InMed Pharmaceuticals Announces Favorable Behavioral Outcomes With INM-901 in Long-Term Preclinical Alzheimer's Disease Study, Confirming Previous Short-Term Pilot Study Data
InMed Pharmaceuticals Announces Favorable Behavioral Outcomes With INM-901 in Long-Term Preclinical Alzheimer's Disease Study, Confirming Previous Short-Term Pilot Study Data
- Results confirm improvements in cognitive function, memory and locomotor activity
- Achieved statistical significance in certain behavioral assessments
- Additional molecular analyses ongoing to elucidate INM-901 mechanisms of action
- 結果確認認知功能、記憶和運動活動的改善。
- 在某些行爲評估方面取得了統計學意義。
- 進行額外的分子分析以闡明INm-901作用機制。
Vancouver, British Columbia–(Newsfile Corp. – July 30, 2024) – InMed Pharmaceuticals Inc. (NASDAQ: INM) ("InMed" or the "Company"), a pharmaceutical company focused on developing a pipeline of proprietary small molecule drug candidates for diseases with high unmet medical needs, today announced positive results from initial data sets from a long-term (7 months of dosing) in vivo preclinical Alzheimer's Disease ("AD") study of INM-901 which confirms previously reported findings from a short-term (3 months of dosing) pilot study, as disclosed in the Company's prior press release dated April 4, 2024.
卑詩省溫哥華市-(新聞稿公司-2024年7月30日)-InMed Pharmaceuticals Inc.(納斯達克:INM)(“InMed”或“公司”),一家專注於開發專有的小分子藥物候選管道以應對高未滿足醫學需求疾病的製藥公司,今天宣佈從INm-901的長期(7個月的投藥)體內臨床前阿爾茨海默病(“AD”)研究的初始數據集中獲得積極結果,該結果確認了公司此前發佈的短期(3個月的投藥)試驗結果,細節可查看公司在2024年4月4日發佈的新聞稿。
Similar to the short-term pilot study, this long-term dosing study was conducted using the 5xFAD amyloidosis model with extended dosing duration and increased sample size as compared to the short-term study. This long-term study had four groupings:
類似於短期試點研究,本長期給藥研究是使用5xFAD澱粉樣變模型,比短期研究的用藥持續時間更長,樣品量也增加了。本長期研究分爲四組:
- Untreated disease-free group;
- INM-901-treated disease-free group;
- Placebo-treated Alzheimer's Disease (amyloidosis) group; and
- INM-901-treated Alzheimer's Disease (amyloidosis) groups with two dosing levels.
- 未治療的無病組;
- 治療INm-901的無病組;
- 安慰劑治療的阿爾茨海默病(澱粉樣變)組;和
- 治療INm-901的阿爾茨海默病(澱粉樣變)組,分爲兩個劑量。
It is important to note that disease severity increases with advancing age in this preclinical amyloidosis model such that groups in the long-term study had more advanced AD than those in the previous short-term pilot study.
在這種體外澱粉樣變模型中,隨着年齡的增長,疾病的嚴重程度會增加,因此長期研究中的組比之前的短期試點研究中的組更爲先進。
The study included an assessment of several behavioral criteria across the four study groupings:
該研究涉及對四個研究組的幾個行爲標準進行評估:
- Novel Object Recognition Test evaluating cognitive function and memory;
- Open Field Test evaluating general locomotor activity level;
- Elevated and Zero Maze Tests measuring anxiety-related behavior;
- Barnes Maze Test measuring spatial learning and memory; and
- Acoustic Startle Test measuring sound awareness.
- 新穎物體識別測試評估認知功能和記憶;
- 開放領域測試評估總體運動活動水平;
- 高架迷宮測試和零迷宮測試評估與焦慮有關的行爲;
- 巴恩斯迷宮測試測量空間學習和記憶;和
- 聲音驚嚇測試測量聲音感知。
All assessments of the INM-901-treated AD groups showed a positive trend towards behaviour similar to the untreated disease-free group, with most assessments demonstrating a clear dose response. Furthermore, INM-901-treated AD groups achieved a statistically significant improvement in certain behavior criteria in comparison to the placebo-treated AD groups. These results not only supported but in several instances improved upon the prior short-term pilot study outcomes.
所有INm-901治療的AD組的評估都顯示出了與未治療無病組類似的積極趨勢,大多數評估都表現出明顯的劑量反應。此外,INm-901治療的AD組在某些行爲標準上比安慰劑治療的AD組實現了統計學上顯著的改善。這些結果不僅支持了之前的短期試點研究結果,而且在幾個方面都有所提高。
Dr. Eric Hsu, InMed's Senior Vice President of Preclinical Research and Development, stated; "We are highly encouraged by the initial data sets from this long-term dosing study, which support the previously observed improvements in behavioral outcomes seen in our initial short-term preclinical Alzheimer's proof-of-concept study. INM-901 continues to demonstrate potential by targeting multiple biological pathways linked to Alzheimer's Disease and may have potential to address the critical need for effective treatments."
InMed公司的高級副總裁,臨床研究和開發負責人Eric Hsu博士表示:“我們對這項長期給藥研究的初步數據集非常鼓舞,這些數據支持了我們最初從短期阿爾茨海默病臨床前概念研究中觀察到的行爲結果的改善。INm-901繼續通過針對與阿爾茨海默病相關的多種生物通路表現出潛力,並可能有潛力解決有效治療的關鍵需求。”
The Company is conducting further molecular analyses to better define the mechanisms of action and potential role of INM-901 in AD treatment. The analyses will focus on the following areas using mRNA, protein and histological measurements:
公司正在開展進一步的分子分析,以更好地確定INm-901在AD治療中的作用機制和潛在作用。這些分析將使用mRNA、蛋白質和組織學測量重點關注以下領域:
- Receptor engagement: CB1/CB2 and PPAR;
- Neuroinflammation: various cytokines and inflammatory marker protein level;
- Neurogenesis: assess markers for neuronal differentiation and neuronal function; and
- Neuroprotection: evaluating stress responses and cellular growth/survival.
- 受體結合:CB1/CB2和PPAR;
- 神經炎症:評估各種細胞因子和炎性標誌蛋白水平;
- 神經生成:評估神經元分化和神經元功能的標誌物;
- 神經保護:評估應激反應和細胞生長/存活。
Additionally, the development of the chemistry, manufacturing, and controls (CMC) for both the drug substance and the drug product formulation is ongoing, with GLP studies in the planning stages to support an IND submission.
此外,藥物物質和藥物產品配方的化學、製造和控制(CMC)正在進行中,規劃中進行GLP研究以支持IND提交。
INM-901 Program to date
迄今的INm-901項目
Research and development activities to date have demonstrated the potential of INM-901 to target several biological pathways associated with AD, including positive pharmacological characteristics such as:
迄今的研發活動已表明INm-901有潛力靶向與AD相關的幾種生物學途徑,具有以下積極的藥理特性:
- A preferential signaling agonist for CB1/CB2 and impacts PPAR signaling pathways;
- Blood/brain barrier (BBB) penetration; may be deliverable via oral administration;
- Demonstrated neuroprotective effects against amyloid-beta-induced cytotoxicity;
- Demonstrated an ability to promote neurite outgrowth, signifying the potential to improve neuronal function;
- Demonstrated reduced neuroinflammation and improved neuronal function; and
- Molecular data supports observations from behavior studies demonstrating improvements in locomotor activity, cognition and memory.
- CB1/CB2的優先信號激動劑,並影響PPAR信號途徑;
- 能夠穿過血腦屏障(BBB),可口服給藥;
- 對抗澱粉樣β-誘導的細胞毒性具有神經保護作用;
- 具有促進神經突起生長的能力,表明有改善神經功能的潛力;
- 減少神經炎症並改善神經功能;
- 分子數據支持行爲研究的觀察結果,證明了運動活動、認知和記憶方面的改善。
About InMed:
關於InMed:
InMed Pharmaceuticals is a pharmaceutical company focused on developing a pipeline of proprietary small molecule drug candidates targeting the CB1/CB2 receptors. InMed's pipeline consists of three separate programs in the treatment of Alzheimer's, ocular and dermatological indications. Together with our subsidiary BayMedica, we are a global leader in the manufacturing, development and commercialization of rare cannabinoids and proprietary small molecule drug candidates. For more information, visit .
InMed Pharmaceuticals是一家制藥公司,專注於開發針對CB1/CB2受體的專有小分子藥物候選品管道。InMed的管道包括三個單獨的計劃,用於治療阿爾茨海默病、眼科和皮膚學指示。與我們的子公司BayMedica一起,我們是罕見的大麻素和專有小分子藥物候選品的製造、開發和商業化的全球領軍者。欲了解更多信息,請訪問。
Investor Contact:
Colin Clancy
Vice President, Investor Relations
and Corporate Communications
T: +1 604 416 0999
E: [email protected]
投資者聯繫人:
Colin Clancy
投資者關係副總裁
和企業通訊
電話號碼:+1 604 416 0999
電子郵箱:[email protected]
Cautionary Note Regarding Forward-Looking Information:
有關前瞻性信息的警示:
This news release contains "forward-looking information" and "forward-looking statements" (collectively, "forward-looking information") within the meaning of applicable securities laws. Forward-looking statements are frequently, but not always, identified by words such as "expects", "anticipates", "believes", "intends", "potential", "possible", "would" and similar expressions. Such statements, based as they are on current expectations of management, inherently involve numerous risks, uncertainties and assumptions, known and unknown, many of which are beyond our control. Forward-looking information is based on management's current expectations and beliefs and is subject to a number of risks and uncertainties that could cause actual results to differ materially from those described in the forward-looking statements. Without limiting the foregoing, forward-looking information in this news release includes, but is not limited to, statements about: the efficacy of INM-901, INM-901's ability to treat AD, marketability and uses for INM-901, the results of further studies into INM-901 and acceleration of the development of InMed's AD program as well as potential GLP studies or IND submissions.
本新聞發佈包含“前瞻性信息”和“前瞻性陳述”(統稱“前瞻性信息”),根據適用證券法規定。前瞻性陳述通常,但並非總是,通過“期望”、“預計”、“相信”、“意圖”、“潛在”、“可能”、“將”等類似表述識別。這些陳述基於管理層目前的預期,本質上涉及許多風險、不確定性和假設,已知和未知,其中許多超出了我們的控制範圍。前瞻性信息基於管理層的當前預期和信念,並受到許多風險和不確定性的影響,可能導致實際結果與前瞻性陳述中所描述的有實質性區別。在不限制前述內容的前提下,在本新聞發佈中的前瞻性資訊包括但不限於,關於INm-901的功效、INm-901治療AD的能力、INm-901的市場價值和用途、進一步研究INm-901的結果,加速InMed的AD項目的發展以及潛在的GLP研究或IND提交的聲明。
Additionally, there are known and unknown risk factors which could cause InMed's actual results, performance, or achievements to be materially different from any future results, performance or achievements expressed or implied by the forward-looking information contained herein. A complete discussion of the risks and uncertainties facing InMed's stand-alone business is disclosed in InMed's Annual Report on Form 10-K and other filings with the Securities and Exchange Commission on www.sec.gov.
此外,已知和未知的風險因素可能會導致InMed的實際結果、表現或成就與這裏所包含的前瞻性信息未來的結果、表現或成就存在實質性的差別。關於InMed的獨立業務所面臨的所有風險和不確定因素的完整討論已在InMed的年報10-K表和其他提交給www.sec.gov的證券交易委員會的文件中披露。
All forward-looking information herein is qualified in its entirety by this cautionary statement, and InMed disclaims any obligation to revise or update any such forward-looking information or to publicly announce the result of any revisions to any of the forward-looking information contained herein to reflect future results, events or developments, except as required by law.
此處所有的前瞻性信息都受到這一警示聲明的限制,並且InMed放棄了對任何此類前瞻性信息進行修訂和更新或公開宣佈任何對此類前瞻性信息所做修訂的結果來反映未來的結果、事件或發展的義務,除非法律要求其這樣做。
To view the source version of this press release, please visit
要查看此新聞發佈的源版本,請訪問