EASL2015:HBV核心抑制剂NVR 3-778的人性化UPA / SCID小鼠模型高抗病

StephenW

HIGH ANTIVIRAL ACTIVITY OF THE HBV CORE INHIBITOR NVR 3-778 IN THE HUMANIZED UPA/SCID MOUSE MODEL
Klaus Klumpp* 1, Takashi Shimada2, Lena Allweiss3, Tassilo Volz3, Marc Luetgehetman3, 4, Osvaldo Flores1, George Hartman1, Angela Lam1, Maura Dandri3, 5
1Novira Therapeutics Inc., Doylestown, United States, 2PhoenixBio Co., Ltd. , Higashi-Hiroshima, Japan, 3Department of Internal Medicine, 4Institute of Microbiology, Virology and Hygiene, University Medical Center Hamburg-Eppendorf, 5German Center for Infection Research, Hamburg-Lübeck-Borstel Partner Site, Hamburg, Germany


Corresponding author’s email: [email protected]


Background and Aims:
NVR 3-778 represents a new class of HBV core inhibitors and is in clinical development for the treatment of chronic hepatitis B. We determined the antiviral activity of NVR 3-778 alone or in combination with PEG-IFN or entecavir in the humanized uPA/SCID mouse model of HBV infection.
Methods:
Thirty six mice infected with HBV genotype C, with serum HBV viremia >106 copies/ml and human serum albumin levels >6 mg/ml were randomized into 6 treatment groups: (1) NVR 3-778, (2) vehicle, (3) entecavir, (4) PEG-IFN, (5) NVR 3-778 + entecavir and (6) NVR 3-778 + PEG-IFN. Virologic endpoints included serum and intrahepatic HBV DNA, HBV antigen, cccDNA and HBV RNA levels.
Results:
All 6 mice in the NVR 3-778 group showed >1.7 log serum viral load reduction from baseline at day 14 (mean (median) viral load reduction 1.9 (1.9) log). This effect was similar to that obtained with entecavir (p > 0.05) and larger than that obtained with PEG-IFN treatment (p < 0.05). The largest viremia reduction across all groups was obtained when NVR 3-778 was combined with PEG-IFN, resulting in a mean (median) viral load reduction of 2.4 (2.4) log at day 14, significantly larger than that obtained with either NVR 3-778 or PEG-IFN alone (p <0.05). The combination of NVR 3-778 and PEG-IFN also showed the largest reduction in intrahepatic HBV DNA loads (median 3.0 log; p< 0.005) as compared to other treatment groups (NVR 3-778 alone 2.0 log, entecavir 2.2 log and PEG-IFN 1.8 log). Intrahepatic HBV RNA loads were reduced significantly in the PEG-IFN groups only. As expected, serum levels of HBsAg were reduced most strongly in the PEG-IFN groups and were only minimally affected by NVR 3-778 alone. Levels of cccDNA were similar across treatment groups. Treatment with NVR 3-778 was not associated with any significant changes in the levels of human serum albumin, serum alanine aminotransferase (ALT) levels, or intrahepatic amounts of human β-globin, indicating that the number of human hepatocytes remained stable during the treatment period.
Conclusions:
The HBV core inhibitor NVR 3-778 demonstrated high intrinsic antiviral activity in HBV infected humanized mice. Serum HBV viral load reduction was larger than that obtained with PEG-IFN and similar to entecavir alone. The combination of NVR 3-778 and PEG-IFN showed higher antiviral activity as compared to NVR 3-778 or PEG-IFN alone, indicating a functionally beneficialinteraction between a core inhibitor and interferon alpha.


Disclosure of Interest: K. Klumpp:  Employee: Novira Therapeutics, T. Shimada:  Employee: PhoenixBio Co., Ltd. , L. Allweiss:  Other: Novira Therapeutics, T. Volz:  Other: Novira Therapeutics, M. Luetgehetman:  Other: Novira Therapeutics, O. Flores:  Employee: Novira Therapeutics, G. Hartman:  Employee: Novira Therapeutics, A. Lam:  Employee: Novira Therapeutics, M. Dandri:  Other: Novira Therapeutics

StephenW

HBV核心抑制剂NVR 3-778的人性化UPA / SCID小鼠模型高抗病毒活性

克劳斯Klumpp的* 1，隆Shimada2，莉娜Allweiss3，塔希洛Volz3，马克Luetgehetman3，4，奥斯瓦尔多Flores1，乔治Hartman1，安吉拉Lam1，莫拉Dandri3，5

1Novira Therapeutics公司，Doylestown的，美国的，2PhoenixBio有限公司，东广岛，日本，内科3Department，微生物学，病毒学和卫生，大学医学中心汉堡Eppendorf公司，5German中心4Institute的感染研究，汉堡-Lübeck-Borstel合作伙伴网站，德国汉堡



通讯作者的邮箱：[email protected]



背景和目的：NVR 3-778代表一类新的HBV核心抑制剂，并在临床开发用于治疗慢性乙型肝炎的治疗，我们确定的NVR单独使用或与PEG-IFN或恩替卡韦组合3-778的抗病毒活性HBV感染的人源化的uPA / SCID小鼠模型。

方法：感染HBV C基因型三十六只小鼠，与血清HBV病毒血症> 106拷贝/ ml的与人血清白蛋白水平> 6毫克/毫升，随机分成6个治疗组：（1）NVR 3-778，（2）的车辆， （3）恩替卡韦，（4）PEG-IFN，（5）的NVR 3-778 +恩替卡韦和（6）的NVR 3-778 + PEG-IFN。病毒学终点包括血清和肝内HBV DNA，HBV抗原的cccDNA和HBV RNA水平。

结果：6小鼠在NVR 3-778组显示从基线的14天（均值（中位数）病毒载量下降1.9（1.9）日志）> 1.7日志血清病毒载量下降。这种效果是相似的恩替卡韦（P> 0.05），比与PEG-IFN治疗（P <0.05）中获得更大的获得。当NVR 3-778物与PEG-IFN，造成的平均（中值）2.4（2.4）的病毒载量减少登录在第14天，获得所有组的最大病毒血症减少，与任一NVR 3比显著放大获得-778或PEG-IFN单独（P <0.05）。 NVR 3-778和PEG-IFN的组合也显示出在肝内的HBV DNA负荷最大减少（平均3.0日志; P <0.005）相比，其它处理组（NVR 3-778单独2.0日志，恩替卡韦2.2日志和PEG -IFN 1.8日志）。肝内HBV RNA的负荷是在仅在PEG-IFN组显著降低。正如预期的那样，乙肝表面抗原血清水平的PEG-IFN组最强烈的减少，只能提供最低限度的影响NVR 3-778孤单。 cccDNA的水平是各治疗组相似。治疗NVR 3-778不与在人血清白蛋白，血清谷丙转氨酶（ALT）的水平，或人β珠蛋白的肝内量的水平的任何显著变化相关，这表明在处理过程中的人肝细胞的数量保持稳定期。

结论：HBV核心抑制剂的NVR 3-778表现出乙型肝炎病毒高特性的抗病毒活性感染的人源化小鼠。血清HBV病毒载量下降比得到用PEG-IFN和类似独自恩替卡韦大。 NVR 3-778和PEG-IFN的组合表现出更高的抗病毒活性比NVR 3-778或PEG-IFN单独，表示芯抑制剂和干扰素α之间的功能上beneficialinteraction。



股权变动：K. Klumpp的：员工：Novira治疗，T.岛田：员工：PhoenixBio有限公司，L. Allweiss：其他：Novira治疗，T. VOLZ：其他：Novira治疗，M. Luetgehetman：其他： Novira治疗，O.弗洛雷斯：员工：Novira治疗，G.哈特曼：员工：Novira治疗，林A.：员工：Novira治疗，M. Dandri：其他：Novira治疗

newchinabok

人源小鼠是经常用的感染模型，不知人体抗病毒如何，8月有结果，老外比中国试验透明些

newchinabok

人源化的uPA / SCID小鼠模型数据与人体有一定差异性，期待11月人体数据，人体抗病毒如何？期待

zgct

期待

StephenW

Novira Therapeutics to Present at 2015 AASLD Meeting in San Francisco
Poster presentation: "Phase 1b Efficacy and Safety of NVR 3-778, a First-In-Class HBV Core Inhibitor, in HBeAg-Positive Patients with Chronic HBV Infection"

Poster presentation: "Encapsidation and secretion of HBV RNA can be inhibited by Core Inhibitors but not by Nucleoside Analogs"

Oral presentation: "Inhibition of Hepatitis B Virus Replication by the HBV Core Inhibitor NVR 3-778"

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DOYLESTOWN, Pa., Oct. 20, 2015 /PRNewswire/ -- Novira Therapeutics, Inc., a privately held, clinical-stage biopharmaceutical company developing novel therapies for curative treatment of chronic hepatitis B virus (HBV) infection, today announced that it will present two posters and one oral presentation for its core inhibitors, including its lead candidate, NVR 3-778, at the upcoming 2015 annual meeting of the American Association for the Study of Liver Diseases (AASLD) in San Francisco.

Late-breaking poster LB-10 on November 16 will describe the safety, pharmacokinetics and HBV DNA reduction efficacy of NVR 3-778 monotherapy in a 28 day Phase 1b clinical study.

Poster 2064 on November 17 will describe the inhibition of HBV RNA encapsidation and secretion by the core inhibitor NVR-3891.

Oral presentation 33 on November 15 at 3:30 PM will describe preclinical antiviral activity of NVR 3-778 against wild-type HBV, HBV nucleos(t)ide resistant variants and representative HBV strains from genotypes A to H.

About NVR 3-778

NVR 3-778 is a small molecule, direct acting antiviral, for oral administration in patients with Chronic Hepatitis B (CHB) that inhibits the HBV core or capsid protein. HBV core is a novel and promising drug target with multiple activities required for viral replication and persistence. Inhibition of the HBV core protein function by NVR 3-778 offers the potential for more efficient suppression of virus production and replication, leading to improved durable viral suppression and functional cure rates. NVR 3-778 completed a Phase 1a clinical trial in 2014 and is currently enrolling a Phase 1b clinical trial.

About HBV

Hepatitis B infection presents a significant unmet medical need with an estimated 350 million people worldwide living with chronic HBV infection. A significant number of patients with chronic infection incur a higher risk of developing cirrhosis and cancer. It is estimated that 60% of hepatocellular carcinoma (liver cancer) is a direct consequence of HBV infection. Current drugs approved for the management of CHB include PEG-Interferon and nucleot(s)ides which can effectively suppress virus replication, but rarely lead to a cure.

About Novira Therapeutics

Novira Therapeutics, Inc., is a privately held biopharmaceutical company focused on discovery and development of first-in-class antiviral drugs for the treatment of chronic HBV infection (CHB), a global disease with a high level of unmet medical need. The company is employing innovative chemistry and biology technologies to discover small molecule inhibitors of the HBV core or capsid protein as well as other drugs with novel mode of action. The company's novel antivirals will offer the potential to address the limitations of current CHB therapies when used either as mono-therapy or in combination with existing standards of care.

For more information, visit www.noviratherapeutics.com.

Contacts:

Corporate Contact
Christian S. Schade
Chief Executive Officer
[email protected]

Media Contacts
David Schull                           
Matt Middleman, M.D.                                    
Russo Partners                                             
T: (212) 845-4271                              
T: (212) 845-4272
[email protected]" rel="nofollow" target="_blank">[email protected]
[email protected]



SOURCE Novira Therapeutics, Inc.

StephenW

Novira治疗将出席在旧金山2015年AASLD会议
海报介绍：“阶段1b疗效和NVR 3-778的安全，创一流HBV核心抑制剂，HBeAg阳性慢性HBV感染”

海报介绍：“包壳和乙肝病毒RNA的分泌，可以通过核心抑制剂抑制，但不被核苷类似物”

口头报告：“乙肝病毒复制的HBV核心抑制剂NVR 3-778抑制”

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DOYLESTOWN，宾夕法尼亚州，二〇一五年十月二十○日/新华美通/ - Novira Therapeutics公司是一家私人持有，临床阶段的生物技术企业，开发创新疗法有效治疗慢性乙型肝炎病毒（HBV）感染，今天宣布，将有两个海报，一个口头报告的核心抑制剂，包括它的主角候选人，NVR 3-778，在美国协会肝病研究（AASLD）在旧金山举行的即将到来的2015年年度会议。

的最新海报LB-10于11月16将描述28天1b期临床研究的NVR 3-778单药治疗的安全性，药代动力学和HBV DNA降低药效。

11月17日海报2064将描述由核心抑制剂NVR-3891的乙肝病毒RNA壳体化和分泌的抑制。

11月15日口头报告33下午3:30将介绍NVR 3-778的临床抗病毒活性，对野生型HBV，HBV核苷（酸）IDE耐药变异和有代表性的乙肝病毒株的基因型A到H

关于NVR 3-778

NVR 3-778是一种小分子，直接作用抗病毒药物，用于口服治疗慢性乙型肝炎（CHB）抑制HBV核心或衣壳蛋白。 HBV核心是一种新颖的和有希望的药物靶，病毒复制所需的和持久性的多个活动。通过NVR 3-778 HBV核心蛋白功能的抑制提供了病毒的生产和复制的效率更高的抑制的潜力，从而提高耐用病毒抑制和功能的治愈率。 NVR 3-778完成了一个阶段1a临床试验于2014年，目前正在招收一个阶段1b临床试验。

关于乙肝病毒

乙肝病毒感染提出了一个显著未满足的医疗需求，估计有3.5亿人生活在全球慢性HBV感染。一个显著一些慢性感染患者产生发展为肝硬化和癌症的风险较高。据估计，肝细胞癌（肝癌）60％是HBV感染的直接结果。批准用于慢性乙型肝炎的管理目前的药物包括PEG干扰素和nucleot（S）集成开发环境可以有效抑制病毒复制，但很少导致治疗。

关于Novira治疗

Novira Therapeutics公司，是一家私人持有的生物制药公司，专注于发现和先入类抗病毒药物开发用于慢性HBV感染（CHB）的处理，以满足医疗需要的高层次的全球性疾病。该公司采用创新的化学和生物技术，发现HBV核心或衣壳蛋白的小分子抑制剂以及其它药物作用的新模式。该公司的新的抗病毒药物将提供使用时无论是作为单一疗法或与关心的现有标准组合，以解决当前的CHB疗法的局限性的潜力。

欲了解更多信息，请访问www.noviratherapeutics.com。

联系方式：

公司联系方式
基督教S.沙德
首席执行官
[email protected]

媒体联系
大卫·斯卡尔
马特中间人，医学博士
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T：（212）845-4271
T：（212）845-4272
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源Novira Therapeutics公司

newchinabok

感谢分享，高度关注

zgct

不是疫苗免疫调节药？

StephenW

zgct 发表于 2015-10-21 13:00
不是疫苗免疫调节药？

HBV核心抑制剂(如 GLS4)