Acute Hepatitis E Infection Accounts for Some Cases of Suspected Drug-Induced Liver Injury
TL;DR: HEV infection contributes to a small but important proportion of cases of acute liver injury that are suspected to be drug induced, andSerologic testing for HEV infection should be performed, particularly if clinical features are compatible with acute viral hepatitis.
About: This article is published in Gastroenterology.The article was published on 2011-11-01 and is currently open access. It has received 295 citations till now. The article focuses on the topics: Hepatitis E & Viral hepatitis.
Summary (4 min read)
Jump to: [Introduction] – [Patient identification and causality analysis] – [Serologic and Virologic Testing] – [Histological Analysis] – [Repeat Causality Analysis] – [Data analysis] – [IRB approval] – [Serological Testing] – [Demographic and Clinical Features of IgM anti-HEV Positive Cases] – [HEV RNA results] – [Causality Analysis/Re-analysis] – [Liver histology of IgM anti-HEV positive cases] and [Discussion]
Introduction
- Drug-induced liver injury is the leading cause of acute liver failure and the primary reason for regulatory action leading to failed drug approval, market withdrawal, usage restrictions and warnings to practicing physicians in the United States.
- The diagnosis is primarily one of exclusion and is made only after elimination of common causes of liver disease, such as alcoholic hepatitis, metabolic and genetic liver diseases, bile duct obstruction, and hepatitis A, B, and C virus infection (HAV, HBV, and HCV).
- 3 Several recent findings have served to alter this opinion.
- The aims of the current study were to assess whether acute hepatitis E accounts for some cases of suspected drug-induced liver injury in the United States and whether testing for HEV infection is warranted in the routine evaluation of patients with acute liver disease of unknown cause.
Patient identification and causality analysis
- The Drug Induced Liver Injury Network consists of multiple (previously 5, and currently 8) U.S. clinical sites and a data coordinating center that have enrolled patients with suspected drug-induced liver injury into a prospective study since 2004.
- The rationale, design and conduct of the DILIN, as well as a summary of the first 300 enrolled cases have been described.
- 16, 17 All enrolled cases were subjected to formal causality assessment independently by three investigators, and a final causality score was obtained by consensus.
- 18 At the same time, a Roussel Uclaf Causality Assessment score 19 was determined and cases were graded for severity using a five-point scale developed by the DILIN.
Serologic and Virologic Testing
- Serum samples were obtained at the time of enrollment, which might be as long as 6 months after the onset of liver injury, and were stored at -80 degrees Celsius in a central repository.
- For the current study, serum samples from the first 318 patients enrolled were tested for IgM and IgG anti-HEV using enzyme immunoassays of established sensitivity and specificity.
- 20, 21 Samples with IgM anti-HEV and those with strongly positive reactions for IgG anti-HEV were further tested for HEV RNA using nested reverse transcription polymerase chain reaction (RT-PCR) 22 and the PCR products were separated by electrophoresis on ethidium bromide-stained agarose gels, extracted from the gel and directly sequenced to provide the consensus sequence.
- A BLAST search of GenBank nucleotide sequences was performed to determine HEV genotype.
- Details of the ELISA assays for anti-HEV and the PCR for HEV RNA are provided in Supplementary Material.
Histological Analysis
- When available, liver biopsies (n=3) were reviewed by a hepatic pathologist (D.E.K.) who was unaware of the medications implicated and results of HEV testing.
- Histological features of inflammation, fibrosis, steatosis, cholestasis, vascular injury and other findings were systematically recorded, along with a description of the overall pattern of injury.
Repeat Causality Analysis
- Cases positive for HEV IgM were subjected to repeat causality analysis by three independent reviewers after the results of HEV serological and RT-PCR testing were available.
- 18 Cases were also judged using the same scale as to the likelihood that the liver injury was due to acute hepatitis E based upon the clinical, biochemical and histological findings.
Data analysis
- Pairwise comparisons were performed between the cases with no serological evidence of HEV infection versus patients with evidence of active or recent HEV infection (defined by presence of HEV IgM) and those with distant and resolved HEV infection (defined by presence of IgG without IgM anti-HEV).
- The Wilcoxon test was used for continuous variables, Fisher's exact test for binary outcomes, and the Pearson chi-squared test for other categorical variables.
IRB approval
- All details of the DILIN Prospective study were reviewed and approved by the institutional review boards of each clinical site and the data coordinating center.
- In addition, the protocol for anti-HEV testing was specifically approved by the institutional review board of the National Institute of Allergy and Infectious Diseases of the intramural program of the National Institutes of Health.
Serological Testing
- Initial and peak serum bilirubin, alanine aminotransferase (ALT) and alkaline phosphatase levels were similar in the three groups of patients.
- Furthermore, the three groups did not different in distribution of pattern of serum enzyme elevations, severity scores or causality scores.
Demographic and Clinical Features of IgM anti-HEV Positive Cases
- Selective demographic and clinical features of the nine IgM anti-HEV positive cases are given in Table 2 , and detailed case summaries of each patient are provided as Supplementary Data.
- The clinical course was considered severe in three patients who manifested signs of hepatic failure such as elevations in INR > 1.5, ascites or hepatic encephalopathy.
- Information on exposures to farm animals or raw pork was not specifically sought but none offered such information or gave a history of travel to an endemic area.
- The patients were geographically diverse and presented at 4 of the 5 DILIN centers including Indiana (n=5), San Francisco (n=2), Connecticut (n=1) and North Carolina (n=1) between 2004 and 2006.
HEV RNA results
- Four patients with IgM anti-HEV were also reactive for HEV RNA, and all four harbored genotype 3.
- Sequencing analyses showed that the four were not closely related phylogenetically (data not shown) and therefore were not likely due to a single source or contamination, presenting in different geographic areas (Indiana, San Francisco and North Carolina).
- The four cases with viremia included both patients with HIV infection.
- Follow-up serum samples, drawn approximately 6 months after enrollment, were available from four IgM anti-HEV-positive subjects: all had an increase in IgG anti-HEV titer, but IgM anti-HEV had diminished in titer or had become negative, consistent with seroconversion after acute infection.
- All were also negative for HEV RNA (two were positive on the earlier specimen) (Table 3 ).
Causality Analysis/Re-analysis
- The initial causality assessment for the nine cases concluded that 4 were highly likely, 3 probably and 2 possibly due to drug-induced liver injury.
- 21 Thus, most cases were considered compatible with drug-induced liver injury on initial assessment in the absence of anti-HEV results.
- Even with the information on HEV serology, two cases (implicated medications being allopurinol and telithromycin) were still considered probably due to drug-induced liver injury rather than hepatitis E. Both patients presented late during the course of illness and initial clinical features and laboratory results were not available.
- The remaining seven cases were considered more likely to be acute hepatitis E than drug-induced liver injury, although four were still considered "possibly" due to the medication.
- Three cases were considered "definite" acute hepatitis E.
Liver histology of IgM anti-HEV positive cases
- Liver biopsy tissue was available from three patients.
- The bile ducts showed mild injury with reactive changes, but without cholestasis.
- Case 4 developed mild acute liver injury with jaundice after taking ezetimibe for one year and underwent liver biopsy during recovery when serum bilirubin (1.4 mg/dL) and ALT levels (60 U/L) were close to normal.
- The biopsy (not shown) showed mild steatosis, ballooning and bridging fibrosis with focal copper accumulation consistent with nonalcoholic steatohepatitis which he was thought to have before onset of the acute injury (based upon chronic ALT elevations and obesity).
- Case 7 developed jaundice and a hepatitis-like syndrome 1.5 years after starting an antiretroviral regimen including nevirapine and on liver biopsy had changes of lobular disarray, spotty hepatocyte necrosis without confluence, marked lobular but scant portal inflammation, mild intrahepatic cholestasis but no bile duct injury, steatosis or fibrosis.
Discussion
- The accurate diagnosis of drug-induced liver injury is critically important not only for patient care, but also for drug development, as even a single episode of severe liver damage associated with a drug during pre-marketing clinical testing may undermine its subsequent approval and marketing.
- These findings suggest that the recent acute HEV infection detected by IgM anti-HEV testing did not account for the acute liver injury in all cases and that co-incidental, subclinical hepatitis E may have preceded the acute liver injury caused by the implicated medication.
- In the remaining five patients the absence of viremia may have been due to the delay between the onset of symptoms and blood sampling for the study, as patients were typically referred by local physicians to the DILIN investigators days or even weeks after initial presentation.
- The presence of serological evidence of acute hepatitis E should also prompt a search for possible sources of infection, such as foreign travel, exposure to farm animals, consumption of undercooked pork or wild game, and close personal contact with chronically immunosuppressed persons.
- Finally, these findings underscore the need for sensitive and reliable, commercially available assays for HEV infection in the United States and reexamination of the possible benefit of an HEV vaccine.
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References
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TL;DR: There was a difference in anti- HEV prevalence in both swine veterinarians and blood donors among the eight selected states, with subjects from Minnesota six times more likely to be anti-HEV positive than those from Alabama, and age was not a factor in the observed differences.
Abstract: Hepatitis E virus (HEV) is endemic in many developing and some industrialized countries. It has been hypothesized that animals may be the source of infection. The recent identification of swine HEV in U.S. pigs and the demonstration of its ability to infect across species have lent credence to this hypothesis. To assess the potential risk of zoonotic HEV infection, we tested a total of 468 veterinarians working with swine (including 389 U.S. swine veterinarians) and 400 normal U.S. blood donors for immunoglobulin G anti-HEV. Recombinant capsid antigens from a U.S. strain of swine HEV and from a human HEV strain (Sar-55) were each used in an enzyme-linked immunosorbent assay. The anti-HEV prevalence assayed with the swine HEV antigen showed 97% concordance with that obtained with the human HEV antigen (κ = 92%). Among the 295 swine veterinarians tested from the eight U.S. states (Minnesota, Indiana, Nebraska, Iowa, Illinois, Missouri, North Carolina, and Alabama) from which normal blood donor samples were available, 26% were positive with Sar-55 antigen and 23% were positive with swine HEV antigen. In contrast, 18% of the blood donors from the same eight U.S. states were positive with Sar-55 antigen and 17% were positive with swine HEV antigen. Swine veterinarians in the eight states were 1.51 times more likely when tested with swine HEV antigen (95% confidence interval, 1.03 to 2.20) and 1.46 times more likely when tested with Sar-55 antigen (95% confidence interval, 0.99 to 2.17) to be anti-HEV positive than normal blood donors. We did not find a difference in anti-HEV prevalence between veterinarians who reported having had a needle stick or cut and those who had not or between those who spent more time (≥80% of the time) and those who spent less time (≤20% of the time) working with pigs. Similarly, we did not find a difference in anti-HEV prevalence according to four job categories (academic, practicing, student, and industry veterinarians). There was a difference in anti-HEV prevalence in both swine veterinarians and blood donors among the eight selected states, with subjects from Minnesota six times more likely to be anti-HEV positive than those from Alabama. Age was not a factor in the observed differences from state to state. Anti-HEV prevalence in swine veterinarians and normal blood donors was age specific and paralleled increasing age. The results suggest that swine veterinarians may be at somewhat higher risk of HEV infection than are normal blood donors.
508 citations
TL;DR: In a high-risk population, the rHEV vaccine was effective in the prevention of hepatitis E and among subjects in a subgroup randomly selected for analysis of injection-site findings and general symptoms, the proportion of subjects with adverse events was similar in the two study groups.
Abstract: Background Hepatitis E virus (HEV) is an important cause of viral hepatitis. We evaluated the safety and efficacy of an HEV recombinant protein (rHEV) vaccine in a phase 2, randomized, double-blind, placebo-controlled trial. Methods In Nepal, we studied 2000 healthy adults susceptible to HEV infection who were randomly assigned to receive three doses of either the rHEV vaccine or placebo at months 0, 1, and 6. Active (including hospital) surveillance was used to identify acute hepatitis and adverse events. The primary end point was the development of hepatitis E after three vaccine doses. Results A total of 1794 subjects (898 in the vaccine group and 896 in the placebo group) received three vaccine doses; the total vaccinated cohort was followed for a median of 804 days. After three vaccine doses, hepatitis E developed in 69 subjects, of whom 66 were in the placebo group. The vaccine efficacy was 95.5% (95% confidence interval [CI], 85.6 to 98.6). In an intention-to-treat analysis that included all 87 sub...
487 citations
TL;DR: DILIN is a multicentre research network charged with improving the understanding of the aetiologies, risk factors and outcomes of DILI in the US and is meeting the targeted enrolment of ten patients per month and is developing a repository of clinical data and biological samples for future studies of D ILI pathogenesis and outcome.
Abstract: Background: Drug-induced liver injury (DILI) is an uncommon adverse drug reaction of increasing importance to the medical community, pharmaceutical industry, regulatory agencies and the general public. Objectives: The Drug-Induced Liver Injury Network (DILIN) was established to advance understanding and research into DILI by initiating a prospective registry of patients with bona fide DILI for future studies of host clinical, genetic, environmental and immunological risk factors. The DILIN was also charged with developing standardized nomenclature, terminology and causality assessment instruments. Methods: Five clinical sites, a data coordinating centre and senior scientists from the National Institute of Diabetes and Digestive and Kidney Diseases initiated the DILIN prospective study in September 2004. Eligible patients are required to meet minimal laboratory or histological criteria within 6 months of DILI onset and have other competing causes of liver injury excluded. Patients in the general community setting with pre-existing HIV, hepatitis B virus or hepatitis C virus infections and/or abnormal baseline liver biochemistries are eligible for enrolment. In addition, subjects with liver injury due to herbal products are eligible to participate. Control patients without DILI are also to be recruited in the future. Results: All referred subjects undergo an extensive review of available laboratory, pathology and imaging studies. Subjects who meet pre-defined eligibility criteria at the 6-month study visit are followed for 2 years to better define the natural history of chronic DILI. Causality assessment is determined by a panel of three hepatologists who independently assign a causality score ranging from 1 (definite) to 5 (unlikely) as well as a severity score ranging from 1 (mild) to 5 (fatal). During the first 3 years, 367 subjects were enrolled into the DILIN prospective study. Conclusion: DILIN is a multicentre research network charged with improving our understanding of the aetiologies, risk factors and outcomes of DILI in the US. The network is meeting the targeted enrolment of ten patients per month and is developing a repository of clinical data and biological samples for future studies of DILI pathogenesis and outcome.
399 citations
TL;DR: Although the authors could not prove that the uncooked boar liver was the source of the HEV infection (since it all had been eaten), it appears likely that this was the case.
Abstract: To the Editor-As was reported in the Journal, by Takahashi et al. [ 1 ] as well as by the authors of a letter to the editor about Takahashi et al.'s article [2], hepatitis E virus (HEV) infection caused by genotypes III and IV seems to be cryptically endemic in Japan, with the transmission mode yet to be resolved. Zoonotic risks have been suggested for sporadic HEV infections, particularly in industrialized countries [3]. We hereby report our recent experience in Japan, which may support the zoonosis hypothesis. A 53-year-old man (patient A) was admitted to one of our hospitals for acute hepatitis on 12 March 2003. His hepatitis was a severe type, as indicated by the levels of total bilirubin (10.2 mg/dL) and prothrombin (only 17%). Despite the initial severity of the disease, he showed a rapid recovery, without developing fulminant hepatic failure. Convalescence serum obtained on 15 April was positive for both IgM and IgG classes of anti-HEV but was negative for HEV RNA. Acute-phase serum from this patient was not available. Later, to our surprise, it was revealed that, on the same day that patient A had been admitted, one of his friends (a 70year-old man; patient B) had been admitted to another hospital, for similarly severe hepatitis (total bilirubin, 17.1 mg/ dL; prothrombin, 40%). Patient B developed hepatic coma and died of fulminant hepatic failure on 13 April. Acute-phase serum obtained on 13 March was found, retrospectively, to be positive for HEV RNA. Determination of a 326-nt partial open-reading frame-1 sequence of his HEV RNA (accession no. AB114178) indicated that this isolate segregates to genotype IV During the 3 months preceding the onset of disease, neither patient A nor patient B had traveled to areas where HEV is endemic, but patient A mentioned that he and patient B had enjoyed eating uncooked boar liver together a total of 5 times from late January to early February. Among the patients' family members and friends, no one had eaten the boar liver and no one had contracted hepatitis. Chandler et al. [4] reported serological evidence suggesting boars and pigs as candidate animal reservoirs for HEV Although we could not prove that the uncooked boar liver was the source of the HEV infection (since it all had been eaten), it appears likely that this was the case.
343 citations
TL;DR: Phylogenetic analyses indicate that HEV US-1 and a recently discovered HEV variant from swine may represent separate isolates of a new strain of HEV, significantly divergent from the Mexican and Burmese strains.
Abstract: A variant of hepatitis E virus (HEV), designated HEV US-1, was identified in a hepatitis patient in the United States (US); the patient had no history of travel to areas where HEV is endemic. Nucleotide sequences were obtained from the 5' end of open reading frame (ORF) 1 (1418 nt), the 3' end of ORF1 (1359 nt), the entire ORF2 and ORF3 regions, and the 3'-untranslated region (2127 nt). The HEV US-1 strain is significantly divergent from other human HEV isolates with nucleotide identities ranging from 76.8 to 77.5%. Phylogenetic analyses indicate that HEV US-1 and a recently discovered HEV variant from swine may represent separate isolates of a new strain of HEV, significantly divergent from the Mexican and Burmese strains. Synthetic peptides derived from the carboxyl amino acids of ORF2 and ORF3 were shown to be useful for detecting exposure to HEV. In addition, IgM class antibodies directed against HEV US-1 synthetic peptides were detected in the US patient infected with HEV US-1, but were absent using synthetic peptides from the Burmese or Mexican strains of HEV. A preferential reactivity to HEV US-1 specific peptides has lead to the identification of a second isolate of this virus also from a patient with acute hepatitis from the US. The discovery of these HEV variants may be important in understanding the worldwide distribution of HEV infection.
339 citations