Thiogenesis Announces Positive Results from Phase 1 Dose-Escalation Study of its Lead Compound TTI-0102
Thiogenesis Announces Positive Results from Phase 1 Dose-Escalation Study of its Lead Compound TTI-0102
- Data demonstrates potential for less frequent drug administration
- TTI-0102 was well tolerated with no Serious Adverse Events reported
- Supports EU and US regulatory submissions for human efficacy trials in multiple disease indications
- 数据显示了降低给药频率的潜力
- TTI-0102耐受性良好,没有严重不良事件报告
- 支持欧盟和美国监管机构提交多个疾病适应症的人类功效试验
San Diego, California--(Newsfile Corp. - May 18, 2022) - Thiogenesis Therapeutics, Corp. (TSXV: TTI) ("Thiogenesis" or the "Company") a clinical-stage biotechnology company developing sulfur-containing therapeutics for serious pediatric diseases, today announces positive results from its Phase 1 clinical study of oral TTI-0102 in healthy volunteers in Australia.
加利福尼亚州圣地亚哥-(Newsfile Corp.-2022年5月18日)-硫化疗法公司(多伦多证券交易所股票代码:TTI)(“硫化”或“公司”)一家临床阶段的生物技术公司为严重的儿科疾病开发含硫疗法,该公司今天宣布,其在澳大利亚健康志愿者身上进行的口服TTI-0102的第一阶段临床研究取得了积极结果。
The Phase 1, "Open-Label, Dose-Escalation Study - to Evaluate Safety, Tolerability and Pharmacokinetics of Oral TTI-0102 Compared to Cystagon® (cysteamine bitartrate) in Healthy Volunteers," demonstrated that TTI-0102, which acts as a precursor to the thiol-active compound cysteamine, was safe and well tolerated at dose levels ranging from 600 mg cysteamine-base equivalent to 2400 mg cysteamine-base equivalent with no serious adverse events. The pharmacokinetic (PK) profile suggests the potential for once-a-day dosing at target therapeutic levels compared to four times a day dosing with Cystagon®.
第一阶段,“开放标签、剂量递增研究--评价口服TTI-0102与Cystagon的安全性、耐受性和药代动力学® (半胱胺重酒石酸盐)在健康志愿者中,结果表明,作为硫醇活性化合物半胱胺前体的TTI-0102在剂量水平上是安全和耐受性良好的,剂量范围从600毫克半胱胺当量到2400毫克半胱胺碱当量,没有严重的不良反应。药代动力学(PK)分析表明,与一天四次给药相比,一天一次给药达到目标治疗水平的可能性。®.
The results from this study will be used to support Thiogenesis' Investigational Medicinal Product Dossier (IMPD) submission in Europe and its Investigational New Drug (IND) submissions in the US for human efficacy trials in multiple disease indications.
这项研究的结果将被用来支持Thienetic公司在欧洲提交的研究药品档案(IMPD)和在美国提交的用于多种疾病适应症的人类疗效试验的研究新药(IND)。
"We are very encouraged with the results of our Phase 1 study exhibiting no serious adverse events for TTI-0102, even at the maximum dosage," said Patrice Rioux, M.D., Thiogenesis' Founder and Chief Executive Officer. "Cysteamine has been studied as a compound with significant promise in a number of indications over several decades, however, its development has been constrained due to its dose-limiting side effects, most notably nausea."
“我们感到非常鼓舞的是,我们的第一阶段研究结果显示,即使在最大剂量下,TTI-0102也没有严重的不良反应,”Thigenation的创始人兼首席执行官帕特里斯·里乌克斯医学博士说。几十年来,半胱胺作为一种化合物在许多适应症中都被作为一种具有重要前景的化合物进行了研究,然而,由于其剂量限制的副作用,最明显的是恶心,其开发一直受到限制。
Dr. Rioux continued, "These PK results demonstrate that TTI-0102 can significantly increase dosing and achieve a higher blood level "area under the curve" (AUC) of the active compound, without increasing its peak concentration or Cmax. The peak Cmax of cysteamine is typically correlated with the timing of its debilitating side effects. With this promising PK data, we intend to submit for regulatory clearance to initiate human efficacy trials with TTI-0102 in mitochondrial disease and Rett's syndrome."
Rioux博士继续说:“这些PK结果表明,TTI-0102可以显著增加剂量,并实现更高的血液水平活性化合物的曲线下面积(AUC),如果没有增加其峰值浓度或Cmax。半胱胺的峰值Cmax通常与其衰弱副作用的出现时间相关。有了这些有希望的PK数据,我们打算申请监管部门批准,启动TTI-0102治疗线粒体疾病和雷特氏综合症的人类疗效试验。“
Summary of TTI-0102 Phase 1 Clinical Trial Data
TTI-0102一期临床试验数据摘要
Trial Design
试行设计
The Phase 1 study enrolled 12 healthy volunteers that were dosed with 600 mg of Cystagon® as a control and patients were later given one of: 600 mg cysteamine-base equivalent; 1200 mg cysteamine-base equivalent; or 2400 mg cysteamine-base equivalent of TTI-0102.
这项第一阶段的研究招募了12名健康志愿者,他们服用了600毫克的胱氨酮® 作为对照,患者随后给予以下一种:600毫克半胱胺当量;1200毫克半胱胺当量;或2400毫克半胱胺当量TTI-0102。
Safety
安全问题
As expected, the most common Treatment Emergent Adverse Effects (TEAEs) reported following the administration of 600 mg of Cystagon® was nausea. Following TTI-0102 administration, no nausea was reported, and the only moderately graded TEAE reported was abnormal skin odor in 3 participants in the 2400 mg cysteamine-base equivalent group.
正如预期的那样,报告的最常见的治疗紧急不良反应(TEAE)是在注射600毫克Cystagon之后® 就是恶心。在服用TTI-0102后,没有恶心的报告,唯一报告的中度TEAE是2400毫克半胱胺等效组中3名参与者的异常皮肤气味。
PK Profile
主键配置文件
The target therapeutic levels of cysteamine for TTI-0102 in the 1200 mg cysteamine-base equivalent group was maintained for over 12 hours, therefore TTI-0102's PK data supports dosing twice-a-day and potentially once a day, depending on the indication.
在相当于1200毫克半胱胺的组中,TTI-0102的半胱胺目标治疗水平保持了12小时以上,因此TTI-0102的PK数据支持一天两次,也可能一天一次,具体取决于适应症。
The Cmax of cysteamine with dosing of 600 mg of Cystagon® was 3.19 ± 1.12 mg/mL compared to 3.49 ± 0.95 mg/mL with dosing of 2400 mg cysteamine-base equivalent of TTI-0102. The difference was not statistically significant (p=0.61) even at the maximum dose of TTI-0102. These results support the ability to administer a higher dose level of TTI-0102 without risking a higher Cmax of cysteamine that is associated with side effects.
600 mg半胱氨酸半胱胺的Cmax® 为3.19±1.12 mg/mL,与2400 mg半胱胺基当量TTI-0102的3.49±0.95 mg/mL相比。即使在TTI-0102的最大剂量下,差异也没有统计学意义(p=0.61)。这些结果支持了给予更高剂量水平的TTI-0102的能力,而不会冒着与副作用相关的半胱胺更高Cmax的风险。
The AUC for the dosing of 600 mg of Cystagon® was 7.32 ± 1.76 hr.mg/mL compared to 20.38 ± 4.27 hr.mg/mL for the 2400 mg cysteamine-base equivalent in the TTI-0102 group. The increase in the AUC was statistically significant, representing an increase of 278% (p<0.01).
600 mg胱氨酮剂量的AUC® TTI-0102组为7.32±1.76小时/毫升,而TTI-0102组为20.38±4.27小时/毫升。AUC的增加具有统计学意义,增加了278%(p
The higher blood level AUC achieved without increasing the Cmax results in an increase in the availability of TTI-0102 to tissue over time, again without an increase in the side effects associated with increased dosing of cysteamine.
在没有增加Cmax的情况下,较高的血液AUC水平导致TTI-0102在组织中的利用率随着时间的推移而增加,同样不会增加与增加半胱胺剂量相关的副作用。
About TTI-0102
关于TTI-0102
Thiogenesis' lead compound, TTI-0102, is an asymmetric disulfide that acts as a precursor to the thiol-active compound cysteamine; it also has additional therapeutic properties that may provide therapeutic advantages over cysteamine. Importantly, TTI-0102 is a new chemical entity (NCE), with an initial US patent granted in November 2021 and additional US and international patents pending. Thiols are versatile bio-active molecules that are known to be involved in a number of chemical reactions and metabolic processes making them exciting candidates for a number of therapeutic applications.
硫化作用的先导化合物TTI-0102是一种不对称的二硫化物,它是硫醇活性化合物半胱胺的前体;它还具有其他治疗特性,可能会提供比半胱胺更好的治疗优势。重要的是,TTI-0102是一种新的化学实体(NCE),最初的美国专利于2021年11月授予,其他美国和国际专利正在申请中。硫醇是一种多功能的生物活性分子,已知参与了许多化学反应和代谢过程,使它们成为许多治疗应用的候选对象。
As an asymmetric disulfide, TTI-0102 consists of two different thiol molecules that have been synthesized into a single compound; the molecules are cysteamine and pantetheine (both contain an active functional R-SH group where the S represents sulfur). TTI-0102 transforms into two active cysteamine molecules in two different steps:
作为一种不对称二硫化物,TTI-0102由两个不同的硫醇分子组成,这两个不同的硫醇分子被合成成一个单一的化合物;这两个分子是半胱胺和泛氨酸(两者都包含一个活性的R-SH基团,其中S代表硫)。TTI-0102通过两个不同的步骤转化为两个活性半胱胺分子:
- First, TTI-0102 is taken orally and as TTI-0102 passes through the gastrointestinal tube it interacts with other thiols, this causes the initial cysteamine molecule to be released.
- Second, the remaining pantetheine molecule moves along to the small intestine, where it comes into contact with certain enzymes (Vanin-1) that hydrolyze it into another cysteamine molecule and pantothenic acid (Vitamin B5).
- 首先,TTI-0102是口服的,当TTI-0102通过胃肠道时,它与其他硫醇相互作用,这导致最初的半胱胺分子被释放。
- 其次,剩下的泛氨酸分子沿着小肠移动,在那里它与某些酶(Vanin-1)接触,这些酶将其水解成另一种半胱胺分子和泛酸(维生素B5)。
This two-stage process occurs over a period of several hours, it is this process that caps the Cmax of cysteamine, extends the duration of the therapeutic levels of TTI-0102 and expands the AUC.
这个两个阶段的过程发生在几个小时的时间内,正是这个过程限制了半胱胺的Cmax,延长了TTI-0102的治疗水平的持续时间,并扩大了AUC。
Potential indications for TTI-0102 as a therapeutic, based on its versatile chemistry as a thiol-active compound:
TTI-0102作为治疗药物的潜在适应症,基于其作为硫醇活性化合物的多种化学成分:
| Mechanism of Action | Indications |
| Increases glutathione - antioxidant | MELAS, Huntington's, Rett's, and NASH |
| Increases Taurine - cytoprotective | MELAS, Huntington's, Rett's, CNS, TBI |
| Promotes BDNF | Huntington's, Rett's, Parkinson's & Alzheimer's diseases |
| Anti-Viral | AIDS, SARS, ARS and COVID-19 |
| Cystine Depletion | Cystinosis |
| 行动机制 | 适应症 |
| 增加谷胱甘肽-抗氧化剂 | Melas、Huntington‘s、Rett’s和Nash |
| 增强牛磺酸的细胞保护作用 | Melas、Huntington‘s、Rett’s、CNS、TBI |
| 推广BDNF | 亨廷顿、雷特、帕金森和阿尔茨海默病 |
| 抗病毒药物 | 艾滋病、非典、急性呼吸综合征和新冠肺炎 |
| 胱氨酸耗竭 | 胱氨酸病 |
About Cysteamine
关于半胱胺
Historically, cysteamine was studied as far back as the 1950's to protect against radiation poisoning. It has also been studied for other diseases including: paracetamol poisoning, lupus, copper chelation, Huntington's disease and non-alcoholic fatty liver disease (NASH) among others. The only indication for which cysteamine has been approved is cystinosis, an ultra-orphan lysosomal storage disease resulting from a build-up of cystine in cells, which is toxic. Cystagon® (immediate release cysteamine bitartrate) approved to treat cystinosis in 1994 and Procysbi® (enterically coated, delayed release cysteamine bitartrate) approved to treat nephropathic cystinosis in 2013, act as cystine depleting drugs. The inability to administer cysteamine at optimal therapeutic doses without side effects has limited its therapeutic development. TTI-0102 was developed to potentially overcome this limitation.
从历史上看,人们早在20世纪50年代就开始研究半胱胺,以防止辐射中毒。它还被用于其他疾病的研究,包括:扑热息痛中毒、狼疮、铜螯合、亨廷顿病和非酒精性脂肪肝(NASH)等。半胱胺已被批准用于治疗的唯一适应症是半胱氨酸病,这是一种超孤儿溶酶体储存疾病,由细胞内胱氨酸积聚引起,具有毒性。半角形® (半胱胺重酒石酸盐速释)于1994年被批准用于治疗胱氨酸病,Procysbi®(肠溶型,缓释型半胱胺酒石酸重酒石酸盐)于2013年被批准用于治疗肾性胱氨酸病,可作为胱氨酸耗竭药物。无法在最佳治疗剂量下给予半胱胺而不产生副作用,限制了其治疗发展。TTI-0102的开发就是为了潜在地克服这一限制。
About Thiogenesis
关于硫化物的发生
Thiogenesis Therapeutics, Corp. (TSXV: TTI), a clinical-stage biopharmaceutical company operating through its wholly subsidiary based in San Diego, CA, is publicly traded on the TSX Venture Exchange. Thiogenesis is developing sulfur-containing therapeutics that are thiol-active compounds, to potentially treat serious pediatric diseases with unmet clinical needs. The Company's leadership team has extensive knowledge and expertise in drug development, having taken multiple pediatric and orphan drugs through clinical trials, regulatory approval and successful commercial launch at Raptor Pharmaceuticals, (formerly Nasdaq: RPTP) and BioMarin Pharmaceutical. (Nasdaq: BMRN). The Company's initial target indications include Mitochondrial Encephalopathy Lactic Acidosis and Stroke (MELAS) and Rett's syndrome.
通过其位于加利福尼亚州圣地亚哥的全资子公司运营的临床阶段生物制药公司Thigenation Treateutics,Corp.(多伦多证券交易所股票代码:TTI)在多伦多证券交易所创业板上市交易。硫化作用正在开发硫醇活性化合物的含硫疗法,以潜在地治疗临床需求未得到满足的严重儿科疾病。该公司的领导团队在药物开发方面拥有广泛的知识和专业知识,曾在猛禽制药公司(前纳斯达克代码:RPTP)和BioMarin制药公司进行临床试验、监管批准并成功推出商业产品,从而开发了多种儿科和孤儿药物。(纳斯达克:宝马)。该公司最初的目标适应症包括线粒体脑病、乳酸酸中毒和中风(MELAS)和雷特综合征。
For further information, please contact:
如需更多信息,请联系:
Brook Riggins, Director and CFO
Email: briggins@thiogenesis.com
Tel.: +420 776 659 259
布鲁克·里金斯,董事和首席财务官
电子邮件:briggins@thienesis.com
电话:+420 776 659 259
Forward-Looking Statements
前瞻性陈述
This news release contains certain forward-looking statements and forward-looking information (collectively referred to herein as "forward-looking statements") within the meaning of Canadian securities laws including, without limitation, statements with respect to the future investments by the Company. All statements other than statements of historical fact are forward-looking statements. Undue reliance should not be placed on forward-looking statements, which are inherently uncertain, are based on estimates and assumptions, and are subject to known and unknown risks and uncertainties (both general and specific) that contribute to the possibility that the future events or circumstances contemplated by the forward-looking statements will not occur. Although the Company believes that the expectations reflected in the forward-looking statements contained in this press release, and the assumptions on which such forward-looking statements are made, are reasonable, there can be no assurance that such expectations will prove to be correct. Readers are cautioned not to place undue reliance on forward-looking statements included in this document, as there can be no assurance that the plans, intentions or expectations upon which the forward-looking statements are based will occur. By their nature, forward-looking statements involve numerous assumptions, known and unknown risks and uncertainties that contribute to the possibility that the predictions, forecasts, projections and other forward-looking statements will not occur, which may cause the Company's actual performance and results in future periods to differ materially from any estimates or projections of future performance or results expressed or implied by such forward-looking statements. The forward-looking statements contained in this news release are made as of the date hereof and the Company does not undertake any obligation to update publicly or to revise any of the included forward-looking statements, except as required by applicable law. The forward-looking statements contained herein are expressly qualified by this cautionary statement.
本新闻稿包含加拿大证券法定义的某些前瞻性陈述和前瞻性信息(本文统称为“前瞻性陈述”),包括但不限于与公司未来投资有关的陈述。除历史事实以外的所有陈述均为前瞻性陈述。不应过分依赖前瞻性陈述,因为这些陈述本身是不确定的,基于估计和假设,并受到已知和未知风险和不确定性(一般和具体的)的影响,这些风险和不确定性导致前瞻性陈述中预期的未来事件或情况可能不会发生。尽管公司相信本新闻稿中包含的前瞻性陈述中反映的预期以及做出这些前瞻性陈述所依据的假设是合理的,但不能保证这些预期将被证明是正确的。告诫读者不要过度依赖本文件中包含的前瞻性陈述,因为不能保证前瞻性陈述所依据的计划、意图或预期将会发生。就其性质而言,前瞻性陈述涉及许多假设、已知和未知的风险和不确定性,这些风险和不确定性导致预测、预测、预测和其他前瞻性陈述不会发生的可能性。, 这可能会导致公司未来的实际业绩和结果与此类前瞻性陈述明示或暗示的对未来业绩或结果的任何估计或预测大不相同。本新闻稿中包含的前瞻性陈述是截至本新闻稿发布之日作出的,公司不承担公开更新或修改任何包含的前瞻性陈述的义务,除非适用法律要求。本文中包含的前瞻性陈述明确地受到这一警告性声明的限制。
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