Epstein-Barr virus: Difference between revisions

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==Background==
= Epstein-Barr virus (EBV) =
===Microbiology===


*A member of the ''Gammaherpesvirinae'' subfamily within the [[Herpesviridae]] family
== Diagnosis ==
*Double-stranded DNA inside an icosahedral protein nucleocapsid surrounded by a lipid envelope with glycoproteins
*Two strains (type 1 and 2) are serologically identical, but have unique epitopes
*Infection can remain quiescent in B cells for life


===Epidemiology===
* '''Anti-VCA''' (viral capsid antigens): most useful
** Anti-VCA IgM: appears early and disappears within 4 to 6 weeks
** Anti-VCA IgG: appears in acute phase, peaks at 2 to 4 weeks, then declines but remains positive for life
* '''Anti-EA''' (early antigen) IgG: appears in acute phase and falls to undetectable within 3 to 6 months (but may persist for years)
** Least useful test
* '''Anti-EBNA''' (EBV nuclear antigen): negative during acute phase converts after 2 to 4 months and stays positive for life
* '''Monospot''' test: cross-reacts with many other conditions, and is often falsely negative in children


*Acquired via oral secretions, e.g. by kissing or sharing of food
=== Serology in immunocompetent hosts ===
*Seroprevalence about 90-95% in adults, with about half of 5 year-olds already being seropositive
**Acquired earlier in low-income countries
*Highest morbidity is with young adults who develop infectious mononucleosis during primary disease
**Includes barracks and universities


===Pathophysiology===
![Graph of serology](EBV serology.jpg)


*Acquired through mucous membrane contact of oral secretions
{|
*Immune response primarily with cytotoxic T cells and NK cells
!align="center"| VCa-IgM
**Atypical lymphocytosis develops from CD8 cells
!align="center"| VCA-IgG
*Early response is against lytic antigens (including VCA and EA), and later response against latent proteins (EBNA1, EBNA2, EBNA3, and EBNALP)
!align="center"| EBNA-IgG
*Response also creates IgM antibodies to sheep, horse, and cow RBCs, called '''heterophile antibodies'''
! Interpretation

==Clinical Manifestations==
===Childhood===

*In childhood, mostly asymptomatic or mild febrile illness
*May develop rashes, neutropenia, or pneumonia
*Can cause lymphadenopathy
*Heterophile antibody may be negative if young; about 80% are positive by 4 years, though

===Infectious Mononucleosis===

*Caused by primary infection, typically in an adolescent or young adult
*EBV causes about 80% of mononucleosis, with the rest being [[CMV]]
*Incubation period [[Usual incubation period::30 to 50 days]], and can have asymptomatic viral shedding for up to a month before symptoms
*Symptoms include a triad of sore throat, fever, and lymphadenopathy (classically posterior cervical chain)
**Often preceded by prodromal symptoms of chils, sweats, anorexia, and malaise
**Can also have retro-orbital headaches, myalgias, and abdominal discomfort
**May have a rash which can take any form, and may have palatal petechiae
**Tonsils are sometimes exudative
**Often has splenomegaly, may have hepatomegaly, and rarely has jaundice
*With exposure to [[amoxicillin]], almost all patients develop a diffuse maculopapular rash
*May have transient heterophile antibodies (see Diagnosis, below), as well as [[Causes::atypical lymphocytosis]]
*Resolves over 2 to 3 weeks, with fevers lasting up to 14 days, and fatigue lasting months

===Complications===

*Linked to a number of '''malignancies''', including Burkitt lymphoma, nasopharyngeal carcinoma, and lymphoproliferative disorders
*'''Neurologic''' complications include meningitis, encephalitis, Guillain-BarrΓ© syndromes, optic neuritis, retrobulber neuritis, cranial nerve palsies, mononeuritis multiplex, brachial plexus neuropathy, seizures, subacute sclerosing panencephalitis, transverse, myelitis, psychosis, demyelination, and hemiplegia

===Chronic Active EBV Disease===

*See also [[Chronic active Epstein-Barr virus disease]]
*Classically in Japan and east Asia, possibly South America
*Progressive disease related to infection of NK or T cells rather than B cells
*Poor prognosis, with patients dying of progressive [[pancytopenia]], hypogammaglobulinemia, or NK/T cell nasal lymphoma within a few years

===Oral Hairy Leukoplakia===

===EBV-Associated Malignancies===
{| class="wikitable"
!Disease!!EBV!!Risk factors
|-
|-
|Lymphoproliferative disease||90%||Transplantation patients and immunosuppression
|align="center"| –
|align="center"| –
|align="center"| –
| Susceptible
|-
|-
|Primary CNS lymphoma||100%||HIV with low CD4 and immunosuppression
|align="center"| –
|align="center"| –
|align="center"| +
| Past infection or non-specific
|-
|-
|Hodgkin lymphoma||50%||Children and young adults
|align="center"| –
|align="center"| +
|align="center"| –
| Acute or past infection
|-
|-
|Nasopharyngeal carcinoma||100%||Southern Chinese, Inuit
|align="center"| –
|align="center"| +
|align="center"| +
| Past infection
|-
|-
|Gastric cancer||4 to 100%||Unknown
|align="center"| +
|align="center"| –
|align="center"| –
| Acute infection or non-specific
|-
|-
|Endemic Burkitt lymphoma||95%||African children
|align="center"| +
|align="center"| –
|align="center"| +
| ??
|-
|-
|Sporadic Burkitt lymphoma||20%||HIV independent of CD4
|align="center"| +
|align="center"| +
|align="center"| –
| Acute infection
|-
|align="center"| +
|align="center"| +
|align="center"| +
| Late primary infection or reactivation
|}
|}


==Diagnosis==
=== Serology in EBV-associated diseases ===
===Point-of-Care Testing===


*'''Monospot''' latex agglutination looking for '''heterophile antibodies'''
{|
**50% sensitive in the first week of illness, but up to 80-95% sensitive by the third week, and 98-100% specific, overall
! Disease
**Less sensitive (10-50%) in young children (<4 years; lowest in those less than 2 years), with much lower negative predictive power
!align="center"| VCA-IgM
**Peak 2 to 5 weeks after symptom onset then usually decline quickly, but can persist for up to 6 to 12 months
!align="center"| VCA-IgG
**False positives are rare but can happen with rheumatoid disease, [[SLE]], [[leukemia]], [[lymphoma]], and other infections including [[malaria]], [[HIV]], [[CMV]], [[rubella]], [[viral hepatitis]] and [[tularemia]], and after administration of [[anti-thymocyte globulin]]
!align="center"| VCA-IgA

!align="center"| EA(D)-IgG
===Serology===
!align="center"| EA(R)-IgG

!align="center"| EA-IgA
*Reviewed in [[CiteRef::de paschale2012se]]
!align="center"| EBNA-IgG
*'''Anti-VCA''' (viral capsid antigens): most useful
**Anti-VCA IgM: appears by presentation and disappears within 4 to 6 weeks; most useful with acute and convalescent
**Anti-VCA IgG: appears in acute phase, peaks at 2 to 4 weeks, then declines but remains positive for life
*'''Anti-EA''' (early antigen) IgG: appears in acute phase and falls to undetectable within 3 to 6 months (but may persist for years)
**Least useful test
*'''Anti-EBNA''' (EBV nuclear antigen): negative during acute phase converts after 2 to 4 months and stays positive for life

====Immunocompetent Hosts====
{| class="wikitable"
! align="center" |VCA-IgM
! align="center" |VCA-IgG
! align="center" |EBNA-IgG
!Interpretation
|-
|-
| rowspan="4" align="center" |–
| Chronic active infection
|align="center"| Β±
| rowspan="2" align="center" |–
|align="center"| ++
| align="center" |–
|Susceptible
|align="center"| Β±
|align="center"| +
|align="center"| ++
|align="center"| –
|align="center"| Β±
|-
|-
| align="center" | +
| Burkitt lymphoma
|Past infection or non-specific
|align="center"| –
|align="center"| ++
|align="center"| –
|align="center"| Β±
|align="center"| ++
|align="center"| –
|align="center"| +
|-
|-
| rowspan="2" align="center" | +
| ENT carcinoma
|align="center"| –
| align="center" |–
|Acute or past infection
|align="center"| ++
|align="center"| +
|align="center"| ++
|align="center"| Β±
|align="center"| +
|align="center"| +
|-
|-
| align="center" | +
| Hodgkin lymphoma
|Past infection
|align="center"| –
|align="center"| ++
|align="center"| –
|align="center"| +
|align="center"| –
|align="center"| –
|align="center"| +
|-
|-
| rowspan="4" align="center" | +
| Reactivation
|align="center"| Β±
| rowspan="2" align="center" |–
|align="center"| ++
| align="center" |–
|Acute infection or non-specific
|align="center"| Β±
|-
|align="center"| +
|align="center"| Β±
| align="center" | +
|Uninterpretable
|align="center"| Β±
|-
|align="center"| Β±
| rowspan="2" align="center" | +
| align="center" |–
|Acute infection
|-
| align="center" | +
|Late primary infection or reactivation
|}
|}

====EBV-Associated Diseases====
{| class="wikitable"
!Disease
! align="center" |VCA-IgM
! align="center" |VCA-IgG
! align="center" |VCA-IgA
! align="center" |EA(D)-IgG
! align="center" |EA(R)-IgG
! align="center" |EA-IgA
! align="center" |EBNA-IgG
|-
|Chronic active infection
| align="center" |Β±
| align="center" | ++
| align="center" |Β±
| align="center" | +
| align="center" | ++
| align="center" |–
| align="center" |Β±
|-
|Burkitt lymphoma
| align="center" |–
| align="center" | ++
| align="center" |–
| align="center" |Β±
| align="center" | ++
| align="center" |–
| align="center" | +
|-
|ENT carcinoma
| align="center" |–
| align="center" | ++
| align="center" | +
| align="center" | ++
| align="center" |Β±
| align="center" | +
| align="center" | +
|-
|Hodgkin lymphoma
| align="center" |–
| align="center" | ++
| align="center" |–
| align="center" | +
| align="center" |–
| align="center" |–
| align="center" | +
|-
|Reactivation
| align="center" |Β±
| align="center" | ++
| align="center" |Β±
| align="center" | +
| align="center" |Β±
| align="center" |Β±
| align="center" |Β±
|}

===PCR===

*Useful for diagnosis of:
**Rare, [[chronic active Epstein-Barr virus disease]]
**Early [[post-transplant lymphoproliferative disease]]
**[[Nasopharyngeal carcinoma]]
*As well as monitoring response to treatment

[[Category:Herpesviridae]]

Latest revision as of 20:20, 7 June 2023

Background

Microbiology

  • A member of the Gammaherpesvirinae subfamily within the Herpesviridae family
  • Double-stranded DNA inside an icosahedral protein nucleocapsid surrounded by a lipid envelope with glycoproteins
  • Two strains (type 1 and 2) are serologically identical, but have unique epitopes
  • Infection can remain quiescent in B cells for life

Epidemiology

  • Acquired via oral secretions, e.g. by kissing or sharing of food
  • Seroprevalence about 90-95% in adults, with about half of 5 year-olds already being seropositive
    • Acquired earlier in low-income countries
  • Highest morbidity is with young adults who develop infectious mononucleosis during primary disease
    • Includes barracks and universities

Pathophysiology

  • Acquired through mucous membrane contact of oral secretions
  • Immune response primarily with cytotoxic T cells and NK cells
    • Atypical lymphocytosis develops from CD8 cells
  • Early response is against lytic antigens (including VCA and EA), and later response against latent proteins (EBNA1, EBNA2, EBNA3, and EBNALP)
  • Response also creates IgM antibodies to sheep, horse, and cow RBCs, called heterophile antibodies

Clinical Manifestations

Childhood

  • In childhood, mostly asymptomatic or mild febrile illness
  • May develop rashes, neutropenia, or pneumonia
  • Can cause lymphadenopathy
  • Heterophile antibody may be negative if young; about 80% are positive by 4 years, though

Infectious Mononucleosis

  • Caused by primary infection, typically in an adolescent or young adult
  • EBV causes about 80% of mononucleosis, with the rest being CMV
  • Incubation period 30 to 50 days, and can have asymptomatic viral shedding for up to a month before symptoms
  • Symptoms include a triad of sore throat, fever, and lymphadenopathy (classically posterior cervical chain)
    • Often preceded by prodromal symptoms of chils, sweats, anorexia, and malaise
    • Can also have retro-orbital headaches, myalgias, and abdominal discomfort
    • May have a rash which can take any form, and may have palatal petechiae
    • Tonsils are sometimes exudative
    • Often has splenomegaly, may have hepatomegaly, and rarely has jaundice
  • With exposure to amoxicillin, almost all patients develop a diffuse maculopapular rash
  • May have transient heterophile antibodies (see Diagnosis, below), as well as atypical lymphocytosis
  • Resolves over 2 to 3 weeks, with fevers lasting up to 14 days, and fatigue lasting months

Complications

  • Linked to a number of malignancies, including Burkitt lymphoma, nasopharyngeal carcinoma, and lymphoproliferative disorders
  • Neurologic complications include meningitis, encephalitis, Guillain-BarrΓ© syndromes, optic neuritis, retrobulber neuritis, cranial nerve palsies, mononeuritis multiplex, brachial plexus neuropathy, seizures, subacute sclerosing panencephalitis, transverse, myelitis, psychosis, demyelination, and hemiplegia

Chronic Active EBV Disease

  • See also Chronic active Epstein-Barr virus disease
  • Classically in Japan and east Asia, possibly South America
  • Progressive disease related to infection of NK or T cells rather than B cells
  • Poor prognosis, with patients dying of progressive pancytopenia, hypogammaglobulinemia, or NK/T cell nasal lymphoma within a few years

Oral Hairy Leukoplakia

EBV-Associated Malignancies

Disease EBV Risk factors
Lymphoproliferative disease 90% Transplantation patients and immunosuppression
Primary CNS lymphoma 100% HIV with low CD4 and immunosuppression
Hodgkin lymphoma 50% Children and young adults
Nasopharyngeal carcinoma 100% Southern Chinese, Inuit
Gastric cancer 4 to 100% Unknown
Endemic Burkitt lymphoma 95% African children
Sporadic Burkitt lymphoma 20% HIV independent of CD4

Diagnosis

Point-of-Care Testing

  • Monospot latex agglutination looking for heterophile antibodies
    • 50% sensitive in the first week of illness, but up to 80-95% sensitive by the third week, and 98-100% specific, overall
    • Less sensitive (10-50%) in young children (<4 years; lowest in those less than 2 years), with much lower negative predictive power
    • Peak 2 to 5 weeks after symptom onset then usually decline quickly, but can persist for up to 6 to 12 months
    • False positives are rare but can happen with rheumatoid disease, SLE, leukemia, lymphoma, and other infections including malaria, HIV, CMV, rubella, viral hepatitis and tularemia, and after administration of anti-thymocyte globulin

Serology

  • Reviewed in 1
  • Anti-VCA (viral capsid antigens): most useful
    • Anti-VCA IgM: appears by presentation and disappears within 4 to 6 weeks; most useful with acute and convalescent
    • Anti-VCA IgG: appears in acute phase, peaks at 2 to 4 weeks, then declines but remains positive for life
  • Anti-EA (early antigen) IgG: appears in acute phase and falls to undetectable within 3 to 6 months (but may persist for years)
    • Least useful test
  • Anti-EBNA (EBV nuclear antigen): negative during acute phase converts after 2 to 4 months and stays positive for life

Immunocompetent Hosts

VCA-IgM VCA-IgG EBNA-IgG Interpretation
– – – Susceptible
+ Past infection or non-specific
+ – Acute or past infection
+ Past infection
+ – – Acute infection or non-specific
+ Uninterpretable
+ – Acute infection
+ Late primary infection or reactivation

EBV-Associated Diseases

Disease VCA-IgM VCA-IgG VCA-IgA EA(D)-IgG EA(R)-IgG EA-IgA EBNA-IgG
Chronic active infection Β± ++ Β± + ++ – Β±
Burkitt lymphoma – ++ – Β± ++ – +
ENT carcinoma – ++ + ++ Β± + +
Hodgkin lymphoma – ++ – + – – +
Reactivation Β± ++ Β± + Β± Β± Β±

PCR

References

  1. ^  Massimo De Paschale. Serological diagnosis of Epstein-Barr virus infection: Problems and solutions. World Journal of Virology. 2012;1(1):31. doi:10.5501/wjv.v1.i1.31.