MP0533: Phase 1 trial continues to demonstrate acceptable safety and antitumor activity up to cohort 6, dosing in cohort 7 ongoing, additional dose escalation cohorts being prepared
Radio-DARPin Therapy (RDT): Lead DLL3 candidate advancing into IND-enabling studies with partner Orano Med, preclinical data to be presented at SNMMI 2024
Switch-DARPin Platform: Initial data to be presented at EHA 2024; Preclinical proof-of-concept studies for c-KIT program planned for H2 2024
MP0317: Final data from Phase 1 dose escalation to be presented at ASCO 2024
Outlook: Funded into 2026 with cash and short-term deposits of CHF 174.1 million; total operating expenses of CHF 70-80 million expected for 2024
ZURICH-SCHLIEREN, Switzerland and CONCORD, Mass., May 16, 2024 (GLOBE NEWSWIRE) -- Ad hoc announcement pursuant to Art. 53 LR Molecular Partners AG (SIX: MOLN; NASDAQ: MOLN), a clinical-stage biotech company pioneering the design and development of DARPin therapeutics for medical challenges that other drug modalities cannot readily address ("Molecular Partners" or the "Company"), today announced corporate highlights and unaudited financial results for the first quarter of 2024.
"This quarter we demonstrated continued progress across our clinical and preclinical pipeline with preparations underway for two new clinical candidates and first-in-human data for our Radio DARPin platform in 2025," said Patrick Amstutz, Ph.D., Molecular Partners' Chief Executive Officer. "Building on encouraging initial data and clinical activity, MP0533 dose escalation will expand and now explore higher potential doses, to see what the true clinical impact can be and which patient subpopulations can benefit most. We plan to share data from these higher dose clinical cohorts starting in the second half of this year. For our emerging pipeline, we plan to announce preclinical data from our Switch-DARPin Platform at EHA and anticipate translational efficacy data in the second half of 2024. Our lead Radio-DARPin candidate is advancing into IND-enabling studies in collaboration with our partner Orano Med, with initiation of clinical studies planned for 2025 and pre-clinical data to be presented at SNMMI in June 2024."
Financial and Business Outlook
For the full year 2024, at constant exchange rates, the Company expects total operating expenses of CHF 70-80 million, remaining consistent with the prior year. Of this figure, approximately CHF 8 million will be non-cash effective costs for share-based payments, IFRS pension accounting and depreciation.
With CHF 174.1 million in cash and short-term time deposits and no debt as of March 31, 2024, the Company expects to be funded well into 2026. This guidance does not include any potential receipts from R&D partnerships.
Research & Development Highlights
MP0533: Clinical update and planned dose escalation expansion
MP0533 (CD33 x CD123 x CD70 x CD3), a novel tetra-specific T cell-engaging DARPin, is currently being evaluated in a Phase 1/2a clinical trial for patients with relapsed/refractory acute myeloid leukemia (r/r AML) and myelodysplastic syndrome/AML (MDS/AML) (NCT05673057).
Results presented at the American Society of Hematology (ASH) Annual Meeting 2023 from the first 11 patients treated with MP0533 indicated a favorable safety profile across the first four dosing regimens (DRs), with no dose-limiting toxicities observed. The study is on track with DR 7 enrollment complete and dosing currently ongoing. Based on the current MP0533 safety data and discussion with treating physicians and key opinion leaders, a protocol amendment was filed on April 25, 2024 to expand enrollment to higher dose cohorts (DRs 8-11) for further characterization of the MP0533 dose-response. The company expects to enroll patients in higher cohorts seamlessly in the second half of 2024.
The mechanism of action of MP0533 is designed to preferentially kill AML cells (blasts and leukemic progenitor and stem cells) that express any combination of the cell surface antigens CD33, CD123, and CD70, while sparing healthy cells which tend to express only one or none of these targets. Updated data, with cut-off as of March 12, 2024, show that MP0533 continues to demonstrate clinical activity similar to what has been reported in earlier dose cohorts. In DRs 5 and 6, an additional 17 patients were treated with MP0533, and of these, 2 patients reached ELN criteria of Morphological Leukemia Free State (MLFS), with additional patients showing early blast reductions in the bone marrow. The drug safety profile remains acceptable with the majority of adverse events reported as infusion-related reactions and cytokine release syndrome. The current data supports expansion to higher dose cohorts to explore the activity of MP0533 in a highly heterogeneous r/r AML patient population. Diverse parameters (e.g., leukemic stem cells, clonal evolution, immune activation) are being examined to inform the next development steps including the potential of earlier lines of treatment, and combination settings. The Company anticipates providing a next clinical update from the study in the second half of 2024 at a scientific congress.
Radio-DARPin Therapy Platform
Molecular Partners continues to advance its RDT platform and programs. At the J.P. Morgan Healthcare Conference in January 2024, the company presented data demonstrating successful increase of tumor uptake and reduction of kidney absorption by applying novel engineering approaches to modify the DARPin backbone (Stealth-DARPins) and its half-life. This enabled further internal progress of the RDT platform and pipeline expansion.
Also in January 2024, Molecular Partners entered a strategic collaboration with Orano Med to co-develop 212Pb-based RDTs for patients with solid tumors. The collaboration combines the power of DARPins, as a highly differentiated modality for tumor-targeted delivery of radioisotopes, with Orano Med's leading capabilities in Targeted Alpha Therapy and supply, to further advance the RDT platform and expand Molecular Partners' RDT portfolio.
The tumor-associated protein Delta-like ligand 3 (DLL3) was selected as the target of the Company's lead RDT program to be advanced into IND-enabling studies in the first half of 2024. The initiation of clinical studies and first-in-human data for our RDT platform are expected in 2025 through co-development with Orano Med.
Molecular Partners will provide an update in an oral presentation at the Society of Nuclear Medicine and Molecular Imaging (SNMMI) Annual Meeting 2024 in Toronto on June 11.
Abstract Title: Lead-212 Radio-DARPin Therapeutic (RDT) targeting delta-like ligand 3 (DLL3) shows promising preclinical antitumor efficacy and tolerability in small cell lung cancer (SCLC)
Session Title: Integrated Session: Radionuclides (CMIIT/RPSC)
Presentation Timing: June 11, 2024; 8:00-9:15 am local time
Molecular Partners also expects to nominate additional targets and RDT candidates in 2024.
In addition, Molecular Partners continued to progress its RDT portfolio of projects in partnership with Novartis.
Switch-DARPin Platform
The Switch-DARPin platform provides a logic-gated "on/off" function (the "Switch") to multispecific DARPin candidates leading to target activation only in the presence of defined antigens. The objective is conditional activation of a targeted immune response. The first Switch-DARPin program (cKIT x CD16a x CD47) was introduced at the annual J.P. Morgan Healthcare Conference in January 2024. This approach is designed to induce exhaustive killing of hematopoietic stem cells as next-generation conditioning regimen to increase long-term disease control post hematopoietic stem cell transplant (HSCT) for AML patients, including those with a poor cytogenetic risk profile, and those currently not eligible for standard high-intensity conditioning. Our intent is to extend the access to potentially curative HSCT for more patients with AML as well as additional hematologic malignancies, and genetic diseases requiring HSC transplant.
The company will present initial preclinical data at the European Hematology Association (EHA) Congress 2024 in Madrid on June 14 and has planned preclinical proof-of-concept studies for the second half of 2024.
EHA 2024 Abstract Title: C-KIT X CD16a X CD47 Switch-DARPin with conditional blockade of CD47: a next-generation targeted conditioning for hematopoietic stem cell transplantation
Session Title: Stem Cell Transplantation – Experimental
Abstract Number for Publication: P1294
Poster Session Timing: June 14, 2024; 6-7 pm CET
MP0317: Final Phase 1 data at ASCO
MP0317 simultaneously targets CD40 and fibroblast activation protein (FAP) to enable tumor-localized immune activation. The phase 1 dose-escalation study of MP0317 in patients with advanced solid tumors (NCT05098405) was completed in January 2024. The final outcomes of the 46 treated patients will be presented at the American Society of Clinical Oncology (ASCO) Annual Meeting 2024 in Chicago, IL on June 1.
Abstract Title: Effect of MP0317, a FAP x CD40 DARPin, on safety profile and tumor-localized CD40 activation in a phase 1 study in patients with advanced solid tumors.
Session Title: Developmental Therapeutics - Immunotherapy
Abstract Number: 2573
Poster Session Timing: June 1, 2024 from 9:00 am CDT (Hall A)
Corporate and Management Highlights
On February 5, 2024 a putative class action complaint against the Company, its directors, and certain of its executive officers was dismissed without prejudice in the Company's favor, and the plaintiff filed a stipulation of dismissal with prejudice on February 23, 2024. The case was ordered closed on February 29, 2024. The original case was filed on July 12, 2022 in the U.S. District Court for the Southern District of New York.
At the Company's Annual General Meeting on April 17 2024, all motions proposed by the Board of Directors at the Annual General Meeting were approved by the shareholders of the Company.
Financial Calendar
August 26, 2024 – Publication of Half-year Results 2024 (unaudited)
October 31, 2024 – Interim Management Statement Q3 2024
MP0533:1期試驗繼續顯示出可接受的安全性和抗腫瘤活性,隊列6仍在繼續,第7隊列的劑量仍在進行中,其他劑量遞增隊列正在準備中
radio-Darpin Therapy(RDT):領先的DLL3候選人與合作伙伴Orano Med一起進入支持IND的研究,臨床前數據將在SNMI 2024上公佈
Switch-DARPIN 平台:初步數據將在 EHA 2024 上公佈;計劃於 2024 年下半年對 C-kit 項目進行臨床前概念驗證研究
MP0317:第 1 階段劑量遞增的最終數據將在 ASCO 2024 上公佈
展望:到2026年,現金和短期存款爲1.741億瑞士法郎;預計2024年的總運營支出爲7000萬至8000萬瑞士法郎
瑞士蘇黎世-施利倫和馬薩諸塞州康科德,2024年5月16日(GLOBE NEWSWIRE)——根據LR Molecular Partners AG(SIX:MOLN;納斯達克股票代碼:MOLN)第53條發佈的臨時公告今天公佈了公司要點。該公司是一家臨床階段的生物技術公司,率先設計和開發DarPin療法,以應對其他藥物模式無法輕易解決的醫學挑戰(“分子合作伙伴” 或 “公司”)以及2024年第一季度未經審計的財務業績。
Molecular Partners首席執行官帕特里克·阿姆斯圖茲博士表示:“本季度,我們的臨床和臨床前產品線持續取得進展,正在準備在2025年爲我們的Radio DarPin平台提供兩種新的臨床候選藥物和首次人體數據。”“在令人鼓舞的初始數據和臨床活動基礎上,MP0533 劑量遞增將擴大,現在將探索更高的潛在劑量,以了解真正的臨床影響以及哪些患者亞群受益最大。我們計劃從今年下半年開始共享來自這些高劑量臨床隊列的數據。對於我們新興的產品線,我們計劃在EHA公佈來自我們的Switch-DARPIN平台的臨床前數據,並預計將在2024年下半年公佈轉化療效數據。我們的主要Radio-DARPIN候選人正在與我們的合作伙伴Orano Med合作推進支持IND的研究,計劃於2025年啓動臨床研究,臨床前數據將於2024年6月在SNMMI上公佈。”
財務和商業展望
2024年全年,按固定匯率計算,公司預計總運營支出爲7000萬至8000萬瑞士法郎,與上年持平。在這一數字中,大約800萬瑞士法郎將是基於股份的支付、國際財務報告準則養老金會計和折舊的非現金有效成本。
公司擁有1.741億瑞士法郎的現金和短期定期存款,截至2024年3月31日沒有債務,預計資金將持續到2026年。本指南不包括來自研發合作伙伴關係的任何潛在收入。
研究與開發亮點
MP0533:臨床更新和計劃中的劑量遞增擴大
MP0533(CD33 x CD123 x CD70 x CD3)是一種新的四特異性T細胞參與DarPIN,目前正在針對復發/難治性急性髓系白血病(r/r AML)和骨髓增生異常綜合徵/AML(MDS/AML)(NCT05673057)患者的1/2a期臨床試驗中進行評估。
在美國血液學會(ASH)2023年年會上公佈的首11名接受 MP0533 治療的患者的結果表明,前四種給藥方案(DR)的安全性良好,未觀察到劑量限制毒性。該研究已步入正軌,DR 7的註冊已完成,目前正在進行給藥。根據當前的 MP0533 安全數據以及與主治醫生和主要意見領袖的討論,2024 年 4 月 25 日提交了一項協議修正案,將入學範圍擴大到更高劑量群組(DRs 8-11),以進一步描述 MP0533 的劑量反應。該公司預計將在2024年下半年無縫地將患者納入更高的群組。
MP0533 的作用機制旨在優先殺死表達細胞表面抗原 CD33、CD123 和 CD70 任意組合的急性髓細胞白血病細胞(細胞、白血病祖細胞和幹細胞),同時保留往往只表達一種或不表達這些靶標的健康細胞。最新數據(截止日期爲 2024 年 3 月 12 日)顯示,MP0533 繼續表現出與早期劑量隊列中報告的臨床活性相似。在 DrS 5 和 6 中,另有 17 名患者接受了 MP0533 治療,其中 2 名患者達到了形態學白血病自由狀態 (MLFS) 的 ELN 標準,還有其他患者表現出骨髓早期爆炸減少的跡象。藥物安全性狀況仍然可以接受,大多數不良事件報告爲輸液相關反應和細胞因子釋放綜合徵。當前的數據支持擴展到更高劑量的隊列,以探索 MP0533 在高度異構的復發/難治性急性髓細胞白血病患者群體中的活性。正在研究各種參數(例如白血病幹細胞、克隆進化、免疫激活),爲下一步的開發步驟提供信息,包括早期治療的潛力和組合設置。該公司預計將於2024年下半年在科學大會上提供該研究的下一次臨床更新。
Radio-DARPIN 治療平台
分子合作伙伴繼續推進其RDT平台和計劃。在2024年1月的摩根大通醫療保健會議上,該公司公佈的數據表明,通過應用新的工程方法來修改DarPin骨幹(Stealth-Darpins)及其半衰期,成功地增加了腫瘤的吸收並減少了腎臟吸收。這使得RDT平台的內部進展和管道擴展得以進一步發展。
同樣在 2024 年 1 月,Molecular Partners 與 Orano Med 建立了戰略合作,爲實體瘤患者共同開發基於 212Pb的RDT。此次合作將DarPins作爲一種高度差異化的腫瘤靶向放射性同位素輸送方式的強大功能與Orano Med在靶向α療法和供應方面的領先能力相結合,以進一步推進RDT平台並擴大分子合作伙伴的RDT產品組合。
腫瘤相關蛋白質Delta樣配體3(DLL3)被選爲公司主要RDT計劃的目標,該項目將在2024年上半年進入支持IND的研究。通過與Orano Med的共同開發,我們的RDT平台的臨床研究和首次人體數據預計將於2025年啓動。
Molecular Partners將於6月11日在多倫多舉行的2024年核醫學與分子影像學會(SNMMI)年會上口頭介紹最新情況。
摘要標題:靶向 delta 樣配體 3 (DLL3) 的 Lead-212 radio-DARPIN 治療 (RDT) 在小細胞肺癌 (SCLC) 中顯示出令人鼓舞的臨床前抗腫瘤療效和耐受性
會議標題:綜合會議:放射性核素(CMIIT/RPSC)
演講時間:2024 年 6 月 11 日;當地時間上午 8:00-9:15
分子合作伙伴還預計將在2024年提名更多靶點和RDT候選人。
此外,Molecular Partners繼續與諾華合作推進其RDT項目組合。
Switch-DARPIN 平台
Switch-Darpin平台爲多特異性darPin候選物提供邏輯門控的 “開/關” 功能(“開關”),只有在已定義的抗原存在的情況下才能激活靶標。目標是有條件地激活靶向免疫反應。第一個Switch-DARPIN計劃(CKit x CD16a x CD47)是在2024年1月的摩根大通醫療保健年度會議上推出的。這種方法旨在誘導徹底殺死造血幹細胞,作爲下一代調理方案,以增強急性髓細胞白血病患者(包括細胞遺傳學風險狀況較差的患者,以及目前沒有資格接受標準高強度調理的患者)在造血幹細胞移植(HSCT)後的長期疾病控制。我們的目的是擴大更多急性髓細胞白血病、其他血液系統惡性腫瘤和需要HSC移植的遺傳性疾病患者獲得可能治癒的HSCT的機會。
該公司將於6月14日在馬德里舉行的2024年歐洲血液學協會(EHA)大會上公佈初步的臨床前數據,並計劃在2024年下半年進行臨床前概念驗證研究。
EHA 2024 摘要標題:C-KIT X CD16a X CD47 switch-DARPIN 帶條件阻斷 CD47:造血幹細胞移植的下一代靶向調節
會議標題:幹細胞移植 — 實驗
出版摘要編號:P1294
海報發佈會時間:2024 年 6 月 14 日;歐洲中部時間下午 6-7 點
MP0317:ASCO 第 1 階段的最終數據
MP0317 同時靶向 CD40 和成纖維細胞活化蛋白 (FAP),以實現腫瘤局部免疫激活。針對晚期實體瘤(NCT05098405)患者 MP0317 的 1 期劑量遞增研究已於 2024 年 1 月完成。46名接受治療的患者的最終結果將於6月1日在伊利諾伊州芝加哥舉行的美國臨床腫瘤學會(ASCO)2024年年會上公佈。
摘要標題:在一項晚期實體瘤患者的 1 期研究中,FAP x CD40 darPin MP0317 對安全性特徵和腫瘤局部 CD40 激活的影響。
會議標題:發育療法-免疫療法
摘要編號:2573
海報發佈會時間:2024 年 6 月 1 日中部夏令時間上午 9:00(A 廳)
企業和管理要點
2024年2月5日,針對公司、其董事和某些執行官的假定集體訴訟在不偏不倚的情況下被駁回,原告於2024年2月23日提出有偏見的解僱規定。該案於2024年2月29日下令結案。最初的案件於2022年7月12日在美國紐約南區地方法院提起。
在2024年4月17日的公司年度股東大會上,董事會在年度股東大會上提出的所有議案均獲得公司股東的批准。
財經日曆
2024 年 8 月 26 日 — 發佈 2024 年半年度業績(未經審計)
2024 年 10 月 31 日 — 2024 年第三季度中期管理聲明
