Hepatitis E virus infection during pregnancy

Hepatitis E virus (HEV) is a hepatotropic infectious agent that generally causes self-limiting acute hepatitis in healthy adults and chronic hepatitis in immunocompromised individuals [1]. Annually, there are an estimated 20 million HEV infections, 3.3 million symptomatic hepatitis E cases, and 60,000 deaths worldwide [1, 2]. In addition to hepatic manifestations, extrahepatic manifestations, including pancreatitis, neurological symptoms, hematological disorders, glomerulonephritis, and mixed cryoglobulinemia have been associated with HEV infection [1, 3]. HEV is classified into 8 major genotypes, with genotypes 1–4 being the predominant strains involved in human infections. Genotypes 1 (HEV-1) and 2 (HEV-2) infect only humans and are transmitted via the fecal-oral route [1, 4], whereas genotypes 3 (HEV-3) and 4 (HEV-4) are zoonotic and are contracted through the consumption of undercooked pork and wild boar meat [5]. Although swine are the most commonly implicated source of HEV-3 and HEV-4, other animals including shellfish, deer, and rabbits can serve as a source of infection [4, 6‐9]. Therefore, HEV-1 and HEV-2 are often associated with epidemics in developing countries due to poor hygiene and sanitation. In contrast, HEV-3 and HEV-4 are prevalent in industrialized countries and are associated with sporadic and clustered cases of hepatitis E in these regions [1, 4]. In recent years, the transmission of HEV-3 and HEV-4 through blood transfusions has been increasingly reported in Europe [1, 4, 10], prompting many countries to consider the screening of blood products for HEV [11]. For these reasons, HEV is now recognized as a global health problem in both developing and industrialized countries [1, 12]. Current therapeutics used to treat HEV infection include the nucleoside analog ribavirin and interferon-α (IFN-α). Ribavirin therapy can be fairly efficient in most cases of chronic hepatitis E [1, 2, 13, 14]. In some specific situations, interferon has also been used successfully [2]. However, until now, there have been no specific direct-acting antiviral agents against HEV, particularly for pregnant women [1, 15]. A recombinant hepatitis E vaccine, HEV 239, has been demonstrated to be well tolerated and effective in the prevention of hepatitis E in China; however, it is currently only approved for use in China and is not yet available elsewhere [2, 16, 17].

HEV infection can cause fulminant hepatitis failure (FHF), especially in pregnant women, with a mortality rate of up to 30% [1, 18‐20]. In addition, HEV can be vertically transmitted from infected mothers to their infants, with significant perinatal morbidity and mortality [20‐22]. Ribavirin and IFN-α are contraindicated in pregnancy because of the risk of teratogenicity [23‐25]. Therefore, only supportive care is provided for pregnant women with HEV infection. In this review, we provide a summary of the current knowledge regarding HEV and highlight HEV infection during pregnancy, which has been poorly understood until now and deserves the utmost attention.

HEV infection is not limited to certain developing countries; it is also endemic in many high-income countries and is largely zoonotic in nature. Despite increasing knowledge, many questions regarding HEV, especially HEV infection during pregnancy, remain unanswered. In addition to immune and hormonal factors, genome heterogeneity and HEV variants may be related to the severity of HEV infection in pregnancy. Therefore, it may be important to investigate the prevalent HEV genotypes and their virulence as well as morbidity in pregnancy; this information could be used to develop guidelines for the intervention and management of HEV infection in pregnancy. HEV can be transmitted via blood transfusion. Increasing prevalence rates of HEV in voluntary blood donors (VBDs) and transfusion-associated HEV infections have been reported [1, 4, 10, 146]. Therefore, screening donors for HEV RNA may need to be considered.

Considering that HEV infection in pregnant women may progress to fulminant hepatitis, especially in the third trimester, with a high mortality rate, screening for and monitoring HEV infection early in pregnancy should become a focus. In addition, it is also necessary to inform pregnant women of the potential effects of HEV on the fetus; they should be advised to avoid eating and drinking contaminated food and water to prevent possible HEV exposure. An HEV vaccine may hold great promise for reducing HEV-associated mortality in pregnant women. Finally, there is also a substantial need for novel therapies to treat HEV in pregnancy.