Y-mAbs Presents SADA Platform Preclinical Data and Trial in Progress Posters at the 2024 American Society Hematology (ASH) Annual Meeting
Y-mAbs Presents SADA Platform Preclinical Data and Trial in Progress Posters at the 2024 American Society Hematology (ASH) Annual Meeting
In addition, Y-mAbs presents a trial-in-progress poster from its ongoing Phase 1 (Trial 1201) clinical study evaluating the safety and tolerability of CD38-SADA PRIT with LuNEW YORK, Dec. 07, 2024 (GLOBE NEWSWIRE) -- Y-mAbs Therapeutics, Inc. (the "Company" or "Y-mAbs") (Nasdaq: YMAB), a commercial-stage biopharmaceutical company focused on the development and commercialization of novel radioimmunotherapy and antibody-based therapeutic products for the treatment of cancer, today announced the presentation of CD38-SADA in Non-Hodgkin Lymphoma (NHL) preclinical data and trial in progress posters at the 66th American Society of Hematology (ASH) Annual Meeting & Exposition being held on December 7 –10, 2024, in San Diego, California.
紐約,2024年12月7日(GLOBE NEWSWIRE)-- Y-mAbs Therapeutics, Inc.(「公司」或「Y-mAbs」)(納斯達克:YMAB),一家商業階段的生物製藥公司,專注於開發和商業化新型放射免疫治療和基於抗體的治療產品以治療癌症,今天宣佈在2024年12月7日至10日在加利福尼亞州聖地亞哥舉行的第66屆美國血液學會(ASH)年會上展示非霍奇金淋巴瘤(NHL)前臨床數據和正在進行的試驗海報。
A poster titled "CD38-SADA, a Self-Assembling and Dis-Assembling Bispecific Fusion Protein for Two-Step Pretargeted Radioimmunotherapy of Non-Hodgkin Lymphoma" characterizes the selective binding of CD38-SADA to DOTA-chelated lanthanide metals and high-avidity binding to CD38, a tumor specific antigen overexpressed across a range of lymphoma cells. Data from this poster demonstrate anti-tumor efficacy of CD38-SADA when used with Lutetium 177 (Lu177)-DOTA in a two-step approach to pre-targeted radioimmunotherapy ("PRIT"). Tumor responses in a xenograft mouse model were rapid and dose-dependent, further supporting the clinical development of CD38-SADA PRIT in patients with CD38-positive lymphoid malignancies.
一個題爲"CD38-SADA,一種自組裝及解組裝的雙特異性融合蛋白,用於非霍奇金淋巴瘤的雙步驟預靶向放射免疫治療"的海報描述了CD38-SADA對DOTA螯合的鑭系金屬的選擇性結合及其對CD38的高親和力結合,CD38是一種在多種淋巴瘤細胞中高表達的腫瘤特異性抗原。該海報的數據展示了當CD38-SADA與177銫- DOTA聯用時在雙步驟預靶向放射免疫治療(「PRIT」)中產生的抗腫瘤療效。在異種移植小鼠模型中,腫瘤反應迅速且隨劑量增加而遞增,進一步支持CD38-SADA PRIT在CD38陽性淋巴系統惡性腫瘤患者中的臨床開發。
"This preclinical analysis provides important insights into the unique pharmacology of CD38-SADA and its therapeutic potential for NHL," said Brian H. Santich, Ph.D., the lead author and co-inventor of the SADA PRIT technology platform. "The anti-tumor efficacy positively correlated with increasing doses of Lu177-DOTA and CD38-SADA, which informed the study design and initial dosing regimen of our Trial 1201 in patients with NHL."
"這項前臨床分析爲CD38-SADA的獨特藥理學及其在NHL中的治療潛力提供了重要的見解,"主要作者及SADA PRIT技術平台的共同發明人Brian H. Santich博士說。"抗腫瘤療效與增加的Lu177-DOTA和CD38-SADA劑量呈正相關,這爲我們在NHL患者中的1201號試驗的研究設計和初始劑量方案提供了信息。"
In addition, Y-mAbs presents a trial-in-progress poster from its ongoing Phase 1 (Trial 1201) clinical study evaluating the safety and tolerability of CD38-SADA PRIT with Lu177-DOTA in adults with relapsed or refractory NHL. Trial 1201 is a first-in-human, dose-escalation, open-label, multicenter study composed of two parts. Part A includes dose escalation of the CD38-SADA bispecific fusion protein to define the optimal safe dose of the CD38-SADA protein, the administration interval between CD38-SADA and Lu177-DOTA, and the Lu177-DOTA dose for tumor imaging. In Part B, dose escalation of Lu177-DOTA will establish the optimal therapeutic dose of the radioactive payload. For each part, the escalation is based on a 3+3 trial design of 4 planned dose levels.
此外,Y-mAbs展示了其正在進行的1期(1201號試驗)臨床研究的進行中海報,該研究評估CD38-SADA PRIT與Lu177-DOTA在復發或難治性NHL成年患者中的安全性和耐受性。1201號試驗是首次在人類中進行的劑量遞增、開放標籤、多中心研究,由兩個部分組成。A部分包括CD38-SADA雙特異性融合蛋白的劑量遞增,以確定CD38-SADA蛋白的最佳安全劑量、CD38-SADA與Lu177-DOTA之間的給藥間隔以及用於腫瘤成像的Lu177-DOTA劑量。在B部分,Lu177-DOTA的劑量遞增將確定放射性藥物的最佳治療劑量。每個部分的遞增基於計劃的4個劑量水平的3+3試驗設計。
"We are pleased to share the details of this Phase 1 clinical trial, which is investigating a potentially transformative approach to pre-targeted radioimmunotherapy for patients with relapsed and refractory NHL," said Vignesh Rajah, MBBS, DCH, MRCP (UK), Chief Medical Officer. "This is our second clinical program evaluating the SADA PRIT technology platform and our first in hematological malignancies."
「我們很高興分享這項第一階段臨床試驗的詳細信息,研究一種可能對複發性和難治性非霍奇金淋巴瘤患者具有變革性的預靶向放射免疫治療方法,」首席醫療官Vignesh Rajah, MBBS, DCH, MRCP (UK)說道。「這是我們第二個臨床項目,評估SADA PRIt技術平台,以及我們在血液惡性腫瘤中的首次應用。」
The abstract details are below:
以下是摘要的詳細信息:
Abstract Title: "CD38-SADA, a Self-Assembling and Dis-Assembling Bispecific Fusion Protein for Two-Step Pretargeted Radioimmunotherapy of Non-Hodgkin Lymphoma"
Format: Poster Presentation, ID: 1599
Date and Time: Saturday, December 7, 2024, 5:30 PM-7:30 PM
摘要標題:「CD38-SADA,一種自組裝和解組裝的雙特異性融合蛋白,用於非霍奇金淋巴瘤的兩步預靶向放射免疫治療」
格式:海報展示,ID:1599
日期和時間:2024年12月7日星期六,下午5:30-7:30
Abstract Title: "CD38-SADA Pretargeted Radioimmunotherapy (PRIT) with Lutetium 177 (Lu177)-DOTA in Adult Patients with Relapsed or Refractory Non-Hodgkin Lymphoma: A First-in-Human Phase 1 Trial"
Format: Poster Presentation, ID: 4434.1
Date and Time: Monday, December 9, 2024, 6:00 PM-8:00 PM
摘要標題:"CD38-SADA預靶向放射免疫治療(PRIT)與鑥177(Lu177)-DOTA在成人復發或難治性非霍奇金淋巴瘤中的首次人類I期試驗"
格式:海報展示,ID:4434.1
日期和時間:2024年12月9日,星期一,下午6:00-8:00
Researchers at Memorial Sloan Kettering Cancer Center (MSK), including Dr. Nai-Kong Cheung, developed the SADA technology for radioimmunotherapy, which is exclusively licensed by MSK to Y-mAbs. Dr. Cheung has intellectual property rights and interests in the technology, and as a result of this licensing arrangement, MSK has institutional financial interests in the technology.
紀念斯隆凱特林癌症中心(MSK)的研究人員,包括Nai-Kong Cheung博士,開發了用於放射免疫治療的SADA技術,該技術由MSK專門許可給Y-mAbs。Cheung博士在該技術上擁有知識產權權利和利益,因此由於這一許可安排,MSK在該技術上有機構財務利益。
About Y-mAbs
Y-mAbs is a commercial-stage biopharmaceutical company focused on the development and commercialization of novel, radioimmunotherapy and antibody-based therapeutic cancer products. The Company's technologies include its investigational Self-Assembly DisAssembly ("SADA") Pretargeted Radioimmunotherapy Platform ("PRIT") and bispecific antibodies generated using the Y-BiClone platform. The Company's broad and advanced product pipeline includes the anti-GD2 therapy DANYELZA (naxitamab-gqgk), the first FDA-approved treatment for patients with relapsed or refractory high-risk neuroblastoma in the bone or bone marrow after a partial response, minor response, or stable disease to prior therapy.
關於Y-mAbs
Y-mAbs是一家商業化生物製藥公司,專注於開發和商業化新型放射免疫治療和基於抗體的癌症治療產品。該公司的技術包括其調查中的自組裝和解組裝("SADA") Pretargeted免疫療法平台("PRIT")和使用Y-BiClone平台生成的雙特異性抗體。公司廣泛而先進的產品管道包括針對GD2的治療DANYELZA(Naxitamab-gqgk),這是FDA首次批准的針對骨骼或骨髓中復發或難治的高風險神經母細胞瘤患者,其之前接受過部分響應、輕微響應或穩定疾病治療的治療。
About CD38-SADA PRIT
CD38-SADA is a bispecific fusion protein that tightly binds to the CD38 antigen and to select radionuclides chelated to tetraxetan (or "DOTA"). CD38-SADA contains a p53-derived domain that drives the self-assembly of CD38-SADA tetramers, which possess four distinct binding sites for CD38. In the first step of pre-targeted radiotherapy, non-radiolabeled-CD38-SADA tetramers are infused and bind with high avidity to CD38-positive tumors, while unbound CD38-SADA disassembles into low molecular weight monomers that are removed by the kidney. The second infusion delivers the "radioactive payload," which binds to the CD38-SADA on tumor cells for localized irradiation. CD38-SADA PRIT with Lutetium 177 (Lu 177)-DOTA is now under clinical investigation in Trial 1201 (NCT05994157).
關於CD38-SADA PRIT
CD38-SADA是一種雙特異性融合蛋白,能夠緊密結合CD38抗原和與四氟乙烯(或「DOTA」)螯合的選擇性放射性核素。CD38-SADA包含一個來自p53的結構域,驅動CD38-SADA四聚體的自組裝,這些四聚體具有四個獨特的CD38結合位點。在預靶向放射治療的第一步中,非放射性標記CD38-SADA四聚體被輸注,並以高親和力與CD38陽性腫瘤結合,而未結合的CD38-SADA則解聚成低分子量單體,被腎臟排除。第二次輸注傳遞「放射性載荷」,與腫瘤細胞上的CD38-SADA結合,以實現局部照射。帶有鉺177(Lu 177)DOTA的CD38-SADA PRIT目前正在臨床研究中,試驗編號爲1201(NCT05994157)。
Forward-Looking Statements
Statements in this press release about future expectations, plans and prospects, as well as any other statements regarding matters that are not historical facts, may constitute "forward-looking statements" within the meaning of Section 27A of the Securities Act of 1933 and Section 21E of the Securities Exchange Act of 1934. Such statements include, but are not limited to, statements about our business model, including financial outlook for 2024 and beyond, including estimated operating expenses, use of cash and cash equivalents and DANYELZA product revenue and sufficiency of cash resources and related assumptions; expectations with respect to the Company's future financial performance; implied and express statements regarding the future of the Company's business, including with respect to expansion and its goals; expectations with respect to the Company's plans and strategies, development, regulatory, commercialization and product distribution plans, including the timing thereof; expectations with respect to the Company's products and product candidates, including potential territory and label expansion of DANYELZA and the potential market opportunity related thereto and potential benefits thereof, and the potential of the SADA PRIT technology and potential benefits and applications thereof; expectations relating to key anticipated development milestones, including potential expansion and advancement of commercialization and development efforts, including potential indications, applications and geographies, and the timing thereof; expectations with respect to current and future clinical and pre-clinical studies and the Company's research and development programs, including with respect to timing and results; expectations regarding collaborations or strategic partnerships and the potential benefits thereof; and other statements that are not historical facts. Words such as ''anticipate,'' ''believe,'' "contemplate," ''continue,'' ''could,'' ''estimate,'' ''expect,'' "hope," ''intend,'' ''may,'' ''might,'' ''plan,'' ''potential,'' ''predict,'' ''project,'' ''should,'' ''target,'' "will," ''would',' "guidance," "goal," "objective," and similar expressions are intended to identify forward-looking statements, although not all forward-looking statements contain these identifying words. Our product candidates and related technologies are novel approaches to cancer treatment that present significant challenges. Actual results may differ materially from those indicated by such forward-looking statements as a result of various factors, including but not limited to: risks associated with the Company's financial condition and need for additional capital; the risks that actual results of the Company's restructuring plan and revised business plan will not be as expected; risks associated with the Company's development work; cost and success of the Company's product development activities and clinical trials; the risks of delay in the timing of the Company's or its partners' regulatory submissions or failure to receive approval of its drug candidates; the risks related to commercializing any approved pharmaceutical product including the rate and degree of market acceptance of product candidates; development of sales and marketing capabilities and risks associated with failure to obtain sufficient reimbursement for products; risks related to the Company's dependence on third parties including for conduct of clinical testing and product manufacture as well as regulatory submissions; the Company's ability to enter into new partnerships or to recognize the anticipated benefits from its existing partnerships; risks related to government regulation; risks related to market approval, risks associated with protection of the Company's intellectual property rights; risks related to employee matters and managing growth; risks related to the Company's common stock, risks associated with macroeconomic conditions, including the conflict between Russia and Ukraine and sanctions related thereto, the state of war between Israel and Hamas and the related risk of a larger regional conflict, inflation, increased interest rates, uncertain global credit and capital markets and disruptions in banking systems; and other risks and uncertainties affecting the Company including those described in the "Risk Factors" section included in the Company's Annual Report on Form 10-K for the fiscal year ended December 31, 2023, and the Company's Quarterly Report on Form 10-Q for the quarterly periods ended March 31, 2024, and September 30, 2024, and future filings and reports by the Company. Any forward-looking statements contained in this press release speak only as of the date hereof, and the Company undertakes no obligation to update any forward-looking statement, whether as a result of new information, future events or otherwise.
前瞻性聲明
本新聞稿中關於未來期望、計劃和前景的聲明,以及任何涉及非歷史事實的事項的聲明,可能構成《1933年證券法》第27A條和《1934年證券交易法》第21E條規定的「前瞻性陳述」。這些聲明包括但不限於關於我們的業務模式,包括2024年及以後的財務展望,包括估計的營業費用、現金及現金等價物的使用以及DANYELZA產品營業收入和現金資源充足性及相關假設;關於公司未來財務表現的期望;暗示和明示關於公司業務未來的聲明,包括擴張和目標;關於公司計劃和戰略、發展、監管、商業化和產品分銷計劃的期望,包括其計劃進行的時間;關於公司產品和產品候選藥物的期望,包括DANYELZA潛在領地和標籤擴展以及潛在市場機會以及其潛在利益,以及SADA PRIt技術的潛力和潛在利益和應用;關於關鍵預期發展里程碑的期望,包括商業化和開發工作的潛在擴展和推進,包括潛在適應症、應用和地理位置,以及時間;關於當前和未來臨床和臨床前研究以及公司研發項目的期望,包括時間和結果;關於合作伙伴關係或戰略合作伙伴關係的期望和潛在利益;以及其他非歷史事實的聲明。諸如「預計」、「相信」、「考慮」、「繼續」、「可能」、「估計」、「期望」、「希望」、「打算」、「可能」、「可能」、「計劃」、「潛力」、「預測」、「項目」、「應該」、「目標」、「將」、「願景」、「目標」和類似表述等旨在識別前瞻性語句,儘管並非所有前瞻性語句都包含這些識別詞。我們的產品候選藥物和相關技術是癌症治療的新穎方法,面臨着重大挑戰。由於各種因素,實際結果可能會有所不同,包括但不限於:與公司財務狀況和需求的風險相關的風險;公司重組計劃和修訂後的業務計劃的實際結果不如預期的風險;與公司開發工作相關的風險;公司產品開發活動和臨床試驗的成本和成功的風險;公司或其合作伙伴的監管提交時間延遲或未收到藥物候選藥的批准的風險;與商業化任何獲批製藥產品相關的風險,包括產品候選藥物的市場接受程度和速度;銷售和營銷能力的發展以及未能獲得足夠產品報銷的風險;涉及第三方的依賴性風險,包括進行臨床試驗和產品製造以及監管提交;公司進入新合作伙伴關係或認識到現有合作伙伴關係所期待的利益的風險;與政府監管相關的風險;與市場批准相關的風險,與保護公司知識產權權益相關的風險;與員工事務和管理增長相關的風險;與公司普通股相關的風險,與宏觀經濟狀況相關的風險,包括俄羅斯與烏克蘭之間的衝突及相關制裁,以色列與哈馬斯之間的戰爭狀態以及與之相關的更大區域衝突風險,通貨膨脹,利率上升,全球信貸和資本市場不確定性以及銀行系統的中斷;影響公司的其他風險和不確定性,包括公司年度報告10-k中包含的描述的風險因素,該報告覆蓋截至2023年1月31日財年的公司年度報告,以及公司截至2024年3月31日和9月30日每季度的公司的季度報告第10-q,以及公司未來的備案和報告。本新聞稿中包含的所有前瞻性聲明僅截至日期,在此之後,公司不承擔更新任何前瞻性聲明的義務,無論是否有新信息、未來事件或其他原因。
SADA, SADA PRIT, DANYELZA and Y-mAbs are registered trademarks of Y-mAbs Therapeutics, Inc.
SADA、SADA PRIt、DANYELZA和Y-mAbs是Y-mAbs Therapeutics, Inc.的註冊商標。
Investor Contact:
Courtney Dugan
VP, Head of Investor Relations
[email protected]
投資者聯繫人:
Courtney Dugan
VP,投資者關係負責人
[email protected]
Source: Y-mAbs Therapeutics, Inc.
來源:Y-mAbs Therapeutics, Inc.
譯文內容由第三人軟體翻譯。
