全球消除乙型肝炎的前景

StephenW

全球消除乙型肝炎的前景
Timothy M Block 1 , Kyong-Mi Chang 2 , Ju-Tao Guo 1
隶属关系
隶属关系

    1
    Baruch S. Blumberg Institute，Doylestown，宾夕法尼亚州 18902，美国；电子邮件：[email protected]。
    2
    下士 Michael J. Crescenz VA 医学中心和宾夕法尼亚大学佩雷​​尔曼医学院，宾夕法尼亚州费城 19104，美国。

    PMID：34586871 DOI：10.1146/annurev-virology-091919-062728

抽象的

慢性乙型肝炎病毒 (HBV) 感染是肝硬化和肝细胞癌的主要原因，估计每年在全球造成约 800,000 人死亡。尽管可以使用有效的疫苗来预防新的 HBV 感染，但对现有慢性乙型肝炎 (CHB) 的治疗是有限的，因为目前的标准抗病毒药物只能抑制病毒复制而无法治愈。 2016 年，世界卫生组织呼吁到 2030 年消除病毒性肝炎这一全球公共卫生威胁。美国和其他国家正在努力通过制定治愈 CHB 和预防 HBV 传播的战略来实现这一宏伟目标。本综述回顾了近期在了解 HBV 病理生物学和开发治疗 CHB 的疗法方面的研究进展，这对于到 2030 年消除乙型肝炎是必要的。

关键词：慢性乙型肝炎；直接作用的抗病毒药物；功能性治愈；乙型肝炎病毒;免疫疗法。

StephenW

Prospects for the Global Elimination of Hepatitis B
Timothy M Block  1 , Kyong-Mi Chang  2 , Ju-Tao Guo  1
Affiliations
Affiliations

    1
    Baruch S. Blumberg Institute, Doylestown, Pennsylvania 18902, USA; email: [email protected].
    2
    The Corporal Michael J. Crescenz VA Medical Center and University of Pennsylvania Perelman School of Medicine, Philadelphia, Pennsylvania 19104, USA.

    PMID: 34586871 DOI: 10.1146/annurev-virology-091919-062728

Abstract

Chronic hepatitis B virus (HBV) infection is the leading cause of liver cirrhosis and hepatocellular carcinoma, estimated to be globally responsible for ∼800,000 deaths annually. Although effective vaccines are available to prevent new HBV infection, treatment of existing chronic hepatitis B (CHB) is limited, as the current standard-of-care antiviral drugs can only suppress viral replication without achieving cure. In 2016, the World Health Organization called for the elimination of viral hepatitis as a global public health threat by 2030. The United States and other nations are working to meet this ambitious goal by developing strategies to cure CHB, as well as prevent HBV transmission. This review considers recent research progress in understanding HBV pathobiology and development of therapeutics for the cure of CHB, which is necessary for elimination of hepatitis B by 2030.

Keywords: chronic hepatitis B; direct-acting antivirals; functional cure; hepatitis B virus; immunotherapy.

StephenW

https://www.annualreviews.org/do ... ology-091919-062728

StephenW

七、结论
尽管取得了令人瞩目的进展，但消除病毒性肝炎的中期目标
世卫组织为 2020 年设定的目标尚未实现。因此，2030 年的消除目标现在将更多
难以实现，甚至不太可能。低诊断率，有限的疫苗接种覆盖率，
在许多发展中国家，目前批准的治疗方法的可及性有限
世界阻碍了减轻疾病负担的努力。除此之外，还有 2019 年冠状病毒病
大流行，这使临床试验停滞并使肝炎外展计划受挫 (148)。
对于预防，目前可用的疫苗是非常有效和改进的策略
将需要针对特定​​国家的交付。对于 elim-
影响 250 至 3 亿 CHB 患者，新药将
需要。 CHB 研究药物数量和多样性的增加提供了基础
的乐观。例如，2010 年，有 3 个临床前和 11 个临床阶段药物在
发展，都主要来自相同的机械类别。到 2020 年，如
乙型肝炎基金会（http://www.hepb.org），正在开发的药物数量有所增长
主要有 17 个临床前和 32 个临床阶段药物，这些药物来自不同的
机制。这种多样性很重要，因为很可能联合治疗
将需要方法。具体来说，抑制病毒的药物以及恢复病毒的药物
可能需要有益的免疫反应。
重要的是，由于感染 HBV 的肝细胞百分比在
那些患有 CHB 的人，存在安全问题，即 HBV 特异性 T 细胞的功能恢复
或阻断免疫调节通路可能导致大规模肝细胞损伤
临床肝功能失代偿。在这方面，治疗过程中必须考虑
对患者潜在肝功能储备、负担的发展和治疗
病毒以及HBV感染肝细胞的比例，以及cy-
安全治愈 CHB 所需的病理性和非细胞病变机制。在似乎很可能
直接作用抑制HBV蛋白表达并减少感染细胞数
抗病毒药物将成为免疫激活疗法的重要组合成分。那里-
因此，尽管雄心勃勃的世卫组织计划面临固有挑战，但消除路线图
HBV 现在存在，如果遵循，最终应减少，如果不能消除，公共卫生
HBV 及其相关疾病的问题。
披露声明
T.M.B.和 J.-T.G.从 Arbutus Biopharma, Inc. 获得研究支持并持有其股票。
K.-M.C.担任 Arbutus Biopharma, Inc 科学顾问委员会成员

StephenW

7. CONCLUSION
Although impressive progress has been made, the intermediate viral hepatitis elimination goals
set by WHO for 2020 have not been achieved. Thus, the 2030 elimination goals will now be more
difficult to achieve, perhaps even unlikely. The low diagnostic rate, limited vaccination coverage,
and limited accessibility of currently approved therapeutics in many developing countries in the
world hamper efforts to reduce the disease burden. Added to this is the coronavirus disease 2019
pandemic, which has stalled clinical trials and frustrated hepatitis outreach programs (148).
For prevention, the currently available vaccines are highly effective and improved strategies
for their delivery that are nation specific will be needed. For the therapeutic component of elim-
ination, which affects between 250 and 300 million people with CHB, new medicines will be
needed. The uptick in the number and diversity of investigational drugs for CHB provides a basis
of optimism. In 2010, for example, there were 3 preclinical- and 11 clinical-stage drugs in de-
velopment, all being largely from the same mechanistic categories. By 2020, as indicated by the
Hepatitis B Foundation (http://www.hepb.org), the number of drugs in development had grown
substantially with 17 preclinical- and 32 clinical-stage drugs, and these drugs are from diverse
mechanisms. This diversity is important because it is quite likely that a combination therapeutic
approach will be needed. Specifically, drugs that suppress the virus as well as those that restore a
beneficial immunological response are likely to be needed.
Importantly, because the percentage of hepatocytes infected with HBV can be quite high in
those with CHB, there are safety concerns that functional restoration of HBV-specific T cells
or blockage of immune regulatory pathways could lead to massive hepatocellular damage with
clinical liver decompensation. In this regard, considerations must be given during therapeutic de-
velopment and treatment to the underlying hepatic functional reserve of the patient, the burden
of the virus as well as the proportion of HBV-infected hepatocytes, and the balance between cy-
topathic and noncytopathic mechanisms that is needed to cure CHB safely. In seems likely that
suppression of HBV protein expression and decrease of infected cell number with direct-acting
antivirals will be an important combination component of immune activation therapies. There-
fore, despite the challenges inherent to the ambitious WHO plans, a road map toward elimination
of HBV now exists and if followed should eventually reduce, if not eliminate, the public health
problem of HBV and the diseases with which it is associated.
DISCLOSURE STATEMENT
T.M.B. and J.-T.G. receive research support from and hold stock in Arbutus Biopharma, Inc.
K.-M.C. serves as a member of the scientific advisory board of Arbutus Biopharma, Inc

lancas

看上去不是好消息~~

StephenW

回复 lancas 的帖子

是的，短期内似乎无治愈 法.