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替诺福韦疫苗组合可消除母婴 HBV 传播 [复制链接]

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发表于 2022-11-8 16:55 |只看该作者 |倒序浏览 |打印
替诺福韦疫苗组合可消除母婴 HBV 传播
— 即使不使用乙型肝炎免疫球蛋白也有 100% 的成功率

作者:Zaina Hamza,MedPage Today 特约撰稿人 2022 年 11 月 7 日
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在中国进行的一项随机试验发现,早期母体富马酸替诺福韦酯(TDF)联合婴儿疫苗接种完全消除了高病毒血症母亲慢性乙型肝炎病毒(HBV)的垂直传播,即使不使用乙型肝炎免疫球蛋白(HBIg)也是如此。

产后 28 周时,母婴传播率相同,均为 0%,从孕 14-16 周开始的早期母体 TDF 治疗(随后是婴儿 HBV 疫苗接种)与从孕 28 周开始的母体 TDF 治疗(随后是婴儿)纽约大学朗格尼健康中心的 Calvin Pan 医学博士报告说。

分娩时,早期 TDF 组母亲的 HBV-DNA 水平显着降低(2.37 vs 3.62 log10 IU/mL,P<0.001),HBV-DNA 低于 200,000 IU/mL 的比例更高(99% vs 94% , P = 0.04)。

根据在美国肝病协会赞助的年度肝脏会议上公布的研究结果,婴儿的先天性缺陷发生率没有显着差异,早期组为 3.1%,晚期组为 6.4%(P=0.22)。肝病研究。

潘说,结合婴儿疫苗接种,研究小组的研究结果表明,在胎龄第 16 周开始 TDF“可以有效地防止传播,这与目前的护理标准相当,没有安全信号。”

俄亥俄州克利夫兰诊所的医学博士 William Carey 告诉 MedPage Today,目前的研究利用 HBIg 供应有限这一事实设计了一种新的更简单的策略——完全省略 HBIg。

没有参与这项研究的凯里说:“可以采取任何措施来简化保护 [a] 婴儿的过程将受到欢迎。”

纽约布法罗大学的医学博士、公共卫生硕士 Andrew Talal 向 MedPage Today 表示,进一步的研究“应该调查这种方法,以确定这些发现对其他人群的普遍性”。

“重要的是要认识到这是一个非常小的样本量,不足以确定不经常发生的潜在危害,”凯里解释说。 “如果得到证实,两步走的策略很可能会成为惯例。”

慢性 HBV 是一种全球公共卫生威胁,影响近 2.96 亿人。对于 HBV DNA 水平大于 200,000 IU/mL 的母亲,世界卫生组织 (WHO) 建议母亲使用 TDF 联合婴儿 HBV 疫苗接种和 HBIg。

鉴于许多发展中国家缺乏 HBIg,研究人员评估了早期母体 TDF 和婴儿疫苗接种,但没有 HBIg,是否同样可以防止母婴 HBV 传播。之前在柬埔寨测试类似策略的一项研究也显示垂直传播率为 0%。

从 2018 年 6 月到 2021 年 2 月,研究人员招募了 265 名患有慢性 HBV(且 HBV DNA 水平高于 200,000 IU/mL)的母亲,她们生下了 269 名婴儿。 TDF 的给药剂量为每天 300 毫克。所有婴儿都接受了主动免疫预防。

母婴传播定义为 HBV 表面抗原 (HBsAg) 阳性或 HBV-DNA 水平高于 20 IU/mL。改良意向治疗分析和符合方案分析的主要结果结果相同,敏感性分析显示早期 TDF 组的母婴传播率为 2%,这表明与当前标准的有效性相当关心。

研究中的母亲平均年龄约为 28 岁,她们的平均体重指数为 22。

Pan 说,TDF 治疗耐受性良好,没有患者因严重不良事件 (AE) 而停药。他解释说,两组安全参数的频率和严重程度相当,例如严重的 AE、治疗期间的肾小球滤过率和产后丙氨酸氨基转移酶 (ALT) 发作。

研究限制包括短期随访和缺乏安慰剂。潘说,早期组中有四名婴儿接受了 HBIg。

    作者['full_name']

    Zaina Hamza 是今日 MedPage 的特约撰稿人,报道胃肠病学和传染病。她常驻芝加哥。

披露

该研究得到了约翰 C. 马丁基金会的支持。 Pan 披露了与 Assembly Bio、Gilead 和 NYU Langone Health 的关系。

主要资源

美国肝病研究协会

来源参考:Pan C 等人“替诺福韦-DF 疗法可防止婴儿没有 HBV 免疫球蛋白的高病毒血症母亲的乙型肝炎垂直传播”AASLD 2022;

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发表于 2022-11-8 16:55 |只看该作者
Tenofovir, Vaccine Combo Eliminates Mom-to-Child HBV Transmission
— 100% success rate even without the use of hepatitis B immunoglobulin

by Zaina Hamza, Staff Writer, MedPage Today November 7, 2022
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This article is a collaboration between MedPage Today and:

Earlier maternal tenofovir disoproxil fumarate (TDF) combined with infant vaccination completely eliminated vertical transmission of chronic hepatitis B virus (HBV) from highly viremic mothers, even without the use of hepatitis B immunoglobulin (HBIg), a randomized trial conducted in China found.

At 28 weeks postpartum, mother-to-child transmission was an identical 0% with early maternal TDF therapy starting at 14-16 weeks gestational age (followed by infant HBV vaccination) versus maternal TDF therapy starting at 28 weeks gestational age (followed by infant vaccination plus HBIg), reported Calvin Pan, MD, of the NYU Langone Health in New York City.

At delivery, mothers in the early TDF group had significantly lower HBV-DNA levels (2.37 vs 3.62 log10 IU/mL, P<0.001), and a higher proportion had HBV-DNA levels below 200,000 IU/mL (99% vs 94%, P=0.04).

There was no significant difference seen in the rates of congenital defects among infants, at 3.1% in the early group and 6.4% in the late group (P=0.22), according to findings presented at the annual Liver Meeting sponsored by the American Association for the Study of Liver Diseases.

In combination with infant vaccination, Pan said the findings in the investigational arm showed that initiating TDF at week 16 of gestational age "could effectively prevent transmission, which is comparable to the current standard of care, with no safety signals."

William Carey, MD, of the Cleveland Clinic in Ohio, told MedPage Today that the current study took advantage of the fact that HBIg is in limited supply to design a new and simpler strategy -- omitting HBIg altogether.

"Anything that can be done to simplify the process of protecting [a] baby would be welcome," said Carey, who was not involved in the study.

Reached for comment, Andrew Talal, MD, MPH, of the University at Buffalo in New York, told MedPage Today that further studies "should investigate this approach to determine the generalizability of these findings to other populations."

"It is important to recognize that this is a very small sample size, inadequate to determine potential harms that occur infrequently," Carey explained. "If confirmed, it is likely that the two-step strategy will become common practice."

Chronic HBV is a global public health threat that affects nearly 296 million individuals. For mothers who have HBV DNA levels greater than 200,000 IU/mL, the World Health Organization (WHO) recommends maternal use of TDF combined with infant HBV vaccination and HBIg.

Given the scarcity of HBIg in many developing countries, the researchers evaluated if earlier maternal TDF and infant vaccination, but without HBIg, could similarly protect against mother-to-child HBV transmission. A prior study in Cambodia testing a similar strategy also showed a 0% vertical transmission rate.

From June 2018 to February 2021, researchers enrolled 265 mothers with chronic HBV (and HBV DNA levels above 200,000 IU/mL) who gave birth to 269 infants. TDF was given at a dose of 300 mg daily. All infants were given active immunoprophylaxis.

Mother-to-child transmission was defined by being positive for HBV surface antigen (HBsAg) or having HBV-DNA levels above 20 IU/mL. Primary outcome results were the same in both modified intention-to-treat and per-protocol analyses, and a sensitivity analysis showed a 2% mother-to-child transmission rate among the early TDF group, indicating a comparable effectiveness to the current standard of care.

Mothers in the study had a mean age of approximately 28, and their average body mass index was 22.

TDF therapy was well tolerated, said Pan, while no patients discontinued because of severe adverse events (AEs). Both groups showed comparable frequency and severity of safety parameters, such as severe AEs, glomerular filtration rates during treatment, and postpartum alanine aminotransferase (ALT) flares, he explained.

Study limitations included a short follow-up and lack of placebo. Four infants in the early group received HBIg, said Pan.

    author['full_name']

    Zaina Hamza is a staff writer for MedPage Today, covering Gastroenterology and Infectious disease. She is based in Chicago.

Disclosures

The study was supported by the John C. Martin Foundation. Pan disclosed relationships with Assembly Bio, Gilead, and NYU Langone Health.

Primary Source

American Association for the Study of Liver Diseases

Source Reference: Pan C, et al "Tenofovir-DF therapy prevents hepatitis B vertical transmission in highly viremic mothers without HBV immunoglobulin for infants" AASLD 2022;

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