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肝移植后拉米夫定耐药乙型肝炎感染的发生情况及临床结局

Occurrence and clinical outcome of lamivudine-resistant hepatitis B infection after liver transplantation.

作者信息

Seehofer D, Rayes N, Steinmüller T, Müller A R, Settmacher U, Neuhaus R, Radke C, Berg T, Hopf U, Neuhaus P

机构信息

Department of General, Visceral, and Transplant Surgery, Campus Virchow, Humboldt University of Berlin, Germany.

出版信息

Liver Transpl. 2001 Nov;7(11):976-82. doi: 10.1053/jlts.2001.28442.

Abstract

Lamivudine treatment of hepatitis B after orthotopic liver transplantation (OLT) is often accompanied by fast viral-resistance formation. Although no clinical data are available, in vitro data indicate that lamivudine-resistant reinfection has a mild course because of defective viral replication. Between 1996 and 1999, a total of 34 patients were treated with lamivudine because of hepatitis B recurrence after OLT. All patients developed reinfection despite long-term passive immunoprophylaxis with hepatitis B immunoglobulin, diagnosed by positive hepatitis B surface antigen and positive hepatitis B virus (HBV) DNA. Before treatment with lamivudine, 21 of these patients underwent a course of famciclovir and developed resistance. Monthly laboratory tests and sequential liver biopsies were performed during the follow-up period. Nineteen of 34 patients (56%) developed lamivudine resistance during the follow-up period of 12 to 49 months. One- and 3-year graft survival rates after the diagnosis of lamivudine resistance were 89% and 66%, respectively. In most cases, lamivudine resistance was associated with high viral replication (3,012 +/- 574 pg/mL 1 month after the diagnosis of lamivudine resistance); however, liver enzyme levels were only moderately elevated (alanine aminotransferase [ALT], 45 +/- 16 U/L). Only 3 patients (15%) showed a rapid increase in ALT level to more than 500 U/L within 3 months after resistance developed. All other patients had mildly elevated liver enzyme levels during the first 6 to 8 months after lamivudine resistance. In the later course, liver enzyme levels increased in most patients. Fourteen patients with elevated transaminase levels were switched to lamivudine plus interferon alfa (n = 8) or lamivudine plus famciclovir therapy (n = 6). This combination was successful in most cases, decreasing HBV DNA and liver enzyme levels. Four patients with lamivudine resistance died during follow-up, only 1 patient because of HBV reinfection. In addition, 2 patients underwent retransplantation because of hepatitis B cirrhosis of the first graft. Compared with historic courses of wild-type recurrence, lamivudine-resistant reinfection is characterized by a milder clinical course. Fulminant cases were not observed; however, in three cases, chronic liver failure developed. The combination of different antivirals diminished viral replication after lamivudine resistance. In the future, new antiviral agents, such as adefovir, might further expand therapeutic options.

摘要

原位肝移植(OLT)后使用拉米夫定治疗乙型肝炎常伴有快速的病毒耐药性形成。虽然尚无临床数据,但体外数据表明,由于病毒复制缺陷,拉米夫定耐药再感染的病程较轻。1996年至1999年期间,共有34例患者因OLT后乙型肝炎复发接受拉米夫定治疗。尽管长期使用乙型肝炎免疫球蛋白进行被动免疫预防,但所有患者均发生了再感染,通过乙型肝炎表面抗原阳性和乙型肝炎病毒(HBV)DNA阳性确诊。在使用拉米夫定治疗前,其中21例患者接受了泛昔洛韦疗程并产生了耐药性。在随访期间进行了每月的实验室检查和系列肝活检。34例患者中有19例(56%)在12至49个月的随访期间出现了拉米夫定耐药。拉米夫定耐药诊断后的1年和3年移植物存活率分别为89%和66%。在大多数情况下,拉米夫定耐药与高病毒复制相关(拉米夫定耐药诊断后1个月为3,012±574 pg/mL);然而,肝酶水平仅中度升高(丙氨酸转氨酶[ALT],45±16 U/L)。只有3例患者(15%)在耐药发生后3个月内ALT水平迅速升高至超过500 U/L。所有其他患者在拉米夫定耐药后的最初6至8个月内肝酶水平轻度升高。在病程后期,大多数患者的肝酶水平升高。14例转氨酶水平升高的患者改用拉米夫定加干扰素α(n = 8)或拉米夫定加泛昔洛韦治疗(n = 6)。这种联合治疗在大多数情况下是成功的,降低了HBV DNA和肝酶水平。4例拉米夫定耐药患者在随访期间死亡,仅1例因HBV再感染死亡。此外,2例患者因首次移植物的乙型肝炎肝硬化接受了再次移植。与野生型复发的既往病程相比,拉米夫定耐药再感染的临床病程较轻。未观察到暴发性病例;然而,有3例患者发生了慢性肝衰竭。不同抗病毒药物联合使用可在拉米夫定耐药后减少病毒复制。未来,诸如阿德福韦等新型抗病毒药物可能会进一步扩大治疗选择。

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