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]

NCT07437950

/ Not yet recruiting临床2期IIT

A Randomized Phase II Trial of ASTX727 With Standard Duration Versus Shorter Duration of Venetoclax in Genomically Heterogenous AML Among Adults Aged 60 or Older and Less Fit for Intensive Therapy: A MyeloMATCH Substudy

This phase II MyeloMATCH treatment trial compares ASTX727 with standard duration versus shorter duration of venetoclax for the treatment of newly diagnosed acute myeloid leukemia (AML). ASTX727 is a combination of decitabine and cedazuridine. 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. 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. 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. Shorter duration venetoclax may be as effective as standard duration venetoclax when given with ASTX727 for the treatment of newly diagnosed AML.

开始日期2026-10-14

申办/合作机构

National Cancer Institute

NCT07175415

/ Not yet recruiting临床1/2期IIT

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]

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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4,791

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.

2026-06-01·BIOORGANIC & MEDICINAL CHEMISTRY LETTERS

Discovery of novel sophocarpine derivatives as potential dual Bcl-2 and Mcl-1 inhibitors: design, synthesis and anti-hepatocellular carcinoma evaluation

Article

作者: Wei, YongQuan ; Jiang, Meiyan ; Wang, Lisheng ; Sun, Die

Hepatocellular carcinoma (HCC) remains one of the leading causes of cancer-related mortality and disease burden worldwide, and its clinical management continues to face substantial challenges. Sorafenib, a widely used systemic therapy for advanced HCC, frequently develops acquired resistance upon long-term treatment, in part due to the overexpression of anti-apoptotic Bcl-2 family proteins. Herein, guided by the structural features of Sorafenib, the selective Bcl-2 inhibitor Venetoclax, and the selective Mcl-1 inhibitor AZD5991, we designed and synthesized a series of novel Sophocarpine-derived analogues bearing a pyridylethyl moiety via a molecular-hybridization strategy. Molecular docking suggested a favorable binding mode, in which the resulting scaffold could occupy the hydrophobic binding pockets of both Bcl-2 and Mcl-1 and engage key residues through hydrogen-bond interactions. In vitro antiproliferative screening (MTT assay) against three human HCC cell lines (Huh-7, MHCC-97H, and HepG2) showed that most compounds exhibited moderate to good activity. Notably, compound S6 emerged as the most potent analogue, with IC₅₀ values of 9.13 ± 0.29 μM (Huh-7), 6.76 ± 0.06 μM (MHCC-97H), and 15.9 ± 0.98 μM (HepG2). Mechanistic studies demonstrated that S6 markedly suppressed proliferation and migration of MHCC-97H cells, induced G1-phase arrest, and promoted apoptosis. Western blot analysis revealed that S6 downregulated anti-apoptotic proteins Bcl-2 and Mcl-1, induced mitochondrial membrane potential (ΔΨm) depolarization, and activated the caspase-dependent apoptotic cascade, as evidenced by caspase-3 activation and PARP1 cleavage. In parallel, a 3D-QSAR (CoMFA) model was constructed to rationalize the structure-activity relationship and to inform further lead optimization. Collectively, these findings identify S6 as a promising Sophocarpine derivative with a putative dual Bcl-2/Mcl-1 targeting profile, with significant anti-HCC activity and potential for preclinical development.

2026-05-01·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Systematic review of real-world data on the effectiveness and safety profiles of first-line therapies in chronic lymphocytic leukemia

Review

作者: Stożek-Tutro, Anita ; Małowicka, Monika ; Kawalec, Paweł ; Janiszewska, Klaudia

OBJECTIVE:

To assess the real-world effectiveness of first-line targeted therapies (1LTT) for chronic lymphocytic leukemia (CLL) and compare these outcomes with those reported in randomized controlled trials (RCT).

METHODS:

A systematic review of MEDLINE and EMBASE was conducted to identify real-world data (RWD). Key endpoints included progression-free survival (PFS), overall survival (OS), time-to-next treatment (TTNT), and treatment discontinuation due to adverse events (TdAE). CRD42024549185.

RESULTS:

Ibrutinib (IBR) demonstrated consistent effectiveness in multiple RWD studies, with 12- and 24-month OS rates of 87-100% and 78-100%, respectively, and PFS rates of 76-94% and 68-94%, respectively, aligning with the results of the RESONATE-2 trial. Zanubrutinib (ZAN) showed a 36-month OS rate of 92% and a PFS rate of 84%, consistent with the outcomes of the SEQUOIA trial. For acalabrutinib (ACA), 12- and 24-month OS was 86-94% and 76-88%, PFS 92% and 81%, respectively, in line with the ELEVATE-TN trial, similarly, for venetoclax+obinutuzumab (VEN+OBI), 12-and 24-month OS was 94% and 86-94%, PFS 94% and 88%-92%, consistent with the CLL14 trial results. In contrast, idelalisib+rituximab (IDE+RTX) was associated with lower 24-month OS (77%), PFS (68%), and the highest TdAE rate (63%).

CONCLUSIONS:

Among 1LTT for CLL, IBR has the most extensive and consistent RWD, with results mirroring RCT outcomes. ZAN, ACA and VEN+OBI show promising results based on RWD, however, these data are less extensive but consistent with RCT outcomes. Findings highlight the value of RWD and the need for more robust data on newer agents.

2,255

项与维奈克拉相关的新闻（医药）

2026-03-27

·PRNewswire

Scalable Biotech Manufacturing Unlocks a $14B Market

Issued on behalf of Avaí Bio, Inc. VANCOUVER, BC, March 27, 2026 /PRNewswire/ -- USANewsGroup.com News Commentary — The global cell therapy manufacturing market is hitting a pivotal inflection point. It's projected to surpass $7 billion in 2026 and reach $14 billion by 2035[1], driven by over 1,000 active clinical candidates globally. To keep up with this massive demand, the FDA just stepped in with new flexibility measures for cell and gene therapies[2]. By easing manufacturing requirements from the lab to commercial launch, regulators are accelerating the timeline for life-saving product approvals. This historic shift toward scalable bioproduction infrastructure is creating deep, sustainable value across a new class of durable therapy developers, including Avaí Bio (OTCQB: AVAI), ImmunityBio (NASDAQ: IBRX), Fate Therapeutics (NASDAQ: FATE), Fractyl Health (NASDAQ: GUTS), and Moleculin Biotech (NASDAQ: MBRX). Wall Street and industry analysts have already identified tight biologics capacity and constrained operations[3] as the defining bottlenecks of the 2026 manufacturing landscape. Production capability is no longer just a background detail; it is a highly coveted strategic asset. Regulators are actively responding to this supply crunch by loosening strict process validation rules and allowing concurrent lot releases[4] for qualified programs. Because of this, scalable GMP foundations have quickly become the primary value driver for companies looking to dominate the next wave of clinical manufacturing. Avaí Bio (OTCQB: AVAI) and joint venture partner Austrianova have begun manufacturing a Master Cell Bank (MCB) of genetically modified cells engineered to produce high levels of the α-Klotho protein, a naturally occurring molecule that researchers have linked to slower aging and lower rates of diseases like Alzheimer's and certain cancers. Peer-reviewed studies have shown that higher circulating Klotho levels correlate with reduced risk of neurodegenerative disease, drawing growing scientific interest to the protein's therapeutic potential. Think of the MCB as a permanent, lab-grade seed vault from which the company will create a Working Cell Bank, while storing the MCB cells for many years to come. Every vial—filled with millions of cloned cells inside—traces back to a single verified cell, manufactured under strict Good Manufacturing Practice (GMP) standards. That matters because when a company eventually scales up production, it needs a clean, consistent starting point. Without one, batches can drift, contamination risk climbs, and regulators start asking hard questions. With a qualified MCB in place, Avaí and Austrianova now have that foundation locked in. "MCBs are a prerequisite for the production of Cell-in-a-Box® encapsulated cell products," said Prof. Walter H. Gunzburg, Chairman of Austrianova. "They provide the foundation for sustainable production and ensure they meet the highest quality standards." The cells, which will make up a smaller Working Cell Bank, will be used for all of the company's research and clinical trials, and feed directly into Austrianova's proprietary Cell-in-a-Box® encapsulation platform, which packages living cells inside a pin-head-sized, sphere-shaped protective capsule so they can be implanted inside the body and continue producing a target protein over time. The end goal is a cell-based therapy that restores circulating Klotho levels in patients, potentially offering durable protection against age-related decline without requiring repeated dosing. "We are excited to enter the first step in the production phase of α-Klotho producing cells as part of our commitment to deliver safe, effective treatments for aging associated diseases," said Chris Winter, CEO of Avaí Bio. The work is being advanced through Klothonova, a Nevada-based joint venture formed last September and owned equally by both companies. Klothonova sits alongside Insulinova, a separate diabetes-focused program, as one of two active pipelines in Avaí's portfolio. Both programs employ Austrianova's encapsulation technology. Avaí Bio recently completed a full rebrand and pivot into biotechnology, formerly operating as Avant Technologies. The company now concentrates on sourcing, developing, and protecting advanced cellular therapies through strategic joint ventures and licensing agreements. All preparatory activities for the MCB were completed in February, allowing the partners to move directly into the production phase without delay. CONTINUED… Read this and more news for Avaí Bio at: In other industry developments: ImmunityBio (NASDAQ: IBRX) has validated a scalable manufacturing pathway for its autologous memory cytokine-enhanced natural killer cell platform, enrolling 74 subjects across its NK2022 and NK2023 programs and completing a Phase 1 safety trial combining M-ceNK cells with ANKTIVA® with zero Grade 4 or 5 treatment-related adverse events and zero cytokine storm events across 10 treated cancer patients. A single apheresis collection now yields up to 5 billion highly pure M-ceNK cells, providing 8-10 therapeutic doses with finished product available within 12 days. "These data demonstrate that potent NK cell therapy can be manufactured at scale and administered safely, potentially offering a reliable autologous source of potent NK cells," said Patrick Soon-Shiong, MD, Founder, Executive Chairman and Global Chief Scientific and Medical Officer of ImmunityBio. "The ability to generate up to 5 billion highly pure NK cells from a single apheresis collection, yielding up to 8-10 therapeutic doses within 12 days, opens the possibility of creating the 'World Bank of Natural Killer Cells', with NK cells able to be universally donated to any patient without HLA matching." With manufacturing methods now established for AI-driven robotic systems under the NANT Leonardo platform, ImmunityBio is positioned to translate its cell banking infrastructure into first-in-human clinical programs at scale. NCI-presented preclinical data from AACR IO 2026 also showed M-ceNK cells combined with ANKTIVA® produced statistically significant tumor volume reductions in two SCLC xenograft models. Fate Therapeutics (NASDAQ: FATE) has achieved a landmark clinical milestone by successfully treating autoimmune patients with its FT819 off-the-shelf CAR T-cell therapy in an outpatient setting, eliminating the extended hospitalization requirements that have restricted patient access to CAR T therapies. Enrollment in the FT819-102 Phase 1 basket trial now spans 16 sites across the U.S., U.K., and EU, with 15 systemic lupus erythematosus patients and four systemic sclerosis patients treated to date, including early evidence of meaningful disease improvement in the first SSc patient reaching a 3-month evaluation. "I am extremely proud of the progress the Fate team delivered in 2025, including bringing to fruition the treatment of FT819 off-the-shelf CAR T cells as outpatient therapy, eliminating the need for extended hospital stay requirements seen today with other CAR T-cell programs, which now uniquely expands autoimmune patient access, including in underserved regions, while significantly improving health system economics," said Bob Valamehr, M.B.A., Ph.D., President and CEO of Fate Therapeutics. "We have a well-capitalized balance sheet ensuring runway through 2027 and believe we are uniquely positioned to drive long-term value creation." Fate Therapeutics closed 2025 with $205.1 million in cash and investments, supporting an operating runway through year-end 2027, underpinned by a 30% reduction in operating expenses versus 2024. The company's next-generation FT836 program also reported early clinical activity in colorectal cancer, including a greater than 50% reduction in CEA levels and tumor reduction across all target lesions, without the use of conditioning chemotherapy. Fractyl Health (NASDAQ: GUTS) has completed randomization in the REMAIN-1 Pivotal Cohort evaluating its Revita® duodenal ablation procedure for post-GLP-1 weight maintenance, with topline 6-month data expected in early Q4 2026 and a potential FDA De Novo marketing application submission targeted for late Q4 2026. New post-hoc analyses from the REMAIN-1 Midpoint Cohort show a statistically significant dose-dependent treatment effect, with participants receiving above-median GLP-1 weight loss retaining 88% of that weight loss at six months versus only 60% in sham participants. "Completion of randomization in the REMAIN-1 Midpoint and Pivotal Cohorts marks a critical execution milestone, and today's new analyses from the Midpoint Cohort 6-month data gives us even greater anticipation for what the pivotal study might show," said Harith Rajagopalan, M.D., Ph.D., Co-Founder and CEO of Fractyl Health. "Approximately 30 million patients are projected to be on GLP-1s by 2035. The majority will face discontinuation and significant weight regain. Fractyl stands alone developing the first potential procedural option for post-GLP-1 weight maintenance with pivotal data expected this year." With cash of approximately $81.5 million as of December 31, 2025, supplemented by $4.1 million in subsequent warrant proceeds, Fractyl Health maintains a runway into early 2027, extending beyond the anticipated pivotal data readout. The company's Rejuva® gene therapy platform is also advancing, with first-in-human dosing of RJVA-001 for type 2 diabetes expected in H2 2026, subject to regulatory authorization. Moleculin Biotech (NASDAQ: MBRX) has enrolled its 45th subject in the pivotal Phase 2B/3 MIRACLE trial evaluating Annamycin in combination with cytarabine for relapsed or refractory acute myeloid leukemia, triggering the protocol-specified interim data unblinding now anticipated for mid-2026. Early blinded composite data from the first 30 patients showed a 40% complete remission rate, including patients who had previously failed venetoclax-based regimens and carried adverse genetic markers, comparing favorably to historical outcomes with cytarabine alone. "We believe this upcoming data readout represents the most important milestone in our history to date," said Walter Klemp, Chairman and CEO of Moleculin. "Reaching the 45 subject mark brings us to the threshold of our first meaningful look at MIRACLE data. Our Phase 2 AML MB-106 clinical trial generated greater efficacy than any drug ever approved for relapsed or refractory AML, and it contributed to the more than 100 patients treated to date without any associated cardiotoxicity." Enrollment continues in parallel as Moleculin Biotech advances toward 90 total subjects, expected to conclude Part A of MIRACLE in Q3 2026, with a second unblinding and Phase 3 dose optimization to follow. The program is designed to support an accelerated approval pathway based on the complete remission primary endpoint, with the adaptive trial structure integrating Phase 2B data directly into the planned Phase 3 registration. Continued Reading: CONTACT: USA NEWS GROUP [email protected] (604) 265-2873 DISCLAIMER: Nothing in this publication should be considered as personalized financial advice. We are not licensed under securities laws to address your particular financial situation. No communication by our employees to you should be deemed as personalized financial advice. Please consult a licensed financial advisor before making any investment decision. This is a paid advertisement and is neither an offer nor recommendation to buy or sell any security. We hold no investment licenses and are thus neither licensed nor qualified to provide investment advice. The content in this report or email is not provided to any individual with a view toward their individual circumstances. USA News Group is a wholly-owned subsidiary of Market IQ Media Group, Inc. ("MIQ"). MIQ has been paid a fee for Avaí Bio, Inc. advertising and digital media from the company directly. There may be 3rd parties who may have shares of Avaí Bio, Inc., and may liquidate their shares which could have a negative effect on the price of the stock. This compensation constitutes a conflict of interest as to our ability to remain objective in our communication regarding the profiled company. Because of this conflict, individuals are strongly encouraged to not use this publication as the basis for any investment decision. The owner/operator of MIQ own shares of Avaí Bio, Inc. which were purchased in the open market. MIQ reserves the right to buy and sell, and will buy and sell shares of Avaí Bio, Inc. at any time thereafter without any further notice. We also expect further compensation as an ongoing digital media effort to increase visibility for the company, no further notice will be given, but let this disclaimer serve as notice that all material disseminated by MIQ has been approved by the above mentioned company; this is a paid advertisement, and we own shares of the mentioned company that we will sell, and we also reserve the right to buy shares of the company in the open market, or through other investment vehicles. While all information is believed to be reliable, it is not guaranteed by us to be accurate. Individuals should assume that all information contained in our newsletter is not trustworthy unless verified by their own independent research. Also, because events and circumstances frequently do not occur as expected, there will likely be differences between any predictions and actual results. Always consult a licensed investment professional before making any investment decision. Be extremely careful, investing in securities carries a high degree of risk; you may likely lose some or all of the investment. SOURCES: ? utm_source=GNE&utm_medium=PressRelease&utm_code=s67rx7&utm_campaign=2182410+-+%2414%2b+Bn+Cell+Therapy+Manufacturing+Market+Trends+and+Forecasts%2c+2035+-+Researchers+are+Exploring+Over+1%2c000+Cell+and+Gene+Therapy+Candidates+Targeting+a+Wide+Range+of+Disease+Indications&utm_exec=chdomspi Logo: 21% more press release views with Request a Demo

临床结果细胞疗法临床2期临床1期

2026-03-27

·维科号

深度解析Ⅱ型抗CD20单抗奥滨尤妥珠单抗的进化之路：从糖基化改造到颠覆肿瘤与自身免疫疾病治疗格局

单克隆抗体技术深刻改变了肿瘤与自身免疫疾病的治疗。其中，CD20抗原作为B细胞的经典标志物，是最具代表性的靶点之一。二十多年前，第一代Ⅰ型抗CD20单抗利妥昔单抗（Rituximab）彻底改变了淋巴瘤和白血病患者的生存轨迹。然而，随着临床应用的深入，其局限性也逐渐暴露：耐药复发频繁、深层组织穿透力不足，且对低表达CD20肿瘤细胞的杀伤力有限。为打破这一僵局，科学界对底层机制进行了重构。奥滨尤妥珠单抗（Obinutuzumab，商品名为GAZYVA®/GAZYVARO®）作为全球首个经糖基化改造的Ⅱ型抗CD20人源化单抗应运而生。它并非简单的升级版，而是在空间构象、效应细胞招募及细胞死亡触发路径上，展现出了截然不同的精确杀伤力。一、从瑞士实验室的分子创想到百亿重磅药物的诞生任何一款划时代的药物，其背后都隐藏着一段充满未知、挑战与坚持的探索史。奥滨尤妥珠单抗的故事，始于对单克隆抗体天然缺陷的深刻反思。 1.1 突破天然免疫瓶颈：“糖基化工程”的觉醒与GlycArt的创立千禧年初，科学家们面临如何提升单抗天然免疫杀伤效率的难题。瑞士苏黎世联邦理工学院（ETH）的著名生化工程先驱James E. Bailey教授指导的年轻学者Pablo Umaña和Joël Jean-Mairet等人敏锐地发现，抗体Fc段上的岩藻糖会在空间上严重削弱抗体与免疫效应细胞表面受体FcγRIIIa的结合亲和力。为了跨越这一障碍，Umaña与其团队在2000年参加了McKinsey/ETH商业计划大赛，尽管未能夺冠，但他们凭借对“抗体去岩藻糖基化”概念的深刻阐述，成功吸引了300万瑞士法郎的种子资金，并于2001年正式创立了衍生公司GlycArt Biotechnology AG。在随后的几年里，他们首创了名为“GlycoMAb”的核心技术。该技术通过基因工程手段，向生产抗体的中国仓鼠卵巢细胞（CHO）宿主中转入两种编码寡糖修饰酶的基因——β-1,4-N-乙酰葡萄糖胺转移酶Ⅲ（GnT Ⅲ）和高尔基体α-甘露糖苷酶Ⅱ（Man Ⅱ）。这一极具创造力的基因重组过程，使得细胞系能够稳定生产出“去岩藻糖基化”的抗体变体，为后续的药物研发奠定了坚实的基础。 1.2 罗氏的战略并购与B-Ly1的“铰链区重塑” 2005年，罗氏全资收购了GlycArt，直接催生了罗氏苏黎世创新中心的建立。在选择抗体骨架时，研究团队相中了一种源于小鼠IgG1的Ⅱ型亲本抗体B-Ly1。通过被业界称为“铰链工程”的精密操作，研究人员将Kabat 11位的亮氨酸精准突变为缬氨酸，使得奥滨尤妥珠单抗的铰链角比利妥昔单抗拓宽了30度。这一微小突变彻底改变了结合构象，赋予了其前所未有的杀伤潜能。二、降维打击：Ⅱ型抗CD20单抗的深层生物学机制重塑要深刻理解奥滨尤妥珠单抗在临床试验中展现出的压倒性优势，我们必须褪去临床数据的外衣，深入到纳米级别的分子战场。Ⅰ型（如利妥昔单抗、奥法木单抗）与Ⅱ型（如奥滨尤妥珠单抗）抗体在分子机制上的分野，是一场杀伤路径的战略性重构。 2.1 空间结合艺术：“蟹钳效应”与抗原内化的规避尽管奥滨尤妥珠单抗与利妥昔单抗结合的CD20表位高度重叠，但其在细胞表面的空间取向却截然不同。结构生物学和晶体学研究表明，当奥滨尤妥珠单抗结合到CD20上时，其Fab段比利妥昔单抗旋转了90度，并向CD20表位的C端倾斜了70度。更具决定性意义的是其“抓取”抗原的方式。Ⅰ型抗体倾向于在相邻的两个CD20四聚体之间建立“桥接”，这种交联作用会促使CD20复合物在B细胞膜上的富胆固醇区域——脂筏中发生大规模聚集。而奥滨尤妥珠单抗凭借其更宽的铰链角，其两个Fab臂能够像“蟹钳”一样，紧紧钳住同一个CD20四聚体内的两个不同表位。这种“蟹钳式”的内部钳合直接阻止了CD20抗原向脂筏的转位。不进入脂筏带来了两个巨大的生物学红利：第一，它极大程度地避免了抗原的内化和“剃须现象”。在利妥昔单抗治疗中，靶细胞往往会通过吞噬受体将抗原-抗体复合物吞入细胞内降解，导致肿瘤细胞表面失去靶点，从而产生耐药性；而奥滨尤妥珠单抗由于不引发抗原内化，能够长时间稳定地锚定在靶细胞表面，为后续持续招募免疫细胞赢得了充足的“战术窗口”。抗CD20单克隆抗体的药效学特征。 (A) I型，非Fc优化单克隆抗体。(B) I型，Fc优化单克隆抗体。(C) II型，非Fc优化单克隆抗体。(D) II型，Fc优化单克隆抗体。（doi：10.1182/blood-2017-03-771832） 2.2 杀伤机制的三重变奏：ADCC、直接死亡与CDC的极端取舍抗CD20抗体摧毁恶性B细胞依赖三大机制，奥滨尤妥珠单抗在此进行了极端的取舍： •战略性放弃：弱化补体激活（CDC）由于奥滨尤妥珠单抗不诱导CD20在脂筏中聚集，它无法像利妥昔单抗那样促使Fc段形成六聚体，因此极大地削弱了固定经典补体途径起始成分C1q的能力。表面上看，丧失CDC效应似乎削弱了抗体的杀伤力，但实际上，这是一种深谋远虑的机制取舍。大量的免疫学研究证实，过度的补体激活往往会消耗效应细胞的活性，甚至血清中的补体成分会物理性地干扰NK细胞的活化和与靶细胞的接触。奥滨尤妥珠单抗通过放弃CDC，排除了补体系统对NK细胞的干扰，为其主力武器的发挥扫清了障碍。 •极致的借刀杀人：百倍增强的ADCC与ADCP效应去岩藻糖基化的GlycoMAb技术，赋予了奥滨尤妥珠单抗对抗体FcγRIIIa受体极度强烈的亲和力。在人体的免疫系统中，由于基因多态性，相当一部分人群的FcγRIIIa受体呈现低亲和力表型（如158F/F或158V/F基因型），这类患者对传统利妥昔单抗的反应往往较差。然而，糖基化改造彻底打破了这一基因壁垒。生化结合实验表明，奥滨尤妥珠单抗与低亲和性FcγRIIIa的结合亲和力（KD值约为55nmol/L），甚至超越了利妥昔单抗与高亲和性受体的结合力（KD值为660nmol/L）。这一数量级的跃升，使得它在体外实验中激发的ADCC效应达到了利妥昔单抗的35至100倍。这意味着，哪怕肿瘤细胞表面的CD20表达量极低，奥滨尤妥珠单抗也能像强力磁铁一样，将NK细胞和巨噬细胞牢牢吸附过来，对恶性B细胞执行“凌迟”般的细胞毒性打击和吞噬清除。 •细胞内的崩溃：独特的非凋亡性直接死亡诱导除了招募外援，奥滨尤妥珠单抗自带强大的“单兵作战”能力。当它与CD20发生同型聚集时，能够不依赖任何免疫细胞，直接在B细胞内部触发死亡信号。与利妥昔单抗诱导的传统Caspase依赖性凋亡不同，奥滨尤妥珠单抗引发的是一种强烈的、依赖肌动蛋白重构的非典型溶酶体细胞死亡途径。更令人瞩目的是，近期针对细胞内信号通路的研究揭示，利妥昔单抗在结合CD20后，会通过激活AKT途径过度磷酸化促凋亡蛋白BAD（如Ser118位点），这种磷酸化反而会将BAD隔离在细胞质中，使其失去抑制抗凋亡蛋白BCL2的能力，从而变相发出了“促生存”信号。相比之下，奥滨尤妥珠单抗不仅不引发这种自我保护的抗凋亡信号，反而通过异常的SYK磷酸化强烈支持细胞凋亡的诱导。此外，奥滨尤妥珠单抗诱导的死亡具有强烈的免疫原性，能够促使肿瘤细胞释放热休克蛋白90等损伤相关模式分子（DAMPs），从而唤醒宿主体内原本休眠的T细胞，形成长效的抗肿瘤免疫记忆。三、临床博弈（上）：在惰性淋巴瘤与白血病中的王者之战奥滨尤妥珠单抗在临床前模型中展现出的摧枯拉朽般的优势，促使罗氏在全球范围内启动了庞大而严密的临床开发计划。其核心策略极具攻击性：直接在利妥昔单抗长期统治的优势适应证中进行“头对头”对决，用无可辩驳的数据重塑全球标准治疗方案。 3.1 慢性淋巴细胞白血病（CLL）：突破并发症人群的生存极限慢性淋巴细胞白血病（CLL）是西方世界最常见的成人白血病，它是一种主要影响老年人的惰性B细胞恶性肿瘤。许多患者在确诊时已步入古稀之年，并伴随心血管、肾脏等多种基础并发症，根本无法耐受强烈的传统化学治疗。 •CLL11研究的破局在这个背景下，关键性Ⅲ期临床试验CLL11研究拉开了帷幕。该研究纳入了781名伴有并发症的初治CLL患者，被随机分配接受奥滨尤妥珠单抗+苯丁酸氮芥（G-Clb）、利妥昔单抗+苯丁酸氮芥（R-Clb）或苯丁酸氮芥单药（Clb）治疗。试验结果引发了血液学界的巨大震动。与经典的标准R-Clb方案相比，G-Clb组的中位无进展生存期（PFS）出现了断层式的领先（28.7个月 vs 15.7个月，疾病进展风险下降了54%，P < 0.0001）。更令人震撼的是微小残留病变（MRD）的清除深度，G-Clb组在骨髓和外周血中实现MRD阴性的比例远超利妥昔单抗组，这意味着肿瘤细胞被清剿到了现代医学仪器难以检测的极低水平。基于这项研究，奥滨尤妥珠单抗成为了FDA首个授予“突破性疗法”称号并火速获批的药物，从此确立了其在CLL一线治疗中的核心地位。 •最新进展（固定疗程的无化疗时代）随着CRISTALLO试验的披露，固定疗程的维奈托克联合奥滨尤妥珠单抗（VenO）展现出极深度的缓解：高达51.5%的患者实现了完全缓解（CR），而其外周血MRD不可测（uMRD）率更是飙升至73%（骨髓uMRD率也达到62%）。在另一项针对高危CLL患者（伴有TP53突变等）的最新研究中，Acalabrutinib（阿可替尼）+ Venetoclax + Obinutuzumab（AVO三联疗法）同样被证明具有极高的耐受性和深度缓解能力。这确立了其作为新兴靶向药“免疫基石”的地位。 3.2 滤泡性淋巴瘤（FL）：从复发难治到一线封神的跨越滤泡性淋巴瘤（FL）是最常见的惰性非霍奇金淋巴瘤（iNHL）。由于其生长缓慢的特性，FL通常被认为是无法彻底治愈的，患者在一生中会经历多次“缓解-复发”的痛苦循环，且每次复发后的治疗难度都会呈指数级上升。 •GADOLIN研究：利妥昔单抗耐药者的破局之刃针对那些已经对利妥昔单抗产生耐药（治疗期间或治疗后6个月内复发）的极高危iNHL患者，GADOLIN研究评估了G-Benda（奥滨尤妥珠单抗+苯达莫司汀）诱导继以奥滨单抗维持治疗的方案。这是一群几乎被死神锁定的患者，但数据却奇迹般地迎来了反转：与单用苯达莫司汀相比，G-Benda组经独立评审委员会（IRC）评估的疾病进展或死亡风险大幅下降了45%（HR=0.55，P=0.0001）。随后长达31.8个月的长期随访更新更是证实了G-Benda方案不仅延长了PFS，还显著降低了死亡风险，改善了总生存期（OS），由此确立了奥滨尤妥珠单抗在复发/难治性FL中的绝对标准疗法地位。 •GALLIUM研究：重塑一线标准（十年磨一剑的长期数据）奥滨尤妥珠单抗真正的王冠，在于对一线初治患者的拯救。纳入1202名初治晚期iNHL患者的关键Ⅲ期GALLIUM研究，直接比较了G-Chemo（联合化疗）与R-Chemo的疗效。随着时间推移，医学界对这批患者进行了长达近十年的追踪。在2023-2024年陆续公布的长期随访数据中，奥滨尤妥珠单抗交出了一份堪称惊艳的答卷。经过中位7.9年（最长达近10年）的长期随访，G-Chemo组的PFS优势不仅没有随着时间衰减，反而展现出平稳的“拖尾效应”。数据显示，G-Chemo组的7年PFS率稳定在63.4%，显著优于R-Chemo组的55.7%（P=0.006）。此外，患者距离需要接受下一次抗淋巴瘤治疗的时间（TTNT）也被大幅延后（74.1% vs 65.4%）。更为关键的是，奥滨尤妥珠单抗显著降低了“24个月内疾病进展（POD24）”的发生率。在FL的病理学生存分析中，一旦患者在初始治疗后24个月内复发（POD24），其后续的死亡风险将成几何倍数增加（风险比HR高达25.5）。奥滨尤妥珠单抗凭借更强大的初始疾病清扫能力，有效规避了这一致命的早复发陷阱，为患者争取到了长达十年的高质量生存期。四、临床博弈（下）：GOYA折戟的深度反思与DLBCL的生物学困境在针对侵袭性极强、恶性度极高的弥漫性大B细胞淋巴瘤（DLBCL）的关键Ⅲ期临床试验GOYA研究中，奥滨尤妥珠单抗迎来了其研发史上最大的一次“滑铁卢”。该研究浩浩荡荡地纳入了1418名初治DLBCL患者，试图用G-CHOP方案（奥滨尤妥珠单抗联合CHOP化疗）一举击败屹立多年的标准R-CHOP方案。然而，2017年的最终分析犹如一盆冷水：G-CHOP组与R-CHOP组相比，研究人员评估的PFS并未出现任何统计学意义上的改善（HR=0.92，P=0.3868），两组的5年PFS率几乎持平（63.8% vs 62.6%）。更令人担忧的是，G-CHOP组由于药物更强的清髓效应，其三级以上的不良反应（如晚发性中性粒细胞减少症和严重感染）发生率反而显著高于对照组。为何在CLL和FL中势如破竹的“神药”，在面对DLBCL时却无功而返？全球的血液学与病理学专家对此进行了极其深刻的复盘，揭示了药物工程学与肿瘤异质性之间错综复杂的博弈逻辑：（1）致命的短板暴露：对CDC（补体依赖细胞毒性）的高度依赖差异 DLBCL是一种侵袭性极强、细胞增殖速度极快的肿瘤，其细胞表面的CD20表达量高且抗原代谢极快。对于这种“暴走”状态的癌细胞，极其迅速的“地毯式轰炸”是至关重要的。研究表明，在DLBCL的早期杀伤中，补体系统介导的CDC效应发挥着不可替代的“穿甲弹”作用。利妥昔单抗作为Ⅰ型抗体，拥有极强的补体激活能力，能在瞬间通过级联反应在细胞膜上打孔；而奥滨尤妥珠单抗正如我们在第二章所言，为了追求极致的ADCC效应，在工程化设计时主动放弃了CDC效应。这种在生长缓慢的惰性淋巴瘤中无关紧要甚至有益的“机制取舍”，在面对迅速恶化增殖的DLBCL时，却成了致命的阿喀琉斯之踵。（2）肿瘤微环境（TME）的“冷热不均”与效应细胞的匮乏奥滨尤妥珠单抗的王牌机制是ADCC，而ADCC的发挥高度依赖于肿瘤微环境中充足的效应细胞（如NK细胞和巨噬细胞）作为“行刑者”。惰性的FL肿瘤微环境相对富含这些免疫浸润细胞，为奥滨尤妥珠单抗提供了充足的“弹药”。相反，DLBCL往往伴随着严重的免疫逃逸和基质屏障，其微环境呈现出典型的“冷肿瘤”特征，效应细胞浸润极度匮乏。即便奥滨尤妥珠单抗的Fc段具有再高的受体亲和力，在缺乏足够NK细胞响应的DLBCL微环境中，也只能是“巧妇难为无米之炊”。（3）药代动力学（PK）的黑洞：“海绵效应” DLBCL患者通常具有巨大的肿瘤负荷和肿块。这些巨大的肿瘤团块在体内形成了一种物理和代谢上的“海绵效应”。当奥滨尤妥珠单抗被注入血液后，大量抗体会迅速被肿瘤外围细胞结合并困在团块内部，导致循环系统中和肿瘤深部的有效抗体浓度难以维持在能够触发强效持续杀伤的阈值之上。 GOYA研究的失败并非全盘否定了奥滨尤妥珠单抗的价值，反而为现代精准医疗提供了一部经典的“反面教材”：抗体药物的疗效从来不是生化机制的线性叠加，而是药物的特定属性（如Fc糖基化修饰）与特定肿瘤组织学亚型（免疫微环境、增殖动力学、抗原密度）之间精密契合的结果。五、跨界突围：在自身免疫疾病领域的二次“黄金期” B淋巴细胞在系统性红斑狼疮（SLE）及其最致命的并发症——狼疮性肾炎（Lupus Nephritis, LN）的发病机制中，扮演着核心的驱动者角色。奥滨尤妥珠单抗凭借强大的组织深层清除能力和极低的靶点内化率，完美契合了这一治疗需求。体外实验清晰地表明，针对RA和SLE患者的全血样本，奥滨尤妥珠单抗对自身反应性B细胞的细胞毒性作用是利妥昔单抗的两倍以上，并且极少发生CD20内化现象。 •里程碑时刻：REGENCY与ALLEGORY研究的震撼发布 (2024-2025年最新突破) 蛰伏数年后，奥滨尤妥珠单抗在自身免疫疾病迎来了真正的爆发。 ① 攻克狼疮性肾炎（REGENCY研究）：在备受瞩目的Ⅲ期REGENCY临床试验中，研究者评估了奥滨尤妥珠单抗联合标准疗法（吗替酚酯MMF+糖皮质激素）在活动性狼疮性肾炎患者中的疗效。发表在2025年《新英格兰医学杂志》（NEJM）上的惊艳数据显示：在76周时，接受奥滨尤妥珠单抗联合治疗的患者中，有高达46.4%达到了极其严苛的完全肾脏反应（CRR），这一比例显著高于单独使用标准疗法的33.1%（组间差异达13.4%，P=0.0232）。更为重要的是，奥滨尤妥珠单抗将患者未来发生肾脏严重复发的风险大幅降低了56%（HR=0.44）。这一压倒性优势不仅证实了其在深层组织中摧毁致病B细胞的能力，更直接促使美国FDA在2024-2025年期间正式批准奥滨尤妥珠单抗用于活动性狼疮性肾炎的治疗，使其成为首个在此领域获批并证实CRR获益的抗CD20靶向药物。 ② 全面控制系统性红斑狼疮（ALLEGORY研究）：紧随其后，在针对更广泛的系统性红斑狼疮（SLE）人群的ALLEGORYⅢ期研究中，奥滨尤妥珠单抗交出了一份无可挑剔的答卷。该研究达到了所有主要和关键次要终点，在第52周时，显著提高了患者的SRI-4（系统性红斑狼疮缓解指数）响应率。真实世界的数据（如上海仁济医院的56例重症SLE队列）也呼应了这一结果：在接受一剂奥滨尤妥珠单抗后，患者的SLEDAI-2K评分从平均11.75骤降至1.45，不仅实现了深度的免疫学缓解，还使得患者能够大幅减少维持生命的糖皮质激素用量。更具科幻色彩的是，在2025年底公布的最新细胞疗法探索中，Artiva Biotherapeutics公司将奥滨尤妥珠单抗与冷冻保存的同种异体自然杀伤细胞（AlloNK）联用治疗顽固性自身免疫疾病。这种“抗体+外源性超级杀手”的组合，在无须清髓预处理的门诊环境下，实现了100%的深度B细胞耗竭，且未发生任何严重的细胞因子释放综合征（CRS）。这标志着奥滨尤妥珠单抗正在开启自身免疫疾病“类CAR-T级别疗效但具有极高安全性”的新纪元。结语奥滨尤妥珠单抗演绎了一部从分子构想、基因工程极端改造到颠覆临床标准的新药进化史。它并非简单的替代品，而是靶向药物从“经验医学”走向“精细化分子工程”的杰出代表。尽管在DLBCL遭遇挫折，但其在CLL与FL中长达十年的生存获益，以及在SLE和狼疮性肾炎领域的历史性破局，都证明了它的非凡价值。未来，它将作为重塑免疫微环境的核心中枢，继续在精准医疗时代发挥不可替代的基石作用。

并购免疫疗法

2026-03-27

·格隆汇

罗氏百亿重磅药奥滨尤妥珠单抗：Ⅱ型抗CD20如何颠覆肿瘤与自免治疗？

单克隆抗体技术深刻改变了肿瘤与自身免疫疾病的治疗。其中，CD20抗原作为B细胞的经典标志物，是最具代表性的靶点之一。二十多年前，第一代Ⅰ型抗CD20单抗利妥昔单抗（Rituximab）彻底改变了淋巴瘤和白血病患者的生存轨迹。然而，随着临床应用的深入，其局限性也逐渐暴露：耐药复发频繁、深层组织穿透力不足，且对低表达CD20肿瘤细胞的杀伤力有限。为打破这一僵局，科学界对底层机制进行了重构。奥滨尤妥珠单抗（Obinutuzumab，商品名为GAZYVA®/GAZYVARO®）作为全球首个经糖基化改造的Ⅱ型抗CD20人源化单抗应运而生。它并非简单的升级版，而是在空间构象、效应细胞招募及细胞死亡触发路径上，展现出了截然不同的精确杀伤力。一、从瑞士实验室的分子创想到百亿重磅药物的诞生任何一款划时代的药物，其背后都隐藏着一段充满未知、挑战与坚持的探索史。奥滨尤妥珠单抗的故事，始于对单克隆抗体天然缺陷的深刻反思。1.1 突破天然免疫瓶颈：“糖基化工程”的觉醒与GlycArt的创立千禧年初，科学家们面临如何提升单抗天然免疫杀伤效率的难题。瑞士苏黎世联邦理工学院（ETH）的著名生化工程先驱James E. Bailey教授指导的年轻学者Pablo Umaña和Joël Jean-Mairet等人敏锐地发现，抗体Fc段上的岩藻糖会在空间上严重削弱抗体与免疫效应细胞表面受体FcγRIIIa的结合亲和力。为了跨越这一障碍，Umaña与其团队在2000年参加了McKinsey/ETH商业计划大赛，尽管未能夺冠，但他们凭借对“抗体去岩藻糖基化”概念的深刻阐述，成功吸引了300万瑞士法郎的种子资金，并于2001年正式创立了衍生公司GlycArt Biotechnology AG。在随后的几年里，他们首创了名为“GlycoMAb”的核心技术。该技术通过基因工程手段，向生产抗体的中国仓鼠卵巢细胞（CHO）宿主中转入两种编码寡糖修饰酶的基因——β-1,4-N-乙酰葡萄糖胺转移酶Ⅲ（GnT Ⅲ）和高尔基体α-甘露糖苷酶Ⅱ（Man Ⅱ）。这一极具创造力的基因重组过程，使得细胞系能够稳定生产出“去岩藻糖基化”的抗体变体，为后续的药物研发奠定了坚实的基础。1.2 罗氏的战略并购与B-Ly1的“铰链区重塑”2005年，罗氏全资收购了GlycArt，直接催生了罗氏苏黎世创新中心的建立。在选择抗体骨架时，研究团队相中了一种源于小鼠IgG1的Ⅱ型亲本抗体B-Ly1。通过被业界称为“铰链工程”的精密操作，研究人员将Kabat 11位的亮氨酸精准突变为缬氨酸，使得奥滨尤妥珠单抗的铰链角比利妥昔单抗拓宽了30度。这一微小突变彻底改变了结合构象，赋予了其前所未有的杀伤潜能。二、降维打击：Ⅱ型抗CD20单抗的深层生物学机制重塑要深刻理解奥滨尤妥珠单抗在临床试验中展现出的压倒性优势，我们必须褪去临床数据的外衣，深入到纳米级别的分子战场。Ⅰ型（如利妥昔单抗、奥法木单抗）与Ⅱ型（如奥滨尤妥珠单抗）抗体在分子机制上的分野，是一场杀伤路径的战略性重构。2.1 空间结合艺术：“蟹钳效应”与抗原内化的规避尽管奥滨尤妥珠单抗与利妥昔单抗结合的CD20表位高度重叠，但其在细胞表面的空间取向却截然不同。结构生物学和晶体学研究表明，当奥滨尤妥珠单抗结合到CD20上时，其Fab段比利妥昔单抗旋转了90度，并向CD20表位的C端倾斜了70度。更具决定性意义的是其“抓取”抗原的方式。Ⅰ型抗体倾向于在相邻的两个CD20四聚体之间建立“桥接”，这种交联作用会促使CD20复合物在B细胞膜上的富胆固醇区域——脂筏中发生大规模聚集。而奥滨尤妥珠单抗凭借其更宽的铰链角，其两个Fab臂能够像“蟹钳”一样，紧紧钳住同一个CD20四聚体内的两个不同表位。这种“蟹钳式”的内部钳合直接阻止了CD20抗原向脂筏的转位。不进入脂筏带来了两个巨大的生物学红利：第一，它极大程度地避免了抗原的内化和“剃须现象”。在利妥昔单抗治疗中，靶细胞往往会通过吞噬受体将抗原-抗体复合物吞入细胞内降解，导致肿瘤细胞表面失去靶点，从而产生耐药性；而奥滨尤妥珠单抗由于不引发抗原内化，能够长时间稳定地锚定在靶细胞表面，为后续持续招募免疫细胞赢得了充足的“战术窗口”。抗CD20单克隆抗体的药效学特征。 (A) I型，非Fc优化单克隆抗体。(B) I型，Fc优化单克隆抗体。(C) II型，非Fc优化单克隆抗体。(D) II型，Fc优化单克隆抗体。（doi：10.1182/blood-2017-03-771832）2.2 杀伤机制的三重变奏：ADCC、直接死亡与CDC的极端取舍抗CD20抗体摧毁恶性B细胞依赖三大机制，奥滨尤妥珠单抗在此进行了极端的取舍：•战略性放弃：弱化补体激活（CDC）由于奥滨尤妥珠单抗不诱导CD20在脂筏中聚集，它无法像利妥昔单抗那样促使Fc段形成六聚体，因此极大地削弱了固定经典补体途径起始成分C1q的能力。表面上看，丧失CDC效应似乎削弱了抗体的杀伤力，但实际上，这是一种深谋远虑的机制取舍。大量的免疫学研究证实，过度的补体激活往往会消耗效应细胞的活性，甚至血清中的补体成分会物理性地干扰NK细胞的活化和与靶细胞的接触。奥滨尤妥珠单抗通过放弃CDC，排除了补体系统对NK细胞的干扰，为其主力武器的发挥扫清了障碍。•极致的借刀杀人：百倍增强的ADCC与ADCP效应去岩藻糖基化的GlycoMAb技术，赋予了奥滨尤妥珠单抗对抗体FcγRIIIa受体极度强烈的亲和力。在人体的免疫系统中，由于基因多态性，相当一部分人群的FcγRIIIa受体呈现低亲和力表型（如158F/F或158V/F基因型），这类患者对传统利妥昔单抗的反应往往较差。然而，糖基化改造彻底打破了这一基因壁垒。生化结合实验表明，奥滨尤妥珠单抗与低亲和性FcγRIIIa的结合亲和力（KD值约为55nmol/L），甚至超越了利妥昔单抗与高亲和性受体的结合力（KD值为660nmol/L）。这一数量级的跃升，使得它在体外实验中激发的ADCC效应达到了利妥昔单抗的35至100倍。这意味着，哪怕肿瘤细胞表面的CD20表达量极低，奥滨尤妥珠单抗也能像强力磁铁一样，将NK细胞和巨噬细胞牢牢吸附过来，对恶性B细胞执行“凌迟”般的细胞毒性打击和吞噬清除。•细胞内的崩溃：独特的非凋亡性直接死亡诱导除了招募外援，奥滨尤妥珠单抗自带强大的“单兵作战”能力。当它与CD20发生同型聚集时，能够不依赖任何免疫细胞，直接在B细胞内部触发死亡信号。与利妥昔单抗诱导的传统Caspase依赖性凋亡不同，奥滨尤妥珠单抗引发的是一种强烈的、依赖肌动蛋白重构的非典型溶酶体细胞死亡途径。更令人瞩目的是，近期针对细胞内信号通路的研究揭示，利妥昔单抗在结合CD20后，会通过激活AKT途径过度磷酸化促凋亡蛋白BAD（如Ser118位点），这种磷酸化反而会将BAD隔离在细胞质中，使其失去抑制抗凋亡蛋白BCL2的能力，从而变相发出了“促生存”信号。相比之下，奥滨尤妥珠单抗不仅不引发这种自我保护的抗凋亡信号，反而通过异常的SYK磷酸化强烈支持细胞凋亡的诱导。此外，奥滨尤妥珠单抗诱导的死亡具有强烈的免疫原性，能够促使肿瘤细胞释放热休克蛋白90等损伤相关模式分子（DAMPs），从而唤醒宿主体内原本休眠的T细胞，形成长效的抗肿瘤免疫记忆。三、临床博弈（上）：在惰性淋巴瘤与白血病中的王者之战奥滨尤妥珠单抗在临床前模型中展现出的摧枯拉朽般的优势，促使罗氏在全球范围内启动了庞大而严密的临床开发计划。其核心策略极具攻击性：直接在利妥昔单抗长期统治的优势适应证中进行“头对头”对决，用无可辩驳的数据重塑全球标准治疗方案。obinutuzumab临床试验信息3.1 慢性淋巴细胞白血病（CLL）：突破并发症人群的生存极限慢性淋巴细胞白血病（CLL）是西方世界最常见的成人白血病，它是一种主要影响老年人的惰性B细胞恶性肿瘤。许多患者在确诊时已步入古稀之年，并伴随心血管、肾脏等多种基础并发症，根本无法耐受强烈的传统化学治疗。•CLL11研究的破局在这个背景下，关键性Ⅲ期临床试验CLL11研究拉开了帷幕。该研究纳入了781名伴有并发症的初治CLL患者，被随机分配接受奥滨尤妥珠单抗+苯丁酸氮芥（G-Clb）、利妥昔单抗+苯丁酸氮芥（R-Clb）或苯丁酸氮芥单药（Clb）治疗。试验结果引发了血液学界的巨大震动。与经典的标准R-Clb方案相比，G-Clb组的中位无进展生存期（PFS）出现了断层式的领先（28.7个月 vs 15.7个月，疾病进展风险下降了54%，P < 0.0001）。更令人震撼的是微小残留病变（MRD）的清除深度，G-Clb组在骨髓和外周血中实现MRD阴性的比例远超利妥昔单抗组，这意味着肿瘤细胞被清剿到了现代医学仪器难以检测的极低水平。基于这项研究，奥滨尤妥珠单抗成为了FDA首个授予“突破性疗法”称号并火速获批的药物，从此确立了其在CLL一线治疗中的核心地位。obinutuzumab特殊审批•最新进展（固定疗程的无化疗时代）随着CRISTALLO试验的披露，固定疗程的维奈托克联合奥滨尤妥珠单抗（VenO）展现出极深度的缓解：高达51.5%的患者实现了完全缓解（CR），而其外周血MRD不可测（uMRD）率更是飙升至73%（骨髓uMRD率也达到62%）。在另一项针对高危CLL患者（伴有TP53突变等）的最新研究中，Acalabrutinib（阿可替尼）+ Venetoclax + Obinutuzumab（AVO三联疗法）同样被证明具有极高的耐受性和深度缓解能力。这确立了其作为新兴靶向药“免疫基石”的地位。3.2 滤泡性淋巴瘤（FL）：从复发难治到一线封神的跨越滤泡性淋巴瘤（FL）是最常见的惰性非霍奇金淋巴瘤（iNHL）。由于其生长缓慢的特性，FL通常被认为是无法彻底治愈的，患者在一生中会经历多次“缓解-复发”的痛苦循环，且每次复发后的治疗难度都会呈指数级上升。•GADOLIN研究：利妥昔单抗耐药者的破局之刃针对那些已经对利妥昔单抗产生耐药（治疗期间或治疗后6个月内复发）的极高危iNHL患者，GADOLIN研究评估了G-Benda（奥滨尤妥珠单抗+苯达莫司汀）诱导继以奥滨单抗维持治疗的方案。这是一群几乎被死神锁定的患者，但数据却奇迹般地迎来了反转：与单用苯达莫司汀相比，G-Benda组经独立评审委员会（IRC）评估的疾病进展或死亡风险大幅下降了45%（HR=0.55，P=0.0001）。随后长达31.8个月的长期随访更新更是证实了G-Benda方案不仅延长了PFS，还显著降低了死亡风险，改善了总生存期（OS），由此确立了奥滨尤妥珠单抗在复发/难治性FL中的绝对标准疗法地位。•GALLIUM研究：重塑一线标准（十年磨一剑的长期数据）奥滨尤妥珠单抗真正的王冠，在于对一线初治患者的拯救。纳入1202名初治晚期iNHL患者的关键Ⅲ期GALLIUM研究，直接比较了G-Chemo（联合化疗）与R-Chemo的疗效。随着时间推移，医学界对这批患者进行了长达近十年的追踪。在2023-2024年陆续公布的长期随访数据中，奥滨尤妥珠单抗交出了一份堪称惊艳的答卷。经过中位7.9年（最长达近10年）的长期随访，G-Chemo组的PFS优势不仅没有随着时间衰减，反而展现出平稳的“拖尾效应”。数据显示，G-Chemo组的7年PFS率稳定在63.4%，显著优于R-Chemo组的55.7%（P=0.006）。此外，患者距离需要接受下一次抗淋巴瘤治疗的时间（TTNT）也被大幅延后（74.1% vs 65.4%）。更为关键的是，奥滨尤妥珠单抗显著降低了“24个月内疾病进展（POD24）”的发生率。在FL的病理学生存分析中，一旦患者在初始治疗后24个月内复发（POD24），其后续的死亡风险将成几何倍数增加（风险比HR高达25.5）。奥滨尤妥珠单抗凭借更强大的初始疾病清扫能力，有效规避了这一致命的早复发陷阱，为患者争取到了长达十年的高质量生存期。四、临床博弈（下）：GOYA折戟的深度反思与DLBCL的生物学困境在针对侵袭性极强、恶性度极高的弥漫性大B细胞淋巴瘤（DLBCL）的关键Ⅲ期临床试验GOYA研究中，奥滨尤妥珠单抗迎来了其研发史上最大的一次“滑铁卢”。该研究浩浩荡荡地纳入了1418名初治DLBCL患者，试图用G-CHOP方案（奥滨尤妥珠单抗联合CHOP化疗）一举击败屹立多年的标准R-CHOP方案。然而，2017年的最终分析犹如一盆冷水：G-CHOP组与R-CHOP组相比，研究人员评估的PFS并未出现任何统计学意义上的改善（HR=0.92，P=0.3868），两组的5年PFS率几乎持平（63.8% vs 62.6%）。更令人担忧的是，G-CHOP组由于药物更强的清髓效应，其三级以上的不良反应（如晚发性中性粒细胞减少症和严重感染）发生率反而显著高于对照组。为何在CLL和FL中势如破竹的“神药”，在面对DLBCL时却无功而返？全球的血液学与病理学专家对此进行了极其深刻的复盘，揭示了药物工程学与肿瘤异质性之间错综复杂的博弈逻辑：（1）致命的短板暴露：对CDC（补体依赖细胞毒性）的高度依赖差异DLBCL是一种侵袭性极强、细胞增殖速度极快的肿瘤，其细胞表面的CD20表达量高且抗原代谢极快。对于这种“暴走”状态的癌细胞，极其迅速的“地毯式轰炸”是至关重要的。研究表明，在DLBCL的早期杀伤中，补体系统介导的CDC效应发挥着不可替代的“穿甲弹”作用。利妥昔单抗作为Ⅰ型抗体，拥有极强的补体激活能力，能在瞬间通过级联反应在细胞膜上打孔；而奥滨尤妥珠单抗正如我们在第二章所言，为了追求极致的ADCC效应，在工程化设计时主动放弃了CDC效应。这种在生长缓慢的惰性淋巴瘤中无关紧要甚至有益的“机制取舍”，在面对迅速恶化增殖的DLBCL时，却成了致命的阿喀琉斯之踵。弥漫性大B细胞淋巴瘤（DLBCL）中抗CD20免疫疗法的耐药机制。（doi: 10.3390/ijms23031501）（2）肿瘤微环境（TME）的“冷热不均”与效应细胞的匮乏奥滨尤妥珠单抗的王牌机制是ADCC，而ADCC的发挥高度依赖于肿瘤微环境中充足的效应细胞（如NK细胞和巨噬细胞）作为“行刑者”。惰性的FL肿瘤微环境相对富含这些免疫浸润细胞，为奥滨尤妥珠单抗提供了充足的“弹药”。相反，DLBCL往往伴随着严重的免疫逃逸和基质屏障，其微环境呈现出典型的“冷肿瘤”特征，效应细胞浸润极度匮乏。即便奥滨尤妥珠单抗的Fc段具有再高的受体亲和力，在缺乏足够NK细胞响应的DLBCL微环境中，也只能是“巧妇难为无米之炊”。（3）药代动力学（PK）的黑洞：“海绵效应”DLBCL患者通常具有巨大的肿瘤负荷和肿块。这些巨大的肿瘤团块在体内形成了一种物理和代谢上的“海绵效应”。当奥滨尤妥珠单抗被注入血液后，大量抗体会迅速被肿瘤外围细胞结合并困在团块内部，导致循环系统中和肿瘤深部的有效抗体浓度难以维持在能够触发强效持续杀伤的阈值之上。GOYA研究的失败并非全盘否定了奥滨尤妥珠单抗的价值，反而为现代精准医疗提供了一部经典的“反面教材”：抗体药物的疗效从来不是生化机制的线性叠加，而是药物的特定属性（如Fc糖基化修饰）与特定肿瘤组织学亚型（免疫微环境、增殖动力学、抗原密度）之间精密契合的结果。五、跨界突围：在自身免疫疾病领域的二次“黄金期”B淋巴细胞在系统性红斑狼疮（SLE）及其最致命的并发症——狼疮性肾炎（Lupus Nephritis, LN）的发病机制中，扮演着核心的驱动者角色。奥滨尤妥珠单抗凭借强大的组织深层清除能力和极低的靶点内化率，完美契合了这一治疗需求。体外实验清晰地表明，针对RA和SLE患者的全血样本，奥滨尤妥珠单抗对自身反应性B细胞的细胞毒性作用是利妥昔单抗的两倍以上，并且极少发生CD20内化现象。•里程碑时刻：REGENCY与ALLEGORY研究的震撼发布 (2024-2025年最新突破)蛰伏数年后，奥滨尤妥珠单抗在自身免疫疾病迎来了真正的爆发。① 攻克狼疮性肾炎（REGENCY研究）：在备受瞩目的Ⅲ期REGENCY临床试验中，研究者评估了奥滨尤妥珠单抗联合标准疗法（吗替酚酯MMF+糖皮质激素）在活动性狼疮性肾炎患者中的疗效。发表在2025年《新英格兰医学杂志》（NEJM）上的惊艳数据显示：在76周时，接受奥滨尤妥珠单抗联合治疗的患者中，有高达46.4%达到了极其严苛的完全肾脏反应（CRR），这一比例显著高于单独使用标准疗法的33.1%（组间差异达13.4%，P=0.0232）。更为重要的是，奥滨尤妥珠单抗将患者未来发生肾脏严重复发的风险大幅降低了56%（HR=0.44）。这一压倒性优势不仅证实了其在深层组织中摧毁致病B细胞的能力，更直接促使美国FDA在2024-2025年期间正式批准奥滨尤妥珠单抗用于活动性狼疮性肾炎的治疗，使其成为首个在此领域获批并证实CRR获益的抗CD20靶向药物。② 全面控制系统性红斑狼疮（ALLEGORY研究）：紧随其后，在针对更广泛的系统性红斑狼疮（SLE）人群的ALLEGORYⅢ期研究中，奥滨尤妥珠单抗交出了一份无可挑剔的答卷。该研究达到了所有主要和关键次要终点，在第52周时，显著提高了患者的SRI-4（系统性红斑狼疮缓解指数）响应率。真实世界的数据（如上海仁济医院的56例重症SLE队列）也呼应了这一结果：在接受一剂奥滨尤妥珠单抗后，患者的SLEDAI-2K评分从平均11.75骤降至1.45，不仅实现了深度的免疫学缓解，还使得患者能够大幅减少维持生命的糖皮质激素用量。系统性红斑狼疮（SLE）患者接受奥妥珠单抗治疗后，临床和血清学指标均有所改善。（doi: 10.3389/fimmu.2025.1702550）更具科幻色彩的是，在2025年底公布的最新细胞疗法探索中，Artiva Biotherapeutics公司将奥滨尤妥珠单抗与冷冻保存的同种异体自然杀伤细胞（AlloNK）联用治疗顽固性自身免疫疾病。这种“抗体+外源性超级杀手”的组合，在无须清髓预处理的门诊环境下，实现了100%的深度B细胞耗竭，且未发生任何严重的细胞因子释放综合征（CRS）。这标志着奥滨尤妥珠单抗正在开启自身免疫疾病“类CAR-T级别疗效但具有极高安全性”的新纪元。结语奥滨尤妥珠单抗演绎了一部从分子构想、基因工程极端改造到颠覆临床标准的新药进化史。它并非简单的替代品，而是靶向药物从“经验医学”走向“精细化分子工程”的杰出代表。尽管在DLBCL遭遇挫折，但其在CLL与FL中长达十年的生存获益，以及在SLE和狼疮性肾炎领域的历史性破局，都证明了它的非凡价值。未来，它将作为重塑免疫微环境的核心中枢，继续在精准医疗时代发挥不可替代的基石作用。

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


NCT04855695 (AACR2026)	临床1/2期	套细胞淋巴瘤	9	ObinutuzumabAcalabrutinibVenetoclaxnib + ObinutuzumabAcalabrutinibVenetoclax + ObinutuzumabAcalabrutinibVenetoclaxab	襯鑰鑰窪簾襯選淵蓋鏇(網繭憲簾襯遞鹽鏇齋壓) = 廠繭糧鏇膚糧觸憲鹹製窪網製鑰獵網窪憲獵積 (鹽簾積鏇衊鹹蓋鬱壓憲 )	积极	2026-04-20
				Obinutuzumab (Durable Response)	襯鑰鑰窪簾襯選淵蓋鏇(網繭憲簾襯遞鹽鏇齋壓) = 繭獵鹽餘夢願襯遞簾製窪網製鑰獵網窪憲獵積 (鹽簾積鏇衊鹹蓋鬱壓憲 )
NCT02471391 (Pubmed \| Blood Adv)	临床2期	边缘区B细胞淋巴瘤	14	Venetoclax and ibrutinib (I+V)	築鑰夢蓋願鹹淵醖願壓(遞鏇憲膚鬱鹽簾願艱範) = 襯襯窪構範構遞繭蓋衊醖蓋範夢膚膚淵網廠鬱 (願鏇遞齋繭膚鑰壓襯淵, 8 ~ 58) 更多	积极	2026-03-10
NCT04330820 (RELAX, Pubmed \| Lancet Haematol)	临床1/2期	急性髓性白血病	55	Venetoclax 400 mg + Venetoclax 400 mgg/m² + Venetoclax 400 mglevel 1-3)	衊憲鏇簾鑰顧積製壓夢(網鏇憲憲鹽醖鹹築艱觸) = 53% 鹽製鹹築糧獵簾艱顧願 (網糧窪窪齋夢廠衊壓鬱 ) 更多	积极	2026-03-01
NCT03504644 (EA9152, CTgov)	临床1/2期	复发性 B 细胞急性淋巴细胞白血病 \| 前体B淋巴细胞淋巴瘤/难治性白血病 \| 复发性T淋巴母细胞淋巴瘤 ... 更多	40	Computed Tomography+Venetoclax+Vincristine Sulfate+Vincristine Liposomal	醖繭鹹構獵繭構鏇鬱積(鬱網壓蓋繭鏇鏇簾鹹積) = 蓋繭鹽憲鹹構壓蓋範窪網獵築襯餘網夢願鹽齋 (網蓋憲壓糧鏇醖構憲繭, 範鹹鹹鑰醖網鬱淵蓋積 ~ 簾糧鹽鏇醖範齋壓廠鑰) 更多	-	2026-02-25
NCT04708054 (Tandem Meetings ASTCT and CIBMTR2026)	临床2期	高危骨髓增生异常综合征	50	Myeloablative Fractionated Busulfan, Fludarabine, Cladribine, Thiotepa, and Venetoclax	願構夢網窪艱夢鏇選製(壓衊壓憲淵淵鏇窪齋獵) = 艱鏇構獵醖顧顧窪鏇鏇餘憲夢壓築餘積壓觸廠 (齋積膚憲範壓齋鏇顧繭, 11 ~ NR) 更多	积极	2026-02-04
				Myeloablative Fractionated Busulfan, Fludarabine, Cladribine, Thiotepa, and Venetoclax (TP53 mutated)	願憲醖糧蓋憲獵窪廠廠(淵壓餘願願鬱憲簾壓鏇) = 願襯襯願願製遞繭鹽夢築膚憲簾襯鬱範鏇築積 (繭築憲鏇鏇衊淵鬱觸醖 ) 更多
NCT04708054 (Tandem Meetings ASTCT and CIBMTR2026)	临床2期	急性髓性白血病	50	Myeloablative Fractionated Busulfan, Fludarabine, Cladribine, Thiotepa, and Venetoclax (Cladillac) Conditioning	膚築構窪糧鏇簾製艱願(鏇艱餘製夢築願鑰構襯) = 餘願蓋襯積遞齋鹹廠鏇顧鹹糧鹽願艱壓膚淵夢 (廠鏇簾壓餘壓衊鏇淵積, 48 ~ 75) 更多	积极	2026-02-04
				Myeloablative Fractionated Busulfan, Fludarabine, Cladribine, Thiotepa, and Venetoclax (Cladillac) Conditioning (TP53 wildtype)	膚築構窪糧鏇簾製艱願(鏇艱餘製夢築願鑰構襯) = 襯網製衊鏇壓顧窪製糧顧鹹糧鹽願艱壓膚淵夢 (廠鏇簾壓餘壓衊鏇淵積 ) 更多
Tandem Meetings ASTCT and CIBMTR2026	N/A	急性髓性白血病	251	Venetoclax+HMA	獵襯範製醖餘齋憲壓鏇(顧築選觸窪壓蓋鏇餘顧) = 範艱餘艱窪憲壓衊餘製繭膚範壓網繭範獵顧網 (網觸鑰餘醖膚憲襯艱鏇 )	积极	2026-02-04
				7+3	簾夢膚顧鏇艱襯鏇蓋壓(選鏇鏇顧糧餘窪衊糧選) = 選網淵糧窪膚選醖夢壓憲壓鑰鹽壓壓鬱鏇顧壓 (鏇鹽繭鏇繭鏇築範獵襯 ) 更多
Tandem Meetings ASTCT and CIBMTR2026	N/A	急性髓性白血病	30	Azacitidine and Venetoclax	鏇繭襯艱觸範獵製衊艱(襯艱鏇醖製構蓋顧醖鏇) = 範獵衊廠構膚淵繭窪築膚簾遞觸廠壓糧艱構醖 (鬱鏇膚膚鹽構衊餘遞蓋 ) 更多	积极	2026-02-04
				Intensive Chemotherapy	鏇繭襯艱觸範獵製衊艱(襯艱鏇醖製構蓋顧醖鏇) = 膚齋壓窪鏇鏇艱窪鑰願膚簾遞觸廠壓糧艱構醖 (鬱鏇膚膚鹽構衊餘遞蓋 ) 更多
NCT02427451 (CTgov)	临床1/2期	复发性慢性淋巴细胞白血病 \| 难治性慢性淋巴细胞白血病	87	Ibrutinib+Bcl-2 Inhibitor GDC-0199+obinutuzumab (Phase 1b Cohort)	艱築遞願獵夢鑰製鑰夢 = 鏇糧廠艱繭遞蓋鹹獵鹹願網顧襯蓋衊鹹範夢醖 (鏇膚範顧衊餘製遞蓋鬱, 膚簾糧醖簾壓衊築築窪 ~ 獵鬱積醖膚構製獵淵積)	-	2026-01-27
				Ibrutinib+Bcl-2 Inhibitor GDC-0199+obinutuzumab (Phase 2 Relapsed/Refractory)	鏇醖製範獵簾選醖製繭 = 鑰鹽網膚衊襯觸顧獵衊廠選顧願願觸餘製夢網 (憲遞憲簾網餘獵廠蓋襯, 築觸醖廠憲廠鹹築廠構 ~ 遞糧憲構蓋夢衊構艱壓) 更多
NCT03539744 (CANOVA, Pubmed \| J Clin Oncol)	临床3期	多发性骨髓瘤末线 t(11;14)-Positive	263	Venetoclax-Dexamethasone	鏇觸築廠廠壓夢鏇淵築(積觸獵醖糧淵遞範襯憲) = 構簾衊鏇網餘衊膚壓網鏇鏇築製製廠窪遞繭襯 (膚鏇衊構網網網艱範鹹, 6.9 ~ 12.6) 更多	不佳	2026-01-20
				Pomalidomide-Dexamethasone	鏇觸築廠廠壓夢鏇淵築(積觸獵醖糧淵遞範襯憲) = 鏇簾鏇鏇襯糧簾鹹餘願鏇鏇築製製廠窪遞繭襯 (膚鏇衊構網網網艱範鹹, 3.8 ~ 9.2) 更多