Arbutus Provides an HBV Pipeline Update

tonychant

Arbutus Provides an HBV Pipeline Update

TKM-HBV Progressing to Phase II in HBV Infected Patients by Year-End
TKM-HBV Phase II S-Antigen Reduction Data Expected in 2016
Initiation of Proprietary Combination Studies in HBV Infected Patients Expected in 2017
Conference Call Scheduled for 7:30AM Pacific

VANCOUVER, British Columbia and DOYLESTOWN, Pa., Oct. 28, 2015 (GLOBE NEWSWIRE) -- Arbutus Biopharma Corporation (Nasdaq:ABUS), an industry-leading therapeutic solutions company focused on developing a cure for chronic hepatitis B virus infection (HBV), today issued an update on the company's HBV pipeline, including plans to progress lead pipeline candidate TKM-HBV into a multi-dose Phase II study in HBV infected patients by year-end.

TKM-HBV Progressing to Phase II in HBV Infected Patients

TKM-HBV, Arbutus' RNAi product candidate for HBV, is progressing to a Phase II multi-dosing study in HBV infected patients based on results to date from a Phase I single ascending dose study. TKM-HBV, which comprises three RNAi triggers that target all HBV transcripts, has been shown in preclinical studies to reduce all viral antigen levels as well as cccDNA. TKM-HBV's design will target hepatitis B surface antigen (HBsAg) expression regardless of its source. The Phase I clinical trial is a randomized, single-blind, placebo-controlled study, involving single ascending doses of TKM-HBV. The study is assessing the safety, tolerability and pharmacokinetics of intravenous administration of two LNP formulations (third and fourth generation) of TKM-HBV in healthy adult subjects. In order to enable maximum TKM-HBV dose escalation, steroid premedication was added to the Phase I protocol. At this time, a maximum tolerated dose has not yet been reached and evaluation of higher doses is under consideration.

TKM-HBV Phase II Study

Pending confirmation from the relevant regulatory authorities, the Phase II study will evaluate two dose levels of TKM-HBV administered as three monthly doses in chronic HBV infected patients who are on stable background nucleot(s)ide analog therapy. In the proposed protocol, eight subjects will be enrolled in each of the dose cohorts with six subjects receiving TKM-HBV, and two receiving placebo. Dosing in this study is expected to begin by year-end. HBsAg reduction results are expected to be reported in 2016. The TKM-HBV product candidate that will be studied in Phase II will be referred to as ARB-1467.

Status update on other HBV pipeline programs

Arbutus believes that direct-acting antiviral drugs such as TKM-HBV, cccDNA formation inhibitors and core protein/capsid assembly inhibitors represent the most important approaches with the highest probability of contributing to a cure. As a result, Arbutus has prioritized and accelerated development of its direct acting antiviral product candidates including the company's cccDNA formation inhibitors and core protein/capsid assembly inhibitors.

cccDNA formation inhibitors. Arbutus has made significant progress with its discovery of potent and unique small molecule cccDNA formation inhibitors, directly targeting this unique viral reservoir. As presented at the 2015 International Meeting on Molecular Biology of Hepatitis B Viruses earlier this month, Arbutus' cccDNA formation inhibitors demonstrate synergy with approved nucleot(s)ide analogs in preclinical models, which supports the potential for added benefit when combining these agents in HBV infected patients. Arbutus expects to file an IND (or equivalent filing) for a cccDNA formation inhibitor in 2H16, with a plan to include the molecule in combination studies in 2017.

Core protein/capsid assembly inhibitors. HBV core protein, or capsid, is required for viral replication and core protein may have additional roles in cccDNA function. Current nucleot(s)side analog therapy significantly reduces serum HBV DNA levels but HBV continues to replicate in the liver, thereby enabling the infection to persist and progress. Effective therapy for patients requires combinations consisting of new agents that will more effectively block viral replication. Arbutus has identified potent and unique HBV core protein/capsid inhibitors that are expected to enter clinical development in 2H16.

TLR9 agonist CYT003. Arbutus' TLR9 agonist, CYT003, is anticipated to be active in boosting the immune system in HBV patients, and will be used in settings where direct acting antiviral agents have reduced viral replication and antigen production. Arbutus is planning to start clinical development of CYT003 in 2016, in time to enable inclusion of this molecule in combination studies in 2017.

Cyclophilin inhibitor OCB-030. After extensive preclinical evaluation of OCB-030 and other cyclophilin inhibitors against HBV, Arbutus has concluded that the data do not support further development of OCB-030 as a single agent or in combination with our other drug candidates. As a result, Arbutus is discontinuing development of OCB-030 and has suspended interest in the cyclophilin inhibitor class so the company can focus its resources on higher priority agents that directly target HBV. This decision is based on a significant amount of research and analysis conducted by Dr. Sofia and his team, which will be presented at the HepDart conference in December.

Proprietary combination timelines. Importantly, the development timelines for Arbutus' HBV pipeline should enable the start of combination studies in 2017 that include TKM-HBV, an approved nucleot(s)ide analog, and one or more of: a cccDNA formation inhibitor, a core protein/capsid assembly inhibitor, or CYT-003. Arbutus' current cash balance is expected to fund operations into late 2018, well beyond the anticipated timeline for initial combination data.

"We are very excited to be advancing TKM-HBV into Phase II and look forward to reporting HBsAg reduction data from this multi-dose study in HBV patients in 2016," said Dr. Mark J. Murray, Arbutus' President and CEO. "I am also delighted with the progress our scientific team is making in advancing our oral direct acting antiviral programs targeting cccDNA formation and core protein/capsid assembly. We believe that our diverse and differentiated pipeline will enable us to initiate important proprietary drug combinations in 2017, on our way to developing curative combination regimens for HBV."

Updated 2016 Goals and Expected Milestones

Arbutus is revising its previously issued pipeline guidance. The company expects to have four HBV products in clinical development by the end of 2016, including the two INDs (or IND equivalents) expected to be filed for the cccDNA formation inhibitor program and the core protein/capsid inhibitor program.

Conference Call Today

Arbutus will hold a conference call and webcast today, Wednesday October 28, 2015, at 7:30 a.m. Pacific Time (10:30 a.m. Eastern Time) to provide a corporate update. A live webcast of the call can be accessed through the Investor section of Arbutus' website at www.arbutusbio.com. Or, alternatively, to access the conference call, please dial 1-914-495-8556 or 1-866-393-1607.

An archived webcast will be available on the Arbutus website approximately two hours after the event. Alternatively, you may access a replay of the conference call by calling 1-404-537-3406 or 1-855-859-2056 and referencing conference ID 69450867.

About Arbutus

Arbutus Biopharma Corporation is a biopharmaceutical company dedicated to discovering, developing and commercializing a cure for patients suffering from chronic HBV infection. Our strategy is to target the three pillars necessary to develop a curative regimen for HBV: suppressing HBV replication within liver cells, stimulating and reactivating the body's immune system so that it can mount an effective defense against the virus and, eliminating the reservoir of viral genomic material known as covalently closed circular DNA, or cccDNA that is the source of HBV persistence. Our portfolio of assets includes a broad pipeline of drug candidates for use in combination to develop a cure for HBV. To support continuous discovery of potential novel drug candidates and technologies, Arbutus has a research collaboration agreement with the Baruch S. Blumberg Institute that provides exclusive rights to in-license any intellectual property generated through the relationship. The Baruch S. Blumberg Institute was established in 2003 by the Hepatitis B Foundation.

Arbutus is headquartered in Vancouver, BC, Canada with offices in Doylestown, PA, USA. For more information, visit www.arbutusbio.com.

Forward Looking Statements and Information

This press release contains forward-looking statements within the meaning of the Section 27A of the Securities Act of 1933 and Section 21E of the Securities Exchange Act of 1934, and forward looking information within the meaning of Canadian securities laws (collectively, "forward-looking statements"). Forward-looking statements in this press release include statements about plans to progress lead pipeline candidate TKM-HBV into a multi-dose Phase II study in HBV infected patients by year-end, pending confirmation from the relevant regulatory authorities, with HBsAg reduction results expected to be reported in 2016; the ability of TKM-HBV to target hepatitis B surface antigen (HBsAg) expression regardless of its source; expectations to file an IND (or equivalent filing) for a cccDNA formation inhibitor in 2H16, with a plan to include the molecule in combination studies in 2017; expectations for potent and unique HBV core protein/capsid inhibitors to enter clinical development in 2H16; the anticipation for Arbutus' TLR9 agonist, CYT003, to be active in boosting the immune system in HBV patients, and to be used in settings where direct acting antiviral agents have reduced viral replication and antigen production; plans to start clinical development of CYT003 in 2016, in time to enable inclusion of the molecule in combination studies in 2017; discontinuing development of OCB-030 and suspending interest in the cyclophilin inhibitor class; the start of combination studies in 2017 that include TKM-HBV, an approved nucleot(s)ide analog, and one or more of a cccDNA formation inhibitor, a core protein/capsid assembly inhibitor, and CYT-003; the expectation that Arbutus' current cash balance will fund operations into late 2018, well beyond the anticipated timeline for initial combination data; initiating important proprietary drug combinations in 2017, on the way to developing curative combination regimens for HBV; the expectation to have four HBV products in clinical development by the end of 2016, including the two INDs (or IND equivalents) expected to be filed for the cccDNA formation inhibitor program and the core protein/capsid inhibitor program; and a strategy to target the three pillars necessary to develop a curative regimen for HBV.

With respect to the forward-looking statements contained in this press release, Arbutus has made numerous assumptions regarding, among other things: the effectiveness of preclinical and clinical trials, and the usefulness of the data; the continued demand for Arbutus' assets; and the stability of economic and market conditions. While Arbutus considers these assumptions to be reasonable, these assumptions are inherently subject to significant business, economic, competitive, market and social uncertainties and contingencies.

Additionally, there are known and unknown risk factors which could cause Arbutus' actual results, performance or achievements to be materially different from any future results, performance or achievements expressed or implied by the forward-looking statements contained herein. Known risk factors include, among others: anticipated pre-clinical and clinical trials may be more costly or take longer to complete than anticipated, and may never be initiated or completed, or may not generate results that warrant future development of the tested drug candidate; Arbutus may not receive the necessary regulatory approvals for the clinical development of Arbutus' products; economic and market conditions may worsen; and market shifts may require a change in strategic focus.

A more complete discussion of the risks and uncertainties facing Arbutus appears in Arbutus' Annual Report on Form 10-K and Arbutus' continuous disclosure filings, which are available at www.sedar.com and at www.sec.gov. All forward-looking statements herein are qualified in their entirety by this cautionary statement, and Arbutus disclaims any obligation to revise or update any such forward-looking statements or to publicly announce the result of any revisions to any of the forward-looking statements contained herein to reflect future results, events or developments, except as required by law.

StephenW

杨梅提供一个HBV管道更新
中国商业电讯
2015年10月28日：08:00 ET

TKM-HBV进行到第二阶段的乙肝病毒感染者到今年年底
TKM-HBV二期表面抗原减少数据预计在2016年
对所有组合在研究乙型肝炎病毒感染患者初始预计在2017年
电话会议定于上午7:30太平洋

温哥华，不列颠哥伦比亚省和DOYLESTOWN，宾夕法尼亚州，2015年10月28日（GLOBE NEWSWIRE） - 杨梅生物制药公司（纳斯达克股票代码：安博），业界领先的治疗解决方案公司，致力于开发一种治疗慢性乙型肝炎病毒感染（HBV ）今天在该公司的乙肝管道发出的最新情况，包括计划进度铅管道的候选人TKM-HBV为乙型肝炎病毒感染的患者多剂量的II期到今年年底。

TKM-HBV进行到第二阶段的乙肝病毒感染者

TKM-HBV，杨梅“的RNAi产品候选人HBV，进展到第二阶段的基础上迄今取得的成就，从一个阶段多给药研究乙型肝炎病毒感染者我单剂量递增的研究。 TKM-HBV，其包含靶向所有的HBV转录物3的RNAi触发器，已经显示出在临床前研究，以减少所有病毒抗原水平以及cccDNA的。 TKM-HBV的设计将针对乙肝表面抗原（HBsAg）的表达，无论其来源。在I期临床试验是一项随机，单盲，安慰剂对照研究，涉及单递增剂量TKM-HBV的。这项研究是评价其安全性，耐受性和两个LNP TKM-HBV制剂（第三和第四代）静脉给药的药代动力学健康成年受试者。为了使最大TKM - HBV剂量递增，类固醇前用药加入到第一阶段的协议。此时，最大耐受剂量尚未达到与较高剂量的评价是在考虑中。

TKM-HBV II期临床研究

待确认来自相关监管部门，第二阶段的研究将评估TKM-HBV的两个剂量水平给予三个每月剂量慢性HBV感染者谁是稳定的背景nucleot（S）IDE模拟治疗。在所提出的协议，8位个体将参加在各剂量群组的六个受试者接受TKM-HBV，和两个接受安慰剂。配料在这项研究预计将于今年年底。 HBsAg的减少结果预计将在2016年进行报道，将研究在第二阶段将被称为ARB，1467年TKM-HBV候选产品。

其他HBV管道程序状态更新

杨梅认为，直接作用的抗病毒药物，例如TKM-HBV，cccDNA的形成抑制剂和核心蛋白​​/衣壳包装抑制剂表示与促进治愈的概率最高的最重要的方法。其结果是，杨梅已优先并加快其直接作用的抗病毒候选产品，包括该公司的cccDNA的形成抑制剂和核心蛋白​​/衣壳组装抑制剂的发展。

cccDNA的形成抑制剂。杨梅曾与它的发现有力和独特的小分子cccDNA的形成抑制剂制成显著的进步，直接瞄准了这一独特的病毒库。由于提出了在上本月初乙肝病毒分子生物学2015年的国际会议，杨梅“的cccDNA形成抑制剂表明协同批准nucleot（S）在临床前模型IDE类似物，在组合中HBV这些代理支持的潜在好处被传染的患者。杨梅预计将提起IND（或等值报）一个cccDNA的形成抑制剂在2H16，有计划，包括联合研究分子在2017年。

核心蛋白/衣壳组装抑制剂。 HBV核心蛋白或衣壳，需要病毒复制和核心蛋白​​可以具有在cccDNA的函数的其他角色。电流nucleot（多个）侧的模拟治疗显著降低血清HBV DNA水平但HBV继续复制在肝脏，由此使感染坚持和进步。有效治疗的患者，需要组合包括新的代理商，这将更加有效地阻断病毒的复制。杨梅已经确定，按照预期在2H16进入临床开发强有力的和独特的乙肝病毒核心蛋白/衣壳抑制剂。

TLR9激动剂CYT003。杨梅“TLR9激动剂，CYT003，预计活跃在刺激免疫系统乙肝患者，并在设置里直接作用抗病毒药物减少病毒的复制和抗原的生产将被使用。杨梅正计划启动CYT003的临床开发于2016年，在时间，使在2017年加入该分子的结合研究。

亲环蛋白抑制剂OCB-030。后OCB-030和抗HBV其他亲环蛋白抑制剂的广泛临床前评价，杨梅的结论是，数据不支持的OCB-030的进一步发展作为单一药剂或与我们的其他候选药物组合。其结果是，杨梅将停止OCB-030的发展，并已悬浮在亲环蛋白抑制剂类兴趣所以公司可以集中在较高优先级的代理直接靶向HBV其资源。这一决定是基于研究和分析索非亚博士和他的团队进行了显著量，这将在12月的HepDart会议上提出的。

专有组合时间表。重要的是，开发时间表杨梅'HBV的管道应该使组合研究的开始，2017年，包括TKM - HBV，经认可的nucleot（多个）的ide类似物，和一个或多个：cccDNA的形成抑制剂，核心蛋白/衣壳装配抑制剂或CYT-003。杨梅目前的现金余额预计运营提供资金到2018年末，远远超出了预期的时间表初始组合数据。

“我们非常高兴能够成为推动TKM-HBV进入第二阶段，并期待着这种多剂量研究乙肝病毒的患者在2016年报告的乙肝表面抗原减少的数据，”马克博士J.默里，杨梅的总裁兼CEO。 “我也很高兴与进步我们的科学团队正在推进针对cccDNA的形成和核心蛋白​​/衣壳的装配，我们的口服直接作用的抗病毒程序。我们相信，我们的多元化和差异化的管道将使我们能够开始重要的专利药物组合在2017年，对我们的方式来开发治疗联合方案乙肝病毒。“

更新2016年的目标和预期里程碑

杨梅正在修订其先前发布的管道指导。该公司预计到2016年年底，包括两个的IND（或IND当量）预计将提出对cccDNA的形成抑制剂方案和核心蛋白​​/衣壳抑制剂方案有四个HBV的产品处于临床开发阶段。

电话会议今天

杨梅将举行电话会议并进行网络广播的今天，2015年10月28日星期三上午7:30太平洋时间（上午十点30分美国东部时间），以提供企业更新。电话会议的网上直播可通过杨梅“网站www.arbutusbio.com的投资者部分进行访问。或者，访问电话会议，请拨打1-914-495-8556或1-866-393-1607。

归档的网络直播将可在杨梅的网站时约两小时后。另外，您也可以拨打1-404-537-3406或1-855-859-2056并引用会议ID 69450867访问电话会议的重播

zgct

好文！感谢！

重韧

2018年是最有可能的在治乙肝的岁月中最具里程碑的一年。

齐欢畅2

好文章

newchinabok

亲环蛋白抑制剂ocb-030。抗乙肝病毒和其他亲环蛋白抑制剂ocb-030广泛的临床前评估后，杨梅已经得出结论，数据不支持进一步的发展ocb-030作为单药或与其他药物组合。因此，杨梅停止发展ocb-030

newchinabok

TKM-HBV Phase II  
cccDNA的形成抑制剂
核心蛋白/衣壳组装抑制剂
TLR9激动剂CYT003
2016进临床

guilin2013

现在最近的是ABX203和ARC-520，16年能够进入中国做临床试验就好了

hao2014

箭头公司要有危机感了

再不抓紧，别人赶上来了

guilin2013

ARC-520明年就开始三期，放在中国做，17年上市，然后来过ARC-520+干扰素半年疗程标准疗法，表抗转阴达到60个点以上，就可以了；然后再慢慢等其它的新药上市，像丙肝一样，慢慢提高治愈离