A Phase 2, Multi-center, Randomized, Double-blind, Placebo-controlled Study to Assess the Safety and Efficacy of Topically-applied AG013 for the Attenuation of Oral Mucositis in Subjects With Cancers of the Head and Neck Receiving Concomitant Chemoradiation Therapy

The purpose of the study is to evaluate the efficacy, safety and tolerability of topically administered AG013 compared to placebo for reducing Oral Mucositis (OM) in patients undergoing chemoradiation for the treatment of head and neck cancer, as measured by the duration, time to development, and overall incidence of OM during the active treatment phase, beginning from the start of chemoradiation therapy (CRT) until 2 weeks following its completion.
The effect of AG013 on patient-reported symptoms and analgesic use during the active treatment phase, and on the cumulative radiation dose administered before the onset of OM will also be evaluated, as will biomarkers and, in a subset of subjects, the PK (pharmacokinetic) profile of AG013.

开始日期2017-07-18

申办/合作机构

Oragenics, Inc.

NCT00938080 / Completed临床1期

A Phase 1b, Multi-center, Single Blinded, Placebo-controlled, Sequential Dose Escalation Study to Assess the Safety and Tolerability of Topically Applied AG013 in Subjects Receiving Induction Chemotherapy for the Treatment of Cancers of the Head and Neck

The purpose of this study is to assess the safety and tolerability of AG013 (genetically modified L. lactis bacteria engineered to secrete human Trefoil Factor 1), and to explore the ability of AG013 to attenuate the course and severity of oral mucositis (OM) in subjects receiving induction chemotherapy for the treatment of head and neck cancer.

开始日期2009-09-01

申办/合作机构

Intrexon ActoBiotics NV

100 项与 Dapatifagene navolactibac 相关的临床结果

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100 项与 Dapatifagene navolactibac 相关的转化医学

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100 项与 Dapatifagene navolactibac 相关的专利（医药）

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项与 Dapatifagene navolactibac 相关的文献（医药）

2020-03-23·Angewandte Chemie (International ed. in English)1区 · 化学

Formation of an Alkynyl‐Protected Ag₁₁₂ Silver Nanocluster as Promoted by Chloride Released In Situ from CH₂Cl₂

1区 · 化学

Article

作者: Wang, Quan‐Ming ; Guan, Zong‐Jie ; Hu, Feng ; Li, Jiao‐Jiao ; Yuan, Shang‐Fu

Abstract:

By directly reducing alkynyl–silver precursors, we successfully obtained a large alkynyl‐protected silver nanocluster, (C7H17ClN)3[Ag112Cl6(C≡CAr)51], which is hitherto the largest structurally characterized silver nanocluster in the alkynyl family. The cluster exhibits four concentric core–shell structures (Ag13@Ag42@Ag48@Ag9), and four types of alkynyl–silver binding modes are observed. Chloride was found to be critical for the stabilization and formation of the silver nanocluster. The release of chloride ions in situ from CH2Cl2 solvent has been confirmed by mass spectrometry. This study suggests that the combination of alkynyl and halide ligands will pave a new way for the synthesis of large silver nanoclusters.

2013-12-15·Cancer1区 · 医学

Phase 1b, multicenter, single blinded, placebo‐controlled, sequential dose escalation study to assess the safety and tolerability of topically applied AG013 in subjects with locally advanced head and neck cancer receiving induction chemotherapy

1区 · 医学

Article

作者: Brennan, Michael T. ; Cilli, Fiona ; Sonis, Stephen T. ; Murphy, Barbara A. ; Colevas, A. Dimitrios ; Limaye, Sewanti Atul ; Hu, Kenneth S. ; Haddad, Robert I.

BACKGROUND:

Oral mucositis (OM) is a significant toxicity of induction chemotherapy for locally advanced head and neck cancer (LAHNC). The safety and tolerability of AG013, an oral rinse containing recombinant Lactococcus lactis secreting mucosal protectant human trefoil factor 1 (hTFF1), was evaluated in a phase 1b study in LAHNC subjects who received induction with cisplatin, 5‐fluorouracil, with or without docetaxel. Preliminary efficacy data were also obtained.

METHODS:

A total of 25 of 52 LAHNC subjects who were followed during induction cycle 1 developed ulcerative oral mucositis (UOM; World Health Organization grade > 2) and were randomized to AG013:placebo (5:2 ratio) for cycle 2. Dosing schedules of 1, 3, or 6 times daily were evaluated (2 × 1011, 6 × 1011, and 1.2 × 1012 colony forming units per day, respectively). OM was evaluated daily from cycle 2, day 1 through 14, using World Health Organization criteria. Pharmacokinetic assessment was also conducted.

RESULTS:

AG013 bacteria were not detected in blood. Oral live AG013 bacterial and hTFF1 levels in saliva and oral mucosa were equivalent among treatment groups. The most frequently occurring adverse events were nausea, oral pain, fatigue, diarrhea, and mucosal inflammation. Only 12% (3 of 25 adverse events), mainly nausea, were attributed to the investigational medicinal product: AG013 or placebo. Efficacy analysis showed a 35% reduction in percentage of days with UOM in AG013‐subjects versus placebo. All placebo subjects experienced ≥ 2 days of UOM, whereas 29% of AG013 subjects had UOM for 0 or 1 day. AG013 use resulted in fewer unscheduled office and emergency room visits. No differences were noted in mouth and throat soreness, opioid use, or gastrostomy tube placement.

CONCLUSIONS:

2010-07-01·Oral oncology2区 · 医学

AG013, a mouth rinse formulation of Lactococcus lactis secreting human Trefoil Factor 1, provides a safe and efficacious therapeutic tool for treating oral mucositis

2区 · 医学

Article

作者: Silvia Caluwaerts ; Peter Vanhoenacker ; Bernard Coulie ; Brynmor Watkins ; Sabine Neirynck ; Sam Corveleyn ; Pieter Rottiers ; Klaas Vandenbroucke ; Stephen Sonis ; Lothar Steidler

Non-clinical studies, focusing on the pharmacodynamics (PD), pharmacokinetics (PK) and safety pharmacology of genetically modified Lactococcus lactis (L. lactis) bacteria, engineered to secrete human Trefoil Factor 1 (hTFF1), were performed to provide proof-of-concept for the treatment of oral mucositis (OM) patients. L. lactis strain sAGX0085 was constructed by stably inserting an htff1 expression cassette into the bacterial genome, and clinically formulated as a mouth rinse (coded AG013). PD studies, using different oral dosing regimens, were performed in a clinically relevant hamster model for radiation-induced OM. The PK profile was assessed in healthy hamsters and in hamsters with radiation-induced OM. In addition, in vitro and in vivo safety pharmacology studies were conducted, in pooled, complement-preserved human serum, and in neutropenic hamsters and rats respectively. Topical administration of L. lactis sAGX0085/AG013 to the oral mucosa significantly reduced the severity and course of radiation-induced OM. PK studies demonstrated that both living L. lactis bacteria, as well as the hTFF1 secreted, could be recovered from the administration site for maximum 24h post-dosing, without systemic exposure. The in vitro and in vivo safety pharmacology studies confirmed that L. lactis sAGX0085 could not survive in systemic circulation, not even under neutropenic conditions. The results from the PD, PK and safety pharmacology studies reported here indicate that in situ secretion of hTFF1 by topically administered L. lactis bacteria provides a safe and efficacious therapeutic tool for the prevention and treatment of OM.

项与 Dapatifagene navolactibac 相关的新闻（医药）

2023-01-25

·药智网

微生物组疗法破冰，是昙花一现还是未来可期？

2022 年，微生物组疗法终于破冰。 2022 年 12 月，FDA 批准由 Ferring Pharmaceuticals 与其旗下 Rebiotix 公司所开发的基于粪菌的活体生物药 Rebyota（RBX2660），该微生物组疗法旨在用于避免 18 岁以上艰难梭菌感染（CDI）病患在接受抗生素治疗后的感染复发。 Rebyota 是首款经 FDA 批准的粪便微生物组疗法，是微生物组疗法发展的重要里程碑。展望未来，微生物组疗法的成功是否只是昙花一现？还是会成为新药研发的下一个宝藏？笔者将从科学环境、临床研发、投资三大方面进行分析。 01微生物组疗法应用场景分析微生物与人类健康，这是一个宏大、远未被了解的生物学领域。微生物包括细菌、病毒、真菌以及一些小型的原生生物、显微藻类等在内的一大类生物群体。在我们的身体内，住着数以万亿计的微生物，他们寄生在皮肤、生殖器、口腔，特别是肠道部位。一些肠道疾病，例如炎症性肠病或者艰难梭菌感染，则会引起肠道中微生物的构成发生变化，进而引发微生物种群失调。近年来的研究已经表明，除了像炎症性肠病这类局部肠道疾病以外，微生物组疗法在呼吸系统、免疫、肿瘤、代谢、神经系统疾病等多种疾病的发生和进展中起到了至关重要的作用。图 1 微生物组疗法治疗领域图片来源：Microbiome Times 以微生物组与神经精神疾病为例，“肠-脑轴”是一个令人兴奋的生物学领域，肠道微生物群与阿尔茨海默病、帕金森病到包括自闭症、抑郁症、焦虑症在内的多种精神疾病的发病机制和疾病进展相关联。根据 Pistollato 等研究者分析，肠埃希菌属、沙门菌属、分枝杆菌属和枯草芽孢杆菌等可诱导神经系统产生淀粉样蛋白纤维，而且大肠埃希菌属的内毒素还可促进β-淀粉样蛋白的形成，进而诱导阿尔茨海默病的发生发展。图 2 肠道菌群紊乱诱导淀粉样蛋白的产生图片来源：参考资料【4】近期，在阿拉巴马大学伯明翰分校开展的一项新研究中，科学家以极高的分辨率对帕金森病患者的微生物组进行了分析，在84种与帕金森病相关的微生物种类中，55种在患者体内丰度异常高，另外29种却难觅踪迹。研究表明，患者体内的微生物失衡现象很可能是疾病进展的重要诱因。图 3 与PD相关的微生物表达情况图片来源：参考资料【5】 2019年，贝勒医学院的神经生物学家 Mauro Costa-Mattioli 博士偶然间发现，自闭症模型的小鼠，肠道中缺乏一种特定的细菌：罗伊氏乳杆菌。补充这种细菌，小鼠的症状会大大减轻。新发表在《Nature Communication》的文章，调查了荷兰鹿特丹研究队列中1054名参与者的粪便微生物组多样性和组成与抑郁症状的关系，并在一个阿姆斯特丹队列的1539名受试者中验证了这些发现。结果表明，13个微生物分类群与抑郁症状的关联。这些细菌已知参与了影响抑郁症的关键神经递质的合成，例如，谷氨酸、丁酸、5-羟色胺和γ-氨基丁酸（GABA）。图 4 显示与抑郁症状有关的13个属的分类树图片来源：参考资料【6】加州理工学院 Sarkis Mazmanian 教授团队的一项研究显示，肠道内的菌群能够将饮食中常见的氨基酸络氨酸转化为4-乙基苯基硫酸酯（4EPS），该物质可穿越血脑屏障并降低大脑中形成髓鞘的神经少突胶质细胞成熟，导致焦虑情绪出现。这项研究有助于揭示肠道微生物群变化与复杂的情绪行为有关的机制。 02众人拾柴火焰高与科学研究齐头并进的，是微生物组领域的临床发展。 2011-2017年间，微生物组新药研发的数量呈现快速增长。目前，医药公司对于微生物组的新药研发主要分为三类：活性生物治疗、小分子药物和生物制剂。其中，活性生物治疗作为各大医药公司发展时间最长的微生物法，是指将一种或多种细菌体外培养后，重新作为“有益菌”定植于肠内行使一定的功能。而小分子药物和生物制剂是影响体内微生物组的构成或者影响微生物与宿主组织之间的相互作用。图 5 2011-2017年微生物组新药研发数量数据来源：参考资料【7】目前从事微生物组新药研发的企业主要为小型生物技术公司，例如，Seres Therapeutics，Evelo Biosciencs，Enterome，MatriSys Bioscience，Caelus Health，Rebiotix 等。根据笔者对在研新药的梳理发现，目前新药研发主要集中在胃肠道系统，皮肤病等领域，但也有针对新适应症（例如，肿瘤，代谢性疾病、神经精神疾病、罕见病）的新品种涌现。进入Ⅲ期临床的品种共有6个。例如，Seres Therapeutics 旗下用于预防艰难梭菌感染引起的肠道疾病的口服活体生物药SER-109已于2022年10月获FDA优先审评资格，在不久的将来也会迎来好消息。表 1 微生物组新药在研情况（列举）资料来源：ClinicalTrials.gov，公司官网，笔者整理此外，制药巨头开始布局抢占微生物疗法新赛道。根据 Back Bay Life Science Advisors 显示，大型制药企业通过开展临床合作研发、授权交易、并购等方式涉足微生物组疗法领域，2013-2019年，共有40多项交易项目。 2022年，Seres Therapeutics 宣布与雀巢健康科学达成协议，雀巢健康科学将获得用于治疗复发性艰难梭菌感染的 SER-109 的美国和加拿大商业化权益。根据协议，雀巢健康的全球制药业务部门 Aimmune Therapeutics 将承担商业化运营的角色。雀巢健康向Seres支付1.75亿美元预付款，后续还将支付总额1.25亿美元的注册批准和销售里程金。 Genome and Company 公司与默沙东合作开展一项2期临床试验，以评估 Genome and Company 旗下的微生物组疗法 GEN001 与默沙东 KEYTRUDA 联合用于胆道癌患者的安全性和疗效。 03资本一再押注 VC 界一直热衷于投资微生物组疗法，2022年已有18亿欧元资金投向微生物组疗法领域，这一金额与创下投资纪录的2021年基本持平。由此可见，虽然近年生物制药资本市场遇冷，但投资者对微生物疗法领域仍旧充满信心。图 6 2022年微生物组疗法风投融资额变化图片来源：Microbiome Times 不少微生物疗法领域的新兴生物公司近年来的融资表现突出。以 Kallyope 公司为例，这是一家基于肠道菌群多组学研究的精准肠道药物研发企业，致力于胃肠道疾病、神经障碍、代谢类疾病新药研发。自2015年成立至今已完成四轮融资，融资总金额高达2.4亿美元。表 2 菌群新药研发药物企业融资、产品布局情况（列举）资料来源：公司官网、笔者整理1. 融资总金额是由 A轮、B轮、C轮、IPO 融资金额合计得来； 04挑战与机遇并存然而，微生物组疗法领域并非一帆风顺。部分在研产品由于临床效果不佳（例如，Synlogic 的 SYNB1020、Oragenics 的AG013）或者企业终止业务或关停微生物在研管线（例如，Assembly Biosciences）等原因终止或暂停了研发。微生物疗法是一个新兴的领域，正在逐步从科学研究阶段向商业化阶段发展。伴随着科学环境研究的不断深入，微生物组疗法应用领域不断扩大，在未来，仍将受到大型制药企业和资本市场的持续关注。该赛道有变数，但也存在机会，下一个入场选手的表现如何，拭目以待。参考资料：1. 公司官网，Microbiome Times官网2. 《里程碑！首款粪便微生物组疗法获FDA批准》，药明康德公众号，2022年12月3. 《药物基于“肠-脑”通路的研究进展》，《药学学报》，2021年第3期4. Pistollato F, Sumalla CS, Elio I, et al. Role of gut microbiota and nutrients in amyloid formation and pathogenesis of Alzheimer's disease. Nutr Rev. 2016, 74: 624-634. DOI:10.1093/nutrit/nuw0235. Achary D. Wallen et al, Metagenomics of Parkinson's disease implicates the gut microbiome in multiple disease mechanisms. Nature Communications. 2022, DOI: 10.1038/s41467-022-34667-x6. Radjabzadeh, D., Bosch, J.A., Uitterlinden, A.G. et al. Gut microbiome-wide association study of depressive symptoms. Nature Communications. Dec 6;13(1):7128. DOI: 10.1038/s41467-022-34502-37. Microbiome Modulator Drugs – The New Generation of Therapeutic，Informa，2018声明：本内容为作者独立观点，不代表药智网立场。如需转载，请务必注明文章作者和来源。对本文有异议或投诉，请联系maxuelian@yaozh.com。责任编辑 | 绿萝转载开白 | 马老师 18323856316（同微信）— Tips —长按/扫码入读者群交流投稿请联系：马老师电话 18996384680微信 18323856316邮箱maxuelian@yaozh.com 阅读原文，是近期最受欢迎的文章哦

微生物疗法临床研究

100 项与 Dapatifagene navolactibac 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
头颈部肿瘤	临床2期	美国	Oragenics, Inc.	2017-07-18
头颈部肿瘤	临床2期	比利时	Oragenics, Inc.	2017-07-18
头颈部肿瘤	临床2期	德国	Oragenics, Inc.	2017-07-18
头颈部肿瘤	临床2期	英国	Oragenics, Inc.	2017-07-18
口腔炎	临床2期	美国	Oragenics, Inc.	2017-07-18
口腔炎	临床2期	比利时	Oragenics, Inc.	2017-07-18
口腔炎	临床2期	德国	Oragenics, Inc.	2017-07-18
口腔炎	临床2期	英国	Oragenics, Inc.	2017-07-18

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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


NCT03234465 (CTgov)	临床2期	口腔炎 \| 头颈部肿瘤	200	AG013 (AG013)	築憲製淵構淵繭艱鏇願(醖獵簾觸積艱艱鑰糧繭) = 積繭淵鏇築廠簾廠願糧廠衊廠繭糧壓顧餘構衊 (蓋膚艱窪願遞製醖衊蓋, 齋築鑰膚積糧醖鹹餘積 ~ 築鏇選鬱廠醖選憲積膚) 更多	-	2020-11-23
				placebo (Placebo)	築憲製淵構淵繭艱鏇願(醖獵簾觸積艱艱鑰糧繭) = 築遞積範網積選遞網願廠衊廠繭糧壓顧餘構衊 (蓋膚艱窪願遞製醖衊蓋, 醖築齋醖廠獵糧憲夢膚 ~ 艱餘顧襯網蓋鬱糧鹹壓) 更多
NCT00938080 (Pubmed \| Cancer) 人工标引	临床1期	头颈部肿瘤	52	AG013	鬱顧範餘顧夢鬱積鏇壓(襯鹹網網簾顧窪鏇觸壓) = 積繭襯憲餘鹹積淵窪顧醖鏇鑰窪範憲糧夢蓋觸 (網製膚衊窪製窪艱艱夢 ) 更多	积极	2013-12-15
				Placebo	-