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CARsgen to Present Zevor-cel, CT071 and CT0590 at ASH 2024 Annual Congress

CARsgen to Present Zevor-cel, CT071 and CT0590 at ASH 2024 Annual Congress

CARsgen將在2024年ASH年度大會上展示Zevor-cel、CT071和CT0590
PR Newswire ·  11/06 21:50

SHANGHAI, Nov. 6, 2024 /PRNewswire/ -- CARsgen Therapeutics Holdings Limited (Stock Code: 2171.HK), a company focused on innovative CAR T-cell therapies for the treatment of hematologic malignancies and solid tumors, announces that the Company will present the clinical data of zevorcabtagene autoleucel, CT071, and CT0590 as posters at the 66th Annual Congress of the American Society of Hematology ("ASH") which is due to take place between Dec 7 – 10, 2024. The abstracts are available on ASH official website.

SHANGHAI,2024年11月6日 / PRNewswire / - 北京康源基因工程有限公司(股票代碼:2171.HK)是一家專注於革新CAR T細胞治療血液惡性腫瘤和實體瘤的公司,宣佈公司將在2024年12月7日至10日舉行的第66屆美國血液學學會("ASH")年會上將齊沃卡布他基因自體白細胞素(Zevorcabtagene Autoleucel)、CT071和CT0590的臨床數據作爲海報展示。摘要可在ASH官方網站上查閱。

"CARsgen is advancing therapeutic options for hematologic malignancies with robust CAR T-cell pipeline, which includes the autologous CAR T-cell therapy zevor-cel, the single-day-culture CT071, and the allogeneic CAR T-cell candidate CT0590. These initiatives underscore CARsgen's strong commitment to innovation in hematology. Leveraging proprietary technology platforms such as CARcelerate and THANK-uCAR, CARsgen is focused on developing differentiated CAR T-cell therapies to address the critical challenges faced by the clinical community. We are excited to share new data and are confident in the potential of our CAR T-cell therapies to benefit patients worldwide," said Raffaele Baffa, M.D., Ph.D., Chief Medical Officer of CARsgen Therapeutics.

「康源正在推進治療血液惡性腫瘤的治療選擇,擁有強大的CAR T細胞流水線,其中包括自體CAR T細胞療法齊沃賽爾(Zevor-cel)、單日培養CT071和同種移植CAR T細胞候選藥CT0590。這些倡議彰顯了康源在血液學創新中的強大承諾。康源利用CARcelerate和THANk-uCAR等專有技術平台,致力於開發差異化CAR T細胞治療方案,以解決臨床社區面臨的關鍵挑戰。我們很高興分享新數據,對我們的CAR T細胞療法在全球患者中獲益的潛力感到充滿信心,」康源基因工程首席醫學官Raffaele Baffa博士表示。

Subgroup Analyses of Phase 2 Study: Evaluating the Efficacy of Fully Human BCMA-Targeting CAR T Cells (Zevorcabtagene Autoleucel) in Patients with Relapsed/Refractory Multiple Myeloma

第2階段研究的亞組分析:評估針對復發/難治性多發性骨髓瘤患者的全人BCMA靶向CAR T細胞(齊沃卡布他基因自體白細胞)的療效

Publication Number: 4762
Presentation Time: 6:00 PM - 8:00 PM, Monday, December 9, 2024 (PST)

出版號:4762
演示時間:2024年12月9日(美國太平洋時間),晚上6:00點至8:00點

In 102 patients with RRMM who had received at least 3 prior lines of therapy including an immunomodulatory drug and a proteasome inhibitor, the objective response rate (ORR) was 92.2%, the stringent complete response (sCR) or complete response (CR) was 71.6%. The ORR or the CR/sCR rate was not affected by any of the baseline characteristics tested. With a median follow-up of 20.3 (range: 0.4 to 27) months, the median duration of response (DOR), progression-free survival (PFS), and overall survival (OS) data were not mature and therefore, 18-month (18m) and estimated 30-month (30m) event free rates were used as efficacy outcomes for subgroup analyses. The DOR, PFS and OS were not impacted by age or ISS.

在102名RRMm患者中,這些患者至少接受了3條先前療程,包括免疫調節藥物和蛋白酶體抑制劑。客觀反應率(ORR)爲92.2%,嚴格完全緩解(sCR)或完全緩解(CR)爲71.6%。基線特徵測試不影響ORR或CR/sCR率。隨訪中位數爲20.3個月(範圍:0.4至27個月),因此,對於亞組分析,中位反應持續時間(DOR)、無進展生存期(PFS)和總生存期(OS)數據還不成熟,因此使用18個月(18m)和估計的30個月(30m)無事件率作爲療效結果。 DOR,PFS和OS不受年齡或ISS的影響。

These subgroup analyses indicate that baseline characteristics have minimal impact on the clinical efficacy of zevorcabtagene autoleucel, demonstrating that even RRMM patients with poor prognostic factors can benefit from zevorcabtagene autoleucel.

這些亞組分析表明,基線特徵對澤沃卡布他格瑞自體T細胞的臨床療效影響很小,表明即使是具有不良預後因素的RRMm患者也可以從澤沃卡布他格瑞自體T細胞中受益。

GPRC5D-Targeted CAR T-Cell Therapy CT071 for the Treatment of Refractory/Relapsed Multiple Myeloma

GPRC5D靶向CAR T細胞療法CT071用於難治/複發性多發性骨髓瘤治療

Publication Number: 3451
Presentation Time: 6:00 PM - 8:00 PM, Sunday, December 8, 2024 (PST)

發表編號: 3451
演示時間: 下午6:00 - 晚上8:00, 2024年12月8日(太平洋標準時間)

CT071 is a fully human GPRC5D-targeting autologous CAR T-cell product manufactured using an expedited CARcelerate platform which shortens the manufacturing process to around 30 hours resulting in shorter vein-to-vein time. Patients with RRMM who had previously received ≥ 3 prior lines of therapy (LOT) or patients who experienced progression or lack of response having been treated with a proteasome inhibitor and an immunomodulatory agent or those who were double class-refractory, all with ECOG score of 0-2 were enrolled. In 17 patients who had been dosed with CT071, 11 patients (64.7%) experienced cytokine release syndrome (CRS), all at Grade 1 (n=8) or 2 (n=3). No immune effector cell-associated neurotoxicity syndrome (ICANS) was observed. No dose limiting toxicity (DLT) occurred.

CT071是一種全人GPRC5D靶向的自體CAR T細胞產品,採用快速CARcelerate平台製造,將製造過程縮短至約30小時,結果使得靜脈到靜脈的時間縮短。曾接受≥3次治療方案(LOT)或曾接受蛋白酶體抑制劑和免疫調節劑治療但出現進展或無反應的RRMm患者,或曾雙重耐藥的患者,所有患者的ECOG評分爲0-2均可以入組。在17名接受CT071治療的患者中,11名患者(64.7%)出現細胞因子釋放綜合徵(CRS),均爲1級(n=8)或2級(n=3)。未觀察到免疫效應細胞相關的神經毒性綜合徵(ICANS)。未出現劑量限制性毒性(DLT)。

The overall response rate (ORR) was 94.1% (16/17), and the stringent complete response (sCR) rate was 52.9% (9/17). Notably, 7 patients achieved complete response or better at week 4. All 4 patients with previous exposure to BCMA or BCMA/CD19 CAR T responded to CT071 (2 with sCR and 2 with partial response).

總體反應率(ORR)爲94.1%(16/17),嚴格完全緩解率(sCR)爲52.9%(9/17)。值得注意的是,7名患者在第4周時完成緩解。之前接受BCMA或BCMA/CD19 CAR T細胞療法的4名患者中,所有患者對CT071作出反應(2名嚴格完全緩解,2名部分緩解)。

A First-in-Human Study of CT0590, a Triple Knock-out, Allogeneic CAR T-Cell Therapy Targeting BCMA and NKG2A, in Subjects with Relapsed/Refractory Multiple Myeloma

CT0590首次人體研究,一種針對BCMA和NKG2A的三重敲除,同種異體CAR T細胞療法,用於難治/複發性多發性骨髓瘤患者

Publication Number: 4843
Presentation Time: 6:00 PM - 8:00 PM, Monday, December 9, 2024 (PST)

發表編號: 4843
演講時間:2024年12月9日(星期一)下午6:00至8:00,太平洋標準時間(PST)

CT0590 is an allogeneic dual CAR T-cell therapy deploying THANK-uCAR technology that targets both BCMA and NKG2A (a membrane protein expressed in NK and T cells), featuring a triple knockout for TRAC/B2M/NKG2A which mitigates against graft-versus-host disease (GvHD), host immune rejection and fratricide.

CT0590是採用THANk-uCAR技術部署的異基因雙CAR T細胞療法,可靶向BCMA和NKG2A(Nk和T細胞表達的膜蛋白),具有針對TRAC/B2M/NKG2A的三重敲除,有助於減輕移植物抗宿主病(GvHD)、宿主免疫排斥和自相殘殺。

This is a first-in-human (FIH), open-label, single center, phase I study of CT0590 in subjects with RRMM to evaluate the safety, tolerability, pharmacokinetics and preliminary efficacy of CT0590 (NCT05066022). As of 22-Apr-2024, 5 subjects were enrolled (4 subjects with RRMM and 1 subject with primary plasma cell leukemia [pPCL] under compassionate use).

這是針對RRMm患者的CT0590的首次人體研究(FIH),爲開放標籤、單中心、I期研究,旨在評估CT0590的安全性、耐受性、藥代動力學和初步療效(NCT05066022)。截至2024年4月22日,共有5名受試者入組(4名RRMm患者和1名原發性漿細胞白血病[pPCL]患者,爲了同情用藥)。

No ≥ 3 grade cytokine release syndrome (CRS) was observed. No cases of immune effector cell-associated neurotoxicity syndrome (ICANS) or GvHD were observed. No dose limiting toxicities were reported and there were no withdrawal from the study or deaths due to adverse events.

未觀察到≥3級細胞因子釋放綜合症(CRS),亦未觀察到免疫效應細胞相關的神經毒性綜合症(ICANS)或GvHD情況。未報告劑量限制性毒性,無受試者退出研究或因不良事件死亡。

With a median follow-up time of 16.6 months (range: 5.1, 24.2), 3 subjects achieved confirmed responses including 2 subjects with stringent complete response (sCR) and 1 subject with partial response (PR). The 2 subjects with sCR include1 RRMM subject [sCR ongoing] with a DOR longer than 23 months as of data cut-off date and 1 pPCL subject with a duration of response (DOR) of 20 months. In the 2 subjects with sCR, CAR copies peaked at > 280,000 copies/μg genomic DNA.

在中位隨訪時間16.6個月(範圍:5.1至24.2)內,3名受試者取得了確認療效,其中2名獲得嚴格完全緩解(sCR),1名獲得部分緩解(PR)。兩名sCR受試者中,一名RRMm受試者[sCR持續中]的DOR超過了截止日期爲止的23個月,另一名pPCL受試者的療效持續時間(DOR)爲20個月。在這兩名sCR受試者中,CAR拷貝峯值超過280,000拷貝/μg基因組DNA。

Preliminary results of this FIH study of the CT0590 allogeneic CAR T-cell therapy demonstrated a manageable safety profile while achieving deep and durable clinical responses.

CT0590異基因CAR T細胞療法的首次人體研究初步結果顯示了可管理的安全性概況,同時實現了深入且持久的臨床療效。

About Zevorcabtagene Autoleucel

關於Zevorcabtagene Autoleucel

Zevorcabtagene autoleucel is a fully human, autologous BCMA CAR T-cell product for the treatment of Multiple Myeloma (MM). Zevorcabtagene autoleucel was approved by the NMPA on February 23, 2024 for the treatment of adult patients with R/R MM who have progressed after at least 3 prior lines of therapy (including a proteasome inhibitor and an immunomodulatory agent). CARsgen is conducting a separate Phase 1b/2 LUMMICAR STUDY 2 clinical trial in North America to evaluate the safety and efficacy of zevorcabtagene autoleucel in R/R MM.

Zevorcabtagene autoleucel是用於治療多發性骨髓瘤(MM)的全人源自體BCMA CAR T細胞產品。Zevorcabtagene autoleucel於2024年2月23日獲得NMPA批准,用於治療經過至少3種先前療法失敗的成人R/R MM患者(包括蛋白酶體抑制劑和免疫調節藥物)。CARsgen正在北美進行獨立的LUMMICAR STUDY 2臨床試驗,以評估Zevorcabtagene autoleucel在R/R MM中的安全性和療效。

Zevorcabtagene autoleucel received Regenerative Medicine Advanced Therapy (RMAT) and Orphan Drug designations from the U.S. FDA in 2019, as well as Priority Medicines (PRIME) and Orphan Medicinal Product designations from the European Medicines Agency (EMA) in 2019 and 2020, respectively.

富智康集團的Zevorcabtagene autoleucel於2019年獲得了美國FDA的再生醫學先進療法(RMAT)和孤兒藥品認定,以及2019年和2020年分別獲得了歐洲藥品管理局(EMA)的優先藥品(PRIME)和孤兒藥品認定。

About CT071

關於CT071

CT071 is a CAR T-cell therapy candidate developed utilizing the proprietary CARcelerate platform of CARsgen targeting GPRC5D for the treatment of relapsed/refractory MM or relapsed/refractory plasma cell leukemia (PCL). An IIT (NCT05838131) is ongoing in China to evaluate the preliminary safety and efficacy of CT071 for the treatment of patients with relapsed/refractory multiple myeloma or plasma cell leukemia. A separate investigator-initiated trial (NCT06407947) is ongoing in China for the treatment of patients with newly diagnosed multiple myeloma (NDMM).

CT071是一種CAR t-電芯療法候選,利用CARsgen的CARcelerate平台針對GPRC5D開發,用於治療復發/難治性多發性骨髓瘤或復發/難治性漿細胞白血病(PCL)。在中國進行了一個IIt(NCT05838131)以評估CT071對復發/難治性多發性骨髓瘤或漿細胞白血病患者的初步安全性和療效。在中國進行了另一個由研究者發起的臨床試驗(NCT06407947),用於治療新診斷的多發性骨髓瘤(NDMM)。

About CT0590

關於CT0590

CT0590 is a BCMA-targeting allogeneic CAR T-cell product candidate deploying CARsgen's THANK-uCAR technology. An IIT is ongoing in China to evaluate the preliminary safety and efficacy of CT0590 for the treatment of R/R MM.

CT0590是一種以BCMA爲靶的異基因CAR t-電芯產品候選,採用CARsgen的THANk-uCAR技術。在中國進行了一個IIt以評估CT0590對復發/難治性多發性骨髓瘤的初步安全性和療效。

About CARsgen Therapeutics Holdings Limited

關於CARsgen Therapeutics Holdings Limited CARsgen是一家在中國和美國擁有業務的生物製藥公司,專注於治療血液惡性腫瘤和實體瘤的創新CAR T細胞療法。CARsgen建立了一個全面的CAR T細胞研發平台,包括靶點發現、創新CAR T細胞研發、臨床試驗和商業化大規模生產。CARsgen擁有自主開發的新技術和產品線,具備解決CAR T細胞療法的主要挑戰,如提高安全性、增強治療固體腫瘤的療效和降低治療成本的全球權利。CARsgen的使命是成爲一個全球性的生物製藥領導者,爲全球癌症患者帶來創新和差異化的細胞治療,使癌症變得可治癒。

CARsgen is a biopharmaceutical company with operations in China and the U.S., focusing on innovative CAR T-cell therapies for the treatment of hematologic malignancies and solid tumors. CARsgen has established a comprehensive CAR T-cell research and development platform that covers target discovery, innovative CAR T-cell development, clinical trials, and commercial-scale production. Internally, CARsgen has developed novel technologies and a product pipeline with global rights to address significant challenges faced by existing CAR T-cell therapies. Efforts include improving safety profile, enhancing the efficacy in treating solid tumors, and reducing treatment costs. CARsgen's mission is to become a global biopharmaceutical leader that provides innovative and differentiated cell therapies for cancer patients worldwide and makes cancer curable.

CARsgen是一家在中國和美國開展業務的生物製藥公司,專注於創新的CAR T細胞療法用於治療血液腫瘤和實體腫瘤。CARsgen建立了一個全面的CAR T細胞研發平台,涵蓋目標發現、創新CAR T細胞研發、臨床試驗和商業規模生產。CARsgen內部開發了新技術和產品管線,並擁有全球權利,以應對現有CAR T細胞療法面臨的重大挑戰。努力包括改善安全性、增強治療實體腫瘤的療效和降低治療成本。CARsgen的使命是成爲全球領先的生物製藥公司,爲全球癌症患者提供創新和差異化的細胞療法,並使癌症可治癒。

Forward-looking Statements

前瞻性聲明

All statements in this press release that are not historical fact or that do not relate to present facts or current conditions are forward-looking statements. Such forward-looking statements express the Group's current views, projections, beliefs and expectations with respect to future events as of the date of this press release. Such forward-looking statements are based on a number of assumptions and factors beyond the Group's control. As a result, they are subject to significant risks and uncertainties, and actual events or results may differ materially from these forward-looking statements and the forward-looking events discussed in this press release might not occur. Such risks and uncertainties include, but are not limited to, those detailed under the heading "Principal Risks and Uncertainties" in our most recent annual report and interim report and other announcements and reports made available on our corporate website, . No representation or warranty is given as to the achievement or reasonableness of, and no reliance should be placed on, any projections, targets, estimates or forecasts contained in this press release.

本新聞稿中所有非歷史性事實或與目前事實或現狀無關的陳述均爲前瞻性陳述。此類前瞻性陳述表達了集團截至本新聞稿發佈日期對未來事件的當前觀點、預測、信念和期望。此類前瞻性陳述基於集團無法控制的一系列假設和因素。因此,它們面臨重大風險和不確定性,並且實際事件或結果可能與這些前瞻性陳述和本新聞稿中討論的前瞻性事件有重大差異。此類風險和不確定性包括但不限於咱們最近的年度報告和中期報告以及其他公佈在咱們公司網站上的公告和報告訪問。不提供關於本新聞稿中包含的任何預測、目標、估計或預測的實現或合理性,並且不應在這些預測、目標、估計或預測中放置任何依賴。

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