An efficacy and cost-effectiveness analysis of combination hepatitis B immune globulin and lamivudine to prevent recurrent hepatitis B after orthotopic liver transplantation compared with hepatitis B immune globulin monotherapy

Han, Steven; Ofman, Joshua J.; Holt, Curtis; King, Kevin; Kunder, Gregg; Chen, Pauline; Dawson, Sherfield; Goldstein, Leonard I.; Yersiz, Hasan; Farmer, Douglas G.; Ghobrial, Rafik M.; Busuttil, Ronald W.; Martin, Paul

doi:10.1053/jlts.2000.18702

Cited by 210 publications

(107 citation statements)

References 35 publications

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“…Multiple studies showed that the mean reinfection rate was only 5.2% (range 0-18%) after 1 to 2 years, 14,15,18,28,43,48,49,75,80,81. Importantly, using highly sensitive PCR, circulating HBV DNA was undetectable in most patients after OLT 7,28,82.…”

Section: Combination Therapies To Prevent Hbv Reinfection After Trmentioning

confidence: 99%

“…Postulated mechanisms include the synergy of: 1) LAM reducing HBV replication and altering synthesis of HBsAg necessary for generation of HBIG escape mutations and 2) HBIG preventing the receptor-mediated entry of HBV into hepatocytes and extrahepatic cells required for production of escape mutations in the YMDD motif. In addition to efficacy, combination therapy is more cost effective because the dosage of expensive HBIG can be reduced 14,49. Combination therapy also permitted effective conversion of a high dose intravenous HBIG regimen to a lower dose intramuscular regimen in 98% of patients 74.…”

Section: Combination Therapies To Prevent Hbv Reinfection After Trmentioning

confidence: 99%

“…Pre-OLT inhibition of HBV replication using lamivudine (LAM) rendered patients with active replication eligible for transplantation, prevented recurrence post-OLT (unless LAM-resistant escape mutations developed) and improved the outcome of patients who became reinfected 13-17. The combination of HBIG and lamivudine enhanced prevention of HBV reinfection 14,18, and the advent of adefovir dipoxil (ADV) provided an safe and efficacious therapeutic option for patients with LAM-resistant infection 19. As a result of this progress in prevention and treatment of HBV reinfection, acute or chronic hepatitis B is now universally accepted as an excellent indication for OLT 8.…”

Section: Introductionmentioning

confidence: 99%

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Management of HBV Infection in Liver Transplantation Patients

Vierling

2005

Int. J. Med. Sci.

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A Ab bs st tr ra ac ct t In the absence of preventative therapy, reinfection of allografts with hepatitis B virus (HBV) after orthotopic liver transplantation (OLT) resulted in dismal allograft and patient survival. Major advances in the management of HBVinfected recipients of OLT during the past 15 years have steadily reduced the rate of reinfection, resulting in improved outcomes. Initially, long-term use of hepatitis B immune globulin (HBIG) as a source of anti-HBs antibodies was effective in preventing or delaying reinfection. Lamivudine monotherapy made it possible to suppress HBV replication prior to OLT, markedly decreasing the risk of reinfection. Although lamivudine monotherapy used before and after OLT could prevent reinfection, its effectiveness was limited by progressive development of lamivudine-resistant mutant infections. Combination therapy with HBIG and lamivudine after OLT reduced both HBV recurrence and the risk of lamivudine resistance even in patients with active HBV replication. Introduction of adefovir provided a safe, alternative oral antiviral able to treat effectively lamivudine-resistant mutants HBV. Available strategies to prevent reinfection have resulted in OLT outcomes for HBV-infected patients comparable to those for patients transplanted for non-HBV indications. In the future, combination therapies of HBIG and both nucleoside and/or nucleotide agents will undoubtedly be optimized. Development of new drugs to treat HBV will increase opportunities to combine agents to enhance safety, efficacy and prevent emergence of HBV escape mutants. New vaccines and adjuvants may make it possible to generate anti-HBs in immunosuppressed patients, eliminating the need for HBIG. K

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Section: Combination Therapies To Prevent Hbv Reinfection After Trmentioning

confidence: 99%

Section: Combination Therapies To Prevent Hbv Reinfection After Trmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Management of HBV Infection in Liver Transplantation Patients

Vierling

2005

Int. J. Med. Sci.

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“…Globally, 30% of cirrhosis and 53% of hepatocellular carcinoma cases are attributed to HBV, with liver transplantation (LT) as the main treatment option. From the mid-1990s until mid-2000s, the gold standard for prevention of HBV reinfection following LT has been hepatitis B immunoglobulin (HBIG) treatment with or without nucleos(t)ide antiviral analogues [2]. Over the past decade, more effective antiviral agents with low incidences of resistance (e.g.…”

Section: Introductionmentioning

confidence: 99%

Low incidence of acute rejection in hepatitis B virus positive liver transplant recipients and the impact of hepatitis B immunoglobulin

Veerappan

VanWagner

Mathew³

et al. 2016

Human Immunology

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Historically, hepatitis B virus (HBV) liver transplantation (LT) recipients have less acute cellular rejection (ACR) than those without HBV. We questioned whether this has persisted in an era of decreased Hepatitis B immunoglobulin use (HBIG) given its in vitro immunoregulatory effects. We compared the incidence, risk factors and outcomes of ACR among 40,593 primary LT recipients with HBV, hepatitis C, steatohepatitis, and immune liver disease (OPTN 2000–2011). We also assessed the in vitro effect of HBIG on alloimmune lymphoproliferation and regulatory T cell generation using mixed lymphocyte reactions. In multivariate analysis, HBV status remained a strong independent predictor of freedom from ACR (OR 0.58, 95% CI: 1.5–2.1). Patient (67.7% vs 72.3%) and graft (60.8% vs 69.1%) survival were significantly lower in patients with ACR versus no ACR for all causes except HBV. HBIG use had no statistical association with ACR. In vitro, HBIG at concentrations equivalent to clinical dosing did not inhibit lymphoproliferation or promote regulatory T cell development. In summary, the incidence and impact of ACR is lower now for HBV LT and does not appear to be secondary to HBIG by our in vitro and in vivo analyses. Rather, it may be due to the innate immunosuppressive properties of chronic HBV infection.

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“…Furthermore, combination prophylaxis with the use of HBIG and antiviral agents has reduced the risk of hepatitis B relapse to 10% or less in the first 2 years following transplantation [8], [9], [10], [11], [12]. As a result, the outcomes of patients with acute and chronic HBV related liver diseases undergoing LT are now similar to or better than those with non-HBV related liver transplantation [13], [14].…”

Section: Introductionmentioning

confidence: 99%

Large Fragment Pre-S Deletion and High Viral Load Independently Predict Hepatitis B Relapse after Liver Transplantation

Chen

Wang

et al. 2012

PLoS ONE

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Hepatitis B virus (HBV) associated end-stage liver diseases are the leading causes of liver transplantation (LT) in Taiwan. Relapse of hepatitis B occurs after LT, raising the risk of graft failure and reducing patient survival. Although several oral antiviral agents have been approved for anti-HBV treatment, lamivudine (LAM) remained to be the most widely used preventive regimen in Taiwan. While several clinical predictors have been identified for hepatitis B relapse, the predictive roles of the histopathological characteristics in liver explants as well as the genotypic features of the viruses in pre-LT serum samples have not been assessed. Between September 2002 and August 2009, 150 consecutive hepatitis B surface antigen (HBsAg) positive patients undergoing LT were included for outcome analysis following assessment of the clinicopathological and virological factors prior to LT. Kaplan-Meier analyses discovered that pre-operative LAM treatment ≤3 months; membranous distribution and higher expression of tissue HBsAg in liver explants; preoperative viral load ≧106 copies/ml; and presence of large fragment (>100 base pairs) pre-S deletion (LFpreSDel) correlated significantly with hepatitis B relapse. Multivariate Cox regression analysis showed that the presence of LFpreSDel (P = 0.001) and viral load ≧106 copies/mL (P = 0.023) were independent predictors for hepatitis B relapse. In conclusion, besides high viral load, LFpreSDel mutation is an important independent predictor for hepatitis B relapse after LT. More aggressive preventive strategies should be applied for patients carrying these risk factors.

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An efficacy and cost-effectiveness analysis of combination hepatitis B immune globulin and lamivudine to prevent recurrent hepatitis B after orthotopic liver transplantation compared with hepatitis B immune globulin monotherapy

Cited by 210 publications

References 35 publications

Management of HBV Infection in Liver Transplantation Patients

Management of HBV Infection in Liver Transplantation Patients

Low incidence of acute rejection in hepatitis B virus positive liver transplant recipients and the impact of hepatitis B immunoglobulin

Large Fragment Pre-S Deletion and High Viral Load Independently Predict Hepatitis B Relapse after Liver Transplantation

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