A Single-Arm, Open-Label, Phase I Study to Determine the Safety, Tolerability and Preliminary Efficacy of Obecabtagene Autoleucel in Patients With Severe, Refractory Systemic Lupus Erythematosus

This is a Phase I study of obecabtagene autoleucel (obe-cel), autologous T cells engineered with a chimeric antigen receptor (CAR) targeting CD19, to establish the tolerability, safety, preliminary efficacy, and pharmacokinetics of obe-cel in patients with severe, refractory SLE.

开始日期2024-02-02

申办/合作机构

Autolus Ltd.

NCT06173518 / Recruiting临床1期

A Single-Arm, Open-Label, Multi-Centre, Phase Ib Study Evaluating the Safety and Preliminary Efficacy of AUTO1 in Pediatric Patients With CD19-Positive Relapsed/ Refractory (r/r) B Cell Acute Lymphoblastic Leukemia (B ALL) and Aggressive Mature B Cell Non-Hodgkin Lymphoma (B NHL)

This is a Phase Ib study to evaluate the safety and efficacy of autologous T cells engineered with a chimeric antigen receptor (CAR) targeting CD19 in pediatric patients with relapsed or refractory (r/r) B cell acute lymphoblastic leukemia (B ALL) and r/r B cell Non-Hodgkin lymphoma (B NHL)

开始日期2023-11-16

申办/合作机构

Autolus Ltd.

ACTRN12621000762853 / Recruiting临床1期

Phase I Clinical Trial of MB.CART19.1 CD19 Chimeric Antigen Receptor (CAR)T Cells in Relapsed or Refractory CD19-Positive Haematological Malignancy

开始日期2021-07-21

申办/合作机构

Metro North Hospital & Health Service

100 项与 Obecabatagene autoleucel 相关的临床结果

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100 项与 Obecabatagene autoleucel 相关的转化医学

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100 项与 Obecabatagene autoleucel 相关的专利（医药）

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156

项与 Obecabatagene autoleucel 相关的文献（医药）

2024-12-01·AMERICAN JOURNAL OF HEMATOLOGY

Toxicities and outcome after CD19‐directed chimeric antigen receptor T‐cell therapy for secondary neurolymphomatosis

Article

作者: Choi, Bryan D. ; El‐Jawahri, Areej ; Shankar, Ganesh ; Barnes, Jeffrey A. ; Karschnia, Philipp ; Soumerai, Jacob D. ; Kaulen, Leon D. ; Doubrovinskaia, Sofia ; Dietrich, Jorg ; Abramson, Jeremy S. ; Martinez‐Lage, Maria ; Maus, Marcela V. ; Chen, Yi‐Bin ; Wick, Wolfgang ; Hochberg, Ephraim P. ; Johnson, P. Connor ; Frigault, Matthew J.

Lymphomatous infiltration of the peripheral nervous system (PNS), termed neurolymphomatosis, represents a distinct extranodal non-Hodgkin lymphoma variant with dismal outcome. CD19-directed chimeric antigen receptor (CD19-CAR) T-cell therapy has emerged as a safe and effective treatment for B-cell lymphomas. We aimed to assess toxicity and efficacy of CD19-CAR T-cells in neurolymphomatosis. Neurolymphomatosis patients treated with CD19 CAR T-cells were retrospectively identified at Massachusetts General Hospital over a six-year period. Toxicities were graded according to the ASTCT classification, management, and response rates were recorded. Eleven neurolymphomatosis patients were identified with a median of 2 lines of PNS-directed treatments (range: 1-3) prior to receiving CD19-CAR T-cells. Neurolymphomatosis localized to the nerve roots (8/11, 73%), plexus (5/11, 45%), peripheral (4/11, 36%) and cranial nerves (5/11, 45%). Low grade cytokine release syndrome (CRS) was detected in 8/11 (73%; grade 1: N = 7; grade 2: N = 1) cases. Low- and high-grade immune cell-associated neurotoxicity syndrome (ICANS) were recorded in 5/11 (45%; grade 1: N = 4; grade 2: N = 1) and 1/11 (9%; grade 4) patients, respectively. CRP levels at infusion were predictive of ICANS (area under the curve: 0.96, p = 0.01). Seven of eleven neurolymphomatosis patients (64%) responded to CD19-CAR T-cells. Complete remissions (CR) were achieved in three cases (27%), with 2 patients in sustained CR nine and 46 months after CD19-CAR infusion. Median progression-free survival (PFS) was 4 months. Collectively, CD19-CAR T-cell treatment was well tolerated and showed promising efficacy in recurrent neurolymphomatosis, a difficult to treat condition with unmet medical need. Findings suggest that CD19-CAR may sufficiently penetrate the blood-nerve barrier. Toxicity and outcomes were overall similar to CAR-T cell therapy in CNS lymphoma.

2024-12-01·Current Research in Translational Medicine

Point of care CD19 chimeric antigen receptor (CAR) T-cells for relapsed/refractory acute myeloid leukemia (AML) with aberrant CD19 antigen expression

Article

作者: Danylesko, Ivetta ; Shimoni, Avichai ; Nagler, Arnon ; Yerushalmi, Ronit ; Jacoby, Elad ; Shem-Tov, Noga ; Itzhaki, Orit ; Toren, Amos ; Avigdor, Abraham ; Shouval, Roni

Relapsed/refractory (r/r) acute myeloid leukemia (AML) is associated with poor prognosis. CD19 is a B-cell marker, is aberrantly expressed in AML, mostly with t(8; 21)(q22; q22.1). Here we report the results of a phase 2 study giving point of care produced CD19 CAR T- cells for r/r AML with aberrant expression of CD19 (NCT04257175). Lymphodepletion included fludarabine and cyclophosphamide The response was evaluated by bone marrow (BM) aspiration on day 28. Six patients (5 adults and 1 child) were included. Median number of previous chemotherapy lines was 4 (range, 3-8) and four patients received CAR T-cells 8-18 months post allogeneic hematopoietic stem cell transplantation (allo-HSCT). Cytokine release syndrome (CRS) of any grade occurred in all patients, and 1 patient had grade 3 CRS. Immune effector cell-associated neurotoxicity syndrome (ICANS) occurred in 2 patients at low grades. Tocilizumab was administered to 2 patients and corticosteroids to 3 patients. Four patients achieved a complete remission (CR), while 2/6 progressed (PD). Three patients (2 with CR and 1 with PD) underwent allo-HSCT (it was the second transplant in 2) 2-5 months post CAR T-cells infusion. The median duration of response in patients achieving CR was 8.5 (range; 3-14) months. However, all patients eventually died within 5 (1-18) months. In conclusion, CD19 CAR T- cell treatment for AML is feasible and safe. However, the response is short and should be followed by allo-HSCT. Hopefully, future long term results will be improved by combining the CAR T- cell therapy with the emerging novel effective anti-leukemic compounds.

2024-09-01·MedComm

Targeting chronic lymphocytic leukemia with B‐cell activating factor receptor CAR T cells

Article

作者: Dronca, Roxana ; Qin, Hong ; Gadd, Martha E. ; To, Tommy ; Kharfan‐Dabaja, Mohamed A. ; Qie, Yaqing ; Shao, Qing ; Murthy, Hemant S. ; Yassine, Farah ; Liu, Andrew ; Luo, Yan ; Rivera‐Valentin, Rocio ; Li, Shuhua

Abstract:

The challenge of disease relapsed/refractory (R/R) remains a therapeutic hurdle in chimeric antigen receptor (CAR) T‐cell therapy, especially for hematological diseases, with chronic lymphocytic leukemia (CLL) being particularly resistant to CD19 CAR T cells. Currently, there is no approved CAR T‐cell therapy for CLL patients. In this study, we aimed to address this unmet medical need by choosing the B‐cell activating factor receptor (BAFF‐R) as a promising target for CAR design against CLL. BAFF‐R is essential for B‐cell survival and is consistently expressed on CLL tumors. Our research discovered that BAFF‐R CAR T‐cell therapy exerted the cytotoxic effects on both CLL cell lines and primary B cells derived from CLL patients. In addition, the CAR T cells exhibited cytotoxicity against CD19‐knockout CLL cells that are resistant to CD19 CAR T therapy. Furthermore, we were able to generate BAFF‐R CAR T cells from small blood samples collected from CLL patients and then demonstrated the cytotoxic effects of these patient‐derived CAR T cells against autologous tumor cells. Given these promising results, BAFF‐R CAR T‐cell therapy has the potential to meet the long‐standing need for an effective treatment on CLL patients.

160

项与 Obecabatagene autoleucel 相关的新闻（医药）

2024-11-14

·PRNewswire

Kyverna Therapeutics Announces New Patient Data Highlighting Potential of KYV-101 for Treatment of Lupus Nephritis in Symposium at ACR Convergence 2024

Positive Sustained Efficacy and Durability at >6-month Follow-Up Observed in Patients With Severe Lupus Nephritis (LN) Treated With KYV-101 Target Dose KYV-101 Treatment Continues to Demonstrate Robust Safety and Tolerability With No High-Grade CRS or ICANS Observed EMERYVILLE, Calif., Nov. 14, 2024 /PRNewswire/ -- Kyverna Therapeutics, Inc. (Kyverna), a clinical-stage biopharmaceutical company focused on developing cell therapies for patients with autoimmune diseases, announces today that it will present updated clinical data from LN patients treated with KYV-101 in ongoing Kyverna-sponsored KYSA-1 and KYSA-3 Phase 1/2 studies and named patient treatments. Kyverna, alongside leading academic collaborators, will highlight all six patients treated with the target dose of 1×108 CD19 CAR T cells, four of which have at least six months of follow-up. All patients at six months of follow-up after treatment at the target dose continue to display sustained efficacy and durability across numerous key clinical measures. These updates will be presented at a company symposium titled, "KYV-101 Anti-CD19 CAR T-Cell Therapy: The Future of Autoimmune Disease Treatment," to be held at 5:45 pm ET on November 18, 2024. Slides from the presentation will be posted to the company website following the symposium. "Lupus nephritis patients encounter a tremendous burden of disease associated with high morbidity and mortality, with up to 30% of patients ultimately experiencing end-stage renal disease that requires dialysis or kidney transplant," said Prof. Georg Schett, M.D. from the Friedrich-Alexander-University in Erlangen, Germany, and one of the presenters. "The data reinforce that treatment with KYV-101 drives deep B cell depletion in patients with LN, and appears to reset the immune system, stabilize eGFR, preserve kidney function and enable clinical improvement in SLE activity. Notably, this clinical benefit is occurring while also eliminating immunosuppressants and reducing glucocorticoids to physiologic levels with a manageable safety profile." "As our KYV-101 clinical datasets mature, we are increasingly able to focus on the right patients, treated at the right dose, with the right protocol. We are excited to share these new data, which continue to reinforce KYV-101's potential for durable and life-changing outcomes in lupus nephritis patients, including those with high chronicity and disease severity," said Warner Biddle, Chief Executive Officer at Kyverna. Additional Updates: Also at ACR Convergence 2024, Kyverna will present data on next-generation approaches, most notably with a poster on Ingenui-T, the Company's preclinical 3-day manufacturing process using autologous whole blood as starting material. Ingenui-T is designed to improve the patient experience by eliminating apheresis, leading to a potential for improved convenience, access and overall cost reduction. As the poster highlights, drug product from the Ingenui-T process manufactured with whole blood from patients with SLE or healthy donors displayed product characteristics similar to KYV-101. In addition, results from collaborative work on the molecular mechanisms underlying immune reset through deep B-cell depletion with CD19 CAR T-cell therapy performed in collaboration with Verily Life Sciences, an Alphabet precision health company, and the University of Erlangen will be shared as an oral presentation. The posters and slides from the oral presentation at ACR Convergence 2024 will be available on the publications page of Kyverna's website. About Lupus Nephritis (LN) Lupus nephritis (LN) is a serious complication of systemic lupus erythematosus (SLE), more commonly known as lupus. Approximately 40 percent of adults diagnosed with lupus eventually develop LN and 60 percent or more of LN patients will fail standard of care and approved treatments1,2. Aside from modest efficacy, current treatments expose these young adults to the well-demonstrated detrimental consequences of chronic treatment with corticosteroids and other powerful immunosuppressants. Up to 30 percent of patients with LN will develop kidney failure, requiring dialysis or a kidney transplant to stay alive3 . About KYV-101 KYV-101 is an autologous, fully human CD19 CAR T-cell product candidate for use in B cell-driven autoimmune diseases. The CAR in KYV-101 was designed by the National Institutes of Health (NIH) to improve tolerability and tested in a 20-patient Phase 1 trial in oncology. Results were published by the NIH in Nature Medicine4. KYV-101 is currently being evaluated in sponsored, open-label, Phase 1/2 and Phase 2 trials in the United States and Germany across two broad areas of autoimmune diseases, rheumatologic and neuroinflammatory, as well as in investigator-initiated trials for multiple indications in multiple geographies. The clinical experience to date with KYV-101 in both oncological and autoimmune diseases highlights the differentiated properties of KYV-101 and the potential to treat autoimmune patients. About Kyverna Therapeutics Kyverna Therapeutics, Inc. (Nasdaq: KYTX) is a patient-centered, clinical-stage biopharmaceutical company focused on developing cell therapies for patients suffering from autoimmune diseases. Our lead CAR T-cell therapy candidate, KYV-101 is advancing through clinical development with sponsored clinical trials across two broad areas of autoimmune disease: rheumatology and neurology, including Phase 2 trials for stiff-person syndrome, multiple sclerosis and myasthenia gravis, a Phase 1/2 trial for systemic sclerosis, and two ongoing multi-center Phase 1/2 trials in the United States and Germany for patients with lupus nephritis. Kyverna's pipeline includes next-generation CAR T-cell therapies in both autologous and allogeneic formats with properties intended to be well suited for use in B cell-driven autoimmune diseases. For more information, please visit . Forward-Looking Statements Statements in this press release about future expectations, plans and prospects, as well as any other statements regarding matters that are not historical facts, may constitute "forward-looking statements." The words, without limitation, "anticipate," "believe," "continue," "could," "estimate," "expect," "intend," "may," "plan," "potential," "predict," "project," "should," "target," "will," "would" and similar expressions are intended to identify forward-looking statements, although not all forward-looking statements contain these or similar identifying words. Forward-looking statements in this press release include, without limitation, those related to: the potential impact of the clinical outcomes from the ongoing clinical programs; the potential impact of the new data on the treatment efficacy and safety profile of KYV-101; the potential that the results of the ongoing trials could drastically change the treatment landscape for the targeted autoimmune diseases; Kyverna's goals to develop certain paradigm-shifting treatment options; the potential for KYV-101 to provide durable, immunosuppressant-free remission for autoimmune disease patients; Kyverna's beliefs about the differentiated properties of KYV-101; and Kyverna's clinical trials and named-patient activities. Actual results may differ materially from those indicated by such forward-looking statements as a result of various important factors, including: uncertainties related to market conditions, and other factors discussed in the "Risk Factors" section of Kyverna's most recent Annual Report on Form 10-K and Quarterly Reports on Form 10-Q that Kyverna has filed or may subsequently file with the U.S. Securities and Exchange Commission. Any forward-looking statements contained in this press release are based on the current expectations of Kyverna's management team and speak only as of the date hereof, and Kyverna specifically disclaims any obligation to update any forward-looking statement, whether as a result of new information, future events or otherwise. Contact: Consort Partners for Kyverna: [email protected] Investors: [email protected] Media: [email protected] 1Anders et al., Nat Rev Dis Primers. 2020; 6:7. 2Parodis et al., Autoimmun Rev. 2024; 23:103418. 3Lateef and Petri, Arthritis Res & Ther. 2012; 14(Suppl 4):S4. 4Brudno et al., Nature Medicine. 2020; 26:270-280. SOURCE Kyverna Therapeutics WANT YOUR COMPANY'S NEWS FEATURED ON PRNEWSWIRE.COM? 440k+ Newsrooms & Influencers 9k+ Digital Media Outlets 270k+ Journalists Opted In GET STARTED

细胞疗法临床1期临床2期免疫疗法临床结果

2024-11-13

·药渡

又一款CAR-T疗法，获批

近日，Autolus Therapeutics（以下简称“Autolus”）公司宣布，其自主研发的创新CD19靶向CAR-T疗法Aucatzyl（商品名，通用名为obecabtagene autoleucel或obe-cel）已成功获得美国FDA的上市批准，用于治疗复发或难治性B细胞急性淋巴细胞白血病（r/r B-ALL）的成年患者。这也是FDA批准的第五款CD19 CAR-T疗法。是新一代靶向CD19的CAR-T疗法据了解，Aucatzyl作为一种自体来源、针对CD19的CAR-T细胞治疗产品，其独特设计在于拥有较快的靶点解离速率，这一特性旨在减轻工程化T细胞的过度活化状态，使其行为更接近自然状态下的T细胞，同时增强了其持续杀伤目标细胞的能力。该疗法的获批依据主要来自于FELIX临床试验的数据支持。在该试验中，共有94名患者接受了至少一次Aucatzyl的输注治疗，其中65例患者在治疗前骨髓中原始细胞比例超过5%，并因此被纳入疗效评估。在这65名可评估疗效的患者中，有63%的患者实现了总体完全缓解（OCR），具体包括51%的完全缓解（CR）和12%的带有部分血液学恢复的完全缓解（CRi）。同时，有42%的患者在3个月内即达到完全缓解，且中位缓解持续时间（DOR）长达14.1个月。不过，Aucatzyl的药品说明书上特别标注了FDA发布的最高级别安全警示——“黑框警告”，明确指出使用该药品可能伴随一系列严重风险，包括细胞因子释放综合征（CRS）、免疫效应细胞相关神经毒性综合征（ICANS）以及T细胞恶性肿瘤。具体来说，有75%的患者在使用过程中出现了CRS（其中3%达到3级严重程度），64%的患者遭遇了神经系统毒性反应（其中12%达到或超过3级），而ICANS的发生率也达到了24%（其中7%为≥3级）。这些数据强调了在使用Aucatzyl时必须高度关注其潜在的安全性问题。另值得一提的是，Aucatzyl的定价也是目前全球获批CAR-T细胞治疗产品中最高的，达52.5万美元。部分CAR-T疗法前三季度销售业绩披露截止目前，在全球范围内，已有超10款CAR-T疗法获批上市，靶点均为CD19或BCMA。日前，随着各大药企相继发布2024年Q3业绩报，部分CAR-T疗法今年前三个季度的成绩单也相应出炉。全球范围内获批上市的CAR-T疗法其中，吉利德两款CAR-T疗法Yescarta和Tecartus第三季度的销售业绩分别为3.87亿美元和0.98亿美元，分别环比下降7%和8%，吉利德方面表示，销售额的下降反映了美国境内和境外竞争激烈，预计这种竞争将持续到2025年，公司将与政府机构和医疗保健协会合作，继续专注于扩大Yescarta、Tecartus的总体使用率。不过，今年前三个季度，Yescarta和Tecartus共计总销售额为14.86亿美元，同比增长了6%。同样手握两款CAR-T疗法的百时美施贵宝则迎来了更好的发展的态势，其靶向CD19的CAR-T疗法Breyanzi第三季度全球销售业绩为2.24亿美元，同比增长143%，靶向BCMA的CAR-T疗法Abecma全球销售业绩为1.24亿美元，同比增长40%，两款产品在第三季度合计为百时美施贵宝贡献了3.48亿美元的业绩收入。较早公布第三季度的强生，其与传奇生物合作开发的CAR-T疗法在2024年Q3销售额达到2.86亿美元，同比增长87.7%。加上第一季度1.57亿美元和第二季度1.86亿美元的销售业绩，今年前三季度，Carvykti的累计销售收入为6.29亿美元，同比增长84.3%。业内预计，Carvykti有望在2024年冲击10亿美元销售大关，迈入重磅炸弹药物行列。再看看国内获批上市的CAR-T疗法方面，截止目前，国内已经有6款CAR-T疗法获批，分别是复星凯特的阿基仑赛、药明巨诺的瑞基奥仑赛、合源生物的纳基奥仑赛、科济药业的泽沃基奥仑赛、驯鹿生物的伊基奥仑赛和传奇生物的西达基奥仑赛，但并未有更多详细的业绩披露。此外，在上个月的2024年国家医保药品目录调整谈判中，此前通过形式审阿基仑赛、瑞基奥仑赛、纳基奥仑赛以及泽沃基奥仑赛全部止步于形式审查，没有通过专家评审，没有进入国谈的现场谈判环节。而在此前三次医保谈判中，CAR-T药物都受制于医保谈判“50万不谈，30万不进”规则，最后都未走上谈判桌。文 | 医谷药渡媒体商务合作媒体公关 | 新闻&会议发稿张经理：18600036371（微信同号）点击下方“药渡“，关注更多精彩内容免责声明 “药渡”公众号所转载该篇文章来源于其他公众号平台，主要目的在于分享行业相关知识，传递当前最新资讯。图片、文章版权均属于原作者所有，如有侵权，请及时告知，我们会在24小时内删除相关信息。微信公众号的推送规则又双叒叕改啦，如果您不点个“在看”或者没设为"星标"，我们可能就消散在茫茫文海之中~点这里，千万不要错过药渡的最新消息哦！👇👇👇

细胞疗法上市批准免疫疗法临床结果ASH会议

2024-11-13

·生物制药小编

第N款CAR-T，你为啥这么贵？

昨日，Autolus Therapeutics宣布，美国FDA已经批准Aucatzyl（obecabtagene autoleucel，obe-cel），用于治疗复发性/难治性成人B细胞急性淋巴细胞白血病（r/r B-ALL）的成人患者。延伸阅读：“连环杀手”CAR-T即将上市，向Tecartus发起挑战 Aucatzyl是美国FDA批准的第五款CD19 CAR-T，其获批适应症与吉利德的Tecartus完全对上。而且根据报道，Aucatzyl的定价为52.5万美元，比Tecartus的价格要高上一大截，作为一款后发的药物，凭啥定更高的价。另外，52.5万美元/剂的Aucatzyl是目前全球获批CAR-T细胞治疗产品中，单价最高的一位。（CAR-T价格目录在文末）更高的安全性 Autolus一直以来，都以“更高的安全性”作为Aucatzyl的卖点。在一个电话会议上，Autolus的首席运营官Christopher Vann对于Aucatzyl的价格高于Tecartus这样解释道：“我们相信，这一定价反映了我们迄今为止观察到的临床证据和益处，以及差异化的安全性，这为医疗保健系统带来了有意义的经济益处。” Aucatzyl是一款自体的、靶向CD19的CAR-T细胞疗法，其被设计为具有快速的靶点解离率（target binding off-rate），以减少工程化T细胞的过度激活，被设计的更类似天然存在的T细胞，同时能够提高对目标细胞的连续杀伤能力。 Aucatzyl的批准是基于FELIX临床研究结果，94名患者接受了至少一次Aucatzyl输注，其中65例患者在筛查和清淋前骨髓中原始细胞>5%，接受了合格产品后具有了可评估的疗效。在疗效可评估的患者中（n=65），63%的患者达到了总体完全缓解（OCR），包括51%的CR和12%的CRi。主要疗效指标为3个月内完全缓解，42%的患者达到，中位缓解持续时间（DOR）为14.1个月。 Aucatzyl显示低水平的细胞因子释放综合征（CRS），有3%的3级事件，无4级或5级事件。7%的患者报告了≥3级免疫效应细胞相关神经毒性综合征（ICANS）。FDA没有对Aucatzyl的REMS要求。Aucatzyl的安全性包括对CRS、神经毒性和继发性血液系统恶性肿瘤的黑框警告。值得注意的是，Aucatzyl是第一个被批准的无需风险评估缓解策略（REMS）的CAR-T疗法。REMS是美国FDA为管理某些药品或生物制品（特别是CAR-T）的已知或潜在严重风险，而要求制药公司制定并实施的一系列措施和干预手段，旨在帮助减少特定严重不良事件的发生或严重程度，确保治疗益处大于风险，并安全有效地使用。令人担忧的销售前景尽管Autolus在吹捧Aucatzyl的安全性和疗效。以及扩大Aucatzyl在全球市场的批准。目前，欧盟和英国的监管机构正在审查obe-cel的上市申请。但是小编仍然不看好Aucatzyl的销售前景。首先，作为Tecartus的竞争对手，Aucatzyl在市场优先性、治疗网点、价格上都没有优势，疗效也差不多，只有安全性突出一些。其次，Tecartus自2021年获得第二个批准用于治疗B-ALL，经历了近4年的销售增长，也来到了瓶颈期，卖不太动了。根据吉利德财报，Tecartus的2024Q3单季度销售额为9800万美元，同比增长2%，环比下滑近9%。说明B-ALL这个市场份额基本上已经被Tecartus消耗的差不多了，这时候Aucatzyl才入局。小编还是不太看好Aucatzyl的销售前景。延伸阅读：低价CAR-T 如有错漏，欢迎留言补充参考资料： 1.https://www.globenewswire.com/news-release/2024/11/08/2977884/0/en/Autolus-Therapeutics-Announces-FDA-Approval-of-AUCATZYL-obecabtagene-autoleucel-obe-cel-for-adults-with-relapsed-refractory-B-cell-acute-lymphoblastic-leukemia-r-r-B-ALL.html 2.https://www.biopharmadive.com/news/autolus-fda-approval-aucatzyl-obe-cel-car-t/732543/ · · · · ·

细胞疗法免疫疗法临床结果ASH会议上市批准

100 项与 Obecabatagene autoleucel 相关的药物交易

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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
前体B细胞急性淋巴细胞白血病	美国	Autolus Ltd.	2024-11-08

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
复发性 B 细胞急性淋巴细胞白血病	申请上市	美国	Autolus Therapeutics Plc	2023-11-29
难治性 B 细胞急性淋巴细胞白血病	申请上市	美国	Autolus Therapeutics Plc	2023-11-29
系统性红斑狼疮	临床1期	西班牙	Autolus Ltd.	2024-02-02
系统性红斑狼疮	临床1期	英国	Autolus Ltd.	2024-02-02
侵袭性 B 细胞非霍奇金淋巴瘤	临床1期	美国	Autolus Ltd.	2023-11-16
侵袭性 B 细胞非霍奇金淋巴瘤	临床1期	西班牙	Autolus Ltd.	2023-11-16
侵袭性 B 细胞非霍奇金淋巴瘤	临床1期	英国	Autolus Ltd.	2023-11-16
伯基特淋巴瘤	临床1期	美国	Autolus Ltd.	2023-11-16
伯基特淋巴瘤	临床1期	西班牙	Autolus Ltd.	2023-11-16
伯基特淋巴瘤	临床1期	英国	Autolus Ltd.	2023-11-16

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临床结果

适应症

分期

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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


ASH2024	N/A	复发性 B 细胞急性淋巴细胞白血病	-	Obecabtagene autoleucel (obe-cel) (High-risk HT score)	範積壓窪選窪膚觸積網(選憲積醖糧網艱網淵願) = 範夢壓糧窪窪憲窪鏇願鏇鹹醖衊範淵願憲鬱襯 (鹽淵糧構廠顧範壓糧鏇, 34.6 ~ 55.6) 更多	-	2024-12-09
				Obecabtagene autoleucel (obe-cel) (Low-risk HT score)	範積壓窪選窪膚觸積網(選憲積醖糧網艱網淵願) = 膚顧鹽糧鏇範襯範顧獵鏇鹹醖衊範淵願憲鬱襯 (鹽淵糧構廠顧範壓糧鏇, 40.2 ~ 82.1) 更多
NCT04404660 (FELIX, ASH2024)	临床1/2期	复发性成人急性淋巴细胞白血病 ClonoSEQ®next-generation sequencing (NGS) assay	127	Obe-cel	鹹網蓋遞鬱繭夢選鬱鑰(鏇網壓鬱網構廠鏇齋鬱) = 夢範夢構窪獵鑰膚鏇夢齋齋糧夢繭糧築膚繭鹹 (廠鏇顧鬱獵糧醖壓齋餘 ) 更多	积极	2024-12-09
NCT04404660 (FELIX, ASH2024)	临床1/2期	复发性成人急性淋巴细胞白血病 CD19	127	Obecabtagene autoleucel (obe-cel)	窪衊衊願鏇積鬱齋鏇簾(願夢簾餘簾簾網壓獵鑰) = 72 (70.6%) were CRS only 鹽鬱遞觸積醖顧糧遞襯 (顧艱鏇網網鏇膚願簾糧 ) 更多	积极	2024-12-09
ASH2024	N/A	复发性成人急性淋巴细胞白血病	-	Bridging Therapies with Inotuzumab Ozogamicin (INO)	艱築繭鹹築顧膚製壓積(鬱積選觸鹽鑰獵選願遞) = 積憲糧壓醖壓襯襯鏇獵選膚鹽構繭簾膚鹹範憲 (醖蓋顧顧衊窪壓積醖網, 4.1 ~ NE) 更多	-	2024-12-08
				Bridging Therapies without Inotuzumab Ozogamicin (INO)	艱築繭鹹築顧膚製壓積(鬱積選觸鹽鑰獵選願遞) = 蓋壓鹹齋膚衊構選願衊選膚鹽構繭簾膚鹹範憲 (醖蓋顧顧衊窪壓積醖網, 6.0 ~ 15.0) 更多
NCT04404660 (FELIX, FDA_CBER) 人工标引	临床1/2期	前体B细胞急性淋巴细胞白血病	112	AUCATZYL (Efficacy Evaluable)	壓膚繭壓遞鹹襯淵遞艱(襯艱簾觸艱遞淵窪遞製) = 壓蓋鏇願鹹願衊觸襯選繭壓廠餘網選繭窪壓鏇 (鬱鹹願膚獵鬱餘糧築艱, 50 ~ 75) 更多	积极	2024-11-08
				AUCATZYL (All Leukapheresed)	壓膚繭壓遞鹹襯淵遞艱(襯艱簾觸艱遞淵窪遞製) = 襯艱艱顧顧艱築餘顧積繭壓廠餘網選繭窪壓鏇 (鬱鹹願膚獵鬱餘糧築艱, 44 ~ 63) 更多
NCT04404660 (FELIX, ASCO2024) 人工标引	临床1/2期	复发性 B 细胞急性淋巴细胞白血病 \| 难治性 B 细胞急性淋巴细胞白血病 CD19 binder	127	Obe-cel	選鏇鑰夢獵獵壓選網觸(襯構鏇糧壓網鹹願鏇衊) = Pts who experienced B-cell recovery had a hazard risk of relapse or death 1.7 times compared with pts without B-cell recovery 廠簾鬱鏇獵膚積繭夢廠 (鬱鹹積鑰築鑰鑰糧憲鏇 ) 更多	积极	2024-05-24
				Obe-cel (with censoring for consolidative SCT or new therapies)
NCT04404660 (FELIX, EHA2024) 人工标引	临床1/2期	前体B细胞急性淋巴细胞白血病	127	Obecabtagene autoleucel (obe-cel)	艱簾蓋糧窪艱糧醖觸夢(糧獵膚製築積廠襯選鹽) = 願簾艱齋艱餘鹹積遞繭齋醖艱鏇醖鏇顧遞築網 (衊夢簾糧願遞醖鏇築醖 ) 更多	积极	2024-05-23
NCT04404660 (FELIX, EHA2024) 人工标引	临床1/2期	复发性成人急性淋巴细胞白血病 \| 难治性成人急性淋巴细胞白血病	127	OBECABTAGENE AUTOLEUCEL (Bridging therapy with INO)	選窪憲顧鹹艱廠憲艱簾(觸齋齋觸糧構獵餘鹽獵) = 選夢繭艱膚衊蓋範顧餘製糧觸衊餘網糧觸襯製 (鹽襯鑰繭壓範選鏇餘窪, 4.1 ~ NE) 更多	积极	2024-05-14
				OBECABTAGENE AUTOLEUCEL (Bridging therapy without INO)	選窪憲顧鹹艱廠憲艱簾(觸齋齋觸糧構獵餘鹽獵) = 構觸鹽廠夢顧鹽憲齋淵製糧觸衊餘網糧觸襯製 (鹽襯鑰繭壓範選鏇餘窪, 6.0 ~ NE) 更多
NCT04404660 (FELIX, EHA2024)	临床1/2期	难治性 B 细胞急性淋巴细胞白血病 CD19 chimeric antigen receptor (CAR)	127	OBECABTAGENE AUTOLEUCEL	蓋鹹獵網鬱醖鏇壓積糧(衊廠艱蓋艱餘夢糧糧膚) = 範醖廠鹽網構繭繭選憲積範糧廠築繭選簾繭襯 (顧構繭觸觸鹹糧餘憲齋 )	积极	2024-05-14
				OBECABTAGENE AUTOLEUCEL	蓋鹹獵網鬱醖鏇壓積糧(衊廠艱蓋艱餘夢糧糧膚) = 選選窪鹽窪鹽繭願觸繭積範糧廠築繭選簾繭襯 (顧構繭觸觸鹹糧餘憲齋 )
FELIX (ASH2023)	N/A	-	90	Obe-cel	憲鹽壓鏇鹽醖膚憲醖築(襯蓋鹽鬱製鹹壓壓窪淵) = 糧簾簾艱襯襯願築艱廠鏇夢襯襯衊鹹繭構選築 (鹽製鑰範鬱簾遞膚衊範 ) 更多	-	2023-12-11