Pasithea Therapeutics Announces Results of Preclinical Study Demonstrating Tolerizing Vaccine Efficacy in Relapsing-Remitting Model of Multiple Sclerosis
Pasithea Therapeutics Announces Results of Preclinical Study Demonstrating Tolerizing Vaccine Efficacy in Relapsing-Remitting Model of Multiple Sclerosis
-- PAS002 is a proprietary DNA tolerizing vaccine construct encoding GlialCAM --
-- PAS002 effectively reduces disease severity, delays onset of illness, while also reducing relapse severity --
-- GlialCAM fragment is present in monkeypox virus, supporting a potential role in current vaccine development --
--PAS002是一种编码GlialCAM的专有DNA耐受疫苗构造--
--PAS002有效地降低了疾病的严重程度,推迟了疾病的发病,同时还降低了复发的严重程度--
--猴痘病毒中存在GlialCAM片段,支持在当前疫苗开发中发挥潜在作用--
MIAMI BEACH, Fla., Aug. 11, 2022 (GLOBE NEWSWIRE) -- Pasithea Therapeutics Corp. (Nasdaq: KTTA) ("Pasithea" or the "Company"), a biotechnology company focused on the discovery, research and development of new and effective treatments for psychiatric and neurological disorders, today announced positive results from a preclinical proof of concept study of PAS002, its tolerizing vaccine program in multiple sclerosis ("MS").
环球通讯社佛罗里达州迈阿密海滩,2022年8月11日-专注于发现、研究和开发治疗精神和神经疾病的新型有效疗法的生物技术公司Pasithea Treateutics Corp.(纳斯达克代码:KTTA)今天宣布,其治疗多发性硬化症(MS)的耐受性疫苗计划PAS002的临床前概念验证研究取得了积极结果。
Earlier this year, a study in Nature, the world's leading science journal, showed that a molecule called GlialCAM found in the brain's white matter is attacked in MS. GlialCAM shares a component of its protein structure that mimics an identical component of the Epstein Barr Virus ("EBV") Nuclear Antigen-1, which plays a critical role in triggering MS.
今年早些时候,世界领先的科学杂志《自然》上的一项研究表明,在大脑白质中发现的一种名为GlialCAM的分子受到了攻击,GlialCAM与其蛋白质结构中的一个成分相似,该成分与爱泼斯坦-巴尔病毒(EBV)核抗原-1的成分相同,后者在引发多发性硬化症中起着关键作用。
In this proof of concept study, relapsing paralysis was established in a mouse model of relapsing-remitting experimental autoimmune encephalomyelitis ("EAE"), the standard animal model of MS. In three groups, a proprietary DNA cassette was engineered to encode GlialCAM and injected to potentially block acute disease and its relapse. These DNA molecules were designed to protect against paralytic disease by tolerizing the immune system so it would not attack myelin in the brain and spinal cord. The engineered DNA molecule creates tolerance, working like an 'inverse vaccine', and was administered intra-muscularly at days 0, 3, 7, 10, and 14. The study had a standard duration of 32 days.
在这项概念验证研究中,在复发-缓解性实验性自身免疫性脑脊髓炎(“EAE”)的小鼠模型上建立了复发性瘫痪,EAE是MS的标准动物模型。在三组中,设计了一种专有的DNA盒来编码GlialCAM并注射,以潜在地阻止急性疾病及其复发。这些DNA分子被设计成通过耐受免疫系统来预防瘫痪疾病,这样它就不会攻击大脑和脊髓中的髓鞘。这种经过改造的DNA分子可以产生耐受性,就像一种“反向疫苗”,在第0天、第3天、第7天、第10天和第14天肌肉注射。这项研究的标准持续时间为32天。
The data showed that the engineered DNA plasmids provide a high level of efficacy in reducing disease severity and incidence of relapse when administered prophylactically in the EAE model, a widely used relapsing-remitting model of MS.
数据显示,当在广泛使用的MS复发-缓解模型EAE模型中预防性给药时,工程DNA质粒在降低疾病严重性和复发率方面提供了高水平的疗效。
Key findings from the study include:
这项研究的主要发现包括:
- treatment with a DNA tolerizing 'inverse vaccine' delayed the onset of paralysis when compared to vehicle (p<0.001);
- a statistically significant reduction in disease severity, when compared to vehicle (p=0.002);
- a statistically significant reduction in relapse severity, when compared to vehicle (p<0.001);
- treatment with a DNA vaccine prevented disease in approximately 50% of the mice, when compared to vehicle (p=0.004).
- 与赋形剂相比,耐受DNA反向疫苗的治疗延迟了瘫痪的发生(p
- 与车辆相比,疾病严重程度在统计学上显著降低(p=0.002);
- 与Vehicle相比,复发严重程度在统计上显著降低(p
- 与使用药物相比,使用DNA疫苗治疗可以预防大约50%的小鼠的疾病(p=0.004)。
The study was conducted at Hooke Laboratories, an independent full-service Contract Research Organization with deep experience in the EAE animal model of MS.
这项研究是在胡克实验室进行的,这是一家独立的全方位服务合同研究机构,在MS的EAE动物模型方面拥有丰富的经验。
"The results of this study show that this technology has the potential to tolerize to GlialCAM, a myelin molecule that has molecular similarity to the Epstein Barr Virus that triggers MS," stated Pasithea's Chairman, National Academy of Sciences Professor Lawrence Steinman, a world recognized leading authority in MS. Prof. Steinman's research led to the development of the drug Tysabri, which is approved to treat patients with MS and Crohn's disease. "Remarkably, the piece of GlialCAM protein shared between EBV and white matter in the brain is also found in the pox viruses, including monkeypox. Monkeypox is rarely associated with brain inflammation, and this new technology may prove useful as a treatment for brain inflammation caused in certain viral infections."
Pasithea主席、国家科学院主席劳伦斯·斯坦曼教授说:“这项研究的结果表明,这项技术有可能耐受GlialCAM,这是一种与引发多发性硬化症的爱泼斯坦-巴尔病毒具有分子相似性的髓鞘分子。”斯坦曼教授是世界公认的领先权威,他的研究导致了药物Tysabri的开发,该药物被批准用于治疗多发性硬化症和克罗恩病患者。值得注意的是,EB病毒和大脑中白质共享的GlialCAM蛋白片段也在猴痘病毒中发现。猴痘病毒很少与脑部炎症有关,这项新技术可能会被证明对治疗某些病毒感染引起的脑部炎症很有用。
Dr. Tiago Reis Marques, Chief Executive Officer of Pasithea, stated, "We're thrilled with the strong preclinical efficacy data shown in this study. Although early stage, we believe these results demonstrate the promise and validity of our tolerizing approach, which is built on recent data on the biological mechanism linking infection with EBV with the development of MS. We have filed a provisional patent application and we will continue to rapidly pursue the PAS002 drug development program."
Pasithea公司首席执行官蒂亚戈·里斯·马奎斯博士说:“我们对这项研究中显示的强大的临床前疗效数据感到兴奋。虽然还处于早期阶段,但我们相信这些结果证明了我们耐受性方法的前景和有效性,这种方法建立在有关EB病毒感染与多发性硬化症发病之间的生物学机制的最新数据的基础上。我们已经提交了临时专利申请,我们将继续快速推进PAS002药物开发计划。”
The Company plans to present data from this study, including histology data and plasma inflammatory markers, in future major international conferences, and also to submit full data for peer-review publication.
该公司计划在未来的主要国际会议上公布这项研究的数据,包括组织学数据和血浆炎症标志物,并提交完整的数据供同行评审发表。
About Multiple Sclerosis
关于多发性硬化症
Multiple Sclerosis ("MS") is a chronic and potentially disabling autoimmune disease, and the most common neurodegenerative disease of the central nervous system in young adults. The pathological hallmark of MS is the formation of demyelinating lesions in the brain and spinal cord, with the immune system attacking the myelin sheath that normally protects nerve fibers in the brain, spinal cord, and optic nerve. There are now 2.8 million people worldwide who have MS, and every five minutes, someone, somewhere in the world is diagnosed with this disorder. While there is no way to predict with any certainty how an individual's disease will progress, four basic MS disease courses (also called types or phenotypes) have been defined: clinically isolated syndrome, relapsing remitting, secondary progressive and primary progressive. The most common affecting around 85 per cent of everyone diagnosed with MS is relapsing remitting MS (RRMS). It means that symptoms appear (a relapse), and then fade away, either partially or completely (remitting).
多发性硬化症(MS)是一种慢性的、可能致残的自身免疫性疾病,也是年轻人最常见的中枢神经系统退行性疾病。多发性硬化症的病理特征是在大脑和脊髓形成脱髓鞘病变,免疫系统攻击通常保护大脑、脊髓和视神经的髓鞘。现在全世界有280万人患有多发性硬化症,每五分钟,世界上某个地方的某个人就会被诊断出患有这种疾病。虽然没有办法确切地预测一个人的疾病将如何发展,但已经定义了四种基本的MS疾病病程(也称为类型或表型):临床孤立综合征、复发缓解、继发性进展性和原发进展性。最常见的影响大约85%被诊断为多发性硬化症的人是复发缓解性多发性硬化症(RRMS)。这意味着症状出现(复发),然后消失,部分或完全(缓解)。
ABOUT PAS002
关于PAS002
PAS002 is an engineered DNA plasmid designed to tolerize the immune system to GlialCAM.
PAS002是一种设计用于耐受GlialCAM的免疫系统的工程DNA质粒。
About Pasithea Therapeutics Corp.
Pasithea治疗公司简介
Pasithea Therapeutics Corporation is a U.S. biotechnology company focused on the discovery, research and development of new and effective treatments for psychiatric and neurological disorders. With an experienced team of experts in the fields of neuroscience and psychopharmacology, Pasithea is developing new molecular entities for the treatment of psychiatric and neurological disorders. Pasithea is also focused on addressing the needs of patients currently suffering with mental illness by providing access to IV ketamine infusions both in clinics and in-home settings.
Pasithea治疗公司是一家美国生物技术公司,专注于发现、研究和开发治疗精神和神经疾病的新的有效疗法。Pasithea拥有一支在神经科学和精神药理学领域经验丰富的专家团队,正在开发用于治疗精神和神经疾病的新分子实体。Pasithea还专注于通过在诊所和家庭环境中提供静脉注射氯胺酮来满足目前患有精神疾病的患者的需求。
Forward Looking Statements
前瞻性陈述
This press release contains statements that constitute "forward-looking statements." Forward-looking statements are subject to numerous conditions, many of which are beyond the control of the Company. While the Company believes these forward-looking statements are reasonable, undue reliance should not be placed on any such forward-looking statements, which are based on information available to the Company on the date of this release. These forward-looking statements are based upon current estimates and assumptions and are subject to various risks and uncertainties, including, without limitation, those set forth in the Company's filings with the SEC. Thus, actual results could be materially different. The Company undertakes no obligation to update these statements whether as a result of new information, future events or otherwise, after the date of this release, except as required by law.
本新闻稿包含构成“前瞻性陈述”的陈述。前瞻性陈述受许多条件的制约,其中许多条件不在公司的控制范围之内。虽然公司相信这些前瞻性陈述是合理的,但不应过度依赖任何此类前瞻性陈述,这些前瞻性陈述是基于公司在本新闻稿发布之日所掌握的信息。这些前瞻性陈述是基于当前的估计和假设,会受到各种风险和不确定性的影响,包括但不限于公司提交给美国证券交易委员会的报告中陈述的风险和不确定性。因此,实际结果可能会有很大不同。除法律要求外,本公司不承担在本新闻稿发布之日后因新信息、未来事件或其他原因而更新这些陈述的义务。
Pasithea Therapeutics Corp. Company Contact
Dr. Tiago Reis Marques
Chief Executive Officer
E: tiago@pasithea.com
Pasithea治疗公司联系人
蒂亚戈·里斯·马奎斯博士
首席执行官
电子邮件:tiago@pasithea.com
Pasithea Therapeutics Corp. Investor Relations
Lisa M. Wilson
In-Site Communications, Inc.
T: 212-452-2793
E: lwilson@insitecony.com
Pasithea治疗公司投资者关系
丽莎·M·威尔逊
现场通信公司
T: 212-452-2793
电子邮箱:lwilson@insiteconi.com