Phase II Study of Cytarabine + Daunorubicin (7 + 3) + Gemtuzumab Ozogamicin vs. Cytarabine + Daunorubicin (7 + 3) + Venetoclax for the Treatment of Newly Diagnosed Core Binding Factor Acute Myeloid Leukemia (CBF-AML) in Younger Adults: A MyeloMATCH Substudy

This phase II MYELOMATCH treatment trial compares the effect of venetoclax to gemtuzumab ozogamicin, when given with cytarabine and daunorubicin ("7+3" regimen), for the treatment of patients with core binding factor acute myeloid leukemia (CBF-AML). 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. Gemtuzumab ozogamicin is a monoclonal antibody, called gemtuzumab, linked to an antitumor antibiotic drug, called ozogamicin. Gemtuzumab is a form of targeted therapy because it attaches to specific molecules (receptors) on the surface of cancer cells, known as CD33 receptors, and delivers ozogamicin to kill them. Chemotherapy drugs, such as cytarabine and daunorubicin work in different ways to stop the growth of cancer cells either by killing the cells, by stopping them from dividing, or by stopping them from spreading. Giving venetoclax with cytarabine and daunorubicin may have fewer side effects and be as effective or better than the combination with gemtuzumab ozogamicin in treating patients with core binding factor AML.

开始日期2027-02-02

申办/合作机构

National Cancer Institute

NCT07582159

/ Not yet recruiting临床2期IIT

A Phase 2 Study of Acalabrutinib, Venetoclax and Tafasitamab (AVT) in Patients With Previously Untreated Chronic Lymphocytic Leukemia/Small Lymphocytic Lymphoma (CLL/SLL)

This phase II trial tests the safety, side effects and how well giving tafasitamab with acalabrutinib and venetoclax works for the treatment of chronic lymphocytic leukemia (CLL)/small cell lymphoma (SLL). A monoclonal antibody is a type of protein that can bind to certain targets in the body, such as molecules that cause the body to make an immune response (antigens). Tafasitamab is a monoclonal antibody that binds to CD19 antigen which is found on the surface of most B cells (a type of white blood cell) and some lymphoma cells. This may help the immune system kill cancer cells. Acalabrutinib is in a class of medications called kinase inhibitors. It blocks a protein called BTK, which is present on B-cell (a type of white blood cells) cancers such as mantle cell lymphoma at abnormal levels. This may help keep cancer cells from growing and spreading. 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. Giving tafasitamab with acalabrutinib and venetoclax may be safe and effective for treating patients with CLL/SLL.

开始日期2026-12-19

申办/合作机构

City of Hope National Medical Center

[+1]

NCT07425808

/ Not yet recruiting临床2/3期IIT

Gilteritinib in Combination With Azacitidine and Venetoclax Compared to Induction Chemotherapy "7+3" in Combination With a FLT3-inhibitor in Fit, Newly Diagnosed, FLT3-ITD Mutated Adult AML Patients: a Randomized Trial of the EORTC Leukemia Group and GIMEMA.

This international, multicenter, randomized (1:1), open-label phase II/III trial will evaluate the efficacy and safety of gilteritinib combined with azacitidine and venetoclax (experimental arm) versus standard "7+3" induction plus a FLT3inhibitor (quizartinib or midostaurin) (control arm) in newly diagnosed FLT3-ITD mutated AML patients eligible for intensive chemotherapy.

开始日期2026-12-01

申办/合作机构

European Organisation for Research & Treatment of Cancer

[+2]

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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5,304

项与维奈克拉相关的文献（医药）

2026-12-01·Blood Research

The role of m6A RNA methyltransferase METTL3 in drug resistance mechanisms in acute myeloid leukemia

Review

作者: Prajapati, Suresh ; Patel, Mansi ; Gupta, Reeshu ; Jyotishi, Charmi

Abstract:

This review examines the role of METTL3, a core RNA methyltransferase, in therapeutic resistance in acute myeloid leukemia (AML) and discusses emerging strategies to address this challenge. METTL3 regulates N 6 -methyladenosine (m 6 A) modifications on transcripts involved in key cellular processes, including apoptosis (BCL2, MCL1), metabolism (PGC-1α, CSRP1), proliferation (MYC), autophagy (FOXO3), and bone marrow microenvironmental interactions (ITGA4, AKT1). These modifications enhance the stability and translation of resistance-associated genes, supporting leukemic cell survival under treatment pressure. Pharmacological targeting of METTL3 has shown efficacy in preclinical AML models. Inhibitors such as STM2457, METTL3-directed PROTACs, and rational drug combinations with agents including venetoclax, anthracyclines, and ATRA, have reversed resistance phenotypes and impaired leukemic cell fitness. Beyond canonical resistance mechanisms, METTL3 also regulates noncoding RNAs, autophagy, and metabolic–epigenetic crosstalk, including histone lactylation, linking epitranscriptomic regulation to broader resistance pathways. By integrating molecular, cellular, and microenvironmental evidence, this review underscores METTL3 as a central driver of drug resistance and a promising therapeutic target in relapsed or refractory AML. Unlike previous summaries, it highlights the convergence of METTL3-mediated m 6 A modifications with noncoding RNA regulation, autophagy, and niche adaptation, and critically evaluates emerging therapeutic approaches, including catalytic inhibitors, PROTACs, and natural compounds.

2026-07-01·LEUKEMIA RESEARCH

Risk factors and fluid management in tumor lysis syndrome of acute myeloid leukemia: A retrospective study

Article

作者: Zhao, Xiaodan ; Lin, Xiangjie ; Yuan, Fei ; Wang, Jinghan

Current tumor lysis syndrome (TLS) risk stratification for acute myeloid leukemia (AML) is insufficient. This retrospective study included 191 AML patients undergoing induction chemotherapy to identify TLS predictors and evaluate fluid management's impact. TLS occurred in 44 (23.1%) patients, 82% within 72 h post-treatment, with severe cases peaking at 12-24 h. Multivariable and LASSO analyses identified independent risk factors: male gender (OR=3.28, p = 0.025), higher blast percentage (OR=1.03, p = 0.006), elevated baseline uric acid (OR=1.01, p = 0.011), IDH1/2 mutation (OR=4.86, p = 0.005), and a trend with venetoclax-based therapy (OR=7.52, p = 0.072). Higher baseline calcium was protective (OR=0.03, p = 0.025). Adequate urine output reduced TLS risk, while excessive positive fluid balance correlated with severe TLS (p = 0.046). Individualized fluid management and 72-hour intensive monitoring are critical for high-risk groups.

2026-07-01·EXPERIMENTAL CELL RESEARCH

The ATF4/PSAT1/JNK signaling axis suppresses ferroptosis to drive venetoclax resistance in AML

Article

作者: Tao, YanLing ; Huang, WenHui ; Zhang, Hao ; Zhang, MingYan ; Zhu, XunXun

Metabolic reprogramming has emerged as a key driver of therapy resistance in acute myeloid leukemia (AML). Here, we identify phosphoserine aminotransferase 1 (PSAT1) as a critical metabolic determinant of venetoclax (VEN) resistance through the suppression of ferroptosis. PSAT1 was consistently upregulated in VEN-resistant cell lines and relapsed patient samples. Mechanistically, the transcription factor ATF4 directly bound the PSAT1 promoter, enhancing its expression and subsequently promoting glutathione synthesis, depleting the labile iron pool, and attenuating lipid peroxidation. Concurrently, PSAT1 functioned to restrain JNK/c-Jun signaling. Knockdown of PSAT1 restored VEN sensitivity by triggering ferroptosis and modulating the expression of BCL-2 and GPX4. Clinically, elevated PSAT1 expression predicted poor patient survival. Our findings unveil the ATF4/PSAT1/JNK axis as a master regulator of ferroptosis in AML, revealing a druggable pathway to overcome VEN resistance.

2,572

项与维奈克拉相关的新闻（医药）

2026-06-04

·BioSpace

Taiho Oncology Announces New England Journal of Medicine Publication of First All-Oral Regimen in Newly Diagnosed Acute Myeloid Leukemia

Publication highlights positive results for the first all-oral decitabine-cedazuridine plus venetoclax regimen in newly diagnosed acute myeloid leukemia patients who are ineligible for intensive induction chemotherapy. PRINCETON, N.J.--(BUSINESS WIRE)--Taiho Oncology, Inc., a company developing and commercializing novel treatments for hematologic malignancies and solid tumors, today announced the publication in the New England Journal of Medicine of results from the ASCERTAIN-V Phase 1/2 clinical trial, which evaluated the first all-oral regimen of decitabine-cedazuridine plus venetoclax in patients with newly diagnosed acute myeloid leukemia (AML) who are ineligible for intensive induction chemotherapy. The study demonstrated favorable response rates and survival with expected myelosuppressive effects. 1 Previously presented at the 2025 ASCO Annual Meeting and the 2025 European Hematology Association Congress, the results suggest this first all-oral regimen may provide outcomes consistent with existing hypomethylating agent–venetoclax–based approaches for patients with newly diagnosed AML who cannot receive intensive induction therapy. Nearly 23,000 people in the U.S. are expected to be diagnosed with AML, a cancer of the blood and bone marrow, in 2026. 2 More than half of those patients will likely be deemed ineligible for intensive induction chemotherapy because of factors such as older age (75 or older) or poor health. 3 For these patients, the standard treatment often combines oral venetoclax with parenteral hypomethylating agents, requiring frequent injections or infusions and an average of 12.9 days per month engaging in healthcare visits. 4 Oral decitabine-cedazuridine is a hypomethylating agent that has demonstrated oral bioavailability and equivalent pharmacokinetic exposure to intravenous decitabine. 5 “We are committed to advancing therapies that improve the lives of patients, their families and their caregivers,” said Harold Keer, MD, PhD, Chief Medical Officer, Taiho Oncology. “An all-oral regimen for AML could help reduce the significant time and cost burden associated with treatment in hospitals or infusion centers.” The ASCERTAIN-V trial evaluated the first all-oral regimen of oral decitabine-cedazuridine plus venetoclax in 189 patients (Phase 1, n=30; Phase 2a, n=58; Phase 2b, n=101). After an initial ramp-up period, patients were treated in 28-day cycles, receiving decitabine-cedazuridine on days one through five and venetoclax daily. Key results include complete response rates, durable remissions and survival, and a safety pro with hypomethylating agent-venetoclax regimens. In the Phase 2b of ASCERTAIN-V: The complete response rate was achieved in 47% of patients (95% CI: 36-57%). The composite of complete response or complete response with incomplete hematologic recovery was 63% (95% CI: 53-73%). The median time to marrow blasts of less than 5% was 28 days (range 22 to 57), and the median time to a complete response or complete response with incomplete hematologic recovery was 35 days (range 27 to 58). Among patients achieving complete response, 80% (95% CI: 64%, 90%) had an ongoing response at six months and 75% (95% CI: 57%, 87%) at 12 months. Median overall survival was 15.5 months (95% CI 7.6-not estimable). The 30- and 60-day mortality rates were 3% and 10%, respectively. The median follow-up period was 11.2 months. Serious adverse events were reported in 84% of patients, consistent with known hypomethylating agent–venetoclax regimens. Common related Grade ≥3 adverse events were anemia (30%), neutropenia (26%) and febrile neutropenia (25%). No drug–drug interactions were observed between decitabine-cedazuridine and venetoclax. In the Phase 2b of ASCERTAIN-V, decitabine-cedazuridine and venetoclax dosing was modified once leukemic blast clearance was achieved as measured by bone marrow morphology assessments. Serious adverse events and febrile neutropenia decreased as venetoclax dosing days decreased with each treatment cycle. This information potentially supports the need to explore a treatment strategy of an initial induction followed by dose-adjusting ongoing cycles to enhance tolerability and minimize cytopenia-related complications in patients who have reached remission. “The positive results of the trial — response rates, safety, pharmacokinetics and tolerability data — suggest that an all-oral regimen could potentially become a meaningful alternative to existing treatment protocols that involve parenteral hypomethylating agents for patients with AML who can’t undergo intensive induction chemotherapy,” said Gail J. Roboz, M.D., the paper’s lead author, a professor of medicine, director of the Clinical and Translational Leukemia Program and a member of the Sandra and Edward Meyer Cancer Center at Weill Cornell Medicine and a hematologist oncologist at NewYork-Presbyterian/Weill Cornell Medical Center in New York City. “An all-oral treatment regimen is a highly anticipated addition to current treatment options for patients with AML.” About Decitabine and Cedazuridine Fixed-Dose Combination This product is an orally administered, fixed dose combination of the approved anti-cancer DNA hypomethylating agent, decitabine, together with cedazuridine, 6 an inhibitor of cytidine deaminase. 7 By inhibiting cytidine deaminase in the gut and the liver, the fixed dose combination is designed to allow for oral delivery of decitabine over five days in a given cycle to achieve comparable systemic exposure to IV decitabine administered over five days. About Taiho Oncology, Inc. The mission of Taiho Oncology, Inc. is to improve the lives of patients with cancer, their families and their caregivers. The company specializes in the development and commercialization of orally administered anti-cancer agents for various tumor types. Taiho Oncology has a robust pipeline of small-molecule clinical candidates targeting solid-tumor and hematological malignancies, with additional candidates in pre-clinical development. Taiho Oncology is a subsidiary of Taiho Pharmaceutical Co., Ltd. which is part of Otsuka Holdings Co., Ltd. Taiho Oncology is headquartered in Princeton, New Jersey and oversees its parent company’s European and Canadian operations, which are located in Baar, Switzerland and Oakville, Ontario, Canada. For more information, visit , and follow us on LinkedIn and X. Taiho Oncology and the Taiho Oncology logo are registered trademarks of Taiho Pharmaceutical Co., Ltd. References Roboz G, Zeidan A, Mannis G, Montesinos P, Arnan M, Savona M, et al. All-Oral Treatment of Newly Diagnosed Acute Myeloid Leukemia. Published June 3, 2026. N Engl J Med 2026;394:2107-2116. Vol 394 No. 21. American Cancer Society. Key Statistics for Acute Myeloid Leukemia (AML). Revised January 13, 2026. Accessed February 4, 2026. Heuser M, Fernandez C, Hauch O, Klibanov OM, Chaudhary T, Rives V. Therapies for acute myeloid leukemia in patients ineligible for standard induction chemotherapy: a systematic review. Future Oncol . 2022;19(11):789-810. . Zeidan A, Zhao R, Voegel A, Christensen D, Zhdanava M, Tardif-Samson A, Vanden Eynde C, Keer H, Pilon D. Time burden of treatment with parenteral hypomethylating agents in combination with venetoclax among patients with newly diagnosed Acute Myeloid Leukemia. [ASH Abstract]. Blood (2025) 146 (Supplement 1): 6990. Garcia-Manero G, McCloskey J, Griffiths EA, et al. Oral decitabine-cedazuridine versus intravenous decitabine for myelodysplastic syndromes and chronic myelomonocytic leukaemia (ASCERTAIN): a registrational, randomised, crossover, pharmacokinetics, phase 3 study. Lancet Haematol 2024;11:e15-e26. (23)00338-1/abstract Oganesian A, Redkar S, Taverna P, Choy G, Joshi-Hangal R, Azab M. Preclinical data in cynomolgus (cyn) monkeys of ASTX727, a novel oral hypomethylating agent (HMA) composed of low-dose oral decitabine combined with a novel cytidine deaminase inhibitor (CDAi) E7727 [ASH Abstract]. Blood 2013;122(21): Abstract 2526. Ferraris D, Duvall B, Delahanty G, Mistry B, Alt, J, Rojas C, et al. Design, synthesis, and pharmacological evaluation of fluorinated tetrahydrouridine derivatives as inhibitors of cytidine deaminase. J Med Chem 2014; 57:2582-2588. Contacts Taiho Oncology Contact: Leigh Labrie +1 609.664.9878 llabrie@taihooncology.com

临床结果临床3期临床2期

2026-06-03

·MPN家园

3・20 中国血小板日现场回顾视频｜常春康教授：2026骨髓纤维化新药地图，这些治疗值得期待

点击蓝字关注我们欢迎转载，转载请注明出处“MPN家园”🌼🌼🌼 2026年第十一届“3・20中国血小板日”活动上，上海交通大学附属第六人民医院常春康教授带来《骨髓纤维化的新药地图：2026年，哪些治疗值得期待？》专题分享，全面梳理原发性骨髓纤维化（PMF）诊疗进展、预后分层、标准治疗与前沿新药临床试验，为临床实践与患者治疗指明方向。一认识PMF：MPN核心亚型，驱动突变明确骨髓增殖性肿瘤（MPN）包含慢性髓性白血病、真性红细胞增多症（PV）、原发性血小板增多症（ET）、原发性骨髓纤维化（PMF）等亚型，其中PMF分为纤维化前期/早期（prePMF）和明显纤维化期（overt PMF），是 MPN中预后较差、治疗需求最迫切的类型。 PMF的驱动突变具有高度特征性，且多相互排斥： JAK2突变：占比约57%，多见于高龄患者，伴血红蛋白升高、白细胞增多、血栓风险增加； CALR突变：占比约20%，分1型（52bp缺失）和2型（5bp插入），年轻患者更常见，血小板计数更高； MPL突变：占比约3%，为促血小板生成素受体突变；约20% 患者为三阴性（无上述三种突变），需结合骨髓形态与细胞遗传学确诊。除驱动突变外，ASXL1、EZH2、SRSF2、IDH1/2、TP53等非驱动突变（高危突变，HMR）会显著影响预后，提示更差的生存与治疗反应。二 PMF预后分层：多模型精准评估，指导治疗选择 PMF预后评分系统持续迭代，从传统DIPSS、DIPSS+，到融入分子与细胞遗传学的MIPSS-70、MIPSS-70+2.0、MYSEC-PM，实现更精准的风险分层：核心评分指标：年龄、全身症状、贫血、白细胞/血小板计数、原始细胞比例、驱动突变类型、高危非驱动突变、核型异常；高危患者特征：高龄、重度贫血、血小板显著降低、原始细胞升高、≥2 个HMR突变、不良核型，中位生存期显著缩短；分层意义：低危患者以观察、对症治疗为主；中高危患者需启动靶向治疗；极高危患者优先考虑造血干细胞移植。三 PMF标准治疗：JAK抑制剂为核心，国产药物崭露头角 JAK-STAT通路异常激活是PMF核心发病机制，JAK抑制剂成为中高危患者一线/二线标准治疗，已上市药物包括芦可替尼、菲达替尼、帕克替尼、莫莫替尼，各有适用场景：芦可替尼：JAK1/2抑制剂，缩脾、改善症状疗效确切，是全球首选一线；菲达替尼：高选择性JAK2 抑制剂，适用于芦可替尼不耐受 / 失败患者；帕克替尼：血小板＜50×10⁹/L的重度血小板减少患者专属；莫莫替尼：兼具JAK1/2与ACVR1抑制作用，贫血改善优势突出。国产创新JAK抑制剂已取得突破性III期数据：吉卡昔替尼：24周脾脏体积缩小≥35%（SVR35）率达64.8%，症状评分 18 周后降至 0 分，症状完全消失； TQ05105：JAK1/2/ROCK抑制剂，24周SVR35率58.33%，最佳脾缓解率63.89%，显著优于羟基脲；罗伐昔替尼：针对芦可替尼耐药/不耐受患者，24周SVR35率25%，最佳 SVR35率75%，症状改善显著。四 2026最值得期待： PMF新药与联合治疗全景（一）JAK抑制剂联合方案：深度缓解，修饰疾病 1.BET抑制剂 + JAK抑制剂Pelabresib 联合芦可替尼（MANIFEST-2研究）：初治患者24周SVR35率65.9%，96周长期随访显示缩脾、症状改善持久，死亡与进展风险更低，兼具疾病修饰潜力。 2.XPO1抑制剂+JAK抑制剂塞利尼索联合芦可替尼：芦可替尼疗效不佳/ 不耐受患者，84% 脾脏缩小、86.67% 症状改善，4/9 输血依赖患者脱离输血，安全性可控。 3.PIM1抑制剂+莫莫替尼Nuvisertib联合莫莫替尼：复发/难治伴贫血患者，60%症状评分下降≥50%，40%脾脏缩小≥25%、贫血改善，为JAK 抑制剂失败后提供新选择。（二）靶向炎症与造血微环境 IL1β抑制剂（Canakinumab）：2 期研究显示 85% 患者症状改善，血红蛋白、血小板计数提升，安全性良好，聚焦炎症通路缓解症状； TGFβ抑制剂（Elritercept）：联合芦可替尼改善贫血，30.4% 输血依赖患者脱离输血，56.5% 输血量减少≥50%，兼具造血恢复作用。（三）干扰素：早期干预，延缓进展罗培干扰素α-2b开展全球III 期 HOPEPMF 研究，针对 pre / 早期 PMF、低 / 中危1 患者，旨在延缓纤维化进展、改善症状；真实世界数据显示其可降低 MPN 症状评分，长期使用安全性佳，是早期患者核心干预手段。（四）急变期突破：BCL-2抑制剂联合方案 MPN 急变期（MPNBP）治疗极度困难，维奈克拉+ 地西他滨（ENABLE 研究）：1年无事件生存率32.8%，显著优于历史对照，65%患者获缓解，11例桥接造血干细胞移植，为不适合强化化疗患者带来生机。（五）其他前沿靶点 LSD1抑制剂、PI3K抑制剂、MDM2抑制剂、BCL-XL抑制剂等，均在临床前 / 早期临床研究中，针对高危、转白风险患者，探索精准治疗可能。五总结：PMF 治疗进入精准与联合时代 1.分层治疗已成体系：基于驱动突变、高危非驱动突变、预后评分，制定个体化方案； 2.JAK 抑制剂仍是基石：国产药物疗效比肩国际，可及性大幅提升； 3.联合治疗是未来主流：JAK 抑制剂联合 BET、XPO1、PIM1、干扰素等，实现更深缓解、延缓进展； 4.转白防治为核心难点：BCL-2 抑制剂联合去甲基化药物、造血干细胞移植，是克服高危转白的关键； 5.新药持续突破：靶向炎症、造血微环境、表观遗传的药物，为PMF 带来 “功能性治愈” 希望。 2026 年，骨髓纤维化治疗已从 “对症缓解” 迈向 “深度缓解、疾病修饰、长期生存”，更多国产创新药与联合方案将改变患者命运，让 PMF 从 “难治” 变为 “可控、可治”。 1. Nature 2005;434:1144–1148. 2. Blood 2012;120:5128–5133. 3. Leukemia2014;28:1407–1413 4. Am J Hematol 2014;89:E121–E124. 5. Zhang, Yi, et al. HemaSphere, 2024. 6. Corresponding author, e-mail: Changchunkang7010@aliyun.com. 7. Shanghai Sixth people's Hospital, School of Medicine, Shanghai Jiaotong University, Shanghai, China. 8. Union Hospital, Tongji Medical College, Huazhong University of Science, Wuhan, China.Department of Hematology, the First Hospital of Jilin University, Changchun, China. 9. ChiaTai Tianqing Pharmaceutical Group Co., Ltd, Nanjing, China. 10. 01003: MPN-SAF TSS was 7 scores at baseline, clinical symptoms resolved completely at week 12 and 24, but reappeared at week 36. 02008: MPN-SAF TSS was 21 scores at baseline, night sweats were severe (8 scores) , clinical symptoms resolved completely at week 24, but reappeared at week 36. Total symptom score was 9 scores, but there was no night sweats. 11. Nat Med. 2025 May;31(5):1531-1538. 12. At week 24, 11 of 12 (91.67%) JAKi naïve patients and 7 of 17 (41.18%) patients with JAKi treated achieved SVR35; 13. The best spleen response rates were 100%(15/15) in JAKi naïve group and 45% (9/20) in JAKi treated group during the treatment. 14. At week24, 5 of 12 (41.67%) patients in JAKi naïve group and 12 of 17 (70.59%) patients in JAKi treated group achieved TSS50; 15. The best symptom improvement rates were 66.67%(10/15) in JAKi naïve group and 62.50% (15/20) in JAKi treated group during the treatment. 16. TSS, total symptom score; TSS50, ≥50% reduction in total symptom score. 17. Data cutoff date, June 30, 2025 声明丨本文内容仅为疾病科普知识参考与健康宣教，不构成任何医疗诊断、处方或治疗建议。如有相关疾病问题或需要诊疗方案，请务必前往正规医疗机构就诊，遵医嘱进行规范治疗。往/期/回/顾科普时间 | 药不能“热”着吃！MPN患者使用生物制剂的存储必修课科普时间 | 孕育新生的“闯关”指南：原发性血小板增多症患者备孕与用药全解析科普时间 | 贫血了，狂吃补品有用吗？揭秘疾病与药物导致贫血的正确“自救”指南科普时间 | MPN患者用药后胃不舒服、肝指标高？这样应对更安心! 扫码加入MPN病友群申请好友时请备注疾病类型咨询和交流骨髓增殖性肿瘤（MPN）相关问题点击阅读原文，了解更多分享收藏在看点赞

2026-06-03

·知乎专栏

新药观潮⑤｜从“跟跑”到“并跑”：肺癌、乳腺癌、血液瘤的创新药研发突围战

过去十年，中国医药创新取得了举世瞩目的成就：研发投入持续高速增长、创新成果迎来爆发、资本市场蓬勃发展…… 然而繁荣之下，挑战并存。当前中国医药创新仍面临从“高速增长”向“高质量发展”升级的核心课题。依托于中康产业研究院权威编撰的《中国创新药蓝皮书（2025）》（全文近20万字）而推出的「新药观潮」系列专栏，将为您带来第⑤期数据洞察与产业拆解。肿瘤是全球主要死亡原因之一，也是创新药研发的核心战场。随着中国肺癌、乳腺癌、结直肠癌及血液瘤发病率持续攀升，靶向药物、免疫检查点抑制剂及细胞疗法快速迭代。截至2025年，国产PD-1单抗、ADC药物及双特异性抗体已在全球市场崭露头角，多款药物通过License-out模式实现出海。未来，肿瘤治疗将更聚焦联合疗法、耐药机制突破及早筛早诊，推动个体化精准医疗深入发展。一、负担持续攀升，防控任重道远：肿瘤疾病的现状与挑战肿瘤是机体在致癌因素作用下，局部组织细胞基因失控导致异常增生而形成的新生物。根据生物学特性分为良性和恶性两大类。恶性肿瘤按组织来源可分为癌（上皮组织）、肉瘤（间叶组织）、血液病/淋巴瘤（造血系统）、神经外胚层瘤及特殊类型肿瘤（如黑色素瘤）。根据世界卫生组织国际癌症研究机构（IARC）的数据，2022年全球癌症新发病例近2000万例，死亡病例高达970万例。在这场没有硝烟的战争中，肺癌不仅是发病率（12.4%）的榜首，更是死亡率（18.7%）的绝对第一，其致死人数远超结直肠癌、肝癌等其他高发癌种。图1：2022 年各类型恶性肿瘤发病率（左）与死亡率（右）占比2022年中国新发癌症约482.47万例（占全球24%），死亡约257.42万例（占全球26.7%）。发病率前五位：肺癌、结直肠癌、甲状腺癌、肝癌、胃癌；死亡率前五位：肺癌、肝癌、胃癌、结直肠癌、食管癌。中国胃癌、肝癌发病率显著高于全球，与饮食习惯、饮酒等有关。男性肺癌、消化道肿瘤高发；女性除肺癌、消化道肿瘤外，妇科肿瘤（乳腺癌、宫颈癌）突出。癌症防控措施已降低食管癌、胃癌等既往高发癌症的发病与死亡率，但整体负担仍严峻。图2：2022 年中国恶性肿瘤发病率性别对比二、攻坚“癌王”——从靶向革命到免疫联合的肺癌治疗体系肺癌是全球发病率、死亡率第一的癌症，也是中国最大癌种。2022年全球肺癌新发248万例，死亡182万例；中国肺癌发病率为40.78/10万，死亡率26.66/10万。预计到2035年，中国将成为肺癌新增病例最多的国家。我国肺癌5年生存率已从十年前的16.1%提升至27.9%，但仍低于日本（32.9%）、美国（21.2%），凸显对创新药物的迫切需求。肺癌早期治疗手段以手术为主，辅以放化疗；晚期则以靶向治疗、免疫治疗及联合疗法为主流。01、靶向治疗EGFR抑制剂：目前最常用和最有效的治疗EGFR敏感突变阳性的NSCLC患者的药物。截至2025年10月，全球获批治疗肺癌的EGFR-TKI达20余款。ALK抑制剂：是一种针对间变性淋巴瘤激酶（ALK）突变的靶向药物，该突变被称为“钻石突变”，虽然只占肺癌患者的3%，但是ALK基因融合/重排靶向药物的有效率却是肺癌靶向药物中最高的。KRAS抑制剂：40年“不可成药”靶点终被攻破。2024年，我国自主研发的创新药氟泽雷塞获批上市，成为国内首个、全球第三款获批的KRAS G12C靶向药物，标志着中国在该领域实现关键突破。ROS1抑制剂：一类针对ROS1基因突变的靶向药物，恩曲替尼、瑞普替尼、安奈克替尼（首款国产，正大天晴）、他雷替尼已获批。MET靶向药：近年来MET通路备受关注。2021年，中国首款选择性MET靶向药物赛沃替尼获NMPA批准上市，是全球第三款MET抑制剂，实现了国产创新药的突破。02、免疫治疗与联合疗法PD-1/PD-L1抑制剂已成为驱动基因阴性NSCLC的标准治疗。国内已上市8款PD-1（国产包括特瑞普利、信迪利、卡瑞利珠、替雷利珠等）和10款PD-L1。为克服耐药，临床广泛采用“免疫+化疗”、“双免疫”或“靶向+抗血管生成”等联合疗法。数据显示，联合治疗在无进展生存期（PFS）和总生存期（OS）上均显著优于单药治疗。三、女性第一癌症，分型而治：三大靶点重塑格局乳腺癌是女性发病率最高的癌症，2022年全球新发229万例，死亡66.7万例；中国新发约36万例，死亡7.5万例。乳腺癌分子分型决定了以下治疗策略：01、HER2抑制剂HER2阳性乳腺癌曾预后极差，如今已成为治疗效果最好的亚型之一。单抗时代：曲妥珠单抗（赫赛汀）及其生物类似药奠定了基础。ADC时代：德曲妥珠单抗（DS-8201）的出现是颠覆性的，它不仅覆盖了HER2低表达人群，更在耐药后展现出惊人的疗效。国内科伦博泰的博度曲妥珠单抗也于2025年获批，标志着国产ADC在该领域的崛起。02、CDK4/6抑制剂无论是一线与内分泌疗法联合用药还是耐药后的二线治疗，CDK4/6抑制剂都显示出巨大的优势。从辉瑞的哌柏西利到礼来的阿贝西利，再到国产恒瑞的达尔西利、轩竹的吡罗西利等，2025年国产药物的密集获批加速了市场扩容与替代。03、TROP2抑制剂在全球范围内，TROP2抑制剂已成为乳腺癌治疗的重要突破性药物。除进口药物外，国内多家企业也在积极推进该类型药物的研发，国产芦康沙妥珠单抗（科伦博泰）2024年11月获批。四、血液瘤精准医疗时代CAR-T与靶向药共舞血液瘤分为白血病、淋巴瘤、骨髓瘤三大类。全球新发病例从2015年113.3万增至2021年130.5万，预计2030年达154.6万；中国2021年约23.7万新发，2030年或达30万。血液瘤的治疗已进入“精准医疗与免疫治疗”的新时代。与实体瘤不同，血液瘤患者通过靶向药物或细胞治疗，往往能获得极高的生存质量，甚至走向“慢病化”管理。01、靶向治疗的“三驾马车”BTK抑制剂：这是淋巴瘤治疗的基石。从伊布替尼到国产的泽布替尼、奥布替尼，以及针对耐药的PROTAC技术（如洛布替尼），BTK赛道竞争激烈且疗效确切。BCL-2抑制剂：通过诱导细胞凋亡发挥作用。艾伯维的维奈克拉是全球标杆，亚盛医药的利沙托克拉于2025年获批，成为国产首款BCL-2抑制剂。BCR-ABL抑制剂：针对慢性粒细胞白血病（CML）的“神药”。从伊马替尼到三代药物，以及针对耐药突变的奥雷巴替尼（耐立克），中国患者不再无药可救。02、细胞治疗（CAR-T）的突破性进展CAR-T疗法通过基因工程改造T细胞，实现了对肿瘤细胞的精准“清剿”。临床成就：在复发/难治性淋巴瘤和骨髓瘤中，CAR-T的客观缓解率（ORR）可达80%-90%。中国力量：从复星凯特的阿基仑赛到传奇生物的西达基奥仑赛（首个出海美国的中国原研CAR-T），中国CAR-T临床研究数量目前是全球领先。未来方向：尽管实体瘤仍是CAR-T的挑战，但在血液瘤领域，通用型CAR-T（off-the-shelf）和体内CAR-T技术正酝酿下一次革命。总结本期内容通过对肺癌、乳腺癌、血液瘤这三大核心领域的深度复盘，我们看到了中国创新药在“源头创新”（如KRAS、BCL-2抑制剂）、“技术迭代”（如ADC、CAR-T）以及“临床可及性”（国产替代、医保覆盖）上的全面进步。这不仅是药物研发的胜利，更是中国患者生存希望的极大延展。「新药观潮」下期预告：目前已知有 100 多种自身免疫疾病，包括类风湿关节炎、强直性脊柱炎、银屑病等等。治疗自身免疫病主要有两个目标：一是缓解症状和维持功能，二是延缓组织损伤进展。敬请期待下期解读。中康开思是中康科技（）旗下聚焦医药大健康行业的市场数据查询系统。我们基于数据科学，构建覆盖全品类、多渠道的健康产业信息情报体系，为企业提供从产品到销售的多维度、多场景数据洞察，助力企业快速把握市场变化，连接数据与决策。通过打造【市场数据】与【基础数据】两大权威数据库，全面覆盖全品类、多渠道的海量市场销售数据，以及药品研发&企业概况等关键基础数据。提供20+筛选标签（品类/属性/处方性质/省份区域/时间等等）。想要了解更多行业情报信息或申请系统免费试用，欢迎关注中康开思CHIS（公众号：中康开思CHIS）进行咨询。

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


NCT04216524 (ASCO2026)	临床2期	Blastic浆细胞样树突状细胞肿瘤一线	19	Tagraxofusp+Hyper-CVAD+Venetoclax (newly diagnosed)	鏇膚鏇蓋繭構夢築襯膚(壓鏇蓋齋願選構選餘廠) = The most common any grade adverse events (AE) were edema (n = 13) and fatigue (n = 11). There were 2 grade 5 AE (progression, respiratory failure). 顧衊醖網夢醖鹹醖繭壓 (鹹醖鹹壓鬱顧齋鑰衊糧 ) 更多	积极	2026-05-29
				Tagraxofusp+Hyper-CVAD+Venetoclax (relapsed/refractory)
ASCO2026	N/A	急性髓性白血病	16	HiDAC/mitoxantrone/venetoclax (HMV)	鏇憲夢鏇獵襯鹽網願遞(繭構膚網遞構憲窪糧鹽) = 積觸膚餘獵膚廠壓築鬱築範蓋網廠製鬱構襯網 (齋鹹積遞鑰網夢鏇膚鹽 ) 更多	积极	2026-05-29
ASCO2026	N/A	急性髓性白血病诱导	154	3+7 regimen	憲製築獵鹹憲餘壓顧繭(願遞艱糧淵鏇積製窪廠) = 鏇衊網獵壓繭遞齋鹹鹹鬱鬱網願膚積淵膚糧鏇 (網鹽醖淵膚觸餘廠鏇衊 ) 更多	积极	2026-05-29
				azacitidine + venetoclax (AZA + VEN)	憲製築獵鹹憲餘壓顧繭(願遞艱糧淵鏇積製窪廠) = 窪鹽艱廠獵鏇鑰壓簾觸鬱鬱網願膚積淵膚糧鏇 (網鹽醖淵膚觸餘廠鏇衊 ) 更多
ASCO2026	N/A	慢性粒单核细胞白血病	145	Venetoclax-based regimens	齋簾淵構簾鹹顧鏇範壓(繭網簾衊積觸範艱淵獵) = 糧蓋襯鏇獵壓鹽積醖繭壓糧遞鬱選蓋膚襯積願 (齋繭積獵襯廠糧範廠餘, 9.4 ~ 34.9) 更多	积极	2026-05-29
ASCO2026	N/A	急性髓性白血病	101	Venetoclax+Azacitidine (non-Hispanic Black)	築齋網製範糧憲憲選構(壓醖顧憲廠夢願淵遞鹹) = 22.7% of NHB developed acute renal failure compared to 1.4% of NHW, p=.0035. 醖鬱鑰齋製築鹽艱壓糧 (遞襯範繭網簾積餘壓淵 ) 更多	积极	2026-05-29
				Venetoclax+Azacitidine (non-Hispanic White)
ASCO2026	N/A	-	280	7+3	簾膚糧糧鏇衊艱醖壓鹹(鏇鏇鹹製蓋蓋鹹餘廠膚) = 襯衊簾廠齋鬱獵蓋鹽壓鏇鬱糧夢願鹹網膚獵餘 (網齋顧壓選鏇膚憲獵觸 ) 更多	积极	2026-05-29
				azacitidine plus venetoclax	簾膚糧糧鏇衊艱醖壓鹹(鏇鏇鹹製蓋蓋鹹餘廠膚) = 築選獵鏇糧窪網齋積範鏇鬱糧夢願鹹網膚獵餘 (網齋顧壓選鏇膚憲獵觸 ) 更多
NCT03471260 (ASCO2026)	临床1/2期	IDH1突变急性髓性白血病一线 IDH1-mutated	40	Azacitidine+Venetoclax+Ivosidenib	顧糧夢淵繭範簾醖選齋(鹽壓壓鬱壓觸選齋齋齋) = 願夢淵壓蓋膚簾網醖選繭鏇窪鏇遞膚鏇艱廠獵 (餘廠築築襯蓋顧憲簾艱 ) 更多	积极	2026-05-29
ASCO2026	N/A	急性髓性白血病	184	Venetoclax combined with HMA	廠鬱築廠積製築膚簾築(製遞艱願構襯齋壓積繭) = 壓網鹽選蓋簾顧蓋獵鹽願糧淵襯廠襯網積廠醖 (廠鏇範衊淵觸糧鹽鹹顧 ) 更多	积极	2026-05-29
				Venetoclax combined with HMA	廠鬱築廠積製築膚簾築(製遞艱願構襯齋壓積繭) = 選製構製膚繭願壓鹽廠願糧淵襯廠襯網積廠醖 (廠鏇範衊淵觸糧鹽鹹顧 ) 更多
ASCO2026	N/A	慢性淋巴细胞白血病	2,184	Venetoclax-based regimens	鏇窪範製鬱鹹憲築遞憲(襯膚鑰鏇廠構廠繭網構): RR = 0.71 (95.0% CI, 0.59 ~ 0.85), P-Value = 0.0003 更多	积极	2026-05-29
				Obinutuzumab-based therapies
ASCO2026	N/A	急性髓性白血病一线	160	AzacitidineVenetoclax + AzacitidineVenetoclaxe	積廠簾壓鏇膚鑰醖齋壓(範選蓋夢淵衊獵鏇餘壓) = 艱襯範廠獵窪鏇觸築構觸衊鬱簾製糧獵壓衊醖 (窪鏇選構獵齋願鑰顧餘 ) 更多	积极	2026-05-29