Hepatitis E risks: pigs or blood—that is the question

BACKGROUND Infection with hepatitis E virus (HEV) Genotype 3 is recognized as a food‐borne zoonosis in developed countries where it usually causes a mild self‐limited acute hepatitis. It may cause a persistent infection in the immunosuppressed human that can progress to cirrhosis. To protect the pat...

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Bibliographic Details
Published in:Transfusion (Philadelphia, Pa.) Pa.), 2017-02, Vol.57 (2), p.267-272
Main Authors: Tedder, Richard S., Ijaz, Samreen, Kitchen, Alan, Ushiro‐Lumb, Ines, Tettmar, Kate I., Hewitt, Patricia, Andrews, Nick
Format: Article
Language:English
Subjects:
Animals
Blood & organ donations
Blood donors
Blood Transfusion
Cirrhosis
Developed countries
Diet
Exposure
Female
Genetic screening
Genotype
Genotypes
Health risks
Hepatitis
Hepatitis E - blood
Hepatitis E - epidemiology
Hepatitis E - genetics
Hepatitis E - transmission
Hepatitis E virus - genetics
Humans
Infections
Liver cirrhosis
Male
Meat - virology
Models, Biological
Questions
Risk
Risk Factors
Seroconversion
Swine
Transfusion
Viremia
Viremia - blood
Viremia - epidemiology
Viremia - genetics
Viremia - transmission
Viruses
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Summary:BACKGROUND Infection with hepatitis E virus (HEV) Genotype 3 is recognized as a food‐borne zoonosis in developed countries where it usually causes a mild self‐limited acute hepatitis. It may cause a persistent infection in the immunosuppressed human that can progress to cirrhosis. To protect the patient from transfusion‐acquired HEV infection, steps have been taken in the United Kingdom to provide for at‐risk patients only components from donors screened for HEV viremia. This strategy does not protect from dietary exposure and calls into question estimation of relative risk between blood transfusion and diet. STUDY DESIGN AND METHODS Using data on HEV viremia, component exposure, residual plasma volume, and resulting transmission, the dose of virus administered and subsequent transmission rates were determined and used to populate a model that can infer the relationship between blood and dietary exposure. RESULTS The annual attack rate of a population, defined as seroconversion, provides an estimate of the risk of receiving a component containing HEV from a viremic donor. The lowest viral dose that resulted in infection was 2 × 104 IUs and 55% of components containing this dose transmitted infection. The transfusion risk of infection only exceeds the annual dietary risk when more than 13 individual donor components are transfused. CONCLUSION For many solid organ transplant patients dietary exposure far exceeds the risk of transfusion from unscreened donors. It is only in the immunosuppressed patient requiring extensive blood component support that transfusion risk dominates. This understanding should inform policy decisions on HEV RNA screening of blood donations.
ISSN:0041-1132
1537-2995
DOI:10.1111/trf.13976