Actinium Highlights Ability of Iomab-B to Overcome High-Risk TP53 Mutation Resulting in Significant Improvement in Overall Survival in Patients With Active Relapsed Refractory AML at the European Bone Marrow Transplant Annual Meeting
Actinium Highlights Ability of Iomab-B to Overcome High-Risk TP53 Mutation Resulting in Significant Improvement in Overall Survival in Patients With Active Relapsed Refractory AML at the European Bone Marrow Transplant Annual Meeting
-- Iomab-B led bone marrow transplant produced high rates of complete remission and durable complete remission regardless of TP53 mutation status in patients age 55 and above with high-risk active relapsed or refractory acute myeloid leukemia
— 無論年齡在55歲及以上的高風險活動性復發或難治性急性髓系白血病患者TP53突變狀態如何,Iomab-B主導的骨髓移植都能產生較高的完全緩解率和持久的完全緩解率
-- Median Overall Survival of 5.49 months observed in patients with a TP53 mutation receiving an Iomab-B led allogeneic bone marrow transplant compared to 1.66 months in patients that did not receive Iomab-B (hazard ratio=0.23, p=0.0002)
— 在接受Iomab-B主導的異基因骨髓移植的TP53突變患者中,觀察到的總存活期中位數爲5.49個月,而未接受Iomab-B的患者的總存活期中位數爲1.66個月(危險比=0.23,p=0.0002)
NEW YORK, April 18, 2024 /PRNewswire/ -- Actinium Pharmaceuticals, Inc. (NYSE AMERICAN: ATNM) (Actinium or the Company), a leader in the development of Antibody Radiation Conjugates (ARCs) and other targeted radiotherapies, today announced that results from the Phase 3 SIERRA trial of Iomab-B were presented in an oral presentation at the 50th Annual European Bone Marrow Transplant Society Meeting (EBMT) held in Glasgow, Scotland on April 14-17. The results showed that an Iomab-B led bone marrow transplant (BMT) results in higher rates of remissions and durable Complete Remission (dCR), which is the primary endpoint of the SIERRA trial, as well as significant improvement in overall survival in TP53 positive patients. Iomab-B is a targeted radiotherapeutic comprised of an anti-CD45 monoclonal antibody with the Iodine-131 radioisotope payload. The Phase 3 SIERRA trial enrolled 153 patients age 55 and above with active relapsed or refractory acute myeloid leukemia (AML) and compared outcomes of patients receiving Iomab-B BMT to those of patients receiving physician's choice of care in the control arm. In total, 24% (37/153) of the patients enrolled on SIERRA had a TP53 mutation, which is associated with limited treatment options and poor outcomes.
紐約,2024 年 4 月 18 日 /PRNewswire/ — Actinium 製藥有限公司 抗體輻射偶聯物(ARC)和其他靶向放射療法開發的領導者(紐約證券交易所美國股票代碼:ATNM)(Actinium或公司)今天宣佈,Iomab-B的IOMAB-B三期SIERRA試驗結果已在50強的口頭陳述中公佈第四 歐洲骨髓移植協會年度會議(EBMT)於4月14日至17日在蘇格蘭格拉斯哥舉行。結果表明,Iomab-B主導的骨髓移植(BMT)可提高緩解率和持久的完全緩解(dCr),這是SIERRA試驗的主要終點,並顯著提高了TP53陽性患者的總體存活率。Iomab-B 是一種靶向放射治療藥物,由具有碘-131放射性同位素有效載荷的抗CD45單克隆抗體組成。SIERRA的3期試驗招收了153名年齡在55歲及以上的活動性復發或難治性急性髓系白血病(AML)患者,並將接受Iomab-B B骨髓移植的患者與在對照組接受醫生選擇的治療的患者的預後進行了比較。總的來說,在SIERRA註冊的患者中,有24%(37/153)的患者有TP53突變,這與治療選擇有限和預後不佳有關。
Data highlighted in the ASH oral presentation, which can be accessed on the investor relations page of Actinium's website, included:
可在Actinium網站的投資者關係頁面上訪問的ASH口頭陳述中重點介紹的數據包括:
Response rates by TP53 Mutation Status:
按 TP53 突變狀態劃分的響應率:
|
Iomab-B & Crossover |
Control Arm | |
|
TP53 Positive |
N=27 |
N=10 |
|
CR |
55.56% (15/27) |
0 % |
|
dCR |
14.81% (4/27) |
0 % |
|
TP53 Wildtype |
N=93 |
N=23 |
|
CR |
58.06% (54/93) |
17.39% (4/23) |
|
dCR |
16.13% (15/93) |
0 % |
|
Iomab-B 和 Crossover |
控制臂 | |
|
TP53 陽性 |
N = 27 |
N = 10 |
|
CR |
55.56% (15/27) |
0% |
|
dCr |
14.81% (4/27) |
0% |
|
TP53 野性類型 |
N = 93 |
N = 23 |
|
CR |
58.06% (54/93) |
17.39% (4/23) |
|
dCr |
16.13% (15/93) |
0% |
Overall Survival in Patients with a TP53 Mutation:
TP53 突變患者的總存活率:
|
Iomab-B & Crossover |
Control Arm | |
|
Median OS |
5.49 months |
1.66 months |
|
Number of Patients |
27 |
10 |
|
Hazard Ratio |
0.23 | |
|
p-value |
0.0002 | |
|
Iomab-B 和 Crossover |
控制臂 | |
|
中位操作系統 |
5.49 個月 |
1.66 個月 |
|
患者人數 |
27 |
10 |
|
危險比率 |
0.23 | |
|
p 值 |
0.0002 | |
Median OS was 6.37 months in TP53 negative patients receiving Iomab-B and 5.72 months for TP53 positive patients demonstrating Iomab-B's ability to overcome TP53 gene mutations.
接受Iomab-B治療的TP53陰性患者的操作系統中位數爲6.37個月,TP53陽性患者的操作系統中位數爲5.72個月,這表明Iomab-B有能力克服TP53基因突變。
Dr. Hannah Choe, Assistant Professor of Medicine at Ohio State University and SIERRA trial investigator, commented, "TP53 mutations are associated with very poor outcomes due to resistance to anti-leukemic therapies with patients rarely offered access to potentially curative transplantation. The SIERRA trial showed that Iomab-B was well tolerated and can enable unprecedented access to transplant in this patient population and induce high complete remission rates despite active, relapsed/refractory disease and a TP53 mutation. These results were very well received at EBMT and demonstrate the novelty and safety of a CD45-directed antibody radiation conjugate. More importantly, we see that these response rates translated into improved overall survival, overcoming the increased risk associated with TP53 mutation while no other viable treatment options exist. We are excited for Iomab-B's potential use and safety for disease control in patients with a TP53 mutation."
俄亥俄州立大學醫學助理教授、SIERRA試驗研究員Hannah Choe博士評論說:“由於抗白血病療法的耐藥性,TP53突變與非常差的預後有關,患者很少有機會獲得潛在的治療性移植。SIERRA試驗表明,Iomab-B具有良好的耐受性,儘管存在活動性、復發/難治性疾病和TP53突變,但仍能爲該患者群體提供前所未有的移植機會,並可誘發較高的完全緩解率。這些結果在EBMT上廣受好評,證明了CD45定向抗體輻射偶聯物的新穎性和安全性。更重要的是,我們看到這些反應率轉化爲總體存活率的提高,克服了與TP53突變相關的增加的風險,而沒有其他可行的治療方案。我們對Iomab-B在TP53突變患者疾病控制中的潛在用途和安全性感到興奮。”
About the EBMT Annual Meeting
關於EBMT年會
The Annual Meeting of the EBMT is attended by more than 5,500 participants, including physicians, nurses, data managers, statisticians, quality managers, cell therapists, paediatricians, pharmacists, psychologists, psychiatrists and psychoanalysts, transplant coordinators, lab scientists, trainees, and patients. This important congress ensures and encourages dialogues and information exchange, education and scientific productivity.
EBMT年會有超過5,500名參與者出席,包括醫生、護士、數據經理、統計學家、質量經理、細胞治療師、兒科醫生、藥劑師、心理學家、精神科醫生和心理分析師、移植協調員、實驗室科學家、學員和患者。這次重要的大會確保並鼓勵對話和信息交流、教育和科學生產力。
The full annual meeting program is available online at:
完整的年會計劃可在以下網址在線獲取:
About Actinium Pharmaceuticals, Inc.
關於 Actinium 製藥公司
Actinium develops targeted radiotherapies to meaningfully improve survival for people who have failed existing oncology therapies. Advanced pipeline candidates Iomab-B (pre-BLA & MAA (EU)), an induction and conditioning agent prior to bone marrow transplant, and Actimab-A (National Cancer Institute CRADA pivotal development path), a therapeutic agent, have demonstrated potential to extend survival outcomes for people with relapsed and refractory acute myeloid leukemia. Actinium plans to advance Iomab-B for other blood cancers and next generation conditioning candidate Iomab-ACT to improve cell and gene therapy outcomes. Actinium holds more than 230 patents and patent applications including several patents related to the manufacture of the isotope Ac-225 in a cyclotron.
Actinium開發了靶向放射療法,以有意義地提高現有腫瘤療法失敗者的存活率。先進的候選藥物Iomab-B(BLA和MAA(歐盟)之前)是骨髓移植前的誘導和調理劑,以及治療藥物Actimab-A(美國國家癌症研究所CRADA關鍵開發路徑)已證明有可能延長復發和難治性急性髓系白血病患者的存活結果。Actinium計劃推進用於其他血液癌的Iomab-B和下一代治療候選藥物Iomab-Act,以改善細胞和基因療法的結果。Actinium擁有230多項專利和專利申請,其中包括多項與在迴旋加速器中製造同位素Ac-225相關的專利。
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Forward-Looking Statements
前瞻性陳述
This press release may contain projections or other "forward-looking statements" within the meaning of the "safe-harbor" provisions of the private securities litigation reform act of 1995 regarding future events or the future financial performance of the Company which the Company undertakes no obligation to update. These statements are based on management's current expectations and are subject to risks and uncertainties that may cause actual results to differ materially from the anticipated or estimated future results, including the risks and uncertainties associated with preliminary study results varying from final results, estimates of potential markets for drugs under development, clinical trials, actions by the FDA and other governmental agencies, regulatory clearances, responses to regulatory matters, the market demand for and acceptance of Actinium's products and services, performance of clinical research organizations and other risks detailed from time to time in Actinium's filings with the Securities and Exchange Commission (the "SEC"), including without limitation its most recent annual report on form 10-K, subsequent quarterly reports on Forms 10-Q and Forms 8-K, each as amended and supplemented from time to time.
本新聞稿可能包含1995年《私人證券訴訟改革法》關於公司未來事件或未來財務業績的 “安全港” 條款所指的預測或其他 “前瞻性陳述”,公司沒有義務更新這些條款。這些聲明基於管理層當前的預期,受風險和不確定性的影響,這些風險和不確定性可能導致實際結果與預期或估計的未來結果存在重大差異,包括與初步研究結果相關的風險和不確定性,這些結果與最終結果、對在研藥物潛在市場的估計、臨床試驗、FDA和其他政府機構的行動、監管許可、對監管問題的回應、市場對Actinium產品的需求和接受度以及服務、臨床研究機構的表現和其他風險在Actinium向美國證券交易委員會(“SEC”)提交的文件中不時詳述,包括但不限於其最新的10-K表年度報告以及隨後的10-Q表和8-K表季度報告,每份報告均不時修訂和補充。
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SOURCE Actinium Pharmaceuticals, Inc.
來源 actinium Pharmicals, Inc
譯文內容由第三人軟體翻譯。