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乙肝治疗与妊娠 [复制链接]

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发表于 2011-11-21 20:23 |只看该作者 |倒序浏览 |打印
最新一期journal of hepatology 关于hbv与妊娠综述
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Good work for getting hold of the editorial.  发表于 2011-11-21 23:47
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发表于 2011-11-21 21:31 |只看该作者
最好直接发文字版上来

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发表于 2011-11-21 23:44 |只看该作者
[I have extracted some parts of the article. Please note, it is an Editorial, not a paper. Please consult your own doctors about treatment during pregnancy.][StephenW]

HBV treatment and pregnancy
Jörg Petersen
Liver Unit, IFI Institute for Interdisciplinary Medicine, Asklepios Klinik St. Georg Hamburg, Germany
Editorial
...........
Even though lamivudine is classified as FDA pregnancy risk category C, it is associated with the risk of birth defects that is not higher than the baseline birth defect rate. A meta-analysis of 10 randomized clinical trials (RCTs) examining 951 HBV carrier mothers
was reported to evaluate the efficacy of lamivudine in reducing in utero transmission of HBV [12]. The RCTs evaluated included newborns who received immunoprophylaxis at birth and women who were treated with lamivudine from 24 to 32 weeks of gestation, until delivery to 1 month post-delivery. Newborns in the lamivudine group had a 13–24% significantly lower incidence of intrauterine exposure and a lower perinatal infection rate at 9–
12 months. This report was limited by the quality of the studies included. On the other hand, in a recent poster presented at EASL 2011 in Berlin [13], Ayres et al. showed that although the therapy with lamivudine achieved an HBV DNA load reduction of
3 log10 IU/ml, in 20% of the pregnant women, the viral load remained high (>1  107 IU/ml) and resistant mutations were detectable only after three months of therapy, calling for more potent antiviral drugs to be used to prevent transmission.
Of the two agents classified as FDA pregnancy risk category B,only tenofovir received this classification based on the data collected in human exposure, so far. There have been no other published studies using entecavir, adefovir, or emtricitabine for preventing HBV vertical transmission, and these drugs should be switched immediately, if a woman becomes pregnant. The experience with tenofovir in pregnant women consists of 606 women in their first trimester and 336 in their second trimester from the APR. The rate of birth defects associated with tenofovir ranges from 1.5% (second-trimester use) to 2.3% (first-trimester
use), which is again similar to the background rate. Telbivudine received its pregnancy risk category B rating based on animal studies; there were few human pregnancy registry data up to now. In this issue of the Journal of Hepatology, Han et al. present a prospective study [14] that evaluates the efficacy of telbivudine for preventing HBV newborn infection performed in 230 pregnant HBsAg positive patients with HBV DNA levels of >1.0  106
copies/ml. The study shows that telbivudine plus vaccination is superior to HBIG and HBV vaccines only in newborns to prevent HBV transmission (0% vs. 8%). This study reconfirms data from a recent study of 31 pregnant women in China, treated with telbivudine
started at weeks 28–32 of pregnancy and continued to 30 days postpartum [15]. All babies received active and passive immunoprophylaxis. The infection rate was 0% in those treated
with telbivudine and 13.3% in the untreated controls. The advantages of the study by Han et al. are the use of telbivudine, a more potent antiviral drug than lamivudine with a
lower risk of HBV drug resistance and the inclusion of a largenumber of pregnant HBsAg positive women. The disadvantages are the short follow up, only seven months after delivery, and the lack of results of virologic breakthrough and resistance data. Furthermore, it is not a randomized study, patients were allocated depending on their own wishes and prophylaxis was started either during the second trimester or during the third trimester
but without a definitive time point. It is unclear whether mothers with high levels of viremia started earlier compared to those with low levels of viremia. The risk of HBV transmission
could have been analyzed even better in relation to the time of starting prophylaxis in addition to HBV DNA levels. The primary end point of the study was defined as undetectable HBsAg and HBV DNA at birth and at month 7. This is a short period of follow-
up to analyze HBV perinatal transmission, at least newborns should be followed for 1 year. Nevertheless, this study is adding very important information to our very limited knowledge of safety of polymerase inhibitors in pregnant women and helps to support the ‘‘B’’ rating of telbivudine
..........
In summary, treatment of HBV infection during pregnancy remains a challenge, the risks and benefits must be weighed carefully and there are still numerous gaps in our knowledge. The benefits of treatment appear to be most pronounced in cases with high maternal viremia to prevent transmission and in mothers with advanced fibrosis to prevent flares. Viable treatment choices are limited to lamivudine, tenofovir, and telbivudine. Of these,
lamivudine and tenofovir appear to be the therapeutic options with reasonable human exposure and safety data in pregnancy and we do see now an increasing number of data for the safety of telbivudine, too.
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发表于 2011-11-21 23:46 |只看该作者
文章中提取的某些部分。请注意,它是一个编辑,而不是论文。在怀孕期间治疗,请咨询您自己的医生。] [StephenW]

HBV治疗和怀孕
约尔格彼得森
肝单位,国际金融机构的跨学科医学研究所,Asklepios Klinik圣乔治,德国汉堡
编辑
...........
即使拉米夫定FDA怀孕的危险C类分类,它是与出生缺陷的风险比基线出生缺陷率不高。一项荟萃分析的10个随机临床试验(随机对照试验)检查951乙型肝炎病毒载体的母亲
据报道,在子宫内的乙肝病毒传播,减少评估拉米夫定的疗效[12]。包括新生儿谁在出生时免疫预防和拉米夫定治疗的妇女从24至32孕周直至分娩1个月后交付,随机对照试验评估。拉米夫定组新生儿宫内暴露了13-24%,显着降低发病率和围产期感染发生率较低的9 -
12个月。这份报告是由包括研究质量有限。另一方面,在最近的海报在欧洲肝病学会2011年在柏林[13],艾尔斯等。表明,尽管与拉米夫定治疗达到HBV DNA载量减少
3 log10的国际单位/毫升,20%的孕妇中,病毒载量仍然很高(> 1 × 107 IU / ml)的耐药性突变检测,仅3个月的治疗后,要求更有效的抗病毒药物,被用来防止传染。
FDA怀孕的风险B类分类的二级代理商,只替诺福韦收到这种分类的基础上收集到的数据,到目前为止,在人体暴露。有没有其他发表的研究报告,使用恩替卡韦,阿德福韦或恩曲他滨预防乙型肝炎病毒母婴垂直传播,而这些药物,应立即进行切换,如果一个女人怀孕。替诺福韦在孕妇的经验,包括606名妇女在他们的头三个月,在他们的APR孕中期336。泰诺福韦范围相关的出生缺陷率,从1.5%(孕中期使用)至2.3%(早孕
使用),这也是类似的背景率。替比夫定收到其怀孕的风险B类评级,基于动物的研究,有少数人怀孕到现在的注册表数据。这个问题,韩等肝病杂志。目前的一项前瞻性研究[14],替比夫定的疗效,为防止新生儿感染HBV在230孕妇乙肝表面抗原阳性患者HBV - DNA水平> 1.0进行评估? 106
拷贝/ ml。研究表明,替比夫定,加上疫苗接种只在新生儿HBIG和乙肝病毒的疫苗,以预防乙肝病毒传播的(0%和8%)优于。这项研究再次证实了最近的一项研究,从31日在中国孕妇的数据,替比夫定治疗
在怀孕28-32周开始,持续30天产后[15]。所有的婴儿收到的主动和被动免疫预防。治疗者,感染率为0%
替比夫定和13.3%未经处理的对照。韩等优势的研究。使用替比夫定比拉米夫定,一种更有效的的抗病毒药物与
风险较低的HBV耐药性和列入孕妇乙肝表面抗原阳性的妇女largenumber。缺点是简短的跟进后仅7个月,交付和缺乏病毒学突破和阻力数据的结果。此外,它不是一项随机研究中,患者被分配取决于自己的意愿和预防开始在孕中期或孕晚期期间
但没有一个明确的时间点。目前还不清楚是否与高水平的病毒血症的母亲血症水平低的人相比起步较早。乙肝病毒传播的风险
本来分析HBV DNA水平,除了预防开始时间甚至更好。这项研究的主要终点是定义为检测不到HBsAg和HBV DNA在出生7个月。这是一个短时期跟随
分析乙肝病毒母婴传播,新生儿至少应为1年。然而,这项研究是非常重要的信息添加我们非常有限的孕妇聚合酶抑制剂的安全知识和帮助,以支持“B”替比夫定的评级
..........
总之,乙肝病毒感染的治疗,在怀孕期间仍然是一个挑战,必须仔细衡量风险和收益,在我们的知识仍有许多空白。治疗的好处似乎是最案件宣判,以防止传输的高产妇血症和晚期肝纤维化,防止耀斑的母亲。拉米夫定,替诺福韦和替比夫定可行的治疗选择是有限的。其中,
拉米夫定和替诺福韦出现,与合理的人体暴露在怀孕期间的安全数据治疗方案,我们看到现在越来越多的替比夫定的安全数据,也。
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发表于 2011-11-22 10:22 |只看该作者
本人不是医生。
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