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标题: Toll样受体7激动剂GS-9620通过I型干扰素依赖性机制诱导对HBV的 [打印本页]

作者: StephenW    时间: 2018-4-8 10:16     标题: Toll样受体7激动剂GS-9620通过I型干扰素依赖性机制诱导对HBV的

Toll-like receptor 7 agonist GS-9620 induces prolonged inhibition of HBV via a type I interferon-dependent mechanismAuthor links open overlay panelCongrongNiu1LiLi1StephaneDaffis1JulieLucifora2MarcBonnin2SarahMaadadi2EduardoSalas1RuthChu1HilarioRamos1Christine M.Livingston1Rudolf K.Beran1Abhishek V.Garg1ScottBalsitis1DavidDurantel2FabienZoulim234William E.DelaneyIV1Simon P.Fletcher1



https://doi.org/10.1016/j.jhep.2017.12.007Get rights and content
Referred to byBertram Bengsch, Robert Thimme
For whom the interferons toll – TLR7 mediated boosting of innate and adaptive immunity against chronic HBV infectionJournal of Hepatology, Volume 68, Issue 5, May 2018, Pages 883-886
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Highlights•

GS-9620 has no direct antiviral activity against HBV.

Type I IFN induced by GS-9620 durably suppresses HBV without reducing cccDNA levels.

GS-9620-induced cytokines enhance HBV antigen presentation.

Established HBV infection does not modulate innate immune sensing or signaling.



Background & Aims

GS-9620, an oral agonist of toll-like receptor 7 (TLR7), is in clinical development for the treatment of chronic hepatitis B (CHB). GS-9620 was previously shown to induce prolonged suppression of serum viral DNA and antigens in the woodchuck and chimpanzee models of CHB. Herein, we investigated the molecular mechanisms that contribute to the antiviral response to GS-9620 using in vitro models of hepatitis B virus (HBV) infection.


Methods

Cryopreserved primary human hepatocytes (PHH) and differentiated HepaRG (dHepaRG) cells were infected with HBV and treated with GS-9620, conditioned media from human peripheral blood mononuclear cells treated with GS-9620 (GS-9620 conditioned media [GS-9620-CM]), or other innate immune stimuli. The antiviral and transcriptional response to these agents was determined.


Results

GS-9620 had no antiviral activity in HBV-infected PHH, consistent with low level TLR7 mRNA expression in human hepatocytes. In contrast, GS-9620-CM induced prolonged reduction of HBV DNA, RNA, and antigen levels in PHH and dHepaRG cells via a type I interferon (IFN)-dependent mechanism. GS-9620-CM did not reduce covalently closed circular DNA (cccDNA) levels in either cell type. Transcriptional profiling demonstrated that GS-9620-CM strongly induced various HBV restriction factors – although not APOBEC3A or the Smc5/6 complex – and indicated that established HBV infection does not modulate innate immune sensing or signaling in cryopreserved PHH. GS-9620-CM also induced expression of immunoproteasome subunits and enhanced presentation of an immunodominant viral peptide in HBV-infected PHH.


Conclusions

Type I IFN induced by GS-9620 durably suppressed HBV in human hepatocytes without reducing cccDNA levels. Moreover, HBV antigen presentation was enhanced, suggesting additional components of the TLR7-induced immune response played a role in the antiviral response to GS-9620 in animal models of CHB.


Lay summary

GS-9620 is a drug currently being tested in clinical trials for the treatment of chronic hepatitis B virus (HBV) infection. GS-9620 has previously been shown to suppress HBV in various animal models, but the underlying antiviral mechanisms were not completely understood. In this study, we determined that GS-9620 does not directly activate antiviral pathways in human liver cells, but can induce prolonged suppression of HBV via induction of an antiviral cytokine called interferon. However, interferon did not destroy the HBV genome, suggesting that other parts of the immune response (e.g. activation of immune cells that kill infected cells) also play an important role in the antiviral response to GS-9620.



Graphical abstract







作者: StephenW    时间: 2018-4-8 10:16

Toll样受体7激动剂GS-9620通过I型干扰素依赖性机制诱导对HBV的延长的抑制
作者链接打开覆盖面板群荣Niu1LiLi1StephaneDaffis1JulieLucifora2MarcBonnin2SarahMaadadi2EduardoSalas1RuthChu1HilarioRamos1Christine M.Livingston1Rudolf K.Beran1Abhishek V.Garg1ScottBalsitis1DavidDurantel2FabienZoulim234William E.DelaneyIV1Simon P.Fletcher1
https://doi.org/10.1016/j.jhep.2017.12.007
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Bertram Bengsch,罗伯特·蒂姆
干扰素使用者收费 - TLR7介导的先天免疫和适应性免疫对慢性HBV感染的促进作用
Journal of Hepatology,第68卷,第5期,2018年5月,第883-886页
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强调



    GS-9620对HBV没有直接的抗病毒活性。


    由GS-9620诱导的I型IFN在不降低cccDNA水平的情况下持久地抑制HBV。


    GS-9620诱导的细胞因子增强HBV抗原呈递。


    已建立的HBV感染不会调节先天免疫感应或信号。

背景和目的

GS-9620是一种Toll样受体7(TLR7)的口服激动剂,正在临床开发用于治疗慢性乙型肝炎(CHB)。先前显示GS-9620在CHB的土拨鼠和黑猩猩模型中诱导血清病毒DNA和抗原的长时间抑制。在此,我们使用乙型肝炎病毒(HBV)感染的体外模型研究了有助于GS-9620的抗病毒应答的分子机制。
方法

用HBV感染冷冻保存的原代人肝细胞(PHH)和分化的HepaRG(dHepaRG)细胞,并用来自用GS-9620处理的人外周血单核细胞的条件培养基GS-9620(GS-9620条件培养基[GS-9620-CM ])或其他先天性免疫刺激。确定了这些药物的抗病毒和转录反应。
结果

GS-9620在HBV感染的PHH中没有抗病毒活性,与人肝细胞中低水平的TLR7 mRNA表达一致。相反,GS-9620-CM通过I型干扰素(IFN)依赖性机制诱导PHH和dHepaRG细胞中HBV DNA,RNA和抗原水平的持续降低。 GS-9620-CM不降低任何细胞类型中的共价闭合环状DNA(cccDNA)水平。转录谱分析表明,GS-9620-CM强烈诱导多种HBV限制因子 - 尽管不是APOBEC3A或Smc5 / 6复合物 - 并且表明建立的HBV感染不调节冷冻保存的PHH中的先天免疫感应或信号传导。 GS-9620-CM还诱导免疫蛋白酶体亚基的表达和增强HBV感染PHH中免疫显性病毒肽的呈递。
结论

由GS-9620诱导的I型IFN在人肝细胞中持续抑制HBV而不降低cccDNA水平。此外,HBV抗原呈递增强,表明TLR7诱导的免疫应答的另外组分在CHB动物模型中对GS-9620的抗病毒应答中发挥作用。
总结

GS-9620是目前正在临床试验中用于治疗慢性乙型肝炎病毒(HBV)感染的药物。先前已经证明GS-9620在各种动物模型中抑制HBV,但是潜在的抗病毒机制尚未完全了解。在这项研究中,我们确定GS-9620不直接激活人肝细胞的抗病毒途径,但可通过诱导称为干扰素的抗病毒细胞因子诱导HBV长期抑制。然而,干扰素不破坏HBV基因组,表明免疫应答的其他部分(例如激活免疫细胞杀死感染的细胞)在GS-9620的抗病毒应答中也起重要作用。
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