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EASL 2020 –乙肝向前迈进,Assembly找到合作伙伴 [复制链接]

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发表于 2020-8-29 12:29 |只看该作者 |倒序浏览 |打印
EASL 2020 – Assembly finds a partner as hepatitis B inches forward

    Amy Brown

As fresh data confirms the promise of RNAi technology in hepatitis B, Assembly brings on Arbutus for its combo strategy.

Arbutus might seem a strange choice of partner for Assembly Biosciences, a company that is already struggling to keep up with bigger players in the hepatitis B space. A recent update on AB-729, the former’s RNAi-based hep B candidate, was poorly received; perhaps Assembly had little choice, with other RNAi projects already tied up in existing deals with big pharma.

The agreement between the two companies, announced yesterday, will see Assembly’s lead core inhibitor, ABI-H0731, tested in combination with AB-729 and a nucleotide reverse transcriptase inhibitor (NRTI); the latter are the standard of care in this disease. The news was timed to coincide with the EASL medical conference, where several updates from other RNAi contenders are due; these will show the standards for which Arbutus and Assembly need to strive.

Data emerging from Vir Biotechnology is of particular interest. VIR-2218 is an siRNA currently not earmarked for triple combination studies; with J&J working with Arrowhead, and Roche and Dicerna paired up, there was some speculation that Vir and Assembly could have struck a deal.

VIR-2218 appears to be efficiently knocking out HBsAg; also known as surface antigen, it is believed that this closely-watched biomarker needs to be suppressed for a functional cure to be achieved. An ongoing phase II trial of 24 patients found that those in a 50mg dose group achieved maximal reductions in HBsAg at week 12, with a mean reduction of 1.5 log10 from baseline.

A mean reduction of 1 log10 was maintained through Week 28 in this cohort, EASL will hear; this seems to be an encouraging update from a four-week cut of the data, released in April (Vir bids to enter the hepatitis B race, April 16, 2020).

EASL will also get a look at Johnson & Johnson’s RNAi contender, licensed from Arrowhead, from a trial conducted in combination with NRTI therapy. Across three doses of JNJ-3989, 22 of 40 patients had sustained HBsAg reductions of more than 1 log10  approximately nine months after the last dose, suggesting impressive durability.

Data from a triple combination study, which adds in a core inhibitor, are eagerly awaited in the wake of data in 12 patients presented at AASLD last year. The longer and larger Reef 1 trial was started last year.

Safety a focus

Elsewhere, early data from a novel antisense project also show what Arbutus and Assembly are up against. A Glaxosmithkline-Ionis presentation of GSK3228836 updates previous AASLD results with a few more patients – across 24 patients, six had HBsAg reductions of more than 3 log10.

Still, one patient in this trial suffered a liver enzyme elevation that was classified as a serious adverse event, although this self resolved. Safety will be closely scrutinised as the full details of all these projects emerge – liver enzyme elevations were seen from Arbutus in March, and this will remain a focus as the Assembly partnership progresses.

Glaxo is confident enough to push on: the company said today that a phase IIb programme will get under way before the end of the year, and it will be interesting to see what combinations it pushes forward.

Assembly and Arbutus, meanwhile, said a phase III triple combination trial will start next year in around 60 virologically suppressed patients. The need for speed in this competitive space is understandable but Assembly is still fighting concerns that its own core inhibitor is underwhelming. An AASLD presentation showed that very few subjects treated with ABI-H0731 managed to achieve a greater than 0.5 log decrease in HBsAg, and an EASL update does not promise to show much more.

Assembly has tried to argue that HBsAg is a less important measure for core inhibitors, and it is true that the project has managed to impressively quash other markers of infection, such as viral DNA and RNA. Mizuho analysts, who recommend buying Assembly shares, point out that making direct comparisons with other agents is not entirely fair due to different doses and combinations used, which is certainly true; at the four week mark ABI-H0731's HBsAg log reduction is in the same ballpark as seen with other projects over a similar timeframe, they argue.

Data due next year from Assembly, looking at what happens to patient's viral load after treatment is reduced, remains a critical milestone for the company (AASLD 2019 – Assembly asks investors to keep the faith, November 13, 2019).

But with both Assembly and Arbutus arguably trailing much bigger rivals in the highly competitive hepatitis B space, it remains to be seen whether this nascent partnership will improve either company's chances.

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发表于 2020-8-29 12:29 |只看该作者
EASL 2020 –乙肝向前迈进,大会找到合作伙伴

    艾米·布朗

由于新数据证实了RNAi技术在乙型肝炎中的应用前景,Assembly将Arbutus用于其组合策略。

Arbutus似乎是Assembly Biosciences合作伙伴的一个奇怪选择,该公司已经在努力跟上乙肝领域的更大参与者。前者基于RNAi的hep B候选物AB-729的最新更新收效甚微;也许Assembly别无选择,其他RNAi项目已经与大型制药公司达成了现有协议。

两家公司昨天宣布的协议将看到Assembly的主要核心抑制剂ABI-H0731与AB-729和核苷酸逆转录酶抑制剂(NRTI)结合测试;后者是这种疾病的护理标准。该消息的发布时间恰逢EASL医学会议,届时其他RNAi竞争者也将进行一些更新。这些将显示杨梅和大会需要努力的标准。

来自Vir Biotechnology的数据特别令人关注。 VIR-2218是目前尚未指定用于三重组合研究的siRNA;强生与Arrowhead合作,而Roche和Dicerna结成对,有人猜测Vir和Assembly可能达成协议。

VIR-2218似乎可以有效地清除HBsAg。也被称为表面抗原,据信需要密切关注这种生物标记才能实现功能性固化。一项正在进行的II期临床试验包括24位患者,发现50mg剂量组的患者在第12周达到HBsAg的最大降低,与基线相比平均降低1.5 log10。

EASL会听到,在这一队列中,直到第28周,平均减少了10 log10。这似乎是4月份发布的为期4周的数据削减的令人鼓舞的更新(Vir计划参加2020年4月16日的乙肝竞赛)。

EASL还将通过结合NRTI疗法进行的试验,了解由Arrowhead许可的强生公司的RNAi竞争者。在三剂JNJ-3989中,40例患者中有22例在最后一剂后约9个月,HBsAg持续降低超过1 log10以上,表明其持久的耐用性。

去年在AASLD上发表的12例患者的数据之后,迫切期待来自三联组合研究的数据,该研究增加了核心抑制剂。去年开始了更长更大型的Reef 1试验。

安全是重点

在其他地方,来自一个新颖的反义项目的早期数据也显示了杨梅和汇编面临的挑战。 Glaskosmithkline-Ionis演示的GSK3228836更新了以前的AASLD结果,增加了几例患者–在24例患者中,有6例HBsAg降低超过3 log10。

尽管如此,该试验中的一名患者尽管自我解决,但肝酶升高被分类为严重不良事件。随着所有这些项目的全部细节的出现,安全性将受到严格审查-3月从杨梅中观察到肝酶升高,随着大会伙伴关系的进展,这将仍然是重点。

葛兰素史克有足够的信心继续前进:该公司今天表示,IIb阶段计划将在今年年底之前开始实施,很高兴看到它将推进哪些组合。

Assembly和Arbutus同时表示,一项III期三联疗法试验将于明年在约60名被病毒抑制的患者中开始。在竞争激烈的空间中对速度的需求是可以理解的,但大会仍在与自己的核心阻碍力不足的担忧作斗争。 AASLD演示文稿显示,很少有接受ABI-H0731治疗的受试者的HBsAg下降幅度大于0.5 log,而EASL更新并不能显示更多。

大会试图证明HBsAg对核心抑制剂的作用不那么重要,这确实是该项目成功地消除了其他感染标志物,例如病毒DNA和RNA。建议购买Assembly股票的瑞穗分析师指出,由于使用了不同的剂量和组合,与其他代理商进行直接比较并不完全公平,这的确是事实。他们认为,在四个星期的时间里,ABI-H0731的HBsAg对数减少与其他项目在相同的时间范围内处于同一水平。

明年来自大会的数据,以观察减少治疗后患者病毒载量的变化,仍然是该公司的重要里程碑(AASLD 2019 –大会要求投资者保持信心,2019年11月13日)。

但是,尽管大会和Arbutus在竞争激烈的乙肝领域都落后于更大的竞争对手,这种新生的伙伴关系是否会增加两家公司的机会还有待观察。

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发表于 2020-8-29 12:54 |只看该作者
l,o731,降DNa和rna还可以,但与其他公司比较,在降hbsag方面较弱(降幅小于○:5个对数。2。市场人士说,hbsag对乙肝来说不重要,在为自己瓣解。3。说明业界不看好o731,这个药。解读完毕

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发表于 2020-8-29 13:20 |只看该作者
本帖最后由 newchinabok 于 2020-8-29 13:56 编辑

都在互相抱团取暖,不能治愈一个人,所以他们都在三期止步。不能治愈一部分人,任何药都别想上市,上市也没市场。除了核衣壳以外,核衣壳+核苷或者核衣壳单药不优于核苷,也不会上市。

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发表于 2020-8-29 18:12 |只看该作者
哎,还不如用工业化大规模的乙肝抗体,每日注射,强力压制表面抗原,看看,长期压制表面对改善机一体功能是不是有效

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发表于 2020-8-29 23:51 |只看该作者
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