Tchervenkov J I, Tector A J, Barkun J S, Sherker A, Forbes C D, Elias N, Cantarovich M, Cleland P, Metrakos P, Meakins J L
Department of Surgery, McGill University, Montreal, Quebec, Canada.
Ann Surg. 1997 Sep;226(3):356-65; discussion 365-8. doi: 10.1097/00000658-199709000-00015.
The authors determined whether pretransplant reduction of hepatitis B virus (HBV) load using alpha-interferon-2b (IFN) and passive immunoprophylaxis using hepatitis B immunoglobulin (HBIg) posttransplantation can prevent HBV recurrence in patients undergoing liver transplantation (LT) for HBV cirrhosis.
Liver transplantation in patients with HBV cirrhosis is associated with a high rate of recurrence and reduced survival. In patients with evidence of replicating virus (HBV-DNA or hepatitis B e antigen [HBeAg]-positive serum or both), recurrence is nearly universal. Passive immunoprophylaxis with HBIg alone is not effective in preventing HBV recurrence posttransplant, especially in patients with evidence of active viral replication pretransplant. Higher doses of HBIg posttransplant has reduced recurrence rates to 30% to 50%. Lamivudine, a nucleoside analogue that has shown early promise, also is associated with significant HBV recurrence. The authors report a reliable method of preventing viral recurrence in patients even with evidence for active HBV replication pretransplant.
Pretransplant patients with evidence of replicating HBV were given IFN starting at 1 million IU 3 times per week subcutaneously. This dose was increased to 2 and then 3 million IU 3 times per week when patient's side effects permitted and was maintained until the patient underwent a LT. All patients were tested every 4 weeks for hepatitis B surface antigen (HBsAg), HBeAg, and HBV-DNA. When patients became negative for HBeAg and HBV-DNA, they were listed for LT. Patients that were only HBsAg positive were listed immediately and received a LT without prior IFN treatment. Post-LT, all patients began receiving HBIg 2000 IU (10 mL) daily from days 1 to 20 and then weekly for the first 2 years. After 2 years, all patients received 2000 IU (10 mL) monthly. Additional HBIg immunoprophylaxis was given during intense immunosuppression for rejection. Posttransplant serum was tested for HBsAg, HBeAg, and HBV-DNA in all patients 1 week, 1 month, and every 3 months thereafter. Liver biopsies were done at least yearly and when liver enzymes were abnormal and were always tested for HBsAg and HBcAg by immunoperoxidase.
Thirteen patients with decompensated HBV cirrhosis were transplanted. Pretransplant, eight patients had evidence of active viral replication at the initial assessment (HBeAg or HBV-DNA-positive serum or both). All eight were successfully treated with IFN (median duration, 24 weeks; range, 8-53) and converted to a negative status before transplantation. Side effects from IFN were minimal and well tolerated, except in one patient who required 6 million IU to convert to a nonreplicating status. The five patients that were only HBsAg positive were not treated with IFN pretransplant. After surgery, HBIg given as described achieved consistently serum levels greater than 1000 IU/L. Twelve of the 13 patients are alive with normal liver function and without serologic evidence of HBV recurrence at a median follow-up of 32 months (range, 9-56 months). None have evidence of HBV recurrence as measured by serum HBsAg/HBeAg/HBV-DNA at recent follow-up. The sera of the seven longest survivors has tested negative for HBV-DNA using the polymerase chain reaction method. In addition, a liver biopsy was obtained in six of these patients, the results of which also tested negative for HBV-DNA using polymerase chain reaction. Liver biopsy specimens have been negative for the presence of HBsAg and HBcAg by immunoperoxidase staining in all 12 patients.
A reduction of viral load pretransplant with IFN and posttransplant HBIg prevents recurrence of hepatitis B and permits LT for HBV cirrhosis, even in patients with evidence of replicating virus. The IFN pretransplant was well tolerated, and the small frequent dosing of HBIg posttransplant did not cause side effects while achieving serum levels > 1000 IU/L.
作者确定移植前使用α-干扰素-2b(IFN)降低乙肝病毒(HBV)载量以及移植后使用乙肝免疫球蛋白(HBIg)进行被动免疫预防能否预防因HBV肝硬化而接受肝移植(LT)患者的HBV复发。
HBV肝硬化患者的肝移植与高复发率和生存率降低相关。在有病毒复制证据(HBV-DNA或乙肝e抗原[HBeAg]阳性血清或两者皆有)的患者中,复发几乎是普遍现象。单独使用HBIg进行被动免疫预防对预防移植后HBV复发无效,尤其是在移植前有病毒活跃复制证据的患者中。移植后更高剂量的HBIg已将复发率降低至30%至50%。拉米夫定,一种早期显示有前景的核苷类似物,也与显著的HBV复发相关。作者报告了一种即使在移植前有活跃HBV复制证据的患者中预防病毒复发的可靠方法。
移植前有HBV复制证据的患者皮下注射IFN,起始剂量为每周三次,每次100万国际单位。当患者副作用允许时,剂量增加至每周三次,每次200万国际单位,然后增加至300万国际单位,并维持至患者接受LT。所有患者每4周检测一次乙肝表面抗原(HBsAg)、HBeAg和HBV-DNA。当患者HBeAg和HBV-DNA转阴时,将其列入LT名单。仅HBsAg阳性的患者立即列入名单并在未接受IFN预处理的情况下接受LT。LT后,所有患者从第1天至第20天每天开始接受2000国际单位(10毫升)HBIg,然后在头2年每周接受一次。2年后,所有患者每月接受2000国际单位(10毫升)。在因排斥反应进行强化免疫抑制期间给予额外的HBIg免疫预防。所有患者在术后1周、1个月以及此后每3个月检测血清中的HBsAg、HBeAg和HBV-DNA。至少每年进行一次肝活检,当肝酶异常时也进行肝活检,并始终通过免疫过氧化物酶检测HBsAg和HBcAg。
13例失代偿性HBV肝硬化患者接受了移植。移植前,8例患者在初始评估时有病毒活跃复制证据(HBeAg或HBV-DNA阳性血清或两者皆有)。所有8例患者均成功接受IFN治疗(中位持续时间,24周;范围,8 - 53周)并在移植前转为阴性状态。IFN的副作用极小且耐受性良好,除了1例患者需要600万国际单位才能转为非复制状态。5例仅HBsAg阳性的患者移植前未接受IFN治疗。手术后,按所述给予的HBIg始终使血清水平高于1000国际单位/升。13例患者中有12例存活,肝功能正常,在中位随访32个月(范围,9 - 56个月)时无HBV复发的血清学证据。在最近的随访中,通过血清HBsAg/HBeAg/HBV-DNA检测,无一例有HBV复发的证据。7例存活时间最长的患者的血清使用聚合酶链反应方法检测HBV-DNA为阴性。此外,其中6例患者进行了肝活检,其结果使用聚合酶链反应检测HBV-DNA也为阴性。所有12例患者的肝活检标本通过免疫过氧化物酶染色检测HBsAg和HBcAg均为阴性。
移植前使用IFN降低病毒载量以及移植后使用HBIg可预防乙肝复发,并允许对HBV肝硬化患者进行LT,即使是有病毒复制证据的患者。移植前使用IFN耐受性良好,移植后频繁小剂量使用HBIg在达到血清水平>1000国际单位/升时未引起副作用。
