预约演示

更新于：2025-10-01

Durvalumab

度伐利尤单抗

更新于：2025-10-01

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

肌层浸润性膀胱癌子宫癌晚期子宫内膜癌+ [194]

非在研适应症

急性髓性白血病肺腺癌前列腺腺癌+ [75]

原研机构

在研机构

+ [17]

非在研机构

Mirati Therapeutics, Inc.

AIO-Studien-gGmbH

Fred Hutchinson Cancer Research Center

+ [6]

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 (澳大利亚)、优先审评 (澳大利亚)、孤儿药 (日本)

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结构/序列

Sequence Code 10069506H

来源: *****

Sequence Code 13384675L

来源: *****

关联

885

项与度伐利尤单抗相关的临床试验

NCT07122089

/ Not yet recruiting临床2期IIT

A Multicenter Open-label, Prospective Study to Evaluate the Efficacy and Safety of SIRT Using Yttrium-90 Glass Microspheres Followed by Durvalumab and Tremelimumab for Treatment of Hepatocellular Carcinoma With Portal Vein Thrombosis

Hepatocellular carcinoma (HCC) is the most common primary liver cancer, being the third leading cause of cancer-related death worldwide, with approximately 745 000 deaths reported annually.
For advanced patients, including patients with tumoral portal vein thrombosis (PVT), most treatment guidelines recommend systemic therapy, either combination immunotherapy (IO) or combination of immunotherapy and anti-angiogenic treatment for first line option.
Results for PVT patients are provided in one trial with a median overall survival of 14.2 months with IO underlying the necessity to improve treatment of PVT patients. Two recent other phase 3 trials also reported positive results for different IO regimen.
Selective internal radiation therapy (SIRT) using yttrium-90 (90Y)-loaded glass microspheres (TheraSphereTM) can be used for patients with early stage to locally advanced HCC including PVT patients without extrahepatic spread (EHS). TheraSphereTM is recognized and is reimbursed in France for PVT patients without EHS, since 2019.Several retrospective studies have shown promising results for PVT patients.
Nowadays use of SIRT in locally advanced HCC is regaining interest based on the results of the randomized DOSISPHERE-01 study including non-operable patients, about 70% with PVT. This randomized Phase II trial using 90Y-loaded microspheres sought was noted the effectiveness of 90Y-loaded microspheres using a personalized dosimetry approach versus a standard dosimetry approach.
The use of a systemic treatment as IO after a locoregional treatment with the strong local debulking effect of SIRT is logical and of interest. Indeed, the most frequent pattern of progression after SIRT is recurrence in an untreated area, including untreated liver or EHS. Patients are then usually referred to IO.
Such kind of therapeutic approach, using SIRT followed by IO has already been evaluated in a phase 2 study using nivolumab after 90Y loaded resin microspheres with promising efficacy without safety deterioration.
The aim of this study is to evaluate SIRT followed by IO used according to their current indications in advanced HCC patient with PVT patients and without EHS.

开始日期2026-01-02

申办/合作机构

Center Eugene Marquis

[+1]

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2025-12-31

申办/合作机构

University of Maryland Baltimore

[+1]

NCT06608940

/ Not yet recruiting临床1/2期IIT

A Phase Ib/II Study of BC3402, a Novel Anti-TIM3 Agent, in Combination With Tremelimumab Plus Durvalumab (STRIDE) in Advanced, Unresectable Hepatocellular Carcinoma

The purpose of this study is to test the safety and efficacy of an investigational (experimental) product called BC3402. This product is considered experimental because it is not approved by the U.S. Food and Drug Administration (FDA).

开始日期2025-11-01

申办/合作机构

The Case Comprehensive Cancer Center

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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2,286

项与度伐利尤单抗相关的文献（医药）

2025-12-31·OncoImmunology

Avelumab induces greater Fc-Fc receptor-dependent natural killer cell activation and dendritic cell crosstalk compared to durvalumab

Article

作者: Makarov, Vladimir ; Srivastava, Raghvendra M ; Rupani, Amit ; Chan, Timothy A ; Osborne, Nicole

Several FDA-approved anti-PD-L1 (programmed cell death ligand-1) monoclonal antibodies (mAbs) are used to treat cancer. While these mAbs primarily target and intercept PD-L1:PD-1 inhibitory signaling in T-cells, the Fc-domains of these mAbs are distinct, and the unique cellular cascades triggered by differing Fc-domains of PD-L1 mAbs have not been directly investigated. In this study, we compared the innate immune effects of two widely used anti-PD-L1 IgG1 mAbs which bear distinct Fc-domains, avelumab (native-Fc) and durvalumab (mutated-Fc), using two-cell and three-cell co-culture systems containing Natural Killer cells (NK-cells), dendritic cells (DCs) and various tumor cell lines of multiple cancer origins. We show a robust enhancement in NK-cell effector function, DC maturation, reciprocal NK:DC crosstalk and DC editing that is unique to avelumab treatment using multiple functional immune assays. By transcriptomic analysis, we show for the first time pivotal differences in gene sets involved in NK-cell effector function, DC maturation, immunoregulatory interactions, and cytokine production between innate immune cells treated with avelumab versus durvalumab. Furthermore, we report several previously unknown Fc-receptor-associated biological pathways uniquely triggered by avelumab. Our findings elucidate novel mechanisms of Fc-dependent actions of PD-L1 mAbs which may inform their use in future clinical trials.

2025-12-31·Human Vaccines & Immunotherapeutics

From PD-1/PD-L1 to tertiary lymphoid structures: Paving the way for precision immunotherapy in cholangiocarcinoma treatment

Review

作者: Fang, Ye-Ying ; Chen, Gang ; Huang, Fang-Ju ; He, Rong-Quan ; Su, Qin-Yan ; Wen, Jia-Ying ; Li, Jian-Jun ; Qin, Di-Yuan ; Chi, Bang-Teng ; Chen, Yi-Yang ; Zeng, Jian-Jia ; Wang, Lei ; Yang, Li-Hua ; Lin, Qian

Cholangiocarcinoma (CCA) is a highly malignant hepatobiliary tumor characterized by limited treatment options and poor prognosis. The recent rise of immunotherapy has significantly influenced research in this field. This study presents a bibliometric analysis of 416 articles retrieved from the WOSCC, Wan fang Data, CNKI and VIP databases, spanning contributions from 32 countries, 589 institutions and 3,200 authors. The analysis identified "PD-L1," "PD-1" and "pembrolizumab" as central research foci, while "immune checkpoint inhibitors," "tumor immune microenvironment," "tertiary lymphoid structures" and "durvalumab" emerged as key areas of interest. These findings emphasize the pivotal role of immunotherapy in improving survival outcomes for CCA, and they highlight the significance of tertiary lymphoid structures within the tumor microenvironment as a promising target for future research. This study offers a strategic overview of the evolving landscape of CCA immunotherapy, providing valuable insights to guide future scientific endeavors in this domain.

2025-12-31·JOURNAL OF MEDICAL ECONOMICS

Cost-effectiveness of perioperative nivolumab + neoadjuvant platinum doublet chemotherapy as treatment for resectable non-small cell lung cancer in the United States

Article

作者: Milev, Sandra ; White, Benjamin ; Harris, Mack ; Sun, Ariel ; Lucherini, Stefano ; Villacorta, Reginald

AIMS:

CheckMate-77T demonstrated the clinical benefit of perioperative nivolumab plus neoadjuvant platinum-doublet chemotherapy (periNivo + neoCT). This study assessed the cost-effectiveness of periNivo + neoCT as treatment for non-metastatic (Stage IIA-IIIB), resectable non-small cell lung cancer (NSCLC) vs. relevant comparators in the US.

MATERIALS AND METHODS:

Following the natural history of non-metastatic NSCLC, a four-state Markov model was developed. Modeled health states were event-free survival, locoregional recurrence, distant metastasis, and death. CheckMate-77T informed time to progression estimates for periNivo + neoCT and neoCT; mortality estimates leveraged longer-term follow-up available from CheckMate-816. Indirect treatment comparison informed efficacy of comparator treatments not considered in CheckMate-77T. Comparators were neoadjuvant treatment strategies (neoadjuvant nivolumab + chemotherapy [neoNivo + CT], neoadjuvant chemotherapy [neoCT], and neoadjuvant chemoradiotherapy [neoCRT]), adjuvant chemotherapy (adjCT), and perioperative immuno-therapy (IO) strategies (perioperative durvalumab + neoadjuvant chemotherapy [periDurva + neoCT] and perioperative pembrolizumab + neoadjuvant chemotherapy [periPembro + neoCT]). Cost inputs were obtained from published literature and standard US sources and expressed in 2024 USD. The base-case analysis adopted the perspective of a commercial payer with a lifetime time horizon and discounted cost and health outcomes by 3% annually.

RESULTS:

Model results showed that periNivo + neoCT is more effective and costly than comparators. Deterministic incremental cost-effectiveness ratios were $84,921, $153,557, $77,976, $60,826, $74,252, $32,069, and $21,974 vs. neoCT, neoNivo + CT, neoCRT, adjCT, surgery, periPembro + neoCT, and periDurva + neoCT, respectively. In probabilistic sensitivity analysis, periNivo + neoCT resulted in an ICER below $150,000/QALY in 93.3%, 58.2%, 82.4%, 95.1%, 98.3%, 69.9%, and 82.1% of iterations vs. neoCT, neoNivo + CT, neoCRT, adjCT, surgery only, periPembro + neoCT, and periDurva + neoCT, respectively.

LIMITATIONS:

Uncertainty in the survival extrapolations reflected the limited body of evidence informing the indirect treatment comparison. ICERs vs. perioperative IO treatment strategies were sensitive to small changes in predicted costs and QALYs, given low incremental base case costs and QALYs.

CONCLUSION:

PeriNivo + neoCT is a cost-effective treatment option for patients with resectable, non-metastatic NSCLC.

1,828

项与度伐利尤单抗相关的新闻（医药）

2025-10-01

·Biotech前瞻

2025ESMO前瞻丨五大重磅胃癌研究，涵盖FGFR、CLDN18.2新靶点、围术期免疫争议、胃癌二线

点击蓝字关注我们本期看点 2025年欧洲肿瘤内科学会（ESMO 2025）将于10月17-21日在德国柏林举行。作为全球肿瘤学领域的顶尖盛会，多项即将改变临床实践的重磅研究将在本届大会发布。目前，大会“突破性摘要”（LBA）的标题已经公布。五项胃癌领域的“重磅 LBA”格外值得关注，涵盖FGFR新靶点、CLDN18.2新靶点靶向治疗联合双抗、围术期免疫治疗的争议、胃癌后线治疗。几项关键临床试验的结果有望对未来标准治疗产生深远影响。本期内容 01 五大重磅研究全景速览 02 安进/再鼎丨FGFR单抗丨胃癌 03 度伐利尤单抗丨MATTERHORN研究 04 CLDN18.2 ADC联合PD-1抑制剂或PD-1/VEGF双抗【01 五大重磅研究全景速览】 LBA10：FORTITUDE-101 研究标题： Bemarituzumab (BEMA) plus chemotherapy for advanced or metastatic FGFR2b-overexpressing gastric or gastroesophageal junction cancer (G/GEJC): FORTITUDE-101 phase 3 study results Bemarituzumab联合化疗用于治疗FGFR2b过表达的晚期或转移性胃癌及胃食管交界癌：FORTITUDE-101的III期研究结果汇报人：Sun Young Rha｜延世大学医学院 LBA81：MATTERHORN 研究标题： Event-free survival (EFS) with pathological outcomes in MATTERHORN: a randomised, Phase 3 study of durvalumab (D) plus 5-fluorouracil, leucovorin, oxaliplatin and docetaxel (FLOT) in resectable gastric/gastroesophageal junction (G/GEJ) adenocarcinoma MATTERHORN试验中无事件生存期及病理结局：度伐利尤单抗联合5-氟尿嘧啶、亚叶酸钙、奥沙利铂与多西他赛（FLOT方案）治疗可切除胃癌/胃食管交界部腺癌的随机III期研究汇报人：Josep Tabernero｜VHIO LBA80：INTEGRATE 研究标题： Regorafenib plus nivolumab vs investigator’s choice of chemotherapy in previously treated gastric or gastroesophageal cancer: INTEGRATE IIb, a randomized phase 3 AGITG Intergroup [NHMRC-CTC/IKF/AIO, ACCRU, TCOG/NHRI] study 瑞戈非尼联合纳武利尤单抗对比研究者选择的化疗方案用于既往接受过治疗的胃癌或胃食管癌：一项由AGITG协作组[含NHMRC-CTC/IKF/AIO、ACCRU、TCOG/NHRI]开展的随机III期研究（INTEGRATE IIb试验）汇报人：David Goldstein｜Prince of Wales Hospital LBA78：KC-WISE 研究标题： KN026 in combination with chemotherapy for previously treated HER2 positive gastric or gastroesophageal carcinomas (GC/GEJC): Interim analysis of KC-WISE KN026联合化疗用于经治HER2阳性胃或胃食管结合部癌：KC-WISE研究中期分析汇报人：徐建明｜中国人民解放军总医院 LBA83 标题： RC118 (CLDN18.2-targeted ADC) combined with PD-1 blockade or RC148 (PD-1/VEGF bispecific antibody) for locally advanced or metastatic gastric/gastroesophageal junction adenocarcinoma (la/m G/GEJA) RC118（CLDN18.2 靶向ADC药物）联合PD-1抑制剂或PD-1/VEGF双特异性抗体（RC148）用于治疗局部晚期或转移性胃/胃食管连接部腺癌汇报人：余一祎｜复旦大学附属中山医院【02 安进/再鼎丨FGFR单抗丨胃癌】 2025年9月3日，再鼎医药发布公告关于FGFR2b抗体贝玛妥珠单抗最新进展。据安进公司，再鼎医药的合作伙伴和该项研究的申办方，评价贝玛妥珠单抗联合化疗（mFOLFOX6）用于一线胃癌治疗的FORTITUDE-101 III 期临床研究已完成最终分析。在该研究预设的中期分析（即主要分析）时，贝玛妥珠单抗联合化疗方案对比单独化疗在总生存期方面显示出具有显著统计学意义和临床意义的改善。然而，在最终分析中，此前观察到的生存获益幅度减弱。安进表示中期分析和最终分析的结果将在即将举行的主要医学会议上公布。 2025年6月30日，安进（Amgen）宣布其与再鼎共同开发的FGFR2b抗体贝马利珠单抗（bemarituzumab）联合化疗在FORTITUDE‑101三期试验中提前达到一线胃癌总生存（OS）主要终点。这一消息再次凸显FGFR2b作为胃癌等肿瘤的关键驱动因素。 FGFR2b是一种成纤维细胞生长因子受体IIb亚型，过表达时可异常激活下游信号通路，促进肿瘤增殖。 FGFR靶点及bemarituzumab作用机制 FGFR2b在晚期胃癌或胃食管结合部癌（G/GEJ）中的过表达率约为38%，其中约16%患者肿瘤细胞≥10%呈现2+/3+阳性。值得注意的是，Fortitude‑101和早期阶段试验均观察到贝马利珠单抗组中眼部不良事件（如角膜炎、干眼等）频发，与其强效阻断FGF10配体有关。未来全试验数据发布后，将更清晰评估其风险/获益比，但这一积极结果已经为FGFR2b靶点在胃癌领域奠定了临床地位。胃癌的现有及新兴治疗靶点与疗法截止到目前为止，仅贝玛妥珠单抗进入针对FGFR2b过表达胃癌一线治疗III期研究阶段，包括联合化疗与联合免疫治疗和化疗两项，以研究其与化疗（FORTITUDE-101）以及与nivolumab和化疗联合使用（FORTITUDE-102）的疗效。 03 度伐利尤单抗丨MATTERHORN研究 2025年7月28日，阿斯利康宣布度伐利尤单抗的补充生物制品许可申请（sBLA）已获得FDA受理并予以优先审评，用于联合标准治疗（FLOT化疗方案，即氟尿嘧啶+亚叶酸钙+奥沙利铂+多西他赛）围手术期治疗可手术切除的早期和局部晚期（II期-IVA期）胃癌和胃食管交界处（GEJ）癌患者。 FDA预计将在2025年第四季度作出审批决定。一旦获批，该治疗组合将成为胃癌领域的第一个围手术期免疫治疗方案。早在2025年3月7日，阿斯利康宣布，3期临床试验MATTERHORN获得积极顶线结果：在主要终点无事件生存期（EFS），试验组较纯化疗组表现出统计学显著且具有临床意义的改善。对于次要终点总生存期（OS），在本次中期分析中观察到Imfinzi治疗方案呈现出明显优势趋势。试验将继续对患者进行随访，并在最终分析中正式评估OS。 MATTERHORN是一项全球多中心、随机、双盲、安慰剂对照的III期试验，旨在评估度伐利尤单抗（Imfinzi）联合FLOT化疗作为围手术期治疗用于可切除的II期至IVA期胃癌和胃食管结合部癌患者的效果。共948名患者随机分组，分别接受术前2周期和术后2周期的度伐利尤单抗（1500 mg）联合FLOT化疗，随后接受术后10周期的度伐利尤单抗单药治疗，或相应的安慰剂治疗。主要终点为无事件生存期（EFS），次要终点包括病理完全缓解（pCR）率和总生存期（OS）。在之前报告的关键次要终点—pCR的中期分析中，度伐利尤单抗联合方案的pCR率是单独新辅助化疗的两倍多（19%对比7%，比值比3.08；p<0.00001）。除了MATTERHORN研究以外，另一项DANTE研究也评估了抗PD-L1单抗（阿替利珠单抗）联合FLOT化疗在围术期中的疗效。但在胃癌围术期阶段，也有失败的研究：胃癌围手术期丨度伐利尤单抗申报适应症，O药、K药先后失败，背后原因浅析 04 荣昌生物丨CLDN18.2 ADC RC118 为荣昌生物开发的 CLDN18.2 靶向 ADC，毒素为 MMAE（vedotin 系列）。在 ESMO 2024 公布的首次人体 I/II 期研究（摘要 1456P）中，给药方案为 q2w 静脉输注，主要终点为安全性与客观缓解率（ORR）。研究者报告 “有前景的抗肿瘤活性且安全性可管理”，并在持续探索最优剂量方案。早期临床与监管节点：公司披露 2022 年的中澳 I 期数据显示耐受性良好；此外，美国 FDA 授予 RC118 两项罕见病用药（ODD）认定（胃癌/GEJ 与胰腺癌），为后续全球开发提供便利。正在进行的联合研究：进入 I/II 期的组合研究（NCT06038396）正在招募/推进，设计为 RC118 联合 PD-1 抑制剂或联合 PD-1/VEGF 双抗 RC148，I 期确定 MTD/RP2D，II 期在局部晚期/转移性胃癌或 GEJ 腺癌人群评估疗效与安全。公司近期渠道与三方登记均持续更新“已显示多线治疗人群具有临床意义的 ORR 信号；联合 PD-1/RC148 的 II 期正在进行”。小结：RC118 已完成早期首次人体验证并获得 ODD，显示出可管理的安全性与初步疗效信号；当前开发重心在与 PD-1 或 PD-1/VEGF 双抗的联合 II 期，以期在 CLDN18.2 阳性的胃/GEJ 腺癌中拓展前线或后线治疗证据。后续关键读出将聚焦 RP2D、ORR/PFS/DoR 及联合毒性可接受性。 ★

抗体药物偶联物临床结果临床3期

2025-09-30

·Biotech前瞻

2025ESMO前瞻丨四大重磅肺癌研究，正在改写治疗格局

点击蓝字关注我们本期看点 2025年欧洲肿瘤内科学会（ESMO 2025）将于10月17-21日在德国柏林举行。作为全球肿瘤学领域的顶尖盛会，多项即将改变临床实践的重磅研究将在本届大会发布。目前，大会“突破性摘要”（LBA）的标题已经公布。四项“重磅 LBA”格外值得关注：NorthStar（EGFR）、SKYSCRAPER-03（III 期不可切除）、MDT-BRIDGE（围手术期）与 Beamion LUNG 1（HER2）。无论是针对 EGFR 突变、HER2 突变，还是局部晚期 III 期不可切除的 NSCLC，几项关键临床试验的结果有望对未来标准治疗产生深远影响。本期内容 01 四大重磅研究全景速览 02 宗艾替尼（Zongertinib）丨Her2 TKI 03 TIGIT作用机制及研发前景 04 总结与展望【01 四大重磅研究全景速览】 LBA72: NorthStar 试验标题： NorthStar: A Phase II Randomized Study of Osimertinib (OSI) With or Without Local Consolidative Therapy (LCT) for Metastatic EGFR-Mutant Non-Small Cell Lung Cancer (NSCLC) NorthStar：奥希替尼（OSI）联合或不联合局部巩固治疗（LCT）用于转移性 EGFR 突变型非小细胞肺癌（NSCLC）的 Ⅱ 期随机研究汇报人：Yasir Y. Elamin 研究设计： II 期随机研究，比较奥希替尼（Tagrisso）单用 vs 奥希替尼 + 局部巩固治疗（手术/放疗）入组人群：EGFR 突变、IIIB–IV 期 NSCLC 主要终点：无进展生存期（PFS）次要终点：总生存期（OS）研究亮点：该研究直击一个核心问题—在靶向治疗时代，局部治疗是否还能进一步延长 EGFR 突变患者的生存？ LBA69: SKYSCRAPER-03 试验标题： SKYSCRAPER-03: Phase 3, open-label, randomised study of atezolizumab (atezo) + tiragolumab (tira) vs durvalumab (durva) in locally advanced, unresectable, stage Ⅲ non-small cell lung cancer (NSCLC) after platinum-based concurrent chemoradiation (cCRT) SKYSCRAPER-03：Ⅲ期、开放标签、随机研究：阿替利珠单抗（atezo）+tiragolumab（TIGIT单抗）对比度伐利尤单抗（durva）治疗铂类同步放化疗（cCRT）后局部晚期、不可切除的 Ⅲ 期非小细胞肺癌（NSCLC）汇报人：Rafal Dziadziuszko Pivotal trials of tiragolumab 研究设计： III 期、开放标签、随机研究比较方案：阿替利珠单抗（Atezo）+ tiragolumab vs 度伐利尤单抗（Durva）入组人群：局部晚期、不可切除 III 期 NSCLC，且在至少 2 个周期同步放化疗后未进展主要终点：PFS 次要终点：OS 背景提醒：前期 SKYSCRAPER-01 研究并未在一线治疗中证明 tiragolumab + 阿替利珠单抗的显著获益，此次结果能否逆袭，备受期待。 LBA65: MDT-BRIDGE 试验标题： Neoadjuvant durvalumab (D) + chemotherapy (CT) followed by either surgery (Sx) and adjuvant D or CRT and consolidation D in patients (pts) with resectable or borderline resectable stage IIB–IIIB NSCLC: interim analysis (IA) of the phase 2 MDT-BRIDGE study 新辅助度伐利尤单抗（D）+ 化疗（CT），随后行手术（Sx）+ 辅助度伐利尤单抗，或放化疗（CRT）+ 巩固度伐利尤单抗，用于可切除或边界可切除 IIB–IIIB 期非小细胞肺癌（NSCLC）患者：II 期 MDT-BRIDGE 研究的期中分析（IA）汇报人：Yasir Y. Elamin 研究设计： II 期单臂研究，探索度伐利尤单抗（D）+ 化疗的新辅助治疗模式主要终点：切除率次要终点：pCR 率、OS、EFS、PFS、ctDNA 清除率等意义：探索如何通过“免疫 + 化疗”新辅助策略，扩大可切除窗口，并在围手术期延长获益。 LBA74: Beamion LUNG 1 试验标题： Zongertinib as first-line treatment in patients with advanced HER2-mutant NSCLC: Beamion LUNG 1 Zongertinib作为晚期HER2突变型非小细胞肺癌（NSCLC）患者的一线治疗：Beamion LUNG 1研究汇报人：Sanjay Popat 研究设计：开放标签、剂量递增 + 扩展研究药物：zongertinib（Hernexeos，原 BI 1810631），HER2 突变靶向药研究进展： Part 1：确定最大耐受剂量（既治患者，HER2 改变实体瘤） Part 2：入组 NSCLC，HER2 突变，既治与初治人群，评估肿瘤缩小率与缓解持续时间里程碑：基于 Beamion LUNG 1 数据，FDA 已于 2025 年 8 月加速批准 zongertinib，用于不可切除或转移性非鳞 NSCLC，HER2 激酶结构域激活突变。【02 宗艾替尼（Zongertinib）丨Her2 TKI】 2025年8 月 29 日，中国 NMPA 批准勃林格殷格翰的宗艾替尼（Zongertinib，BI 1810631）片上市，单药用于治疗存在 HER2（ERBB2）激活突变且既往接受过至少一种系统治疗的不可切除局晚期或转移性 NSCLC 成人患者。来源：NMPA 官网宗艾替尼为选择性 HER2 抑制剂，可共价结合 HER2 外显子 20 突变的激酶结构域，对主要 HER2 突变（含 YVMA 插入）均具强抑制活性，且不抑制 EGFR 野生型，有望降低泛-HER TKI 常见的野生型 EGFR 相关毒性。2024 年 4 月，宗艾替尼被纳入勃林格殷格翰 × 中国生物制药在中国大陆的战略合作。核心证据（BEAMION LUNG-1 试验，Ib 期）该开放性 Ia/Ib 剂量递增与扩展研究在 HER2 异常的晚期/转移性实体瘤人群开展，主要终点为 BICR 与研究者评估的 ORR。Ib 期设置多队列：队列1（经治 HER2-TKD 突变 NSCLC，QD 120mg 或 240mg；期中确定120mg为后续剂量）、队列3（经治 HER2 突变 NSCLC，含 TKD 与非 TKD）、队列5（经治 HER2-TKD，且既往含铂 + HER2-ADC）。关键疗效截至 2024-11-29：队列1（n=75，120mg） BICR-ORR 71%、DCR 96%，中位 DoR 14.1 个月、中位 PFS 12.4 个月；合并脑转移的可评价患者（n=27）颅内 ORR 41%、DCR 81%。队列3（非 TKD，n=20） ORR 30%、DCR 65%（DoR/PFS 未成熟）。队列5（ADC 后，n=31） ORR 48%、DCR 97%，中位 DoR 5.3 个月、中位 PFS 6.8 个月。此前 ESMO Asia 与 AACR 公布的数据与 NEJM 同步发表，显示疗效持久且具临床意义。安全性概览不良事件以腹泻最常见；药物相关 AE（全部/≥3 级）发生率：队列1 97%/17%、队列3 80%/25%、队列5 77%/3%；未见药物相关 ILD 或心脏毒性。总体安全谱可管理，支持进一步在一线联合/序贯及特殊亚组（如脑转移）中的探索。 03 TIGIT作用机制及研发前景 TIGIT 靶点与机制 TIGIT与其同源配体PVR的结合直接抑制淋巴细胞激活。TIGIT和PVR广泛表达在不同类型的实体瘤中，说明TIGIT-PVR信号通路可能是一种主要的肿瘤免疫逃逸机制，是继PD-1/PD-L1之后的新型免疫检查点。但曾被寄予厚望的TIGIT靶点。但TIGIT单抗接连失利，为该赛道的研发蒙上阴影。阻断 TIGIT 通路，理论上可增强 PD-(L)1 抑制剂的疗效，因此成为免疫联合的重要新方向。临床探索：阿替利珠单抗 + TIGIT 抗体（tiragolumab） SKYSCRAPER-01（III 期，一线转移性 NSCLC）比较 tiragolumab + 阿替利珠单抗 vs 阿替利珠单抗单药。结果：未显著改善 PFS 或 OS，让业界对 TIGIT 路线的信心受挫。 SKYSCRAPER-03（III 期，局部晚期不可切除 NSCLC）人群：完成至少 2 周期同步放化疗未进展的 III 期患者。设计：阿替利珠单抗 + tiragolumab vs 度伐利尤单抗。主要终点为 PFS。意义：尝试在 cCRT 后巩固治疗场景对抗 “度伐利尤单抗独霸”的格局。市场与临床高度关注结果能否“翻盘”，决定 TIGIT 路线未来走向。 TIGIT 在肺癌的现状与前景挫折与希望并存：SKYSCRAPER-01 的失败让 TIGIT 通路的普适性受到质疑，但在免疫微环境不同的场景（如 III 期 cCRT 后），仍可能展现独特价值。生物标志物需求：未来或需结合 PD-L1、TMB、免疫谱，精细筛选最可能受益的亚群。开发趋势：目前多家药企（罗氏、百济神州等）都在积极推进 TIGIT 抗体单药或联合方案，焦点逐渐转向耐药后的二次机会和围手术期探索。 04 总结与展望 2025 年 ESMO 大会前夕，肺癌领域的四项重磅研究（NorthStar、SKYSCRAPER-03、MDT-BRIDGE、Beamion LUNG 1）共同勾勒出未来治疗格局的新图景。靶点突变（EGFR、HER2）仍是驱动治疗升级的核心，免疫联合在局部晚期与围手术期的探索持续深入，而 ctDNA、pCR 等新型终点也逐渐走向舞台中央。短期来看，这些研究将直接影响临床指南的更新，推动“系统+局部”的综合管理、“新辅助+巩固”的一体化路径，以及 HER2 靶点从 ADC 向小分子+ADC 双轮驱动的演进。长期来看，真正的挑战在于：如何通过精准分层，将合适的患者匹配到最有价值的方案，并在多种策略之间找到最佳时机与组合。可以预见，随着这些试验结果的揭晓，肺癌治疗将进入一个更加多维度、个体化的新阶段。对于临床医生，这是决策复杂度提升的开始；而对药企与研发者而言，则是重塑赛道格局的窗口期。 ★

临床3期临床2期临床结果临床成功

2025-09-30

·ir.nanobiotix.com

NANOBIOTIX Provides Business Update and Reports Half Year 2025 Financial Results

PARIS and CAMBRIDGE, Mass., Sept. 30, 2025 (GLOBE NEWSWIRE) -- NANOBIOTIX (Euronext: NANO - NASDAQ: NBTX - the “Company”), a late-clinical stage biotechnology company pioneering nanotherapeutic approaches to expand treatment possibilities for patients with cancer and other major diseases, provided an update on operational progress and announced its half year financial results for the six-month period ended June 30, 2025. Operational Highlights of the 2025 Half Year Period and To Date Expanding clinical development program evaluating the potential broad applicability of JNJ-1900 (NBTXR3) continues to build significant momentum: First patient dosed in the CONVERGE study, a Johnson & Johnson (“J&J”)-sponsored randomized Phase 2 study evaluating JNJ-1900 (NBTXR3) for patients with Stage 3 unresectable non-small cell lung cancer receiving standard of care chemoradiation followed by consolidation durvalumab First data announced from the completed dose escalation part of a Phase 1 study evaluating JNJ-1900 (NBTXR3) as a 2L+ therapy for patients with locally advanced NSCLC, sponsored by the University of Texas MD Anderson Cancer Center Announced full data from the completed MD Anderson Phase 1 study evaluating JNJ-1900 (NBTXR3) in pancreatic cancer along with the launch of a new cohort and expansion of the trial Achieved regulatory harmonization of JNJ-1900 (NBTXR3) after agreement with health authorities in major European countries to reclassify JNJ-1900 (NBTXR3) from a medical device to a drug Filed a new composition of matter patent for JNJ-1900 (NBTXR3) that aims to reinforce the intellectual property foundation supporting the product candidate First data announced from a Nanobiotix-sponsored Phase 1 study evaluating JNJ-1900 (NBTXR3) in combination with immune checkpoint inhibitors for patients with primary cutaneous melanoma resistant to anti-PD-1 Updated data announced from a Nanobiotix-sponsored Phase 1 study continuing to support JNJ-1900 (NBTXR3) plus anti-PD-1 as a potential new 1L or 2L+ option in anti-PD-1 naïve or resistant R/M-HNSCC Further execution of disciplined financial plan to reinforce pathway to long-term, self-sustained growth: Strengthened financial position through amendment of the JNJ-1900 (NBTXR3) global licensing agreement extending cash visibility to mid-2026 In active discussions regarding non-dilutive financing, intended to meaningfully extend its cash runway beyond mid-2026. Half Year 2025 Financial Results Revenue and Other Income: Revenue and other income have increased for the six months ended June 30, 2025, up to €26.6 million, compared to €9.3 million for the same period in 2024. Further to J&J amendment letter signed in March 2025 reducing the Company’s funding obligation on the future NANORAY-312 study costs, a positive non-cash revenue impact amounting to €21.2m was recorded in accordance with IFRS15 revenue recognition accounting principles application, offsetting the negative non-cash revenue impact recognized in 2024 results following the transfer of NANORAY-312 study sponsorship to J&J signed at the end of 2024. In addition, revenue towards J&J also included €3.4m of clinical product sales to J&J and R&D tax credit income of 1.7 million. Research and Development (“R&D”) Expenses: R&D expenses consist primarily of preclinical, clinical and manufacturing expenses including employee-related payroll expenses related to the development of JNJ-1900 (NBTXR3). These expenses for the six months ending June 30 2025, were €14.5 million compared to €22.0 million for the same period in 2024. This favorable R&D cost decrease was primarily driven by lower clinical development activities in NANORAY-312 study further to the transfer of sponsorship to J&J which has assumed nearly all remaining study expanses, less a small portion of costs that remain covered by the Company. Selling, General and Administrative (“SG&A”) Expenses: SG&A expenses consist primarily of administrative employee-related payroll expenses, legal and other professional fees, patent filing and maintenance fees, and insurance. Total SG&A expenses for the six months ending June 30, 2025, were €11.3 million, which is quite stable compared to €10.8 million for the same period in 2024. This slight unfavorable variance is mainly due to a phasing issue of social contributions expenses. Net loss: Net loss attributable to common shareholders for the six months ending June 30, 2025, was €5.4 million, or a €0.11 basic loss per share. This compares to a net loss attributable to common shareholders of €21.9 million, or €0.46 basic loss per share, for the same period in 2024. Cash and Cash Equivalents: Cash and cash equivalents as of June 30, 2025, were €28.8 million, compared to €49.7 million as of December 31, 2024. Financial Guidance: Based on the current operating plan and financial projections, the Company anticipates that the cash and cash equivalents of €28.8 million as of June 30, 2025, will fund its operations into mid-2026, similar to its prior guidance. Going Concern: In March 2025, the Company and J&J executed an amendment to the License Agreement. The amendment provides that J&J will assume nearly all remaining costs for the ongoing pivotal Phase 3 trial through completion, less a small portion of costs that will remain covered by the Company, allowing the Company to extend its cash runway and to reduce its operating cash outflows post this amendment, including the period beyond mid-2026. With the available €28.8 million of cash and cash equivalents as of June 30, 2025 and based on its current operating plan, the Company anticipates that its existing cash and cash equivalents will be insufficient to fund its operations over the next twelve months following the issuance of interim condensed consolidated financial statements. These events and conditions indicate that a material uncertainty exists that may cast significant doubt on the Company’s ability to continue as a going concern and, therefore, the Company may be unable to realize its assets and discharge its liabilities in the normal course of business. However, as the Company is in active discussions regarding non-dilutive financing intended to meaningfully extend its cash runway beyond the 12 months, the executive board determined it is appropriate to prepare the interim condensed consolidated financial statements as of and for the six-month period ended June 30, 2025, on a going concern basis, assuming the Company will continue to operate for the foreseeable future and to address its liquidity challenges by pursuing activities to generate additional cash inflows and by closely managing its operating expenditures, based on assumptions described in the half-year 2025 financial report. Availability of the Half Year 2025 Financial Reports The 2025 half-year financial report has been filed with the French financial market authority (Autorité des marchés financiers). It is available to the public on the Company’s website, www.nanobiotix.com. About NANOBIOTIX Nanobiotix is a late-stage clinical biotechnology company pioneering disruptive, physics-based therapeutic approaches to revolutionize treatment outcomes for millions of patients; supported by people committed to making a difference for humanity. The Company’s philosophy is rooted in the concept of pushing past the boundaries of what is known to expand possibilities for human life. Incorporated in 2003, Nanobiotix is headquartered in Paris, France and is listed on Euronext Paris since 2012 and on the Nasdaq Global Select Market in New York City since December 2020. The Company has subsidiaries in Cambridge, Massachusetts (United States) amongst other locations. Nanobiotix is the owner of more than 25 patent families associated with three (3) nanotechnology platforms with applications in 1) oncology; 2) bioavailability and biodistribution; and 3) disorders of the central nervous system. For more information about Nanobiotix, visit us at www.nanobiotix.com or follow us on LinkedIn and Twitter. DisclaimerThis press release contains “forward-looking” statements within the meaning of the “safe harbor” provisions of the Private Securities Litigation Reform Act of 1995, including, but not limited to, statements regarding the use of proceed therefrom, and the period of time through which the Company’s anticipates its financial resources will be adequate to support operations. Words such as “expects”, “intends”, “can”, “could”, “may”, “might”, “plan”, “potential”, “should” and “will” or the negative of these and similar expressions are intended to identify forward-looking statements. These forward-looking statements which are based on the Company’ management’s current expectations and assumptions and on information currently available to management. These forward-looking statements involve known and unknown risks, uncertainties and other factors that could cause actual results to differ materially from those implied by the forward-looking statements, including risks related to Nanobiotix’s business and financial performance, which include the risk that assumptions underlying the Company’s cash runway projections are not realized. Further information on the risk factors that may affect company business and financial performance is included in Nanobiotix’s Annual Report on Form 20-F filed with the SEC on April 2, 2025 under “Item 3.D. Risk Factors”, in Nanobiotix’s 2024 universal registration document filed with the AMF on April 2, 2025 under “chapter 1.5 Risk Factors”, and subsequent filings Nanobiotix makes with the SEC and AMF from time to time, including the Half-Year Report at June 30, 2025 which are available on the SEC’s website at www.sec.gov and on the AMF's website at www.amf.org, The forward-looking statements included in this press release speak only as of the date of this press release, and except as required by law, Nanobiotix assumes no obligation to update these forward-looking statements publicly. Contacts Attachment 2025-09-30 -- NBTX -- 1H25 Financial Results -- FINAL

临床1期财报引进/卖出临床2期

100 项与度伐利尤单抗相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D10808	度伐利尤单抗	L01XC28	DB11714

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
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
复发性子宫内膜癌	列支敦士登	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	挪威	AstraZeneca AB	2024-08-15
可切除非小细胞肺癌	英国	AstraZeneca PLC	2024-07-09
晚期胆道癌	美国	AstraZeneca UK Ltd.	2024-06-14
错配修复缺陷子宫内膜癌	美国	AstraZeneca UK Ltd.	2024-06-14
非小细胞肺癌 III期	美国	AstraZeneca UK Ltd.	2024-06-14
晚期肝细胞癌	欧盟	AstraZeneca AB	2023-04-14
晚期肝细胞癌	冰岛	AstraZeneca AB	2023-04-14
晚期肝细胞癌	列支敦士登	AstraZeneca AB	2023-04-14
晚期肝细胞癌	挪威	AstraZeneca AB	2023-04-14
转移性胆道癌	欧盟	AstraZeneca AB	2023-04-14
转移性胆道癌	冰岛	AstraZeneca AB	2023-04-14

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
胃食管交界处癌	申请上市	美国	AstraZeneca PLC	2025-07-28
胃食管交界处腺癌	申请上市	澳大利亚	AstraZeneca Pty Ltd.	2025-06-11
胃癌	申请上市	澳大利亚	AstraZeneca Pty Ltd.	2025-06-11
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
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

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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


NCT03518606 (MOVIE, Pubmed \| Breast)	临床2期	晚期乳腺癌 ER Negative \| PR Negative \| HER2 Negative	30	Tremelimumab plus Durvalumab combined to metronomic oral Vinorelbine	夢顧繭衊憲顧窪積壓鏇(鹹製廠廠餘艱衊淵醖簾) = 壓築糧繭築選觸繭構遞鬱壓憲範襯廠鬱糧構窪 (顧鹽夢鏇鑰糧鹹顧艱製, 5.5 ~ 29.8) 更多	不佳	2025-10-01
NCT03019003 (CTgov)	临床1期	转移性头颈部鳞状细胞癌 \| 头颈部肿瘤	13	Oral decitabine+Durvalumab	膚醖繭衊淵製淵壓鹽網 = 衊憲選醖築淵齋鹹蓋醖餘鹹範顧糧衊鏇鏇製獵 (顧鹽構醖選壓製糧衊繭, 製範範蓋淵蓋遞膚製築 ~ 襯夢衊繭製鑰鑰醖構範) 更多	-	2025-09-16
NCT03800134 (AEGEAN, WCLC2025)	临床3期	非小细胞肺癌新辅助 PD-L1 status	740	Neoadjuvant chemotherapy plus durvalumab	範醖鑰積醖願襯窪築觸(築艱鏇艱廠顧觸鏇壓襯) = 憲鬱鹽繭鹽鬱獵鹹蓋繭鏇簾窪觸廠齋鏇鏇廠鑰 (構蓋艱壓遞鑰網夢遞壓 ) 更多	积极	2025-09-09
NCT03800134 (AEGEAN, WCLC2025)	临床3期	非小细胞肺癌新辅助 PD-L1 status	740	Neoadjuvant chemotherapy plus placebo	範醖鑰積醖願襯窪築觸(築艱鏇艱廠顧觸鏇壓襯) = 夢鑰製遞憲艱蓋膚憲餘鏇簾窪觸廠齋鏇鏇廠鑰 (構蓋艱壓遞鑰網夢遞壓 ) 更多	积极	2025-09-09
NCT03638141 (CTgov)	临床2期	肝细胞癌	21	Tremelimumab+Durvalumab	選積廠選簾夢鬱窪製餘 = 齋襯範糧夢壓選鹽鑰憲襯獵壓選壓築獵鏇淵艱 (鹹築夢鏇選鏇糧鬱鑰襯, 製積蓋顧鹹鑰簾繭廠積 ~ 憲壓壓衊鬱獵齋壓鹽遞) 更多	-	2025-08-17
NCT04336943 (CTgov)	临床2期	非转移性前列腺癌 \| 前列腺腺癌	6	Quality-of-Life Assessment+Olaparib+Durvalumab	壓鹹襯鏇鹹網衊膚簾衊(餘構範鬱膚醖顧網觸鹽) = 膚願鏇淵鹽襯醖範願衊衊艱觸願構夢淵衊壓觸 (憲窪窪齋壓壓憲糧築鹹, 範鏇鹹網鹽網顧遞鬱鹽 ~ 顧餘簾觸遞餘願構範襯) 更多	-	2025-08-11
NCT05061550 (NeoCOAST-2, Pubmed \| Nat Med) 人工标引	临床2期	可切除非小细胞肺癌一线 \| 辅助 \| 新辅助	199	Durvalumab + Platinum-doublet chemotherapy + Oleclumab	憲襯鬱顧鹽範襯衊憲願(鬱窪廠鏇顧艱積廠鬱餘) = 積餘窪鏇積醖鏇鹽鑰遞蓋齋餘廠積積廠窪齋鏇 (簾簾糧夢膚夢積膚範積, 11.8 ~ 31.2) 更多	积极	2025-08-01
NCT05061550 (NeoCOAST-2, Pubmed \| Nat Med) 人工标引	临床2期	可切除非小细胞肺癌一线 \| 辅助 \| 新辅助	199	Durvalumab + Platinum-doublet chemotherapy + Monalizumab	憲襯鬱顧鹽範襯衊憲願(鬱窪廠鏇顧艱積廠鬱餘) = 獵蓋糧壓醖築醖窪艱蓋蓋齋餘廠積積廠窪齋鏇 (簾簾糧夢膚夢積膚範積, 16.0 ~ 37.6) 更多	积极	2025-08-01
NCT03703297 (ADRIATIC, CTgov)	临床3期	局限期小细胞肺癌	730	Durvalumab (Durvalumab)	齋觸願鏇獵淵襯積壓觸(憲選鹹範憲醖餘獵繭餘) = 選範範壓網範蓋夢廠鏇憲願鬱廠獵範齋壓糧鬱 (構範齋齋網製餘壓艱艱, 積夢廠簾壓構製觸鏇遞 ~ 襯鏇範鬱製範憲鑰膚淵) 更多	-	2025-08-01
NCT03703297 (ADRIATIC, CTgov)	临床3期	局限期小细胞肺癌	730	placebo (Placebo)	齋觸願鏇獵淵襯積壓觸(憲選鹹範憲醖餘獵繭餘) = 製選製鏇遞網製鏇築醖憲願鬱廠獵範齋壓糧鬱 (構範齋齋網製餘壓艱艱, 夢繭鑰糧築鬱衊窪憲醖 ~ 製遞鹹廠鏇願淵製憲鏇) 更多	-	2025-08-01
NCT05927142 (DURIPANC, GlobeNewswire) 人工标引	临床2期	转移性胰腺癌	14	rintatolimod + durvalumab	衊範衊範窪獵壓製淵艱(顧鹽夢蓋淵築築積遞遞) = 衊醖繭襯衊範鬱壓簾積夢廠選餘願鬱鹽窪遞築 (網膚選餘餘願鏇壓範夢 ) 更多	积极	2025-07-28
NCT04026412 (CheckMate 73L \| CheckMate73L \| CheckMate -73L, CTgov)	临床3期	局部晚期非小细胞肺癌	925	Nivolumab+Ipilimumab (Arm A:Nivo + CCRT/Nivo + Ipi)	艱夢簾齋蓋鏇鹽糧願觸(窪壓鹹壓積齋鬱觸鑰餘) = 製遞艱獵簾構繭衊餘築範襯選繭獵顧鹽蓋顧夢 (製構壓觸築夢蓋範簾遞, 積膚簾繭鏇遞蓋餘網鹹 ~ 夢鬱構窪築構鏇憲夢艱) 更多	-	2025-07-24
	临床3期	局部晚期非小细胞肺癌	925	Durvalumab (Arm C: CCRT/Durva)	艱夢簾齋蓋鏇鹽糧願觸(窪壓鹹壓積齋鬱觸鑰餘) = 選艱鬱衊醖觸艱醖構鹽範襯選繭獵顧鹽蓋顧夢 (製構壓觸築夢蓋範簾遞, 艱鑰製艱選簾蓋積艱顧 ~ 齋糧齋願觸網觸築願顧) 更多	-	2025-07-24
NCT03529422 (NCT02000947, CTgov)	临床2期	淋巴间质性肺炎 \| 头颈部鳞状细胞癌 \| 消化系统疾病 ... 更多	18	Intensity Modulated Radiotherapy Treatments+Durvalumab	鏇選膚膚廠簾網積艱衊 = 齋憲積壓齋糧網範衊構製製壓繭醖鏇醖選夢遞 (遞積製製繭夢範壓顧憲, 遞網醖鹽醖選淵簾遞憲 ~ 積繭衊遞鹽製積簾鹹構) 更多	-	2025-07-20