Herpes simplex virus: Difference between revisions
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* |
*Comprises herpes simplex virus 1 (HSV-1) and HSV-2, which are members of the [[Herpesviridae]] family |
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* |
*Cause typical painful vesicular lesions on labia or external genitals |
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* |
*Occasionally cause a viral encephalitis |
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== |
==Background== |
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=== |
===Microbiology=== |
||
* Enveloped, double-stranded DNA virus |
|||
* HSV-1 and HSV-2 are morphologically and genetically distinct viruses |
|||
* Can be infected with both |
|||
*Enveloped, double-stranded DNA virus |
|||
=== Epidemiology === |
|||
*HSV-1 and HSV-2 are morphologically and genetically distinct viruses |
|||
* Worldwide distribution, and only found in humans |
|||
*Can be infected with both |
|||
** 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 adults[[CiteRef::howard2003re]] |
|||
** Often acquired in childhood in Asia and Africa |
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** More common in lower SES populations |
|||
* HSV-2 has seroprevalence of 15-20% in Canada[[CiteRef::howard2003re]] |
|||
** More common in women than men, in HIV-infected people, and in MSM |
|||
** May be subclinical if already infected with HSV-1 |
|||
===Mechanisms of Resistance=== |
|||
=== 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 |
|||
*'''Resistance''' to acyclovir is usually conferred by a deficiency in thymidine kinase (which phosphorylates acyclovir) |
|||
== Clinical Presentation == |
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**Will also be resistant to valacyclovir and famciclovir |
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=== |
===Epidemiology=== |
||
* Incubation period usually within 5 days for primary infection |
|||
* Mucocutaneous lesiosn may become secondarily infected |
|||
*Worldwide distribution, and only found in humans |
|||
==== Orofacial infection ==== |
|||
* |
**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 |
|||
** Includes lesions on hard and soft palate, gingiva, tongue, lips, and face |
|||
*Spread through person-to-person contact with skin or mucosa; not spread via fomits |
|||
** Pharyngeal lesions may be exudative or ulcerative |
|||
*HSV-1 has seroprevalence of 50-90% among Canadian adults[[CiteRef::howard2003re]] |
|||
* May also have malaise, myalgias, anorexia or odynophagia, and cervical lymphadenopathy |
|||
**Often acquired in childhood in Asia and Africa |
|||
* Self-resolving after 3 to 14 days |
|||
**More common in lower SES populations |
|||
* Can cause a [[Bell palsy]] |
|||
*HSV-2 has seroprevalence of 15-20% in Canada[[CiteRef::howard2003re]] |
|||
**More common in women than men, in HIV-infected people, and in MSM |
|||
**May be subclinical if already infected with HSV-1 |
|||
=== |
===Pathophysiology=== |
||
* 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 |
|||
*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 |
|||
===== Neurological complications ===== |
|||
*Internal capsid is released, which makes its way to the nucleus |
|||
* These can include aseptic meningitis, transverse myelitis, and sacral radiculopathy |
|||
*Viral DNA polymerase enzyme and viral DNA helicase are targets of antivirals |
|||
* Typically occur in conjunction with first episode of genital HSV-2 infection |
|||
*Viral DNA may remain latent in about 10% of nearby neurons, characterized by latency-associated transcripts (LATs) |
|||
* '''Aseptic meningitis''' |
|||
**Despite being latent, virus can still be shed in mucosa anywhere from 1/10 to 3/4 of days |
|||
** Mengitis is more common with HSV-2 than HSV-1 |
|||
*HSV-1 prefers trigeminal ganglia as well as cervical ganglia, or sacral nerve root ganglia if genital |
|||
** 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) |
|||
==Clinical Manifestations== |
|||
===== Pelvic inflammatory disease ===== |
|||
* Rare cause of PID, possibly representing dual infection with a typical bacterial copathogen |
|||
===Primary Infection=== |
|||
===== 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 |
|||
*Incubation period usually [[Usual incubation period::within 5 days]] for primary infection |
|||
=== Reactivation === |
|||
*Mucocutaneous lesiosn may become secondarily infected |
|||
* 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 |
|||
=== |
====Orofacial Infection==== |
||
* 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 |
|||
*Most common sites of primary infection are gingivostomatitis and pharyngitis |
|||
=== Herpes gladiatorum === |
|||
**Includes lesions on hard and soft palate, gingiva, tongue, lips, and face |
|||
* Herpes simplex infection essentially anywhere on the body (chest, ears, face, and hands) associated with wrestling |
|||
**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==== |
||
* '''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 |
|||
*Genital lesions typically last 10 to 12 days, especially with first episode |
|||
=== Encephalitis === |
|||
**Often widely spaced bilateral lesions |
|||
* Most commonly caused by HSV-1 (05% of cases) |
|||
**First episode often also involves fever, headache, malaise, and myalgias |
|||
* In children, it is often during primary infection |
|||
**May have pain, itching, dysuria, genital discharge, and inguinal lymphadenopathy |
|||
* Less clear in adults, where it may be primary, infection with a new strain, or reactivation of latent infection |
|||
*May develop extragenital sites of infection, including buttock, groin, and thigh with HSV-2 and perioral area with HSV-1 |
|||
* Characterized by acute onset fever and neurologic symptoms |
|||
**Rarely fingers and eyes |
|||
** Often affects temporal lobe, with behaviour changes |
|||
**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===== |
|||
=== 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 |
|||
*These can include aseptic meningitis, transverse myelitis, and sacral radiculopathy |
|||
=== HIV coinfection === |
|||
*Typically occur in conjunction with first episode of genital HSV-2 infection |
|||
* HSV, and specifically HSV-2, may be persistent in HIV coinfection |
|||
*'''Aseptic meningitis''' |
|||
* HSV-2 also predisposes to HIV infection |
|||
**Mengitis is more common with HSV-2 than HSV-1 |
|||
* There is more frequent asymptomatic shedding of HSV, inversely proportional to CD4 count |
|||
**Often concurrent with primary genital infection, typically 3 to 12 days after start of symptoms |
|||
* Frequency of lesions is lower on ART |
|||
**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===== |
|||
=== 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 |
|||
*Rare cause of PID, possibly representing dual infection with a typical bacterial copathogen |
|||
=== Pregancy === |
|||
* See [[HSV in pregnancy]] |
|||
=====Disseminated Disease===== |
|||
=== 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 |
|||
*Rarely can disseminate |
|||
== Diagnosis == |
|||
*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 (95% 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 |
|||
*CSF findings |
|||
**CSF PCR may be negative initially, so may need to repeat LP |
|||
**''May'' not have a cerebrospinal pleiocytosis (normal CSF in 3%) |
|||
===Visceral and 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 immunosuppression |
|||
**Focal necrotizing pneumonitis or bilateral interstitial pneumonitis, depending on pattern of spread |
|||
**80% mortality |
|||
**However, must be distinguished from asymptomatic shedding during an intercurrent illness |
|||
*'''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=== |
|||
*See [[HSV in 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 |
|||
**Large granular plasma cells in CSF are the hallmark of Mollaret meningitis |
|||
==Management== |
|||
===Genital and Rectal Herpes=== |
|||
*Mild-to-moderate infection |
|||
**First episode |
|||
***[[Is treated by::Acyclovir]] 400 mg po tid, [[Is treated by::acyclovir]] 200 mg po 5x/day, [[Is treated by::famciclovir]] 250 mg po tid, or [[Is treated by::valacyclovir]] 1 g po bid |
|||
***Duration 5 to 10 days |
|||
**Recurrence |
|||
***[[Is treated by::Acyclovir]] 400 mg po tid, [[Is treated by::acyclovir]] 800 mg po bid, [[Is treated by::acyclovir]] 800 mg po tid, [[Is treated by::valacyclovir]] 500 mg po bid, [[Is treated by::famciclovir]] 125 mg po tid |
|||
***Duration 5 days, except valacyclovir that is 3 days |
|||
**Suppressive therapy |
|||
***[[Is treated by::Acyclovir]] 400 mg po bid, [[Is treated by::famciclovir]] 250 mg po bid, [[Is treated by::valacyclovir]] 500 mg po daily, or [[Is treated by::valacyclovir]] 1 g po daily |
|||
*HIV patients |
|||
**Recurrence |
|||
***[[Is treated by::acyclovir]] 400 mg po tid, [[Is treated by::valacyclovir]] 1 g po bid, [[Is treated by::famciclovir]] 500 mg po tid |
|||
***Duration 5 to 10 days |
|||
**Suppressive therapy |
|||
**[[Is treated by::Acyclovir]] 400 to 800 mg po bid to tid, [[Is treated by::famciclovir]] 500 mg po bid, or [[Is treated by::valacyclovir]] 500 mg po bid |
|||
*Severe infections, including CNS or ocular involvement, or disseminated disease |
|||
**[[Is treated by::Acyclovir]] 5 to 10 mg/kg IV q8h for 5 to 7 days and until clinical resolution |
|||
**For encephalitis, extend to 21 days |
|||
**For neonates, extend IV to 21 days then step down to oral for 6 months |
|||
*Pregnant: use [[Is treated by::acyclovir]] |
|||
===Stomatitis=== |
|||
*[[Is treated by::Acyclovir]] 400 mg po tid, [[Is treated by::acyclovir]] 200 mg po 5x/d, [[Is treated by::famciclovir]] 250 mg po tid, [[Is treated by::valacyclovir]] 1 g po bid |
|||
*Duration 7 to 10 days |
|||
===Esophagitis=== |
|||
*[[Is treated by::Acyclovir]] 400 to 800 mg po 5x/day, [[Is treated by::famciclovir]] 500 mg po bid to tid, [[Is treated by::valacyclovir]] 1 g po bid, or [[Is treated by::acyclovir]] 5 mg/kg IV q8h |
|||
*Duration 7 to 10 days |
|||
===Herpes Labialis Prophylaxis=== |
|||
*[[Is treated by::Acyclovir]] 400 mg po bid, [[Is treated by::famciclovir]] 250 mg po bid, [[Is treated by::valacyclovir]] 250 mg po bid or 500 mg po daily or 1 g po daily |
|||
===Encephalitis and Meningitis=== |
|||
*[[Is treated by::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: [[Is treated by::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: [[Is treated by::acyclovir]] 400 to 800 mg po bid to tid, [[Is treated by::valacyclovir]] 500 mg po daily, or [[Is treated by::famciclovir]] 500 mg po bid |
|||
*Burn patients: [[Is treated by::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 [[Is treated by::foscarnet]] 40 to 80 mg/kg IV q8h until clinical resolution |
|||
*Can try [[Is treated by::cidofovir]] 5 mg/kg once weekly if severe infection |
|||
[[Category:Herpesviridae]] |
[[Category:Herpesviridae]] |
Latest revision as of 16:29, 2 May 2023
- Comprises herpes simplex virus 1 (HSV-1) and HSV-2, which are members of the Herpesviridae 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
Mechanisms of Resistance
- Resistance to acyclovir is usually conferred by a deficiency in thymidine kinase (which phosphorylates acyclovir)
- Will also be resistant to valacyclovir and famciclovir
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 Manifestations
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 (95% 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
- CSF findings
- CSF PCR may be negative initially, so may need to repeat LP
- May not have a cerebrospinal pleiocytosis (normal CSF in 3%)
Visceral and 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 immunosuppression
- Focal necrotizing pneumonitis or bilateral interstitial pneumonitis, depending on pattern of spread
- 80% mortality
- However, must be distinguished from asymptomatic shedding during an intercurrent illness
- 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
- See HSV in 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
- Large granular plasma cells in CSF are the hallmark of Mollaret meningitis
Management
Genital and Rectal Herpes
- Mild-to-moderate infection
- First episode
- Acyclovir 400 mg po tid, acyclovir 200 mg po 5x/day, famciclovir 250 mg po tid, or valacyclovir 1 g po bid
- Duration 5 to 10 days
- Recurrence
- Acyclovir 400 mg po tid, acyclovir 800 mg po bid, acyclovir 800 mg po tid, valacyclovir 500 mg po bid, famciclovir 125 mg po tid
- Duration 5 days, except valacyclovir that is 3 days
- Suppressive therapy
- Acyclovir 400 mg po bid, famciclovir 250 mg po bid, valacyclovir 500 mg po daily, or valacyclovir 1 g po daily
- First episode
- HIV patients
- Recurrence
- acyclovir 400 mg po tid, valacyclovir 1 g po bid, famciclovir 500 mg po tid
- Duration 5 to 10 days
- Suppressive therapy
- Acyclovir 400 to 800 mg po bid to tid, famciclovir 500 mg po bid, or valacyclovir 500 mg po bid
- Recurrence
- Severe infections, including CNS or ocular involvement, or disseminated disease
- Acyclovir 5 to 10 mg/kg IV q8h for 5 to 7 days and until clinical resolution
- For encephalitis, extend to 21 days
- For neonates, extend IV to 21 days then step down to oral for 6 months
- Pregnant: use acyclovir
Stomatitis
- Acyclovir 400 mg po tid, acyclovir 200 mg po 5x/d, famciclovir 250 mg po tid, valacyclovir 1 g po bid
- Duration 7 to 10 days
Esophagitis
- Acyclovir 400 to 800 mg po 5x/day, famciclovir 500 mg po bid to tid, valacyclovir 1 g po bid, or acyclovir 5 mg/kg IV q8h
- Duration 7 to 10 days
Herpes Labialis Prophylaxis
- Acyclovir 400 mg po bid, famciclovir 250 mg po bid, valacyclovir 250 mg po bid or 500 mg po daily or 1 g po daily
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
References
- 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.