预约演示

更新于：2026-04-21

Durvalumab

度伐利尤单抗

更新于：2026-04-21

概要

基本信息

药物类型

单克隆抗体

别名

Durvalumab (Genetical Recombination)、Durvalumab (genetical recombination) (JAN)、Durvalumab (USAN/INN)

+ [10]

靶点

PDL1

作用方式

抑制剂

作用机制

PDL1抑制剂(程序性死亡配体1抑制剂)

治疗领域

肿瘤消化系统疾病呼吸系统疾病+ [11]

在研适应症

胃食管交界处腺癌胃癌早期胃癌+ [190]

非在研适应症

急性髓性白血病肺腺癌前列腺腺癌+ [83]

原研机构

在研机构

+ [17]

非在研机构

Fred Hutchinson Cancer Research Center

AVEO Pharmaceuticals, Inc.

Plexxikon, Inc.

+ [7]

权益机构

MedImmune Pharma BV

Ultimovacs ASAVall d'Hebron Institut d'Oncologia

+ [14]

最高研发阶段批准上市

首次获批日期

美国 (2017-05-01),

尿路上皮癌

最高研发阶段(中国)批准上市

特殊审评优先审评 (美国)、突破性疗法 (美国)、加速批准 (美国)、孤儿药 (美国)、孤儿药 (日本)、优先审评 (澳大利亚)、孤儿药 (澳大利亚)

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结构/序列

Sequence Code 10069506H

来源: *****

Sequence Code 13384675L

来源: *****

关联

897

项与度伐利尤单抗相关的临床试验

NCT07507968

/ Not yet recruiting临床2期IIT

Total Neoadjuvant Treatment With Preoperative FLOT/Durvalumab Plus Postoperative Durvalumab for Resectable Gastroesophageal Adenocarcinoma

This trial is designed to evaluate a total neoadjuvant approach using D-FLOT as the new standard backbone in patients with resectable esophagogastric adenocarcinoma. It addresses major limitations of current treatment paradigms, builds directly on the strong clinical signal from the MATTERHORN trial, and offers a rational, biologically sound framework for future therapy intensification and innovation.
By moving systemic therapy entirely into the preoperative phase, we aim to:
* Improve patient outcomes through better adherence and deeper response
* Minimize postoperative therapy-related dropout
* Create a platform for rational post-surgical drug testing and individualized treatment escalation The trial will provide pivotal evidence to guide the next generation of curative-intent treatment strategies for EGA.

开始日期2026-07-01

申办/合作机构

AstraZeneca PLC

NCT05403723

/ Suspended临床1期IIT

A Phase 1b Trial of Adaptive Stereotactic Body Radiotherapy in Combination With Durvalumab (MEDI4736), Platinum, and Etoposide in Extensive Stage Small Cell Lung Cancer

This is trial studying the safety of adaptive stereotactic body radiotherapy (SBRT) combined with durvalumab immunotherapy, platinum chemotherapy, and etoposide chemotherapy in platinum refractory extensive stage small cell lung cancer (SCLC).

开始日期2026-06-30

申办/合作机构

University of Maryland Baltimore

[+1]

NCT07339059

/ Recruiting临床2期IIT

Phase II Study of Sacituzumab Govitecan With Atezolizumab/Durvalumab as Maintenance Therapy for Extensive-Stage Small Cell Lung Cancer

The goal of this clinical trial is to learn if the combination of sacituzumab govetican (SG) and atezolizumab/durvalumab is effective in controlling cancer tumor growth in adults with extensive stage small cell lung cancer. These drugs are FDA approved individually in different cancers. This combination is evaluated in breast cancer and showed promising combination.
The effectiveness of this treatment combination will be measured by changes in tumor size and appearance of new tumors.
Participants in the trial will:
* receive treatment SG and immunotherapy every 21 days for up to 2 years or until it is no longer works for the patient.
* CT scans at 6weeks for first 6 cycles and then every 9-12 weeks and MRI brain every 12 weeks.
* provide tissue (optional) and blood for additional testing (learn about the cancer).

开始日期2026-06-01

申办/合作机构

Henry Ford Health System

[+1]

100 项与度伐利尤单抗相关的临床结果

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100 项与度伐利尤单抗相关的转化医学

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100 项与度伐利尤单抗相关的专利（医药）

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2,093

项与度伐利尤单抗相关的文献（医药）

2026-05-01·CANCER LETTERS

ERRα-ETV5 axis drives PD-L1 upregulation and immune escape in gallbladder cancer

Article

作者: Chen, Yu ; Guo, Xingmei ; Chen, Daozhen ; Lu, Xinyi ; Wen, SiJia ; Wang, Lei ; Wu, Fan ; Sun, Ping ; Zhao, Hui ; Yang, Mengmeng ; Gong, Wanwan

Gallbladder cancer (GBC) is a highly aggressive malignancy with a poor response to immune checkpoint blockade (ICB), highlighting an urgent need to understand the mechanisms of immune evasion. We identified the orphan nuclear receptor ERRα as a critical regulator of the immunosuppressive tumor microenvironment in GBC. Mechanistically, we discovered that ERRα transcriptionally upregulates the ETS-family transcription factor ETV5, which in turn directly binds to and activates the PD-L1 (CD274) promoter, establishing a novel ERRα-ETV5-PD-L1 signaling axis. In clinical specimens, ERRα expression positively correlated with PD-L1 levels and served as an independent prognostic factor for poor survival. Using a combination of human GBC tissues, in vitro co-culture systems, and a humanized mouse model, we demonstrated that genetic or pharmacological inhibition of ERRα downregulated PD-L1 and potentiated CD8⁺ T cell-mediated cytotoxicity. Critically, combined targeting of ERRα (using the inverse agonist XCT790) and PD-L1 (using durvalumab) synergistically suppressed tumor growth and enhanced intratumoral T cell infiltration in vivo. Our findings reveal ERRα as a master transcriptional regulator of immune evasion and highlight the therapeutic potential of co-inhibiting the ERRα-ETV5-PD-L1 axis to overcome immunotherapy resistance in GBC.

2026-05-01·Clinical and Translational Radiation Oncology

Radiotherapy patterns and factors associated with pneumonitis in PACIFIC-R, a real-world study of patients with unresectable stage III non-small-cell lung cancer treated with durvalumab after chemoradiotherapy

Article

作者: Kao, Steven ; Haakensen, Vilde Drageset ; Field, John K ; Mornex, Francoise ; Van Den Heuvel, Michel M ; Chander, Pratibha ; Moskovitz, Mor ; Garassino, Marina Chiara ; McDonald, Fiona ; Filippi, Andrea R ; Peters, Solange ; Girard, Nicolas ; Solomon, Benjamin ; Fietkau, Rainer ; Faria, Jolyon ; Qiao, Yao ; Garrido, Pilar ; Vercauter, Piet ; Bar, Jair ; Christoph, Daniel C ; Smit, Hans J M

Background and purpose:

Consolidation durvalumab, standard-of-care treatment for patients with unresectable stage III non-small-cell lung cancer (NSCLC) and no disease progression after chemoradiotherapy, may be associated with pneumonitis. We performed exploratory analyses of radiotherapy patterns and potential risk factors for symptomatic pneumonitis (SP) in PACIFIC-R.

Materials and methods:

PACIFIC-R is an ongoing, international, observational study based on medical chart data for patients in the durvalumab early access program. Patients with no missing data for candidate SP risk factors were included. SP was defined as a pneumonitis event (any cause) of grade ≥ 2 or requiring corticosteroids. Multivariable logistic regression identified variables associated with SP during durvalumab treatment; sensitivity analyses used a Cox proportional hazards model to account for time to SP.

Results:

Analyses included 268 patients; most received concurrent (86.6%) versus sequential (13.4%) chemoradiotherapy and intensity-modulated (IMRT; 66.8%) versus three-dimensional conformal (25.7%) radiotherapy, with between-country differences. Patients receiving IMRT were older, more frequently had nonsquamous histology, and had larger tumors. Fifty-two patients (19.4%) had SP during durvalumab treatment. Higher mean lung radiotherapy dose (log transformed) and prior chronic obstructive pulmonary disease (COPD) were associated with higher SP risk, with odds ratios (95% confidence interval [CI]) of 4.73 (1.66-15.07) and 2.60 (1.21-5.65), respectively, and hazard ratios (95% CI) of 3.28 (1.54-6.95) and 1.93 (1.04-3.56), respectively.

Conclusions:

Concurrent chemoradiotherapy and IMRT were the most common radiotherapy approaches. Higher mean lung radiotherapy dose and prior COPD were associated with higher SP risk during consolidation durvalumab for unresectable stage III NSCLC.

2026-04-01·Gynecologic Oncology Reports

Cost effectiveness analysis of immunotherapy regimens currently approved in advanced or recurrent endometrial cancer: An analysis of the NRG-GY 018, RUBY, and DUO-E trials

Article

作者: Richardson, Michael T ; Chan, John K ; Choi, Eunji ; Kapp, Daniel S ; Francoeur, Alex A ; Johnson, Caitlin R ; Tewari, Krishnansu S ; Liang, Su-Ying ; File, Brittany ; Brameld, Max

Background:

The purpose of this project was to evaluate the cost-effectiveness of novel FDA approved regimens incorporating immunotherapy into upfront treatment with chemotherapy in advanced or recurrent endometrial cancer in the mismatch repair deficient (dMMR) and mismatch repair proficient (pMMR) cohorts.

Methods:

Partitioned survival models were established based on the RUBY, NRG-GY 018, and DUO-E trials, as well as available FDA data. Incremental cost-effectiveness ratios (ICERs) were estimated based on quality adjusted progression free life years saved (QA-PFLYS). Tree Age software was used to perform partitioned survival modeling. Outcomes for dMMR and pMMR groups were compared based on the current FDA approvals. Costs were obtained from Redbook Micromedex pricing and adjusted for inflation from study activation to public dissemination of trial results.

Results:

The addition of pembrolizumab, dostarlimab, or durvalumab to chemotherapy in patients with dMMR tumors resulted in improvements in progression free life years saved. Based on QA-PFLYS, the ICER for pembrolizumab was $217,713, followed by $351,280 for durvalumab, and $451,750 for dostarlimab. When continuing durvalumab for 2 years, the ICER was $262,087. When looking at patients with pMMR tumors, the ICER for pembrolizumab was $250,535 while the ICER for dostarlimab was $1,349,776.

Conclusions:

Recognizing existing differences in study design, both pembrolizumab and durvalumab may be more cost effective than dostarlimab in our model. This appears to largely be driven by differences in duration of maintenance therapy rather than differences in effectiveness or individual drug cost. Immunotherapy does not appear to be as cost effective in the pMMR population.

2,591

项与度伐利尤单抗相关的新闻（医药）

2026-04-20

·Firstwordpharma

Arcus reports another TIGIT failure as Gilead pulls back from partnership

Arcus Biosciences has axed another late-stage study of its anti-TIGIT antibody, domvanalimab, due to futility. The decision to discontinue the Phase III STAR-121 trial in patients with non–small-cell lung cancer (NSCLC) came the same day the biotech's oncology partner, Gilead Sciences, let its option rights to some of Arcus' early stage programmes lapse, according to a notice filed Monday with the US Securities and Exchange Commission (SEC).The pair had linked up for a 10-year collaboration in 2020, with Gilead splashing $175 million upfront alongside a $200-million equity investment to jointly develop immuno-oncology therapeutics. The next year, it exercised its options for domvanalimab and two other cancer assets, paying $725 million.Gilead was responsible for running STAR-121, which was evaluating a first-line regimen comprising domvanalimab, the anti–PD-1 antibody zimberelimab, and chemotherapy against Merck & Co.'s PD-1 inhibitor Keytruda (pembrolizumab) plus chemotherapy in patients with metastatic NSCLC. Following a planned analysis, an independent data monitoring committee recommended the trial's discontinuation; Arcus will also bin the Phase II EDGE-Lung study. The TIGIT blow comes shortly after Arcus discontinued the Phase III STAR-221 trial assessing the same triplet combo involving domvanalimab as a first-line treatment for patients with upper gastrointestinal tract cancers. An interim analysis found no survival advantage for the regimen compared with Bristol Myers Squibb's Opdivo (nivolumab) plus chemotherapy (see – Vital Signs: Finding the next oncology failure in the wake of TIGIT's demise).According to Arcus' website, the only trial of domvanalimab left ongoing is the Phase III PACIFIC-8 study, which is being run by AstraZeneca. The UK pharma is evaluating the anti-TIGIT mAb in combination with Imfinzi (durvalumab), following chemotherapy and radiation, in patients with unresectable NSCLC. With just that TIGIT shot left on goal, Arcus has turned its focus to casdatifan, an HIF-2α inhibitor in Phase III testing for kidney cancer — and also the first programme under their partnership that Gilead didn't opt in for, letting its rights for casdatifan expire last year. Arcus has since moved forward to develop the cancer candidate solo. At the American Society of Clinical Oncology (ASCO) meeting last year, the biotech presented data from the Phase I/Ib ARC-20 study of patients with clear cell renal cell carcinoma (ccRCC) who had progressed on prior immunotherapy. Of 24 evaluable patients who received casdatifan plus Exelixis' tyrosine kinase inhibitor Cabometyx (cabozantinib), one had a complete response (4%) and 10 experienced partial responses (42%).Now, Gilead appears to be further backing away from its partnership with Arcus. Per Monday's SEC filing, the drugmaker did not make its option continuation payment, and certain rights will expire on July 14.While Gilead will retain time-limited options to four assets — AXL inhibitor B801, anti-CD39 mAb AB598, MRGPRX2 antagonist AB102, and an investigational TNF small molecule inhibitor — it does not hold any rights to early-stage programmes including those targeting CCR6, CD89 and CD40L.

临床3期ASCO会议免疫疗法临床2期临床失败

2026-04-20

·谈思生物

涨得最猛的biotech，数据兑现了！

说明：欢迎约稿、业务洽谈、媒体合作及行业交流。如需加入行业交流群，或发现内容涉及侵权需修改，请联系小助手微信：Taaslabs18 君实终于公布了备受各界关注的数据，近段时间以来，君实生物股价大幅上扬，推动其上涨的主要因素，大多是对AACR相关进展，以及PD-1×VEGF双抗、EGFR×HER3 ADC的商务拓展（BD）预期。如今数据已出，我们可以详细对比分析一番了。先给出结论，情况有喜有忧。喜的是，双抗JS207在结直肠癌和肝癌治疗领域的数据表现相当出色，具备开展商务拓展（BD）的充分可能性；忧的是，双抗ADC与同靶点的EGFR×HER3 ADC对照时，数据表现稍显逊色，这有可能是随访时间过短所造成的。我们先来聚焦JS207，目前它在一线肝细胞癌（HCC）和一线转移性结直肠癌（mCRC）这两个适应症上同步开展研究。外界所看到的，是两张数据表格，其中最引人注目的，当属HCC的71.4%客观缓解率（ORR）和mCRC的67.7%客观缓解率（ORR）。这些数据十分亮眼，但也正因为如此亮眼，容易引发两种截然相反的误读：要么是过度亢奋，要么直接以“样本量太小”将其一笔带过。这篇文章要做的，便是在这两种极端认知之间探寻出第三种解读方式——JS207真正的差异化优势究竟体现在何处，以及它到底需要达成怎样的证明，才能最大程度地实现出海目标。这是关于肝癌一线治疗的数据表格，当下最为主流的治疗方案，便是O药联合BMS的CTLA - 4单抗。观察JS207的数据时，人们最容易犯的错误，就是直接将它与已获批的注册级III期数据进行对比。看到71.4%与36%的对比，便得出“JS207碾压O药＋Y药”的结论。这一结论不仅不够严谨，在现实情况中更是根本站不住脚。这里有两件事必须阐述清楚：样本量以及研究设计。就HCC（肝细胞癌）方面而言，71.4%这个客观缓解率（ORR）源自NCT06954467试验的剂量探索期高剂量组，样本数n = 7。其置信区间大约在28%至96%之间——这意味着，这个数据的真实值有可能低至28%，也有可能高至96%，跨度接近70个百分点。倘若在7个人当中，有1个人从有效变为无效，ORR就会从71.4%下降到57.1%；要是再多1个人出现这种情况，ORR就降至42.9%。而且，该研究没有独立影像核查（BICR），也未设置随机化对照，所有评估均依靠研究者自行评判。与之形成鲜明对比的是，CheckMate 9DW是样本数n = 335的随机对照III期试验，IMbrave150是样本数n = 336的III期试验，其评估标准采用的是独立影像委员会（BICR/IRF）。君实的数据尽管十分出色、令人惊艳，但无奈样本量实在太小，我们可以说它存在很大的机会，但仍需继续等待后续结果。在mCRC（转移性结直肠癌）领域，情况虽稍有改善，但本质并无二致。JS207联合XELOX方案取得的67.7%客观缓解率（ORR），是基于31名可评估患者得出的数据，且中位随访时间仅仅为4.19个月。将其与AK112联合FOLFOXIRI方案（n = 22）取得的81.8% ORR，以及SSGJ - 707联合XELOX/FOLFOX方案（n = 68）取得的58.8%至62.5% ORR进行对比时，除了要考虑化疗方案骨架强度存在系统性差异这一因素外，样本量和随访时间的差异，实际上也并不足以支持直接进行数字层面的比对。我们不妨在这里深入阐释一下，康方生物的数据为何如此亮眼：关键在于其联用的化疗药物存在差异。康方生物采用的是三药联合化疗方案，其中伊立替康（作为第三种药物）的加入，从根源上改变了肿瘤所处的微环境，进而放大了PD - 1×VEGF双抗的协同作用效果。但三药方案并非没有代价——从历史数据来看，FOLFOXIRI方案的3/4级不良事件（AE）发生率约为55 - 70%，明显高于XELOX方案的约30 - 35%。所以，AK112能取得高客观缓解率（ORR），是以承受更高毒性为代价换来的，并非源于分子层面的优势。JS207和SSGJ - 707选择两药方案，是出于主动降低风险、扩大适用患者群体的策略考量，并非无奈之下的次优选择。那么对于JS212而言，最值得关注的差异点究竟是什么呢？笔者认为，关键还在于肝癌领域。一线肝细胞癌（HCC）治疗市场，如今已近乎被瓜分完毕。阿特珠单抗+贝伐珠单抗（atezo + bev，2020年获FDA批准）、度伐利尤单抗+曲美木单抗（durvalumab + tremelimumab，2022年获批）、纳武利尤单抗+伊匹木单抗（nivo + ipi，预计2025年4月，基于CheckMate 9DW研究，中位总生存期mOS为23.7个月，客观缓解率ORR为36%）。这三种治疗方案，涵盖了PD - 1/PD - L1、VEGF抗体和CTLA - 4，从治疗理念上几乎将免疫治疗与抗血管生成治疗的两两组合都覆盖到了。 JS207联合JS007若想在一线肝细胞癌（HCC）治疗领域站稳脚跟，其倚仗的并非又一套免疫与抗血管生成的两两组合方案，而是一种在HCC领域迄今尚未有人尝试过的三重免疫阻断设计：PD - 1/VEGF双特异性抗体（JS207）搭配独立的CTLA - 4抑制剂（JS007）。从机制层面剖析，其内在逻辑并不复杂：HCC的免疫微环境呈现出以调节性T细胞（Treg）浸润以及血管内皮生长因子（VEGF）介导的血管异常为主要特征的抑制性状态。CTLA - 4在T细胞活化过程中处于上游环节——它能够扩增效应T细胞的数量，同时清除Treg细胞；而JS207所具备的PD - 1/VEGF双抗功能则可同时发挥两方面作用：PD - 1阻断能够解除对效应T细胞的抑制，VEGF阻断则可促使血管正常化，改善T细胞向肿瘤部位的归巢。这三个关键节点，理论上全面覆盖了免疫抑制的上游（CTLA - 4）、末端效应（PD - 1）以及物理屏障（VEGF）。然而，理论逻辑清晰是一码事，实际数据表现又是另一码事。在一线HCC治疗领域，近期可作为竞品参照的是COMPASSION - 08研究（卡度尼利单抗+仑伐替尼），其B队列（15mg/kg，每3周一次，n = 28）的客观缓解率（ORR）为35.7%（95%置信区间：18.6 - 55.9%），中位无进展生存期（mPFS）为9.8个月，中位总生存期（mOS）尚未达到（随访时长27.4个月），中位缓解持续时间（mDoR）为13.67个月。这已然是目前在该设计空间内数据最为成熟的参照点——但即便样本量n = 28，置信区间的宽度仍达37个百分点，这充分表明HCC这一适应症对于小样本数据的考验极为严苛。 JS207的样本量n = 7，其置信区间宽得离谱；Cado联合Len方案所产生的毒性，主要源自仑伐替尼；而且这三组试验在设计以及入组人群方面，均不具有可比性。 COMPASSION - 08研究存在一个常被低估的复杂情况：仑伐替尼单独使用时，就能带来约18%至20%的客观缓解率（ORR）。所以，很难从35.7%这一合并数据中，单独分辨出卡度尼利单抗（cadonilimab）所做出的独立贡献。这意味着，COMPASSION - 08研究所证明的是“卡度尼利单抗+仑伐替尼”这一整体方案的有效性，而非卡度尼利单抗对一线肝细胞癌（HCC）免疫微环境的改变作用。这正是JS207+JS007研究设计中最具价值的核心所在：其随机扩展期预先设定了1:1的对照模式——即JS207+JS007联合用药组与JS207单药组进行对比。只要双抗与CTLA - 4联用的机制逻辑能自洽——联合用药组的客观缓解率（ORR）显著高于单药组（预计差距达到或超过15至20个百分点），便能为“三重免疫封锁策略在肝细胞癌（HCC）治疗中具有增量价值”提供首个基于随机对照试验的证据。在一线HCC的免疫联合治疗方案研究领域，这无疑是独一无二的设计。一旦机制逻辑得到验证，君实生物极有可能重新定义肝癌一线治疗的新范式。然而，在安全性方面有一个关键信号需要持续密切关注：治疗相关不良事件（TRAE）中，丙氨酸氨基转移酶（ALT）升高和天门冬氨酸氨基转移酶（AST）升高的比例各占50%。对于HCC患者群体而言，这一比例所带来的风险远高于其他实体瘤患者——由于HCC患者的基础肝功能储备相对有限，即便Child - Pugh分级为A级的患者亦是如此。倘若高剂量JS007所引发的CTLA - 4相关效应与免疫性肝炎叠加，很可能在扩展期成为阻碍研究推进的实际瓶颈。这是目前最需要警惕的信号，其重要性远超过单纯的数字表现。基于上述考量，我们预测HCC相关产品的销售峰值将达到30亿元。在结直肠癌（CRC）领域其实没什么太多可赘述的。我们都清楚，微卫星稳定型（MSS）CRC堪称一片亟待开发的蓝海市场，就目前而言，完全有足够的空间容纳三款双特异性抗体药物展开竞争。不过，当下最关键的问题在于，JS207的疗效能否保持稳定，其客观缓解率（ORR）能否持续稳定在60%以上。倘若JS207真能达到这一疗效标准，那么我们完全有理由为JS207在一线CRC治疗市场的销售峰值设定得更高一些，达到30亿。也就是说，这两款药品的销售峰值已然攀升至60亿元。鉴于当下PD - 1×VEGF赛道竞争极为激烈、内卷严重的状况，即便采用两倍的市销率（PS）进行估值，且暂不将肺癌适应症纳入考量，这条产品管线目前的估值也已高达120亿元！这无疑是值得欣喜的一面，然而，接下来也有令人忧虑的情况。JS212在针对奥希替尼耐药患者的治疗中，疗效未能达到预期。我们仅聚焦于1.8mg/kg及以上剂量组，其客观缓解率（ORR）仅有30%。这一疗效数据与BL - B01D1相比，差距十分显著；和SKB264相比，也远远不及；甚至与dato - dxd相比，也处于劣势，要知道dato - dxd单药治疗的ORR就达到了42.7%（95%置信区间：33.6% - 52.2%），其中奥希替尼经治亚组的ORR更是高达44.8%（95%置信区间：34.6% - 55.3%）。当然，我们尚可抱有一丝期待，毕竟当前随访时长过短，仅有三个月。或许随着随访时间的延长、数据的进一步积累，会有更多原本处于疾病稳定（SD）状态的患者转化为部分缓解（PR）状态。不过，在其他癌种的治疗中，这两者的表现倒是较为接近，食管鳞癌（ESCC）和乳腺癌的相关数据如下图所示。当下最为关键、重中之重的问题，便是后续JS207与JS212联合用于二期临床试验的数据揭晓情况，这一结果预计在今年年内就会公布。我多次提及过这个关键叙事，它堪称当下中国创新药领域最重要的叙事线索之一。尽管JS212目前的表现稍显逊色，但我们仍应给予它更多的随访时间，让它有机会证明自身的价值。综合各方面因素考量，可从以下三个维度进行分析： HCC领域：采用三重免疫阻断策略，内部设置随机对照环节，聚焦于一个此前医药界尚未有人解答的难题。这个答案预计会在2026至2027年随机扩展期的中期数据中得以揭晓。 mCRC领域：以两药XELOX方案作为基础框架，主动舍弃三药方案所带来的短期数据上的优势，转而追求毒性的可控性以及更广泛的适用患者群体。只有当HARMONi - GI6在相同的化疗强度基准下公布相关数据时，JS207才真正进入差异化验证的关键阶段。还有第三个维度，也是当下最需要着重强调的：JS207与JS212的联合用药临床试验正在推进当中，这是整个君实生物产品管线叙事中最具灵活性和潜力的部分。一旦试验结果超出预期，君实生物就不只是在单纯售卖两个独立的药品资产，而是在讲述一个“双平台协同增效”的精彩故事——对于商务拓展（BD）合作方而言，这意味着谈判的筹码从单一产品管线升级到了联合开发（co - co）层面。特瑞普利单抗演绎的是先发制人的故事，其核心竞争力在于抢占先机的速度优势。而JS207所讲述的则是平台化发展的故事，它的立足点在于产品管线的宽度以及不同产品间的协同效应。JS212的加入，让原本单一层次的平台叙事，成功升级为更具深度和广度的双层架构。此次数据公布，说实话，对君实生物的市值必然会产生较大幅度的波动，商务拓展（BD）方面的合作预期也可以持续释放。接下来，就让我们共同期待君实生物双抗与双抗ADC联用方案后续的精彩表现。 ►►► CGT创新合作交流群 CGT Asia 亚洲细胞与基因治疗创新峰会旨在搭建高效合作平台，促进研究人员、临床医生、企业家与投资人之间的深度对话与实质性合作，深入探讨技术创新与临床转化，破解研发、工艺、产业化难题，汇聚各方力量，加速颠覆性疗法上市，使更多疾病得以治愈与改善。即刻扫码加入 “CGT创新合作交流群” 免责声明：本文内容来源于官方网站，旨在为大家提供知识共享，不构成任何专业建议。本资料中含少量AI生成内容，同时所涉及的图片、及文字仅供参考，目的是为了将好的内容分享给更多人，版权依旧归原作者所有，若侵犯肖像权或者著作者权等知识产权，请联系我方删除。信息来源：公众号潮药Bar END 近期峰会活动谈思特别推荐 *谈思生物特色社群* 谈思生物聚焦国内外生物医药产业最新动态，专注为细胞治疗、基因治疗、类器官、核酸、疫苗、医美、神经系统、核药、医药制造等细分领域提供线上线下交流分享的专业平台，赋能中国生物医药产业发展，助力打造全球生物医药产业高地。每年谈思生物举办数十场线上线下品牌活动，拥有数十个生物医药行业精品社群，覆盖Novaris、赛诺菲、复宏汉霖、齐鲁制药、药明康德、辉瑞、阿斯利康、百济神州、赛默飞世尔等百家国内外领先的药企、CRO/CDMO等，已经服务上万名生物医药行业上下游从业者。专属社群：细胞治疗、基因治疗、医美、类器官、核酸药物、生物医药、RNA疫苗、工艺技术、中枢神经系统、核药、医药制造等，现专题社群仍然开放，入满即止。演讲/赞助/参展/进群/媒体/直播 133 4168 3667 sara.an@taaslabs.com

抗体药物偶联物AACR会议临床结果临床3期

2026-04-20

·BioSpace

Innate Pharma to Present MATISSE Phase 2 Interim Results of IPH5201 in Clinical Trials Plenary Session at AACR 2026

Encouraging early results catalyze continued investigation in the MATISSE Phase 2 study evaluating IPH5201, a first-in-class anti-CD39 monoclonal antibody, in combination with durvalumab and chemotherapy in resectable NSCLC; these results will be presented at the Clinical Trials Plenary Session at the AACR Annual Meeting 2026, on April 21 MARSEILLE, France--(BUSINESS WIRE)-- #immunotherapy --Regulatory News: Innate Pharma SA (Euronext Paris: IPH; Nasdaq: IPHA) (“ Innate ” or the “ Company ”), today announced that interim results from the MATISSE Phase 2 study evaluating IPH5201 in combination with durvalumab and platinum-based chemotherapy in resectable non-small cell lung cancer (NSCLC) will be presented in one of the Clinical Trials Plenary Sessions at the American Association for Cancer Research (AACR) Annual Meeting 2026, taking place April 17–22, 2026 in San Diego, California. The MATISSE study ( NCT05742607 ) is a single arm Phase 2 clinical trial evaluating perioperative IPH5201, an anti-CD39 blocking antibody, in combination with perioperative durvalumab (anti-PD-L1) in addition to neoadjuvant platinum-based chemotherapy in previously untreated patients with resectable NSCLC. The trial is designed to assess whether dual inhibition of the CD39 and PD-L1 pathways, together with chemotherapy, can enhance anti-tumor immune responses and improve clinical outcomes in early-stage lung cancer. These results follow a pre-planned interim analysis on 40 patients. The combination of IPH5201 with durvalumab and chemotherapy demonstrated higher pathological complete response (pCR) rates compared with the benchmark set by durvalumab plus chemotherapy alone. Notably, pCR was 35.7% and 50% in patients with tumors expressing PD-L1 ≥1% and PD-L1 ≥50%, respectively. Based on these results, the study continues to recruit patients with tumors expressing PD-L1≥1%. “ Patients with resectable NSCLC remain at significant risk of recurrence, underscoring the need for novel perioperative treatment strategies. Disrupting the adenosine pathway through CD39 inhibition with IPH5201, in combination with PD-1 blockade and chemotherapy, could enhance anti-tumor immune responses—particularly in patients with PD-L1 positive tumors, where we observed up to 50% pCR rate in the MATISSE trial. This signal will be further investigated as we complete enrollment of the study in the PD-L1-positive population ,” commented Dr. Sonia Quaratino, Chief Medical Officer of Innate Pharma . The presentation will be available in the publication section of Innate Pharma’s website . Abstract details Dual CD39 and PD-L1 inhibition: Interim results from the Phase 2 MATISSE trial of IPH5201 plus durvalumab and platinum-based chemotherapy in patients with resectable NSCLC Abstract Code: CT231 Session: CTPL04 – Advances in Immunotherapy Session Date/Time: Tuesday, April 21, 2026, 10:45 – 11:00 AM PDT Presenter: Pr. Fabrice Barlesi, CEO of Institut Gustave Roussy About IPH5201 IPH5201 is a first-in-class monoclonal antibody targeting CD39, a key immunosuppressive enzyme in the adenosine pathway. CD39 is expressed on tumor-infiltrating immune and stromal cells and contributes to immunosuppression by degrading extracellular adenosine triphosphate (ATP) into adenosine monophosphate (AMP), which is then further degraded into adenosine by CD73. By blocking CD39, IPH5201 promotes the accumulation of immunostimulatory ATP and reduces the production of immunosuppressive adenosine, thereby enhancing anti-tumor immune responses. IPH5201 is being co-developed in collaboration with AstraZeneca and is currently being evaluated in the Phase 2 MATISSE trial (NCT05742607), a multicenter study investigating perioperative treatment with IPH5201 in combination with durvalumab (anti-PD-L1) and platinum-based chemotherapy in patients with resectable non-small cell lung cancer (NSCLC). The MATISSE trial is designed to assess anti-tumor activity, including pathological complete response, and safety, with the goal of determining whether dual inhibition of the CD39 and PD-L1 pathways, in combination with chemotherapy, can enhance anti-tumor immunity and improve clinical outcomes in early-stage NSCLC. About Innate Pharma Innate Pharma S.A. is a global, clinical-stage biotechnology company developing immunotherapies for cancer patients. Leveraging its expertise on antibody-engineering and innovative target identification, Innate Pharma is developing innovative and differentiated next-generation antibody therapeutics. Innate Pharma is advancing a portfolio of differentiated potential first- and/or best-in-class assets, focused on areas of high unmet medical need, including IPH4502, a differentiated Nectin-4 ADC developed in solid tumors, lacutamab, an anti-KIR3DL2 antibody developed in cutaneous T cell lymphomas and peripheral T cell lymphomas, and monalizumab, an anti-NKG2A antibody developed in collaboration with AstraZeneca in non-small cell lung cancer. Innate Pharma has established collaborations with leading biopharmaceutical companies, including Sanofi and AstraZeneca, as well as renowned academic and research institutions, to advance innovation in immuno-oncology. Headquartered in Marseille, France with a US office in Rockville, MD, Innate Pharma is listed on Euronext Paris and Nasdaq in the US. Learn more about Innate Pharma at and follow us on LinkedIn and X. Information about Innate Pharma shares ISIN code Ticker code LEI FR0010331421 Euronext: IPH Nasdaq: IPHA 9695002Y8420ZB8HJE29 Disclaimer on forward-looking information and risk factors This press release contains certain forward-looking statements, including those within the meaning of applicable securities laws, including Section 27A of the Securities Act of 1933, as amended, and Section 21E of the Securities Exchange Act of 1934, as amended, and the Private Securities Litigation Reform Act of 1995. These are based on the management’s current beliefs, expectations and assumptions about future events, conditions and results and on information currently available to the management. When used in this press release, certain words, including “anticipate,” “plan,” “believe,” “can,” “could,” “estimate,” “project,” “expect,” “may,” “might,” “potential,” “expect” “should,” “will,” or the negative of these and similar expressions, identify forward-looking statements. Although the Company believes its expectations are based on reasonable assumptions, these forward-looking statements are subject to numerous risks and uncertainties, which could cause actual results to differ materially from those anticipated. These risks and uncertainties include, among other things, the uncertainties inherent in research and development, including related to safety, progression of and results from its ongoing and planned clinical trials and preclinical studies, review and approvals by regulatory authorities of its product candidates, enrolment, results and other milestones of its preclinical trials, the Company’s reliance on third parties to manufacture its product candidates, the Company’s commercialization efforts and the Company’s continued ability to raise capital to fund its development and product trials given its current cash position and the impact an inability to raise further financing would have on the Company’s ability to meet its financial or business objectives. For an additional discussion of risks and uncertainties, which could cause the Company's actual results, financial condition, performance or achievements to differ materially from those contained in the forward-looking statements, please refer to the Risk Factors (“Facteurs de Risque") section of the Universal Registration Document filed with the French Financial Markets Authority (“AMF”), which is available on the AMF website or on Innate Pharma’s website, and public filings and reports filed with the U.S. Securities and Exchange Commission (“SEC”), including the Company’s Annual Report on Form 20-F for the year ended December 31, 2025, and subsequent filings and reports filed with the AMF or SEC, or otherwise made public by the Company. References to the Company’s website and the AMF website are included for information only and the content contained therein, or that can be accessed through them, are not incorporated by reference into, and do not constitute a part of, this press release. In light of the significant uncertainties in these forward-looking statements, you should not regard these statements as a representation or warranty by the Company or any other person that the Company will achieve its objectives and plans in any specified time frame or at all. The Company undertakes no obligation to publicly update any forward-looking statements, whether as a result of new information, future events or otherwise, except as required by law. This press release and the information contained herein do not constitute an offer to sell or a solicitation of an offer to buy or subscribe to shares in Innate Pharma in any country. Contacts For more information Investors & Media Relations Innate Pharma Stéphanie Cornen stephanie.cornen@innate-pharma.fr Investor Relations investors@innate-pharma.fr Media communication@innate-pharma.fr

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适应症	国家/地区	公司	日期
胃食管交界处腺癌	欧盟	AstraZeneca AB	2026-03-16
胃食管交界处腺癌	冰岛	AstraZeneca AB	2026-03-16
胃食管交界处腺癌	列支敦士登	AstraZeneca AB	2026-03-16
胃食管交界处腺癌	挪威	AstraZeneca AB	2026-03-16
胃癌	欧盟	AstraZeneca AB	2026-03-16
胃癌	冰岛	AstraZeneca AB	2026-03-16
胃癌	列支敦士登	AstraZeneca AB	2026-03-16
胃癌	挪威	AstraZeneca AB	2026-03-16
早期胃癌	美国	AstraZeneca PLC	2025-11-25
胃食管交界处癌	美国	AstraZeneca PLC	2025-11-25
局部晚期胃癌	美国	AstraZeneca PLC	2025-11-25
不可切除的非小细胞肺癌	中国	AstraZeneca UK Ltd.	2025-11-18
肌层浸润性膀胱癌	美国	AstraZeneca UK Ltd.	2025-03-28
子宫癌	日本	阿斯利康制药有限公司	2024-11-22
晚期子宫内膜癌	欧盟	AstraZeneca AB	2024-08-15
晚期子宫内膜癌	冰岛	AstraZeneca AB	2024-08-15
晚期子宫内膜癌	列支敦士登	AstraZeneca AB	2024-08-15
晚期子宫内膜癌	挪威	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	欧盟	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	冰岛	AstraZeneca AB	2024-08-15

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适应症	最高研发状态	国家/地区	公司	日期
ALK阳性非小细胞肺癌	申请上市	中国	AstraZeneca AB	2025-02-21
EGFR突变的非小细胞肺癌	申请上市	中国	AstraZeneca UK Ltd.	2025-02-21
卵巢上皮癌	申请上市	中国	AstraZeneca UK Ltd.	2024-08-16
pMMR/MSS Locally Advanced Colon Cancer	临床3期	西班牙	AstraZeneca PLC	2024-12-30
PD-L1阳性三阴性乳腺癌	临床3期	美国	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	中国	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	日本	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	阿根廷	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	澳大利亚	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	巴西	AstraZeneca PLC	2023-11-23

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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


NCT03694236 (AACR2026)	临床2期	非小细胞肺癌新辅助	30	Neoadjuvant durvalumab combined with concurrent chemoradiotherapy	遞觸壓製築獵蓋壓鏇顧(選窪製觸遞鑰鑰鹽願製) = 獵齋淵夢鏇鏇顧獵構遞遞膚觸範憲糧築夢遞鹹 (築簾選築襯窪鏇網遞積 ) 更多	积极	2026-04-22
NCT05640791 (DURGAP, AACR2026)	临床2期	胆道癌新辅助 CD8+ \| CD4+ \| regulatory T cells (Tregs)	8	Neoadjuvant DurGAP therapy (TRG1)	繭餘願鬱獵積艱鬱艱獵(夢衊壓製範願願選餘鹽) = 鏇鬱廠遞顧憲廠構築膚構範遞觸選襯構鑰鏇獵 (範襯壓築膚繭簾鏇簾繭 ) 更多	积极	2026-04-22
NCT06526104 (STRIDE in CP-B, AACR2026)	临床2期	肝细胞癌一线	30	Tremelimumab 300 mg + Durvalumab 1500 mg (Hepatocellular Carcinoma + Child-Pugh B cirrhosis)	顧鑰鬱衊繭鏇蓋蓋淵築(蓋壓餘衊顧觸蓋製夢選) = 醖鹹鬱餘蓋築製遞積構積鏇觸夢艱顧鹽鹽鹽齋 (鏇觸獵衊獵餘製鏇構繭 ) 更多	积极	2026-04-21
NCT04308174 (DEBATE, AACR2026)	临床2期	胆道癌新辅助	45	Durvalumab plus Gemcitabine-Cisplatin (D+GP)	顧鑰鬱壓鏇壓膚積願網(積窪鏇廠築齋鹽選遞鬱) = 願製窪衊積淵範積鏇鹽鹹糧鏇繭網範簾夢簾齋 (齋淵憲鑰壓齋廠蓋遞鹹 ) 更多	积极	2026-04-21
NCT04308174 (DEBATE, AACR2026)	临床2期	胆道癌新辅助	45	Gemcitabine-Cisplatin (GP)	顧鑰鬱壓鏇壓膚積願網(積窪鏇廠築齋鹽選遞鬱) = 範顧積醖簾繭鏇網壓艱鹹糧鏇繭網範簾夢簾齋 (齋淵憲鑰壓齋廠蓋遞鹹 ) 更多	积极	2026-04-21
NCT03820141 (AACR2026)	临床2期	HER2阳性乳腺癌 ER-negative \| PR-negative \| HER2-Enriched	37	durvalumab+trastuzumab+pertuzumab	顧選鏇鏇夢齋醖積膚網(選鏇窪壓鹹網鹽壓壓餘) = 簾蓋壓齋夢壓選鏇夢淵選餘壓構獵積齋鹽顧鬱 (網構廠艱簾膚網夢餘築 )	积极	2026-04-21
AACR2026	临床2/3期	膀胱癌一线	200	ICI-only regimen(Durvalumab, Durvalumab+Tremelimumab, Pembrolizumab)	選簾顧鹽襯壓廠製襯壓(蓋製鹽蓋壓範範獵製憲): HR = 1.92 (95.0% CI, 1.63 ~ 2.25) 更多	不佳	2026-04-21
AACR2026	临床2/3期	膀胱癌一线	200	chemotherapy		不佳	2026-04-21
IMforte (AACR2026)	临床3期	广泛期小细胞肺癌维持	452	Lurbinectedin plus atezolizumab	壓衊觸夢顧淵簾獵製鹽(夢簾衊顧廠鑰憲鏇鹽憲) = 廠網衊鹹網艱鏇餘鏇憲構顧鏇艱蓋齋鑰築觸築 (觸廠齋衊窪膚獵鑰繭鑰 ) 更多	积极	2026-04-20
IMforte (AACR2026)	临床3期	广泛期小细胞肺癌维持	452	Durvalumab	壓衊觸夢顧淵簾獵製鹽(夢簾衊顧廠鑰憲鏇鹽憲) = 襯艱鏇餘遞齋壓衊繭鬱構顧鏇艱蓋齋鑰築觸築 (觸廠齋衊窪膚獵鑰繭鑰 ) 更多	积极	2026-04-20
NCT03820141 (DTP, CTgov)	临床2期	乳腺癌 \| HER2 阴性乳腺癌	51	Trastuzumab+Pertuzumab+Durvalumab	衊積選築顧齋窪積蓋窪 = 築餘醖糧獵窪鬱觸廠壓鏇遞範憲廠憲淵衊鹽夢 (襯顧衊網製衊膚醖糧膚, 願艱鹽襯齋醖艱積鏇壓 ~ 網獵築醖糧築築範築願) 更多	-	2026-04-20
AAD2026	N/A	黑色素瘤 PD-1 \| PD-L1 \| CTLA-4 ... 更多	24,720	LAG-3 inhibitors	鑰廠糧鑰範鬱衊構網夢(積鹹築鏇窪鏇觸網壓廠) = 鏇鬱醖製鹽積膚齋網繭獵襯構製獵遞衊淵鏇繭 (醖糧膚壓糧築鏇鏇製鹹 ) 更多	积极	2026-03-27
NCT04637594 (IMAGINE, CTgov)	临床3期	膀胱尿路上皮癌 \| 转移性尿道尿路上皮癌 \| 局部晚期尿路上皮癌 ... 更多	3	Nivolumab+Avelumab+Atezolizumab+Pembrolizumab+Durvalumab (Arm A (Immune Checkpoint Inhibitor))	鹽蓋製鬱窪選構構窪窪 = 顧憲構範鹽製獵鹹簾範鑰糧觸鏇鬱餘繭網鑰觸 (醖襯鬱壓鑰餘簾鹹鹹繭, 衊築壓顧廠蓋遞觸獵壓 ~ 獵糧壓願製範淵廠膚壓) 更多	-	2026-03-20
NCT04637594 (IMAGINE, CTgov)	临床3期	膀胱尿路上皮癌 \| 转移性尿道尿路上皮癌 \| 局部晚期尿路上皮癌 ... 更多	3	Nivolumab+Avelumab+Atezolizumab+Pembrolizumab+Durvalumab (Arm B (Immune Checkpoint Inhibitor))	鹽蓋製鬱窪選構構窪窪 = 襯繭繭選窪網構鏇壓選鑰糧觸鏇鬱餘繭網鑰觸 (醖襯鬱壓鑰餘簾鹹鹹繭, 鹽淵網廠繭廠網襯糧選 ~ 簾淵鑰衊鹹範顧窪餘衊) 更多	-	2026-03-20