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]

NCT07311746

/ Not yet recruiting临床1/2期IIT

Phase Ib/II Trial of Cladribine/Ruxolitinib/Venetoclax in Patients With Relapsed/Refractory T-cell Prolymphocytic Leukemia

The goal of this clinical research study is to learn if the combination of ruxolitinib with cladribine and venetoclax can help to control the disease in patients with R/R T-PLL.

开始日期2026-06-01

申办/合作机构

The University of Texas MD Anderson Cancer Center

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2026-05-27

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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4,687

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 ; Chen, Tongsheng ; Wang, Yue ; 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.

2026-02-01·BIOORGANIC CHEMISTRY

Zinc(II)–berberine-based complexes targeting mitochondria exhibit enhanced antiproliferative activity as single drugs or in combination with ABT-199

Article

作者: Liang, Hong ; Wu, Run-Chun ; Qin, Aimiao ; Qin, Qi-Pin ; Wang, Zhen-Feng ; Zhang, Shu-Hua ; Huang, Xiao-Qiong ; Tan, Min-Xiong

Myeloid cell leukemia-1 (Mcl-1), a protein mainly located in mitochondria, exhibits antiapoptotic activity, promoting tumor growth. Herein, we designed an innovative strategy for targeting mitochondria to inhibit Mcl-1 expression effectively. To this end, we synthesized a novel berberine-based ligand, BerT. We also synthesized and comprehensively characterized its corresponding Zn(II) complexes, including [Zn(BerT)(H₂O)Cl₂] (BerT1), [Zn(BerT)(ppe)Cl]Cl (BerT2), [Zn(BerT)(ipq)Cl]Cl (BerT3), [Zn(BerT)(phe)Cl]Cl (BerT4), [Zn(BerT)(bph)Cl]Cl (BerT5), [Zn(BerT)(dph)Cl]Cl (BerT6), [Zn(BerT)(pha)Cl]Cl (BerT7) and [Zn(BerT)(mph)Cl]Cl (BerT8) [ppe = 1,2-bis(diphenylphosphino)ethane, ipq = 2-(1H-imidazo[4,5-f][1,10]phenanthrolin-2-yl)quinolin-8-ol, phe = 1,10-phenanthroline, bph = bathophenanthroline, dph = 4,7-dichloro-1,10-phenanthroline, pha = 1,10-phenanthrolin-5-amine and mph = 5,6-dimethyl-1,10-phenanthroline]. In human breast MDA-MB-231cancer cells, compounds BerT1-BerT8 exhibited potent cancer growth inhibitory capability ranging (IC₅₀ = 0.52-1.97 μM), as compared to cisplatin (IC₅₀ = 10.04 ± 0.61 μM). BerT1 and BerT3 exhibited intrinsic green fluorescence, indicating their potential utility in mitochondrial imaging applications. To the best of our knowledge, BerT1 and BerT3 are the first Zn(II)-berberine-based complexes that target mitochondria. They can selectively bind to Mcl-1 with high affinity, exhibiting enhanced anticancer efficacy in MDA-MB-231 tumor cells. These two complexes also caused Bax/Bak-dependent apoptosis in MDA-MB-231 cells and acted synergistically with ABT-199 to kill ABT-199 resistant cells in multiple tumor models. BerT3 was effective and tolerable as a single probe or in combination with ABT-199 in MDA-MB-231 BALB/c mouse models. Thus, we conclude that Zn(II)-berberine-based derivatives have potential for the non‑platinum drugs development aimed at treating cancer tissue.

1,959

项与维奈克拉相关的新闻（医药）

2026-01-09

·aptevotherapeutics.gcs-web.com

Aptevo Therapeutics Secures $60 Million Equity Line of Credit to Support Multispecific Portfolio Advancement, Increase Strategic Optionality

Together with cash on hand, the fully leveraged facility extends Aptevo's funding runway into 2029, enabling achievement of key clinical and preclinical milestones SEATTLE, WA / ACCESS Newswire / January 9, 2026 / Aptevo Therapeutics Inc. (NASDAQ:APVO), a clinical-stage biotechnology Company focused on developing novel immune-oncology therapeutics based on its proprietary ADAPTIR® and ADAPTIR-FLEX® platform technologies, today announced that the Company has entered into a $60 million equity line of credit (ELOC) agreement with Yorkville Advisors Global, LP, strengthening the Company's financial flexibility as it continues to advance its clinical and preclinical pipeline of multispecific anti-cancer agents that are differentiated by design. The facility provides Aptevo with access to capital, allowing the Company to raise funds incrementally, at its discretion, and under market-based conditions. Further, an ELOC offers affordable capital financing with minimal fees and no warrants. Proceeds from the ELOC will be used to support ongoing clinical development, advance preclinical programs, and fund general corporate purposes. "This agreement offers added flexibility and control over how and when we access capital," said Daphne Taylor, Chief Financial Officer at Aptevo. "Importantly, the fully leveraged facility plus cash on hand is sufficient to fund us for three years, into 2029. During this time, we plan to continue generating clinical data and advancing differentiated assets across the portfolio focusing on execution and value creation." The ELOC complements Aptevo's existing capital resources and is designed to support the Company's disciplined approach to balance sheet management, while preserving optionality around future strategic and growth decisions. Under the terms of the agreement, Aptevo has the right, but not the obligation, to sell shares to the counterparty from time to time, subject to customary conditions and limitations. The Company is not required to draw on the facility and retains full discretion over its use. Aptevo's portfolio includes five CD3-engaging assets anchored by mipletamig, a first-in-class CD123 x CD3 bispecific currently being evaluated in RAINIER, a Phase 1b/2 trial for frontline AML. In total, mipletamig has been evaluated in more than 100 patients across three trials, where mipletamig has consistently demonstrated high remission rates and a favorable safety and tolerability profile, with no observed events of cytokine release syndrome in frontline patients treated to date. Building on this clinical validation, Aptevo has built a portfolio of tumor-directed CD3 programs, including bispecific candidates APVO442 (PSMA × CD3) for prostate cancer and APVO455 (Nectin-4 × CD3) for solid tumors, as well as trispecific candidates APVO451 and APVO452. All incorporate the Company's proprietary application and unique use of the CRIS-7-derived CD3 binding domain, designed to enable tumor-focused immune activation with the potential for meaningful antitumor activity while also prioritizing safety and tolerability. About Aptevo Therapeutics Aptevo Therapeutics Inc. (NASDAQ:APVO) is a clinical-stage biotechnology company focused on developing novel bispecific and trispecific immunotherapies for the treatment of cancer. The Company has two clinical candidates. Mipletamig is currently being evaluated in RAINIER, a two-part Phase 1b/2 trial for the treatment of frontline acute myeloid leukemia in combination with standard-of-care venetoclax + azacitidine. Mipletamig has received orphan drug designation ("orphan status") for AML according to the Orphan Drug Act. ALG.APV-527, a bispecific conditional 4-1BB agonist, designed to only be active upon simultaneous binding to 4-1BB and 5T4, is being co-developed with Alligator Bioscience and was most recently evaluated in a Phase 1 clinical trial for the treatment of multiple solid tumor types likely to express 5T4. The Company has six preclinical candidates with different mechanisms of action designed to target a range of solid tumors. All pipeline candidates were created from two proprietary platforms, ADAPTIRand ADAPTIR-FLEX. The Aptevo mission is to improve treatment outcomes and transform the lives of cancer patients. For more information, please visit www.aptevotherapeutics.com. Safe Harbor Statement This press release includes forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. All statements, other than statements of historical fact, including, without limitation, Aptevo's expectations about the activity, efficacy, safety, tolerability and durability of its therapeutic candidates and potential use of any such candidates, including in combination with other drugs, as therapeutics for treatment of disease, its expectations regarding the effectiveness of its ADAPTIR and ADAPTIR-FLEX platforms, statements related to the progress of Aptevo's clinical programs, including statements related to anticipated clinical and regulatory milestones, whether further study of mipletamig in a Phase 1b dose optimization trial focusing on multiple doses of mipletamig in combination with venetoclax + azacitidine on a targeted patient population will continue to show remissions, whether Aptevo's final trial results will vary from its earlier assessment, whether Aptevo's strategy will translate into an improved overall survival in AML, especially among patient subgroups with poor prognosis, whether further study of ALG.APV-527 across multiple tumor types will continue to show clinical benefit, the possibility and timing of interim data readouts for ALG.APV-527, development and continued development of Aptevo's current and potential future molecules, statements related to Aptevo's cash position and balance sheet, statements related to Aptevo's ability to access to capital and funding runway, statements related to Aptevo's ability to generate stockholder value, whether Aptevo will continue to have momentum in its business in the future, and any other statements containing the words "may," "continue to," "believes," "knows," "expects," "optimism," "potential," "designed," "promising," "plans," "will" and similar expressions are intended to identify forward-looking statements. These forward-looking statements are based on Aptevo's current intentions, beliefs, and expectations regarding future events. Aptevo cannot guarantee that any forward-looking statement will be accurate. Investors should realize that if underlying assumptions prove inaccurate or unknown risks or uncertainties materialize, actual results could differ materially from Aptevo's expectations. Investors are, therefore, cautioned not to place undue reliance on any forward-looking statement. There are several important factors that could cause Aptevo's actual results to differ materially from those indicated by such forward-looking statements, including Aptevo's need to obtain shareholder approval to access the full capacity of the ELOC, a deterioration in Aptevo's business or prospects; further assessment of preliminary or interim data or different results from later clinical trials; adverse events and unanticipated problems, adverse developments in clinical development, including unexpected safety issues observed during a clinical trial; and changes in regulatory, social, macroeconomic and political conditions. For instance, actual results may differ materially from those indicated by such forward-looking statements as a result of various important factors, including the uncertainties inherent in the results of preliminary or interim data and preclinical studies being predictive of the results of later-stage clinical trials, initiation, enrollment and maintenance of patients, and the completion of clinical trials, the availability and timing of data from ongoing clinical trials, the trial design includes combination therapies that may make it difficult to accurately ascertain the benefits of mipletamig, expectations for the timing and steps required in the regulatory review process, expectations for regulatory approvals, the impact of competitive products, our ability to enter into agreements with strategic partners or raise funds on acceptable terms or at all and other matters that could affect the availability or commercial potential of Aptevo's product candidates, business or economic disruptions due to catastrophes or other events, including natural disasters or public health crises, geopolitical risks, including the current war between Russia and Ukraine and any other military event that could evolve out of any of the current conflicts, and macroeconomic conditions such as economic uncertainty, imposition of tariffs, rising inflation and interest rates, continued market volatility and decreased consumer confidence. These risks are not exhaustive, Aptevo faces known and unknown risks. Additional risks and factors that may affect results are set forth in Aptevo's filings with the Securities and Exchange Commission, including its Annual Report on Form 10-K for the fiscal year ended December 31, 2024, and its subsequent reports on Form 10-Q and current reports on Form 8-K. The foregoing sets forth many, but not all, of the factors that could cause actual results to differ from Aptevo's expectations in any forward-looking statement. Any forward-looking statement speaks only as of the date of this press release, and, except as required by law, Aptevo does not assume any obligation to update any forward-looking statement to reflect new information, events, or circumstances. CONTACT: Miriam Weber Miller Head, Investor Relations & Corporate Communications Aptevo Therapeutics Email: IR@apvo.com or Millerm@apvo.com Phone: 206-859-6628 SOURCE: Aptevo Therapeutics

临床1期免疫疗法孤儿药临床结果

2026-01-08

·药研苑

百济神州BCL2抑制剂索托克拉国内获批

“药品营销避坑”试读：药品导入期管理视频课（试听）药品生命周期管理（案例）药品立项需要注意什么（案例） 2026年1月6日，百济神州宣布百悦达®（索托克拉片）获得国家药品监督管理局（NMPA）附条件批准，用于治疗既往接受过至少包含布鲁顿酪氨酸激酶（BTK）抑制剂在内的一种系统治疗的慢性淋巴细胞白血病（CLL）/小淋巴细胞淋巴瘤（SLL）成人患者，以及既往接受过至少两种系统性治疗（含布鲁顿酪氨酸激酶[BTK]抑制剂）的复发或难治性套细胞淋巴瘤（MCL）成人患者。此次获批基于BGB-11417-201和BGB-11417-202两项临床试验的研究结果。 BGB-11417-201为全球多中心、单臂、开放性1/2期临床试验。共纳入125名既往接受抗CD20及 BTK抑制剂治疗复发或难治性套细胞淋巴瘤（MCL）成人患者。在1期阶段22名患者接受索托克拉160mg 或320 mg，一天一次。在2期阶段103名患者接受索托克拉320 mg，一天一次治疗。研究结果显示确认总体缓解率（ORR）为52.4%（95% CI: 42.4, 62.4），完全缓解（CR）率为15.5%（95% CI: 9.1, 24.0），中位缓解持续时间（mDOR）为15.8个月（95% CI : 7.4, NE）。34例中国患者的ORR达到61.8%（95% CI: 43.6, 77.8），CR率为26.5%（95% CI: 12.9, 44.4）。 BGB-11417-202为单臂、多中心、开放性2期临床试验。共纳入100名既往BTK抑制剂联合化疗免疫治疗（CIT）不耐受或治疗失败，但未接受过BCL2抑制剂治疗的患者。入组患者接受索托克拉320 mg，一天一次。研究结果显示确认总体缓解率（ORR）为80.5%（95% CI: 70.3, 88.4），完全缓解或完全缓解伴骨髓造血不完全恢复（CR/CRi）率为26.8%（95% CI: 17.6, 37.8），12个月时的缓解持续时间（DOR）无事件率为84.7%。在安全性方面≥30%治疗期间不良事件（TEAE）包括中性粒细胞计数下降（54.0%），血小板减少（41.0%）、贫血（33.0%）、高尿酸血症（33.0%）和白细胞计数下降（30.0%）。61.0%的患者发生≥3级治疗期间不良事件。治疗期间严重不良事件（TESAE）的发生率为38.0%。≥3级且发生率≥10%的治疗期间不良事件的发生率为中性粒细胞计数下降（33.0%）、肺炎（17.0%）、血小板计数减少（11.0%），白细胞计数减少（10.0%）。未发生临床意义的肿瘤溶解综合征（TLS）。4.0%的患者性实验室意义的TLS，均为3级，中位数缓解天数为3.5天（2-8），无一例患者由于TLS导致治疗中止或死亡。5.0%患者由于TEAE导致减药，6.0%患者中止治疗。5人（5.0%）因TEAE死亡，均被认为与治疗无关（Shuhua Yi, 2025）。索托克拉（Sonrotoclax，BGB-11417）为BCL2抑制剂，对于BCL2的选择性远高于Bcl-xL，索托克拉对于野生型和G101V突变型BCL2都具有较强的抑制作用，并且强于维奈克拉Venetoclax、利沙托克拉Lisaftoclax和Lacutoclax（Yunhang Guo., 2024）。相关阅读：爱科百发复方氯丝右哌甲酯国内获批治疗注意缺陷多动障碍赛诺菲普乐司兰国内获批降低FCS甘油三酯水平默沙东索特西普国内获批治疗肺动脉高压清普生物发布QP-6211镇痛3期临床试验研究数据新型抗炎药Vilobelimab用于坏疽性脓皮病3期研究新数据发布 2025年1-3季度口溶膜制剂哪家强？强生提前中止双特异性抗体JNJ-5939 2b期临床试验 FDA批准口服神经激肽-1受体拮抗剂Tradipitant治疗晕动症依普隆特生国内获批治疗TTR淀粉样变性多发性神经病免疫检查点抑制剂，谁将成为下一个王者？质子泵相关抑酸类药物市场即将回暖改剂型，口服液体制剂“金矿”还是“陷阱” 生物仿制药不再要求必须开展临床试验，FDA发布新指导原则草案中药1类新药距离封神还有多远药品导入期管理视频课相关内容只作为药物研发的参信息。不构成任何与用药咨询有关的建议。如需发稿，您可通过在药研苑公众号下以发送信息的方式将官网或官方公众号的稿件链接和标题发送给我们。我们将择优确定是否发布。

临床结果临床2期

2026-01-08

·ioncology

ASH国际视野丨 Wojciech Jurczak教授：BRUIN CLL-313研究首发，非共价BTKi或重塑一线CLL/SLL治疗格局

编者按慢性淋巴细胞白血病（CLL）/小淋巴细胞淋巴瘤（SLL）是一类主要发生于中老年人群的成熟B细胞克隆性增殖性肿瘤，具有独特免疫表型。在2025年ASH大会LBA专场中，玛丽亚·斯克沃多夫斯卡-居里国家肿瘤研究所Wojciech Jurczak教授报告了BRUIN CLL-313研究的首次结果，该随机Ⅲ期试验比较了非共价BTK抑制剂匹妥布替尼与苯达莫司汀联合利妥昔单抗（BR）在初治CLL/SLL患者中的疗效与安全性。《肿瘤瞭望-血液时讯》现场特邀Wojciech Jurczak教授对研究背景、设计及临床意义进行解读，为临床实践提供前沿参考。《肿瘤瞭望-血液时讯》 01 在本次ASH大会上，您报告了匹妥布替尼与苯达莫司汀联合利妥昔单抗（BR）治疗未治疗CLL/SLL患者的比较研究。可以请您详细介绍一下这项研究的背景和研究设计，以及为何选择将匹妥布替尼与BR进行对比？ Wojciech Jurczak教授：欢迎来到奥兰多2025 ASH年会。我很荣幸向各位介绍BRUIN CLL-313研究。这是一项针对初治CLL患者的随机对照试验，旨在比较口服BTK抑制剂匹妥布替尼与苯达莫司汀联合利妥昔单抗（BR方案）的疗效。入组患者均需符合iwCLL 2018标准的治疗指征。在研究设计阶段，化学免疫治疗对包括高危患者在内的所有病例仍被视为合理选择。当时，靶向治疗主要以BTK抑制剂为基础，大多数接受治疗的患者采用无限期BTK抑制剂方案。虽然化学免疫治疗仍可作为备选方案，但如今临床实践已发生显著变化。值得注意的是，尽管17p缺失患者未被纳入研究，但中心实验室分析显示约10%的患者存在TP53突变。这些患者被纳入研究方案，并在两治疗组间分布均衡。上下滑动查看英文 Oncology Frontier-Hematology Frontier：At this ASH meeting, you reported on the study comparing pirtobrutinib with bendamustine plus rituximab (BR) in treatment-naïve CLL/SLL patients. Could you please elaborate on the background and design of this study, and why you chose to compare pirtobrutinib with BR? Professor Wojciech Jurczak：Welcome to the 2025 ASH Annual Meeting in Orlando. It is my honor to present the BRUIN CLL-313 study. This is a randomized controlled trial evaluating the oral BTK inhibitor pirtobrutinib versus bendamustine plus rituximab (BR regimen) in treatment-naïve patients with chronic lymphocytic leukemia (CLL) who meet treatment criteria according to the iwCLL 2018 guidelines. At the time of study design, chemoimmunotherapy was still considered a reasonable option for all patients, including those with high-risk features. Targeted therapy was then primarily based on BTK inhibitors, with the majority of treated patients receiving indefinite BTK inhibitor therapy. Although chemoimmunotherapy remained an alternative at that time, clinical practice has since evolved substantially. Notably, while patients with 17p deletion were excluded from the study, central laboratory analysis revealed that approximately 10% of enrolled patients harbored TP53 mutations. These patients were included in the trial and were evenly distributed between the two treatment arms. 《肿瘤瞭望-血液时讯》 02 研究结果表明，匹妥布替尼显著改善了IRC评估的无进展生存期（PFS）和总体缓解率（ORR）。并且，匹妥布替尼在IGHV突变型和非突变型患者中均表现出一致的PFS获益，您认为这一发现对临床治疗有何重要意义？ Wojciech Jurczak教授：本研究的主要终点为独立评审委员会评估的无进展生存期（PFS）。苯达莫司汀联合利妥昔单抗（BR）组中位PFS为34个月，而匹妥布替尼组尚未达到。在两年随访分析中，匹妥布替尼组的PFS率为94%，BR组为70%，差异具有统计学意义和临床意义。两组的风险比为0.20，为同类比较中的最佳水平；相比之下，其他BTK抑制剂的风险比接近0.3至0.4。这表明，匹妥布替尼可将患者疾病进展或任何原因导致死亡的风险降低80%，具有显著的临床意义。总体生存期（OS）中期分析尚未成熟，但已显示有利趋势。2年OS率在匹妥布替尼组为98%，BR组为94%。在此过程中，匹妥布替尼组报告3例死亡，BR组报告12例死亡。上下滑动查看英文 Oncology Frontier-Hematology Frontier：The results show that pirtobrutinib significantly improved IRC-assessed progression-free survival (PFS) and overall response rate (ORR). Additionally, pirtobrutinib showed consistent PFS benefit in both IGHV-mutated and unmutated patients. What do you think is the clinical significance of this finding? Professor Wojciech Jurczak：The primary endpoint of this study was progression-free survival (PFS) assessed by an independent review committee. The median PFS was 34 months in the bendamustine plus rituximab (BR) arm, while it was not reached in the pirtobrutinib arm. At the two-year follow-up analysis, the PFS rate was 94% in the pirtobrutinib arm compared with 70% in the BR arm, with the difference being statistically and clinically significant. The hazard ratio between the two arms was 0.20, representing the best level among similar comparisons; in contrast, other BTK inhibitors had hazard ratios close to 0.3–0.4. This indicates that pirtobrutinib reduced the risk of disease progression or death from any cause by 80%, demonstrating substantial clinical benefit. The interim analysis of overall survival (OS) is still immature but shows a favorable trend. The two-year OS rate was 98% in the pirtobrutinib arm and 94% in the BR arm. During this period, there were 3 deaths reported in the pirtobrutinib arm and 12 deaths in the BR arm. 《肿瘤瞭望-血液时讯》 03 尽管目前OS数据尚不成熟，但您在研究中观察到有利匹妥布替尼的生存趋势。您如何看待匹妥布替尼在未治疗CLL/SLL患者中的潜力，特别是在可能仅接受一线治疗的老年患者中？ Wojciech Jurczak教授：本研究显示匹妥布替尼在PFS方面具有显著优势，并显示出潜在的OS获益，结合BRUIN CLL-314研究结果，有望推动匹妥布替尼获批用于初治慢性淋巴细胞白血病（CLL）患者。匹妥布替尼于2023年12月首次获FDA加速批准，用于既往接受过BTK抑制剂和BCL2抑制剂治疗的双重耐药患者；2025年12月3日，其适应症进一步扩展至所有经共价BTK抑制剂治疗后疾病进展的患者。若上述两项随机对照研究数据获得监管机构认可，匹妥布替尼有望成为初治CLL患者的治疗选择。从临床实践角度，BTK抑制剂已不再是靶向治疗的唯一核心选项。当前治疗策略已扩展至固定疗程联合方案，包括维奈克拉联合抗CD20单抗，或BTK抑制剂联合BCL2抑制剂。对于年轻且身体状态良好的患者，尤其是希望在治疗结束后恢复正常生活质量的患者，优先推荐固定疗程方案。而对于老年或伴有共病的体弱患者，治疗决策需综合考虑其功能状态。此类患者日常活动受限，每次就医可能增加感染风险甚至危及生命，因此每日单药口服、便于基层管理的方案可能更具实用性和安全性。上下滑动查看英文 Oncology Frontier-Hematology Frontier：Although the overall survival (OS) data is not yet fully mature, you observed a trend favoring pirtobrutinib in survival. How do you assess the potential of pirtobrutinib in treatment-naïve CLL/SLL patients, particularly in elderly patients who may only receive first-line treatment? Professor Wojciech Jurczak：The present study demonstrates that pirtobrutinib confers a significant advantage in progression-free survival (PFS) and suggests potential overall survival (OS) benefit. Combined with results from the BRUIN CLL-314 study, these findings are expected to support regulatory submission for approval of pirtobrutinib in treatment-naïve patients with chronic lymphocytic leukemia (CLL). Pirtobrutinib initially received accelerated FDA approval in December 2023 for patients previously treated with both a BTK inhibitor and a BCL2 inhibitor (double-exposed population). On December 3, 2025, the indication was expanded to include all patients whose disease progressed after treatment with a covalent BTK inhibitor. If the data from the aforementioned randomized controlled trials are accepted by regulatory authorities, pirtobrutinib may become an additional treatment option for treatment-naïve CLL patients. From a clinical practice perspective, BTK inhibitors are no longer the sole cornerstone of targeted therapy. Current strategies have broadened to include fixed-duration combination regimens, such as venetoclax plus an anti-CD20 antibody, or a BTK inhibitor combined with a BCL2 inhibitor. For younger patients with good performance status—particularly those seeking to regain near-normal quality of life post-treatment—fixed-duration regimens are preferentially recommended to enable a treatment-free interval. In contrast, for elderly or frail patients with comorbidities, treatment decisions must account for functional status. These patients often have limited daily activity, and frequent medical visits may heighten infection risk or pose life-threatening challenges. Consequently, a once-daily oral monotherapy that facilitates community-based management may offer greater practicality and safety. 《肿瘤瞭望-血液时讯》 04 研究还显示，匹妥布替尼具有较低的治疗相关不良事件（TEAE）发生率，尤其是与BR相比。您能否进一步探讨匹妥布替尼的安全性和耐受性，特别是对于年长患者或有合并症的患者？ Wojciech Jurczak教授：匹妥布替尼表现出良好的耐受性。在安全性分析中，患者平均接受匹妥布替尼治疗33个月，而固定苯达莫司汀联合利妥昔单抗（BR）方案仅为6个月。即使在原始数据中，匹妥布替尼的不良事件发生率亦较低，尤其是CTCAE 3级及以上的不良事件。时间校正分析显示，匹妥布替尼所有不良事件的发生率均低于BR方案，出血倾向虽略高，但大多数为轻度，仅观察到一例3级出血。在BTK抑制剂特别关注的不良事件中，房颤及房扑的发生率维持在低水平，研究中20名75岁以上患者仅有一例发生房颤。因此，匹妥布替尼可被视为安全性良好的治疗药物。需要指出的是，接受长期治疗的患者可能存在免疫功能受损的情况。基于经验，一旦患者出现感染，应考虑暂停匹妥布替尼及所有BTK抑制剂，以避免药物相互作用，同时使全科医生能够根据当地标准对感染进行规范治疗。若在使用BTK抑制剂期间同时给予某些抗生素（不包括抗真菌药物），可能导致BTK抑制剂血药浓度升高，从而影响免疫功能并潜在干扰治疗效果。上述内容为在随机化研究方案基础上的补充说明，其中最后部分为个人经验性建议，不应作为普遍引用的指导。上下滑动查看英文 Oncology Frontier-Hematology Frontier：The study also shows that pirtobrutinib has a lower incidence of treatment-emergent adverse events (TEAEs), especially compared to BR. Could you further discuss the safety and tolerability of pirtobrutinib, particularly for elderly patients or those with comorbidities? Professor Wojciech Jurczak：Pirtobrutinib demonstrates a favorable tolerability profile. In the safety analysis, patients received pirtobrutinib for an average of 33 months, compared with only 6 months for the fixed-duration bendamustine plus rituximab (BR) regimen. Even in the raw data, the incidence of adverse events with pirtobrutinib was lower, particularly for CTCAE grade 3 or higher events. Time-adjusted analyses indicated that the incidence of all adverse events was lower with pirtobrutinib than with BR, although bleeding tendency was slightly higher; most events were mild, with only a single grade 3 hemorrhage observed. Among adverse events of special interest for BTK inhibitors, the incidence of atrial fibrillation and flutter remained low, with only one case occurring among 20 patients over 75 years of age. Therefore, pirtobrutinib can be considered a treatment with a favorable safety profile. It should be noted that patients receiving long-term therapy may experience impaired immune function. Based on clinical experience, if a patient develops an infection, it is advisable to temporarily suspend pirtobrutinib and all BTK inhibitors to avoid drug interactions and allow general practitioners to manage the infection according to local standards. Concomitant use of certain antibiotics (excluding antifungals) with BTK inhibitors may increase BTK inhibitor blood concentrations, potentially impairing immune function and affecting treatment outcomes. The above statements are supplementary to data obtained from randomized trial protocols; the final section reflects personal clinical experience and should not be considered as broadly generalizable guidance. 专家简介 Wojciech Jurczak 教授玛丽亚·斯克沃多夫斯卡-居里国家肿瘤研究所医学博士，血液学顾问及教授玛丽亚·斯克沃多夫斯卡-居里国家肿瘤研究所（Maria Skłodowska-Curie National Research Institute of Oncology）科室主任（来源：《肿瘤瞭望–血液时讯》编辑部）声明凡署名原创的文章版权属《肿瘤瞭望》所有，欢迎分享、转载。本文仅供医疗卫生专业人士了解最新医药资讯参考使用，不代表本平台观点。该等信息不能以任何方式取代专业的医疗指导，也不应被视为诊疗建议，如果该信息被用于资讯以外的目的，本站及作者不承担相关责任。

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	AbbVie, Inc.	2022-10-01
复发性急性髓细胞白血病	临床3期	美国	Genentech, Inc.	2022-10-01

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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


NCT05799079 (CTgov)	临床2期	复发性急性髓细胞白血病 \| 复发性急性白血病	1	DEC-C+Venetoclax	遞蓋齋鬱鏇鹹願鏇繭餘 = 觸觸鑰窪窪願壓鬱觸壓網遞衊壓淵壓構網糧膚 (醖觸鹹願獵壓範廠齋蓋, 顧壓範淵齋簾衊夢觸廠 ~ 遞願構襯餘網鹹廠壓構) 更多	-	2026-01-09
NCT06763666 (ASH2025)	临床2期	难治性急性髓细胞白血病	79	Venetoclax + CLAG regimen	壓獵觸壓鏇網蓋淵餘膚(構壓壓憲鑰築遞襯廠鏇) = 構選淵遞繭鬱艱構夢淵網醖鬱壓鏇範糧築鏇醖 (築顧鑰範觸簾糧窪獵窪 ) 更多	积极	2025-12-06
				CLAG regimen	壓獵觸壓鏇網蓋淵餘膚(構壓壓憲鑰築遞襯廠鏇) = 廠網餘願壓鑰衊醖選構網醖鬱壓鏇範糧築鏇醖 (築顧鑰範觸簾糧窪獵窪 ) 更多
ASH2025	N/A	慢性淋巴细胞白血病 \| 小淋巴细胞淋巴瘤	45	Zanubrutinib+venetoclax	廠選壓選獵壓築構遞艱(製蓋廠遞窪膚齋鹽鏇獵) = The most common any grade AE that occurred in 20% or more pts were fatigue (56%), diarrhea (53%), hypertension (31%), nausea (27%), upper respiratory infection (27%), arthralgia (27%), bruising (24%), neutropenia (22%), thrombocytopenia (22%), and rash (20%). No atrial fibrillation was recorded. 齋壓製鬱繭簾範選衊築 (製窪窪鬱簾鑰憲獵鏇遞 ) 更多	积极	2025-12-06
ASH2025	N/A	骨髓增生异常综合征	1,198	Hypomethylating agent (HMA) + Venetoclax	簾鑰繭鑰齋蓋遞壓願膚(製壓鑰鬱齋鏇範憲獵鹹) = 簾齋齋衊積衊糧築積繭淵糧鹹簾選簾窪簾範齋 (糧獵淵壓鏇壓鹽範蓋網 ) 更多	积极	2025-12-06
				Hypomethylating agent (HMA)	簾鑰繭鑰齋蓋遞壓願膚(製壓鑰鬱齋鏇範憲獵鹹) = 壓艱廠遞齋憲構鏇鏇積淵糧鹹簾選簾窪簾範齋 (糧獵淵壓鏇壓鹽範蓋網 ) 更多
ASH2025	N/A	慢性淋巴细胞白血病一线	3,844	Second-generation BTKi	鏇夢鏇簾鏇鹹鏇鹽鑰窪(鏇簾顧衊衊淵糧夢糧膚) = 廠襯蓋選積廠鹹壓鏇觸餘顧夢願餘艱憲顧憲顧 (觸鹹鹽窪夢獵醖簾窪壓 )	积极	2025-12-06
				V+O	鏇夢鏇簾鏇鹹鏇鹽鑰窪(鏇簾顧衊衊淵糧夢糧膚) = 構繭構鹽廠夢鹹簾獵觸餘顧夢願餘艱憲顧憲顧 (觸鹹鹽窪夢獵醖簾窪壓 )
ASH2025	临床2期	急性白血病维持	58	Venetoclax 200 mgAzacitidine 32 mg/m2 + Venetoclax 200 mgAzacitidine 32 mg/m2	範鏇鹹顧鹽顧選夢築顧(蓋鏇選窪鹹窪鏇廠淵鹹) = 製願顧廠顧網範襯壓築顧齋鑰築壓廠遞蓋鏇網 (遞壓願壓艱繭製繭廠願, 51.4 ~ 78.1) 更多	积极	2025-12-06
flamsaclax (ASH2025)	临床1/2期	高危骨髓增生异常综合征	9	Venetoclax + FLAMSA + Treosulfan	膚遞構餘蓋鹹糧膚繭襯(網鬱遞窪構繭窪膚淵願) = Adverse events included grade 3 to 4 hematotoxicity as well as gastrointestinal disorders, febrile neutropenia, infections and electrolyte imbalances typical for the early phase after alloHSCT. There was no VOD and no specific unexpected toxicity attributable to Venetoclax identified. 鹽鏇願膚鏇範夢觸夢鏇 (構鏇壓鏇簾觸壓鑰憲獵 )	积极	2025-12-06
ASH2025	N/A	慢性淋巴细胞白血病	294	Venetoclax	顧範窪製鏇製衊窪膚遞(醖憲選鹹蓋壓壓窪構壓) = 膚觸鬱選餘簾鑰餘積鬱觸窪選夢齋餘顧網繭製 (製餘構醖繭窪艱醖衊繭 ) 更多	积极	2025-12-06
				Ibrutinib	顧範窪製鏇製衊窪膚遞(醖憲選鹹蓋壓壓窪構壓) = 夢蓋壓鑰積繭醖獵醖齋觸窪選夢齋餘顧網繭製 (製餘構醖繭窪艱醖衊繭 ) 更多
ASH2025	N/A	急性髓性白血病 \| 骨髓增生异常/骨髓增生性疾病	61	Venetoclax for >14 days	繭簾艱蓋製範選膚襯膚(襯膚鹽範醖淵鑰鏇遞鑰) = 壓觸窪顧齋襯鹹夢鹹簾鹹夢網膚膚憲襯築鹽簾 (積膚廠鏇鹹憲築鏇範築 ) 更多	积极	2025-12-06
				Venetoclax for 14 days	繭簾艱蓋製範選膚襯膚(襯膚鹽範醖淵鑰鏇遞鑰) = 膚廠艱鹹淵糧簾構夢繭鹹夢網膚膚憲襯築鹽簾 (積膚廠鏇鹹憲築鏇範築 ) 更多
ASH2025	N/A	伴有 FLT3/ITD 突变的急性髓系白血病 FLT3-ITD mutation	48	AzacitidineVenetoclaxGilteritinib + AzacitidineVenetoclaxGilteritinib + AzacitidineVenetoclaxGilteritinib (FLT3-ITD mutated AML + Refractory/Relapsed disease or persistent MRD)	夢鏇艱簾願簾窪醖廠壓(壓鹹獵餘獵淵廠糧獵蓋) = 憲糧壓夢齋顧蓋獵網鑰襯蓋醖積繭構窪觸壓窪 (廠衊簾艱淵膚積積構積, 3.8 ~ 21.0) 更多	积极	2025-12-06