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停止HBeAg阴性慢性乙型肝炎核苷(酸)类似物治疗后乙型肝炎 [复制链接]

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发表于 2018-9-13 20:06 |只看该作者 |倒序浏览 |打印
Hepatitis B virus-specific T cell responses after stopping nucleos(t)ide analogue therapy in HBeAg-negative chronic hepatitis B [url=]Franziska Rinker[/url]†
,  [url=]Christine L. Zimmer[/url]†
,  [url=]Christoph Höner zu Siederdissen[/url]
,  [url=]Michael P. Manns[/url]
,  [url=]Anke R.M. Kraft[/url]
,  [url=]Heiner Wedemeyer[/url]
,  [url=]Niklas K. Björkström[/url]†
,  [url=]Markus Cornberg[/url]†,[url=]Correspondence information about the author  Markus Cornberg[/url]Email the author  Markus Cornberg

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DOI: https://doi.org/10.1016/j.jhep.2018.05.004 |

Article Info






Highlights
  • •Discontinuation of NA therapy leads to higher HBsAg loss rates in HBeAg-negative CHB patients.
  • •T cells from patients with subsequent HBsAg loss show a less exhausted phenotype.
  • •These T cells also express higher levels of activation and proliferation markers at week 12 after discontinuation of therapy.
  • •Relapse of active HBV replication may trigger immunological environment that enhances responsiveness of HBV-specific T cells in vitro.

Background & AimsTreatment with nucleos(t)ide analogues (NA) leads to hepatitis B virus (HBV) DNA suppression in most patients with chronic hepatitis B (CHB), but HBV surface antigen (HBsAg) loss rates are low. Upon NA discontinuation, HBV DNA can return rapidly with ensuing alanine aminotransferase flares and induction of cytokines. Several studies reported higher HBsAg loss rates after stopping therapy, but at present it is unclear if cell-mediated immune responses are altered after treatment discontinuation. The aim of this study was to characterise T cell responses during the early phase of virological relapse, following discontinuation of NA therapy in HBeAg-negative patients.


MethodsA total of 15 HBeAg-negative patients with CHB on long-term NA treatment were included in a prospective study and subjected to structured NA discontinuation. T cell responses were studied at the end of NA therapy and 4, 8 and 12 weeks thereafter.


ResultsThe T cell phenotype of patients with CHB on long-term NA therapy was markedly different compared to healthy individuals, but was only slightly altered after discontinuation of therapy. T cells from patients with HBsAg loss expressed low levels of KLRG1 and PD-1 at all time-points and high levels of Ki-67 and CD38 at week 12 after treatment cessation. In vitro peptide stimulated HBV-specific T cell responses were increased in several patients after NA cessation. Blocking of PD-L1 further enhanced HBV-specific T cell responses, especially after discontinuation of therapy.


ConclusionRelapse of active HBV replication after stopping therapy may trigger an immunological environment that enhances the responsiveness of HBV-specific T cells in vitro. Together with other immune interventions, this approach might be of interest for the development of novel therapeutic options to induce HBsAg loss in CHB.


Lay summaryRelapse of hepatitis B virus replication after discontinuation of nucleos(t)ide analogue therapy in certain patients with chronic hepatitis B may alter the phenotype of T cells and enhance the responsiveness of hepatitis B virus-specific T cells to in vitro peptide stimulation. Blocking PD-L1 can further augment these hepatitis B virus-specific T cell responses. Interestingly, T cells of patients that subsequently achieve hepatitis B surface antigen loss are less exhausted at all time-points after stopping treatment and display a higher proliferative capacity 12-weeks after treatment discontinuation. These findings contribute to the understanding of the immunological events that occur during discontinuation of nucleos(t)ide analogue therapy.



Keywords:                [url=https://www.journal-of-hepatology.eu/action/doSearch?searchType=quick&occurrences=all<rlSrch=true&searchScope=series&searchText=Chronic hepatitis B&seriesISSN=0168-8278]Chronic hepatitis B[/url], [url=https://www.journal-of-hepatology.eu/action/doSearch?searchType=quick&occurrences=all<rlSrch=true&searchScope=series&searchText=Nucleos(t)ide analogue (NA)&seriesISSN=0168-8278]Nucleos(t)ide anal[/url]

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发表于 2018-9-13 20:06 |只看该作者
停止HBeAg阴性慢性乙型肝炎核苷(酸)类似物治疗后乙型肝炎病毒特异性T细胞反应
Franziska Rinker†
,Christine L. Zimmer†
,ChristophHönerzuSiederdissen
,Michael P. Manns
,Anke R.M.卡夫
,海纳韦德迈尔
,NiklasK.Björkström†
,Markus Cornberg†,'关于作者Markus Cornberg的通讯信息电子邮件作者Markus Cornberg
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DOI:https://doi.org/10.1016/j.jhep.2018.05.004 |
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强调

    •停用NA治疗会导致HBeAg阴性CHB患者的HBsAg丢失率升高。
    •患有后续HBsAg丢失的患者的T细胞表现出较少的表型。
    •这些T细胞在停止治疗后第12周也表达更高水平的激活和增殖标志物。
    •活跃的HBV复制的复发可能引发免疫环境,增强体外HBV特异性T细胞的反应性。

背景与目的

用核苷(酸)类似物(NA)治疗导致大多数慢性乙型肝炎(CHB)患者的乙型肝炎病毒(HBV)DNA抑制,但HBV表面抗原(HBsAg)丢失率低。在NA停止后,HBV DNA可迅速恢复,随后出现丙氨酸氨基转移酶突发和细胞因子的诱导。一些研究报道停止治疗后HBsAg的丢失率较高,但目前尚不清楚治疗中断后细胞介导的免疫反应是否会改变。本研究的目的是在HBeAg阴性患者中停止NA治疗后,在病毒学复发的早期阶段表征T细胞应答。
方法

在一项前瞻性研究中,共有15名HBeAg阴性的CHB长期NA治疗患者被纳入结构性NA停药。在NA治疗结束时和之后的4,8和12周研究T细胞应答。
结果

与健康个体相比,长期NA治疗的CHB患者的T细胞表型显着不同,但在停止治疗后仅略有改变。来自HBsAg丢失患者的T细胞在治疗停止后第12周时在所有时间点表达低水平的KLRG1和PD-1,并且表达高水平的Ki-67和CD38。在NA停止后,几名患者体外肽刺激的HBV特异性T细胞应答增加。阻断PD-L1进一步增强了HBV特异性T细胞应答,特别是在停止治疗后。
结论

停止治疗后复发的活性HBV复制可能引发免疫环境,从而增强体外HBV特异性T细胞的反应性。与其他免疫干预一起,这种方法可能对开发诱导CHB中HBsAg丢失的新型治疗选择感兴趣。
放置摘要

在某些慢性乙型肝炎患者中停用核苷(酸)类似物治疗后乙型肝炎病毒复制的复发可能改变T细胞的表型并增强乙型肝炎病毒特异性T细胞对体外肽刺激的反应性。阻断PD-L1可以进一步增强这些乙型肝炎病毒特异性T细胞应答。有趣的是,随后实现乙型肝炎表面抗原丢失的患者的T细胞在停止治疗后的所有时间点都较少疲劳,并且在治疗中断后12周显示出更高的增殖能力。这些发现有助于理解在核苷(酸)类似物治疗中断期间发生的免疫事件。
关键词:
慢性乙型肝炎,Nucleos(t)ide肛门

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发表于 2018-9-14 15:25 |只看该作者
结果
与健康个体相比,长期NA治疗的CHB患者的T细胞表型显着不同,但在停止治疗后仅略有改变。来自HBsAg丢失患者的T细胞在治疗停止后第12周时在所有时间点表达低水平的KLRG1和PD-1,并且表达高水平的Ki-67和CD38。在NA停止后,几名患者体外肽刺激的HBV特异性T细胞应答增加。阻断PD-L1进一步增强了HBV特异性T细胞应答,特别是在停止治疗后。

结论
停止治疗后复发的活性HBV复制可能引发免疫环境,从而增强体外HBV特异性T细胞的反应性。与其他免疫干预一起,这种方法可能对开发诱导CHB中HBsAg丢失的新型治疗选择感兴趣。

这个还需要要研究,哪些战友可以停药,停药过程中监控哪些指标。
如果有变化,应该怎么来监控,什么情况下可以继续停,什么情况下需要恢复用药。
这里面未知数据还是太多。

但是总体上说,有助于表抗下降
CHB战友交流: 234101235 每天吐槽HBV动态,不断同步TAF咨询
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