other skin afflictions of the era. Ancient physicians, including the Roman encyclopedist Aulus Cornelius Celsus (c. 25 BCE–50 CE), recognized the disease's distinctive belt-shaped ("zoster" from Greek for girdle) manifestation along nerve pathways, using the term "herpes zoster" for the first time. In the 18th century, British physician William Heberden advanced the understanding of the disease with a detailed clinical description in 1768, highlighting the vesicular eruption confined to a single dermatome, often with severe pain, and its tendency to occur in older individuals, setting it apart from more generalized herpes infections or smallpox. This characterization laid the groundwork for recognizing shingles as a distinct entity and influenced subsequent medical literature. By the 19th century, connections began to emerge between shingles and chickenpox, with Hungarian physician János von Bókay proposing in 1909 that the two were manifestations of the same infectious agent, based on epidemiological observations of varicella outbreaks following zoster cases in households. Von Bókay's work, building on his earlier 1892 suggestions, documented instances where susceptible children developed chickenpox after exposure to adults with shingles, prefiguring the viral etiology and challenging the view of zoster as merely a degenerative nerve condition. This linkage shifted perceptions toward an infectious origin, though the causative agent remained unidentified until the mid-20th century. The definitive confirmation of shingles' cause came in 1953, when American virologist Thomas H. Weller successfully isolated the varicella-zoster virus (VZV) from vesicular fluid of patients with both varicella and herpes zoster, demonstrating that the same pathogen was responsible for primary chickenpox infection and its later reactivation as shingles. Weller's breakthrough, achieved through human tissue cell culture techniques, not only verified von Bókay's hypothesis but also enabled serological and virological studies that solidified the understanding of VZV latency in dorsal root ganglia. This isolation marked a pivotal advancement, transforming shingles from a clinically observed syndrome into a well-defined viral disease.

Vaccine Development

The development of vaccines for shingles, resulting from varicella-zoster virus (VZV) reactivation, originated in the mid-20th century following the virus's initial isolation. In the 1950s, VZV was first successfully cultured in human embryonic lung cells, enabling foundational virological research. Specifically, in 1953, Thomas Weller isolated VZV from vesicular fluid of patients with varicella or zoster using cell culture techniques, marking a critical step toward vaccine development. These efforts laid the groundwork for attenuated vaccines targeting VZV. In the 1970s, live attenuated vaccines were developed primarily for preventing primary VZV infection (chickenpox), which indirectly informed shingles prevention strategies. Japanese researcher Michiaki Takahashi isolated the Oka strain from a child with varicella in 1971 and attenuated it through serial passage in human and guinea pig cells by 1974, creating the first viable live varicella vaccine. This Oka strain became the basis for subsequent shingles vaccines, as it demonstrated the potential to stimulate cell-mediated immunity against VZV latency and reactivation. The first dedicated shingles vaccine, Zostavax, received FDA approval in 2006 as a live attenuated formulation using a higher potency (14 times that of the varicella vaccine) of the Oka strain. Administered as a single intramuscular dose to adults aged 60 and older, Zostavax aimed to reduce the incidence of herpes zoster by approximately 51% and postherpetic neuralgia by 67% in clinical trials. Subsequent innovations addressed Zostavax's limitations, such as waning efficacy over time and contraindications in immunocompromised individuals, leading to Shingrix. Approved by the FDA in October 2017 and by the EMA in 2018, Shingrix is a non-live recombinant vaccine comprising VZV glycoprotein E (gE) antigen combined with the AS01B liposome-based adjuvant to enhance T-cell and antibody responses. Pivotal phase 3 trials—ZOE-50 in adults aged 50 and older, and ZOE-70 in those aged 70 and older—showed vaccine efficacy of 97.2% and 89.8% against shingles, respectively, with pooled efficacy exceeding 90% and sustained reduction in postherpetic neuralgia by over 88%. By 2025, Shingrix has become the standard, with universal CDC recommendations for two doses in immunocompetent adults aged 50 and older, and in immunocompromised adults aged 19 and older, following Zostavax's discontinuation in 2020 due to superior alternatives. The WHO recommends Shingrix for adults ≥50 years in high-income settings as of 2023. Long-term follow-up data from the ZOE-LTFU study indicate Shingrix retains 79.7% efficacy against shingles 6 to 11 years after vaccination in adults aged 50 and older. This durability supports current guidelines without routine boosters, though ongoing research explores additional dosing to extend protection beyond 10 years, particularly in high-risk populations.

Etymology

Origin of the Term

The English term "shingles" for the disease emerged in the late 14th century, derived from Medieval Latin cingulus, a variant of cingulum meaning "girdle" or "belt." This etymology stems from the Latin verb cingere, "to gird," capturing the rash's typical band-like distribution around the torso or other body areas. The word entered Middle English through medical texts, reflecting the observable pattern of the skin eruption that resembles a fastened belt. The medical nomenclature herpes zoster originates from ancient Greek roots. Herpes comes from herpein (ἕρπω), meaning "to creep," which describes the progressive, spreading character of the vesicular lesions along nerve paths. Zoster derives from zōstēr (ζωστήρ), denoting a "girdle" or "warrior's belt," again emphasizing the encircling, dermatomal rash. The term "herpes zoster" was first used by the Roman encyclopedist Aulus Cornelius Celsus (c. 25 BC – c. 50 AD), based on earlier classical Greek descriptions of similar skin conditions. Another historical name is "zona," borrowed from Latin zona, itself from Greek zōnē (ζώνη), signifying a "belt," "zone," or "girdle." The term gained medical usage in the 1st century AD when Roman physician Scribonius Largus linked it to herpes-like conditions, highlighting the zonal eruption pattern. In French, the disease is termed zona, preserving this classical root to denote the belt-shaped affliction.

Research

Current Studies

Recent clinical trials have extended understanding of the Shingrix vaccine's long-term efficacy, demonstrating sustained protection against herpes zoster (shingles) for over a decade. An interim analysis of long-term follow-up data from phase 3 trials indicated that Shingrix maintains efficacy of 84.0% against shingles over approximately 5.1–7.1 years of follow-up, with data extending to a mean of 5.6 to 9.6 years in adults aged 50 and older. Final analyses of the ZOE-LTFU study further confirmed efficacy of 79.7% six to 11 years after vaccination in this population. Additionally, 2025 observational data have linked Shingrix to a reduction in dementia risk, with a natural experiment showing a 3.5 percentage point absolute decrease in the probability of a new dementia diagnosis over seven years among vaccinated individuals. Innovations in antiviral therapies for shingles focus on addressing varicella-zoster virus (VZV) reactivation, particularly in complicated cases. Low-dose, long-term oral valacyclovir has shown benefits in reducing ocular complications and persistent pain in patients with herpes zoster ophthalmicus, a severe form of shingles affecting the eye, by lowering recurrence rates and improving outcomes in a 2025 study. For resistant or refractory VZV infections, emerging research explores novel formulations like GS-1, a compound of undecylenic acid and L-arginine, which inhibits viral entry and reduces symptoms and contagiousness in preclinical and early clinical evaluations as of 2025. These approaches aim to provide longer-acting options beyond standard acyclovir, though specific trials for highly resistant VZV strains remain limited. Phase 3 trials of monoclonal antibodies targeting nerve growth factor (NGF) continue to investigate their potential for postherpetic neuralgia (PHN), the chronic pain complication following shingles. Anti-NGF agents like tanezumab have demonstrated efficacy in reducing neuropathic pain in broader chronic pain studies, with pooled analyses from over 5,000 patients showing significant improvements in pain scores and function, though primarily evaluated in osteoarthritis contexts. For PHN specifically, investigational anti-NGF therapies, such as fulranumab, have been evaluated in phase 2 trials, showing potential in pain relief without FDA approval. Longitudinal population studies in 2025 have established connections between shingles vaccination and reduced cardiovascular risks. A May 2025 analysis reported a 23% relative risk reduction in major cardiovascular events, including heart attacks and strokes, among vaccinated adults compared to unvaccinated controls, based on large cohort data. Systematic reviews and meta-analyses further support this, finding 18% and 16% reductions in composite cardiovascular outcomes for recombinant zoster vaccine (RZV) and zoster vaccine live (ZVL) recipients, respectively, with stronger effects in higher-risk groups like older males. These findings underscore the vaccine's broader protective role beyond shingles prevention.

Emerging Therapies

Recent advancements in shingles research have focused on next-generation vaccines utilizing mRNA technology to enhance prevention strategies. mRNA-based vaccines targeting varicella-zoster virus (VZV) glycoproteins, such as glycoprotein E (gE), are currently in phase I/II clinical trials as of 2025, with candidates like those developed by Pfizer/BioNTech demonstrating robust immunogenicity in preclinical models. These vaccines aim to provide single-dose efficacy and broader cellular immunity, including stronger CD8+ T cell responses compared to existing recombinant zoster vaccines, potentially offering longer-lasting protection against reactivation. In mouse studies, low doses (1 µg) of lyophilized mRNA constructs elicited IgG levels and T cell activation superior to benchmarks, with stability maintained for up to 24 months under refrigeration, addressing logistical challenges in vaccine deployment. Gene editing technologies, particularly CRISPR/Cas9, represent a preclinical frontier for eradicating latent VZV reservoirs in sensory ganglia to prevent reactivation. Approaches using Staphylococcus aureus Cas9 (saCas9) delivered via adeno-associated virus (AAV2) vectors target duplicated VZV open reading frames (ORF62/71), essential for viral replication and latency maintenance. In human embryonic stem cell-derived neuron models simulating ganglionic latency, CRISPR editing reduced infectious virus production by over 100-fold upon induced reactivation and limited cell-to-cell spread, without evidence of off-target effects in neuronal cultures. Although in vivo animal models for VZV latency remain limited due to species specificity, these findings suggest potential for disrupting persistent viral genomes, paving the way for therapies that could eliminate the risk of shingles in latently infected individuals. Neuroprotective agents, including small-molecule modulators of inflammatory pathways, are under investigation to mitigate postherpetic neuralgia (PHN) by preserving neuronal integrity during acute VZV infection. Compounds like olodanrigan (EMA401), an angiotensin II type 2 receptor (AT2R) antagonist, have shown promise in phase II trials by reducing neuroinflammation and pain signaling in PHN models, though development was paused due to preclinical hepatotoxicity concerns. Similarly, LANCL2 activators such as LAT8881 target anti-inflammatory cascades to dampen glial activation and cytokine release, with early-phase studies indicating safety but mixed efficacy in preventing chronic pain progression. These agents operate via pathways that inhibit pro-inflammatory mediators like TNF-α and IL-6, offering a complementary approach to antivirals by addressing the neuropathic sequelae of shingles at the molecular level. Prophylactic long-term suppressive antiviral therapies are being evaluated in clinical trials for high-risk immunocompromised populations to suppress VZV reactivation beyond acute treatment durations. In hematopoietic cell transplantation (HCT) recipients, one-year regimens of acyclovir or valacyclovir have demonstrated significant reductions in herpes zoster incidence, with rates dropping below 1% during prophylaxis and no rebound effect observed post-discontinuation. Extended protocols, lasting until immunosuppression resolves, further lower disease occurrence but highlight the need for personalized durations, as approximately 6% of patients experienced breakthrough events in the second year. Ongoing trials emphasize low-dose oral formulations to balance efficacy with tolerability in groups like solid organ transplant recipients, aiming to integrate these with vaccination for sustained prevention. Looking toward the 2025 horizon, AI-driven predictive models are emerging to forecast shingles reactivation risk by analyzing immune biomarkers, enabling targeted interventions. Machine learning algorithms integrating multi-omics data, such as CD8+ T cell frequencies and cytokine profiles, have shown high accuracy in stratifying reactivation probabilities in herpesvirus models, with applications extending to VZV in immunocompromised cohorts. For instance, predictive scoring systems like AIRMET, validated in post-allogeneic HCT patients, incorporate biomarkers of immune reconstitution to identify late-onset risks, achieving reliable stratification for prophylactic decisions. These tools leverage temporal data on immune surveillance to simulate reactivation triggers, potentially reducing shingles burden through precision medicine.

References

  1. [1]
    About Shingles (Herpes Zoster) - CDC
    Jan 17, 2025 · Shingles is a painful rash illness. People get shingles when the varicella-zoster virus (VZV), which causes chickenpox, reactivates in their bodies.
  2. [2]
    Shingles - Symptoms & causes - Mayo Clinic
    Shingles is characterized by pain or a tingling sensation in a limited area on one side of the face or torso, followed by a red rash with small, fluid-filled ...Diagnosis & treatment · Shingles · Shingles treatment · Shingles affects the nerves
  3. [3]
    Shingles (herpes zoster) - World Health Organization (WHO)
    Mar 24, 2025 · Shingles is a painful rash caused by the reactivation of the varicella-zoster virus (VZV), the same virus that causes chickenpox.
  4. [4]
    Herpes Zoster - StatPearls - NCBI Bookshelf
    Herpes zoster, also known as shingles, is a viral syndrome caused by reactivation of the varicella-zoster virus. After an episode of varicella (chicken-pox), ...
  5. [5]
    Clinical Features of Shingles (Herpes Zoster) - CDC
    May 10, 2024 · People with herpes zoster have a rash in one or two adjacent dermatomes. The rash most commonly appears on the trunk along a thoracic dermatome ...
  6. [6]
    Clinical Overview of Shingles (Herpes Zoster) - CDC
    Jun 27, 2024 · Herpes zoster (shingles) is caused by the reactivation of varicella-zoster virus (VZV) and can be prevented with Shingrix vaccine.
  7. [7]
    Shingles Symptoms and Complications - CDC
    Apr 19, 2024 · Shingles is a painful rash illness caused by the varicella-zoster virus (VZV). Protect yourself from serious complications by getting vaccinated ...
  8. [8]
    Herpes Zoster Clinical Presentation: History, Physical Examination ...
    Mar 11, 2025 · Symptoms typically include prodromal sensory phenomena along one or more skin dermatomes lasting 1-10 days (average, 48 hours), which usually ...
  9. [9]
    Shingles Facts and Stats - CDC
    Apr 12, 2024 · Shingles (Herpes Zoster). Shingles is a painful rash illness caused by the varicella-zoster virus (VZV). Protect yourself from serious ...Key Points · Highlights · U.S. Data
  10. [10]
    Herpes zoster: A Review of Clinical Manifestations and Management
    Jan 19, 2022 · Clinical symptoms appear in three stages—pre-eruptive, acute exsudative, and chronic [12]. The pre-eruptive stage presents with burning or pain ...
  11. [11]
    Postherpetic Neuralgia - StatPearls - NCBI Bookshelf - NIH
    One month after the onset of shingles, 9 to 14.3% of patients develop postherpetic neuralgia, and at three months, this percentage becomes 5%. At one year, 3% ...Continuing Education Activity · Introduction · Epidemiology · Evaluation
  12. [12]
    Prevention of Herpes Zoster Recommendations of the ... - CDC
    May 15, 2008 · Approximately 1%--4% of zoster episodes result in hospitalization, with a mean duration of 4.8 days. (196--199). Health-care use for zoster and ...
  13. [13]
    The Incidence of Herpes Zoster Complications - PubMed Central - NIH
    The relative incidence of disseminated HZ was 0.3–8.2% in the general population, 0–0.5% in the immunocompetent, and 0–20.6% in patients with comorbidities.
  14. [14]
    Herpes Zoster Ophthalmicus - StatPearls - NCBI Bookshelf
    Sep 14, 2025 · Prolonged inflammation and corneal scarring can lead to serious complications, including permanent vision loss. Neurotrophic keratopathy ...
  15. [15]
    Varicella Virus-Host Interactions During Latency and Reactivation
    Following primary infection, VZV establishes latency in the sensory ganglia and can reactivate to cause herpes zoster, more commonly known as shingles, which ...Abstract · Simian Varicella Virus... · The Important Role of T Cells...Missing: lifecycle pathophysiology
  16. [16]
    https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3176736/
  17. [17]
    Repression of varicella zoster virus gene expression during ...
    This phase of infection is characterized by restricted viral gene expression, lack of detectable protein and no infectious viral particles. Upon reactivation, ...
  18. [18]
    Mechanisms of Pain and Itch Caused by Herpes Zoster (Shingles)
    It is here that VZV lies dormant until reactivation during zoster. Newly synthesized viral particles undergo axonal transport along the central and distal axons ...
  19. [19]
    Immunobiology of Varicella-Zoster Virus Infection - Oxford Academic
    Sep 22, 2018 · Antibodies prevent primary VZV infection, whereas T cells are fundamental to resolving disease, limiting severity, and preventing reactivation.
  20. [20]
    Risk Factors for Herpes Zoster Infection: A Meta-Analysis - PMC
    Herpes zoster (HZ) or shingles, as its commonly known, results from reactivation of the varicella zoster virus (VZV), which lies dormant in the spinal and ...
  21. [21]
    Herpes Zoster Risk in Immunocompromised Adults in the United ...
    Abstract. Background. The primary reported risk factors for herpes zoster (HZ) include increasing age and immunodeficiency, yet estimates of HZ risk by ...
  22. [22]
    https://pmc.ncbi.nlm.nih.gov/articles/PMC8012754/
  23. [23]
    Risk Factors for Herpes Zoster Among Adults - Oxford Academic
    Jun 11, 2016 · APPENDIX. Questions asked to inquire about potential risk factors for herpes zoster. Ever family history of shingles? Yes No. If yes, who ( ...
  24. [24]
    Children vaccinated against varicella less likely to get herpes zoster
    Jun 10, 2019 · Children's rates of herpes zoster (shingles) were 78% lower when they had been vaccinated against varicella (chickenpox), according to a new study.
  25. [25]
    Shingles - Diagnosis & treatment - Mayo Clinic
    Health care providers usually diagnose shingles based on the history of pain on one side of your body, along with the telltale rash and blisters.Symptoms & causes · Shingles and alcohol · Shingles · Shingles affects the nerves
  26. [26]
    Laboratory Testing for Varicella-Zoster Virus (VZV) - CDC
    May 10, 2024 · PCR is the most useful laboratory test for confirming suspected varicella and herpes zoster. PCR can detect VZV DNA rapidly and sensitively in skin lesions.
  27. [27]
    Herpes Zoster Workup - Medscape Reference
    Mar 11, 2025 · Both DFA and PCR have far greater sensitivity and specificity than the Tzanck smear and allow differentiation between herpes simplex virus ...
  28. [28]
    Laboratory diagnosis of herpes zoster - ScienceDirect.com
    PCR results confirmed the clinical diagnosis of zoster in 95%. Primers selected from varicella-zoster virus (VZV) gene 28 proved to be most sensitive.
  29. [29]
    Efficacy of an Adjuvanted Herpes Zoster Subunit Vaccine in Older ...
    Apr 28, 2015 · Zostavax showed 51.3% efficacy against herpes zoster and 66.5% efficacy against postherpetic neuralgia in participants who were 60 years of age ...
  30. [30]
    [PDF] ZOSTAVAX (Zoster vaccine Live) Refrigerated Package Insert - FDA
    Efficacy of ZOSTAVAX was evaluated in the Shingles Prevention Study (SPS), a placebo-controlled, double-blind clinical trial in which 38,546 subjects 60 years ...<|control11|><|separator|>
  31. [31]
    [PDF] Package Insert - SHINGRIX - FDA
    Do not administer SHINGRIX to anyone with a history of a severe allergic reaction (e.g., anaphylaxis) to any component of the vaccine or after a previous dose ...
  32. [32]
    [PDF] Shingrix, INN-Herpes zoster vaccine (recombinant, adjuvanted)
    By combining the VZV specific antigen (gE) with an adjuvant system (AS01B), Shingrix is designed to induce antigen-specific cellular and humoral immune ...
  33. [33]
    Herpes Zoster Vaccine Guidance: For Providers - CDC
    Information about Shingrix vaccine composition, dosage, and administration, and vaccine efficacy, duration of protection, reactogenicity
  34. [34]
    Clinical Considerations for Shingrix Use in Immunocompromised ...
    Jul 9, 2024 · ACIP recommends 2 doses of recombinant zoster vaccine (RZV, Shingrix) for the prevention of shingles and related complications in adults aged ≥19 years.
  35. [35]
    Vaccination to Prevent Shingles - U.S. Pharmacist
    Feb 19, 2025 · In adults aged 50 years and older, Shingrix was 91% effective in preventing PHN, and in those aged 70 years and older, it was 89% effective. • ...
  36. [36]
    A natural experiment on the effect of herpes zoster vaccination on ...
    Apr 2, 2025 · We show that receiving the zoster vaccine reduced the probability of a new dementia diagnosis over a follow-up period of 7 years by 3.5 percentage points.
  37. [37]
    Study strengthens link between shingles vaccine and lower ...
    more than any ...
  38. [38]
    Healthy ageing: Herpes zoster infection and the role of zoster ... - NIH
    Nov 28, 2023 · Vaccination as a preventive strategy should span the life course, including adults and older adults as well as children23, and life-course ...Healthy Ageing · Herpes Zoster · Recombinant Zoster Vaccine<|control11|><|separator|>
  39. [39]
    Shingles Immunity and Health Functioning in the Elderly: Tai Chi ...
    Dec 1, 2004 · Tai chi chih (TCC), results in improvements in health functioning and immunity to VZV in older adults as compared with a control group.Missing: diet | Show results with:diet
  40. [40]
    Immune Alterations with Aging: Mechanisms and Intervention ...
    (1) Lifestyle interventions include adjustments in diet, exercise, and sleep patterns. (2) Pharmacological interventions encompass anti-inflammatory drugs ...<|separator|>
  41. [41]
    Perceived psychological stress and risk of herpes zoster
    Psychological stress may reduce cellular immunity, but its role in triggering latent infections, including herpes zoster (HZ), is controversial.Missing: trauma | Show results with:trauma
  42. [42]
    Shingles and Stress: Is There a Connection? - Healthline
    May 25, 2016 · Shingles, or herpes zoster, is a common viral infection. It causes a large, painful rash with blisters. The rash usually appears on one side of ...Missing: female | Show results with:female
  43. [43]
    Corticosteroid Use and Risk of Herpes Zoster in a Population-Based ...
    The risk of zoster was 59% higher in those using systemic corticosteroids (adjusted hazard ratio [aHR], 1.59; 95% CI, 1.48 to 1.71) and greater with higher ...
  44. [44]
    Associations of Lifestyle and Anthropometric Factors With the Risk of ...
    The role of lifestyle in development of herpes zoster remains unclear. We examined whether smoking status, alcohol consumption, body mass index, or physical ...
  45. [45]
    Chickenpox Vaccine and Shingles Risk - HistoryOfVaccines.org
    Jun 12, 2019 · New evidence was published showing that children who receive the two recommended doses of the chickenpox vaccine are less likely to develop shingles later in ...
  46. [46]
    Preventing VZV Transmission in Healthcare Settings - CDC
    Apr 19, 2024 · Determine the best ways to prevent the spread of shingles (herpes zoster) in healthcare settings and among healthcare personnel.
  47. [47]
    Treatment of herpes zoster - UpToDate
    May 9, 2025 · Antiviral therapy · - Goals of therapy · - Indications · Patients who present within 72 hours of onset · Limited role for adjunctive therapies ...
  48. [48]
    Low-Dose Valacyclovir in Herpes Zoster Ophthalmicus
    This randomized clinical trial investigates if 1 year of suppressive treatment for herpes zoster ophthalmicus with valcyclovir compared with placebo.
  49. [49]
    Long-Term Antivirals Reduce HZO Eye Complications
    Feb 1, 2025 · An extended, low-dose course of the antiviral medication valacyclovir reduced the risk of ocular complications associated with shingles ...
  50. [50]
    Herpes Zoster Treatment & Management - Medscape Reference
    Mar 11, 2025 · Conservative therapy includes nonsteroidal anti-inflammatory drugs (NSAIDs); wet dressings with 5% aluminum acetate (Burow solution), applied for 30-60 minutes ...
  51. [51]
    Herpes Zoster and Postherpetic Neuralgia: Prevention and ... - AAFP
    Nov 15, 2017 · Testing is typically not needed, but it may be considered in patients with recurring lesions that are suspicious for herpes simplex, or in those ...
  52. [52]
    S2k guidelines for the diagnosis and treatment of herpes zoster and ...
    Jan 17, 2020 · Analgesic treatment of nociceptive pain based on the WHO's pain relief ladder is recommended (Figure 2). Mild pain intensity: NSAIDs or ...
  53. [53]
    Postherpetic neuralgia: epidemiology, pathophysiology, and pain ...
    Sep 21, 2016 · It stems from damage to peripheral and central neurons that may be a byproduct of the immune/inflammatory response accompanying varicella zoster ...
  54. [54]
    Modalities in managing postherpetic neuralgia - PMC
    Oct 1, 2018 · Anticonvulsants, antidepressants, topical therapies including lidocaine and capsaicin, and opioids, are the most widely used therapies for the treatment of PHN.
  55. [55]
    Diagnosing and Managing Postherpetic Neuralgia - PMC
    First-line therapies for PHN include tricyclic antidepressants, gabapentin and pregabalin, and the lidocaine 5 % patch.
  56. [56]
    Herpes Zoster Ophthalmicus - EyeWiki
    Jun 8, 2025 · Management. General Treatment. Skin rash treatment should prevent ... A clinical report on herpes zoster ophthalmicus (shingles affecting the ...
  57. [57]
    How to manage herpes zoster ophthalmicus - PMC - NIH
    Mar 30, 2020 · Treatment includes intravenous aciclovir 10–15 mg/kg for 2 weeks, followed by oral valaciclovir 1 g three times daily for a further 6 weeks.
  58. [58]
    Herpes Zoster Ophthalmicus - American Academy of Ophthalmology
    Jan 1, 2020 · The standard treatment for HZ is antiviral medication, preferably initiated within 72 hours of rash onset.1 Antivirals reduce pain, speed rash- ...
  59. [59]
    Ramsay Hunt Syndrome - StatPearls - NCBI Bookshelf - NIH
    Herpes zoster is generally self-limiting in nature. · High-dose corticosteroids, either oral or intravenous, should be co-administered with antiviral treatment.Continuing Education Activity · Introduction · Treatment / Management · Prognosis
  60. [60]
    Ramsay Hunt syndrome - Diagnosis & treatment - Mayo Clinic
    Treatment of herpes zoster in the immunocompetent host. https://www.uptodate ... Ramsay Hunt syndrome - Diagnosis & treatment - Mayo Clinic ...
  61. [61]
    Antiviral therapy for Ramsay Hunt syndrome (herpes zoster oticus ...
    The standard first‐line treatment for herpes zoster infections at sites in the body other than the ear is the anti‐viral agent acyclovir, which is given either ...
  62. [62]
    Low-Dose Valacyclovir in Herpes Zoster Ophthalmicus - PubMed
    Apr 1, 2025 · Importance: High-quality evidence regarding suppressive valacyclovir treatment in herpes zoster ophthalmicus (HZO) is necessary to guide care.Missing: long- | Show results with:long-
  63. [63]
    Long-term, low-dose antiviral treatment benefits patients with eye ...
    Oct 24, 2024 · New research suggests long-term, low-dose antiviral treatment reduces the risk for potentially vision-damaging bouts of shingles-related eye inflammation.
  64. [64]
    Topical and Systemic Therapeutic Approaches in the Treatment of ...
    Sep 1, 2025 · 60% recurrence-free in valacyclovir group vs. 38% in placebo (p = 0.041); time to first recurrence longer with valacyclovir (13.1 vs. 9.6 ...<|control11|><|separator|>
  65. [65]
    Shingles | Johns Hopkins Medicine
    Skin sensitivity, tingling, itching, or pain in the area of the skin before the rash appears · Rash. The rash usually shows up 1 to 5 days after symptoms start.Missing: rates | Show results with:rates
  66. [66]
    Acute Herpes Zoster and Postherpetic Neuralgia
    The initial HZ rash resolves typically in 2-4 weeks. Despite treatment, approximately 20% of patients over the age of 60 years will develop persistent pain 6 ...
  67. [67]
    Postherpetic neuralgia in the elderly - PMC - NIH
    PHN persisting at 3 months may occur in 10–20% of HZ patients aged > 50 years (15,19–21). Other less frequently occurring complications may be neurological ( ...
  68. [68]
    Herpes Zoster Recurrence: A Narrative Review of the Literature - PMC
    Feb 28, 2024 · Recognized risk factors for HZ recurrence include immunocompromised status, female sex, family history, and comorbidities such as diabetes.
  69. [69]
    Herpes Zoster and Recurrent Herpes Zoster - PMC - NIH
    The incidence of recurrent herpes zoster (HZ) and the relationship between initial and recurrent HZ are not clear. The Miyazaki Dermatologist Society has ...Missing: adjacent | Show results with:adjacent
  70. [70]
    Shingles Scars: Why They Happen and How to Prevent Them
    May 9, 2025 · It's possible for shingles to cause permanent scarring and skin discoloration, though this is often minor. If you develop shingles, it's ...
  71. [71]
    Herpes Zoster Ophthalmicus Clinical Presentation and Risk Factors ...
    Feb 8, 2021 · Purpose: To determine the rate of moderate and severe vision loss following herpes zoster ophthalmicus (HZO) and to identify associated factors.
  72. [72]
    Incidence of Herpes Zoster Among Children: 2003–2014 - PMC
    Jun 10, 2019 · Another reported rate among US 0- to 14-year-olds before vaccine introduction was 46 per 100 000. In our study, pediatric HZ incidence rates in ...
  73. [73]
    The Incidence of Herpes Zoster in a United States Administrative ...
    HZ rates rose sharply with age, and were highest among individuals over age 80 (10.9 per 1,000 person-years) (95% CI, 10.2 to 11.6). The incidence of HZ per ...
  74. [74]
    Study Data | SHINGRIX (Zoster Vaccine Recombinant, Adjuvanted)
    SHINGRIX delivered greater than 90 percent efficacy against shingles. graphic Data from ZOE-50 and pooled analysis from ZOE-50/-70.
  75. [75]
    A systematic review and meta-analysis of risk factors for postherpetic ...
    PHN is the most common complication of zoster; an estimated 12.5% of patients with zoster aged ≥50 years have PHN 3 months after zoster onset, and the ...
  76. [76]
    A systematic literature review of herpes zoster incidence worldwide
    Incidence rates were 6.6–9.03 per 1,000 person-years for North America, 5.23–10.9 per 1,000 person-years for Europe and 10.9 per 1,000 person-years in the Asia- ...
  77. [77]
    Systematic review of incidence and complications of herpes zoster
    Hospitalisation rates ranged from 2 to 25/100 000 person-years, with higher rates among elderly populations. Conclusions HZ is a significant global health ...Incidence Rates Of Hz · Risk Of Phn · Discussion
  78. [78]
    Herpes zoster and HIV-1 infection in a rural Ugandan cohort
    Aug 5, 2025 · The cumulative incidence of a first episode of herpes zoster was 7.6% at 2 years, 12.6% at 4 years and 24.0% at 6 years after seroconversion; ...<|separator|>
  79. [79]
    https://bmjopen.bmj.com/content/4/6/e004833
  80. [80]
    Zeroing in on zoster: a tale of many disorders produced by one virus
    Because the name herpes zoster is so descriptive, it is likely that ancient physicians recognized the dermatomal distribution of disease. The word “shingles” ...
  81. [81]
    Zeroing in on zoster: A tale of many disorders produced by one virus
    Nov 15, 2015 · ... herpes zoster (shingles) after reactivation of latent VZV. ... Hippocrates first used the word to describe an ulcerative skin lesion that ...
  82. [82]
    The legacy of William Heberden the Elder (1710–1801)
    Aug 7, 2025 · In the 20th century, varicella zoster virus (VZV) was shown to cause varicella upon primary (first-time) infection and herpes zoster (shingles) ...
  83. [83]
    Did William Heberden Distinguish Chickenpox From Smallpox in ...
    Jan 3, 2022 · “While herpes zoster infection has been recognized since antiquity, chickenpox (varicella) ... 1768, Heberden described the clinical ...
  84. [84]
    Shingles - Hektoen International
    Feb 27, 2025 · Von Bokay first described the relationship between chickenpox and herpes zoster in 18928 and more fully in 1909. The chickenpox varicella–zoster ...
  85. [85]
    Chickenpox - an overview | ScienceDirect Topics
    In 1909 Von Bokay suggested that chickenpox and shingles were related infections, an idea that was experimentally confirmed in the 1920s and 1930s when children ...
  86. [86]
    Thomas H. Weller – Biographical - NobelPrize.org
    In virology his studies of varicella and herpes zoster resulted in his isolation for the first time of the viruses responsible for these diseases, and also in ...Missing: VZV | Show results with:VZV
  87. [87]
    Introduction - Varicella-Zoster Virus - Cambridge University Press
    In 1953, in addition to isolating VZV from cases of chickenpox and zoster, Dr. Weller was able to show that the same virus is responsible for both illnesses.Missing: shingles | Show results with:shingles
  88. [88]
    THE ETIOLOGIC AGENTS OF VARICELLA AND HERPES ZOSTER
    THE ETIOLOGIC AGENTS OF VARICELLA AND HERPES ZOSTER. ISOLATION, PROPAGATION, AND CULTURAL CHARACTERISTICS IN VITRO. Thomas H Weller. Thomas H Weller. 1 ...Missing: VZV | Show results with:VZV
  89. [89]
    Live Attenuated Varicella Vaccine: Prevention of ... - Oxford Academic
    Sep 30, 2021 · Michiaki Takahashi developed the live attenuated varicella vaccine in 1974. This was the first, and is still the only, herpesvirus vaccine.
  90. [90]
    Shingrix: A New Herpes Zoster Vaccine - PMC - NIH
    The original herpes zoster vaccine, Zostavax® or Zoster Vaccine Live (ZVL), was approved in 2006. However, the efficacy of ZVL in preventing herpes zoster ...
  91. [91]
    Efficacy of the Herpes Zoster Subunit Vaccine in Adults 70 Years of ...
    Sep 15, 2016 · In our trial, HZ/su was found to reduce the risks of herpes zoster and postherpetic neuralgia among adults 70 years of age or older.
  92. [92]
    Shingles Vaccination | Shingles (Herpes Zoster) - CDC
    Aug 19, 2025 · Shingles is a painful rash illness caused by the varicella-zoster virus (VZV). Protect yourself from serious complications by getting vaccinated ...
  93. [93]
    New long-term data show Shingrix continues to provide high ... - GSK
    Apr 17, 2024 · End-of-trial data show 79.7% efficacy in participants aged 50 years and over, six to 11 years after vaccination.
  94. [94]
    Shingles - Etymology, Origin & Meaning
    Originating from Medieval Latin cingulus, meaning "girdle," this term denotes an inflammatory skin disease named for its belt-like spread around the body.
  95. [95]
    shingles - Middle English Compendium - University of Michigan
    Etymology, From ML cingulus herpes (var. of L cingulum) or pl. of OF cengle ... A skin disease, prob. herpes zoster, characterized by eruptions and a ...
  96. [96]
    Zoster - Etymology, Origin & Meaning
    Shingles, from Latin herpes zoster and Greek zōstēr meaning "girdle" or "warrior's belt," refers to a viral infection causing a painful skin rash.<|control11|><|separator|>
  97. [97]
    Whence 'zoster'? The convoluted classical origins of a ... - PubMed
    But in antiquity the meaning of 'zoster', a Latin word originating from the Greek for a belt or girdle, was variously associated in men with a form of body ...Missing: disease | Show results with:disease
  98. [98]
    https://www.etymonline.com/word/shingles
  99. [99]
    GSKpro Efficacy | SHINGRIX
    SHINGRIX has demonstrated protection against shingles that lasts for up to 10 years post vaccination (range 5.6 to 9.6 years) in an interim analysis of a long ...
  100. [100]
    Final analysis of the ZOE-LTFU trial to 11 years post-vaccination
    ZOE-LTFU started approximately 5 years post-vaccination in ZOE-50/70 and participants were followed for 6 years. The primary objective was to assess vaccine ...
  101. [101]
    New formula may reduce shingles and cold sore pain - Medical Xpress
    May 6, 2025 · Researchers have developed a new treatment formula—known as GS-1—that could reduce the symptoms and contagiousness of the viruses behind ...
  102. [102]
    Pooled Analyses of Phase III Clinical Studies in Over 5000 Patients ...
    Jul 18, 2023 · Background: Tanezumab, a humanized anti-nerve growth factor antibody, was developed for the treatment of pain associated with osteoarthritis.Missing: postherpetic 2025
  103. [103]
    Investigational Drugs for the Treatment of Postherpetic Neuralgia
    Aug 20, 2023 · Despite several Phase II and III trials showed positive efficacy results using anti-NGF molecules (such as tanezumab), there is not any FDA- ...
  104. [104]
    Shingles vaccine may reduce dementia, heart disease risk by 50%
    Oct 23, 2025 · For example, a study published in May 2025 found that the shingles vaccine may help lower a person's risk for cardiovascular events by 23%. And ...
  105. [105]
    New systematic review and meta-analysis shows an association ...
    Aug 28, 2025 · The research found that vaccination against shingles, with either RZV or ZVL, was associated with an 18% and 16% reduction in risk of ...Missing: boosters | Show results with:boosters
  106. [106]
    A highly stable lyophilized mRNA vaccine for Herpes Zoster ... - Nature
    Mar 14, 2025 · Some of these investigational VZV modRNA candidates, including a lyophilized presentation, are currently being tested in a Phase I/II clinical ...
  107. [107]
    NCT05703607 | A Study to Learn About a Modified RNA Vaccine ...
    This substudy is the Phase 1 portion of the study. In this substudy, participants will receive 1 of 3 VZV modRNA vaccine candidates (different construct ...Missing: mRNA- | Show results with:mRNA-
  108. [108]
    Antiviral Targeting of Varicella Zoster Virus Replication and ...
    Feb 12, 2022 · A goal of VZV targeting by gene editing is to reduce the capacity of latent genomes to reactivate and induce zoster disease, not only by ...
  109. [109]
    https://www.escardio.org/The-ESC/Press-Office/Press-releases/New-systematic-review-and-meta-analysis-shows-an-association-between-shingles-vaccination-and-lower-risk-of-heart-attack-and-stroke
  110. [110]
    One-year acyclovir prophylaxis for preventing varicella-zoster virus ...
    In conclusion, acyclovir/valacyclovir prophylaxis given for 1 year led to a persistent benefit after drug discontinuation and no evidence of a rebound effect.
  111. [111]
    Prevention of herpes zoster in acquired immunocompromised ... - NIH
    Mar 10, 2025 · Antiviral prophylactic medications and vaccinations are critical tools in preventing HZ in IC patients, as outlined in Table 1. Despite their ...
  112. [112]
    The Role of Artificial Intelligence in Herpesvirus Detection ...
    Predicting Viral Persistence and Reactivation Triggers: AI models can also predict what conditions might trigger the reactivation of latent herpesvirus ...Missing: shingles | Show results with:shingles
  113. [113]
    P1507: A PREDICTIVE MODEL OF HERPES ZOSTER AFTER ...
    A predictive model (AIRMET) was developed and validated, and this is the first scoring system predicting the incidence of late HZ after allo-HSCT.Missing: emerging | Show results with:emerging