A Randomised, Placebo Controlled, Double Blind, Multicentre Proof of Concept Study to Assess the Safety and Efficacy of Two Doses of VAD044 in Patients With Hereditary Hemorrhagic Telangiectasia (HHT)

The purpose of this Phase 1b proof of concept study, randomised, placebo controlled, double blind, multicentre study is to asssess safety and efficacy of 2 doses of VAD044 in adult HHT patients

开始日期2022-07-18

申办/合作机构

Vaderis Therapeutics AG

NL-OMON53637 / RecruitingN/A

A randomised, placebo controlled, double blind, multicentre proof of concept study to assess the safety and efficacy of two doses of VAD044 in patients with hereditary haemorrhagic telangiectasia (HHT) - VAD044C002

开始日期2022-01-18

申办/合作机构

Vaderis Therapeutics AG

100 项与 VAD044 相关的临床结果

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100 项与 VAD044 相关的转化医学

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100 项与 VAD044 相关的专利（医药）

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项与 VAD044 相关的文献（医药）

2023-08-15·Bioorganic & medicinal chemistry letters

Discovery of benzodiazepine derivatives as a new class of covalent inhibitors of SARS-CoV-2 main protease.

Article

作者: Wu, Yunjie ; Zhao, Xiu ; Li, Yueshan ; Wang, Falu ; Qiao, Jingxin ; Liu, Yuanzhi ; Zeng, Rui ; Lei, Jian ; Yang, Shengyong ; Li, Feng ; Xia, Anjie

The COVID-19 pandemic has caused people immense suffering all over the world. Although the World Health Organization (WHO) has announced the end of the pandemic, the sporadic virus epidemic is still ongoing and may exist permanently. Effective antivirals against SARS-CoV-2 are important to deal with the long-term threat. The main protease (M^pro) is a crucial target for drug development due to its role in the process of virus's replication and transcription. Herein, we report benzodiazepine derivatives as a new class of M^pro inhibitors. Structure-activity relationship (SAR) studies led to the discovery of the most active compound, methyl 10-(2-chloroacetyl)-1-oxo-11-(4-(trifluoromethyl)phenyl)-2,3,4,5,10,11-hexahydro-1H-dibenzo[b,e][1,4]-diazepine-7-carboxylate (11a), which shows an IC₅₀ value of 0.180 ± 0.004 μM. The X-ray crystal structure shows that 11a covalently binds to M^pro. Collectively, we have obtained a new small molecule inhibitor targeting M^pro, which can serve as a lead compound for subsequent drug discovery against SARS-CoV-2.

2014-10-15·Journal of agricultural and food chemistry1区 · 农林科学

Design, Synthesis, and Antiviral, Fungicidal, and Insecticidal Activities of Tetrahydro-β-carboline-3-carbohydrazide Derivatives

1区 · 农林科学

Article

作者: Shang, Hui ; Liu, Yuxiu ; Yang, Peiwen ; Liu, Yongxian ; Li, Yongqiang ; Song, Hongjian ; Huang, Yuanqiong ; Wang, Qingmin ; Xiao, Zhixin ; Li, Jiarui ; Song, Yuchuan ; Zhao, Sheng

According to our previous research on the antiviral activity of β-carboline and tetrahydro-β-carboline derivatives, using (1S,3S)-1-methyl-2,3,4,9-tetrahydro-1H-pyrido[3,4-b]indole-3-carbohydrazide (1) as a lead compound, series of novel tetrahydro-β-carboline derivatives containing acylhydrazone moiety were designed, synthesized, and first evaluated for their biological activities. Most of these compounds exhibited excellent antiviral activity both in vitro and in vivo. The in vivo inactivation, curative, and protection activities of compounds 8, 9, 12, 16, 28, 29, and 30 were much higher than that of ribavirin (37.6%, 39.4%, and 37.9% at 500 μg/mL) and the lead compound (40.0%, 42.3%, and 39.6% at 500 μg/mL). Especially, the in vitro and in vivo activities of compound 16 (36.9%, 33.6%, 30.2%, and 35.8%) at 100 μg/mL, which were very close to that of ribavirin (40.0% for in vitro activity) at 500 μg/mL. Compounds 9 and 29 were chosen for the field trials of antiviral efficacy against TMV (tobacco mosaic virus); the results exhibited that both compounds, especially compound 29, showed better activities than control plant virus inhibitors. At the same time, the fungicidal results showed that compounds 6, 9, and 11 exhibited good fungicidal activities against 14 kinds of phytopathogens. Additionally, compounds 3 and 23 exhibited moderate insecticidal activity against the four tested species of insects.

2010-06-01·The Journal of pharmacology and experimental therapeutics3区 · 医学

Inhibition of IκB Kinase-β Protects Dopamine Neurons Against Lipopolysaccharide-Induced Neurotoxicity

3区 · 医学

Article

作者: Shi, Jing-Shan ; Zhang, Feng ; Flood, Patrick M. ; Qian, Li ; Hong, Jau-Shyong ; Gao, Hui-Ming

Parkinson's disease (PD) is a progressive neurological disorder characterized by a selective loss of dopamine (DA) neurons in the substantia nigra (SN). Although current therapy can control symptoms of this disorder, there is no effective therapy available to halt its progression. Recently, neuroinflammation has been recognized as an important contributor to the pathogenesis of PD, and nuclear factor-kappaB (NF-kappaB) plays a key role in regulating neuroinflammation. Hence, the modulation of NF-kappaB pathway may have therapeutic potential for PD. Activation of NF-kappaB depends on the phosphorylation of its inhibitor, IkappaB, by the specific IkappaB kinase (IKK) subunit IKK-beta. Compound A (7-[2-(cyclopropylmethoxy)-6-hydroxyphenyl]-5-[(3S)-3-piperidinyl]-1, 4-dihydro-2H-pyrido[2,3-d][1,3]oxazin-2-one hydrochloride), a potent and selective inhibitor of IKK-beta, has recently been reported to provide cardioprotection through specific suppression of NF-kappaB signaling. The present study, for the first time, elucidates neuroprotective effects of compound A. Daily subcutaneous injection of compound A (1 mg/kg) for 7 days inhibited the activation of microglia induced by nigral stereotaxic injection of lipopolysaccharide (LPS) and significantly attenuated LPS-induced loss of DA neurons in the SN. In vitro mechanistic studies revealed that neuroprotective effects of compound A were mediated by 1) suppressing the activity of microglial NADPH oxidase and decreasing the production of reactive oxygen species, and 2) inhibiting NF-kappaB-mediated gene transcription of various proinflammatory mediators in microglia via IKK-beta suppression. These findings indicate that compound A afforded potent neuroprotection against LPS-induced neurodegeneration through selective inhibition of NF-kappaB activation and may be of potential benefit in the treatment of PD.

项与 VAD044 相关的新闻（医药）

2024-08-27

·药明康德

突破性小分子疗法获FDA优先审评资格；别构AKT抑制剂获得临床概念验证……

▎药明康德内容团队编辑小分子疗法获FDA优先审评资格 Soleno Therapeutics今天宣布，美国FDA已接受为其在研疗法DCCR缓释片递交的新药申请（NDA），用于治疗4岁及以上经基因检测确认的Prader-Willi综合征（PWS）患者的暴食症。FDA同时授予这一申请优先审评资格，预计在今年年底之前完成审评。DCCR是一款二氮嗪胆碱（diazoxide choline）缓释片剂，已经获得美国FDA授予的突破性疗法认定和快速通道资格，并在美国和欧盟获得孤儿药资格。 DCCR是一种含有二氮嗪胆碱的创新专有缓释剂型，每日口服一次。DCCR开发项目的数据支持来自五项在健康志愿者中完成的1期临床研究和3项完成的2期临床研究，其中一项是在PWS患者中进行的。在PWS的3期临床开发项目中，DCCR在解决PWS的标志性症状暴食症以及其他几种症状（如攻击性/破坏性行为、脂肪质量和其他代谢参数）方面显示出可喜的效果。别构AKT抑制剂概念验证临床试验获积极结果 Vaderis Therapeutics公司今日宣布，在研别构AKT抑制剂VAD044在治疗遗传性出血性毛细血管扩张症（Hereditary Haemorrhagic Telangiectasia，HHT）患者的随机双盲、安慰剂对照概念验证（POC）临床试验中取得了积极结果。 HHT是世界上第二常见的遗传性出血性疾病，常常导致严重的疾病负担、降低预期寿命和生活质量。尽管如此，目前全球范围内尚无获批的HHT治疗方法。Vaderis正在开发VAD044，这是一种口服、每日一次的别构AKT抑制剂。在这项双盲对照试验中，75名来自美国和欧洲的患者被随机分配接受安慰剂、30 mg或40 mg的VAD044治疗，为期12周。安全性是主要终点，VAD044在脱靶不良事件（AEs）的发生频率和严重程度上与安慰剂相似。与AKT通路抑制相关的不良事件大多为轻度、短暂并可在研究期间解决。几乎所有HHT患者都遭受不可预测、频繁且使人衰弱的鼻出血，这被认为是衡量整体HHT疾病活动和疾病负担的关键指标。在本研究中，VAD044在HHT的次要和探索性疗效终点上表现出剂量依赖性应答，包括关键的鼻出血终点。在12周治疗期结束时，接受40 mg剂量的患者在鼻出血频率、持续时间和无鼻出血天数方面均有临床意义的改善。为癌症患者发现靶向治疗选择，FDA批准Illumina癌症生物标志物检测 Illumina公司今天宣布，其体外诊断（IVD）产品TruSight Oncology（TSO）Comprehensive检测获得美国FDA的批准，并获得了首批两项伴随诊断（CDx）适应症的批准。该检测可分析超过500个基因，以对患者的实体瘤进行全面分析，从而提高识别免疫肿瘤学生物标志物或临床可操作性生物标志物的可能性，这些标志物可以用于指导靶向治疗的选择或帮助临床试验患者入组。 TSO Comprehensive已获FDA批准作为伴随诊断工具，识别携带神经营养性酪氨酸受体激酶（NTRK）基因融合的成人和儿童实体瘤患者，这些患者可能从拜耳公司的Vitrakvi（larotrectinib）治疗中受益。该检测还获批用于识别RET融合阳性的局部晚期或转移性非小细胞肺癌（NSCLC）成人患者，这些患者可能从礼来公司的Retevmo（selpercatinib）治疗中受益。新闻稿指出，大多数CDx测试通常仅针对一种类型的癌症，而TSO Comprehensive获得批准用于NTRK伴随诊断的所有实体瘤适应症，这有助于最大化每位患者活检中找到可针对信息的可能性。 ▲欲了解更多前沿技术在生物医药产业中的应用，请长按扫描上方二维码，即可访问“药明直播间”，观看相关话题的直播讨论与精彩回放参考资料： [1] Soleno Therapeutics Announces U.S. FDA Acceptance for Filing and Priority Review of NDA for DCCR (Diazoxide Choline) Extended-Release Tablets in Prader-Willi Syndrome. Retrieved August 27, 2024, from https://www.globenewswire.com/news-release/2024/08/27/2936152/0/en/Soleno-Therapeutics-Announces-U-S-FDA-Acceptance-for-Filing-and-Priority-Review-of-NDA-for-DCCR-Diazoxide-Choline-Extended-Release-Tablets-in-Prader-Willi-Syndrome.html [2] Vaderis Announces Positive Clinical Proof-of-Concept Trial in HHT. Retrieved August 27, 2024, from https://www.prnewswire.com/news-releases/vaderis-announces-positive-clinical-proof-of-concept-trial-in-hht-302230320.html [3] FDA approves Illumina cancer biomarker test with two companion diagnostics to rapidly match patients to targeted therapies. Retrieved August 27, 2024, fromhttps://www.prnewswire.com/news-releases/fda-approves-illumina-cancer-biomarker-test-with-two-companion-diagnostics-to-rapidly-match-patients-to-targeted-therapies-302230979.html 免责声明：药明康德内容团队专注介绍全球生物医药健康研究进展。本文仅作信息交流之目的，文中观点不代表药明康德立场，亦不代表药明康德支持或反对文中观点。本文也不是治疗方案推荐。如需获得治疗方案指导，请前往正规医院就诊。版权说明：本文来自药明康德内容团队，欢迎个人转发至朋友圈，谢绝媒体或机构未经授权以任何形式转载至其他平台。转载授权请在「药明康德」微信公众号回复“转载”，获取转载须知。分享，点赞，在看，聚焦全球生物医药健康创新

优先审批临床2期孤儿药突破性疗法快速通道

2024-08-27

·FierceBiotech

Vaderis scores win against rare blood vessel disorder as trial shows its drug reduces nosebleeds

Hereditary hemorrhagic telangiectasia is the second most common inherited bleeding disorder in the world and has been linked to severe disease burden, reduced life expectancy and a reduced quality of life. Vaderis Therapeutics’ goal to develop the first drug aimed specifically at a certain rare blood vessel disorder came one step closer today with the news that the therapy is safe and reduced nosebleeds.The therapy in question, a once-daily allosteric AKT inhibitor dubbed VAD044, was trialed in 75 patients with hereditary hemorrhagic telangiectasia (HHT), a genetic disorder that leads to abnormal blood vessels forming in the skin, mucous membranes and certain organs.Almost all HHT patients suffer from unpredictable and often debilitating nosebleeds. After 12 weeks, patients who received the 40-mg dose of VAD044 experienced “clinically meaningful” reductions in the frequency of their nosebleeds, a secondary endpoint of the trial, Vaderis said in an Aug. 27 release.The release was light on any actual data, but the Swiss company did say that regression of HHT-associated vascular lesions was also observed.Patients in the phase 1 trial either received the 40-mg dose, a 30-mg dose or placebo. The primary endpoint of the study was safety, and the data showed that VAD044 was similar to placebo when it came to the frequency and severity of off-target adverse events (AEs). On-target AEs associated with inhibiting the AKT pathway—which helps cells survive and grow in response to extracellular signals—were mostly mild, transient and resolved, the company said.Some of the patients have since been enrolled in a 12-month open-label extension, where they are receiving a 40-mg daily dose of VAD044. Interim six-month data from 27 of these patients “continue to show favorable safety and tolerability profiles with further improvements” in nosebleeds, Vaderis said.CEO Nicholas Benedict said the company is already “interacting with major health authorities to plan the pivotal phase of development for VAD044 in HHT.”“The excitement surrounding the results of the initial 12-week double-blind part of this trial is amplified by the continued improvements experienced by patients through six months,” Benedict added. HHT is the second most common inherited bleeding disorder in the world and has been linked to severe disease burden, reduced life expectancy and a reduced quality of life. Despite this health impact, there are no approved treatments for the condition, according to Vaderis, which described VAD044 as “the first novel therapy intended specifically for the treatment of HHT.”The company is also lining up the therapy to test in breast and prostate cancers, according to Vaderis’ website.“We … already see that after six months of continuous treatment with VAD044 patients experience further improvements in all [nose bleeding] endpoints compared to those seen at 12 weeks,” Hans-Jurgen Mager, M.D., Ph.D., head of the Netherlands Reference Centre for HHT and the study’s co-primary investigator, said in a statement.“It seems that VAD044 has not yet reached its peak effect on HHT disease activity at 12 weeks, and patients continue to improve over time without paying an unexpected price in terms of safety or tolerability,” Mager added.Academic centers in the U.S. are currently enrolling patients to test whether Novartis’ sarcoma drug Votrient can reduce the severity of nosebleeds in HHT. Votrient is a tyrosine kinase inhibitor that has been shown to inhibit the PI3K/Akt signaling pathway.Novartis has a more direct link to Vaderis, with the biotech having been set up in 2019 by two veterans of the Swiss Big Pharma, including Benedict himself.

临床结果临床1期

2024-08-27

·PRNewswire

Vaderis Announces Positive Clinical Proof-of-Concept Trial in HHT

Trial delivers positive results in first ever industry-led clinical trial in Hereditary Haemorrhagic Telangiectasia (HHT) VAD044 showed favourable safety and tolerability, together with exploratory efficacy across key manifestations of the disease Ongoing Open Label Extension (OLE) data at 6 months show consistent safety, tolerability and continued improvement in bleeding parameters BASEL, Switzerland, Aug. 27, 2024 /PRNewswire/ -- Vaderis Therapeutics AG (Vaderis), a clinical stage biotechnology company focused on developing treatments for rare diseases associated with vascular malformations, today announces positive results from its randomized, double-blind, dose-finding placebo-controlled Proof-of-Concept (POC) clinical trial in patients suffering from HHT. HHT, an Orphan Disease, is the second most common inherited bleeding disorder in the world frequently causing severe disease burden, reduced life expectancy and impaired Quality of Life. Despite this, there remains no approved treatment for HHT anywhere in the world. Vaderis is developing VAD044, an oral, once-daily allosteric AKT-inhibitor, the first novel therapy intended specifically for the treatment of HHT. In this controlled, double-blind trial, seventy-five patients across USA and Europe were randomized to receive either placebo, 30mg or 40mg of VAD044 for 12 weeks. Safety was the primary endpoint and VAD044 was similar to placebo as measured by both the frequency and severity of off-target adverse events (AEs). On-target AEs associated with AKT pathway inhibition, were mostly mild, transient and resolved on study drug. Almost all HHT patients suffer from unpredictable, often frequent and debilitating epistaxis which is considered the best measure of overall HHT disease activity and a key measure of disease burden. In this study, VAD044 showed a dose response on secondary and exploratory efficacy endpoints in HHT, including key epistaxis endpoints. At the end of the 12-week treatment period, patients receiving the 40mg dose experienced clinically meaningful improvements in epistaxis frequency, duration and epistaxis-free days. Regression of HHT-associated vascular lesions was also observed. Following the 12-week randomised double-blind period, patients from selected study centres were enrolled into a 12-month OLE to the study where they all receive up to 40mg VAD044 daily. Interim data for twenty-nine patients through the 6 month timepoint continue to show favourable safety and tolerability profiles with further improvements in epistaxis. Dr. Hanny Al-Samkari, the Peggy S. Blitz Endowed Chair in Hematology/Oncology at Massachusetts General Hospital and Associate Professor of Medicine at Harvard Medical School (USA), co-primary investigator in the VAD044 POC trial, commented, "In this pioneering clinical trial we see already at 12 weeks substantial and clinically meaningful dose-dependent improvements in HHT disease activity with once-daily VAD044, particularly as measured by epistaxis parameters." Dr. Hans-Jurgen Mager, pulmonologist and head of the Netherlands Reference Centre for HHT at St. Antonius Hospital, Utrecht (NL), also co-primary investigator in the VAD044 POC trial, added, "These exciting results have supported the assessment of long-term treatment of HHT patients with VAD044. We have added an open-label extension to the POC trial and already see that after 6 months of continuous treatment with VAD044 patients experience further improvements in all epistaxis endpoints compared to those seen at 12 weeks. It seems that VAD044 has not yet reached its peak effect on HHT disease activity at 12 weeks, and patients continue to improve over time without paying an unexpected price in terms of safety or tolerability." Nicholas Benedict, CEO and co-Founder of Vaderis Therapeutics, commented, "The excitement surrounding the results of the initial 12-week double-blind part of this trial is amplified by the continued improvements experienced by patients through 6 months. Excellent collaboration with patient and physician organisations such as CureHHT has been a cornerstone of successful implementation of this ground-breaking trial which was achieved in a much shorter timeframe than planned. Vaderis is currently interacting with major health authorities to plan the pivotal phase of development for VAD044 in HHT." About Vaderis Vaderis is a clinical stage biotech company developing treatments for rare and orphan diseases associated with vascular malformations. There is a significant number of debilitating and largely untreated rare diseases, such as HHT (Hereditary Haemorrhagic Telangiectasia), in which patients have overactivation of AKT triggered by upstream genetic mutations resulting in vascular overgrowth. Vaderis is developing VAD044, a daily, oral allosteric AKT inhibitor, which has been investigated in a clinical proof of concept study in HHT patients and is currently in a 12 month Open Label Extension. There are no drugs approved to treat HHT and Vaderis aims to be the first company to develop a medicine for the treatment of HHT and other diseases associated with vascular malformations. Logo: For further information, please contact:

临床结果孤儿药

100 项与 VAD044 相关的药物交易

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研发状态

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适应症	最高研发状态	国家/地区	公司	日期
遗传性出血性毛细血管扩张	临床1期	瑞士	Vaderis Therapeutics AG	2022-01-30
动静脉畸形	临床1期	-	Vaderis Therapeutics AG	-
淋巴管畸形	临床1期	-	Vaderis Therapeutics AG	-