Progress and Challenges in the Management of Congenital Cytomegalovirus Infection
Abstract
:1. Introduction
2. Laboratory Diagnosis of CMV Infection
2.1. Maternal Infection
2.2. Foetal CMV Infection
2.3. Diagnosis of CCI in Neonates
3. Management of Congenital Cytomegalovirus Infection
3.1. Ganciclovir and Valganciclovir—Recommendation for Antiviral Therapy
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- Neonates with evidence of CNS disease should receive antiviral treatment (Quality rating A, Strength of recommendation 1). Treatment should preferably be for 6 months (Quality rating B, Strength of recommendation 2);
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- Neonates with no clinical or laboratory findings consistent with CMV disease should not receive treatment; there is no evidence to support treatment in this cohort (Quality D, Strength 1);
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- Infants with evidence of life-threatening disease or severe single or multiple organ disease should receive treatment. The evidence is limited, especially for life-threatening disease, but there was a consensus that treatment should be considered in this group (Quality B, Strength 1). There was no consensus about the duration of treatment in this group;
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- Oral valganciclovir is now the drug of choice. Intravenous ganciclovir should be used in infants who cannot tolerate oral medication or whose gastrointestinal absorption is uncertain (Quality A, Strength 1) [31].
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- Oral valganciclovir is the drug of choice. Ganciclovir can be used in infants who cannot take enteral medications or in very severe cases, with a switch to the oral route as soon as possible (Grade B);
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- Antiviral treatment should be started as soon as possible and before 1 month of age (Grade A). Treatment started between 1 and 3 months of age may be beneficial. After 3 months of age, case-by-case assessment with an expert is recommended (Grade C);
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- Six weeks of antiviral treatment is recommended for infants with isolated persistent hepatitis and no other manifestations of CCI at birth (grade D), and antiviral treatment is recommended for infants with isolated persistent thrombocytopenia and no other manifestations of CCI at birth (Grade D);
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- Treatment for infants with isolated intrauterine growth restriction (IUGR) without other manifestations of CCI at birth is not recommended (Grade D) [19].
3.2. Adverse Effects of Ganciclovir and Valganciclovir
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- Neutropenia, which is the primary adverse effect of intravenous GCV. It has been observed in 25% to 60% of infants who received this antiviral drug. It also occurs with VGCV use, although less commonly, affecting approximately 20% of these patients. Fortunately, severe cases are not common, and most often, neutropenia resolves when withholding treatment for 1 to 7 days. After this period, it is usually possible to restart the therapy without reducing the dose;
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- Thrombocytopenia, which occurs in 6% of babies who received intravenous GCV. However, it is common for children born with CCI to have a low platelet count at birth. In a randomized controlled trial, Kimberlin et al. reported that there was a similar incidence of low platelet counts (<50,000/mm3) in newborns treated with intravenous GCV and in untreated infants (7% vs. 5%, respectively);
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- Nephrotoxicity: an increase in serum creatinine concentration was reported in less than 1% of infants;
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- Hepatotoxicity: children treated with IV GCV, especially at a dose of 6 mg/kg or higher, may experience elevated levels of hepatic transaminase;
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3.3. An Overview of Research Supporting Antiviral Treatment
4. Monitoring
5. An Alternative and Supportive Therapy
5.1. Antiviral Drugs
5.2. Hyperimmune Globulin
5.3. Supportive Treatment
6. Prophylaxis and Preventive Strategies
6.1. Valaciclovir
6.2. Primary Prevention
7. Conclusions
Author Contributions
Funding
Informed Consent Statement
Conflicts of Interest
References
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Moderate to severe symptomatic CCD | Mild symptomatic CCD |
| One or two isolated manifestations of CCI that are mild and transient (e.g., mild hepatomegaly or a single measurement of low platelet count or raised levels of alanine aminotransferase). |
Asymptomatic CCD with isolated SNHL | Asymptomatic CCD |
No apparent abnormalities to suggest CCD, but SNHL is present (≥21 decibels) | No apparent abnormalities to suggest CCD; normal hearing |
Physical Examination Small for gestational age (birth weight <−2 SD for gestational age) Petechiae or purpura (usually found within hours of birth and persist for several weeks) Blueberry muffin rash (intra dermal hematopoiesis) Jaundice 1 Hepatomegaly, splenomegaly Neurologic physical examination Microcephaly (head circumference <−2 SD for gestational age) 2 Neurologic signs (lethargy, hypotonia, seizures, poor sucking reflex) Abnormalities detected incidentally or through subsequent investigation/specialist examination Laboratory results Anemia Thrombocytopenia (occurs in the 1st week but platelets often increase spontaneously after the 2nd week) 3 Leukopenia, isolated neutropenia Elevated liver enzymes (ALT/AST) Conjugated hyperbilirubinemia Cerebrospinal fluid; abnormal cerebral fluid indices, positive CMV DNA Neuroimaging Calcifications, periventricular cysts, ventricular dilatation, subependymal pseudocysts, germinolytic cysts, white matter abnormalities, cortical atrophy, migration disorders, cerebellar hypoplasia, lenticulostriatal vasculopathy 4 Hearing test Sensorineural hearing loss uni- or bilaterally Visual examination Chorioretinitis, cataracts Retinal hemorrhage, optic atrophy, strabismus |
Other indications: Maternal serology: Evidence of maternal seroconversion (considered in women with known CMV infection who are known to be IgG-seropositive at start of pregnancy), particularly, if symptoms or virologic examination are consistent with suspected CMV reactivation/reinfection Prematurity (baseline screening to differentiate between congenital and postnatal CMV infection is helpful for extremely premature infants) Older children: Sensorineural hearing loss: new diagnosis Complementary information on indications for diagnosis of congenital infection 1. Prolonged jaundice with transaminitis 2. Considered if symmetrically small for gestational age 3. Unexplained thrombocytopenia, considered if leucopenia or anemia is present 4. Considered in the case of periventricular cysts, subependymal pseudocysts, germinolytic cysts, white matter abnormalities, cortical atrophy, migration disorders, cerebellar hypoplasia, or lenticulostriate vasculopathy |
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Szulc, W.; Szydłowska, N.; Smyk, J.M.; Majewska, A. Progress and Challenges in the Management of Congenital Cytomegalovirus Infection. Clin. Pract. 2024, 14, 2445-2462. https://doi.org/10.3390/clinpract14060191
Szulc W, Szydłowska N, Smyk JM, Majewska A. Progress and Challenges in the Management of Congenital Cytomegalovirus Infection. Clinics and Practice. 2024; 14(6):2445-2462. https://doi.org/10.3390/clinpract14060191
Chicago/Turabian StyleSzulc, Weronika, Natalia Szydłowska, Julia M. Smyk, and Anna Majewska. 2024. "Progress and Challenges in the Management of Congenital Cytomegalovirus Infection" Clinics and Practice 14, no. 6: 2445-2462. https://doi.org/10.3390/clinpract14060191
APA StyleSzulc, W., Szydłowska, N., Smyk, J. M., & Majewska, A. (2024). Progress and Challenges in the Management of Congenital Cytomegalovirus Infection. Clinics and Practice, 14(6), 2445-2462. https://doi.org/10.3390/clinpract14060191