Hemostemix's 4th Heart Study Published in Stem Cell Research & Therapy Confirms Breakthrough Treatment for Heart Disease
Hemostemix's 4th Heart Study Published in Stem Cell Research & Therapy Confirms Breakthrough Treatment for Heart Disease
Calgary, Alberta--(Newsfile Corp. - October 30, 2023) - Hemostemix Inc. (TSXV: HEM) (OTCQB: HMTXF) (FSE: 2VF0) is pleased to announce that Stem Cell Research & Therapy published the Company's seventh peer reviewed study of ACP-01 - the third peer reviewed study of ACP-01 as a treatment for heart disease (ischemic and non-ischemic dilated cardiomyopathy), which demonstrates ACP-01 regenerates and improves cardiac function by up to 24.1% at 12 months in ischemic cardiomyopathy, and regenerates and improves cardiac function in non-ischemic cardiomyopathy patients by up to 47.1% at 12 months (dLVEF%/iLVEF%).
艾伯塔省卡爾加里--(Newsfile Corp.,2023年10月30日)——Hemostemix Inc.(多倫多證券交易所股票代碼:HEM)(OTCQB:HMTXF)(FSE:2VF0)很高興地宣佈 幹細胞研究與治療 發表了公司關於 ACP-01 的第七項同行評審研究,這是第三項關於 ACP-01 治療心臟病(缺血性和非缺血性擴張型心肌病)的同行評審研究,該研究表明 ACP-01 在缺血性心肌病中 12 個月時可再生和改善心臟功能多達 24.1%,非缺血性心肌病患者的心臟功能在 12 歲時再生和改善多達 47.1% 月 (dlvef%/ilvef%)。
Cardiomyopathy is chronic disease of heart muscle due to an acquired or hereditary condition. Ischemic cardiomyopathy is the most common form, resulting from inadequate blood flow to the heart, and affecting 2.5 million persons in the USA, with a mortality of 200,000 annually. Non-ischemic dilated cardiomyopathy - due to autoimmune, infectious, infiltrative or familial (genetic) causes - results in dilation and ineffectiveness of the heart wall, with a prevalence of approximately 400,000 persons in the U.S.A., annual mortality of 10 -50%, and is a major cause for cardiac transplantation in children.
心肌病是由於獲得性或遺傳性疾病引起的心肌慢性疾病。缺血性心肌病是最常見的形式,由流向心臟的血液不足引起,在美國,有250萬人受到影響,每年死亡20萬人。由於自身免疫、傳染性、浸潤性或家族(遺傳)原因導致的非缺血性擴張型心肌病會導致心壁擴張和無效,在美國患病率約爲40萬人,年死亡率爲10-50%,是兒童心臟移植的主要原因。
Stem cell transplantation is an emerging therapy for severe cardiomyopathy. Angiogenic cell precursors (ACP-01) are autologous cells (obtained from the patient in a simple blood draw), lineage-specific (programmed to form blood vessels), with strong potential to effectively engraft, and support tissue survival and regeneration.
幹細胞移植是嚴重心肌病的新興療法。血管生成細胞前體(ACP-01)是自體細胞(通過簡單的抽血從患者身上獲得),具有譜系特異性(編程形成血管),具有有效移植和支持組織存活和再生的強大潛力。
This study, published in Stem Cell Research and Therapy, is an IRB approved, peer reviewed retrospective analysis of 53 adult patients who underwent endovascular implantation of ACP-01 through a catheter for treatment of ischemic cardiomyopathy and non-ischemic dilated cardiomyopathy . The study was not randomized. Cardiac function was assessed by measurement of the left ventricular ejection fraction (LVEF) - the percentage of heart volume pumped out with each heart beat. A normal LVEF is 52-72% in men, 54%-74% in women.
這項研究發表於 幹細胞研究與治療,是一項經IRB批准的、經過同行評審的回顧性分析,對53名通過導管進行血管內植入 ACP-01 以治療缺血性心肌病和非缺血性擴張型心肌病的成年患者。該研究不是隨機進行的。心臟功能是通過測量左心室射血分數(LVEF)來評估的,左心室射血分數(每次心跳時抽出的心臟容量的百分比)。男性的正常LVEF爲52-72%,女性爲54%-74%。
Four months after implantation of ACP-01, those patients with ischemic cardiomyopathy (n = 41) improved by 4.7% (p < 0.004), and by 12 months the LVEF had increased from an initial 29.9 % to 38.2% (p < 0.004). The increase (dLVEF%/iLVEF%) represents an increase in cardiac function of 24.1% at 12 months.
在植入 ACP-01 四個月後,那些患有缺血性心肌病的患者(n = 41) 提高了 4.7% (p p
Improvements were more striking in the non-ischemic dilated cardiomyopathy subgroup (n = 8) in whom LVEF increased by 7.5% at 4 months (p < 0.017) and 12.2% at 12 months, from an initial 25.9% to 38.1% (p < 0.003). The increase of LVEF in non-ischemic cardiomyopathy (dLVEF%/ iLVEF%) represents an increase in cardiac function of 47.1 % at 12 months.
非缺血性擴張型心肌病亞組的改善更爲顯著(n = 8) 其中 LVEF 在 4 個月內增長了 7.5% (p p
The improvement was most marked in the patients with the most severe cardiomyopathy (LVEF < 20%), in whom there is a high risk of sudden death. In this group, the LVEF increased from 14.6% before treatment to 28.4 % at 12 months.
這種改善在最嚴重的心肌病(LVEF
Complications included one death from an unrecognized silent MI one month before treatment, 2 respiratory infections and 2 patients requiring cardioversion. There were no complications attributed to the ACP-01.
併發症包括在治療前一個月因未被識別的無症狀心肌梗死的一例死亡、兩例呼吸道感染和兩名需要心臟復律的患者。沒有可歸因於 ACP-01 的併發症。
This study was not prospective and randomized. However, in the context of 2 previous studies of cardiomyopathy patients who underwent implantation of ACP-01 on a compassionate use basis, the significant results of this study provides a compelling impetus to proceed with a Phase 2 randomised, prospective trial of ACP-01 for treatment of ischemic and non-ischemic dilated cardiomyopthy.
這項研究不是前瞻性的,是隨機的。但是,在先前對在同情心基礎上植入 ACP-01 的心肌病患者的兩項研究背景下,這項研究的顯著結果爲進行一項治療缺血性和非缺血性擴張型心肌病的 ACP-01 的 2 期隨機前瞻性試驗提供了令人信服的動力。
Published Abstract:
Methods: This IRB approved outcome analysis reports upon 74 consecutive patients who failed medical management for severe cardiomyopathy, and were selected to undergo transcatheter intramyocardial or intracoronary implantation of ACP-01. Serious adverse events (SAEs) were reported. Cell analysis was conducted for each treatment. The left ventricular ejection fraction (LVEF) was measured by multi-gated acquisition scan (MUGA) or echocardiogram at 4 (+/- 1.9) months and 12 (+/-5.5) months. Patients reported quality of life statements at 6 months (+/- 5.6 months).
Results: Fifty-four of 74 patients met requirements for inclusion (48 males , 5females; age 68.1 +/- 11.3 years).
The mean treatment cell number of 57 × 106 ACP-01 included 7.7 × 106 CD34 + cells, and 21 × 106 CD31 + cells with 97.6% viability. SAEs included one death (previously unrecognized silent MI), ventricular tachycardia (n = 2) requiring cardioversion, and respiratory infection (n = 2). LVEF in the ischemic subgroup (n = 41) improved by 4.7% (+/- 9.7) from pre-procedure to the first follow-up (4 months +/-1.9 months) (p < 0.004) and by 7.2% +/- 10.9 at final follow-up (n = 25) at average 12 months (p < 0.004). The non-ischemic dilated cardiomyopathy subgroup (n = 8) improved by 7.5% +/- 6.0 at the first follow-up (p < 0.017) and by 12.2% +/- 6.4 at final follow-up (p < 0.003, n = 6). Overall improvement in LVEF from pre-procedure to post-procedure was significant (Fisher's exact test p < 0.004). LVEF improvement was most marked in the patients with the most severe cardiomyopathy (LVEF < 20%) improving from a mean 14.6% +/-3.4% pre-procedurally to 28.4% +/- 8% at final follow-up. Quality of life statements reflected improvement in 33/50 (66%), no change in 14/50 (28%), and worsening in 3/50 (6%).
Conclusion: Transcatheter implantation of ACP-01 for cardiomyopathy is safe, and improves LVEF in the setting of ischemic and non-ischemic cardiomyopathy. The results warrant further investigation in a prospective, blinded, and controlled clinical study.
已發佈的摘要:
方法:該IRB批准的結果分析報告了連續74名因嚴重心肌病而未通過醫療管理的患者,他們被選中接受經導管心肌內或冠狀動脈內植入 ACP-01。報告了嚴重不良事件(SAE)。對每種治療進行了細胞分析。在4(+/-1.9)個月零12(+/-5.5)個月時,通過多門採集掃描(MUGA)或超聲心動圖測量了左心室射血分數(LVEF)。患者報告的生活質量報告顯示爲6個月(+/-5.6個月)。
結果: 74名患者中有54名符合納入要求(48名男性,5名女性;年齡68.1 +/-11.3歲)。
平均治療細胞數爲 57 × 106 ACP-01 包含 7.7 × 106 CD34 + 細胞,以及 21 × 106 CD31 + 細胞的存活率爲 97.6%。SAE 包括一例死亡(以前無法識別的無症狀心肌梗死)、心室性心動過速(n = 2) 需要心臟復律和呼吸道感染 (n = 2)。缺血亞組中的 LVEF (n = 41) 從術前到首次隨訪(4 個月 +/-1.9 個月)改善了 4.7%(+/-9.7)(p n = 25) 平均 12 個月 (p n = 8) 在第一次隨訪時改善了 7.5% +/-6.0 (p p n = 6)。從術前到術後,LVEF的總體改善是顯著的(費舍爾的精確測試) p 結論: 經導管植入治療心肌病的 ACP-01 是安全的,並且可以改善缺血性和非缺血性心肌病背景下的 LVEF。該結果值得在一項前瞻性、盲目和對照臨床研究中進行進一步研究。
"I want to thank the studies authors, including Jane R. Schubart, Amirhossein Zare , Roberto M. Fernandez‐de‐Castro, Hector Rosario Figueroa, Ina Sarel, Kelly Tuchman, Kaitlyn Esposito, Fraser C. Henderson Sr and Ernst von Schwarz," stated Thomas Smeenk, CEO. "This is our third peer reviewed study of heart disease (41, 106 and 53 heart patients, respectively). Completed by three independent teams, each study confirms ACP-01 is a breakthrough treatment for ischemic and non ischemic cardiomyopathy."
首席執行官托馬斯·斯梅恩克表示:“我要感謝研究的作者,包括簡·舒巴特、阿米爾侯賽因·扎爾、羅伯託·費爾南德斯·德卡斯特羅、赫克託·羅薩里奧·菲格羅亞、伊娜·薩雷爾、凱利·塔赫曼、凱特琳·埃斯波西託、老弗雷澤·亨德森和恩斯特·馮·施瓦茲。”“這是我們對心臟病的第三項同行評審研究(分別爲41、106和53名心臟病患者)。每項研究均由三個獨立小組完成,證實 ACP-01 是缺血性和非缺血性心肌病的突破性治療方法。”
Dr. Fraser Henderson Sr, Hemostemix CMO, commented: "This peer reviewed study, though not prospective or randomized, provides clear data to suggest that transcatheter implantation of ACP-01 results in a significant improvement in cardiac function, especially in those most severely debilitated with very low left ventricular ejection fractions, and in those with non-ischemic dilated cardiomyopathy."
Hemostemix 首席營銷官 Fraser Henderson Sr 博士評論說:“這項經過同行評審的研究雖然不是前瞻性的,也不是隨機的,但提供了明確的數據,表明經導管植入 ACP-01 可顯著改善心臟功能,尤其是左心室射血分數非常低的虛弱患者以及非缺血性擴張型心肌病患者。”
"The results of these three studies significantly derisk a phase II randomized clinical trial," stated Thomas Smeenk. "With it we have attracted and assembled some of the most accomplished stem cell scientists, transplant surgeons and cardiologists at the McGill University Health Center, to complete this study. That will enable Hemostemix to make ACP available in the near future to the large number of patients suffering with cardiomyopathy," Smeenk said.
托馬斯·斯梅恩克說:“這三項研究的結果顯著降低了二期隨機臨床試驗的風險。”“通過它,我們在麥吉爾大學健康中心吸引並召集了一些最有成就的幹細胞科學家、移植外科醫生和心臟病專家,來完成這項研究。這將使Hemostemix能夠在不久的將來向大量心肌病患者提供ACP,” 斯梅恩克說。
ABOUT HEMOSTEMIX
關於 HEMOSTEMIX
Hemostemix is an autologous stem cell therapy company, founded in 2003. A winner of the World Economic Forum Technology Pioneer Award, the Company has developed, patented, and is scaling a patient's blood-based stem cell therapeutics platform that includes angiogenic cell precursors, neuronal cell precursor and cardiomyocyte cell precursors. For more information, please visit .
Hemostemix 是一家自體幹細胞療法公司,成立於 2003 年。作爲世界經濟論壇技術先鋒獎的獲得者,該公司開發了包括血管生成細胞前體、神經元細胞前體和心肌細胞前體在內的患者血液基幹細胞治療平台,並正在擴大其專利。欲了解更多信息,請訪問 。
For a copy of the publication:
如需該出版物的副本:
For further information, please contact: Thomas Smeenk, President, CEO & Co-Founder
EM: tsmeenk@hemostemix.com PH: 905-580-4170
欲了解更多信息,請聯繫: Thomas Smeenk,總裁、首席執行官兼聯合創始人
EM: tsmeenk@hemostemix.com 電話:905-580-4170
Neither the TSX Venture Exchange nor its Regulation Service Provider (as that term is defined under the policies of the TSX Venture Exchange) accepts responsibility for the adequacy or accuracy of this release.
多倫多證券交易所風險交易所及其監管服務提供商(該術語由多倫多證券交易所風險交易所的政策定義)均不對本新聞稿的充分性或準確性承擔責任。
Forward-Looking Information: This news release contains "forward-looking information" within the meaning of applicable Canadian securities legislation. All statements, other than statements of historical fact, included herein are forward-looking information. In particular, this news release contains forward-looking information in relation to: financing of the Company and its lead product ACP-01, the Phase II Clinical Trial of ischemic cardiomyopathy and related results, the retrospective study of ischemic and dilated cardiomyopathy, and the commercialization of ACP-01 via the sale of compassionate treatments approved by regulators. There can be no assurance that such forward-looking information will prove to be accurate. Actual results and future events could differ materially from those anticipated in such forward-looking information. This forward-looking information reflects Hemostemix's current beliefs and is based on information currently available to Hemostemix and on assumptions Hemostemix believes are reasonable. These assumptions include, but are not limited to: the underlying value of Hemostemix and its Common Shares; the successful resolution of the litigation that Hemostemix is pursuing or defending (the "Litigation"); the results of ACP-01 research, trials, studies and analyses, including the analysis being equivalent to or better than previous research, trials or studies; the receipt of all required regulatory approvals for research, trials or studies; the level of activity, market acceptance and market trends in the healthcare sector; the economy generally; consumer interest in Hemostemix's services and products; competition and Hemostemix's competitive advantages; and Hemostemix obtaining satisfactory financing to fund Hemostemix's operations including any research, trials or studies, and any Litigation. Forward-looking information is Subject to known and unknown risks, uncertainties and other factors that may cause the actual results, level of activity, performance or achievements of Hemostemix to be materially different from those expressed or implied by such forward-looking information. Such risks and other factors may include, but are not limited to: the ability of Hemostemix to complete clinical trials, complete a satisfactory analyses and file the results of such analyses to gain regulatory approval of a phase II or phase III clinical trial of ACP-01; potential litigation Hemostemix may face; general business, economic, competitive, political and social uncertainties; general capital market conditions and market prices for securities; delay or failure to receive board or regulatory approvals; the actual results of future operations including the actual results of future research, trials or studies; competition; changes in legislation affecting Hemostemix; the timing and availability of external financing on acceptable terms; long-term capital requirements and future developments in Hemostemix's markets and the markets in which it expects to compete; lack of qualified, skilled labour or loss of key individuals; and risks related to the COVID-19 pandemic including various recommendations, orders and measures of governmental authorities to try to limit the pandemic, including travel restrictions, border closures, non-essential business closures service disruptions, quarantines, self-isolations, shelters-in-place and social distancing, disruptions to markets, disruptions to economic activity and financings, disruptions to supply chains and sales channels, and a deterioration of general economic conditions including a possible national or global recession or depression; the potential impact that the COVID-19 pandemic may have on Hemostemix which may include a decreased demand for the services that Hemostemix offers; and a deterioration of financial markets that could limit Hemostemix's ability to obtain external financing. A description of additional risk factors that may cause actual results to differ materially from forward-looking information can be found in Hemostemix's disclosure documents on the SEDAR website at . Although Hemostemix has attempted to identify important factors that could cause actual results to differ materially from those contained in forward-looking information, there may be other factors that cause results not to be as anticipated, estimated or intended. Readers are cautioned that the foregoing list of factors is not exhaustive. Readers are further cautioned not to place undue reliance on forward-looking information as there can be no assurance that the plans, intentions or expectations upon which they are placed will occur. Forward-looking information contained in this news release is expressly qualified by this cautionary statement. The forward-looking information contained in this news release represents the expectations of Hemostemix as of the date of this news release and, accordingly, it is subject to change after such date. However, Hemostemix expressly disclaims any intention or obligation to update or revise any forward-looking information, whether as a result of new information, future events or otherwise, except as expressly required by applicable securities law.
前瞻性信息:本新聞稿包含適用的加拿大證券立法所指的 “前瞻性信息”。除歷史事實陳述外,此處包含的所有陳述均爲前瞻性信息。特別是,本新聞稿包含與以下方面的前瞻性信息:公司及其主要產品 ACP-01 的融資、缺血性心肌病的二期臨床試驗及相關結果、缺血性和擴張型心肌病的回顧性研究,以及通過銷售監管機構批准的同情療法實現 ACP-01 的商業化。There 無法保證此類前瞻性信息將被證明是準確的。實際結果和未來事件可能與此類前瞻性信息中的預期存在重大差異。這些前瞻性信息反映了Hemostemix當前的信念,基於Hemostemix目前獲得的信息以及Hemostemix認爲合理的假設。這些假設包括但不限於:Hemostemix及其普通股的基本價值;Hemostemix提起或辯護的訴訟的成功解決(”訴訟“);ACP-01 研究、試驗、研究和分析的結果,包括分析等同於或優於先前的研究、試驗或研究;研究、試驗或研究所需的所有監管approvals 的收據;醫療保健行業的活動水平、市場接受度和市場趨勢;一般economy;Hemostemix 中的消費者interest服務和產品;競爭和Hemostemix 的競爭優勢;以及Hemostemix獲得令人滿意的融資, 爲Hemostemix的業務(包括任何研究、試驗或研究以及任何訴訟)提供資金。前瞻性信息受已知和未知風險、不確定性和其他因素的影響,這些因素可能導致Hemostemix的實際結果、活動水平、業績或成就與此類前瞻性信息所表達或暗示的結果存在重大差異。此類風險和其他因素可能包括但不限於:Hemostemix完成臨床試驗、完成令人滿意的分析並提交此類分析結果以獲得監管部門批准 ACP-01 的二期或三期臨床試驗的能力;Hemostemix可能面臨的潛在訴訟;一般業務、經濟、競爭、政治和社會的不確定性;一般資本市場狀況和證券市場價格;延遲或未能獲得董事會或監管機構的批准;未來運營的實際結果,包括未來研究、試驗或研究的實際結果;競爭;立法變化affecting Hemostemix;在可接受條件下外部融資的時機和可用性;Hemostemix市場及其預期競爭市場的長期資本要求和未來發展; 缺乏合格熟練勞動力或關鍵人員流失;以及風險related 到 COVID-19 疫情,包括政府當局向try 提出的限制疫情的各種建議、命令和措施,包括旅行限制、邊境關閉、非必要企業關閉、服務中斷、隔離、自我隔離、就地避難和保持社交距離、市場中斷、經濟活動中斷以及financings,供應鏈和銷售渠道中斷,總體經濟狀況惡化,包括possible 全國或全球衰退或蕭條;COVID-19 疫情可能對Hemostemix產生的潛在影響,其中可能包括對Hemostemix提供的服務的需求減少;以及金融市場的惡化可能限制Hemostemix獲得外部融資的能力。有關可能導致實際業績與前瞻性信息存在重大差異的其他風險因素的描述,可在SEDAR網站上Hemostemix的披露文件中找到,網址爲。儘管Hemostemix試圖確定可能導致實際結果與前瞻性信息中包含的結果存在重大差異的重要因素,但可能還有其他因素導致結果與預期、估計或預期的結果不符。請讀者注意,上述因素清單並不詳盡。還提醒讀者不要過分依賴前瞻性信息,因爲無法保證他們所依據的計劃、意圖或期望會實現。本警示聲明明確限制了本新聞稿中包含的前瞻性信息。本新聞稿中包含的前瞻性信息代表了Hemostemix截至本新聞發佈之日的預期,因此,在此日期之後可能會發生變化。但是,除非適用的證券法明確要求,否則Hemostemix明確表示不打算或承擔任何更新或修改任何前瞻性信息的意圖或義務,無論這些信息是由於新信息、未來事件還是其他原因造成的。
To view the source version of this press release, please visit
要查看本新聞稿的源版本,請訪問
譯文內容由第三人軟體翻譯。