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 乙肝衣壳抑制剂在早期研究中看起来很有前途 ...
查看: 2690|回复: 15
go

乙肝衣壳抑制剂在早期研究中看起来很有前途 [复制链接]

Rank: 10Rank: 10Rank: 10

现金
20661 元 
精华
帖子
12793 
注册时间
2013-12-29 
最后登录
2024-11-3 
1
发表于 2018-7-30 21:59 |只看该作者 |倒序浏览 |打印
本帖最后由 newchinabok 于 2018-7-30 21:59 编辑

http://www.infohep.org/Hepatitis ... udies/page/3257815/
已有 1 人评分现金 收起 理由
hfdr + 1

总评分: 现金 + 1   查看全部评分

Rank: 10Rank: 10Rank: 10

现金
20661 元 
精华
帖子
12793 
注册时间
2013-12-29 
最后登录
2024-11-3 
2
发表于 2018-7-30 22:00 |只看该作者
Hepatitis B capsid inhibitors look promising in early studies
Liz Highleyman
Published:18 April 2018Tweet

Edward Gane at The International Liver Congress, 2018. Photo by Liz Highleyman.
JUMP TO
RO7049389
JNJ-379
Two experimental drugs that interfere with assembly of the hepatitis B virus (HBV) capsid and prevent production of functional new virus demonstrated good safety and promising antiviral activity in early clinical trials, according to reports presented at the 2018 International Liver Congress last week in Paris.
Nucleoside/nucleotide antivirals such as tenofovir DF (Viread), tenofovir alafenamide (Vemlidy) and entecavir (Baraclude) can suppress HBV replication indefinitely during long-term therapy, but they seldom lead to a cure, typically defined as hepatitis B surface antigen (HBsAg) clearance.
Capsid inhibitors are among several novel agents being explored as finite treatments, potentially for use in combination therapy.
Glossary
natural killer cells
Cells in the immune system which attack and destroy infected cells or tumour cells.
MORE FROM THE GLOSSARY
RO7049389, being developed by Roche, is a core protein allosteric modulator. It causes production of defective HBV core proteins that lead to assembly of a defective nucleocapsid, the shell that encloses viral genetic material. JNJ-379, being developed by Janssen, is a capsid inhibitor with a dual mode of action. It appears to interfere with both disassembly of the capsid when the virus enters a cell – necessary to release viral DNA – and assembly of capsids for newly produced HBV particles.
RO7049389
Edward Gane of Auckland Clinical Studies in New Zealand presented findings from a phase 1 study evaluating the safety, tolerability, pharmacokinetics and anti-HBV activity of RO7049389.
Part 1 of the study, which enrolled 65 healthy volunteers without HBV, looked at the safety and pharmacokinetics of single ascending oral doses ranging from 150mg to 2000mg, with and without food, and multiple ascending doses ranging from 200mg to 600mg twice daily for 14 days. All were men, about 70% were white, 16% were Asian and the median age was approximately 25 years.
The second part, enrolling people with chronic HBV infection, is assessing the drug's antiviral activity at multiple doses. Gane reported findings from the first cohort of six patients treated with 200mg RO7049389 twice daily for 28 days plus one placebo recipient. Five were men, six were Asian, one was white and the median age was 40 years; three were hepatitis B 'e' antigen (HBeAg) positive, which is more difficult to treat. They were not currently on HBV treatment, did not have liver cirrhosis or high ALT elevation and had a viral loads of least 2000 IU/ml if HBeAg negative or 20,000 IU/ml if HBeAg positive.
RO7049389 had a favourable pharmacokinetic profile, with a half-life of 5.5 hours. Treatment was well tolerated by both healthy volunteers and people with HBV. Only three people had adverse events that were considered drug-related (nausea, abdominal upset, skin rash and headache) and all were mild. There were no clinically meaningful changes in laboratory results.
All participants with hepatitis B who took RO7049389 for four weeks experienced "rapid and profound" viral load suppression, Gane reported. The median HBV DNA decline was -2.7 log10 and the maximum decline was -3.4 log10. The three HBeAg-negative people, who started with lower viral levels, became undetectable; viral load was still declining in the HBeAg-positive participants.
Gane did not report changes in HBsAg or HBeAg levels, but preclinical studies showed that higher doses of RO7049389 reduced HBsAg and HBeAg in mice.
"These preliminary data support the further development of RO7049389 as a potential component of a novel combination HBV cure regimen," the researchers concluded.
Gane said that other cohorts in this ongoing study will evaluate higher doses and a once-daily dosing schedule.
In a related presentation, Lu Gao and colleagues of the Roche Innovation Centre in Basel reported findings from a mouse study testing RO7049389 in combination with the toll-like receptor 7 (TLR7) agonist RO7020531, a drug that activates T cells, B cells and natural killer cells.
The combination produced sustained HBV DNA suppression that lasted for six weeks after the drug was stopped in four of the seven treated mice. It also led to HBsAg loss in five mice and some developed anti-HBs antibodies.
JNJ-379
Fabien Zoulim of INSERM Cancer Research Institute in Lyon, France, and colleagues evaluated the safety, pharmacokinetics and antiviral activity of multiple ascending doses of JNJ-56136379 (JNJ-379 for short) in people with chronic hepatitis B.
This ongoing phase 1b trial study enrolled 36 people with previously untreated chronic hepatitis B and had HBV DNA levels above 2000 IU/ml. Most (83%) were men, three-quarters were white and the median age was approximately 43 years. A quarter were HBeAg positive and a majority had HBV genotype D. Most had absent or mild liver fibrosis; people with cirrhosis and highly elevated ALT were excluded.
Participants were randomly assigned to receive JNJ-379 at once-daily doses of 25mg (starting with a 100mg loading dose), 75mg or 150mg, or a placebo, for 28 days; a 250mg cohort is still underway.
After 28 days of treatment, HBV DNA declined by -2.16, -2.89 and -2.70 log10 in the 25mg, 150mg and 75mg dose groups, respectively. HBV RNA levels fell by -2.3, -1.85 and -1.67 log10,. There were no relevant changes in HBsAg levels, which Zoulim said was to be expected for such a short treatment period.
Again, treatment was safe and well tolerated. Only one person in the highest dose group experienced a severe adverse event and stopped treatment for this reason.
A phase 2a study of both previously untreated and virally suppressed people with chronic hepatitis B is underway to further evaluate JNJ-379 alone and in combination with nucleoside/nucleotide analogues.
References
Gane E et al. RO7049389, a core protein allosteric modulator, demonstrates robust anti-HBV activity in chronic hepatitis B patients and is safe and well tolerated. The International Liver Congress, Paris, abstract LBO-003, 2018. Journal of Hepatology 68:S101, 2018.
Dai L et al. Combination treatment of a TLR7 agonist RO7020531 and a core protein allosteric modulator RO7049389 achieved sustainable viral load suppression and HBsAg loss in an AAV-HBV mouse model. The International Liver Congress, Paris, abstract PS-028, 2018. Journal of Hepatology 68:S17, 2018.
Zoulim F et al. Safety, pharmakokinetics and antiviral activity of novel capsid assembly modulator (CAM) JNJ-56136379 (JNJ-6379) in treatment- naive chronic hepatitis B (CHB) patients without cirrhosis
. The International Liver Congress, Paris, abstract LBO-004, 2018. Journal of Hepatology 68:S102, 2018

Rank: 7Rank: 7Rank: 7

现金
6395 元 
精华
帖子
3365 
注册时间
2007-6-13 
最后登录
2023-2-10 
3
发表于 2018-7-30 22:48 |只看该作者
不错

Rank: 4

现金
75 元 
精华
帖子
58 
注册时间
2018-7-3 
最后登录
2019-5-22 
4
发表于 2018-7-31 12:58 |只看该作者
这是很早以前的研究了,罗氏的这两个药其实效果并不好

Rank: 4

现金
66 元 
精华
帖子
59 
注册时间
2015-10-6 
最后登录
2020-6-11 
5
发表于 2018-7-31 17:40 |只看该作者
多谢。不是说FDA已经几乎批准了一种新的壳抑制剂了吗?看来进展不错。

Rank: 4

现金
257 元 
精华
帖子
164 
注册时间
2010-6-13 
最后登录
2022-3-9 
6
发表于 2018-8-1 12:43 |只看该作者
求教楼主,我看了您的好几篇核衣壳的文章,请问核衣壳可以耗竭CCCDNA?那是不是就意味着可以耗竭hbsag,核衣壳有比核苷类强大很多的间接降低CCCDNA的能力,只是如果单用,耗竭时间会比较长。

Rank: 10Rank: 10Rank: 10

现金
20661 元 
精华
帖子
12793 
注册时间
2013-12-29 
最后登录
2024-11-3 
7
发表于 2018-8-1 15:10 |只看该作者
爱上静 发表于 2018-8-1 12:43
求教楼主,我看了您的好几篇核衣壳的文章,请问核衣壳可以耗竭CCCDNA?那是不是就意味着可以耗竭hbsag,核 ...

http://wap.ulabmed.com/content-134-4519-1.html

Rank: 10Rank: 10Rank: 10

现金
20661 元 
精华
帖子
12793 
注册时间
2013-12-29 
最后登录
2024-11-3 
8
发表于 2018-8-1 15:12 |只看该作者
HBsAg 和 HBeAg 的血液水平可以是HBV感染的肝细胞中cccDNA存在的生物标志物。因此,预期这些标志物的下降与cccDNA产生的抑制相关。

Rank: 4

现金
257 元 
精华
帖子
164 
注册时间
2010-6-13 
最后登录
2022-3-9 
9
发表于 2018-8-1 17:41 |只看该作者
回复 newchinabok 的帖子

哇,刚去看了下这个一诺医学的网站,真的很多前沿消息啊。

Rank: 10Rank: 10Rank: 10

现金
20661 元 
精华
帖子
12793 
注册时间
2013-12-29 
最后登录
2024-11-3 
10
发表于 2018-8-1 17:49 |只看该作者
爱上静 发表于 2018-8-1 17:41
回复 newchinabok 的帖子

哇,刚去看了下这个一诺医学的网站,真的很多前沿消息啊。 ...

http://www.natap.org/这个乙肝栏目更牛
‹ 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, 2024-11-15 22:30 , Processed in 0.019152 second(s), 11 queries , Gzip On.

Powered by Discuz! X1.5

© 2001-2010 Comsenz Inc.