The majority (82%) of post HEV-IgG and all seroconverters samples were tested for HEV RNA. Borderline positive and negative samples were designated as positive and negative, respectively.
Donor specimens were not available for testing. Results: Among the 255 pre-LT samples 97 (38%, 95% CI 32-44%) were anti-HEV-IgG positive and none were positive for anti-HEV IgM. Age, gender, race, and etiology of cirrhosis were not significantly different in patients with or without anti-HEV. All 97 patients with anti-HEV IgG before transplant remained positive on the post-LT sample and 1 was IgM anti-HEV positive 4 yrs post-LT. Among the158 LT recipients who tested negative for IgG anti-HEV before transplant, 3 (1.9%, 95% CI: 0.4-5.4%) VX-770 order became anti-HEV IgG positive during follow up (median 114 days, IQR 85-133), one of whom was also anti-HEV IgM positive. The 3 incident infection cases were all females, median age 57 yrs, Hispanic White (n=2) or Black (N=1), received deceased (N=1) or living (N=2) donors and were transplanted for non-viral causes of cirrhosis. All 3 cases were HEV RNA negative. Conclusions: In this geographically diverse LT population, prevalent HEV infection was common among
patients undergoing LT — present in 38%. Incident infections after LT were rare, with only 1.9% (3 cases) identified and none with persistent click here infection. This natural history contrasts sharply with the reports from Europe and suggests unique epidemiologic risks in Europe. We conclude that HEV is not a major cause of unexplained chronic hepatitis in US liver transplant populations. Disclosures: Norah Terrault – Advisory Committees or Review Panels: Eisai, Biotest; Consulting: BMS, Merck; Grant/Research Support: Eisai, Biotest, Vertex, Gilead, AbbVie, Novartis, Merck The following people have nothing to disclose: Ronald E. Engle, Jennifer L. Dodge, Chris
Freise, Averell H. Sherker, Patrizia Farci, Robert H. Purcell Background: Hepatitis selleck chemicals E virus (HEV) is an emerging cause of autochthonous infections among immunocompromised individuals in developed nations. Among solid organ transplant (SOT) recipients, HEV infection has been associated with acute hepatitis, liver graft dysfunction, cirrhosis, and chronic infection in up to 65% of cases. While thrombocytopenia, leukopenia, and tacrolimus use have been associated with the development of chronic HEV infection among SOT recipients in Europe, risk factors for HEV infection among SOT recipients in North America have not been previously characterized. Methods: We conducted a nested case-control study of 16 SOT recipients at our institution with evidence of post-transplant HEV infection (evidenced by anti-HEV IgM, IgG seroconversion, or positive PCR at 6 months post-transplant), to determine risk factors for HEV infection following SOT. Categorical variables included age (by quartile), gender, immunosuppressive regimen, leukopenia (WBC< 4.
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