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The role of HBsAg quantification for monitoring natural history and treatment outcome

机译:HBsAg定量在监测自然病史和治疗结果中的作用

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摘要

Since its discovery by Blumberg in 1965, the hepatitis B virus antigen (HBsAg) is used as the fingerprint of hepatitis B infection. The HBsAg level is a reflection of the transcriptional activity of cccDNA. It is an important marker that not only indicates active hepatitis B infection but can also predict clinical and treatment outcomes. Assays for HBsAg quantification are fully automated and have high output. HBsAg titres are higher in HBe antigen (HBeAg)(+) than in HBeAg(-) patients and are negatively correlated with liver fibrosis in HBeAg(+) patients. In HBeAg(-) chronic hepatitis B, an HBsAg level <1000 IU/ml and an HBV DNA titre <2000 IU/ml accurately identify inactive carriers. During PEG-IFN treatment, HBsAg quantification is used to identify patients who will not benefit from therapy as early as week 12 on therapy, so that treatment may be stopped or switched- 'week 12 stopping rule'. With nucleos(t)ide analogues (NA), the role of HBsAg quantification must be clarified. Several studies show that baseline and on-treatment HBsAg levels might identify patients that can be treated with no subsequent risk of reactivation. In clinical practice, HBsAg quantification is a simple and reproducible tool that can be used in association with HBV DNA to classify patients during the natural history of HBV and to monitor therapy.
机译:自1965年由布隆伯格(Blumberg)发现以来,乙肝病毒抗原(HBsAg)被用作乙肝感染的指纹。 HBsAg水平反映了cccDNA的转录活性。它是重要的标志物,不仅表明活动性乙型肝炎感染,而且还可以预测临床和治疗结果。 HBsAg定量测定是全自动的,具有很高的产量。 HBe抗原(HBeAg)(+)中的HBsAg滴度高于HBeAg(-)患者,并且与HBeAg(+)患者的肝纤维化呈负相关。在HBeAg(-)慢性乙型肝炎中,HBsAg水平<1000 IU / ml和HBV DNA滴度<2000 IU / ml可以准确识别出非活性携带者。在PEG-IFN治疗期间,HBsAg定量可用于识别最早在治疗第12周不能从治疗中受益的患者,因此可以停止治疗或改用“第12周停止规则”。对于核苷酸(t)化物类似物(NA),必须阐明HBsAg定量的作用。几项研究表明,基线和治疗中的HBsAg水平可能会确定可以接受治疗的患者,而没有随后的重新激活风险。在临床实践中,HBsAg定量是一种简单且可重复的工具,可与HBV DNA结合使用,以在HBV的自然病程中对患者进行分类并监测治疗。

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