难以治疗的自身免疫性肝炎和原发性胆汁性胆管炎:药物治疗新时代的曙光。

IF 14 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Clinical and Molecular Hepatology Pub Date : 2024-11-11 DOI:10.3350/cmh.2024.0821
Atsumasa Komori, Yuki Kugiyama
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引用次数: 0

摘要

难以治疗的自身免疫性肝炎(AIH)或原发性胆汁性胆管炎(PBC)患者被事后定义为对药物治疗反应不充分或不耐受的患者,因此无法达到与长期无肝脏相关事件生存相关的生化替代终点。最近没有统一的 "6 个月内完全生化应答(CBR≤6M)"定义,即在开始治疗后≤6 个月内血清转氨酶和 IgG 水平正常化,低于正常上限(ULN),这被视为难以治疗的 AIH。CBR≤6M 的实施反过来又促进了临床试验,例如硫唑嘌呤和霉酚酸酯之间的试验,以重新考虑适当的一线类固醇疏导药物,从而减少了难以治疗的 AIH 病例数量。关于 PBC,对难治患者的一个广泛定义是不符合 POISE 标准,即在使用熊去氧胆酸后的 12 个月内通过血清碱性磷酸酶和胆红素水平进行评估。不符合 POISE 标准的难治性 PBC 患者最近已成为美国 FDA 批准的二线药物依来氟和塞拉得巴的目标人群。在未来的 AIH 和 PBC 药物治疗中,AIH 的主要目标可能是通过个性化的类固醇减量治疗方案减少难以治疗的患者人数。PBC 治疗的一个挑战性目标是进一步优化治疗代用终点,甚至是更严格的 ALP 正常化,这样可能会扩大二线或三线药物的适应症,但最终可能会延长患者的长期生存期。
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Hard-to-treat autoimmune hepatitis and primary biliary cholangitis: The dawn of a new era of pharmacological treatment.

Patients with hard-to-treat autoimmune hepatitis (AIH) or primary biliary cholangitis (PBC) are defined a posteriori as those who do not show a sufficient response or are intolerant to pharmacological treatments, thus not achieving biochemical surrogate endpoints that are associated with long-term liver-related-event-free survival. The absence of a recently harmonized definition of 'complete biochemical response within 6 months (CBR≤6M)', which is defined as the normalization of serum transaminase and IgG levels below the upper limit of normal (ULN) at ≤6 months after treatment initiation is regarded as hard-to-treat AIH. The implementation of CBR≤6M, in turn, has been facilitating clinical trials, e.g., between azathioprine and mycophenolate mofetil, to reconsider appropriate first-line steroid sparing agents, leading to a reduction in the number of hard-to-treat AIH cases. Regarding PBC, one of the disseminated definitions of hard-to-treat patients is the absence of POISE criteria, which are evaluated at 12 months with serum alkaline phosphatase and bilirubin levels, after the introduction of ursodeoxycholic acid. Hard-to-treat PBC not meeting the POISE criteria has very recently been the target population for the U.S. FDA-approved second-line drugs, elafibranor and seladelpar. In future pharmacological treatment of AIH and PBC, the primary objective for AIH is likely to focus on lowering the number of hard-to-treat patients with personalized steroid sparing treatment regimens. A challenging goal in PBC treatment is the further optimization of treatment surrogate endpoints, even to the stricter ALP normalization, with which an indication of second- or later-line drugs might be expanded, but could ultimately lengthen patients' long-term survival.

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来源期刊
Clinical and Molecular Hepatology
Clinical and Molecular Hepatology Medicine-Hepatology
CiteScore
15.60
自引率
9.00%
发文量
89
审稿时长
10 weeks
期刊介绍: Clinical and Molecular Hepatology is an internationally recognized, peer-reviewed, open-access journal published quarterly in English. Its mission is to disseminate cutting-edge knowledge, trends, and insights into hepatobiliary diseases, fostering an inclusive academic platform for robust debate and discussion among clinical practitioners, translational researchers, and basic scientists. With a multidisciplinary approach, the journal strives to enhance public health, particularly in the resource-limited Asia-Pacific region, which faces significant challenges such as high prevalence of B viral infection and hepatocellular carcinoma. Furthermore, Clinical and Molecular Hepatology prioritizes epidemiological studies of hepatobiliary diseases across diverse regions including East Asia, North Asia, Southeast Asia, Central Asia, South Asia, Southwest Asia, Pacific, Africa, Central Europe, Eastern Europe, Central America, and South America. The journal publishes a wide range of content, including original research papers, meta-analyses, letters to the editor, case reports, reviews, guidelines, editorials, and liver images and pathology, encompassing all facets of hepatology.
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