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Innovation Pharmaceuticals Announces Publication of Scientific Article on the Antifungal Activity of Brilacidin

Innovation Pharmaceuticals Announces Publication of Scientific Article on the Antifungal Activity of Brilacidin

创新制药公司宣布发表关于Brilacidin抗真菌活性的科学文章
GlobeNewswire ·  2022/10/04 07:35
  • In pre-clinical studies, Brilacidin shown to synergize with marketed antifungals against pathogenic species of aspergillosis, candidiasis, cryptococcosis and mucormycosis, and further exhibited potent stand-alone efficacy against Cryptococcus neoformans
  • These data suggest Brilacidin has potential as a novel antifungal agent
  • 在临床前研究中,Brilacidin被证明与市场上销售的抗真菌药物对致病物种有协同作用曲霉病, 念珠菌病, 隐球菌病毛霉病,并进一步显示出强大的单项效力新生隐球菌
  • 这些数据表明Brilacidin具有作为一种新的抗真菌药物的潜力

WAKEFIELD, MA, Oct. 04, 2022 (GLOBE NEWSWIRE) -- via NewMediaWire – Innovation Pharmaceuticals (OTCQB:IPIX) ("the Company"), a clinical stage biopharmaceutical company, today announced publication of a scientific article on the antifungal activity of Brilacidin, the Company's defensin-mimetic drug candidate with antimicrobial and immunomodulatory properties. The paper, accessible at the link below as a preprint and to be submitted for peer review, is based on independent research conducted primarily by scientists at the University of São Paulo, Brazil. A corresponding patent application related to this work has been filed.

马萨诸塞州韦克菲尔德,2022年10月4日(环球网)--临床阶段生物制药公司Via NewMediaWire-Innovation PharmPharmticals(场外交易市场代码:IPIX)今天宣布发表一篇关于Brilacidin抗真菌活性的科学文章,Brilacidin是该公司的防御素类候选药物,具有抗微生物和免疫调节特性。这篇论文主要基于巴西圣保罗大学的科学家进行的独立研究,可通过以下链接获得预印本并提交同行审查。与这项工作相关的相应专利申请已经提交。

  • Fernanda dos Reis T, Alves de Castro P, Bastos R, Pinzan CF, Souza PFN, Ackloo S, Hossain MA, Drewry D, Alkhazraji S, Ibrahim A, Hyunil J, DeGrado WF. "A Host Defense Peptide Mimetic, Brilacidin, Potentiates Caspofungin Antifungal Activity Against Human Pathogenic Fungi."
  • Fernanda dos Reis T,Alves de Castro P,Bastos R,Pinzan CF,Souza PFN,Ackloo S,Hossain MA,Drewry D,AlKhazraji S,Ibrahim A,Hyunil J,DeGrado WF。一种宿主防御肽模拟物,Brilacidin,增强卡泊芬净对人类病原真菌的抗真菌活性。

bioRxiv 2022.09.28.509882; doi.org/10.1101/2022.09.28.509882

BioRxiv 2022.09.28.509882;doi.org/10.1101/2022.09.28.509882

Summary of Brilacidin Antifungal Research Findings

Brilacidin抗真菌研究进展综述

Following an in vitro drug screening of 1,402 compounds, Brilacidin showed promising antifungal activity and was subsequently selected for additional pre-clinical evaluation, including in combination with caspofungin (CAS), voriconazole (VOR), and posaconazole (POSA), all current antifungal treatments.

在此之后体外培养在1,402种化合物的药物筛选中,Brilacidin显示出良好的抗真菌活性,随后被选中进行额外的临床前评估,包括与卡泊芬净(CAS)、伏立康唑(VOR)和泊沙康唑(POSA)的联合使用,这些都是目前的抗真菌治疗方法。

In cell culture, in Aspergillus fumigatus (A. fumigatus), Brilacidin converted CAS from a fungistatic into a fungicidal drug, enabling it to overcome both drug resistance and biofilm formation. Brilacidin exerted, to a lesser degree, synergistic effects with VOR in A. fumigatus. Further in vitro testing showed Brilacidin synergized with CAS in C. albicans, C. auris and C. neoformans. In an A. fumigatus immunosuppressed mouse model in invasive pulmonary aspergillosis, Brilacidin plus CAS cleared infection in the lungs by almost 95 percent, compared to ~50 percent when each compound was administered individually. Brilacidin also showed in vitro an additive inhibitory effect when combined with POSA in several species of Mucorales, the main etiological agents of mucormycosis, commonly referred to as black fungus. Mortality rates can be as high as 90 percent in this fungal disease.

在细胞培养中,烟曲霉菌 (烟曲霉菌),Brilacidin将CAS从抗真菌药物转变为杀菌药物,使其能够克服耐药性和生物被膜形成。Brilacidin与VOR在不同程度上有协同作用烟曲霉菌。进一步体外培养测试显示Brilacidin与CAS在白色念珠菌, C.Auris新生芽孢杆菌。在一个烟曲霉菌在侵袭性肺曲霉菌病免疫抑制小鼠模型中,Brilacidin加CAS可清除肺部感染近95%,而单独给予两种化合物时约50%。Brilacidin还展示了体外培养当与POSA结合时,在几种毛霉目中具有相加的抑制作用,主要病原体是毛霉病,通常被称为黑木耳。这种真菌病的死亡率可能高达90%。

Interestingly, Brilacidin showed potent in vitro stand-alone efficacy (MIC=2.5µM) in C. neoformans, a major driver of illness in people living with HIV/AIDS. C. neoformans, for which few effective treatments are available, causes an estimated 220,000 cases of cryptococcal meningitis worldwide each year and is associated with an 80 percent mortality rate.

有趣的是,Brilacidin显示出强大的体外培养单机效能(MIC=2.5微米)新生芽孢杆菌它是艾滋病毒/艾滋病患者患病的主要驱动力。新生芽孢杆菌几乎没有有效的治疗方法,每年在全球范围内造成约22万例隐球菌性脑膜炎,并与80%的死亡率有关。

A proposed antifungal mechanism of action of Brilacidin involves membrane depolarization by impacting calcineurin and cell wall integrity, as informed by protein kinase inhibitory experiments and genetic screenings of protein phosphatase null mutants.

一种已提出的Brilacidin的抗真菌作用机制涉及通过影响钙调神经磷酸酶和细胞壁完整性来实现膜去极化,这一信息来自于蛋白激酶抑制实验和对蛋白磷酸酶缺失突变体的遗传筛选。

"It is a remarkable feature of Brilacidin that it can potentiate multiple antifungals, in different pathogenic fungi, including hard-to-treat species. New antifungal combination strategies are urgently needed due to a scarcity of novel agents, alongside emerging resistance in the clinical setting," commented Gustavo Henrique Goldman, Professor of Molecular Biology, University of São Paulo, Brazil, and a Chief Editor for Frontiers in Fungal Biology, a peer-reviewed journal dedicated to the study of mycology. "Another notable finding from our research is that Brilacidin shows exceptional potency of its own as a monotherapy against C. neoformans, a particularly problematic fungus. We look forward to broadening our planned studies of Brilacidin's antifungal properties."

巴西圣保罗大学分子生物学教授、《每日电讯报》主编古斯塔沃·恩里克·戈德曼评论说:“Brilacidin的显著特点是,它可以在不同的病原真菌中增强多种抗真菌药物,包括难以治疗的物种。由于缺乏新药,加上临床环境中新出现的耐药性,迫切需要新的抗真菌联合策略。”真菌生物学前沿,这是一本致力于真菌学研究的同行评议期刊。“我们研究的另一个值得注意的发现是,Brilacidin作为一种单一疗法显示出非凡的效力。新生芽孢杆菌,一种特别有问题的真菌。我们期待着扩大我们计划的对Brilacidin抗真菌特性的研究。“

About Antifungal Diseases 1, 2, 3

关于抗真菌疾病1, 2, 3

There are up to 5 million fungal species populating the earth, of which approximately 100,000 species have been identified. About 300 fungal species cause disease in humans. Overall, Candida, Cryptococcus and Aspergillus represent the main causative organisms of invasive fungal infections. There is a large unmet medical need for developing novel antifungal agents, particularly given the emergence of resistance in the clinical setting. The utility of current antifungal treatments is limited due to toxicity, fungistatic and not fungicidal properties, as well as drug interaction concerns. In the United States, antifungal drugs can qualify for expedited clinical development, under Qualified Infectious Disease Product designation, Orphan Drug designation, and the limited population pathway development program. Pivotal clinical trials for antifungal drugs are generally smaller than those in other infectious disease areas, requiring between 300 and 600 patients. Caspofungin sales were estimated to be $414 million in 2021, with the global antifungal drugs market estimated at $14.8 billion in 2021 and expected to reach $20.5 billion by 2030.

地球上有多达500万种真菌物种,其中约10万种已被确认。大约有300种真菌会导致人类患病。总的来说,念珠菌, 隐球菌曲霉菌代表侵袭性真菌感染的主要致病微生物。开发新的抗真菌药物有大量未得到满足的医学需求,特别是在临床环境中出现耐药性的情况下。由于毒性、抗真菌而不是杀菌特性以及药物相互作用的考虑,目前抗真菌治疗的效用有限。在美国,根据合格的传染病产品指定、孤儿药物指定和有限人口途径发展计划,抗真菌药物可以获得加速临床开发的资格。抗真菌药物的关键临床试验通常比其他传染病领域的试验规模小,需要300至600名患者。2021年卡泊芬净的销售额估计为4.14亿美元,2021年全球抗真菌药物市场估计为148亿美元,预计到2030年将达到205亿美元。

1 Current Antimycotics, New Prospects, and Future Approaches to Antifungal Therapy

1当前抗真菌药物、新前景和未来抗真菌治疗方法

2 Global Caspofungin Market Research Report 2022 (Status and Outlook)

2《2022年全球卡泊芬净市场研究报告》(现状与展望)

3 Antifungal Drugs Market Size to be worth $20.5 Billion by 2030: Grand View Research, Inc.

3抗真菌药物市场规模到2030年将达到205亿美元:Grand View Research,Inc.

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About Innovation Pharmaceuticals

关于创新制药公司

Innovation Pharmaceuticals Inc. (IPIX) is a clinical stage biopharmaceutical company developing a portfolio of innovative therapies addressing multiple areas of unmet medical need, including inflammatory diseases, cancer, and infectious diseases. The Company is also active in evaluating other potential investment opportunities that can add value and diversify its portfolio.

创新制药公司(IPIX)是一家临床阶段的生物制药公司,开发一系列创新疗法,以解决多种未得到满足的医疗需求领域,包括炎症性疾病、癌症和传染病。该公司还积极评估其他潜在的投资机会,以增加价值并使其投资组合多样化。

Forward-Looking Statements: This press release contains forward-looking statements made pursuant to the safe harbor provisions of the Private Securities Litigation Reform Act of 1995 including, without limitation, statements concerning future product development plans, including with respect to specific indications; statements regarding the therapeutic potential and capabilities of the StingRay System; future regulatory developments; and any other statements which are other than statements of historical fact. These statements involve risks, uncertainties and assumptions that could cause actual results and experience to differ materially from anticipated results and expectations expressed in these forward-looking statements. The Company has in some cases identified forward-looking statements by using words such as "anticipates," "believes," "hopes," "estimates," "looks," "expects," "plans," "intends," "goal," "potential," "may," "suggest," and similar expressions. Among other factors that could cause actual results to differ materially from those expressed in forward-looking statements are risks related to conducting pre-clinical studies and clinical trials and seeking regulatory and licensing approvals in the United States and other jurisdictions, including without limitation that compounds and devices may not successfully complete pre-clinical or clinical testing, or be granted regulatory approval to be sold and marketed in the United States or elsewhere; prior test results may not be replicated in future studies and trials; the Company's need for, and the availability of, substantial capital in the future to fund its operations and research and development, including the amount and timing of the sale of shares of common stock under securities purchase agreements; and the Company's licensee(s) may not successfully complete pre-clinical or clinical testing and the Company will not receive milestone payments. A more complete description of these and other risk factors is included in the Company's filings with the Securities and Exchange Commission. Many of these risks, uncertainties and assumptions are beyond the Company's ability to control or predict. You should not place undue reliance on any forward-looking statements. The forward-looking statements speak only as of the information currently available to the Company on the date they are made, and the Company undertakes no obligation to release publicly the results of any revisions to any such forward-looking statements that may be made to reflect events or circumstances after the date of this press release or to reflect the occurrence of unanticipated events, except as required by applicable law or regulation.

前瞻性陈述:本新闻稿包含根据1995年《私人证券诉讼改革法》的安全港条款作出的前瞻性陈述,包括但不限于有关未来产品开发计划的陈述,包括有关特定适应症的陈述;有关黄貂鱼系统治疗潜力和能力的陈述;未来监管发展;以及除历史事实陈述之外的任何其他陈述。这些陈述涉及风险、不确定性和假设,可能导致实际结果和经验与这些前瞻性陈述中表达的预期结果和预期大不相同。在某些情况下,公司通过使用诸如“预期”、“相信”、“希望”、“估计”、“展望”、“预期”、“计划”、“打算”、“目标”、“潜在”、“可能”、“建议”以及类似的表达方式来识别前瞻性陈述。可能导致实际结果与前瞻性陈述中表述的结果大不相同的其他因素包括,与在美国和其他司法管辖区进行临床前研究和临床试验以及寻求监管和许可批准有关的风险,包括但不限于化合物和设备可能无法成功完成临床前或临床测试,或未获得在美国或其他地方销售和销售的监管批准;以前的测试结果可能不会在未来的研究和试验中复制;公司未来需要和获得大量资本来资助其运营和研发, 包括根据证券购买协议出售普通股的金额和时间;公司的被许可人可能无法成功完成临床前或临床测试,公司将不会收到里程碑式的付款。关于这些和其他风险因素的更完整的描述包括在该公司提交给证券交易委员会的文件中。其中许多风险、不确定性和假设超出了公司的控制或预测能力。您不应过度依赖任何前瞻性陈述。前瞻性陈述仅代表公司在发布之日目前掌握的信息,公司没有义务公开发布对任何此类前瞻性陈述的任何修订结果,除非适用法律或法规要求,否则这些修订可能反映本新闻稿发布之日之后的事件或情况,或反映意外事件的发生。

INVESTOR AND MEDIA CONTACTS 
Innovation Pharmaceuticals Inc. 
Leo Ehrlich 
info@ipharminc.com

投资者和媒体联系
创新制药公司。
利奥·埃尔利希
邮箱:Info@ipharminc.com


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