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肝胆相照论坛 论坛 学术讨论& HBV English AASLD2018[409]以Cccdna为目标的新型候选药物 HBV ...
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AASLD2018[409]以Cccdna为目标的新型候选药物 HBV [复制链接]

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发表于 2018-10-17 18:53 |只看该作者 |倒序浏览 |打印
409
Novel Candidate Drugs That Target Cccdna of
HBV
Yoshiki Murakami1, Michiyo Hayakawa1, Saori Itami-
Matsumoto1, Mari Ando1, Yutaka Yata1,2, Masaru Enomoto1,
Akihiro Tamori1, Norifumi Kawada1, Takashi Honda3,
Yoshihiko Yano4, Mitsuo Iwadate5 and Hideaki Umeyama5,
(1)Department of Hepatology, Osaka City University, (2)
Department of Gastroenterology, Hanwa Sumiyoshi General
Hospital, (3)Department of Gastroenterology and Hepatology,
Nagoya University School of Medicine, (4)Department
of Gastroenterology, Kobe University, (5)Department of
Biological Science, Chuo University
Background: Antiviral drugs that treat chronic hepatitis
B with nucleos(t)ide analogues are considered effective.
Although the frequency of emerging escape mutant viruses
has decreased, most drugs of this class frequently result
in viral relapse after cessation of therapy. Persistent viral
infections require the presence of the viral genome in
the infected cell in a stable form that is not lost during cell
division. For hepadnaviruses, the viral genome persists in the
nucleus as covalently closed circle (ccc) DNA. Sp1, a group
of transcription factors that bind specifically to DNA, regulates
the expression of the Hepatitis B virus X (HBx) gene. The
HBx protein affects the epigenetic function of nuclear HBV
cccDNA via several nuclear transcription factors. Moreover
cyclin D2 regulated HBV replication by enhancing the activity
of HBV core and Sp1 promoters. To develop more efficient
drugs to treat chronic hepatitis B, it is necessary to focus on
the viral replication process, excluding reverse-transcription.
We aimed to identify low molecular compounds that suppress
the transcription of cccDNA. Methods: Fifteen chemical
compounds for Sp1 inhibitors were chosen from a library
of chemical compounds (AKos GmbH, Steinen, Germany)
using in silico screening. PXB cells (Phoenix bio, Hiroshima,
Japan) with HBV infection were cultured. The medium was
changed every five days and one chemical compound was
added each time the medium was changed. The quantities
of HBVDNA in the medium and cccDNA in the nucleus were
measured using real-time PCR. The human albumin content
in the medium was detected using the Human albumin
ELISA quantitation kit (Bethyl, Montgomery, AL, USA).
Results: Four of the 15 compounds were able to suppress
viral replication without cytotoxicity. The level of HBVDNA
treated with candidate No.15 (1-[3-(4-tert-butylcyclohexyl)
oxy-2-hydroxypropyl]-2,2,6,6-tetramethylpiperidin-4-ol) is
the same as that of entecavir (ETV). Anti-HBV effect of this
chemical compound is dose-depending manner and the IC
50 is 66 nM. Moreover, candidate No.15 was able to reduce
significantly the expression level of ccc DNA, as compared
to ETV (p<0.05). Conclusion: In this study, we developed
novel anti-viral candidates that decreased viral replication
by targeting cccDNA. Identifying candidate for controlling
nuclear transcription factor facilitates development of novel
medicines that combine novel anti-viral drugs and nucleos(t)
ide analogues for HBV treatment

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发表于 2018-10-17 18:54 |只看该作者
409
以Cccdna为目标的新型候选药物
HBV
Yoshiki Murakami1,Michiyo Hayakawa1,Saori Itami-
Matsumoto1,Mari Ando1,Yutaka Yata1,2,Masaru Enomoto1,
Akihiro Tamori1,Norifumi Kawada1,Takashi Honda3,
Yoshihiko Yano4,Mitsuo Iwadate5和Hideaki Umeyama5,
(1)大阪市立大学肝病学系,(2)
Hanwa Sumiyoshi General消化系
医院,(3)胃肠病学和肝病学系,
名古屋大学医学部,(4)系
神户大学消化内科,(5)
中央大学生物科学
背景:治疗慢性肝炎的抗病毒药物
具有核苷(t)ide类似物的B被认为是有效的。
虽然出现逃逸突变病毒的频率
已经减少,这类药物的大多数药物经常出现
在停止治疗后病毒复发。持久的病毒
感染需要病毒基因组的存在
受感染的细胞以稳定的形式存在,在细胞内不会丢失
师。对于嗜肝DNA病毒,病毒基因组持续存在
核作为共价闭合圆(ccc)DNA。 Sp1,一群人
调节特异性结合DNA的转录因子
乙型肝炎病毒X(HBx)基因的表达。该
HBx蛋白影响核HBV的表观遗传功能
cccDNA通过几种核转录因子。此外
细胞周期蛋白D2通过增强活性来调节HBV复制
HBV核心和Sp1启动子。发展更有效率
治疗慢性乙型肝炎的药物,有必要重点关注
病毒复制过程,不包括逆转录。
我们的目标是识别抑制的低分子化合物
cccDNA的转录。方法:十五化学
用于Sp1抑制剂的化合物选自文库
化学化合物(AKos GmbH,Steinen,Germany)
使用计算机筛选。 PXB细胞(凤凰生物,广岛,
日本人)用HBV感染培养。媒体是
每五天换一次,一种化合物就是
每次更换介质时都会添加。数量
HBVDNA在培养基和细胞核中的cccDNA中的表达均为
使用实时PCR测量。人体白蛋白含量
在培养基中使用人白蛋白检测
ELISA定量试剂盒(Bethyl,Montgomery,AL,USA)。
结果:15种化合物中有4种能够抑制
病毒复制无细胞毒性。 HBVDNA的水平
候选者No.15(1- [3-(4-叔丁基环己基))处理
氧基-2-羟丙基] -2,2,6,6-四甲基哌啶-4-醇)
与恩替卡韦(ETV)相同。这对抗HBV的影响
化学化合物是剂量依赖的方式和IC
50是66nM。而且,候选人No.15能够减少
与之相比,ccc DNA的表达水平显着
到ETV(p <0.05)。结论:在这项研究中,我们开发了
减少病毒复制的新型抗病毒候选物
通过靶向cccDNA。确定控制候选人
核转录因子促进了小说的发展
结合新型抗病毒药物和核苷的药物(t)
用于HBV治疗的ide类似物

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发表于 2018-10-17 19:28 |只看该作者
本帖最后由 newchinabok 于 2018-10-17 19:30 编辑
StephenW 发表于 2018-10-17 18哟西:54
409哟西
以Cccdna为目标的新型候选药物
HBV

哟西,哟西,新药的有,大大的干活

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发表于 2018-10-17 21:01 |只看该作者
感谢分享。

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发表于 2018-10-17 22:28 |只看该作者
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