Herpes simplex virus: Difference between revisions

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* Similar to other patients, asymptomatic shedding is also common, especially for 2 to 3 weeks after grafting
* Similar to other patients, asymptomatic shedding is also common, especially for 2 to 3 weeks after grafting


=== Pregancy ===
=== Pregnancy ===
* See [[HSV in pregnancy]]
* See [[HSV in pregnancy]]



Revision as of 02:13, 17 October 2019

  • Comprises herpes simplex virus 1 (HSV-1) and HSV-2, which are members of the Human herpesvirus family
  • Cause typical painful vesicular lesions on labia or external genitals
  • Occasionally cause a viral encephalitis

Background

Microbiology

  • Enveloped, double-stranded DNA virus
  • HSV-1 and HSV-2 are morphologically and genetically distinct viruses
  • Can be infected with both

Epidemiology

  • Worldwide distribution, and only found in humans
    • Most common cause of genital lesions
    • Most common cause of acute viral encephalitis in the US, with age peaks at 5 to 30 years and over 50 years
  • Spread through person-to-person contact with skin or mucosa; not spread via fomits
  • HSV-1 has seroprevalence of 50-90% among Canadian adults1
    • Often acquired in childhood in Asia and Africa
    • More common in lower SES populations
  • HSV-2 has seroprevalence of 15-20% in Canada1
    • More common in women than men, in HIV-infected people, and in MSM
    • May be subclinical if already infected with HSV-1

Pathophysiology

  • Fusion of envelope and cell membrane is mediated by viral glycoproteins B, C, and D and host cell proteins cellular heparin sulfate, TNF receptors, and immunoglobulins
  • Internal capsid is released, which makes its way to the nucleus
  • Viral DNA polymerase enzyme and viral DNA helicase are targets of antivirals
  • Viral DNA may remain latent in about 10% of nearby neurons, characterized by latency-associated transcripts (LATs)
    • Despite being latent, virus can still be shed in mucosa anywhere from 1/10 to 3/4 of days
  • HSV-1 prefers trigeminal ganglia as well as cervical ganglia, or sacral nerve root ganglia if genital

Clinical Presentation

Primary infection

  • Incubation period usually within 5 days for primary infection
  • Mucocutaneous lesiosn may become secondarily infected

Orofacial infection

  • Most common sites of primary infection are gingivostomatitis and pharyngitis
    • Includes lesions on hard and soft palate, gingiva, tongue, lips, and face
    • Pharyngeal lesions may be exudative or ulcerative
  • May also have malaise, myalgias, anorexia or odynophagia, and cervical lymphadenopathy
  • Self-resolving after 3 to 14 days
  • Can cause a Bell palsy

Genital infection

  • Genital lesions typically last 10 to 12 days, especially with first episode
    • Often widely spaced bilateral lesions
    • First episode often also involves fever, headache, malaise, and myalgias
    • May have pain, itching, dysuria, genital discharge, and inguinal lymphadenopathy
  • May develop extragenital sites of infection, including buttock, groin, and thigh with HSV-2 and perioral area with HSV-1
    • Rarely fingers and eyes
    • Develop around 14 days into the disease, likely from autoinoculation
  • HSV-2 genital infections are less severe if the person has had HSV-1
  • 12-month recurrence rate is up to 90% for HSV-2 and 55% for HSV-1
Neurological complications
  • These can include aseptic meningitis, transverse myelitis, and sacral radiculopathy
  • Typically occur in conjunction with first episode of genital HSV-2 infection
  • Aseptic meningitis
    • Mengitis is more common with HSV-2 than HSV-1
    • Often concurrent with primary genital infection, typically 3 to 12 days after start of symptoms
    • HSV-2 may also cause Mollaret's meningitis (benign recurrent lymphocytic meningitis)
  • Autonomic dysfunction
    • May have hyperesthesia or anaesthesia of perineum, lumbar or sacrum, as well as urinary retention and constipation
    • Resolves over 4 to 8 weeks
  • Transverse myelitis
    • Decreased strength and deep tendon reflexes in lower extremities in conjunction with autonomic dysfunction (as above)
Pelvic inflammatory disease
  • Rare cause of PID, possibly representing dual infection with a typical bacterial copathogen
Disseminated disease
  • Rarely can disseminate
  • Can be cutaneous, with concurrent meningitis, hepatitis, and pneumonitis
  • Can also involve monocular arthritis, thrombocytopenia, adrenal necrosis, and myoglobinuria
  • Patient factors include primary genital HSV in pregnancy, reactivation of genital HSV in a patient with cellular immunocompromise

Reactivation

  • Typically localized to a single mucocutaneous area
  • Symptoms are usually more minor than first-episode or primary infection, and include itching and pain
    • Lesions may be atypical, with fissures and unusual ulcers
    • May be subclinical, with intermittent viral shedding
    • May be preceded by a prodrome of tingling up to 2 days
  • Average duration of an episode of reactivation orolabial herpes is 5 days
  • HSV-1 reactivates more frequently around mouth, and HSV-2 in genitals
  • Frequency
    • HSV-2 reactivates on average 4 to 5 times annually, with a gradual decrease over time

Herpetic whitlow

  • HSV infection of the finger, with acute onset swelling, pain, and tenderness with vesicles
  • Also fever and regional lymphadenopathy
  • Can be either acquired from parson-to-person exposure or through autoinoculation
  • Higher rates in healtcare settins

Herpes gladiatorum

  • Herpes simplex infection essentially anywhere on the body (chest, ears, face, and hands) associated with wrestling

Ocular herpes

  • Keratitis, which presents with pain, blurred vision, chemosis, conjunctivitis, and corneal lesions
  • May also cause blepharitis and conjunctivitis
  • May cause chorioretinitis in infants and immunocompromised
  • Acute necrotizing retinitis
    • Presents with painless vision loss in immunocompetent people as well as immunocompromised
    • 25% of cases are bilateral

Encephalitis

  • Most commonly caused by HSV-1 (05% of cases)
  • In children, it is often during primary infection
  • Less clear in adults, where it may be primary, infection with a new strain, or reactivation of latent infection
  • Characterized by acute onset fever and neurologic symptoms
    • Often affects temporal lobe, with behaviour changes

Visceral/pulmonary herpes

  • Can disseminate hematogenously to organs
  • Includes esophagus, lung, and liver most commonly
  • Esophagitis is more common in patients with advanced HIV
    • Symptoms include odynophagia, dysphagia, chest pain, and weight loss
  • Pneumonitis may occur in patients with immunodupression
    • Focal necrotizing pneumonitis or bilateral interstitial pneumonitis, depending on pattern of spread
    • 80% mortality
  • Hepatitis is rare but can be quite severe
    • May also have fever, leukopenia, and DIC

HIV coinfection

  • HSV, and specifically HSV-2, may be persistent in HIV coinfection
  • HSV-2 also predisposes to HIV infection
  • There is more frequent asymptomatic shedding of HSV, inversely proportional to CD4 count
  • Frequency of lesions is lower on ART

Other immunocompromised patients

  • Higher risk for severe HSV infections in organ transplantation, chemotherapy, malnutrition, or severe burns or eczema
  • In these patients, it can disseminate to adrenals, liver, bone marrow, and GI tract
  • Can also develop oropharyngeal and esophageal lesions
    • May be difficult to distinguish from chemotherapy mucositis
  • Similar to other patients, asymptomatic shedding is also common, especially for 2 to 3 weeks after grafting

Pregnancy

Neonatal herpes

  • Can be acquired perinatally even without active lesions
    • Mostly HSV-2
    • Rarely can be congenital, with microcephaly, hydrocephalus, and chorioretinitis
  • High risk for disseminated disease, including CNS in 70% of cases
  • Requires prolonged treatment, with initial IV acyclovir for 21 days followed by 6 months of oral

Diagnosis

  • Serology
    • Species-specific HSV-1 and HSV-2 antibody assays, most commonly to glycoproteins gG1 and gG2
    • Antibodies will be positive life-long, though you can use acute and convalescent titres for diagnosis of primary infection (not helpful for reactivation)
  • Molecular tests
    • PCR is current standard, given its high sensitivity
  • Viral culture
  • Histology, with Wright, Giemsa, or Papanicolaou stains that show giant cells or intranuclear inclusions that are typical of HSV

Management

Genital and rectal herpes

Stomatitis

Esophagitis

Herpes labialis prophylaxis

Encephalitis and meningitis

  • Acyclovir 10 mg/kg IV q8h for 21 days
  • Duration 21 days for encephalitis or 7 to 10 days for meningitis
  • In neonates, this is followed by oral suppressive therapy

Ocular infections

  • Consult Ophthalmology

Immunosuppressed patients

  • HSV seropositive transplant patients: Acyclovir 5 mg/kg IV q8h for 7 days, followed by 200 to 400 mg po 3-5x/day for 1 to 3 months
  • HIV patients: acyclovir 400 to 800 mg po bid to tid, valacyclovir 500 mg po daily, or famciclovir 500 mg po bid
  • Burn patients: acyclovir 5 mg/kg IV q8h for 7 days, followed by 200 mg po 5x/day for 7 to 14 days

Acyclovir resistance

  • If unresponsive to acyclovir, consider foscarnet 40 to 80 mg/kg IV q8h until clinical resolution
  • Can try cidofovir 5 mg/kg once weekly if severe infection

References

  1. a b  M. Howard, J. W. Sellors, D. Jang, N. J. Robinson, M. Fearon, J. Kaczorowski, M. Chernesky. Regional Distribution of Antibodies to Herpes Simplex Virus Type 1 (HSV-1) and HSV-2 in Men and Women in Ontario, Canada. Journal of Clinical Microbiology. 2003;41(1):84-89. doi:10.1128/jcm.41.1.84-89.2003.