Hepion Pharmaceuticals Announces Publication of Phase 2a ‘AMBITION’ Clinical Trial Results
Hepion Pharmaceuticals Announces Publication of Phase 2a ‘AMBITION’ Clinical Trial Results
- Study met safety, tolerability, and pharmacokinetics primary endpoints -
-研究符合安全性、耐受性和药代动力学主要终点-
- Reductions in ALT, ProC3, and C6M suggest direct antifibrotic effects with longer treatment duration -
-ALT、ProC3和C6M的减少表明,治疗持续时间更长,具有直接的抗纤维化作用-
- Enrollment initiated in Phase 2b 'ASCEND-NASH' trial evaluating the safety and efficacy of rencofilstat in 336 biopsy confirmed F2 / F3 NASH subjects -
--在2b阶段的“Ascend-Nash”试验中开始登记,评估336名活检确诊的F2/F3 NASH受试者中使用rencofilstat的安全性和有效性。
EDISON, N.J., Oct. 26, 2022 (GLOBE NEWSWIRE) -- Hepion Pharmaceuticals, Inc. (NASDAQ:HEPA), a clinical stage biopharmaceutical company focused on Artificial Intelligence ("AI")-driven therapeutic drug development for the treatment of fibrotic diseases, including non-alcoholic steatohepatitis ("NASH"), hepatocellular carcinoma ("HCC"), and other chronic liver diseases, today announced that the peer-reviewed journal, Hepatology Communications, has published a paper by Harrison et al. entitled, "Rencofilstat, a cyclophilin inhibitor: A phase 2a, multicenter, single-blind, placebo-controlled study in F2/F3 NASH," reviewing the results of Hepion's 'AMBITION' clinical trial.
新泽西州爱迪生,2022年10月26日(环球网)--赫平制药公司(纳斯达克:HEPA)是一家临床阶段的生物制药公司,专注于人工智能(AI)驱动的治疗药物开发,用于治疗纤维化疾病,包括非酒精性脂肪性肝炎(NASH)、肝细胞癌(肝癌)和其他慢性肝病。《肝病通讯》发表了哈里森等人的一篇论文。题为“Rencofilstat,一种亲环素抑制剂:F2/F3 NASH中的2a期多中心、单盲、安慰剂对照研究”,回顾了赫平公司的“雄心”临床试验的结果。
The Phase 2a, multicenter, single-blind, placebo-controlled study randomized 49 presumed F2/F3 NASH subjects to receive either 75 mg or 225 mg of rencofilstat, or placebo, once daily for 28 days. The aim of the study was to determine safety, tolerability, and pharmacokinetics, while exploring NASH efficacy biomarkers, including multi-omic and AI-POWR™ analyses.
这项2a阶段的多中心、单盲、安慰剂对照研究随机选择了49名F2/F3 NASH受试者,让他们每天服用75 毫克或225毫克的瑞可非司坦,或安慰剂,共28 天。该研究的目的是确定安全性、耐受性和药代动力学,同时探索纳什疗效生物标记物,包括多组学和AI-POWR™分析。
As previously reported, the AMBITION clinical trial demonstrated rencofilstat was safe and well tolerated. A majority of subjects (28/47; 59.6%) who were dosed with rencofilstat, or placebo experienced no adverse events. Of the 36 adverse events recorded in total, 97.2% were graded as mild to moderate, none were serious, and the majority (27/36; 75%) were considered unrelated to administration of rencofilstat. Additionally, blood concentrations of rencofilstat in the NASH subjects were similar to those observed previously in healthy subjects.
正如之前报道的那样,Ambition临床试验证明瑞可非司特是安全的,耐受性良好。服用瑞可非司坦或安慰剂的大多数受试者(28/47;59.6%)没有发生不良事件。在总共记录的36个不良事件中,97.2%被评级为轻度至中度,没有严重,大多数(27/36;75%)被认为与瑞可非司坦的使用无关。此外,NASH受试者的血药浓度与先前在健康受试者中观察到的相似。
The reductions in alanine transaminase ("ALT"), a biomarker of liver damage, were greater in the rencofilstat arms versus the placebo groups and was statistically different in the 225-mg cohort compared to the placebo cohort (−16.3 ± 25.5% versus −0.7 ± 13.4%, respectively). Reductions in Pro-C3, a biomarker of collagen formation and fibrosis, and C6M, a biomarker of tissue remodeling, were statistically significant in rencofilstat subjects with baseline Pro-C3 levels above 15.0 ng/mL. Pro-C3 levels greater than 15-20 ng/mL are generally accepted to represent active NASH disease and a marker of fibrosis in the primary patient population for treatment by many NASH drug candidates. The paper concluded that the reductions in ALT, Pro-C3, and C6M suggest that rencofilstat has direct antifibrotic effects with longer treatment duration, supporting the advancement of rencofilstat into a larger and longer Phase 2b study.
肝损伤的生物标志物丙氨酸氨基转移酶(“ALT”)的降幅在瑞可司坦组比安慰剂组更大,225毫克组与安慰剂组相比有统计学差异(−分别为16.3 ± 25.5%和−0.7 ± 13.4%)。Pro-C3是胶原形成和纤维化的生物标志物,C6M是组织重塑的生物标志物,在基线Pro-C3水平高于15.0 ng/mL的受试者中,Pro-C3和C6M的减少具有统计学意义。Pre-C3水平高于15-20 ng/ml被普遍认为是活动性NASH病的代表,也是许多NASH候选药物治疗的主要患者群体中纤维化的标志。这篇论文的结论是,ALT、Pro-C3和C6M的降低表明瑞可非司特具有直接的抗纤维化作用,治疗时间更长,支持肾可非司特进入更大规模和更长时间的2b期研究。
"The findings of this paper further strengthen the rationale behind our ongoing Phase 2b 'ASCEND-NASH' trial, which initiated screening at the end of August," said Robert Foster, PharmD, PhD, CEO of Hepion. "The degree of decline in Pro-C3 observed in the AMBITION trial, which had a duration of only 28 days, was comparable to Pro-C3 declines seen in similar studies with durations of several months, particularly in subjects with Pro-C3 levels indicating more advanced disease. Given this observation, we are very much looking forward to seeing the magnitude of rencofilstat's antifibrotic effects over a 12-month-period in our ongoing Phase 2b trial."
“这篇论文的发现进一步加强了我们正在进行的2b期‘Ascend-Nash’试验背后的理由,该试验于8月底开始筛查,”赫皮恩公司首席执行官、制药博士罗伯特·福斯特说。在仅持续28天的Ambition试验中观察到的Pro-C3下降的程度与类似研究中持续几个月的Pro-C3下降的程度相当,特别是在Pro-C3水平表明疾病更晚期的受试者中。鉴于这一观察,我们非常期待在我们正在进行的2b阶段试验中看到12个月内Rencofilstat的抗纤维化作用的幅度。
The article may be accessed at:
这篇文章可以在以下网站上访问:
About Hepion Pharmaceuticals
关于赫皮恩制药公司
The Company's lead drug candidate, rencofilstat, is a potent inhibitor of cyclophilins, which are involved in many disease processes. Rencofilstat is currently in clinical-phase development for the treatment of NASH, with the potential to play an important role in the overall treatment of liver disease - from triggering events through to end-stage disease. Rencofilstat has been shown to reduce liver fibrosis and hepatocellular carcinoma tumor burden in experimental models of NASH, and has demonstrated antiviral activities towards HBV, HCV, and HDV through several mechanisms, in nonclinical studies. In November 2021, the U.S. Food and Drug Administration ("FDA") granted Fast Track designation for rencofilstat for the treatment of NASH. That was followed in June 2022 by the FDA's granting of Orphan Drug designation to rencofilstat for the treatment of HCC.
该公司的主要候选药物rencofilstat是亲环素的有效抑制剂,亲环素参与许多疾病的过程。Rencofilstat目前正处于治疗NASH的临床开发阶段,有可能在肝病的整体治疗中发挥重要作用-从引发事件到终末期疾病。在NASH的实验模型中,瑞可非司特已被证明可以减轻肝纤维化和肝细胞癌的肿瘤负担,并在非临床研究中通过几种机制显示了对乙肝病毒、丙型肝炎病毒和HDV的抗病毒活性。2021年11月,美国食品和药物管理局(FDA)批准了治疗NASH的瑞可非司坦的快速通道指定。紧随其后的是2022年6月FDA授予Rencofilstat治疗肝癌的孤儿药物名称。
Hepion has created a proprietary AI platform, called AI-POWR™, which stands for Artificial Intelligence - Precision Medicine; Omics (including genomics, proteomics, metabolomics, transcriptomics, and lipidomics); World database access; and Response and clinical outcomes. Hepion intends to use AI-POWR™ to help identify which NASH patients will best respond to rencofilstat, potentially shortening development timelines and increasing the delta between placebo and treatment groups. In addition to using AI-POWR™ to drive its ongoing NASH clinical development program, Hepion intends to use the platform to identify additional potential indications for rencofilstat to expand the company's footprint in the cyclophilin inhibition therapeutic space.
赫皮翁创建了一个专有的人工智能平台,名为AI-POWR™,意思是A人工智能-P累进医学;OMICs(包括基因组学、蛋白质组学、代谢组学、转录组学和脂类组学);W世界数据库访问;以及R反应和临床结果。HEPION打算使用AI-POWR™来帮助确定哪些NASH患者对Rencofilstat的反应最好,这可能会缩短开发时间线,并增加安慰剂组和治疗组之间的差值。除了使用AI-POWR™来推动其正在进行的NASH临床开发计划外,赫世安还打算利用该平台为Rencofilstat确定更多的潜在适应症,以扩大该公司在亲环素抑制治疗领域的足迹。
Forward-Looking Statements
前瞻性陈述
Certain statements in this press release are forward-looking within the meaning of the Private Securities Litigation Reform Act of 1995. These statements may be identified by the use of forward-looking words such as "anticipate," "believe," "forecast," "estimated," and "intend," among others. These forward-looking statements are based on Hepion Pharmaceuticals' current expectations and actual results could differ materially. There are a number of factors that could cause actual events to differ materially from those indicated by such forward-looking statements. These factors include, but are not limited to, substantial competition; our ability to continue as a going concern; our need for additional financing; uncertainties of patent protection and litigation; risks associated with delays, increased costs and funding shortages caused by the COVID-19 pandemic; uncertainties with respect to lengthy and expensive clinical trials, that results of earlier studies and trials may not be predictive of future trial results; uncertainties of government or third party payer reimbursement; limited sales and marketing efforts and dependence upon third parties; and risks related to failure to obtain FDA clearances or approvals and noncompliance with FDA regulations. As with any drug candidates under development, there are significant risks in the development, regulatory approval, and commercialization of new products. There are no guarantees that future clinical trials discussed in this press release will be completed or successful, or that any product will receive regulatory approval for any indication or prove to be commercially successful. Hepion Pharmaceuticals does not undertake an obligation to update or revise any forward-looking statement. Investors should read the risk factors set forth in Hepion Pharmaceuticals' Form 10-K for the year ended December 31, 2021, and other periodic reports filed with the Securities and Exchange Commission.
本新闻稿中的某些陈述属于1995年《私人证券诉讼改革法》所指的前瞻性陈述。这些陈述可以通过使用“预期”、“相信”、“预测”、“估计”和“打算”等前瞻性词汇来识别。这些前瞻性陈述是基于赫平制药公司目前的预期,实际结果可能与此大不相同。有许多因素可能导致实际事件与这些前瞻性陈述所表明的情况大不相同。这些因素包括但不限于:激烈的竞争;持续经营的能力;额外融资的需求;专利保护和诉讼的不确定性;与新冠肺炎疫情导致的延迟、成本增加和资金短缺相关的风险;早期研究和试验结果可能无法预测未来试验结果的不确定性;政府或第三方付款人偿付款项的不确定性;销售和营销努力有限及对第三方的依赖;以及未能获得美国食品和药物管理局的批准和批准以及不遵守美国食品和药物管理局的监管规定相关的风险。与任何正在开发的候选药物一样,新产品的开发、监管批准和商业化存在重大风险。不能保证本新闻稿中讨论的未来临床试验将完成或成功,也不能保证任何产品的任何适应症都将获得监管部门的批准或被证明是商业上的成功。赫皮恩制药公司不承担更新或修改任何前瞻性陈述的义务。投资者应阅读赫平制药公司截至2021年12月31日的10-K表格中列出的风险因素, 以及提交给美国证券交易委员会的其他定期报告。
For further information, please contact:
如需更多信息,请联系:
Stephen Kilmer
Hepion Pharmaceuticals Investor Relations
Direct: (646) 274-3580
skilmer@hepionpharma.com
斯蒂芬·基尔默
赫皮恩制药公司投资者关系
直拨:(646)274-3580
邮箱:skilmer@hepopharma.com