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标题: 发现和机械研究苯甲酰胺衍生品,调节乙型肝炎病毒衣壳组装 [打印本页]

作者: newchinabok    时间: 2017-11-7 14:36     标题: 发现和机械研究苯甲酰胺衍生品,调节乙型肝炎病毒衣壳组装

本帖最后由 newchinabok 于 2017-11-7 14:42 编辑

http://jvi.asm.org/content/91/16 ... 0-b87b-7b8261dbad27
作者: newchinabok    时间: 2017-11-7 14:46

ABSTRACT
Chronic hepatitis B virus (HBV) infection is a global public health problem. Although the currently approved medications can reliably reduce the viral load and prevent the progression of liver diseases, they fail to cure the viral infection. In an effort toward discovery of novel antiviral agents against HBV, a group of benzamide (BA) derivatives that significantly reduced the amount of cytoplasmic HBV DNA were discovered. The initial lead optimization efforts identified two BA derivatives with improved antiviral activity for further mechanistic studies. Interestingly, similar to our previously reported sulfamoylbenzamides (SBAs), the BAs promote the formation of empty capsids through specific interaction with HBV core protein but not other viral and host cellular components. Genetic evidence suggested that both SBAs and BAs inhibited HBV nucleocapsid assembly by binding to the heteroaryldihydropyrimidine (HAP) pocket between core protein dimer-dimer interfaces. However, unlike SBAs, BA compounds uniquely induced the formation of empty capsids that migrated more slowly in native agarose gel electrophoresis from A36V mutant than from the wild-type core protein. Moreover, we showed that the assembly of chimeric capsids from wild-type and drug-resistant core proteins was susceptible to multiple capsid assembly modulators. Hence, HBV core protein is a dominant antiviral target that may suppress the selection of drug-resistant viruses during core protein-targeting antiviral therapy. Our studies thus indicate that BAs are a chemically and mechanistically unique type of HBV capsid assembly modulators and warranted for further development as antiviral agents against HBV.
IMPORTANCE HBV core protein plays essential roles in many steps of the viral replication cycle. In addition to packaging viral pregenomic RNA (pgRNA) and DNA polymerase complex into nucleocapsids for reverse transcriptional DNA replication to take place, the core protein dimers, existing in several different quaternary structures in infected hepatocytes, participate in and regulate HBV virion assembly, capsid uncoating, and covalently closed circular DNA (cccDNA) formation. It is anticipated that small molecular core protein assembly modulators may disrupt one or multiple steps of HBV replication, depending on their interaction with the distinct quaternary structures of core protein. The discovery of novel core protein-targeting antivirals, such as benzamide derivatives reported here, and investigation of their antiviral mechanism may lead to the identification of antiviral therapeutics for the cure of chronic hepatitis B.
作者: newchinabok    时间: 2017-11-7 15:24

这个药就是abus后续核衣壳抑制剂
作者: windu    时间: 2017-11-7 15:27

JVI:华人科学家郭巨涛教授发现新型乙肝病毒抑制剂
http://www.alabmed.com/content-134-4075-1.html
作者: newchinabok    时间: 2017-11-7 17:15

明年进临床
作者: windu    时间: 2017-11-7 20:05

newchinabok 发表于 2017-11-7 17:15
明年进临床

能临床的就值得关注,在哪里临床?
作者: newchinabok    时间: 2017-11-7 20:13

回复 windu 的帖子

1Q18: Initiate AB-423 Phase II multi ascending dose (MAD) study in HBV patients.
Mid-2018: AB-506 IND (or equivalent) filing.
Mid-2018: AB-452 IND (or equivalent) filing.
Mid-2018: Results from AB-423 multi-dosing study in HBV patients.
2H18: Interim on-treatment results from triple combination study of ARB-1467, tenofovir, and pegylated interferon.
作者: newchinabok    时间: 2017-11-7 20:20

AB-506,作为第二代衣壳抑制剂被提名进行IND能力研究。 临床前研究显示,AB-506具有相对于我们的主要衣壳抑制剂AB-423具有更具效力和更优异的药代动力学的潜力,将成为同类最佳的衣壳抑制剂。 该分子具有每日一次口服给药的潜力。 预计在2018年,AB-506将成为IND(或等值的)备案的目标。
作者: windu    时间: 2017-11-8 08:51

不知道杨梅公司的市场线路是怎么样的,多个类型的药物同时进行一代和二代药物临床,是一定要解决HBV之困顿吗?表抗降到0之后,一针干扰素应该能解决战斗了




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