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失代偿期肝硬化患者再代偿的长期预后

谢志伟 李波 林丽花 谭颖 李剑萍 关玉娟 王亚萍

引用本文:
Citation:

失代偿期肝硬化患者再代偿的长期预后

DOI: 10.12449/JCH260602
基金项目: 

广东省医学科学技术研究基金 (A2024653);

广州市市校(院)企联合资助项目 (2025A03J3731);

广州市市校(院)企联合资助项目 (2024A03J0860);

广州医科大学科研能力提升计划重大临床研究项目 (GMUCR2024-02027)

利益冲突声明:本文不存在任何利益冲突。
作者贡献声明:谢志伟负责文章设计和撰写;李波、林丽花、谭颖负责查阅文献;李剑萍、关玉娟、王亚萍负责拟定文章思路,修改并最终定稿。
详细信息
    通信作者:

    王亚萍, xiruo0833@sina.com (ORCID: 0000-0002-0609-9115)

Long-term prognosis of recompensation in patients with decompensated liver cirrhosis

Research funding: 

Medical Science and Technology Research Fund of Guangdong Province (A2024653);

Guangzhou Municipal-University/Institutes-Enterprises Joint Funding Project (2025A03J3731);

Guangzhou Municipal-University/Institutes-Enterprises Joint Funding Project (2024A03J0860);

Major Clinical Research Project of the Scientific Research Capacity Enhancement Program of Guangzhou Medical University (GMUCR2024-02027)

More Information
    Corresponding author: WANG Yaping, xiruo0833@sina.com (ORCID: 0000-0002-0609-9115)
  • 摘要: 肝硬化再代偿指失代偿期肝硬化患者经病因治疗或对症治疗后,失代偿并发症消失,肝功能及临床表型恢复至代偿期状态的过程。近年来,随着肝硬化病因的有效控制和对失代偿并发症的治疗或预防,再代偿的临床意义日益受到关注。本文从再代偿的定义与诊断标准、影响因素、对长期预后的影响机制及临床管理策略几个方面展开综述,结合最新研究证据探讨其在改善患者生存质量、降低终末期事件风险中的核心价值,为优化肝硬化全程管理提供依据。

     

  • 图  1  肝硬化自然史

    Figure  1.  The natural history of liver cirrhosis

    表  1  不同国家及地区对失代偿期肝硬化再代偿的定义

    Table  1.   Definitions of liver cirrhosis recompensation across different countries and regions

    国家 年份 主要定义
    中国 2017年7 乙型肝炎、丙型肝炎相关肝硬化失代偿期患者给予及时抗病毒、抗炎保肝等治疗,患者肝功能明显改
    善,无腹水等并发症
    加拿大 2017年9 未针对并发症预防性治疗且不再出现腹水、肝性胸腔积液及周围组织水肿、肝性脑病、消化道出血等
    失代偿事件;MELD评分降至15分,且持续≥6个月
    中国 2019年10 肝硬化患者出现失代偿后,由于病因控制或治疗等原因,肝功能逐渐恢复并稳定,在较长时间内未再
    出现肝硬化失代偿事件
    欧洲 2021年11 需符合以下所有标准:(1)消除或控制肝脏疾病的主要病因,例如:严格戒酒或肝炎病毒的清除或抑
    制;(2)临床症状消失,如腹腔积液(不同时使用利尿剂)、肝性脑病(不使用预防性药物)、至少12个月
    无静脉曲张出血复发;(3)肝功能检查指标的稳定改善,如血清白蛋白、国际标准化比值和总胆红素
    水平
    中国 2022年12 在病因消除或控制的基础上,至少1年内未再出现腹水、肝性脑病、食管胃静脉曲张出血等严重并发症
    (停用药物治疗),伴稳定的肝功能改善,具体标准为:MELD评分<10分和/或Child-Pugh分级A级(白
    蛋白>35 g/L、国际标准化比值<1.5、总胆红素<34 μmol/L)
    韩国 2022年13 Child-Pugh分级B、C级的乙型肝炎患者,首次失代偿事件后开始抗病毒治疗,治疗后肝功能改善至
    Child-Pugh评分5分

    注:MELD,终末期肝病模型;Child-Pugh分级,蔡尔德-皮尤分级。

    下载: 导出CSV

    表  2  不同病因失代偿期肝硬化的再代偿发生率

    Table  2.   Recompensation incidence rates in decompensated liver cirrhosis with different etiologies

    类型 随访时间(年) 再代偿发生率(%)
    乙型肝炎815 1 53
    2.5 56.2
    5 53
    丙型肝炎16-18 1.4 24.7
    5 29.03
    8.4 36.6
    酒精性肝病19-20 2 18.1
    3 31.1
    自身免疫性肝病21-22 3.5 16.7
    4.2 15.3
    下载: 导出CSV
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