|
- 现金
- 62111 元
- 精华
- 26
- 帖子
- 30437
- 注册时间
- 2009-10-5
- 最后登录
- 2022-12-28
|
Anti-Hep B Tx Drives Changes in Liver Transplantation
by Scott Harris
Contributing Writer, MedPage Today
Action Points
Powerful anti-hepatitis B virus drugs can potentially decrease the recurrence of the HBV in liver transplant patients, and even lower the number of transplants that result from complications related to HBV.
Note that the patients who developed breakthrough hepatitis B infection improved after they were switched from monotherapy to a different oral agent or a combination of agents.
Powerful anti-hepatitis B virus (HBV) drugs can potentially decrease the recurrence of the HBV in liver transplant patients, and even lower the number of transplants that result from complications related to HBV, according to a retrospective study.
After a median follow-up of 82 months, the rate of post-liver transplant survival was 89% and the rate of HBV recurrence was 11% in over 100 patients, reported Waleed Al-Hamoudi, MD, of King Saud University College of Medicine in Riyadh, and colleagues.
In addition, from 2001 to 2006, 50% of the liver transplants performed at the center were caused by cirrhosis induced by the hepatitis C virus, while 17% of the transplants were caused by HBV-induced cirrhosis, and 12% by nonalcoholic steatohepatitis-related cirrhosis (NASH), they wrote in the World Journal of Gastroenterology.
From January 2007 to January 2012, HBV fell behind NASH to become the third-leading indication for liver transplant, with 16% of all cases, they added.
"The use of highly potent anti-hepatitis B virus agents has led to adequate control of viral replication, significant biochemical remission, histological improvement, and the prevention of hepatic decompensation," they explained. "These effects are expected to subsequently result in a reduction in the rate of hepatitis B virus-related liver transplantation."
The study included data from 133 patients who underwent liver transplants for HBV-related cirrhosis at Saudi Arabia's King Faisal Specialist Hospital and Research Center from 1990 to 2012.
The majority of the patients were treated with HBV immune globulin and at least one nucleos(t)ide analog drug, such as lamivudine (Epivir), adefovir (Hepsera), entecavir (Baraclude), or tenofovir (Viread). The immune globulin was administered intravenously at a dose of 10,000 units during the anhepatic phase and 5,000 units daily during the first week, with an ultimate target being an HBV surface antibody titer of >500 IU/mL.
The authors reported that patients who were positive for the HBV antigen before a liver transplant were more likely to experience recurrence versus those who tested negative for the antigen (OR=9.6, 95% CI 2.99 to 30.85, P<0.0001). Patients with positive HBV DNA levels before a transplant were almost four times as likely to experience a recurrence than those who did not (OR=4.1, 95% CI 1.08 to 15.5, P=0.04), according to the study.
"The availability of a newer generation of nucleos(t)ide analogs has resulted in a significant improvement in the outcome of liver transplantation for hepatitis B virus-related liver disease," the authors wrote. "Controlling viral replication ... will improve transplantation outcomes."
Among pretransplant patients, the majority (61%) took lamivudine, followed by a combination of lamivudine and adefovir (15%). The disease recurred in only 15 patients (11%) after transplantation.
The 15 patients who developed breakthrough hepatitis B infection -- defined in the study as a "re-emergence of hepatitis B virus DNA or hepatitis B surface antigen" -- improved after they were switched from monotherapy to a different oral agent or a combination of agents.
"The development of potent hepatitis B virus drugs with high genetic barriers to resistance has resulted in significant suppression of viral replication," the authors wrote. "As a result, overall patient survival has improved due to the prevention of disease progression to cirrhosis ...The decline in hepatitis B-related liver disease as an indication for liver transplantation is likely related both to the various mass screening programs ... and to the introduction of effective antiviral treatment."
Furthermore, 71 of 96 patients treated with tenofovir experienced a regression of their cirrhosis, which was confirmed through paired biopsies after 5 years.
"This finding could be related to improvements in the control of viral replication with potent medications (entecavir and tenofovir), which has prevented the progression of liver disease to more advanced stages of fibrosis and has prevented decompensation in already cirrhotic patients," they stated.
The study had some limitations including its retrospective design. Also, HBV immunoprophylaxis during the posttransplant follow-up period was not consistent for all patients, and data on pretransplantation HBV DNA status, pretransplantation HBV serological markers, and HDV coinfection were not available for some of the participants.
|
|
发表于 2015-8-27 16:51