Editas Medicine Presents Data on SLEEK Gene Editing Technology at the American Society of Gene and Cell Therapy Annual Meeting
Editas Medicine Presents Data on SLEEK Gene Editing Technology at the American Society of Gene and Cell Therapy Annual Meeting
SLEEK results in highly efficient multi-transgene knock-in and enables tunability of transgene expression
SLEEK可實現高效的多基因敲入,並實現轉基因表達的可調性
Double knock-in iNK cells demonstrate strong tumor killing effect and prolonged in vivo persistence in an ovarian cancer mouse model
雙敲入墨水細胞在卵巢癌小鼠模型中顯示出較強的腫瘤殺傷作用和較長的體內存活率
CAMBRIDGE, Mass., May 18, 2022 (GLOBE NEWSWIRE) -- Editas Medicine, Inc. (Nasdaq: EDIT), a leading genome editing company, will present data later today on its SLEEK (SeLection by Essential- gene Exon Knock-in) gene editing technology during the New Gene Editing Technologies and Applications Session at the 25th Annual Meeting of the American Society of Gene and Cell Therapy (ASGCT) being held in Washington, D.C., and virtually, May 16 – 19, 2022.
馬薩諸塞州坎布里奇,2022年5月18日(環球社)--領先的基因組編輯公司Editas Medicine,Inc.(納斯達克:EDIT)今天晚些時候將在2022年5月16-19日在華盛頓舉行的第25屆美國基因與細胞治療學會年會上,在新基因編輯技術和應用會議上公佈其時尚(由必需基因外顯子敲入選擇)基因編輯技術的數據。
"Despite recent progress, many cell-based medicines suffer from inefficient knock-in of transgene cargos and high heterogeneity that may reduce efficacy and pose potential safety issues. SLEEK is designed to address these challenges, by achieving efficient knock-in of multiple transgenes, avoiding silencing of transgene cargos over time, and enabling efficient knock-in using non-viral DNA donor templates," said Mark S. Shearman, Ph.D., Executive Vice President and Chief Scientific Officer, Editas Medicine. "We have used SLEEK to achieve very high knock-in efficiencies in T cells, B cells and natural killer (NK) cells. Our SLEEK-edited, iPSC-derived double knock-in NK cells resulted in impressive tumor clearance, improved survival, and prolonged in vivo persistence in an ovarian cancer mouse model. We believe this technology has the potential to fundamentally improve the next generation of cell-based medicines, beginning with EDIT-202, our first iPSC-derived NK cell oncology program now in preclinical studies."
Editas Medicine執行副總裁兼首席科學官馬克·S·謝爾曼博士説:儘管最近取得了進展,但許多基於細胞的藥物存在轉基因貨物低效敲入和高度異質性的問題,這可能會降低療效並帶來潛在的安全問題。SLEK旨在通過實現多個轉基因的高效敲入,避免隨着時間的推移而使轉基因貨物沉默,並使用非病毒DNA供體模板實現高效的敲入。我們已經使用SLEK在T細胞、B細胞和自然殺傷(NK)細胞中實現了非常高的敲入效率。我們經過光滑編輯的IPSC衍生的雙重敲入NK細胞導致了令人印象深刻的腫瘤清除,提高了存活率,並延長了時間體內在卵巢癌小鼠模型中的持久性。我們相信,這項技術有可能從根本上改進下一代基於細胞的藥物,從EDIT-202開始,這是我們第一個由iPSC衍生的NK細胞腫瘤學項目,目前正在進行臨牀前研究。“
SLEEK was used to insert CD16 and mbIL-15 cargos into iPSCs which generated NK cells with significantly improved tumor killing and survival compared to wild-type NK cells. SLEEK-edited cells also demonstrated strong antibody-dependent cellular cytotoxicity and improved persistence, without the need for exogenous cytokine support.
SLEK被用來將CD16和MBIL-15貨物插入到IPSCs中,與野生型NK細胞相比,其產生的NK細胞具有顯着的腫瘤殺傷力和存活率。光滑編輯的細胞還顯示出強大的抗體依賴的細胞毒性和改善的持久性,不需要外源性細胞因子支持。
Further key findings presented about SLEEK include:
關於Sleek的其他重要發現包括:
- Enables knock-in editing efficiencies of over 90% in relevant cell types, without impacting long-term viability or expansion.
- Permits constitutive and robust expression in iPSC-derived cell types where transgene promoter silencing has been a major challenge during the differentiation process.
- Demonstrated utility with clinically important cargos including chimeric antigen receptors (CARs) and allogeneic shields.
- Provides targeted knock-in to clinically important ex vivo cell types including T cells, B cells, and NK cells.
- Allows for tunability of transgene expression based on different promoter strengths of various essential genes.
- Enables use of non-viral DNA templates matching performance of the AAV6 gold standard on key attributes, potentially supporting more complex knock-in cassettes by avoiding AA6 cargo capacity limits.
- 在不影響長期生存或擴展的情況下,使相關單元類型的敲擊編輯效率達到90%以上。
- 在IPSC來源的細胞類型中,轉基因啟動子沉默一直是分化過程中的主要挑戰,允許在這些類型的細胞中進行構成和強勁的表達。
- 展示了對臨牀重要貨物的效用,包括嵌合抗原受體(CARS)和同種異體盾牌。
- 提供針對臨牀上重要的體外細胞類型的靶向敲入,包括T細胞、B細胞和NK細胞。
- 允許根據不同基本基因的不同啟動子強度來調節轉基因表達。
- 支持使用在關鍵屬性上與AAV6黃金標準性能匹配的非病毒DNA模板,通過避免AA6貨物容量限制,潛在地支持更復雜的嵌入盒。
Additional Presentations at ASGCT
In an oral presentation at the ASGCT Annual Meeting on Monday, May 16, 2022, Editas presented data on its EDIT-101 program for the treatment for Leber Congenital Amaurosis 10 (LCA10), a CEP290-related retinal degenerative disorder, demonstrating a favorable immunogenicity profile.
在ASGCT上的其他演講
在2022年5月16日星期一舉行的ASGCT年會上的口頭演示中,Editas介紹了其治療Leber先天性黑色素沉着症10(LCA10)的EDIT-101計劃的數據,LCA10是一種與CEP290相關的視網膜退行性疾病,展示了良好的免疫原性特徵。
On Thursday, May 19, 2022, Editas will provide an oral presentation on its EDIT-103 program, in development for the treatment of rhodopsin-associated autosomal dominant retinitis pigmentosa (RHO-adRP). The presentation will highlight preclinical data from non-human primate studies of EDIT-103, demonstrating nearly 100% gene editing knockout of endogenous RHO gene and more than 30% replacement protein levels.
2022年5月19日星期四,Editas將口頭介紹其EDIT-103計劃,該計劃正在開發中,用於治療視紫紅質相關的常染色體顯性視網膜色素變性(RHO-ADRP)。報告將重點介紹EDIT-103的非人類靈長類研究的臨牀前數據,展示了內源性Rho基因近100%的基因編輯敲除和超過30%的替換蛋白水平。
The complete list of Editas Medicine presentations at ASGCT is below. Abstracts can be accessed on the ASGCT website, and the presentations will be posted on the Editas Medicine website during the conference.
以下是在ASGCT上的Editas Medicine演示文稿的完整列表。摘要可在ASGCT網站上查閲,演講將在會議期間發佈在Editas Medicine網站上。
Oral Presentations:
Title: Exploratory Immuno-Safety Profile of EDIT-101, a First-in-Human In Vivo CRISPR Gene Editing Therapy for CEP290-Related Retinal Degeneration
Session Date and Time: Monday, May 16, 2022, 1:30 p.m. – 3:15 p.m. ET
Presentation Time: 2:45 p.m. – 3:00 p.m. ET
Session title: Gene and Cell Therapy Trials in Progress
口頭陳述:
標題:人類首例EDIT-101的免疫安全性研究在活體中CRISPR基因編輯療法CEP290與視網膜相關的變性
會議日期和時間:2022年5月16日星期一下午1:30-下午3:15外星人
演示時間:下午2:45-下午3:00外星人
會議標題:基因和細胞治療試驗正在進行中
Title: SLEEK: A Method for Highly Efficient Knock-in and Expression of Transgene Cargos for Next-generation Cell-based Medicines
Session Date and Time: Wednesday, May 18, 2022, 3:45 p.m. – 5:30 p.m. ET
Presentation Time: 5:00 p.m. – 5:15 p.m. ET
Session title: New Gene Editing Technologies and Applications
Title: A Mutation-Independent CRISPR/Cas9-Based ʻKnockout and Replaceʼ Strategy to Treat Rhodopsin-Associated Autosomal Dominant Retinitis Pigmentosa
Session Date and Time: Thursday May 19, 2022, 10:15 a.m. – 12:00 p.m. ET
Presentation Time: 10:15 a.m. – 10:30 a.m. ET
Session title: Ophthalmic and Auditory Diseases
標題:SLEK:一種用於下一代細胞藥物的轉基因貨物的高效敲入和表達方法
會議日期和時間:2022年5月18日星期三下午3:45-下午5:30外星人
演示時間:下午5:00-下午5:15外星人
會議標題:基因編輯新技術及其應用
標題:基於突變非依賴性CRISPR/CAS9的ʻ基因敲除和替換ʼ策略治療視紫紅質相關性常染色體顯性視網膜色素變性
會話日期和時間:2022年5月19日星期四上午10:15-下午12:00外星人
演示時間:上午10:15-上午10:30外星人
會議標題:眼科和聽力疾病
Poster Presentation:
Title: EDIT-202, A Multiplexed CRISPR-Cas12a Gene-Edited iPSC-Derived NK Cell Therapy has Prolonged Persistence, Promotes High Cytotoxicity, and Enhances In Vivo Tumor Killing
Session Date and Time: Wednesday, May 18, 2022, 5:30 p.m. – 6:30 p.m. ET
Session Title: Cancer - Targeted Gene and Cell Therapy II
海報演示文稿:
標題:編輯-202,一種多路CRISPR-Cas12a基因編輯的IPSC來源的NK細胞療法具有持久的持久性,促進高細胞毒性,並增強在活體中腫瘤殺傷
會議日期和時間:2022年5月18日星期三下午5:30-下午6:30外星人
會議標題:腫瘤靶向基因與細胞治療II
About SLEEK Gene Editing
SLEEK (SeLection by Essential-gene Exon Knock-in) gene editing is an optimized approach to developing the next generation of cell therapy medicines for cancer and other serious diseases. Utilizing Editas Medicine's proprietary engineered AsCas12a nuclease, SLEEK enables high efficiency, multi-transgene knock-in of induced pluripotent stem cells (iPSCs), T cells, and natural killer (NK) cells while ensuring robust, transgene expression. Editas Medicine is currently leveraging SLEEK technology in its oncology programs.
關於時髦的基因編輯
SLEKK(由必需基因外顯子敲入選擇)基因編輯是開發治療癌症和其他嚴重疾病的下一代細胞治療藥物的優化方法。利用Editas Medicine專有的AsCas12a核酸酶,SLEK能夠高效、多基因敲入誘導的多潛能幹細胞(IPSCs)、T細胞和自然殺傷(NK)細胞,同時確保強勁的轉基因表達。Editas Medicine目前正在其腫瘤學計劃中利用時髦的技術。
About Editas Medicine
As a leading genome editing company, Editas Medicine is focused on translating the power and potential of the CRISPR/Cas9 and CRISPR/Cas12a (also known as Cpf1) genome editing systems into a robust pipeline of treatments for people living with serious diseases around the world. Editas Medicine aims to discover, develop, manufacture, and commercialize transformative, durable, precision genomic medicines for a broad class of diseases. For the latest information and scientific presentations, please visit .
關於Editas Medicine
作為一家領先的基因組編輯公司,Editas Medicine專注於將CRISPR/Cas9和CRISPR/Cas12a(也稱為Cpf1)基因組編輯系統的能力和潛力轉化為全球嚴重疾病患者的強大治療流水線。Editas Medicine的目標是發現、開發、製造和商業化治療各種疾病的變革性、耐用性、精確度高的基因組藥物。有關最新信息和科學演示,請訪問。
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CONTACT: Contacts: Media Cristi Barnett (617) 401-0113 cristi.barnett@editasmed.com Investors Ron Moldaver (617) 401-9052 ir@editasmed.com
聯繫人:媒體克里斯蒂·巴尼特電話:(617)401-0113電子郵件:cristi.barnett@editasmed.com投資者羅恩·莫爾達弗電話:(617)401-9052
譯文內容由第三人軟體翻譯。