[拉米夫定治疗后实现HBeAg持续血清学转换的乙肝病毒特异性CD8 + T细胞]

[HBV-specific CD8+ T cells for sustained HBeAg seroconversion after lamivudine therapy].

作者信息

Lee Chun Kyon, Han Kwang-Hyub, Suh Jeong Hun, Cho Young Suk, Won Sun Young, Chon Chae Yoon, Moon Young Myoung, Park In Suh

机构信息

Department of Internal Medicine, National Health Insurance Corporation Ilsan Hospital, Koyang, Korea.

出版信息

Korean J Hepatol. 2005 Mar;11(1):34-42.

PMID:15788883

Abstract

BACKGROUND/AIMS: Viral suppression of the hepatitis B virus (HBV) can be induced by lamivudine, but the relapse seen in many patients after cessation of lamivudine therapy is troublesome. We thought that the host immune response is important to prevent viral relapse. We compared the frequency of HBV-specific CD8+ T cells in the peripheral blood and their expansion capacity after exposure to viral antigen between the patients showing sustained HBeAg seroconversion after use of lamivudine and those patients without sustained response.

METHODS

We analyzed HBV-specific CD8+ T cells that were isolated from the blood of 14 patients with HLA-A2 who showed lamivudine induced HBeAg seroconversion (HBV DNA < 0.5 pg/mL, and the cells were negative for HBeAg) at the end of lamivudine therapy. The purified T cells were directly stained ex vivo, after they had been stimulate with synthetic peptide, using the HBV core 18-27-specific HLA tetramer (Tc 18-27) and monoclonal antibody to CD8. The HBV viral load was quantified by the Amplicor HBV Monitor assay.

RESULTS

In patients with a sustained HBeAg response (the sustained group) for a duration of 15.5 months of follow-up, the median number of Tc 18-27 cells out of the 5 X 10(4) CD8+ T cells was 49.5 (15-135). On the contrary, in patients who experienced relapse (the relapsed group) during a median of 7.5 months of follow-up, the median number of Tc 18-27 cells out of the 5 X 10(4) CD8+ T cells was 13.5 (0-95). Especially, among patients with a viral load of HBV DNA < 1 X 10(3) copies at the end of treatment, the median number of Tc 18-27 cells out of 5 X 10(4) CD8+ T cells was 87 (45-135) in sustained group compared to 12 (6-50) in the relapsed group. All patients in the sustained group demonstrated a vigorous expansion of the core 18-27-specific CD8+ T cells after stimulation with viral peptide, in contrast to only 3 out of 8 patients in the relapsed group.

CONCLUSIONS

This study demonstrates that the frequency and functional responsiveness of the circulating HBV-specific CD8+ T cells may be important for obtaining a sustained HBeAg response to lamivudine.

摘要

背景/目的：拉米夫定可诱导乙型肝炎病毒（HBV）的病毒抑制，但许多患者在拉米夫定治疗停止后出现的复发情况很棘手。我们认为宿主免疫反应对于预防病毒复发很重要。我们比较了拉米夫定治疗后出现持续HBeAg血清学转换的患者与未出现持续反应的患者外周血中HBV特异性CD8 + T细胞的频率及其在接触病毒抗原后的扩增能力。

方法

我们分析了从14例HLA - A2患者血液中分离出的HBV特异性CD8 + T细胞，这些患者在拉米夫定治疗结束时出现拉米夫定诱导的HBeAg血清学转换（HBV DNA < 0.5 pg/mL，且细胞HBeAg为阴性）。纯化的T细胞在用合成肽刺激后，使用HBV核心18 - 27特异性HLA四聚体（Tc 18 - 27）和抗CD8单克隆抗体进行体外直接染色。通过Amplicor HBV Monitor检测法定量HBV病毒载量。

结果

在随访15.5个月的持续HBeAg反应患者（持续组）中，每5×10⁴ CD8 + T细胞中Tc 18 - 27细胞的中位数为49.5（15 - 135）。相反，在随访中位数为7.5个月期间出现复发的患者（复发组）中，每5×10⁴ CD8 + T细胞中Tc 18 - 27细胞的中位数为13.5（0 - 95）。特别是，在治疗结束时HBV DNA病毒载量< 1×10³拷贝的患者中，持续组每5×10⁴ CD8 + T细胞中Tc 18 - 27细胞的中位数为87（45 - 135），而复发组为12（6 - 50）。持续组的所有患者在用病毒肽刺激后均表现出核心18 - 27特异性CD8 + T细胞的强烈扩增，相比之下，复发组8例患者中只有3例如此。