ITCC-104: HEM-iSMART International Proof of Concept Therapeutic Stratification Trial of Molecular Anomalies in Relapsed or Refractory HEMatological Malignancies in Children, Sub-Protocol E: Capivasertib + Venetoclax + Dexamethasone in Pediatric Patients With Relapsed or Refractory Hematological Malignancies

HEM-iSMART is a master protocol which investigates multiple investigational medicinal products in children, adolescents and young adults (AYA) with relapsed/refractory (R/R) ALL and LBL. Sub-protocol E is a phase I/II trial evaluating the safety and efficacy of capivasertib + venetocolax in combination with dexamethasone in children and AYA with R/R ped ALL/LBL whose tumor present with alterations of the PAM pathway, or lacking any mutations.

开始日期2026-10-01

申办/合作机构

Princess Maxima Centre For Pediatric Oncology

[+2]

NCT06802523

/ Recruiting临床1期IIT

A Phase I Study of Lintuzumab-Ac-225 in Combination With Venetoclax and ASTX-727 in Adults With Newly Diagnosed AML

This phase I trial tests the safety, side effects, and best dose of lintuzumab-Ac225 in combination with venetoclax and ASTX-727, and how well they work in treating patients with newly diagnosed acute myeloid leukemia (AML). Lintuzumab-Ac225 is a monoclonal antibody, called lintuzumab, linked to a radioactive agent called actinium Ac 225. Lintuzumab attaches to CD33 positive cancer cells in a targeted way and delivers actinium Ac 225 to kill them. Venetoclax is in a class of medications called B-cell lymphoma-2 (BCL-2) inhibitors. It may stop the growth of cancer cells by blocking Bcl-2, a protein needed for cancer cell survival. ASTX-727 is a combination of two drugs, cedazuridine and decitabine. Cedazuridine is in a class of medications called cytidine deaminase inhibitors. It prevents the breakdown of decitabine, making it more available in the body so that decitabine will have a greater effect. Decitabine is in a class of medications called hypomethylation agents. It works by helping the bone marrow produce normal blood cells and by killing abnormal cells in the bone marrow. Giving lintuzumab-Ac225 in combination with venetoclax and ASTX-727 may be safe and tolerable in treating patients with newly diagnosed AML and may improve the chance of going into remission and staying in remission for a longer period of time.

开始日期2026-04-21

申办/合作机构

National Cancer Institute

NCT07153497

/ Not yet recruiting临床2期IIT

A Randomized Phase 2 Trial of Olutasidenib-Based Therapies in Patients With Newly Diagnosed IDH1-Mutant Myeloid Malignancies: A MyeloMATCH Substudy

This phase II MyeloMATCH treatment substudy tests the addition of olutasidenib to usual treatment in patients with higher-risk myelodysplastic syndrome (MDS) or patients with acute myeloid leukemia (AML) with a mutation in the IDH1 gene. Olutasidenib blocks the protein made by the mutated IDH1 gene. Blocking this protein may help keep cancer cells from growing. For patients with MDS, olutasidenib will be added to decitabine-cedazuridine (also called ASTX727). Decitabine is in a class of medications called hypomethylating agents and is the standard treatment for MDS. It works by helping the bone marrow produce normal blood cells and by killing abnormal cells in the bone marrow. The cedazuridine makes it possible to take the decitabine by mouth. Adding olutasidenib to the usual treatment for MDS (ASTX727) may increase the likelihood of going into remission. For patients with AML, olutasidenib and ASTX727 will be combined with venetoclax, a class of medications called B-cell lymphoma-2 (BCL-2) inhibitors. Venetoclax may stop the growth of cancer cells by blocking BCL-2, a protein needed for cancer cell survival. Adding olutasidenib to the usual treatment for AML (ASTX727 and venetoclax) may increase the likelihood of going into remission. For low risk MDS, the substudy tests whether giving olutasidenib alone helps improve blood counts.

开始日期2026-02-26

申办/合作机构

National Cancer Institute

100 项与维奈克拉相关的临床结果

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100 项与维奈克拉相关的转化医学

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100 项与维奈克拉相关的专利（医药）

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4,902

项与维奈克拉相关的文献（医药）

2026-02-01·COMPUTATIONAL BIOLOGY AND CHEMISTRY

GC/MS analysis and computational evaluation of C. cinerea EO constituents for colorectal cancer: Molecular docking, dynamics, and quantum chemical insights into Cis-Verbenyl acetate

Article

作者: Bekkar, Yahia ; Bouraoui, Rania ; Neghmouche Nacer, Salah ; Lanez, Touhami ; Bourougaa, Lotfi ; Lanez, Elhafnaoui ; Garzoli, Stefania ; Larbi Benamor, Mohammed ; Samah, Bouchagra

The essential oil of Cotula cinerea was subjected to gas chromatography-mass spectrometry (GC-MS) analysis, leading to the identification of 31 chemical constituents. The major compounds were selected for comprehensive computational investigations to explore their potential anti-colorectal cancer activity. Among the identified constituents, cis-verbenyl acetate (CVA) exhibited the most favorable binding affinities across a panel of fifteen protein targets implicated in colorectal cancer. Notably, Tankyrase1 (PDB ID: 4OA7) and Tankyrase2 (PDB ID: 4UFU) emerged as the most promising targets, with docking scores of -9.49 and -8.46 kcal/mol, respectively. Molecular dynamics simulations conducted over 300 nanoseconds demonstrated the structural stability and sustained interactions of the CVA-protein complexes, characterized by low root mean square deviation (RMSD) values and limited conformational fluctuations. These findings were corroborated by molecular mechanics Poisson-Boltzmann surface area (MM-PBSA) calculations, which revealed highly favorable binding free energies, particularly in the CVA- TNKS2 complex (ΔGtotal = -45.64 kcal/mol). In silico ADMET profiling indicated high oral bioavailability and low predicted toxicity for CVA compared to native ligands. Furthermore, density functional theory (DFT) analysis provided insight into the electronic properties of CVA, revealing a stable electronic configuration, suitable frontier molecular orbital energies, and a well-distributed electrostatic potential surface. Thermodynamic evaluations supported its chemical stability, showing a consistent increase in entropy, enthalpy, and heat capacity with rising temperature. Collectively, these computational findings suggest that CVA is a thermodynamically stable, pharmacokinetically favorable, and potentially bioactive compound with dual-target affinity against colorectal cancer-related proteins, meriting further experimental validation.

2026-02-01·JOURNAL OF BIOTECHNOLOGY

FRET two-hybrid assay-based target drug screening in living cells

Article

作者: Chang, Yuan ; Wang, Xiaoping ; Gan, Tian ; Qu, Rumeng ; Cao, Gengqiang ; Sun, Beini ; Wang, Yue ; Chen, Tongsheng ; Hu, Lin ; Hu, Min

Precise targeted drug screening is the key to improve the efficiency of tumour targeted therapy. This report presents a live cell FRET two-hybrid assay-based targeted drug screening method (FRET-HBTDS). In FRET-HBTDS, the cells co-expressing donor- and acceptor-labelled targets were cultured in 96-well plates, quantitative FRET imaging was then performed on a self-built automated FRET microscope (FRETscope) well-by-well, and FRET two-hybrid assay was used to obtain the maximum donor-centre FRET efficiency (E_Dmax), maximum acceptor-centre FRET efficiency (E_Amax) and stoichiometric ratios (N_A/N_D). The FRET-HBTDS method was performed on the FRETscope with a 20 × objective for the cells co-expressing CFP-Bcl-xL and YFP-Bak to assess the action of eight compounds (A1331852, S63845, AC, DSF/Cu, Met, REGO, SOFA, ABT199) on the interaction between Bcl-xL and Bak. After 7 h of treatment with these compounds respectively, only the A1331852 group showed significantly lower E_Dmax and E_Amax compared to the control group, and a significant increase in N_A/N_D, suggesting that A1331852 unlocks the direct interaction between Bcl-xL and Bak, thus releasing Bak to induce cell death. In addition, the N_A/N_D of the DSF/Cu group was significantly higher than of the control group, suggesting that DSF/Cu altered the stoichiometry of the Bcl-xL-Bak complex. Our data firmly demonstrate that A1331852 unlocks the binding state of Bcl-xL and Bak, while DSF/Cu modifies the structure of the Bcl-xL-Bak complex. These findings demonstrate that FRET-HBTDS can be used to assess the efficacy of a drug by revealing the binding state and complex molecular structure of the target proteins using FRET technology in living cells, which may be a potential targeted drug screening method.

2026-01-01·BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR BASIS OF DISEASE

Metabolic reprogramming represents a targetable mechanism to overcome acquired resistance to venetoclax in acute myeloid leukemia

Article

作者: de Franca Basto Silva, Marina ; Lima, Keli ; Campregher, Paulo Vidal ; Costa-Lotufo, Leticia Veras ; Cortez, Luiz Gustavo Ferreira ; Machado-Neto, João Agostinho ; de Queiroz, Gustavo Nery ; Guedes, Rafael Lucas Muniz ; Câmara, Niels Olsen Saraiva ; Tomaz, Victoria ; Cipelli, Marcella ; Rego, Eduardo Magalhães

Acute myeloid leukemia (AML) often develops resistance to the BCL2 inhibitor venetoclax through metabolic reprogramming. This study established acquired venetoclax-resistant AML models (MV4-11VR and MOLM-13VR) to explore resistance mechanisms and therapeutic strategies. Cell viability and apoptosis assays revealed robust acquired resistance to venetoclax upon intermittent drug exposure. Metabolic profiling revealed distinct adaptations: MV4-11VR cells favored glycolysis, while MOLM-13VR cells increased oxidative phosphorylation. Proteomic analysis supported these findings, showing pathway enrichment for carbohydrate metabolism in MV4-11VR and aerobic energy production in MOLM-13VR. Despite these differences, both models shared hyperactivation of the PI3K/AKT/mTOR pathway, as shown by RPS6 hyperphosphorylation. Apoptotic regulation also diverged between the cellular models in relation to modulated BCL2-related genes and activation of the MAPK signaling pathway. Targeting these metabolic changes with metformin (a mitochondrial complex I inhibitor) or KPT-9274 (a NAMPT inhibitor) re-sensitized resistant cells to venetoclax. Combination treatments showed strong synergy and near-complete cell elimination. These results highlight metabolic reprogramming as a heterogeneous but targetable resistance mechanism and support combining metabolic inhibitors with BCL2 blockade to treat refractory AML.

1,825

项与维奈克拉相关的新闻（医药）

2025-12-06

·生物谷

Blood Adv：老年白血病治疗大变革！

迈阿密大学西尔维斯特综合癌症中心等机构的科学家们领衔制定了2025年新版老年AML治疗指南，该指南基于最新临床证据，系统回答了老年AML治疗中最关键的九个问题，涵盖是否治疗、如何选药、移植时机等。当我们谈论急性髓系白血病（AML）时，一组数字或许会让你心头一紧，AML是成人中最常见的急性白血病，而60岁以上患者占所有AML病例的近一半，且随着年龄增长，治疗难度与死亡率显著上升。过去，许多老年患者因身体无法耐受高强度化疗，只能选择支持性护理，生存期往往以月计算。但如今，随着靶向药物、低强度化疗及个体化治疗策略的飞速发展，老年AML的治疗图景正在发生翻天覆地的变化。近日，发表在国际杂志Blood Advances上题为“American Society of Hematology 2025 guidelines for treating newly diagnosed acute myeloid leukemia in older adults”的研究报告中，迈阿密大学西尔维斯特综合癌症中心等机构的科学家们领衔制定了2025年新版老年AML治疗指南，该指南基于最新临床证据，系统回答了老年AML治疗中最关键的九个问题，涵盖是否治疗、如何选药、移植时机乃至安宁疗护中的输血支持等方面。值得关注的是，这份指南特别强调“以患者为中心”的对话模式，将医患共同决策过程融入建议之中。Sekeres 博士表示，我们不想回避那些患者和医生都在挣扎的难题，第一个问题往往是：我该接受治疗吗？从“要不要治”到“怎么精准治”：治疗观念的三大转变（1）积极治疗优于支持护理新版指南明确建议，只要身体条件允许，老年患者应接受抗白血病治疗，而不应仅停留在输血、抗感染等支持性手段。尤其是60多岁、基因预后较好的患者，仍可考虑传统高强度化疗。（2）靶向药物成为“明星选手” 如果患者无法耐受强化疗，可选择去甲基化药物（比如阿扎胞苷）或低剂量阿糖胞苷，并联合 Venetoclax—这是一种近年来获批的BCL-2抑制剂，能精准促使白血病细胞凋亡。更令人振奋的是，针对特定基因突变的靶向药已写入一线推荐：1）FLT3突变→FLT3抑制剂；IDH1/IDH2突变→去甲基化药物联合IDH抑制剂（比如伊沃西替尼）。研究者表示，患者的基因会说话，它告诉我们谁适合用靶向药，谁的复发风险高，谁需要移植。（3）移植门槛降低，更多患者有了“根治”机会以往，骨髓移植被视为年轻患者的“专利”；如今，移植技术改进、半相合供者的应用，使得更多60岁以上、高风险AML患者也能获得移植机会。移植能显著延长生命，委员会强烈建议更多高危患者考虑它，”研究者强调。如果不符合移植条件，患者也可通过低强度联合方案进行维持治疗，预防复发。不仅是治病，更是护人：指南中的人文亮色除了“硬核”治疗建议，新版指南还关注到生命末期的尊严照护，很多安宁疗护机构曾拒绝为白血病患者输血，而美国血液学会此次明确表态，输血支持应作为姑息治疗与安宁疗护的一部分，研究者们坚定认为，血液制品输血是舒缓护理的一部分。未来已来：AML治疗的下一步是什么？尽管当前进展喜人，AML的治疗探索并未止步。MENIN抑制剂、Venetoclax 联合新方案等研究正在推进；微小残留病灶检测技术也在不断精进，帮助医生更早预测复发、更准筛选移植人群。研究者表示，他们正把越来越多的患者推进“获益优势组”，即那些对新疗法反应良好、活得也更长的群体。随着人口老龄化加剧，老年AML已成为血液科医生必须直面的一场硬仗。所幸，医学的进步让我们不再束手无策，从“治不治”的犹豫到“怎么治”的精细规划，再到“如何陪他们走好最后一程”的全人关怀，今天的老年白血病治疗，正向着更科学、也更温暖的方向迈进。（生物谷Bioon.com）参考文献： Mikkael A Sekeres,Ryan J Mattison,Andrew S. Artz, et al. American Society of Hematology 2025 guidelines for treating newly diagnosed acute myeloid leukemia in older adults, Blood Advances (2025). DOI:10.1182/bloodadvances.2025017934

2025-12-06

·aptose.com

Aptose’s Tuspetinib Triple Drug Therapy Featured at the 2025 ASH Annual Meeting; High Rate of Frontline Clinical Responses Continues Across AML Populations

TUS+VEN+AZA triplet frontline therapy demonstrates high rates of efficacy and MRD-negative remissions in newly diagnosed AML patients with diverse mutations Safety continues to be a notable hallmark of TUS-based therapies 100% response rate (CR/CRh) at the two higher dose levels (80 and 120 mg TUS dose) CR/CRh observed in FLT3 wildtype subjects, representing ~70% of AML patients CR/CRh observed in AML with TP53/complex karyotype, RAS, and MDS-related mutations SAN DIEGO and TORONTO, Dec. 06, 2025 (GLOBE NEWSWIRE) -- Aptose Biosciences Inc. (“Aptose” or the “Company”) (NASDAQ: APTO, TSX: APS), a clinical-stage precision oncology company developing highly differentiated targeted agents to treat hematologic malignancies, today featured clinical data for its lead compound tuspetinib (TUS) combined with standard dosing of venetoclax (VEN) and azacitidine (AZA) in a poster presentation at the 67th American Society of Hematology (ASH) Annual Meeting in Orlando, FL. Updated data from patients in the TUSCANY trial across all three cohorts, 40 mg, 80 mg or 120 mg TUS dose in TUS+VEN+AZA, reveal promising clinical safety and antileukemic activity and support the use of TUS in combination with standard of care treatment across a broad range of AML populations, including those with adverse mutations regardless of FLT3 mutation status. Poster title: “TUSCANY study demonstrates safety and efficacy of tuspetinib plus standard of care venetoclax and azacitidine in patients with newly diagnosed AML ineligible for induction chemotherapy” Key Findings and Messages: In newly diagnosed AML patients, TUS+VEN+AZA shows promising safety, tolerability and resilient efficacy, including MRD-negative remissions across a broad mutational spectrum High-quality clinical responses (CR/CRh): 90% across 40, 80 and 120 mg dose levels 100% at the higher 80 mg and 120 mg dose levels Observed in FLT3-WT, FLT3-ITD, and NPM1c genetic subgroups Observed in biallelic TP53/complex karyotype and RAS adverse genetic subgroups Observed in AML with MDS-related mutations MRD negativity: 78% by central flow cytometry in responding subjects TUS targets VEN resistance mechanisms; inhibits kinase-driven abnormal signaling Two subjects transitioned to stem cell transplantation and both returned for TUS maintenance TUS+VEN+AZA triplet therapy was well tolerated with no dose-limiting toxicities (DLTs) across all evaluable TUS dose levels No DLTs including no prolonged myelosuppression for subjects in remission in Cycle 1 No drug-related deaths, differentiation syndrome, QTc prolongation, or CPK elevation reported 8/10 evaluable subjects experienced red cell and platelet transfusion independence for > 8 weeks after their best response Febrile neutropenia was reported in 2 subjects (16.7%), with 1 subject related to TUS At the recently enrolled 160 mg dose level, preliminary findings show patients achieving early blast clearance with MRD-negativity and formal responses in the first few weeks of treatment (not included in poster data cut). 90% across 40, 80 and 120 mg dose levels 100% at the higher 80 mg and 120 mg dose levels Observed in FLT3-WT, FLT3-ITD, and NPM1c genetic subgroups Observed in biallelic TP53/complex karyotype and RAS adverse genetic subgroups Observed in AML with MDS-related mutations No DLTs including no prolonged myelosuppression for subjects in remission in Cycle 1 No drug-related deaths, differentiation syndrome, QTc prolongation, or CPK elevation reported 8/10 evaluable subjects experienced red cell and platelet transfusion independence for > 8 weeks after their best response Febrile neutropenia was reported in 2 subjects (16.7%), with 1 subject related to TUS “Tuspetinib, as part of a triple drug therapy, continues to perform well, achieving 100% clinical response in the two higher doses we have evaluated to date,” said Rafael Bejar, MD, PhD, Chief Medical Officer at Aptose. “We recently commenced treating patients at the highest dose level of 160 mg TUS and have already achieved early responses. With no dose-limiting toxicities and activity across diverse mutations, TUS+VEN+AZA targets AML’s greatest unmet needs and largest populations.” The ASH poster presentation is available here. About Tuspetinib Aptose’s lead compound tuspetinib is a convenient once daily oral agent that potently targets SYK, mutated and wild type forms of FLT3, mutated KIT, JAK1/2, and RSK2 kinases, while avoiding many typical toxicity concerns observed with other agents. The ongoing TUSCANY triplet Phase 1/2 study is designed to test various doses and schedules of TUS in combination with standard dosing of azacitidine and venetoclax in newly diagnosed patients with AML who are ineligible to receive induction chemotherapy. Data from the first three dose cohorts demonstrate safety, CRs and minimal residual disease (MRD) negativity across patients with diverse mutations. The early data showed that 9 out of 10 patients responded to the TUS triplet therapy, with 100% complete remission (CR/CRh) achieved in the 80mg and 120mg cohorts. Notably, patients with difficult-to-treat mutations in TP53, RAS and FLT3 genes also achieved a 100% CR/CRh rate. About Aptose Aptose Biosciences is a clinical-stage biotechnology company committed to developing precision medicines addressing unmet medical needs in oncology, with an initial focus on hematology. The Company's small molecule cancer therapeutics pipeline includes products designed to provide single agent efficacy and to enhance the efficacy of other anti-cancer therapies without overlapping toxicities. The Company’s lead clinical-stage compound tuspetinib (TUS), is an oral kinase inhibitor that has demonstrated activity as monotherapy and in combination therapy in patients with relapsed or refractory acute myeloid leukemia (AML) and is being developed as a frontline triplet therapy in newly diagnosed AML. For more information, please visit www.aptose.com. Forward Looking Statements This press release may contain forward-looking statements within the meaning of Canadian and U.S. securities laws, including, but not limited to, statements relating to the therapeutic potential of tuspetinib, its clinical development and safety profile including its tolerability and resilient efficacy, as well as statements relating to the Company’s plans, objectives, expectations and intentions and other statements including words such as “continue”, “expect”, “intend”, “will”, “should”, “would”, “may”, and other similar expressions. Such statements reflect our current views with respect to future events and are subject to risks and uncertainties and are necessarily based upon a number of estimates and assumptions that, while considered reasonable by us are inherently subject to significant business, economic, competitive, political and social uncertainties and contingencies. Many factors could cause our actual results, performance or achievements to be materially different from any future results, performance or achievements described in this press release. Such factors could include, among others: our ability to obtain the capital required for research and operations and to continue as a going concern; the inherent risks in early stage drug development including demonstrating efficacy; development time/cost and the regulatory approval process; the progress of our clinical trials; our ability to find and enter into agreements with potential partners; our ability to attract and retain key personnel; changing market conditions; inability of new manufacturers to produce acceptable batches of GMP in sufficient quantities; unexpected manufacturing defects; and other risks detailed from time-to-time in our ongoing quarterly filings, annual information forms, annual reports and annual filings with Canadian securities regulators and the United States Securities and Exchange Commission. Should one or more of these risks or uncertainties materialize, or should the assumptions set out in the section entitled "Risk Factors" in our filings with Canadian securities regulators and the United States Securities and Exchange Commission underlying those forward-looking statements prove incorrect, actual results may vary materially from those described herein. These forward-looking statements are made as of the date of this press release and we do not intend, and do not assume any obligation, to update these forward-looking statements, except as required by law. We cannot assure you that such statements will prove to be accurate as actual results and future events could differ materially from those anticipated in such statements. Investors are cautioned that forward-looking statements are not guarantees of future performance and accordingly investors are cautioned not to put undue reliance on forward-looking statements due to the inherent uncertainty therein. For further information, please contact: Aptose Biosciences Inc. Susan Pietropaolo Corporate Communications & Investor Relations 201-923-2049 spietropaolo@aptose.com Released December 6, 2025

临床结果ASH会议临床研究

2025-12-05

·GlobeNewswire-Health Care

ImCheck Announces Oral Presentation of ICT01 First-Line AML Data at the 67th ASH Annual Meeting

ImCheck Announces Oral Presentation of ICT01 First-Line AML Data at the 67th ASH Annual Meeting Marseille, France, December 5, 2025 05:00 a.m. ET / 11:00 a.m. CET– ImCheck Therapeutics announced today an oral presentation at the upcoming American Society of Hematology (ASH) Annual Meeting 2025, taking place from December 6 to December 9, in Orlando, FL, USA. The presentation will highlight the high remission rates and overall survival observed in EVICTION, ImCheck’s open-label, randomized Phase I/II study evaluating ICT01, a first-in-class γ9δ2 T-cell activator, in combination with azacitidine and venetoclax in older or unfit patients with newly diagnosed acute myeloid leukemia (AML). Details of the oral presentation at ASH 2025 are: Abstract Title: “γ9δ2 T-cell (γ9δ2TC) activation with ICT01 and azacitidine-venetoclax (Aza-Ven) induces high rates of remission and overall survival in patients with newly diagnosed (ND) acute myeloid leukemia (AML): Results from the phase 1/2 study eviction”Presenter: Sylvain GRACIAZ, MD, PhD, Institut Paoli-Calmettes, Marseille, FranceSession: 616. Acute Myeloid Leukemias: Investigational Drug and Cellular Therapies: Immunotherapy and chemotherapy combinations in AMLRoom: OCCC - Chapin Theater (320)Date: Sunday, December 7, 2025Time: 5:15 p.m.- 5:30 p.m. ET The ASH presentation will be available on ImCheck’s corporate website after the presentation has been held. *** About the EVICTION Study EVICTION is a first-in-human, dose-escalation (Part 1) and cohort-expansion (Part 2) clinical study of ICT01 in patients with various advanced relapsed or refractory solid or hematologic cancers that have exhausted standard-of-care treatment options. Part 1 (Phase I) is designed to characterize the preliminary safety, tolerability, and pharmacodynamic activity of increasing doses of ICT01 as monotherapy (Group A: solid tumors; Group B: hematologic tumors) and in combination with pembrolizumab (Group C: solid tumors). Part 2 comprises randomized dose-optimizing and efficacy estimating expansion cohorts of monotherapy (Group D: ovarian cancer; Group E: prostate cancer) and combination treatment of patients with AML (Group F), melanoma (Group G), urothelial cell carcinoma (Group H), or head-and-neck squamous cell carcinoma (Group I). More information on the EVICTION study can be found at clinicaltrials.gov (NCT04243499). About ICT01 ICT01 is a humanized, anti-BTN3A (also known as CD277) monoclonal antibody that selectively activates γ9δ2 T cells, which are responsible for immunosurveillance of malignancy and infections. The three isoforms of BTN3A targeted by ICT01 are overexpressed on many solid tumors (e.g., melanoma, urothelial cell, colorectal, ovarian, pancreatic, and lung cancer) and hematologic malignancies (e.g., leukemia and lymphomas) and also expressed on the surface of innate (e.g., γδ T cells and NK cells) and adaptive immune cells (T cells and B cells). BTN3A is essential for the activation of the anti-tumor immune response of γ9δ2 T cells. As demonstrated by data presented at past AACR, ASCO, ASH, ESMO and SITC conferences, ICT01 selectively activates circulating γ9δ2 T cells leading to migration of γ9δ2 T cells out of the circulation and into the tumor tissue and triggers a downstream immunological cascade through secretion of pro-inflammatory cytokines, including but not limited to IFNγ and TNFα, further augmenting the anti-tumor immune response. Anti-tumor activity and efficacy of ICT01 have been shown in patients across several cancer indications. About IMCHECK THERAPEUTICS ImCheck Therapeutics is developing a new generation of immunotherapeutic antibodies targeting butyrophilins, a novel superfamily of immunomodulators. By unlocking the power of γ9δ2 T cells, ImCheck’s innovative approach has the potential to transform treatments across oncology, autoimmune, and infectious diseases. The lead clinical-stage program, ICT01, has been advancing to late-stage trials, demonstrating a unique mechanism of action that modulates both innate and adaptive immunity. These “first-in-class” activating antibodies may deliver superior clinical outcomes compared to first-generation immunotherapy approaches, in particular in rationale combinations with immune checkpoint inhibitors and immunomodulatory anti-cancer drugs. Additionally, ImCheck’s pipeline compounds are progressing toward clinical development for autoimmune and infectious diseases.The company benefits from the pioneering research of Prof. Daniel Olive (INSERM, CNRS, Institut Paoli Calmettes, Aix-Marseille University), a global leader in γ9δ2 T cells and butyrophilins, as well as the expertise of a seasoned management team and the commitment of leading U.S. and European investors. As announced on October 22, Ipsen (Euronext: IPN; ADR: IPSEY) and ImCheck have entered into a definitive share purchase agreement in which Ipsen will acquire all issued and outstanding shares of ImCheck, with the transaction close anticipated by the end of Q1 2026. For further information: https://www.imchecktherapeutics.com/ Press contacts: US and EU Trophic CommunicationsGretchen Schweitzer +49 (0) 172 861 8540imcheck@trophic.eu FranceATCG PARTNERSCéline Voisin+33 (0)6 62 12 53 39imcheck@atcg-partners.com Attachment PR in english

免疫疗法ASH会议AACR会议临床1期细胞疗法

100 项与维奈克拉相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D10679	维奈克拉	L01XX52	DB11581

研发状态

批准上市

10 条最早获批的记录,

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适应症	国家/地区	公司	日期
复发性套细胞淋巴瘤	日本	AbbVie LLC	2025-03-27
难治性套细胞淋巴瘤	日本	AbbVie LLC	2025-03-27
难治性慢性淋巴细胞白血病	日本	AbbVie LLC	2019-09-20
复发性慢性淋巴细胞白血病	日本	AbbVie LLC	2019-09-20
小淋巴细胞淋巴瘤	美国	AbbVie, Inc.	2018-06-08
成人急性髓性白血病	欧盟	AbbVie Deutschland GmbH & Co. KG	2016-12-04
成人急性髓性白血病	冰岛	AbbVie Deutschland GmbH & Co. KG	2016-12-04
成人急性髓性白血病	列支敦士登	AbbVie Deutschland GmbH & Co. KG	2016-12-04
成人急性髓性白血病	挪威	AbbVie Deutschland GmbH & Co. KG	2016-12-04
急性髓性白血病	加拿大	AbbVie AS	2016-10-31
慢性淋巴细胞白血病	美国	AbbVie, Inc.	2016-04-11

未上市

10 条进展最快的记录,

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适应症	最高研发状态	国家/地区	公司	日期
肿瘤溶解综合征	临床3期	美国	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	澳大利亚	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	法国	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	希腊	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	塞尔维亚	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	西班牙	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	中国台湾	AbbVie, Inc.	2024-08-05
肿瘤溶解综合征	临床3期	英国	AbbVie, Inc.	2024-08-05
复发性急性髓细胞白血病	临床3期	美国	Genentech, Inc.	2022-10-01
复发性急性髓细胞白血病	临床3期	美国	AbbVie, Inc.	2022-10-01

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临床结果

适应症

分期

评价

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT03751436 (Pubmed \| Cancer Chemother Pharmacol)	临床1期	转移性去势抵抗性前列腺癌 BCL-2	10	Enzalutamide (160 mg/d) with Venetoclax (metastatic castration-resistant prostate cancer)	糧醖範製鹽獵鏇壓鬱蓋(艱製鹽廠鬱積齋窪鹽繭) = 廠襯獵醖築襯憲構網壓糧廠鹽夢鑰齋鬱膚鬱糧 (顧簾鹽觸鑰選淵餘廠衊, 1 ~ 35) 更多	积极	2025-12-01
NCT05464836 (CTgov)	临床2期	急性淋巴细胞白血病 \| 前体T淋巴细胞白血病淋巴瘤 \| T细胞急性淋巴细胞白血病复发 ... 更多	2	Venetoclax+CB-103	鬱製範窪範觸鏇窪鏇憲 = 鑰壓窪鹽膚範壓鑰築網簾衊鬱願願壓製齋願衊 (鬱糧鑰範餘窪餘鹽淵鏇, 壓構醖憲壓構衊觸襯積 ~ 蓋窪鏇膚壓遞蓋憲選壓) 更多	-	2025-11-26
NCT04874194 (CTgov)	临床1/2期	复发性急性髓细胞白血病 \| 急性双表型白血病 \| 难治性骨髓增生异常综合征 ... 更多	24	Omacetaxine Mepesuccinate+Venetoclax (Ph 1 Arm B (MDS) Dose + 1)	繭鏇製醖膚積膚鹽廠繭(選餘構醖淵襯鏇繭積願) = 壓鬱憲遞餘壓糧網餘糧餘憲蓋願窪醖製鏇襯淵 (壓構夢齋願顧網選壓膚, 膚淵鏇鹽憲獵齋觸製壓 ~ 觸襯繭醖範夢餘醖觸繭) 更多	-	2025-11-03
NCT04874194 (CTgov)	临床1/2期	复发性急性髓细胞白血病 \| 急性双表型白血病 \| 难治性骨髓增生异常综合征 ... 更多	24	Omacetaxine Mepesuccinate+Venetoclax (Ph 1 Arm A (AML) Dose 0)	壓齋獵膚襯壓鬱廠夢餘 = 觸蓋網獵築顧壓製製繭襯鏇鬱齋廠衊願糧齋鹹 (蓋網選遞顧蓋範衊鹹遞, 構窪糧構壓廠築繭鹹簾 ~ 壓範窪醖糧鹽醖夢鏇餘) 更多	-	2025-11-03
NCT04092179 (ENAVEN-AML, Pubmed \| Lancet Haematol)	临床1/2期	复发性急性髓细胞白血病 \| 骨髓增生异常综合征 IDH2 mutation	27	Venetoclax 400 mgEnasidenib 100 mg + Venetoclax 400 mgEnasidenib 100 mg	醖顧齋糧選構鹽觸顧築(製窪襯簾築積淵壓衊網) = 壓壓獵築築憲糧簾膚願願壓艱鑰範壓構積壓網 (廠範鑰選憲遞糧選網糧, 41 ~ 80) 更多	积极	2025-11-01
ChiCTR2200063954 (Nat Rev Drug Discov) 人工标引	临床2期	急性髓性白血病一线	38	Granulocyte colony-stimulating factor + venetoclax + azacitidine	鏇積艱鑰遞廠鬱網醖願(製壓鹽簾鏇觸壓壓憲構) = 獵醖願積簾願鑰獵願壓築蓋衊構構糧構餘觸襯 (鏇鏇憲鬱願餘選醖襯淵 ) 更多	积极	2025-10-27
ChiCTR2200063954 (Nat Rev Drug Discov) 人工标引	临床2期	急性髓性白血病一线	38	Granulocyte colony-stimulating factor + venetoclax + azacitidine (ELN favorable risk)	鏇積艱鑰遞廠鬱網醖願(製壓鹽簾鏇觸壓壓憲構) = 網製淵襯積鹽選糧遞選築蓋衊構構糧構餘觸襯 (鏇鏇憲鬱願餘選醖襯淵 ) 更多	积极	2025-10-27
ESMO2025	N/A	急性髓性白血病	81	Venetoclax-containing regimens	餘築糧製積遞蓋鹽艱鏇(艱鹽範餘積範襯積鬱構) = 網齋蓋齋築齋積廠築憲選遞鏇繭膚淵觸膚壓築 (淵夢膚糧鹹遞壓衊憲餘 ) 更多	积极	2025-10-17
NCT05184842 (Phase II, CTgov)	临床2期	急性髓性白血病 \| 慢性粒单核细胞白血病 \| 骨髓增生异常综合征	-	Venetoclax+Decitabine	選憲蓋衊齋廠簾艱憲構 = 膚壓構鏇遞繭顧襯餘願築繭鹽膚鹽製餘窪顧鹹 (網選憲膚願顧醖窪夢憲, 構願蓋獵築鏇願廠膚築 ~ 膚憲繭鹽醖構構衊簾膚) 更多	-	2025-08-26
NCT04102020 (VIALE-M, CTgov)	临床3期	急性髓性白血病	112	Venetoclax+Azacitidine (Part 1: Venetoclax 400 mg + Azacitidine 20 mg/m^2)	膚範製獵製襯繭醖顧夢 = 齋範窪窪鏇築觸壓願積醖淵繭餘糧廠鹽憲築構 (遞獵餘艱積襯鹽餘獵鏇, 鹹鏇齋鹹繭鏇鬱鹽鬱膚 ~ 齋齋構選製構構鏇鏇積) 更多	-	2025-08-20
NCT04102020 (VIALE-M, CTgov)	临床3期	急性髓性白血病	112	Venetoclax+Azacitidine (Part 1: Venetoclax 400 mg + Azacitidine 36 mg/m^2)	膚範製獵製襯繭醖顧夢 = 醖簾獵遞醖蓋鹹遞獵餘醖淵繭餘糧廠鹽憲築構 (遞獵餘艱積襯鹽餘獵鏇, 繭膚膚餘夢窪襯鬱網製 ~ 糧鬱獵廠淵獵齋蓋遞艱) 更多	-	2025-08-20
NCT03580928 (AMPLIFY \| AVO, CTgov)	临床2期	慢性淋巴细胞白血病	72	Acalabrutinib+Venetoclax+Obinutuzumab (Acalabrutinib/Venetoclax/Obinutuzumab (AVO) With Non-high-risk CLL Disease)	餘鏇製艱繭選鬱壓夢廠 = 網觸願壓築醖餘艱鏇壓鏇廠淵選膚鹹壓夢淵網 (鬱繭衊醖壓鹹襯積遞餘, 窪齋壓夢憲窪鏇壓鹽選 ~ 壓鑰蓋醖鑰鑰願艱衊憲) 更多	-	2025-08-12
NCT03580928 (AMPLIFY \| AVO, CTgov)	临床2期	慢性淋巴细胞白血病	72	Acalabrutinib+Venetoclax+Obinutuzumab (Acalabrutinib/Venetoclax/Obinutuzumab (AVO) With High-risk CLL Disease)	餘鏇製艱繭選鬱壓夢廠 = 觸齋選廠網顧壓艱積選鏇廠淵選膚鹹壓夢淵網 (鬱繭衊醖壓鹹襯積遞餘, 簾繭齋餘簾願願憲顧繭 ~ 範積淵鹹遞觸鏇遞窪積) 更多	-	2025-08-12
NCT03013998 (Pubmed \| J Clin Oncol)	临床1期	难治性急性髓细胞白血病 NPM1m \| KMT2Ar	43	Azacitidine, Venetoclax, and Revumenib	構繭壓廠觸鑰願願窪鏇(構選繭廠糧製範襯繭窪) = present in 8 (19%) patients 壓鑰襯築襯積齋齋鑰遞 (憲鹹壓鑰築餘築憲繭鏇 ) 更多	积极	2025-08-10