Omega Therapeutics Presents Preclinical Data on OTX-2002, First-in-Class Epigenomic Controller, as Potential Treatment for Hepatocellular Carcinoma at the AACR Annual Meeting 2022
Omega Therapeutics Presents Preclinical Data on OTX-2002, First-in-Class Epigenomic Controller, as Potential Treatment for Hepatocellular Carcinoma at the AACR Annual Meeting 2022
- OTX-2002 suppresses c-Myc gene expression resulting in a loss of cancer cell viability in vitro and reduces tumor growth in in vivo xenograft models
- Data support the potential of the OMEGA Epigenomic Programming™ platform to engineer programmable epigenetic mRNA therapeutics that successfully regulate gene expression
- Robust data support filing of Investigational New Drug application in the first half of 2022 and positions the OTX-2002 program for further development
- OTX-2002抑制c-Myc基因表達導致癌細胞活力喪失體外培養並減少腫瘤的生長體內異種移植模型
- 數據支持omega表觀基因組編程™平臺設計成功調控基因表達的可編程表觀遺傳基因療法的潛力
- 強勁的數據支持2022年上半年研究用新藥申請的提交,併為OTX-2002計劃的進一步發展做好準備
CAMBRIDGE, Mass., April 8, 2022 /PRNewswire/ -- Omega Therapeutics (NASDAQ: OMGA) (Omega), a development-stage biotechnology company pioneering the first systematic approach to use mRNA therapeutics as a new class of programmable epigenetic medicines by leveraging its OMEGA Epigenomic Programming™ platform, will present preclinical data highlighting the potential of its lead Omega Epigenomic Controller™, OTX-2002, to regulate overexpression of the c-Myc (MYC) oncogene in models of hepatocellular carcinoma (HCC) in a poster presentation at the American Association for Cancer Research (AACR) Annual Meeting 2022, taking place in New Orleans, Louisiana, April 8-13, 2022.
馬薩諸塞州坎布里奇2022年4月8日發展階段生物技術公司歐米茄治療公司(納斯達克代碼:OMGA)(歐米茄)利用其歐米茄表觀基因組編程™平臺開創了將信使核糖核酸療法作為一種新型可編程表觀遺傳藥物的系統方法的先河,該公司將在2022年在美國路易斯安那州新奧爾良舉行的美國癌症研究協會年會上的海報演示中公佈臨牀前數據,突顯其領先的歐米茄表觀基因組控制器™在肝細胞癌模型中調節c-myc癌基因過度表達的潛力2022年4月8日-13日.
"Despite its essential role in a broad range of cancers, MYC has remained undruggable to date," said Thomas McCauley, Ph.D., Chief Scientific Officer of Omega Therapeutics. "However, we believe that targeting the MYC gene pre-transcriptionally within its Insulated Genomic Domain (IGD), and epigenetically tuning it using our epigenomic controller, could overcome the challenges that have limited previous technologies including small molecules, antisense oligos and siRNA. We believe that these data strongly support OTX-2002's ability to tune and restore MYC expression to a normal range and demonstrate the broader potential of our Epigenomic Programming platform to tackle previously intractable diseases. We are excited to continue advancing OTX-2002 into clinical trials and look forward to filing an Investigational New Drug application in the first half of this year."
Omega治療公司的首席科學官Thomas McCauley博士説:“儘管MYC在多種癌症中發揮了重要作用,但到目前為止,它仍然無法用藥。”然而,我們認為,在其絕緣基因組結構域(IGD)中預先轉錄MYC基因,並使用我們的表觀基因組控制器對其進行表觀遺傳調整,可以克服限制以前技術的挑戰,包括小分子、反義寡核苷酸和siRNA。我們相信,這些數據有力地支持了OTX-2002調整MYC表達並將其恢復到正常範圍的能力,並展示了我們的表觀基因組編程平臺在解決以前難以治癒的疾病方面的更廣泛潛力。我們為繼續將OTX-2002推進臨牀試驗而感到興奮,並期待着在今年上半年提交研究性新藥申請。“
Key findings
主要發現
- A single dose of OTX-2002 induced durable changes in the epigenetic profile of the MYC gene
- OTX-2002 reduced MYC mRNA expression and protein levels over approximately 2 weeks in vitro
- Downregulation of MYC in multiple HCC cell lines resulted in significant loss in viability of MYC-addicted cancer cells while sparing normal cells
- In murine xenograft HCC models, OTX-2002 significantly reduced tumor growth and was well-tolerated
- 單劑量OTX-2002誘導MYC基因表觀遺傳圖譜的持久變化
- OTX-2002在大約兩週內降低了MYC mRNA的表達和蛋白水平在……裏面 體外
- MYC在多個肝癌細胞系中的下調導致MYC成癮的癌細胞活力顯著下降,而正常細胞則倖免於難
- 在小鼠異種移植肝癌模型中,OTX-2002顯著抑制了腫瘤生長,且耐受性良好
Cumulatively, these data support the filing of an Investigational New Drug application with the U.S. Food and Drug Administration for the clinical development of OTX-2002 in the first half of 2022.
總而言之,這些數據支持在2022年上半年向美國食品和藥物管理局提交OTX-2002臨牀開發的研究新藥申請。
The poster can be viewed on the Omega website at
海報可在歐米茄網站上查看,網址為
About OTX-2002
關於OTX-2002
OTX-2002 is a first-in-class Omega Epigenomic Controller™ in development for the treatment of hepatocellular carcinoma (HCC). OTX-2002 is designed to modulate levels of c-MYC (MYC) expression by utilizing targeted mRNA-expressed proteins to mediate epigenetic regulation while potentially overcoming MYC autoregulation. The MYC oncogene is associated with aggressive disease in up to ~70% of patients with HCC. Omega is currently evaluating OTX-2002 in Investigational New Drug (IND)-enabling studies.
OTX2002是一種一流的歐米茄表觀基因組控制器™,正在開發中,用於治療肝細胞癌。OTX-2002旨在通過利用靶向mRNA表達的蛋白來調節c-MYC(MYC)的表達水平,以介導表觀遺傳調節,同時潛在地克服MYC的自身調節。在高達70%的肝癌患者中,MYC癌基因與侵襲性疾病有關。歐米茄公司目前正在評估OTX-2002的研究性新藥(IND)支持研究。
About Omega Therapeutics
關於歐米茄治療公司
Omega Therapeutics, founded by Flagship Pioneering, is a development-stage biotechnology company pioneering the first systematic approach to use mRNA therapeutics as a new class of programmable epigenetic medicines. The company's OMEGA Epigenomic Programming™ platform harnesses the power of epigenetics, the mechanism that controls gene expression and every aspect of an organism's life from cell genesis, growth, and differentiation to cell death. Using a suite of technologies, paired with Omega's process of systematic, rational, and integrative drug design, the deterministic OMEGA platform enables control of fundamental epigenetic processes to correct the root cause of disease by returning aberrant gene expression to a normal range without altering native nucleic acid sequences. Omega's modular and programmable mRNA epigenetic medicines, Omega Epigenomic Controllers™, target specific epigenomic loci within insulated genomic domains, EpiZips™, from amongst thousands of unique, mapped, and validated genome-wide DNA-sequences, with high specificity to durably tune single or multiple genes to treat and cure diseases through Precision Genomic Control™. Omega is currently advancing a broad pipeline of development candidates spanning a range of disease areas, including oncology, regenerative medicine, multigenic diseases including immunology, and select monogenic diseases.
歐米茄治療公司由旗艦先鋒公司創立,是一家處於發展階段的生物技術公司,開創了將信使核糖核酸療法作為一種新型可編程表觀遺傳藥物的第一種系統方法。該公司的歐米茄表觀基因組編程™平臺利用表觀遺傳學的力量,這是一種控制基因表達和生物體生命的方方面面的機制,從細胞發生、生長和分化到細胞死亡。使用一套技術,結合Omega的系統、理性和綜合藥物設計過程,確定性omega平臺能夠控制基本的表觀遺傳過程,通過在不改變天然核酸序列的情況下將異常基因表達恢復到正常範圍來糾正疾病的根本原因。歐米茄模塊化和可編程的mRNA表遺傳藥物歐米茄表觀基因組控制器™針對隔離基因組域中的特定表觀基因組位置EpiZips™,從數以千計的獨特、繪製和驗證的全基因組™序列中進行定位,具有高度的特異性,通過精密基因組控制DNA持久地調整單個或多個基因來治療和治療疾病。歐米茄目前正在推進廣泛的候選開發管道,涵蓋一系列疾病領域,包括腫瘤學、再生醫學、包括免疫學在內的多基因疾病,以及特定的單基因疾病。
For more information, visit omegatherapeutics.com, or follow us on Twitter and LinkedIn
欲瞭解更多信息,請訪問omegaTreateutics.com,或在Twitter和LinkedIn上關注我們
Forward-Looking Statements
This press release contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. All statements contained in this press release that do not relate to matters of historical fact should be considered forward-looking statements, including without limitation statements regarding our expectations surrounding the potential of our product candidates, including our lead OEC candidate OTX-2002; and our plans to present preclinical data on OTX-2002 and file an Investigational New Drug application for it in the first half of 2022. These statements are neither promises nor guarantees, but involve known and unknown risks, uncertainties and other important factors that may cause our actual results, performance or achievements to be materially different from any future results, performance or achievements expressed or implied by the forward-looking statements, including, but not limited to, the following: the novel technology on which our product candidates are based makes it difficult to predict the time and cost of preclinical and clinical development and subsequently obtaining regulatory approval, if at all; the substantial development and regulatory risks associated with epigenomic controller machines due to the novel and unprecedented nature of this new category of medicines; our limited operating history; the incurrence of significant losses and the fact that we expect to continue to incur significant additional losses for the foreseeable future; our need for substantial additional financing; our investments in research and development efforts that further enhance the OMEGA platform, and their impact on our results; uncertainty regarding preclinical development, especially for a new class of medicines such as epigenomic controllers; the fact that our product candidates may be associated with serious adverse events, undesirable side effects or have other properties that could halt their regulatory development, prevent their regulatory approval, limit their commercial potential, or result in significant negative consequences; the impact of increased demand for the manufacture of mRNA and LNP based vaccines to treat COVID-19 on our development plans; difficulties manufacturing the novel technology on which our OEC candidates are based; our ability to adapt to rapid and significant technological change; our reliance on third parties for the manufacture of materials; our ability to successfully acquire and establish our own manufacturing facilities and infrastructure; our reliance on a limited number of suppliers for lipid excipients used in our product candidates; our ability to advance our product candidates to clinical development; and our ability to obtain, maintain, enforce and adequately protect our intellectual property rights. These and other important factors discussed under the caption "Risk Factors" in our Annual Report on Form 10-K for the period ended December 31, 2021, and our other filings with the SEC could cause actual results to differ materially from those indicated by the forward-looking statements made in this press release. Any such forward-looking statements represent management's estimates as of the date of this press release. While we may elect to update such forward-looking statements at some point in the future, we disclaim any obligation to do so, even if subsequent events cause our views to change.
前瞻性陳述
本新聞稿包含符合1995年私人證券訴訟改革法的前瞻性陳述。本新聞稿中包含的所有與歷史事實無關的陳述都應被視為前瞻性陳述,包括但不限於有關我們對我們候選產品的潛力的期望的陳述,包括我們的主要候選OTX-2002;以及我們計劃在2022年上半年提交關於OTX-2002的臨牀前數據併為其提交研究新藥申請。這些陳述既不是承諾也不是保證,而是涉及已知和未知的風險、不確定性和其他重要因素,這些風險、不確定因素和其他重要因素可能導致我們的實際結果、業績或成就與前瞻性陳述中明示或暗示的任何未來結果、業績或成就大不相同,包括但不限於:我們候選產品所基於的新技術使我們難以預測臨牀前和臨牀開發以及隨後獲得監管批准的時間和成本(如果有的話);由於這一新類別藥物的新穎和前所未有的性質,與表觀控制器機器相關的實質性開發和監管風險;我們有限的運營歷史;重大虧損的發生以及我們預計在可預見的未來將繼續遭受重大額外虧損的事實;我們對大量額外融資的需求;我們對進一步增強omega平臺的研發努力的投資及其對我們業績的影響;有關臨牀前開發的不確定性,特別是對於表觀基因組控制器等新類別藥物的不確定性;我們的候選產品可能與嚴重的不良事件有關的事實, 這些不利的副作用或其他特性可能會導致我們的產品研發停滯、阻礙監管批准、限制其商業潛力或導致重大負面後果;我們的發展計劃受到以下方面的影響:對核糖核酸和核糖核酸疫苗生產的需求增加;我們的OEC候選疫苗所基於的新技術難以製造;我們適應快速而重大的技術變化的能力;我們依賴第三方進行材料製造的能力;我們成功收購併建立自己的製造設施和基礎設施的能力;我們對我們候選產品中使用的脂肪輔料的依賴數量有限的供應商;我們將我們的候選產品推向臨牀開發的能力,以及我們獲得、維護、執行和充分保護我們知識產權的能力。在截至2021年12月31日的10-K表格年度報告以及我們提交給美國證券交易委員會的其他文件中,在“風險因素”一欄下討論的這些和其他重要因素可能會導致實際結果與本新聞稿中的前瞻性聲明所表示的結果大不相同。任何此類前瞻性陳述均代表管理層截至本新聞稿發佈之日的估計。雖然我們可能會選擇在未來的某個時候更新這些前瞻性陳述,但我們沒有義務這樣做,即使隨後發生的事件會導致我們的觀點發生變化。
Contacts
Media contact:
Jason Braco
LifeSci Communications
646.751.4361
[email protected]
聯繫人
媒體聯繫人:
傑森·布拉科
生活科學傳播
646.751.4361
[受電子郵件保護]
Investor contact:
Kevin Murphy/Brendan Burns
Argot Partners
212.600.1902
[email protected]
投資者聯繫方式:
凱文·墨菲/布蘭登·伯恩斯
隱語合夥人
212.600.1902
[受電子郵件保護]
SOURCE Omega Therapeutics
來源:歐米茄治療公司
譯文內容由第三人軟體翻譯。