A Trial in Participants With Chronic Obstructive Pulmonary Disease (COPD) to Evaluate the Impact of Vapendavir on the Development of Lower Respiratory Tract Symptoms Following Rhinovirus Challenge

Vapendavir (VPV) is a drug being developed to treat human rhinovirus (RV) infection, one virus responsible for the common cold. Vapendavir prevents the virus from entering cells and making more infectious copies of itself. A study is being planned to investigate VPV in patients with chronic obstructive pulmonary disease (COPD, a lung disease making it difficult to breathe) who develop a rhinoviral infection; however, VPV has not been approved for use in treating any indication (disease) by the FDA or any other global regulatory agency. Therefore, VPV is considered investigational, and the study doctor is conducting this investigational research study. Safety will be monitored throughout the entire study.

开始日期2023-11-20

申办/合作机构

Altesa BioSciences, Inc.

[+1]

NCT05962645 / Completed临床1期

A Phase 1 Study to Confirm the Single- and Multiple-dose Pharmacokinetics and to Evaluate Food Effect of Vapendavir in Healthy Participants and Participants With COPD

Vapendavir (VPV) is potent virostatic antiviral agent active against all known enterovirus species. VPV binds to the viral capsid, thereby inhibiting viral attachment to the target cell and, independently, preventing release of viral RNA (ribonucleic acid) into the cell. Alt VPV-101 is meant to investigate vapendavir in patients with chronic obstructive pulmonary disease (COPD) who develop a rhinoviral infection. This is a Phase 1, open-label, unblinded study. The primary objective of this study is to characterize single and multiple dose (plus a loading dose) plasma PK profiles of VPV in healthy participants (Group A) and participants with COPD (Group B). Group A is an open-label, 2-sequence, and up to a 3-period, cross-over study to assess the single-dose PK parameters and safety of VPV. Healthy participants may opt to participate in only the first 2 periods, all 3 periods or BID dosing, but it is preferred that participants complete all 3 periods. Group B is an open-label, multi-dose investigation of VPV PK parameters and safety in participants with COPD. Post-dose, follow up will continue for a minimum of 14 days and a maximum of 30 days, depending on which Group the participant is in and which periods said participant completes. There is a target for up to 24 adult participants comprised of healthy participants and participants with COPD.

开始日期2023-05-19

申办/合作机构

Altesa BioSciences, Inc.

NCT02877264 / Completed临床1期

A Randomized, Single-Center, Open-Label, Three-Period, Six-Sequence, Crossover, Comparative Study to Compare the Oral Bioavailability of Single Doses of Three Vapendavir Drug Product Formulations in Healthy Volunteers

This is a randomized, single-center, open-label, three-period, six-sequence, crossover, comparative study to evaluate the oral bioavailability of single doses of three vapendavir drug product formulations (the 264 mg free base tablet [test drug], 264 mg free base oral suspension [test drug], and two 132 mg phosphate salt capsules [reference drug]) in healthy volunteers. The study design consists of six dosing sequences. Each sequence comprises 3 periods and each subject is administered one of the three dosing formulations in the first period. A subject receives a different formulation in each of the subsequent periods, so that all subjects receive each formulation. The periods are separated by an approximate 7-day washout.

开始日期2016-06-01

申办/合作机构

Aviragen Therapeutics

100 项与 Vapendavir 相关的临床结果

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100 项与 Vapendavir 相关的转化医学

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100 项与 Vapendavir 相关的专利（医药）

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项与 Vapendavir 相关的文献（医药）

2024-10-01·European Journal of Medicinal Chemistry

New potent EV-A71 antivirals targeting capsid

Article

作者: Vanelle, Patrice ; Silvestri, Romano ; Majdi, Chaimae ; Roux, Hugo ; Touret, Franck ; Di Giorgio, Carole ; Sciò, Pietro ; Khoumeri, Omar ; Roche, Manon ; Coluccia, Antonio

The enterovirus is a genus of single-stranded, highly diverse positive-sense RNA viruses, including Human Enterovirus A-D and Human Rhinovirus A-C species. They are responsible for numerous diseases and some infections can progress to life-threatening complications, particularly in children or immunocompromised patients. To date, there is no treatment against enteroviruses on the market, except for polioviruses (vaccine) and EV-A71 (vaccine in China). Following a decrease in enterovirus infections during and shortly after the (SARS-Cov2) lockdown, enterovirus outbreaks were once again detected, notably in young children. This reemergence highlights on the need to develop broad-spectrum treatment against enteroviruses. Over the last year, our research team has identified a new class of small-molecule inhibitors showing anti-EV activity. Targeting the well-known hydrophobic pocket in the viral capsid, these compounds show micromolar activity against EV-A71 and a high selectivity index (SI) (5h: EC_{50, MRC-5} = 0.57 μM, CC_{50, MRC-5} >20 μM, SI > 35; EC_{50, RD} = 4.38 μM, CC_{50, RD} > 40 μM, SI > 9; 6c: EC_{50, MRC-5} = 0.29 μM, CC_{50, MRC-5} >20 μM, SI > 69; EC_{50, RD} = 1.66 μM, CC_{50, RD} > 40 μM, SI > 24; Reference: Vapendavir EC_{50, MRC-5} = 0.36 μM, CC_{50, MRC-5} > 20 μM, EC_{50, RD} = 0.53 μM, CC_{50, RD} > 40 μM, SI > 63). The binding mode of these compounds in complex with enterovirus capsids was analyzed and showed a series of conserved interactions. Consequently, 6c and its derivatives are promising candidates for the treatment of enterovirus infections.

2019-09-17·Proceedings of the National Academy of Sciences1区 · 综合性期刊

Cryo-EM structure of pleconaril-resistant rhinovirus-B5 complexed to the antiviral OBR-5-340 reveals unexpected binding site

1区 · 综合性期刊

Article

作者: Kirchmair, Johannes ; Goessweiner-Mohr, Nikolaus ; Zanella, Irene ; Pasin, Marion ; Mathai, Neann ; Blaas, Dieter ; Walther, Christin ; Richter, Martina ; Marlovits, Thomas C. ; Real-Hohn, Antonio ; Wald, Jiri ; Schmidtke, Michaela ; Makarov, Vadim A. ; Verdaguer, Nuria

Viral inhibitors, such as pleconaril and vapendavir, target conserved regions in the capsids of rhinoviruses (RVs) and enteroviruses (EVs) by binding to a hydrophobic pocket in viral capsid protein 1 (VP1). In resistant RVs and EVs, bulky residues in this pocket prevent their binding. However, recently developed pyrazolopyrimidines inhibit pleconaril-resistant RVs and EVs, and computational modeling has suggested that they also bind to the hydrophobic pocket in VP1. We studied the mechanism of inhibition of pleconaril-resistant RVs using RV-B5 (1 of the 7 naturally pleconaril-resistant rhinoviruses) and OBR-5-340, a bioavailable pyrazolopyrimidine with proven in vivo activity, and determined the 3D-structure of the protein-ligand complex to 3.6 Å with cryoelectron microscopy. Our data indicate that, similar to other capsid binders, OBR-5-340 induces thermostability and inhibits viral adsorption and uncoating. However, we found that OBR-5-340 attaches closer to the entrance of the pocket than most other capsid binders, whose viral complexes have been studied so far, showing only marginal overlaps of the attachment sites. Comparing the experimentally determined 3D structure with the control, RV-B5 incubated with solvent only and determined to 3.2 Å, revealed no gross conformational changes upon OBR-5-340 binding. The pocket of the naturally OBR-5-340-resistant RV-A89 likewise incubated with OBR-5-340 and solved to 2.9 Å was empty. Pyrazolopyrimidines have a rigid molecular scaffold and may thus be less affected by a loss of entropy upon binding. They interact with less-conserved regions than known capsid binders. Overall, pyrazolopyrimidines could be more suitable for the development of new, broadly active inhibitors.

2015-12-01·Antimicrobial Agents and Chemotherapy2区 · 医学

Antiviral Activity of Broad-Spectrum and Enterovirus-Specific Inhibitors against Clinical Isolates of Enterovirus D68

2区 · 医学

Article

作者: Leyssen, Pieter ; van Kuppeveld, Frank J. M. ; George, Shyla ; Vernachio, John ; Froeyen, Mathy ; Thibaut, Hendrik Jan ; Baggen, Jim ; Hilgenfeld, Rolf ; Zhang, Linlin ; Delang, Leen ; Neyts, Johan ; Meijer, Adam ; Sun, Liang

ABSTRACTWe investigated the susceptibility of 10 enterovirus D68 (EV-D68) isolates (belonging to clusters A, B, and C) to (entero)virus inhibitors with different mechanisms of action. The 3C-protease inhibitors proved to be more efficient than enviroxime and pleconaril, which in turn were more effective than vapendavir and pirodavir. Favipiravir proved to be a weak inhibitor. Resistance to pleconaril maps to V69A in the VP1 protein, and resistance to rupintrivir maps to V104I in the 3C protease. A structural explanation of why both substitutions may cause resistance is provided.

项与 Vapendavir 相关的新闻（医药）

2022-05-27

·BioSpace

Altesa BioSciences to Initiate Clinical Trials of Promising Antiviral

ATLANTA--(BUSINESS WIRE)-- Altesa BioSciences, Inc. (Altesa), a clinical-stage biopharmaceutical company developing and commercializing novel antiviral drugs against common respiratory viruses and global viral threats, has U.S. Food & Drug Administration approval to proceed with a clinical study of a promising antiviral treatment, vapendavir. Accordingly, Altesa will initiate this trial and a series of others later this year and early next year, respectively. Brett P. Giroir, MD, Altesa Chief Executive Officer and former United States Assistant Secretary for Health, announced the news today at the 2022 AdvanSE Life Science Conference in Atlanta. “The green light from the FDA in response to our investigational new drug application (IND) is a significant step forward as we continue the clinical development of vapendavir, a Phase 2 oral antiviral drug,” Dr. Giroir said. “We believe vapendavir is well poised to mitigate the serious consequences resulting from viral respiratory infections in vulnerable populations. We are committed to evaluating its safety and effectiveness for patients in need.” The broad spectrum viral capsid inhibitor, vapendavir, is Altesa’s lead clinical stage antiviral drug, which was in-licensed in 2021. Based on prior evaluations in nearly 700 trial participants and patients, vapendavir was well tolerated and showed clear evidence of an antiviral response. Andrea True Kelly, PhD, Altesa’s Vice President of Clinical Development and Medical Affairs (formerly with Trimeris and Istari), said Altesa will initiate a clinical study this year to evaluate a new formulation of vapendavir. The study will be rapidly followed by Phase 2b clinical trials in 2023 to treat viral infections in vulnerable patients living with chronic obstructive pulmonary disease (COPD). “Our goal at Altesa is to provide simple, safe, and effective treatments, especially for those at greatest risk from the most common viral respiratory infections,” Dr. Kelly said. “We look forward to finalizing our development partners and initiating trials for this promising therapy in the coming months.” Over 16 million Americans suffer from COPD, the 4th leading cause of mortality in the U.S., which is anticipated to account for over $800 billion in direct medical expenditures from 2019 through 2038. Rhinoviruses, typically responsible for the common cold, are one of the viruses most commonly associated with serious disease exacerbation in patients suffering from COPD. In healthy individuals, rhinoviruses generally cause self-limiting upper respiratory tract infections, but in people with COPD, infection is readily associated with persistent lung inflammation, airflow obstruction and frequently with secondary bacterial infections, all of which can be life-threatening. By targeting rhinovirus, vapendavir holds great promise to reduce the severity of – or possibly prevent – excacerbations in infected patients with COPD. About Altesa Altesa BioSciences, Inc., is a biopharmaceutical company based in Atlanta, GA focused on developing antivirals to addresses diseases of global importance. Altesa has a preferred partnership with Emory DRIVE, a wholly-owned, not-for-profit drug discovery entity within Emory University. That collaboration includes a license to ALT-2023, a broadly active nucleoside analogue that is IND-enabled, as well as options to additional compounds targeting RNA viruses. In 2021, Altesa in-licensed vapendavir, a Phase 2 antiviral, broadly active against enteroviruses, including rhinovirus, from Vaxart. Altesa intends to progress vapendavir into a Phase 2b trial in the coming months for treatment of rhinoviral infection in vulnerable people suffering from chronic obstructive pulmonary disease (COPD).www.altesabio.com

小分子药物引进/卖出合作

100 项与 Vapendavir 相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
-	-	-	DB05181

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
呼吸道感染	临床3期	-	Vaxart, Inc.	2017-01-18
慢性呼吸道疾病	临床2期	英国	Altesa BioSciences, Inc.	2023-11-20
并发症	临床2期	英国	Altesa BioSciences, Inc.	2023-11-20
气肿	临床2期	英国	Altesa BioSciences, Inc.	2023-11-20
肠道病毒感染	临床2期	英国	Altesa BioSciences, Inc.	2023-11-20
慢性阻塞性肺疾病	临床2期	英国	Altesa BioSciences, Inc.	2023-11-20
呼吸障碍	临床2期	英国	Altesa BioSciences, Inc.	2023-11-20
哮喘	药物发现	美国	Biota Scientific Management Pty Ltd.	2010-08-01
鼻病毒感染	药物发现	美国	Biota Scientific Management Pty Ltd.	2010-08-01
鼻病毒感染	药物发现	美国	Biota Scientific Management Pty Ltd.	2010-08-01

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临床结果

适应症

分期

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT01175226 (RHINO, CTgov)	临床2期	鼻病毒感染 \| 哮喘	300	BTA798 (BTA798)	憲顧糧觸鑰夢觸鹽廠繭(蓋網壓窪膚鹽淵鏇夢膚) = 積鏇鹽淵壓積淵鹹膚鹽餘餘獵願夢觸齋鹹鑰觸 (範觸淵構構鏇蓋獵選製, 艱鹽範遞淵鏇淵選鬱顧 ~ 夢鬱構糧衊築齋顧觸齋) 更多	-	2017-06-01
				Placebo (Placebo)	憲顧糧觸鑰夢觸鹽廠繭(蓋網壓窪膚鹽淵鏇夢膚) = 網鹽繭餘艱顧鏇窪鏇齋餘餘獵願夢觸齋鹹鑰觸 (範觸淵構構鏇蓋獵選製, 餘襯鹹艱築繭鑰築憲淵 ~ 醖願範選齋鹽淵糧蓋遞) 更多