Late Onset Post-Transfusion Hepatitis E Developing during Chemotherapy for Acute Promyelocytic Leukemia

Fuse, Kyoko; Matsuyama, Yuichi; Matsushima, Masato; Miyakoshi, Shukuko; Shibasaki, Yasuhiko; Takizawa, Jun; Furukawa, Tatsuo; Fuse, Ichiro; Matsumura, Hiro; Uchida, Shigeharu; Takahashi, Yoshifumi; Kamimura, Kenya; Abé, Hiroyuki; Suda, Takafumi; Aoyagi, Yoshinobu; Sone, Hirohito; Masuko, Masayoshi

doi:10.2169/internalmedicine.54.2332

Cited by 21 publications

(14 citation statements)

References 23 publications

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“…Additionally, donor screening of five of the six involved donations revealed no HEV RNA ( 6 ). In Japan, seven further posttransfusion hepatitis E cases (six cases of RBC transfusion, one case of PC transfusion) were detected, according to the official announcement of the Japanese Red Cross Society, but no information on either donor or patient antibody status or the infectious dose were available ( 26 ). The German authorities also announced four further posttransfusion hepatitis E cases (two RBC, two PC) in their actual hemovigilance report so far, without detailed case information ( 47 ).…”

Section: Discussionmentioning

confidence: 99%

Transfusion-Transmitted Hepatitis E: NAT Screening of Blood Donations and Infectious Dose

2018

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The risk and importance of transfusion-transmitted hepatitis E virus (TT-HEV) infections by contaminated blood products is currently a controversial discussed topic in transfusion medicine. The infectious dose, in particular, remains an unknown quantity. In the present study, we illuminate and review this aspect seen from the viewpoint of a blood donation service with more than 2 years of experience in routine HEV blood donor screening. We systematically review the actual status of presently known cases of TT-HEV infections and available routine NAT-screening assays. The review of the literature revealed a significant variation regarding the infectious dose causing hepatitis E. We also present the outcome of six cases confronted with HEV-contaminated blood products, identified by routine HEV RNA screening of minipools using the highly sensitive RealStar HEV RT-PCR Kit (95% LOD: 4.7 IU/mL). Finally, the distribution of viral RNA in different blood components [plasma, red blood cell concentrate (RBC), platelet concentrates (PC)] was quantified using the first WHO international standard for HEV RNA for NAT-based assays. None of the six patients receiving an HEV-contaminated blood product from five different donors (donor 1: RBC, donor 2–5: APC) developed an acute hepatitis E infection, most likely due to low viral load in donor plasma (<100 IU/mL). Of note, the distribution of viral RNA in blood components depends on the plasma content of the component; nonetheless, HEV RNA could be detected in RBCs even when low viral plasma loads of 100–1,000 IU/mL are present. Comprehensive retrospective studies of TT-HEV infection offered further insights into the infectivity of HEV RNA-positive blood products. Minipool HEV NAT screening (96 samples) of blood donations should be adequate as a routine screening assay to identify high viremic donors and will cover at least a large part of viremic phases.

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Section: Discussionmentioning

confidence: 99%

Transfusion-Transmitted Hepatitis E: NAT Screening of Blood Donations and Infectious Dose

2018

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“…Hewitt and colleagues showed that the risk relied on the type of blood product ranging from 25% for RBCs, 50% for platelets, and 100% for fresh‐frozen plasma. It should be noted that the majority of posttransfusional acute hepatitis E cases have been reported in immunosuppressed patients, with a low number of reports in immunocompetent subjects …”

Section: Discussionmentioning

confidence: 99%

Red blood cell transfusion‐transmitted acute hepatitis E in an immunocompetent subject in Europe: a case report

et al. 2016

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“…HEV‐gt‐3 has been investigated among blood donors in several western countries, with a prevalence ranging from 0.01% to 0.13% . Transmission of HEV‐gt‐3 from blood components has been described in the United Kingdom, France, and Japan . Most studies examining the prevalence of blood donor‐related HEV are based on initially pooled donor samples and thus are biased toward detection of donors with higher viral loads.…”

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confidence: 99%

“…2,[9][10][11][12][13][14][15] Transmission of HEV-gt-3 from blood components has been described in the United Kingdom, France, and Japan. 12,[16][17][18][19] Most studies examining the prevalence of blood donor-related HEV are based on initially pooled donor samples and thus are biased toward detection of donors with higher viral loads. As a result, underestimation of the true prevalence of HEV is likely.…”

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confidence: 99%

Low transfusion transmission of hepatitis E among 25,637 single‐donation, nucleic acid‐tested blood donors

et al. 2016

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Late Onset Post-Transfusion Hepatitis E Developing during Chemotherapy for Acute Promyelocytic Leukemia

Cited by 21 publications

References 23 publications

Transfusion-Transmitted Hepatitis E: NAT Screening of Blood Donations and Infectious Dose

Transfusion-Transmitted Hepatitis E: NAT Screening of Blood Donations and Infectious Dose

Red blood cell transfusion‐transmitted acute hepatitis E in an immunocompetent subject in Europe: a case report

Low transfusion transmission of hepatitis E among 25,637 single‐donation, nucleic acid‐tested blood donors

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