Service de Rhumatologie, Centre Hospitalier Universitaire Conception, 147 Boulevard Baille, 13385 Marseille, France.
Arthritis Res Ther. 2009;11(6):R179. doi: 10.1186/ar2868. Epub 2009 Nov 26.
Reactivation of hepatitis B virus (HBV) infection in patients with past infection has been described in 5% to 10% of individuals undergoing immunosuppressive therapies. No data are available to date on the outcome of patients treated by tumour necrosis factor-alpha (TNFalpha) inhibitors for chronic arthritis with a serological pattern of past HBV infection. The aim of our study was to monitor HBV markers in HBV surface antigen (HBsAg)-negative/anti-HBcAb-positive patients treated with a TNFalpha inhibitor for inflammatory arthritides.
Twenty-one HBsAg-negative/anti-HBcAb-positive patients were included. HBV serological patterns were compared with those determined before starting TNFalpha inhibitors. Serum HBV DNA testing by polymerase chain reaction was additionally performed. Spearman correlation analysis was used and P < 0.05 was chosen as the significance threshold.
Before starting therapy, mean anti-HBsAb titre was 725 IU/L, no patient had an anti-HBsAb titre <10 IU/L, and 18 patients had an anti-HBsAb >100 IU/L. At a mean time of 27.2 months following therapy introduction, mean anti-HBsAb titre was 675 IU/L and anti-HBsAb titre remained >100 IU/L in 17 patients. There was a strong correlation between the first and second anti-HBsAb titres (r = 0.98, P = 0.013). Moreover, no patient had an anti-HBsAb titre below 10 IU/L or HBV reactivation (HBsAg seroreversion or positive HBV DNA detection). However, the anti-HBsAb titre decreased by more than 30% in 6 patients. The mean anti-HBsAb titre at baseline was significantly lower (P = 0.006) and the mean duration of anti-TNFalpha therapy, although non-significant (P = 0.09), was longer in these six patients as compared to patients without a decrease in anti-HBsAb titre.
Anti-TNFalpha treatments are likely to be safe in patients with past hepatitis B serological pattern. However, the significant decrease of anti-HBsAb titre observed in a proportion of patients deserves HBV virological follow-up in these patients, especially in those with a low anti-HBsAb titre at baseline.
在接受免疫抑制治疗的患者中,有 5%至 10%的患者曾出现乙型肝炎病毒(HBV)再激活感染。目前尚无关于使用肿瘤坏死因子-α(TNFα)抑制剂治疗慢性关节炎且 HBV 感染血清学模式为既往感染的患者结局的数据。我们研究的目的是监测 HBsAg 阴性/抗-HBcAb 阳性患者在接受 TNFα 抑制剂治疗炎症性关节炎时 HBV 标志物的变化。
共纳入 21 名 HBsAg 阴性/抗-HBcAb 阳性患者。将 HBV 血清学模式与开始使用 TNFα 抑制剂前的结果进行比较。另外还进行了聚合酶链反应法检测血清 HBV DNA。采用 Spearman 相关性分析,选择 P < 0.05 作为显著性阈值。
在开始治疗前,平均抗-HBsAb 滴度为 725 IU/L,无患者的抗-HBsAb 滴度<10 IU/L,18 名患者的抗-HBsAb 滴度>100 IU/L。在开始治疗后平均 27.2 个月时,平均抗-HBsAb 滴度为 675 IU/L,17 名患者的抗-HBsAb 滴度仍>100 IU/L。首次和第二次抗-HBsAb 滴度之间存在很强的相关性(r = 0.98,P = 0.013)。此外,无患者的抗-HBsAb 滴度<10 IU/L 或 HBV 再激活(HBsAg 血清学转换或 HBV DNA 检测阳性)。然而,有 6 名患者的抗-HBsAb 滴度下降超过 30%。这 6 名患者的基线抗-HBsAb 滴度显著较低(P = 0.006),尽管无统计学意义(P = 0.09),但他们接受抗-TNFα 治疗的平均时间较长。
在过去有 HBV 血清学模式的患者中,使用抗-TNFα 治疗可能是安全的。然而,在一部分患者中观察到抗-HBsAb 滴度显著下降,这些患者需要进行 HBV 病毒学随访,特别是在基线时抗-HBsAb 滴度较低的患者。
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