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肝胆相照论坛 论坛 学术讨论& HBV English 箭头提交申请书开始ARC- 520阶段2a试验
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箭头提交申请书开始ARC- 520阶段2a试验   [复制链接]

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发表于 2013-11-26 03:12 |只看该作者 |倒序浏览 |打印

Arrowhead Submits Application to Begin Phase 2a Trial of ARC-520 for the Treatment of Chronic Hepatitis B Infection


PASADENA, Calif. - November 25, 2013 - Arrowhead Research Corporation (NASDAQ: ARWR), a biopharmaceutical company developing targeted RNAi therapeutics, today announced that it recently filed an application for approval to begin a phase 2a clinical trial of its RNAi-based therapeutic candidate, ARC-520, for the potential treatment of chronic hepatitis B virus infection. Pending approval, Arrowhead intends to proceed with a multicenter, randomized, double-blind, placebo-controlled, dose-escalation study. The study is being conducted to determine the depth and duration of hepatitis B surface antigen (HBsAg) reduction after a single intravenous dose of ARC-520 in combination with entecavir in patients with chronic HBV infection. Additional details on study design and anticipated timelines will be provided when patient enrollment begins.


An application for a Certificate for Clinical Trial was submitted to the Hong Kong Department of Health, and the study protocol, investigator brochure, and informed consent were submitted to the ethics committees at two sites in Hong Kong. Hong Kong was chosen as the location for the study based on the high prevalence of chronic HBV infection and for the advanced healthcare and regulatory system, which has a history of successful participation in clinical trials for antiviral agents.


Principal investigators Professor Man-Fung Yuen, Chief of Gastroenterology and Hepatology at The University of Hong Kong, Queen Mary Hospital, and Professor Henry LY Chan, Head of Gastroenterology and Hepatology at The Chinese University of Hong Kong, Prince of Wales Hospital, will conduct the study. These investigators and sites were selected based on their large pool of patients currently under care, their international standing as HBV researchers, and track record of high accrual rates for clinical trials involving viral hepatitis.

About ARC-520

Approximately 350 million people worldwide are chronically infected with the hepatitis B virus. Chronic HBV infection can lead to cirrhosis of the liver and is responsible for 80% of primary liver cancers globally. Arrowhead's RNAi-based candidate ARC-520 is designed to treat chronic HBV infection by reducing the expression and release of new viral particles and key viral proteins. The goal is to achieve a functional cure, which is an immune clearant state characterized by hepatitis B s-antigen negative serum with or without sero-conversion. The siRNAs in ARC-520 intervene at the mRNA level, upstream of where nucleotide and nucleoside analogues act. In transient and transgenic mouse models of HBV infection, a single co-injection of Arrowhead's DPC delivery vehicle with cholesterol-conjugated siRNA targeting HBV sequences resulted in multi-log knockdown of HBV RNA, proteins and viral DNA with long duration of effect. In a chimpanzee chronically infected with HBV and high viremia and antigenemia, ARC-520 induced rapid reductions of 90-95% in HBV DNA, e-antigen, and s-antigen. Arrowhead has completed enrollment in a phase 1 single ascending dose study in normal volunteers, which the company expects to follow with a phase 2a study in chronic HBV patients.


About Arrowhead Research Corporation

Arrowhead Research Corporation is a biopharmaceutical company developing targeted RNAi therapeutics. The company is leveraging its proprietary drug delivery technologies to develop targeted drugs based on the RNA interference mechanism that efficiently silence disease-causing genes. Arrowhead technologies also enable partners to create peptide-drug conjugates that specifically home to cell types of interest while sparing off-target tissues. Arrowhead's pipeline includes clinical programs in chronic hepatitis B virus and obesity and partner-based programs in oncology.


For more information please visit http://www.arrowheadresearch.com, or follow us on Twitter @ArrowRes. To be added to the Company's email list to receive news directly, please send an email to [email protected]


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发表于 2013-11-26 03:13 |只看该作者
箭头提交已应用到开始ARC- 520阶段2a试验为慢性乙型肝炎病毒感染的治疗

帕萨迪纳,加利福尼亚州 - 2013年11月25日 - 箭头研究公司(纳斯达克股票代码: ARWR ) ,一家生物制药公司,开发有针对性的RNAi治疗,今天宣布,它最近提出有关申请后,开始其基于RNAi的治疗一个阶段2a临床试验候选人, ARC- 520 ,用于治疗慢性乙肝病毒感染的潜在治疗。待审批,箭头拟进行的多中心,随机,双盲,安慰剂对照,剂量递增研究。这项研究正在开展,以确定乙肝表面抗原单次静脉剂量的ARC - 520与联合恩替卡韦治疗慢性乙肝病毒感染后( HBsAg)的降低的深度和持续时间。当病人登记开始研究设计和预期时间表的更多详细信息将被提供。

对于临床试验证明书的申请已提交卫生香港部,研究方案,研究者手册和知情同意是在香港的两个站点提交给伦理委员会。香港被选为该研究基于对慢性HBV感染的高流行和先进的医疗保健和监管体系,它在为抗病毒药物临床试验成功参与的历史位置。

主要研究者教授文凤园,胃肠病学和肝脏病学的院长在香港大学玛丽医院和教授亨利LY陈,胃肠病学和肝病学系主任香港的中国大学,威尔斯亲王医院,将进行这项研究。这些研究者和网站根据他们的大目前正在照顾,他们的国际地位为乙肝病毒研究人员,病人池被选定并跟踪高计提率的纪录,涉及病毒性肝炎的临床试验。

关于ARC -520
全球约有3.5亿人感染慢性B型肝炎病毒。慢性HBV感染可导致肝硬化,负责80 %的全球原发性肝癌。箭头的RNAi为基础的候选ARC- 520旨在通过减少新病毒颗粒和病毒的关键蛋白质的表达和释放治疗慢性HBV感染。我们的目标是实现一个功能的固化,这是其特征在于, B型肝炎表面抗原阴性血清有或无血清转换的免疫clearant状态。在ARC- 520的siRNA的干预在mRNA水平,其中的核苷酸和核苷类似物充当上游。在HBV感染中,单个共同注入箭头的DPC递送载体的胆固醇缀合的siRNA靶向的瞬态和转基因小鼠模型的HBV序列导致了HBV RNA,蛋白质和病毒DNA带的效果持续时间长的多记录击倒。在黑猩猩慢性乙型肝炎病毒感染和高病毒血症和抗原, ARC- 520诱导的90-95 %的速度快速降低HBV-DNA , e抗原和表面抗原。慈姑已完成招生第一阶段的单剂量递增研究中正常的志愿者,该公司预计跟随在慢性HBV患者相2a研究。



关于箭头研究公司

箭头研究公司是一家生物制药公司,开发有针对性的RNAi疗法。该公司利用其专有的给药技术,开发基于该有效地沉默致病基因的RNA干扰机制,有针对性的药物。慈姑技术也使合作伙伴创造肽偶联药物,专门在家细胞类型的利益而不惜脱靶组织。箭头的管道包括在慢性乙型肝炎病毒与肥胖和伙伴为基础的方案在肿瘤学临床方案。

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发表于 2013-11-26 13:03 |只看该作者
好啊!进军香港了!估计明年会有好消息传来。但愿是震撼性的好消息。深圳、广州的战友多前往转转,能报名上药的可能早点上岸,不报名的也可多多刮回一波又一波的好消息。
似乎现在就可以给玛丽医院的某博士写封情深意切的英文信了。

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发表于 2013-11-26 14:06 |只看该作者
本帖最后由 StephenW 于 2013-11-26 14:07 编辑

回复 候月 的帖子

"主要研究者教授文凤园,胃肠病学和肝脏病学的院长在香港大学玛丽医院和教授亨利LY陈"

两位教授, 特别是教授 Henry 陈,非常有名,非常有经验进行临床研究和临床试验.
几年前陈教授和他的小组发现,低水平血清HBsAg可以预测HBsAg血清学转换.

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发表于 2013-11-26 14:32 |只看该作者
绝对的好消息,同志们,有希望了!

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发表于 2013-11-26 15:43 |只看该作者
绿儿利谷牛斯
核苷类:拉米夫定、阿德福韦酯、恩替卡韦、替比夫定、替诺福韦

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发表于 2013-11-26 15:47 |只看该作者
本帖最后由 StephenW 于 2013-11-26 15:54 编辑

Some gossip:

A few days ago, a member (under Viread treatment) of the American Hepatitis B forum wrote:

"My liver doctor is Dr. Ira Jacobson of New York. I saw him last month, and
he said that with some immune system boosters that are in the pipeline,
that he thinks he can totally cure me within 2 or 3 years"

Dr Ira Jacobson is a well known liver specialists. We don't know what the "immune boosters" are, we can speculate ?:
1. ARC520
2. GS9620
3. GS4774

We are all hopeful.

一些八卦:

前几天,一个美国乙肝论坛的成员(Viread药物治疗下)写:

“我的肝脏医生是纽约的艾拉·雅各布森博士,上个月我看见他.
他说,一些免疫系统的助推器是在发展管道,
他认为,他完全可以在2年或3年治好我的病“

艾拉·雅各布森博士是一个众所周知的肝脏专家。我们不知道是什么“免疫助推器”,可以推测:
1。 ARC520
2。 GS9620
3。 GS4774

   我们都充满期望.


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发表于 2013-11-26 16:20 |只看该作者
好消息,
祝福他们早日取得好成绩,祝福我们自己早日得以治愈。

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发表于 2013-11-26 20:09 |只看该作者
的确是好消息。没想到这么快,香港的效率就是高啊,感谢不列颠。
日行一善(百善孝为先)

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发表于 2013-11-26 20:49 |只看该作者
感觉比rep靠谱,但愿进展顺利
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