15/10/02说明:此前论坛服务器频繁出错,现已更换服务器。今后论坛继续数据库备份,不备份上传附件。

肝胆相照论坛

 

 

肝胆相照论坛 论坛 学术讨论& HBV English AASLD2019[87]新型EYP001的体外表征 和选择性FXR激动剂 ...
查看: 464|回复: 1
go

AASLD2019[87]新型EYP001的体外表征 和选择性FXR激动剂进入第二阶 [复制链接]

Rank: 8Rank: 8

现金
62111 元 
精华
26 
帖子
30437 
注册时间
2009-10-5 
最后登录
2022-12-28 

才高八斗

1
发表于 2019-10-23 15:27 |只看该作者 |倒序浏览 |打印
IN VITRO CHARACTERIZATION OF EYP001 A NOVEL, POTENT
AND SELECTIVE FXR AGONIST ENTERING PHASE 2 CLINICAL
TRIALS IN CHRONIC HEPATITIS B
Raphaël Darteil1, Stéphane Joly1, Pauline Radreau1, Marine
Porcherot1, Jacky Vonderscher1, Pietro Scalfaro1, Eric
Meldrum1 and Patrice Andre2, (1)Enyo Pharma SA, (2)
Inserm U1111 - Cnrs UMR5308 - Université Lyon 1 and Ecole
Normale Supérieure De Lyon, Ciri
Background: More than 240 million individuals worldwide
are chronically infected with hepatitis B virus (HBV), one
of the main causes of liver-related morbidity and mortality
Nucleos(t)ide-analogue (NUCs) therapy achieves potent
viral suppression and reduces the incidence of liver-related
complications However, cure rates are low and most patients
require life-long medication There is therefore a need for new
therapeutic approaches for chronic hepatitis B (CHB) One
novel approach for CHB targets the farnesoid X bile acid
receptor (FXR). It is known that HBV infection modifies bile
acid metabolism to impact the FXR pathway FXR agonists
have been reported to inhibit HBV cccDNA transcription
in primary human hepatocytes (PHH) EYP001 is a novel
and selective non-bile acid second generation FXR agonist
currently being evaluated in clinical Phase 2 against CHB
and NASH Methods: EYP001, other FXR agonists in clinical
development, and NUCs were tested in in vitro models
supporting the complete HBV replication cycle: differentiated
HepaRG cells and/or PHH. A broad range of HBV markers
were measured, including viral antigens and nucleic acids
Results: EYP001 repressed significantly all HBV markers
in a dose-dependent manner in HepaRG cells: secreted
HBsAg (60% inhibition), HBeAg (60% inhibition) and rcDNA
(79% inhibition), and intracellular pg/pcRNA (75% inhibition)
and cccDNA (71% inhibition) A comparison of EYP001 with
other FXR agonists currently in clinical development was
carried out All FXR agonists tested do not share the same
antiviral potency and maximal efficacy. Extensive combination
experiments with EYP001 and NUCs were also carried out in
infected HepaRG cells Unlike EYP001, NUCs alone showed
negligible effects on HBsAg, HBeAg and cccDNA levels
and combining with the EYP001 FXR agonist resulted in a
profile superior to NUCs alone. All compound concentrations
presented in this work were shown not to be cytotoxic
Conclusion: The non-bile acid specific FXR agonist EYP001
was shown to repress the replication of HBV in 2 in vitro
hepatic models of full viral cycle Other FXR agonists in clinical
development have similar effects but do not share the same
antiviral potency and maximal efficacy. The mode of action
of FXR agonists against HBV is currently under investigation
with evidence showing a reliance on FXR for the recruitment of
HBx and other cellular factors to the trans-activating complex
on the cccDNA (Lacombe et al EASL ILC 2019, SAT-175)
The effects of EYP001 on both cccDNA transcription and
HBsAg secretion, along with additive effects observed in
combination treatments with NUCs make of EYP001 a good
clinical candidate to achieve CHB functional cure in humans

Rank: 8Rank: 8

现金
62111 元 
精华
26 
帖子
30437 
注册时间
2009-10-5 
最后登录
2022-12-28 

才高八斗

2
发表于 2019-10-23 15:27 |只看该作者
新型EYP001的体外表征
和选择性FXR激动剂进入第二阶段临床
慢性乙型肝炎的试验
RaphaëlDarteil1,StéphaneJoly1,Pauline Radreau1,海军陆战队
Porcherot1,Jacky Vonderscher1,Pietro Scalfaro1,Eric
Meldrum1和Patrice Andre2,(1)Enyo Pharma SA,(2)
Inserm U1111-Cnrs UMR5308-里昂1大学和巴黎高中
西里师范大学里昂师范大学
背景:全球超过2.4亿人
长期感染了乙型肝炎病毒(HBV)
肝相关发病率和死亡率的主要原因
核苷类似物(NUCs)治疗取得了有效
病毒抑制并降低肝脏相关的发生率
并发症然而,治愈率很低,大多数患者
需要终身服药因此需要新的
慢性乙型肝炎(CHB)的治疗方法之一
CHB的新方法靶向法呢素X胆汁酸
受体(FXR)。已知HBV感染会改变胆汁
酸代谢影响FXR途径FXR激动剂
据报道可抑制HBV cccDNA转录
EYP001在人类原代肝细胞(PHH)中的作用
和选择性非胆汁酸第二代FXR激动剂
目前正在临床第二阶段针对CHB进行评估
和NASH方法:EYP001,临床上其他的FXR激动剂
发育,并且在体外模型中测试了NUC
支持完整的HBV复制周期:差异化
HepaRG细胞和/或PHH。广泛的HBV标记
进行了检测,包括病毒抗原和核酸
结果:EYP001显着抑制所有HBV标记
在HepaRG细胞中呈剂量依赖性:分泌
HBsAg(抑制60%),HBeAg(抑制60%)和rcDNA
(79%抑制)和细胞内pg / pcRNA(75%抑制)
和cccDNA(抑制率达71%)EYP001与
目前临床开发中的其他FXR激动剂是
进行的所有测试的FXR激动剂都不相同
抗病毒效力和最大功效。广泛的组合
EYP001和NUC的实验也在
感染的HepaRG细胞与EYP001不同,仅NUCs可显示
对HBsAg,HBeAg和cccDNA水平的影响可忽略不计
并与EYP001 FXR激动剂结合使用
优于单独的NUC。所有化合物浓度
在这项工作中提出的被证明没有细胞毒性
结论:非胆汁酸特异性FXR激动剂EYP001
被证明在体外抑制了HBV的复制2
全病毒周期的肝模型临床上其他FXR激动剂
发展有相似的效果,但并不相同
抗病毒效力和最大功效。行动方式
目前正在研究针对HBV的FXR激动剂
有证据表明在招聘FXR时依赖FXR
HBx和其他细胞因子参与反式激活复合物
在cccDNA上的表达(Lacombe et al EASL ILC 2019,SAT-175)
EYP001对cccDNA转录和转录的影响。
HBsAg分泌,以及在
NUC联合治疗使EYP001很好
在人类中实现CHB功能治愈的临床候选者
‹ 上一主题|下一主题
你需要登录后才可以回帖 登录 | 注册

肝胆相照论坛

GMT+8, 2024-11-20 20:39 , Processed in 0.013430 second(s), 11 queries , Gzip On.

Powered by Discuz! X1.5

© 2001-2010 Comsenz Inc.