Hepatitis E Virus Species C Infection in Humans, Hong Kong

Author:

Sridhar Siddharth123ORCID,Yip Cyril Chik-Yan1,Lo Kelvin Hon-Yin1,Wu Shusheng1,Situ Jianwen1,Chew Nicholas Foo-Siong1,Leung Kit-Hang1,Chan Helen Shuk-Ying4,Wong Sally Cheuk-Ying4,Leung Anthony Wai-Shing5,Tse Cindy Wing-Sze6,Fung Kitty S C7,Tsang Owen Tak-Yin5,Hon Kam-Lun8,Cheng Vincent Chi-Chung1,Ng Ken Ho-Leung9,Yuen Kwok-Yung12310

Affiliation:

1. Department of Microbiology, Li Ka Shing Faculty of Medicine, The University of Hong Kong, Hong Kong, China

2. State Key Laboratory of Emerging Infectious Diseases, The University of Hong Kong, China

3. Carol Yu Centre for Infection, The University of Hong Kong, China

4. Queen Elizabeth Hospital, Hong Kong, China

5. Princess Margaret Hospital, Hong Kong, China

6. Kwong Wah Hospital, Hong Kong, China

7. United Christian Hospital, Hong Kong, China

8. The Hong Kong Children’s Hospital, Hong Kong, China

9. Public Health Laboratory Services Branch, Department of Health, Hong Kong, China

10. The Collaborative Innovation Center for Diagnosis and Treatment of Infectious Diseases, The University of Hong Kong, Hong Kong, China

Abstract

Abstract Background Hepatitis E virus (HEV) variants belonging to Orthohepevirus species A (HEV-A) are the primary cause of human hepatitis E. However, we previously reported that Orthohepevirus species C genotype 1 (HEV-C1), a divergent HEV variant commonly found in rats, also causes hepatitis in humans. Here, we present a clinical-epidemiological investigation of human HEV-C1 infections detected in Hong Kong, with an emphasis on outcomes in immunocompromised individuals. Methods A surveillance system for detecting human HEV-C1 infections was established in Hong Kong. Epidemiological and clinical characteristics of HEV-C1 cases identified via this system between 1 August 2019 and 31 December 2020 were retrieved. Phylogenetic analysis of HEV-C1 strain sequences was performed. Infection outcomes of immunocompromised individuals with HEV-A and HEV-C1 infections were analyzed. Results HEV-C1 accounted for 8 of 53 (15.1%) reverse-transcription polymerase chain reaction (RT-PCR)–confirmed HEV infections in Hong Kong during the study period, raising the total number of HEV-C1 infections detected in the city to 16. Two distinct HEV-C1 strain groups caused human infections. Patients were elderly and/or immunocompromised; half tested negative for HEV immunoglobulin M. Cumulatively, HEV-C1 accounted for 9 of 21 (42.9%) cases of hepatitis E recorded in immunocompromised patients in Hong Kong. Immunocompromised HEV-C1 patients progressed to persistent hepatitis at similar rates (7/9 [77.8%]) as HEV-A patients (10/12 [75%]). HEV-C1 patients responded to oral ribavirin, although response to first course was sometimes poor or delayed. Conclusions Dedicated RT-PCR–based surveillance detected human HEV-C1 cases that evade conventional hepatitis E diagnostic testing. Immunosuppressed HEV-C1–infected patients frequently progress to persistent HEV-C1 infection, for which ribavirin is a suitable treatment option.

Funder

Health and Medical Research

Food and Health Bureau

Hong Kong Special Administrative Region

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Microbiology (medical)

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