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肝移植后,通过大剂量乙肝免疫球蛋白筛选出具有抗原性改变的乙肝表面抗原的乙肝病毒。

Hepatitis B virus with antigenically altered hepatitis B surface antigen is selected by high-dose hepatitis B immune globulin after liver transplantation.

作者信息

Protzer-Knolle U, Naumann U, Bartenschlager R, Berg T, Hopf U, Meyer zum Büschenfelde K H, Neuhaus P, Gerken G

机构信息

First Medical Department, Johannes Gutenberg-University, Mainz, Germany.

出版信息

Hepatology. 1998 Jan;27(1):254-63. doi: 10.1002/hep.510270138.

Abstract

"Escape" variants of hepatitis B virus (HBV) can cause infection despite previous immunization. These viruses show alterations of the immunogenic major hydrophilic loop of the HBV small surface protein (s-protein). We studied whether HBV "escape" variants were selected in patients with graft infection after liver transplantation for HBV-related diseases who received passive immunoprophylaxis with high-dose polyclonal hepatitis B hyperimmune globulin (HBIG). For that, pre- and posttransplantation sera of 34 patients were analyzed for the occurence of HBV S-gene variants. In addition, binding of in vitro-translated variant s-proteins to HBIG was studied. Variants with exchanges of amino acid (aa) 144 (s144) in HBV genotype A and 145 in genotype D (s145) were found to emerge, persist, and predominate during HBIG, and thus fulfilled criteria of "escape" variants selected. In addition to already-known variants sG145R/K/E, we could demonstrate that newly described variants sX144G and sG145A were antigenically altered and showed impaired recognition by polyclonal HBIG in vitro. Diminished recognition of variant s-proteins correlated with the failure of HBIG to prevent infection of the liver graft with antigenically altered variant HBV Patients infected with "escape" variants s144 or s145 showed a worse clinical outcome compared with the other patients on high-dose, long-term HBIG prophylaxis (44% vs. 23% graft failure caused by HBV infection). Our results suggest that antigenically altered HBV variants s144 and s145 can be selected by HBIG and can influence clinical outcome after liver transplantation.

摘要

乙型肝炎病毒(HBV)的“逃逸”变异株即使在先前已接种疫苗的情况下仍可导致感染。这些病毒的乙型肝炎病毒小表面蛋白(s蛋白)的免疫原性主要亲水性环发生了改变。我们研究了在接受高剂量多克隆乙型肝炎免疫球蛋白(HBIG)进行被动免疫预防的HBV相关疾病肝移植患者的移植物感染中,是否会选择出HBV“逃逸”变异株。为此,分析了34例患者移植前和移植后的血清中HBV S基因变异的发生情况。此外,还研究了体外翻译的变异s蛋白与HBIG的结合情况。发现在HBIG治疗期间,乙型肝炎病毒A基因型中氨基酸(aa)144(s144)和D基因型中145(s145)发生交换的变异株出现、持续存在并占主导地位,因此符合被选择的“逃逸”变异株标准。除了已知的变异株sG145R/K/E外,我们还证实新描述的变异株sX144G和sG145A在抗原性上发生了改变,并且在体外显示出被多克隆HBIG识别的能力受损。变异s蛋白识别能力的降低与HBIG未能预防肝脏移植物被抗原性改变的变异HBV感染相关。与接受高剂量、长期HBIG预防的其他患者相比,感染“逃逸”变异株s144或s145的患者临床结局更差(HBV感染导致的移植失败率分别为44%和23%)。我们的结果表明,抗原性改变的HBV变异株s144和s145可被HBIG选择出来,并可影响肝移植后的临床结局。

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