后自发和核苷（酸）类似物IDE治疗乙肝表面抗原血清学清除

StephenW

Clinical outcomes after spontaneous and nucleos(t)ide analogue-treated HBsAg seroclearance in chronic HBV infection

    Y. C. Chen1,2,*, W. J. Jeng1,2, R. N. Chien3, C. M. Chu1,2 andY. F. Liaw1

Article first published online: 12 APR 2016

DOI: 10.1111/apt.13630

© 2016 John Wiley & Sons Ltd

Issue
Cover image for Vol. 43 Issue 10
Alimentary Pharmacology & Therapeutics

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Summary
Background

Both spontaneous and nucleos(t)ide analogue (Nuc)-treated hepatitis B surface antigen (HBsAg) seroclearance are associated with excellent clinical outcomes.
Aim

To conduct a case–control study to explore whether there is difference of clinical outcomes between these two groups.
Methods

A total of 312 chronic hepatitis B patients with spontaneous HBsAg seroclearance and 110 patients with Nuc-treated HBsAg seroclearance were recruited retrospectively. Propensity score (PS) matching method produced 98 patients in each group for comparison. The development of hepatocellular carcinoma (HCC), hepatic complications and cumulative incidence of antibody to HBsAg (anti-HBs) was compared.
Results

During a mean follow-up period of 107 months after HBsAg seroclearance, five patients developed HCC after a mean period of 75.3 months (four and one patients with spontaneous and Nuc-treated HBsAg seroclearance, respectively) in overall population. One died of pneumonia with sepsis and one experienced variceal bleeding in Nuc-treated patients but none in spontaneous group. The incidence of anti-HBs seroconversion was comparable between spontaneous and Nuc-treated HBsAg seroclearance (69.6% vs. 66.4%, respectively, P = 0.617). There were no significant differences in HCC development (2% vs. 1.1%), overall mortality (0% vs. 1%), variceal bleeding (0% vs. 4.2%) and 6-year cumulative incidence of anti-HBs seroconversion (62.3% vs. 61.5%) among PS-matched patients with spontaneous and Nuc-treated HBsAg seroclearance.
Conclusions

The clinical outcomes between patients with spontaneous and Nuc-treated HBsAg seroclearance are comparable. HCC can develop at a low rate during long-term follow-up and periodic surveillance after HBsAg seroclearance is still mandatory.

StephenW

后自发和核苷（酸）类似物IDE治疗乙肝表面抗原血清学清除慢性乙型肝炎临床转归

    Y. C. Chen1,2，* W. J. Jeng1,2，R. N. Chien3，C. M. Chu1,2安迪。 F. Liaw1

文章首次在线发表时间：2016年4月12日

DOI：10.1111 / apt.13630

2016年©约翰·威利父子有限公司

问题
封面图片的卷。 43第10期
消化系统药理学和治疗

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概要
背景

自发性和核苷（酸）类似物IDE（NUC）治疗乙肝表面抗原（HBsAg）血清学清除与优异的临床结果。
目标

要进行病例对照研究，探讨是否有这两个群体之间的临床结果的差异。
方法

共有312慢性乙型肝炎患者自发转阴的HBsAg和110例NUC-治疗乙肝表面抗原血清学清除进行回顾性招聘。倾向评分（PS）的匹配方法产生98各组患者进行比较。肝细胞癌（HCC），肝并发症和抗体对HBsAg（抗HBs）的累积发生率的发展进行比较。
结果

在乙肝表面抗原血清学清除后107个月，平均随访时间，五名患者为75.3个月（四个例患者自发性和国统会处理的HBsAg血清学清除，分别）在总人口平均期后发生HCC。其中死于肺炎在自发组败血症和国统会治疗一个病人经验丰富的静脉破裂出血，但没有。抗-HBs阳转的发生是自发的和国统会处理的HBsAg血清学清除（69.6％和66.4％，分别为P = 0.617）之间的可比性。有在HCC的发展（2％和1.1％），总死亡率（0％对1％），静脉曲张出血（0％对4.2％）和抗HBs血清转换的6年累计发生率（无显著差异62.3％对61.5％），PS-匹配的患者自发的和国统会处理的HBsAg血清学清除之列。
结论

患者自发和国统会处理的HBsAg血清学清除的临床结果具有可比性。 HCC可以在长期随访和定期监督率低开发后的HBsAg血清学清除仍然是必须的。

StephenW

HCC development and hepatic complications after HBsAg seroclearance

Of the 312 patients with spontaneous HBsAg seroclearance, four male patients developed HCC during follow-up. A 49-year-old noncirrhotic, genotype C patient developed HCC 61.5 months after HBsAg seroclearance. The remaining three patients were 52, 53 and 63 years of age and had evidence of cirrhosis at the time of HBsAg seroclearance (2 genotype B and 1 undetermined) and HCC occurred 110.2, 117.2 and 31 months, respectively, after HBsAg seroclearance. Of the 110 Nuc-treated patients with HBsAg seroclearance, a 59-year-old noncirrhotic, genotype B male patient developed HCC 56.7 months after HBsAg seroclearance. The estimated annual incidence of HCC development was 0.13% and 0.14% in spontaneous and Nuc-treated groups, respectively (P = 0.906). The estimated annual incidence of HCC development was corrected with SIR and the corresponding figures were 0.13% and 0.16%, respectively. In Nuc-treated group, one patient died of pneumonia with sepsis and another patient with pre-existing cirrhosis experienced oesophageal variceal bleeding during follow-up. None of patients in spontaneous group died or had subsequent hepatic complication. Among the PS-matched patients, there was no significant difference in HCC development (2% vs. 1.1%), overall mortality (0% vs. 1%) and variceal bleeding episode (0% vs. 4.2%) (P = 1.000) (Table 2). The estimated annual incidence of HCC was comparable between spontaneous and Nuc-treated groups (0.31% vs. 0.16%, P = 0.735).

After excluding the 44 patients with cirrhosis at the time of HBsAg seroclearance, one of 290 patients with spontaneous HBsAg seroclearance and one of 88 Nuc-treated patients with HBsAg seroclearance developed HCC during a mean follow-up period of 117.5 and 79 months, respectively. The estimated annual incidence of HCC was 0.035% and 0.17%, respectively (P = 0.292). The corresponding figures were corrected as 0.036% and 0.22% with SIR. PS-matching method produced 62 patients each in spontaneous and Nuc-treated HBsAg seroclearance groups. There was one patient with Nuc-treated HBsAg seroclearance but none with spontaneous HBsAg seroclearance developed HCC during a mean follow-up period of 80.8 and 80.9 months, respectively. There was no significant difference in the estimated annual incidence of HCC (0% vs. 0.24%, P = 0.606) between patients with spontaneous and Nuc-treated HBsAg seroclearance. None in both groups had the occurrence of death or hepatic complication.
Anti-HBs seroconversion after HBsAg seroclearance

The rate of anti-HBs seroconversion was 69.6% and 66.4% in spontaneous and Nuc-treated groups, respectively (P = 0.617) (Table 1). Among the PS-matched patients, the anti-HBs seroconversion was comparable (60.2% vs. 65.3%, P = 0.555) between two groups (Table 2). The 6-year cumulative incidence of anti-HBs seroconversion was 62.3% and 61.1% in spontaneous and Nuc-treated groups, respectively (P = 0.431) (Figure 1). The incidence reached plateau after 7-year follow-up.
image

Figure 1. The comparison of cumulative incidence of anti-HBs seroconversion between patients with spontaneous and Nuc-treated HBsAg seroclearance in propensity score-matched cohort. There is no significant difference in anti-HBs seroconversion between two groups (62.3% vs. 61.1%, P = 0.431). Nuc, nucleos(t)ide analogue.
Discussion

The interaction among HBV, hepatocytes and host immunity results in the distinct phases of the natural course in CHB infection.[1] HBsAg seroclearance usually represents sustained immune control of HBV and is the ultimate goal of antiviral therapy.[10, 28, 29] The results of the present study have shown that HBsAg seroclearance in Nuc-treated patients occurred at a significantly younger age (47.4 vs. 51.5 years), more frequently in those with cirrhosis but the clinical outcomes were similar as compared with spontaneous HBsAg seroclearance. Of note is that spontaneous HBsAg seroclearance usually occurs in patients more than 10 years after they have entered inactive phase.[2] In contrast, Nuc therapy is initiated in patients with active hepatitis at an age and the status of HBV infection not favouring spontaneous HBsAg seroclearance. This may imply that, despite HBsAg seroclearance rate is <1% per year, Nuc therapy may accelerate immune control and HBsAg seroclearance.

Both spontaneous and Nuc-treated HBsAg seroclearance in CHB patients indicate excellent clinical outcomes in previous studies.[3-8, 15, 17] As far as our knowledge, this is the first study with long-term follow-up period (mean >6 years) to explore whether there is difference in the clinical outcomes after HBsAg seroclearance between CHB patients with spontaneous and Nuc-treated HBsAg seroclearance. Previous studies have shown that old age (≥50 years) or cirrhosis at the time of HBsAg seroclearance, male gender and concurrent HCV or HDV infection are risk factors for HCC development after HBsAg seroclearance.[3, 7, 8] A total of five patients developed HCC at a mean follow-up period of 75.3 months after HBsAg seroclearance in the present study. All were male, three had pre-existing cirrhosis and all were older than 55 years at the time of HCC detection. As the direct effect of integration of HBV DNA into hepatocyte chromosomes is a possible aetiology of HCC development in CHB infection,[30] HCC can occur in the absence of cirrhosis after HBsAg seroclearance[7, 9] as observed in two patients in the present study. However, no histological evidence was available to confirm that these two patients had not developed cirrhosis prior to HBsAg seroclearance. Of the 110 Nuc-treated patients with HBsAg seroclearance, HCC developed in one (0.9%) patient with an estimated annual incidence of 0.14%. It is lower than 0.35% in a recent Korean study.[15] Younger age at the time of HBsAg seroclearance (mean 47.4 years) and predominant genotype B HBV infection in the present Taiwanese study might explain this discrepancy. The estimated annual incidence of HCC at 0.13% in patients with spontaneous HBsAg seroclearance in the present study is similar to the findings of previous studies.[3-9] Among each PS-matched cohort of 98 patients, the estimated annual incidence of HCC development was similar between spontaneous and Nuc-treated groups (P = 0.735) during a mean follow-up period of 76–97 months. The present study also showed comparable rates of death and variceal bleeding between two groups.

Since sustained remission of hepatitis during follow-up is significantly correlated with HBsAg seroclearance in the natural course[22] and that active necroinflammation and moderate to advanced histological fibrosis in liver are indications of antiviral therapy for CHB patients,[10, 28, 29] the patients with Nuc-treated HBsAg seroclearance were observed to have significantly higher proportion of cirrhosis than those with spontaneous HBsAg seroclearance in both overall population and PS-matched cohorts of the present study. Although there was no statistically significant difference, the estimated annual incidence of HCC was higher in Nuc-treated patients than those with spontaneous HBsAg seroclearance in overall population (0.17% vs. 0.035%) and in PS-matched cohort (0.24% vs. 0%) among the patients without cirrhosis at the time of HBsAg seroclearance. The patients with Nuc-treated HBsAg seroclearance might have higher possibility to develop HCC after longer time follow-up because of the pre-existing fibrosis before and during Nuc treatment.

The 6-year cumulative incidence of anti-HBs seroconversion in 110 Nuc-treated patients was 68.3%, which is similar to a rate of 68.9% in a recent Hong Kong study.[17] Among the PS-matched patients, there was no significant difference in the 6-year cumulative incidence of anti-HBs seroconversion between spontaneous and Nuc-treated groups (P = 0.431) (Figure 1).

Surveillance for HCC is cost-effective if the expected annual incidence exceeds 1.5% in cirrhotic patients, irrespective of its aetiology and 0.2% in patients with CHB infection.[26, 31] The recommended screening interval is 6 months and a shorter follow-up period (every 3–4 months) is suggested for cirrhotic patients in current guidelines.[26, 31] However, there is no consensus of the follow-up interval for those with HBsAg seroclearance.[3, 8, 9] Since cirrhosis, coinfection of HCV or HDV, male gender and old age (≥50 years) have been reported as independent risk factors of HCC development after HBsAg seroclearance,[3, 7, 8] periodic surveillance according to established clinical guidelines[26, 31] for detection of early HCC with ultrasound and AFP in subjects who cleared HBsAg with the above clinical characteristics is necessary. Considering cost-effectiveness, it seems reasonable to increase the interval of follow-up to 12 months after HBsAg seroclearance for subjects without the above risk factors.[3] Given that the clinical outcomes were comparable between spontaneous and Nuc-treated HBsAg seroclearance, perhaps similar surveillance policy is applicable to Nuc-treated patients with HBsAg seroclearance.

There are limitations in the present study. First, the number of patients in this retrospective study may not be large enough for the comparison in the clinical outcomes after HBsAg seroclearance between spontaneous and Nuc-treated patients. The small number of observed clinical events after HBsAg seroclearance, which was similar to the findings of previous studies,[3-9] also made the statistical power not strong enough to make a definite conclusion. Nevertheless, the mean follow-up duration of more than 6 years is long enough to observe the potential development of hepatic complications, even though much longer follow-up may be needed for assessing HCC development in the patients with Nuc-treated HBsAg seroclearance. Second, the discrepancy in age distribution and number size between patients with spontaneous and Nuc-treated HBsAg seroclearance may lead to bias in annual incidence and statistical comparison of clinical outcomes. The results have been corrected by SIR method and are consistent. Third, genotype was not assayed in the majority of patients in the present study due to unavailable stored serum or low/undetectable HBV DNA. However, the finding of predominant genotype B in our study population (71%) was comparable to the geographic distribution in Taiwan.[32] The genotype of the five patients with HCC development in the present study showed similar distribution (3 genotype B, 1 genotype C and 1 undetermined). Perhaps genotype is no more a factor for HCC development once patients lost HBsAg. Further longer follow-up studies may be needed to test the impact of HBV genotype on HCC development after HBsAg seroclearance.

In conclusion, the clinical outcomes between patients with spontaneous and Nuc-treated HBsAg seroclearance were similar. Higher rate of cirrhosis in Nuc-treated patients at the time of HBsAg seroclearance might reflect previously persistent hepatic necroinflammatory process. HCC can develop in a low rate during long-term follow-up after both spontaneous and Nuc-treated HBsAg seroclearance. HCC surveillance after HBsAg seroclearance using liver ultrasound and AFP is still mandatory.

StephenW

肝癌的发展和肝脏并发症的HBsAg血清清除后

312例乙肝表面抗原自发转阴，四级男性患者在随访过程中发生HCC。一名49岁的非肝硬化，C基因型患者的HBsAg血清清除后61.5个月开发肝癌。剩余的三个病人分别为52，53和63岁及患有肝硬化的证据在HBsAg的血清清除（2基因型B和1未确定）的时间和HCC分别发生110.2，117.2和31个月，HBsAg的血清清除之后。 110国统会治疗的患者用HBsAg血清学清除的，一个59岁的非肝硬化，B型男性患者的HBsAg血清清除后56.7个月开发肝癌。肝癌发展的预计年发病率为0.13％，在自发和国统会处理组，分别为（P = 0.906），0.14％。肝癌发展的估计年发病率与SIR纠正和相应的数字分别为0.13％和0.16％。在国统会处理组，1例肺炎死于败血症，并与原有的肝硬化另一个病人经历食管静脉曲张随访期间出血。患者在自发性组无死亡或肝后续并发症。其中PS-匹配的患者中，有在HCC发展（2％和1.1％），总死亡率无显著差异（0％对1％）和静脉曲张出血发作（0％和4.2％）（P = 1.000 ）（表2）。肝癌的估计年发病率是自发和国统会处理组（0.31％和0.16％，P = 0.735）之间的可比性。

在乙肝表面抗原血清学清除的290例自发性的HBsAg血清学清除之一的88国统会治疗的患者的HBsAg血清学清除之一的时间不包括44例肝硬化后，在117.5和79个月，平均随访时间开发的HCC分别。肝癌的估计每年发生率分别为0.035％和0.17％（P = 0.292）。相应的数字分别为纠正0.036％和SIR 0.22％。 PS-匹配方法生产的每62例自发性和国统会处理的HBsAg血清学清除组。有一个病人与国统会处理的HBsAg血清学清除，但分别在80.8 80.9个月，平均随访时间开发的肝癌，乙肝表面抗原自发转阴没有。有肝癌的预计年发病患者自发的和国统会处理的HBsAg血清学清除之间没有显著差异（0％和0.24％，P = 0.606）。没有在这两个组具有死亡或肝并发症的发生。
乙肝表面抗原血清学清除后抗-HBs阳转

抗HBs血清转化率为69.6％，在自发和NUC-治疗组，分别为（P = 0.617）（表1）66.4％。间对PS-匹配患者中，抗HBs血清转换为具有可比性（60.2％对65.3％，P = 0.555）两组（表2）之间。抗HBs血清转换的6年累积发生率是62.3％，并在自发和NUC-治疗组，分别为（P = 0.431）（图1）61.1％。发病后达到7年的随访高原。
图片

图1.患者的倾向评分匹配队列自发的和国统会处理的HBsAg血清学清除的抗-HBs阳转的累计发生率的比较。有两组（62.3％对61.1％，P = 0.431）间的抗-HBs阳转无显著差异。国统会，核苷（酸）类似物IDE。
讨论

在慢性乙型肝炎感染的自然过程的不同阶段的HBV，肝细胞和宿主免疫结果之间的相互作用。[1]的HBsAg血清清除通常代表HBV的持续免疫控制，是抗病毒治疗的最终目标。[10，28，29]本研究的结果表明，在NUC-治疗的患者的HBsAg血清清除发生在一个显著低龄（47.4对比51.5年），更经常地在那些与肝硬化，但临床结果与自发的HBsAg血清清除相比相似。值得注意的是，自发的HBsAg血清学清除通常发生在患者10年以上，他们已经进入了非激活阶段之后。[2]相比之下，国统会治疗的患者活动性肝炎上了年纪发起和HBV感染的状况不利于自发的HBsAg血清学清除。这可能意味着，尽管HBsAg的血清清除率<每年1％，国统疗法可能会加速免疫控制与HBsAg血清清除。

是自发性的，慢性乙型肝炎患者NUC-治疗乙肝表面抗原血清学清除表示在以往的研究极好的临床疗效。[3-8，15，17]至于我们所知，这是首次研究长期随访期间（平均> 6年），探讨是否有CHB患者自发和国统会处理的HBsAg血清学清除乙肝表面抗原之间转阴后临床结果的差异。以往的研究表明，高龄（≥50岁），或在肝硬化的HBsAg血清学清除，男性和并发HCV或HDV感染的时间是乙肝表面抗原血清学清除后，HCC发展的危险因素。[3，7，8]的共有五患者发展为肝癌在本研究中的HBsAg血清清除后75.3个月，平均随访时间。全部为男性，三过预先存在的肝硬化和肝癌在检测时所有年龄超过55岁。作为HBV-DNA整合入肝细胞染色体的直接效果是肝癌发展的慢性乙型肝炎感染的可能的病因，[30]的HCC可以发生在HBsAg的血清清除后没有肝硬化[7,9]作为两个患者中观察到，在本研究。然而，没有组织学证据是来确认这两个病人尚未制定之前，乙肝表面抗原血清学清除肝硬化。 110 NUC-治疗的患者用HBsAg血清清除的，肝癌在一个（0.9％）的患者开发了的0.14％，预计每年的发病率。这是在最近的韩国研究低于0.35％。[15]在乙肝表面抗原血清学清除时年龄较轻（平均47.4年）和主要的B基因型HBV感染在目前台湾的研究或许可以解释这种差异。在患者在本研究中乙肝表面抗原自发转阴0.13％HCC的估计年发病率是类似于以前的研究结果。[3-9]在98例各PS-匹配队列，肝癌发展的预计年发病率是期间76-97个月，平均随访时间自发的和国统会处理组（P = 0.735）相似。本研究还表明死亡和静脉曲张的可比费率两组出血。

由于在随访期间肝炎的持续缓解与乙肝表面抗原血清学清除的自然病程[22]和活跃的坏死性炎症显著相关性和适中的先进组织纤维化肝是慢性乙肝患者抗病毒治疗的适应症，[10，28，29]观察用NUC-处理的HBsAg血清清除患者具有肝硬化的比那些在这两个总人口和本研究的PS-匹配队列自发的HBsAg血清清除显著比例较高。虽然没有统计学差异显著，肝癌的预计年发病率在国统会治疗的患者比那些在总人口（0.17％和0.035％），乙肝表面抗原自发转阴和PS-匹配队列（0.24％和0较高％）中患者无肝硬化的HBsAg在转阴的时间。与国统会处理的HBsAg血清学清除患者可能有更高的可能性后，较长时间的随访，因为现有的预纤维化之前和国统会在治疗过程中发生HCC。

在110 NUC-治疗的患者抗HBs血清转换的6年累积发生率是68.3％，这是类似的68.9％在最近香港研究的速率。[17]在对PS-匹配的患者，也没有在自发和国统会处理组（P = 0.431）（图1）之间的抗-HBs阳转的6年累积发病率显著差异。

如果预期年发病超过1.5％的肝硬化患者，不论其病因和CHB患者感染0.2％的监视肝癌是划算的。[26，31]建议筛选的时间间隔为6个月，更短的后续期间（每3-4个月），建议对肝硬化患者在当前的指南[26，31]但是，对于那些有乙肝表面抗原血清学清除无后续区间的共识。[3，8，9]由于肝硬化， HCV或HDV，男性和老年（≥50岁）的合并感染已经被报告为乙肝表面抗原血清学清除后，HCC发展的独立危险因素，[3，7，8，根据既定的临床指南定期监督[26，31]检测早期肝癌超声和AFP的科目谁与上述临床特征清除乙肝表面抗原是必要的。考虑到成本效益，它似乎是合理的增加随访至12个月的HBsAg血清清除后受试者的时间间隔没有上述危险因素。[3]鉴于临床结果是自发和国统会处理的HBsAg血清学清除具有可比性，或许类似的监视策略适用于国统会治疗的患者用HBsAg血清学清除。

有在本研究的限制。首先，患者在本回顾性研究的数量可能不够大，自发的和国统会治疗的患者的HBsAg之间转阴后，在临床结果的比较。少数乙肝表面抗原血清学清除后观察临床事件，这是类似于以前的研究结果，[3-9]也做了统计力量没有强大到足以使一个明确的结论。尽管如此，6年以上，平均随访时间足够长，以观察肝脏并发症的发展潜力，尽管大量长期随访，可能需要在患者的NUC-治疗乙肝表面抗原血清学清除评估HCC的发展。第二，在患者自发和NUC-处理的HBsAg血清清除之间年龄分布和数量大小的差异可能导致每年发病和临床结果的统计比较偏向。结果已经由SIR方法来校正和是一致的。三，基因型不占多数的患者在本研究中，由于无法储存血清或低/检测不到HBV DNA检测。然而，主要基因型B在我们的研究人群（71％）的发现相媲美了台湾的地理分布。[32]五例在本研究中肝癌发展的基因表现出相似的分布（3基因型B，1 C基因型和1未确定）。也许基因型是没有更多的肝癌发展的一个因素，一旦患者的HBsAg失去。进一步较长，可能需要后续的研究来检验HBV基因型的对肝癌发展的HBsAg血清清除后的影响。

总之，患者自发的和国统会处理的HBsAg血清学清除的临床结果相似。在乙肝表面抗原血清学清除的时间NUC-治疗的患者肝硬化率较高可能反映了此前持续性肝坏死性炎症过程。肝癌可以是自发性的，国统会处理的HBsAg血清清除后长期随访过程中低速率发展。采用肝脏超声和AFP仍然是必须的HBsAg血清清除后，HCC监测。

StephenW

全文:
http://onlinelibrary.wiley.com/doi/10.1111/apt.13630/full

疯一点好

早都说了表面抗原清除了也没多大用处。

四十己过

自发转阴的，也要坚持三到六个月AFP和B超检查！尤其是过了40岁。

zgct

好！