Cytomegalovirus: Difference between revisions

Revision as of 01:09, 24 October 2019

A dsDNA virus and the largest member of the human herpesvirus family
DNA in the nucleoprotein core is embedded in matrix proteins and pp65 antigen, which is surrounded by lipid envelope
UL54 encodes DNA polymerase and is highly conserved
UL97 encodes a phosphotransferase enzymes required to phosphorylate (and therefore activate) ganciclovir
May have four genotypes

CMV causes 21% of IM
Fever, lymphadenopathy, and lymphocytosis
Often mild liver abnormalities
Occasionally cold agglutinin disease, RF positivity, cryoglobulinemia, and ANA positivity
Symptoms can persist or relapse over months (average 2 months, but up to 8)

Low risk until day 21 post-transplantation, when cell lines begin to return
May presents as asymptomatic viremia
Most common symptomatic presentation is pneumonitis (an interstitial pneumonia)
- Can also present with GI involvement

Pneumonitis
- Can cause an interstitial pneumonia
- Severe in SCT patients, mild in mononucleosis patients
Hepatitis
- Usually mild
- Can include granulomatous hepatitis in the context of mononucleosis
Guillain-Barré syndrome
- Sensory and motor palsies in the extremities and cranial nerves
- Resolves over months
Meningoencephalitis
- Headache, photophobia, lethargy, and pyramidal tract dysfunction
- May have concurrent motor and sensory palsies
Myocarditis
- Rare
Thrombocytopenia and hemolytic anemia
- Common in congenital infection, and occasionally seen in adults
Rashes
- Can cause maculopapular or rubelliform rashes following treatment with amipicillin

CBC showing leukopenia or pancytopenia
Mild elevation in liver enzymes
CMV-IgG positive
Detectable CMV DNA in peripheral blood, though it can rise during intercurrent illness

Serology
- IgG useful for prior exposure (suggesting latent infection)
- IgG avidity can confirm recent infection
- IgM >300 U/mL can help diagnose acute infection
Quantitative PCR is most useful for diagnosis and monitoring response to treatment
- Can be done on blood, BAL, urine, saliva, etc.
- Standards for reporting are defined by WHO
- However, can shed CMV asymptomatically during an acute illness, so must be taken within the clinical context
- Sensitivity/specificity for CMV disease depends on the laboratory methods and cutoff used
Microscopy of tissue biopsy or cytology may demonstrate large nuclear inclusions, and can use immunofluorescence to pp65 antigen to confirm diagnosis
Viral culture can be done with human fibroblast cells, but is slow

Antivirals
- First-line: valganciclovir or ganciclovir
  - Measure baseline CBC first due to risk of cytopenias
- Second-line, if cytopenias: foscarnet
- Third-line: cidofovir, maribavir, letermovir
At McMaster, expect 1-log drop within 2 weeks (lab-dependent)
Continue treatment until PCR is negative

Inherent acyclovir resistance
Tyrosine kinase mutation UL97? confers resistance to (val)ganciclovir
Polymerase mutation U54? confers resistance to (val)ganciclovir and foscarnet
Consider resistance if CMV DNA titres not decreasing despite appropriate treatment
Resistance genotyping available

Solid-organ transplant
- Donor+/Recipient– high risk for reactivation, the the donor organ infecting the recipient
- Donor–/Recipient+ intermediate risk
- Donor+/Recipient+ intermediate risk
- Donor–/Recipient– lowest risk
- High and intermediate risk patients get prophylaxis with valganciclovir 900 mg po bid for some amount of duration...
Hematologic stem cell transplant
- Donor+/Recipient+ high risk for reactivation
- Donor–/Recipient+ high risk
- Donor+/Recipient– intermediate risk
- Donor–/Recipient– lowest risk
- Preemptive monitoring with weekly CMV DNA PCR starting week 2
Treat if greater than threshold (1425 at McMaster) or if rising titre with symptoms

Even when dormant, can cause mild immunosuppression that predisposes to fungal infections
Asymptomatic shedding in lungs during intercurrent illness
Viremia with influenza-like illness
End-orgam damage
- CMV colitis
- Retinitis in AIDS patient (CD4 < 50-100)
- Organ inflammation of solid-organ transplants
- Pneumonitis in stem cell transplants

^ Michael J. Cannon, D. Scott Schmid, Terri B. Hyde. Review of cytomegalovirus seroprevalence and demographic characteristics associated with infection. Reviews in Medical Virology. 2010;20(4):202-213. doi:10.1002/rmv.655.
^ Jutta K. Preiksaitis, R. P. Bryce Larke, Glory J. Froese. Comparative seroepidemiology of cytomegalovirus infection in the Canadian Arctic and an Urban center. Journal of Medical Virology. 1988;24(3):299-307. doi:10.1002/jmv.1890240307.

@@ Line 16: / Line 16: @@
 == Clinical Presentation ==
-* Asymptomatic when young
+* Often asymptomatic when young
 === Infectious mononucleosis syndrome ===
@@ Line 28: / Line 28: @@
 * Low risk until day 21 post-transplantation, when cell lines begin to return
 * May presents as asymptomatic viremia
-* Most common symptomatic presentation is pneumonitis
+* Most common symptomatic presentation is pneumonitis (an interstitial pneumonia)
 ** Can also present with GI involvement
@@ Line 34: / Line 34: @@
 * Tends to reactivate within the transplanted organ
 * However, all can have GI involvement
+=== Advanced HIV ===
+* Can cause polyradiculopathy and myopathy
+=== Complications ===
+* '''Pneumonitis'''
+** Can cause an interstitial pneumonia
+** Severe in SCT patients, mild in mononucleosis patients
+* '''Hepatitis'''
+** Usually mild
+** Can include granulomatous hepatitis in the context of mononucleosis
+* '''[[Guillain-Barré syndrome]]'''
+** Sensory and motor palsies in the extremities and cranial nerves
+** Resolves over months
+* '''Meningoencephalitis'''
+** Headache, photophobia, lethargy, and pyramidal tract dysfunction
+** May have concurrent motor and sensory palsies
+* '''Myocarditis'''
+** Rare
+* '''Thrombocytopenia and hemolytic anemia'''
+** Common in congenital infection, and occasionally seen in adults
+* '''Rashes'''
+** Can cause maculopapular or rubelliform rashes following treatment with amipicillin
 == Investigations ==