Ribavirin as a First Treatment Approach for Hepatitis E Virus Infection in Transplant Recipient Patients
Abstract
:1. Introduction
2. Description of Cases
2.1. Case 1
2.2. Case 2
2.3. Ethics
3. Discussion
4. Conclusions
Author Contributions
Funding
Conflicts of Interest
References
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Recommendation | EASL | GeHEP/SEIMC | BTS |
---|---|---|---|
Reference | [13] | [12] | [23] |
Drug | RBV | RBV | RBV |
Treatment duration | 12 weeks | 12 weeks | 12 weeks |
Dosage | Not specified | Weight-adjusted | Not specified |
Monitoring HEV RNA during therapy | At week 12 | At weeks 4 and 12 | At weeks 1, 4, 8 and 12 |
Increase therapy duration after completion of 12 weeks | Up to 24 weeks if detectable viral load at week 12 in plasma/serum or feces | Up to 24 weeks if detectable viral load at week 12 in plasma/serum or feces | Continue until 2 stools > 1 month apart are both negative or continue for 24 weeks |
Retreatment | RBV for 24 weeks. If failure, consider treatment with Peg-IFN alpha for 12 weeks * | RBV for 24 weeks. If failure, consider treatment with Peg-IFN alpha for 12 weeks * | RBV for 24 weeks. If failure, consider treatment with Peg-IFN alpha for 12 weeks * |
Reference | n | Transplant | Country | Genotype | Duration, Median (Range) or Mean (SD) | Dosage | SVR (%) * | Note |
---|---|---|---|---|---|---|---|---|
Studies on kidney transplant patients | ||||||||
Present study | 1 | Kidney | Spain | 3 | 12 weeks | 600 mg/day | 1 (100) | |
[24] | 2 | Kidney | Japan | 3 | 12 weeks | 600 mg/day | 2 (100) | |
[25] | 16 | Kidney | Germany | 3 | 12 weeks | 600 mg/day (200–800 mg) | 15 (93.7) | Patients started therapy within the first 2 weeks after diagnosis of HEV infection |
[26] | 1 | Kidney | France | 3 | 12 weeks | 1200 mg/day | 1 (100) | Patient started therapy at the same week of diagnosis due to acute graft rejection |
[34] | 16 | Kidney | Germany | 3 | 15.2 (11.6) | 85.7 mg (200 mg, thrice a week) and 1000 mg/day | 11 (68.5) | |
[35] | 1 | Kidney | Argentina | 3 | 16 weeks | 1000 mg/day | 1 (100) | |
[36] | 1 | Kidney | France | 3 | 68 weeks | 10 mg/kg | 1 (100) | |
[27] | 2 | Kidney | Spain | Unknown | 12 weeks | 600–800 mg/day | 2 (100) | |
[37] | 1 | Kidney | The Netherlands | 3 | 16 weeks | 400–600 mg/day | 0 | |
[14] | 4 | Kidney | Germany | 3 | 20 weeks | 600–1200 mg/day | 4 (100) | |
[11] | 6 | Kidney | France | 3 | 12 weeks | 800 mg/day | 4 (66.6) | |
[38] | 1 | Kidney pediatric | Germany | 3 | 12 weeks | 10 mg/kg | 0 | Withdrew at week 4 due to severe adverse events |
[18] | 4 | Kidney pediatric | Germany | 3 | 12 weeks | 9.7 mg/kg (range: 3.6 to 15.4 mg/kg) | 3 (75) | Patient who did not achieve SVR experienced viral relapse after 2 months of therapy |
[39] | 1 | Kidney-pancreas | France | 3 | 12 weeks | 12 mg/kg | 1 (100) | |
Studies on liver transplant recipients | ||||||||
Present study | 1 | Liver | Spain | 3 | 12 weeks | 600 mg/day | 1 (100) | |
[40] | 1 | Liver | Uruguay | 3 | 9 weeks | 1200 mg/day | 1 (100) | |
[41] | 4 | Liver | Portugal | 3 | 24 weeks | 800–1200 mg/day | 4 (100) | |
[20] | 1 | Liver | Japan | 3 | 20 weeks | 800 mg/day | 1 (100) | |
[42] | 1 | Liver | Japan | 3 | 20 weeks | 200 mg/day and gradually increased up to 600 mg/day | 1 (100) | |
[28] | 4 | Liver | Germany | 3 | 12 weeks | 600 mg/day (200–800) | 3 (75) | |
[43] | 1 | Liver | Australia | 3 | 12 weeks | 200 mg/day | 1 (100) | |
[44] | 1 | Liver | Germany | 3 | 16 weeks | 600 mg/day | 1 (100) | |
[14] | 4 | Liver | Germany | 3 | 20 weeks | 600–1200 mg/day | 3 (75) | One death before completing treatment |
[21] | 1 | Liver pediatric | Germany | 3 | 24 weeks | 400 mg/day | 1 (100) | |
Studies on Heart transplant recipients | ||||||||
[45] | 1 | Heart | France | 3 | 12 weeks | 800 mg/day | 0 | |
[46] | 1 | Heart | France | 3 | 10 weeks | 200 mg/day and gradually increased up to 400 mg/day | 0 | Patient deceased at the end of therapy with detectable viral load |
[47] | 1 | Heart | Sweden | 3 | 36 weeks | 800 mg/day for 18 weeks and 1200 mg/day for 18 weeks | 1 (100) | |
[16] | 4 | Heart | The Netherlands | 3 | 12–36 weeks | 200–800 mg/day | 3 (75) | |
[48] | 4 | Heart | Germany | 3 | 20 weeks | 800 mg/day | 3 (75) | |
[49] | 1 | Heart | France | 3 | 12 weeks | 17 mg/kg | 1 (100) | |
Studies on Lung transplant recipients | ||||||||
[50] | 4 | Lung | Germany | 3 | 18 weeks | 400–800 mg/day | 2 (50) | One patient died at week 4 of therapy due to acute graft rejection |
[51] | 2 | Lung | The Netherlands | 3 | 16 weeks | 400 mg/day | 2 (100) | One patient showed detectable HEV RNA in stools at evaluation of SVR |
[14] | 3 | Lung | Germany | 3 | 20 weeks | 600–1200 mg/day | 2 (66.6) | One death before treatment completion |
Studies on alloHSCT | ||||||||
[52] | 13 | alloHSCT | France | 3 | 12 weeks (3–49 weeks) | 400–1000 mg/day | 11 (84.6) | One death before treatment completion |
[22] | 8 | alloHSCT | France, Germany, the Netherlands and Scotland | 3 | 12 weeks (1–32 weeks) | 10 mg/kg (range: 5 to 22 mg/kg) | 7 (87.5) | Patients 3, 1 and 4 received therapy with viral shedding <12, 12–24, and >24 weeks, respectively |
Studies not reporting SVR per type of transplant | ||||||||
[29] | 48 | Kidney (n = 29) Liver (n = 13) Heart (n = 3) Lung (n = 1) Kidney/Pancreas (n = 2) | France | 3 | 12 weeks | 600 mg/day (600–800 mg/day) | 38 (79.1) | |
[30] | 8 | Kidney (n = 5) Liver (n = 2) Bone marrow (n = 1) | Singapore | 3 | 12 weeks | 600 mg/day (400–800 mg/day) | 2 (25) | All kidney transplant recipients fail to respond to therapy |
[53] | 63 | Kidney (n = 45) Liver (n = 10) Heart (n = 5) Lung (n = 3) | France | 3 | 12 weeks (12–72 weeks) | 600 mg/day (200–1200 mg/day) | 42 (66.6) | 40 patients previously included in Kamar et al. NEJM 2014 |
[31] | 35 | Kidney (n = 22) Liver (n = 8) Heart (n = 3) Lung (n = 1) Kidney/Pancreas (n = 1) | France | 3 | 12 weeks | 600 mg/day (200–1200 mg/day) | 22 (62.8) | 22 patients previously included in Kamar et al. NEJM 2014 |
[32] | 4 | Liver (n = 1) Kidney (n = 2) Liver/Kidney (n = 1) | Spain | 3 | 12 weeks | 600–800 mg/day | 3 (75) | |
[33] | 24 | Kidney (n = 16) Liver (n = 5) Heart (n = 2) Lung (n = 1) | France | 3 | 12 weeks | 600 mg/day (200–1200 mg/day) | 15 (62.5) | |
[54] | 15 | Not specified | Germany | 3 | Not specified | Not specified | 13 (86.6) | |
[55] | 59 | Kidney (n = 37) Liver (n = 10) Heart (n = 5) Lung (n = 2) Kidney/Pancreas (n = 5) | France | 3 | 12 weeks (4–72 weeks) | 600 mg/day (29–1200) | 46 (77.9) | |
[56] | 41 | Kidney (n = 26) Liver (n = 9) Heart (n = 3) Kidney/pancreas (n = 1) Lung (n = 1) Liver/kidney (n = 1) | France | 3 | 12 weeks | 9.7 mg/kg/day (2.7–16.3) | 25 (61%) | |
Studies on transplant patients infected by HEV genotype different than 3 | ||||||||
[19] | 1 | Kidney | China | 4 | 24 weeks | RBV (not specified) | 0 | |
[57] | 3 | Kidney | China | 4 | 12 weeks | RBV (800 mg/day) | 2 (66.6) | |
[17] | 1 | Liver | Switzerland | 3ra | 16 weeks RBV + 24 weeks RBV/SOF + 16 weeks RBV | RBV (1129–3700 ng/mL) and SOF (400 mg/day) | 0 | |
[58] | 1 | Not specified | Switzerland | 3ra | 12 weeks | RBV (not specified) | 1 (100) | |
[30] | 1 | Liver | Singapore (patient from United Arab Emirates) | 7 | 12 weeks | 600 mg/day (400–800 mg/day) | 1 (100) |
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Rivero-Juarez, A.; Vallejo, N.; Lopez-Lopez, P.; Díaz-Mareque, A.I.; Frias, M.; Vallejo, A.; Caballero-Gómez, J.; Rodríguez-Velasco, M.; Molina, E.; Aguilera, A. Ribavirin as a First Treatment Approach for Hepatitis E Virus Infection in Transplant Recipient Patients. Microorganisms 2020, 8, 51. https://doi.org/10.3390/microorganisms8010051
Rivero-Juarez A, Vallejo N, Lopez-Lopez P, Díaz-Mareque AI, Frias M, Vallejo A, Caballero-Gómez J, Rodríguez-Velasco M, Molina E, Aguilera A. Ribavirin as a First Treatment Approach for Hepatitis E Virus Infection in Transplant Recipient Patients. Microorganisms. 2020; 8(1):51. https://doi.org/10.3390/microorganisms8010051
Chicago/Turabian StyleRivero-Juarez, Antonio, Nicolau Vallejo, Pedro Lopez-Lopez, Ana Isabel Díaz-Mareque, Mario Frias, Aldara Vallejo, Javier Caballero-Gómez, María Rodríguez-Velasco, Esther Molina, and Antonio Aguilera. 2020. "Ribavirin as a First Treatment Approach for Hepatitis E Virus Infection in Transplant Recipient Patients" Microorganisms 8, no. 1: 51. https://doi.org/10.3390/microorganisms8010051
APA StyleRivero-Juarez, A., Vallejo, N., Lopez-Lopez, P., Díaz-Mareque, A. I., Frias, M., Vallejo, A., Caballero-Gómez, J., Rodríguez-Velasco, M., Molina, E., & Aguilera, A. (2020). Ribavirin as a First Treatment Approach for Hepatitis E Virus Infection in Transplant Recipient Patients. Microorganisms, 8(1), 51. https://doi.org/10.3390/microorganisms8010051