The primary objective of this study is to determine the recommended phase 2 dose (RP2D) and characterize the safety profile of TG-1801. As per protocol v3.0, ublituximab will be discontinued.

开始日期2021-04-28

申办/合作机构

TG Therapeutics, Inc.

NCT03804996

/ Completed临床1期

A Phase 1 First-in-Human Study of Bispecific Antibody TG-1801 in Subjects With B-Cell Lymphoma

Phase 1 first in human Study to Assess the Bispecific Antibody TG-1801 in Subjects with B-Cell Lymphoma

开始日期2019-03-05

申办/合作机构

TG Therapeutics, Inc.

100 项与 TG-1801 相关的临床结果

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100 项与 TG-1801 相关的转化医学

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100 项与 TG-1801 相关的专利（医药）

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项与 TG-1801 相关的文献（医药）

2023-01-01·Frontiers in immunology

G protein-coupled receptor 183 mediates the sensitization of Burkitt lymphoma tumors to CD47 immune checkpoint blockade by anti-CD20/PI3Kδi dual therapy.

Article

作者: Armengol, Marc ; Normant, Emmanuel ; Roué, Gael ; Profitós-Pelejà, Núria ; Fernández-Serrano, Miranda ; Santos, Juliana Carvalho ; Blecua, Pedro ; Reyes-Garau, Diana ; Bosch, Francesc ; Ribeiro, Marcelo Lima ; Miskin, Hari P ; Esteller, Manel

Background:

Immunotherapy-based regimens have considerably improved the survival rate of B-cell non-Hodgkin lymphoma (B-NHL) patients in the last decades; however, most disease subtypes remain almost incurable. TG-1801, a bispecific antibody that targets CD47 selectively on CD19+ B-cells, is under clinical evaluation in relapsed/refractory (R/R) B-NHL patients either as a single-agent or in combination with ublituximab, a new generation CD20 antibody.

Methods:

A set of eight B-NHL cell lines and primary samples were cultured in vitro in the presence of bone marrow-derived stromal cells, M2-polarized primary macrophages, and primary circulating PBMCs as a source of effector cells. Cell response to TG-1801 alone or combined with the U2 regimen associating ublituximab to the PI3Kδ inhibitor umbralisib, was analyzed by proliferation assay, western blot, transcriptomic analysis (qPCR array and RNA sequencing followed by gene set enrichment analysis) and/or quantification of antibody-dependent cell death (ADCC) and antibody-dependent cell phagocytosis (ADCP). CRISPR-Cas9 gene edition was used to selectively abrogate GPR183 gene expression in B-NHL cells. In vivo, drug efficacy was determined in immunodeficient (NSG mice) or immune-competent (chicken embryo chorioallantoic membrane (CAM)) B-NHL xenograft models.

Results:

Using a panel of B-NHL co-cultures, we show that TG-1801, by disrupting the CD47-SIRPα axis, potentiates anti-CD20-mediated ADCC and ADCP. This led to a remarkable and durable antitumor effect of the triplet therapy composed by TG-1801 and U2 regimen, in vitro, as well as in mice and CAM xenograft models of B-NHL. Transcriptomic analysis also uncovered the upregulation of the G protein-coupled and inflammatory receptor, GPR183, as a crucial event associated with the efficacy of the triplet combination. Genetic depletion and pharmacological inhibition of GPR183 impaired ADCP initiation, cytoskeleton remodeling and cell migration in 2D and 3D spheroid B-NHL co-cultures, and disrupted macrophage-mediated control of tumor growth in B-NHL CAM xenografts.

Conclusions:

Altogether, our results support a crucial role for GPR183 in the recognition and elimination of malignant B cells upon concomitant targeting of CD20, CD47 and PI3Kδ, and warrant further clinical evaluation of this triplet regimen in B-NHL.

2022-12-01·Experimental Hematology & Oncology3区 · 医学

CD47xCD19 bispecific antibody triggers recruitment and activation of innate immune effector cells in a B-cell lymphoma xenograft model

3区 · 医学

ArticleOA

作者: Chatel, Laurence ; Cons, Laura ; Pontini, Guillemette ; Masternak, Krzysztof ; Moine, Valéry ; Daubeuf, Bruno ; Chauchet, Xavier ; Malinge, Pauline ; Didelot, Gérard ; Chollet, Didier ; Shang, Limin ; Buatois, Vanessa ; Ferlin, Walter

Abstract:

Background:

CD47/SIRPα axis is recognized as an innate immune checkpoint and emerging clinical data validate the interest of interrupting this pathway in cancer, particularly in hematological malignancies. In preclinical models, CD47/SIRPα blocking agents have been shown to mobilize phagocytic cells and trigger adaptive immune responses to eliminate tumors. Here, we describe the mechanisms afforded by a CD47xCD19 bispecific antibody (NI-1701) at controlling tumor growth in a mouse xenograft B-cell lymphoma model.

Methods:

The contribution of immune effector cell subsets behind the antitumor activity of NI-1701 was investigated using flow cytometry, transcriptomic analysis, and in vivo immune-cell depletion experiments.

Results:

We showed that NI-1701 treatment transformed the tumor microenvironment (TME) into a more anti-tumorigenic state with increased NK cells, monocytes, dendritic cells (DC) and MHCIIhi tumor-associated macrophages (TAMs) and decreased granulocytic myeloid-derived suppressor cells. Notably, molecular analysis of isolated tumor-infiltrating leukocytes following NI-1701 administration revealed an upregulation of genes linked to immune activation, including IFNγ and IL-12b. Moreover, TAM-mediated phagocytosis of lymphoma tumor cells was enhanced in the TME in the presence of NI-1701, highlighting the role of macrophages in tumor control. In vivo cell depletion experiments demonstrated that both macrophages and NK cells contribute to the antitumor activity. In addition, NI-1701 enhanced dendritic cell-mediated phagocytosis of tumor cells in vitro, resulting in an increased cross-priming of tumor-specific CD8 T cells.

Conclusions:

The study described the mechanisms afforded by the CD47xCD19 bispecific antibody, NI-1701, at controlling tumor growth in lymphoma mouse model. NI-1701 is currently being evaluated in a Phase I clinical trial for the treatment of refractory or relapsed B-cell lymphoma (NCT04806035).

2018-08-01·Molecular cancer therapeutics2区 · 医学

Preclinical Development of a Bispecific Antibody that Safely and Effectively Targets CD19 and CD47 for the Treatment of B-Cell Lymphoma and Leukemia

2区 · 医学

Article

作者: D'Asaro, Matilde ; Masternak, Krzysztof ; Ribera, José María ; Rettig, Michael ; Fielding, Adele K. ; Ritchey, Julie ; Genescà Ferrer, Eulàlia ; DiPersio, John F. ; Salgado-Pires, Susana ; Eissenberg, Linda ; LeGallou, Simon ; Fischer, Nicolas ; Kosco-Vilbois, Marie H. ; Ferlin, Walter G. ; Johnson, Zoë ; Matthes, Thomas ; Chauchet, Xavier ; Papaioannou, Anne ; Broyer, Lucile ; Bailey, Katharine ; Hatterer, Eric ; Tarte, Karin ; Clarke Hinojosa, Robert K. ; Cons, Laura ; Dey, Aditi ; Daubeuf, Bruno ; Barba, Leticia ; Fest, Thierry ; Richard, Françoise ; Buatois, Vanessa ; Shang, Limin

Abstract:

CD47, an ubiquitously expressed innate immune checkpoint receptor that serves as a universal “don't eat me” signal of phagocytosis, is often upregulated by hematologic and solid cancers to evade immune surveillance. Development of CD47-targeted modalities is hindered by the ubiquitous expression of the target, often leading to rapid drug elimination and hemotoxicity including anemia. To overcome such liabilities, we have developed a fully human bispecific antibody, NI-1701, designed to coengage CD47 and CD19 selectively on B cells. NI-1701 demonstrates favorable elimination kinetics with no deleterious effects seen on hematologic parameters following single or multiple administrations to nonhuman primates. Potent in vitro and in vivo activity is induced by NI-1701 to kill cancer cells across a plethora of B-cell malignancies and control tumor growth in xenograft mouse models. The mechanism affording maximal tumor growth inhibition by NI-1701 is dependent on the coengagement of CD47/CD19 on B cells inducing potent antibody-dependent cellular phagocytosis of the targeted cells. NI-1701–induced control of tumor growth in immunodeficient NOD/SCID mice was more effective than that achieved with the anti-CD20 targeted antibody, rituximab. Interestingly, a synergistic effect was seen when tumor-implanted mice were coadministered NI-1701 and rituximab leading to significantly improved tumor growth inhibition and regression in some animals. We describe herein, a novel bispecific antibody approach aimed at sensitizing B cells to become more readily phagocytosed and eliminated thus offering an alternative or adjunct therapeutic option to patients with B-cell malignancies refractory/resistant to anti-CD20–targeted therapy. Mol Cancer Ther; 17(8); 1739–51. ©2018 AACR.

项与 TG-1801 相关的新闻（医药）

2024-11-27

·lightchainbio.com

ASH-2024 generation of FcRH5xCD28 bispecific antibodies

Light Chain Bioscience is leveraging its proprietary bispecific antibody format to advance immune therapies in oncology and beyond. The Swiss biopharmaceutical company Light Chain Bioscience has developed a novel and unique class of human, bispecific antibodies dubbed κλ bodies, so-called because they combine a κ light chain that recognizes a first target and a λ light chain that recognizes a second one, into a native human antibody structure. In collaboration with TG Therapeutics, Light Chain has brought one internally developed κλ body, TG-1801 (formerly NI-1701), into clinical trials for relapsed/refractory B cell lymphoma, and has a number of others in the pipeline for the treatment of various tumors and blood disorders. Light Chain emerged from Novimmune, which over the past 20 years has developed monoclonal antibodies (mAbs) in inflammatory and autoimmune diseases, with seven reaching clinical trials and one, the anti-interferon mAb Gamifant (emapalumab), gaining approval by the US Food and Drug Administration (FDA) in 2018 as the first treatment for hemophagocytic lymphohistiocytosis. In July 2019, Novimmune divested Gamifant and related activities, and rebranded as Light Chain Bioscience with a focus on bispecific antibodies. Light Chain, which draws on decades of experience in immunology and antibody-based therapies gained as Novimmune, is now seeking partners to take forward candidates identified by Light Chain, as well as partners seeking to apply Light Chain’s expertise and technology platform to their own projects. “Building on Novimmune’s long experience in antibody discovery and development, Light Chain Bioscience now focuses on leveraging the unique features of its bispecific antibody format”, said Erich Hunziker, Chairman of Light Chain Bioscience. Bispecific antibodies represent a rapidly growing therapeutic approach, and many methods have been devised for their production. Often this has required extensive engineering of antibodies at their interfaces, or addition of linkers and other foreign sequences, to facilitate assembly and allow the cells expressing the antibodies to produce the bispecific product in sufficient quantities. LightChain’s approach is different, creating bispecific antibodies that are essentially fully human, with no engineering required. The method for creating bispecific κλ bodies is simple: a production cell expresses a single heavy chain, alongside κ and λ light chains, which self-assemble into functional antibodies. This process creates a mixture of antibodies, 25% of which are monospecific containing two κ identical chains, 25% are monospecific with two identical λ chains and 50% are bispecific κλ bodies, which can be very effectively purified from the supernatant using affinity reagents binding to the two different light chains. Light Chain’s bispecific platform not only bypasses engineering challenges but also offers a simple and scalable manufacturing process. Working with contract manufacturing company Lonza Pharma & Biotech, Light Chain has already manufactured κλ bodies under good manufacturing practice (GMP) on a 1,000-litre scale in several runs, with high yields (Fig. 1). «Building on Novimmune’s long experience in antibody discovery and development, Light Chain Bioscience now focuses on leveraging the unique features of its bispecific antibody format» Erich Hunziker, Chairman, Light Chain Bioscience As more and more bispecific antibodies have entered clinical trials, immunogenicity potentially associated with engineered or foreign elements in the antibodies is emerging as a significant concern. Light Chain’s κλ bodies have no modifications, except for the loops present in the extremities of the light chains that create the desired target specificity, as in any normal human antibody. “Over the last decade challenges linked to bispecific antibodies engineering and manufacturing have been overcome. The field is now beginning to face the issue of immunogenicity,” said Nicolas Fischer, CEO of Light Chain Bioscience. “The native structure of κλ bodies is likely to represent a significant advantage.” Targeting innate immune checkpoints Light Chain’s most advanced bispecific κλ body candidate is TG-1801, which has binding moieties for CD47 and the B cell surface antigen CD19, and is in phase 1 trials for relapsed/refractory B cell lymphoma. CD47 is an immune checkpoint protein that functions as a regulator of phagocytosis. Cancer immunotherapies that target adaptive immune checkpoints have demonstrated clinical benefits in a range of cancers, and in recent years the idea of targeting innate immune checkpoints has emerged as a hot topic, with CD47 widely seen as an exciting new innate checkpoint molecule. CD47 is a membrane-bound protein expressed on tumor cells, as well as all normal cells in the body, where it acts as a ‘don’t eat me!’ signal. CD47 communicates this message by binding to signal-regulatory protein-α (SIRPα) on phagocytic cells, particularly macrophages; this binding in turn inhibits phagocytosis. Tumor cells frequently hijack this system and overexpress CD47, which translates clinically into worse prognoses across several cancer indications. Blocking the signalling between CD47 and SIRPα with anti-CD47 mAbs increases the phagocytosis and killing of tumor cells. However, early examples of this approach contained a fully functional Fc portion that led to indiscriminate binding and killing of normal cells, including red blood cells (RBCs) and platelets,which resulted in dangerous thrombocytopenia. To overcome the challenge of hemotoxicity, anti- CD47 mAbs that carry a silenced Fc portion have been developed, but these have to be administered alongside a second mAb directed against a tumorassociated antigen (TAA) such as HER2 (also known as ERBB2), CD19 or CD20. Light Chain’s TG-1801 combines the functions of two antibodies, with one light chain binding to CD47 and the other to CD19. The CD47-binding domain has been optimized so that it binds with relatively low affinity, which ensures that it does not remain bound to normal cells, including RBCs and platelets. The CD19- binding domain, however, binds to its ligand tightly and anchors TG-1801 on the surface of B cells, where it can then co-bind to CD47. Because TG-1801 only binds strongly to CD47 in the presence of CD19 on B cells, it is able to retain a fully functional Fc portion without causing hemotoxicity (Fig. 2). Crucially, because the Fc portion is fully functional in TG-1801, it can recruit macrophages as well as other effector cells in the tumor microenvironment to eat and kill tumor cells that they would otherwise ignore. Studies with non-human primates have shown that in a model system in which CD47 is ubiquitously expressed, TG-1801 has good pharmacokinetic properties and does not cause hemotoxicity. TG-1801 is being jointly developed with TG Therapeutics and is currently in a phase 1 trial for B cell lymphoma. TG-1801 established proof of principle for the bispecific κλ body approach, and Light Chain has six other bispecific candidates coming through the pipeline, developed internally or in collaboration with partners. NI-1801, a follow-on molecule, also contains a CD47-binding light chain and has the same mechanism of action as TG-1801. However, instead of co-binding with CD19, NI-1801 binds to mesothelin. Light Chain anticipates that NI-1801, which is being developed to target a range of solid tumors, will be ready to enter the clinic in 2021. In addition, Light Chain has developed candidates for indications beyond oncology, including NI-2101 for Takeda, which targets factor IX and factor X for the treatment of hemophilia. «Our dual targeting strategy has the potential of combining CD47 inhibition with an improved safety and pharmacokinetic profile, allowing for more drug to reach and target the tumor» Walter Ferlin, CSO, Light Chain Bioscience “Emerging clinical data put CD47 under the spotlight. Our dual targeting strategy has the potential of combiningCD47 inhibition with an improved safety and pharmacokinetic profile, allowing for more drug to reach and target the tumor,” said Walter Ferlin, CSO of Light Chain Bioscience. Light Chain is also developing T cell retargeting therapies using bispecific antibodies. This approach was first validated by the approval of Blincyto (blinatumomab; Amgen) for the treatment of refractory acute lymphoblastic leukemia. Since then, T cell retargeting has been widely developed and represents one of the main applications of bispecific antibodies in oncology. This mechanism of action can readily be achieved with bodies and several programs are being developed with partners for the treatment of solid cancers. Beyond bispecifics Looking into the future, Light Chain is leveraging a feature of its technology platform that enables the production from a single cell of well-controlled mixtures of monospecific and/or bispecific antibodies. Subsets composed of a few bispecific antibodies can be readily purified using affinity chromatography. The combination of therapeutic modalities is clearly the way forward to achieve responses in cancer patients. As more and more combinations of antibodies are being developed to treat complex diseases, the generation of a product consisting of several mono- or bispecific antibodies represents an attractive possibility for next-generation therapeutics. Today Light Chain seeks partners to work on projects in immuno-oncology and other therapeutic areas. Light Chain would like to hear from companies with the skills and expertise to co-develop internally discovered candidates such as NI-1801 and take them into the clinical stages of development. In addition, Light Chain welcomes discussions with prospective partners who want to draw on Light Chain’s deep well of expertise in bispecific antibodies for CD47 targeting and T cell retargeting, as well as other approaches outside oncology. Next-generation immunotherapy with native bispecific antibodies (PDF Download)

免疫疗法临床1期上市批准

2024-11-22

·Business Wire

B-cell Lymphoma Pipeline Insight 2024, with Comprehensive Insights for 295+ Companies and 300+ Pipeline Drugs - ResearchAndMarkets.com

DUBLIN--( BUSINESS WIRE )--The "B-cell Lymphoma - Pipeline Insight, 2024" clinical trials has been added to ResearchAndMarkets.com's offering. This "B-cell Lymphoma- Pipeline Insight, 2024" report provides comprehensive insights about 295+ companies and 300+ pipeline drugs in B-cell Lymphoma pipeline landscape. It covers the pipeline drug profiles, including clinical and nonclinical stage products. It also covers the therapeutics assessment by product type, stage, route of administration, and molecule type. It further highlights the inactive pipeline products in this space. Report Highlights The companies and academics are working to assess challenges and seek opportunities that could influence B-cell Lymphoma R&D. The therapies under development are focused on novel approaches to treat/improve B-cell Lymphoma. B-cell Lymphoma Emerging Drugs Chapters This segment of the B-cell Lymphoma report encloses its detailed analysis of various drugs in different stages of clinical development, including phase III, II, II/III I, preclinical and Discovery. It also helps to understand clinical trial details, expressive pharmacological action, agreements and collaborations, and the latest news and press releases. B-cell Lymphoma: Therapeutic Assessment This segment of the report provides insights about the different B-cell Lymphoma drugs segregated based on following parameters that define the scope of the report, such as: Major Players in B-cell Lymphoma There are approx. 295+ key companies which are developing the therapies for B-cell Lymphoma. The companies which have their B-cell Lymphoma drug candidates in the most advanced stage, i.e. Phase III include, Denovo BioPharma. The report covers 300+ products under different phases of clinical development like: Late stage products (Phase III) Mid-stage products (Phase II) Early-stage product (Phase I) along with the details of Pre-clinical and Discovery stage candidates Discontinued & Inactive candidates Route of Administration B-cell Lymphoma pipeline report provides the therapeutic assessment of the pipeline drugs by the Route of Administration. Products have been categorized under various ROAs such as Intravenous Subcutaneous Oral Intramuscular Molecule Type Products have been categorized under various Molecule types such as Monoclonal antibody Small molecule Peptide Product Type Drugs have been categorized under various product types like Mono, Combination and Mono/Combination. B-cell Lymphoma: Pipeline Development Activities The report provides insights into different therapeutic candidates in phase II, I, preclinical and discovery stage. It also analyses B-cell Lymphoma therapeutic drugs key players involved in developing key drugs. Pipeline Development Activities The report covers the detailed information of collaborations, acquisition and merger, licensing along with a thorough therapeutic assessment of emerging B-cell Lymphoma drugs. B-cell Lymphoma Report Insights B-cell Lymphoma Pipeline Analysis Therapeutic Assessment Unmet Needs Impact of Drugs B-cell Lymphoma Report Assessment Pipeline Product Profiles Therapeutic Assessment Pipeline Assessment Inactive drugs assessment Unmet Needs Key Questions Current Treatment Scenario and Emerging Therapies: How many companies are developing B-cell Lymphoma drugs? How many B-cell Lymphoma drugs are developed by each company? How many emerging drugs are in mid-stage, and late-stage of development for the treatment of B-cell Lymphoma? What are the key collaborations (Industry-Industry, Industry-Academia), Mergers and acquisitions, licensing activities related to the B-cell Lymphoma therapeutics? What are the recent trends, drug types and novel technologies developed to overcome the limitation of existing therapies? What are the clinical studies going on for B-cell Lymphoma and their status? What are the key designations that have been granted to the emerging drugs? Key Players Lisocabtagene maraleucel Hoffmann-La Roche Nektar Therapeutics Miltenyi Biomedicine AVM Biotechnology Lin BioScience Incyte Corporation ADC Therapeutics Genor Biopharma Beijing InnoCare Pharma Tech Co., Ltd. CARGO Therapeutics Chia Tai Tianqing Pharmaceutical Group Co., Ltd. SystImmune LIBO PHARMA Abclon BeiGene Cellectis Iovance Biotherapeutics, Inc. Guangzhou Excelmab Y-mAbs Therapeutics TG Therapeutics Sutro Biopharma AbbVie Aleta Biotherapeutics Janssen Research & Development Lantern Pharma Beijing Immunochina Medical Science and Technology Bantam Pharmaceutical Lin Bioscience SFA Therapeutics neoX Biotech March Biosciences HUTCHMED Key Products Bristol Myers Squibb Glofitamab NKTR-255 Zamtocabtagene autoleucel MB-CART20.1 AVM0703 LBS-007 Parsaclisib Loncastuximab tesirine GB-241 ICP-248 CRG-022 TQB3702 GNC-038 NM-IL-12 AT101 BGB-16673 UCART20x22 IOV-2001 EX103 CD38-SADA TG-1801 STRO-001 ABBV-319 ALETA-001 JNJ-80948543 LP-284 INS19 CAR-T Cells BTM 3566 LBS-007 SFA-001 NXD07 MB-105 HMPL A067 For more information about this clinical trials report visit https://www.researchandmarkets.com/r/qxd94m About ResearchAndMarkets.com ResearchAndMarkets.com is the world's leading source for international market research reports and market data. We provide you with the latest data on international and regional markets, key industries, the top companies, new products and the latest trends.

临床2期ASCO会议细胞疗法临床1期

2023-07-11

·药融圈

制药巨头垂涎的资产：CD20抗体专家，TG Therapeutics

▲8月03-04日 CMC-China大会 · 限时免费扫码报名中注：本文不构成任何投资意见和建议，以官方/公司公告为准；本文仅作医疗健康相关药物介绍，非治疗方案推荐（若涉及），不代表平台立场。任何文章转载需得到授权。多发性硬化症(multiple sclerosis,MS)是中枢神经系统（CNS）的慢性脱髓鞘疾病，是中枢神经系统最常见的慢性炎症性疾病，包括复发-缓解型多发性硬化（RRMS）患者和持续复发的继发性进行性多发性硬化（SPMS）患者。多发性硬化发生在中枢神经系统，由自身免疫系统攻击髓鞘引起。髓鞘是包裹和保护大脑和脊髓中神经纤维的脂质物。疾病导致的炎症和组织损伤会破坏大脑、视神经和脊髓的正常功能。临床症状表现为极度疲劳、麻木、虚弱、视力困难等。病因尚不明确，可能与遗传、环境、病毒感染等多种因素相关。主要发病年龄在20至40岁，是仅次于创伤的中青年人致残原因，目前尚无治愈性疗法。根据《中国多发性硬化患者综合社会调查报告》统计，中国患病率较低，高纬度高发。高加索人种有着更高的患病率，约50-300/10万人，远高于亚洲人，海外市场空间巨大。药融圈旗下，药融云数据www.pharnexcloud.com显示：2022年12月28日，美国FDA批准TG Therapeutics的CD20单抗Briumvi®（Ublituximab-XIIY）上市，用于治疗复发型多发性硬化症(RMS)，包括成人的临床孤立综合征、复发缓解型疾病和活动性继发性进展性疾病。2023年1月26日，该公司宣布在美国商业推出Briumvi®（Ublituximab-XIIY）。截至2023年3月31日，TG治疗从Briumvi的药品销售中获得了780万美元的收入。2023年6月1日，TG治疗公司宣布，欧盟委员会（EC）已批准Briumvi®（Ublituximab-XIIY）用于治疗患有复发性多发性硬化症（RMS）的成年患者，这些患者的活动性疾病由临床或影像学特征确定。有了这一批准，集中上市许可现在在所有欧盟（EU）成员国、冰岛、挪威和列支敦士登都有效。抗CD20抗体已经改变了复发性多发性硬化症患者的治疗前景在美国，每年约8万患者都会开始首次或转换到新的多发性硬化症治疗；50%以上的患者会选择抗CD20抗体作为一种新的多发性硬化症治疗；大于10万多发性硬化症患者目前正在使用抗CD20抗体。TG治疗公司称，Briumvi有潜力成为美国市场No.1 CD20单抗处方药。该公司董事长兼首席执行官Michael S. Weiss表示：“我们非常高兴欧盟委员会批准Briumvi用于治疗患有多发性硬化症的成年患者。这使我们离为欧洲多发性硬化症患者提供替代治疗方案的目标更近了一步，该治疗方案可以在开始剂量后每6个月输注一小时，我们的目标是在今年晚些时候投入商业使用。”TG Therapeutics公司总裁兼CEO-Michael S.Weiss 公司简介 TG Therapeutics（TGTX）是一家全面整合、处于商业化阶段的生物制药公司，专注于B细胞疾病新疗法的收购、开发和商业化。于1993年在美国特拉华州注册成立，2005年10月上市纳斯达克，截至2023年5月1日，公司拥有237名全职员工。目前公司市值约37亿美元。TG治疗公司已获得美国食品和药物管理局(FDA)批准BRIUMVI(ublituximab-xiiy)用于治疗复发型多发性硬化症(RMS)成年患者，包括成人中的临床孤立综合征、复发-缓解性疾病和活动性继发性进行性疾病，BRIUMVI也是该公司目前唯一上市的产品。该公司正在开发用于B细胞疾病的TG-1701（BTK抑制剂）和TG-1801（抗CD47/CD19双特异性抗体），目前正在进行1期临床试验。三款候选药物 TG治疗公司候选药物的临床试验状态-截至2023年4月01Briumvi（Ublituximab-XIIY）Briumvi旨在实现高效的B细胞低剂量耗竭Briumvi是第一个也是唯一一个获批用于RMS患者的抗CD20单克隆抗体。Briumvi是一款糖工程化单克隆抗体，靶向B细胞表达的CD20抗原上的独特抗原表位。当Briumvi与B细胞结合时，可以引发抗体依赖性细胞毒性（ADCC）和补体依赖性细胞毒性（CDC）等一系列免疫反应以摧毁致病B细胞。这些细胞被认为是导致髓鞘和神经细胞轴突损伤的关键因素。Briumvi的一个独特之处在于通过糖工程化去除了抗体中某些糖分子，显从而著增强Briumvi的效力，尤其是ADCC活性。Briumvi的批准主要基于UltimateI和UltimateII3期试验。每项试验均为独立、全面、随机、多中心、双盲、双模拟、活性对照研究，比较了ublituximab（每6个月静脉滴注1小时，剂量为450mg，随后在4小时内滴注1次150mg，在1小时内滴注15次450mg）与teriflunomide（每日一次口服14mg片剂）对RMS受试者的疗效和安全性/耐受性。这些试验是在FDA的特殊方案评估（SPA）下进行的。最终的I和II试验由医学博士劳伦斯·斯坦曼（Lawrence Steinman）领导，全部招募工作于2018年10月完成，两项研究共招募了约1，100名受试者。2020年12月，该公司宣布了最终I和II试验的积极结果。两项研究均在96周内达到了显著降低ARR的主要终点（每项研究中P<0.005），Briumvi在每项研究中的ARR均<0.10。与teriflunomide相比，在UltimateI和II中分别观察到ARR相对降低约60%和50%。也达到了关键的次要MRI终点。2022年8月22日，《新英格兰医学杂志》（New England Journal of Medicine）发表了最终I和II试验的完整结果。2022年12月28日，TG治疗公司宣布FDA批准Briumvi用于治疗成人RMS，包括临床孤立综合征、复发-缓解型疾病和活动性继发性进展性疾病，主要基于最终I和II3期试验的结果。02TG-1701 (BTK 抑制剂）TG-1701是一种新型的、口服的、共价结合的Bruton酪氨酸激酶（BTK）抑制剂，在体外激酶筛选中对BTK表现出很强的选择性。在B细胞白血病或淋巴瘤患者中，B细胞受体（BCR）信号传导对正常B细胞发育至关重要，并支持恶性B细胞的存活和生长。靶向BTK是BCR信号通路的基本元件，调节B淋巴细胞的存活、活化、增殖和分化，在B细胞恶性肿瘤中显示出显著的疗效和可接受的安全性。该公司目前正在评估TG-1701在B细胞恶性肿瘤患者中的1期、多中心、剂量递增临床试验。关键的次要目标包括药代动力学（PK）、药效学和初步抗癌活性的评估。该试验的数据在2021年美国血液学会（ASH）年会上公布。本品最早由恒瑞医药研发，代号为SHR1459。03TG-1801(抗CD47/抗CD19双特异性单克隆抗体)G-1801是第一类双特异性CD47和CD19抗体。这是第一个同时靶向CD19和CD47的疗法，CD19是一种在B细胞恶性肿瘤中广泛表达的B细胞特异性市场，CD47是健康细胞和肿瘤细胞用来逃避巨噬细胞介导的吞噬作用的“不要吃我”信号。CD47在正常细胞上广泛表达，包括红细胞和血小板。CD19是一种特异性B细胞标记物，在前B细胞个体发育早期表达，直到终末分化为早期浆细胞。大多数B细胞系恶性肿瘤（90%以上）表达CD19，包括非霍奇金淋巴瘤（NHL）、慢性淋巴细胞白血病（CLL）和急性淋巴细胞白血病（ALL）。已经发现在抗CD20mAb治疗后失去CD20表达的肿瘤B细胞维持CD19的表达，使得CD19成为治疗B细胞恶性肿瘤的有吸引力的靶标。2019年第一季度，TG治疗公司开始了TG-1801的1期首次人体剂量递增研究。这项研究正在评估在B细胞淋巴瘤患者中逐步增加TG-1801的剂量。该研究的主要目的是确定推荐的2期剂量，并描述TG-1801的安全性。关键的次要目标是评估TG-1801的药代动力学及其初步抗癌活性。2022年12月，在第64届美国血液学会（ASH）年会暨博览会上公布了这项首次人体1期研究的初步结果。TG-1801单药治疗和与Ublituximab联合治疗耐受性良好，未发现MTD，并在多种复发性或难治性B细胞淋巴瘤中表现出初步疗效。2021年上半年，TG治疗在美国开始了TG-1801的第二个1期研究，以继续优化单药治疗和与Ublituximab联合治疗的剂量，该研究的招募工作仍在进行中。TG治疗公司许可协议合作情况TG治疗与多家公司结成了战略联盟以生产和销售产品，以下是该公司目前主要许可协议合作情况：01BRIUMVI(ublituximab-xiiy)—LFB BiotechnologiesS.A.S，GTC Biotherapeutics，LFB/GTCLLC2012年1月，TG治疗与LFB集团的全资子公司LFB Biotechnologies、GTC Biotherapeutics和LFB/GTCLLC就Ublituximab的开发签订了独家许可协议（LFB许可协议）。根据LFB许可协议的条款，TG治疗获得了开发和商业化Ublituximab的全球独家权利（法国/比利时除外）。截至2022年12月31日，根据LFB许可协议的条款，已支付约2500万美元的里程碑相关费用，其中1200万美元与FDA批准Briumvi相关的里程碑相关。在实现某些监管里程碑后，LFB集团有资格获得约600万美元的未来付款。ILDONG PharmaceuticalCo.Ltd.(ILDONG)2012年11月，TG治疗与ILDONG就Ublituximab在韩国和东南亚的开发和商业化签订了独家（区域内）分许可协议。根据分许可协议的条款，ILDONG已被授予特许权使用费，包括授予分许可的权利，以在韩国、台湾、新加坡、印度尼西亚、马来西亚、泰国、菲律宾、越南和缅甸开发和商业化Ublituximab。到目前为止，ILDONG已经从ILDONG收到了200万美元的预付款，并有资格获得总额高达500万美元的基于销售的里程碑付款，以及Ublituximab净销售额的特许权使用费。02TG-1701（BTK抑制剂）2018年1月，TG治疗与江苏恒瑞签订了一份全球独家许可协议，以获得全球知识产权（不包括亚洲，但包括日本），并研究、开发、制造和商业化含有或包含任何恒瑞Bruton酪氨酸激酶抑制剂（含有TG1701（SHR1459或EBI1459）或TG1702（SHR1266或EBI1266）化合物）的产品。恒瑞有资格在实现某些里程碑后获得总计约3.5亿美元的里程碑付款。2020年7月，TG治疗根据许可协议向恒瑞支付了200万美元，作为里程碑的一部分。03TG-1801（抗CD47/抗CD19双特异性抗体）2018年6月，TG治疗与Novimmune签订了一项合资和许可选择协议，以合作开发和商业化Novimmune的新型一流抗CD47/抗CD19双特异性抗体TG1801（之前为Ni1701）。两家公司将在全球范围内联合开发该产品，重点关注血液B细胞恶性肿瘤领域的适应症。TG治疗是产品开发、制造和商业化的主要责任方。里程碑付款将根据早期临床开发支付，TG治疗将负责该产品的临床开发费用，直至2期临床试验结束，之后公司和Novimmune将共同负责所有开发和商业化费用。TG治疗及Novimmune将各自保留独家选择权，可在开发期间的特定时间行使对TG1801的许可权，在这种情况下，Novimmune有资格获得总额约为1.85亿美元的额外里程碑付款。04UKONIQ（umbralisib）2014年9月，TG治疗行使了向Umbralisib授予全球许可权的选择权，从而与Rhizen Pharmaceuticals，SA（Rhizen）就Umbralisib的开发和商业化达成了独家许可协议（Umbralisib许可）。Rhizen有资格获得批准和基于销售的里程碑付款，总额约为1.75亿美元。05Cosibelimab2015年3月，TG治疗与Checkpoint Therapeutics，Inc.达成全球合作（合作协议）。（Checkpoint）用于开发和商业化Checkpoint在血液恶性肿瘤领域的抗PD-L1和抗GITR抗体研究项目，并可选择获得自身免疫性疾病的权利。根据协议条款，TG治疗将支付总额约为1.1亿美元的开发和销售里程碑付款，并将为净销售额支付低两位数的分级特许权使用费。财务状况自成立以来，TG治疗公司遭受了重大的经营亏损，几乎所有的经营亏损都是由与研发项目有关的成本以及与经营（包括商业化活动）有关的销售、一般和管理成本造成的。截至2023年3月31日，TG治疗公司累计赤字为16亿美元，主要现金来源是私募和公开发行股权证券的收益，以及与Hercules Capital，Inc.签署的贷款和担保协议的收益。截至2023年3月31日，TG治疗公司拥有1.397亿美元的现金和现金等价物以及投资证券。2022财年TG治疗公司产品营收278.5万美元，相较于上一年营收668.9万美元有所减少，原因是该公司此前唯一一款商业化产品UKONIQ于2022年5月自愿退出市场，导致产品净收入减少。2022年TG治疗公司总研发成本1.25亿美元，净亏损1.98亿美元。2023年5月8日，TG治疗公司公布2023年一季度报告。2023Q1 TG治疗公司实现营收780.3万美元，而2022年Q1营收约为200万美元，超出市场预期130.86%；每股收益为-0.28美元，前值为-0.51美元，预期值为-0.37美元，超出市场预期24.32%。研发费用方面，2023Q1总研发费用为1587万美元，而在2022年Q1该值为4804.2万美元。2023年1月，TG治疗公司在FDA批准后开始在美国境内进行BRIUMVI的商业销售。截至2 023年3月31日，该公司从Briumvi的药品销售中获得了780万美元的收入。2023年Q1TG治疗公司经营活动中使用的现金为5990万美元，而上一年同期为6870万美元，经营活动中使用的净现金减少主要是由于与生产和临床试验费用相关的支出减少。此外，2023年Q1该公司融资活动产生的净现金为2520万美元，而2022年Q1融资活动产生的净现金为90万美元。融资活动产生净现金的增加主要是由于在2023年3月31日与Hercules签订的第一修正案中提取了2500万美元的预付款。发展战略作为一家全面整合的商业化生物制药公司，TG治疗专注于B细胞疾病新疗法的收购、开发和商业化，该公司发展战略：在美国成功将治疗复发性多发性硬化症的Briumvi商业化；在Briumvi批准的基础上，评估Briumvi在其他MS适应症和/或其他自身免疫性疾病中的其他用途；继续扩大对B细胞介导疾病的重要机制的产品线；评估潜在的战略合作，以最大限度地提高B细胞定向平台的价值；发展业务的同时，保持“患者至上”的文化。参考：NMPA/CDE；药融云数据，www.pharnexcloud.com；FDA/EMA/PMDA；相关公司公开披露（除标注外，正文图片均来自企业官方）；https://www.tgtherapeutics.comhttps://ir.tgtherapeutics.com/eventshttps://mp.weixin.qq.com/s/fiTXcXjTiJeOQv_mzKBjuQhttps://Briumvi.com/about-Briumvi/see-the-results点分享点点赞点在看

上市批准临床研究

100 项与 TG-1801 相关的药物交易

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研发状态

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适应症	最高研发状态	国家/地区	公司	日期
B细胞恶性肿瘤	临床1期	瑞士	TG Therapeutics, Inc.	2022-01-30
B细胞恶性肿瘤	临床1期	瑞士	NovImmune SA	2022-01-30
慢性淋巴细胞白血病	临床1期	美国	TG Therapeutics, Inc.	2021-04-28
滤泡性淋巴瘤	临床1期	美国	TG Therapeutics, Inc.	2021-04-28
套细胞淋巴瘤	临床1期	美国	TG Therapeutics, Inc.	2021-04-28
边缘区B细胞淋巴瘤	临床1期	美国	TG Therapeutics, Inc.	2021-04-28
纵隔大b细胞淋巴瘤	临床1期	美国	TG Therapeutics, Inc.	2021-04-28
小淋巴细胞淋巴瘤	临床1期	美国	TG Therapeutics, Inc.	2021-04-28
B细胞淋巴瘤	临床1期	澳大利亚	TG Therapeutics, Inc.	2019-03-05

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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


NCT03804996 (FIH Study of TG-1801, ICML2023)	临床1期	B细胞淋巴瘤 CD19+ \| CD47	30	TG-1801 monotherapy	淵廠鏇壓遞膚製遞鏇廠(顧鏇遞獵簾窪鹽選築網) = 窪鬱廠齋鹽鹽鹽製艱獵積淵餘簾遞憲繭襯齋壓 (夢鑰憲壓糧淵夢憲鹽壓 )	积极	2023-06-09
				TG-1801 + ublituximab combination therapy	壓糧構構願艱簾鑰顧顧(選積網淵範網醖壓廠網) = 醖襯鹹顧襯選鹽襯鹽廠憲顧願廠壓顧艱夢淵範 (鏇鹽窪獵築選鹽選獵觸 ) 更多
NCT03804996 (ASH2022) 人工标引	临床1期	B细胞淋巴瘤	30	TG-1801	醖衊範鬱壓蓋衊鏇憲餘(鏇範憲鬱選觸簾醖簾簾) = 1 infusion reaction [500 mg monotherapy], 1 rash [360 mg monotherapy] 簾夢鹽衊醖觸觸網糧膚 (製夢廠觸糧壓淵窪壓範 ) 更多	积极	2022-12-11
				TG-1801+ublituximab