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Hematopoietic stem cell transplantation in HCV-infected patients. Francesco Paolo Russo, MD PhD Gastroenterology/ Multivisceral Transplant Unit Department of Surgery Oncology and Gastroenterology University Hospital Padova , Italy. francescopaolo.russo@unipd.it
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Hematopoietic stem cell transplantation in HCV-infected patients Francesco Paolo Russo, MD PhD Gastroenterology/Multivisceral Transplant Unit Department of Surgery Oncology and Gastroenterology University Hospital Padova, Italy francescopaolo.russo@unipd.it epatitivirali.aopd@aopd.veneto.it
Outline • Prevalence of HCV in HSCT recipients • HCV positive donors • Chronic hepatitis C in HSCT recipients
Outline • Prevalence of HCV in HSCT recipients • HCV positive donors • Chronic hepatitis C in HSCT recipients
Global prevalence and genotype distribution of hepatitis C virus infection in 2015: a modelling study Lancet Gastro Hep2017
Prevalence in HSCT recipients InfectiousDiseasesWorking Party (IDWP) 6 % Locasciulli et al BMT 2003
Risk of hepatitis reactivation in HCV-infected patients undergoing allogeneic (a) vs autologous (b) HSCT Locasciulli et al BMT 2003
Outline • Prevalence of HCV in HSCT recipients • HCV positive donors • Chronic hepatitis C in HSCT recipients
The HCV-RNA-positive donor-American recommendations- • HCV infection in donors should not be an absolute contraindication for HSCT (class I, level C). • The risk of HCV transmission is extremely low when HCV-RNA- candidates receive HSCT from anti-HCV+/HCV-RNA- donor (class I, level C). • In case of HCV-RNA+ donor, antiviral therapy should be started, ideally attaining undetectable HCV-RNA before stem cell harvest (class I, level C). Biology of Blood and MarrowTransplantation2015
HCV-related liver disease of donors • HCV-infected donors should be assessed for advanced chronic liver disease and other extrahepatic manifestations of HCV to recommend an optimal management of their disease (class I, level C). Biology of Blood and MarrowTransplantation2015
The HCV-RNA-positive donor-Europeanrecommendations- • In general, HCV-RNA-positive donors should not be considered, because they will transmit HCV to the recipient. But it could be considered if other donor options are inferior. In this case, the donor should be treated with new direct-acting antivirals (DAAs) (class III, level B) Lancet InfectionDisease 2016
Outline • Prevalence of HCV in HSCT recipients • HCV positive donors • Chronic hepatitis C in HSCT recipients
Chronic hepatitis C in recipient of HSCT They are at high risk for liver complications: • viralreactivation • acute hepatitis • accelerated liver disease progression • veno-occusivedisease Ramoset al Haematologica2009
Physiopathology of liver lesions in HSCT recipients with chronic hepatitis C Peffault de Latour et al. JHep2008
Monitoring HCV in HSCT Recipients with Chronic HCV Infection-American recommendations- • In HSCT recipients with chronic HCV infection, ALT level should be evaluated at entry into care, 2 to 8 weeks after completion of the conditioning regimen, every 2 to 8 weeks during maintenance chemotherapy or immunosuppressive treatment, and every 3 to 6 months thereafter (class II, level C). • In HSCT recipients with chronic HCV infection, routine monitoring of HCV RNA is not recommended. However, viral load should be considered for patients who have an unexplained elevation of ALT (class II, level C). • HCV RNA should be measured in all patients at entry into care, and monitoring of viral load should be performed in patients receiving HCV treatment according to the AASLD-IDSA HCV guidance (http://www.hcvguidelines.org/) (class I, level C).
Severe hepatitis C reactivation as an early complication of hematopoietic cell transplantation Oliver et al. BMT 2017
Long-term outcome A more rapid rate of liver fibrosis progression is observed in HCV-infected HSCT patients vs HCV patients, with an expected median time to cirrhosis of about 18 vs 40 years, respectively. Peffault de Latour et al. JHep2008
Timing of antiviral treatment in the HCV+ recipient • DAAs should be considered before HSCT. • The alternative is to treat the recipient after HSCT using DAAs after immune reconstitution. • It is urgent for: • patients with fibrosingcholestatic hepatitis • patients with cirrhosis whose condition is deteriorating
Hepatitis C virus infection in patients undergoing hematopoietic cell transplantation in the era of DAAs 64 HCV-infected patients underwent allogenic and autologous HSCT 2009-2015 • Treated patients had: • fewer relapse of non-Hodgkin lymphomas, 20% vs 86%, p=.015 • higher 5-year survival, 75% vs 39%, p=.02 • trend toward lower rate of progression to cirrhosis, 5% vs 21%, p=.06 Kyvernitakiset al. BMT 2017
Hepatitis C virus infection in patients undergoing hematopoietic cell transplantation in the era of DAAs • SVR in 32% of cases with IFN-based and 85% with DAA-based antiviral therapy. • 13% HCV-RNA negative after HSCT • HCV seropositivity can be lost post-HSCT posing a diagnostic challenge Kyvernitakiset al. BMT 2017
Drug–Drug Interactions in HCV-Infected HCT Candidates and Recipients Receiving DAAs and Conditioning Regimens or Immunosuppressive Agents • DDI can be pharmacokinetic, resulting in changes in drug concentrations, or pharmacodynamic, resulting in additive, synergistic, or antagonistic effects on efficacy or toxicity • Physicians should frequently assess for DDI in HCV-infected HCT recipients (class I, level C). • HCT candidates should not receive DAAs concomitantly with the chemotherapy preparative regimen if the potential for DDI exists (class I, level C).
Successful treatment of hepatitis C virus infection with DAAs during hematopoietic cell transplant Cunningham et al. TransplInfectDis 2019
Successful treatment of hepatitis C virus infection with DAAs during hematopoietic cell transplant • Delaying HCT to complete antiviral therapy presented an unacceptable risk for AML relapse • Untreated infection during chemotherapy or HCT is associated with accelerated liver disease, HCV exacerbation, and increased mortality Cunningham et al. TransplInfectDis 2019
Conclusions • Very high prevalence of viral reactivation • HCV represents a significant cause of morbidity and mortality in HSCT recipients. • Treatment of HCV infection should be offered to donors and recipients, because it improves outcomes, increases overall survival, and lowers relapse rates. • Those patients can be safely treated with DAAs, with monitoring for potential drug-drug interaction.