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更新于：2025-01-21

Durvalumab

度伐利尤单抗

更新于：2025-01-21

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+ [12]

在研适应症

局限期小细胞肺癌子宫癌晚期子宫内膜癌+ [178]

非在研适应症

急性髓性白血病大肠腺癌晚期头颈癌+ [60]

原研机构

在研机构

+ [17]

非在研机构

Mirati Therapeutics, Inc.

Circio Holding ASA

Fred Hutchinson Cancer Research Center

+ [4]

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)

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结构/序列

Sequence Code 10069506H

来源: *****

Sequence Code 13384675L

来源: *****

关联

864

项与度伐利尤单抗相关的临床试验

NCT06287775

/ Recruiting临床1/2期IIT

A Phase I Dose Finding and Phase II Randomized Trial of Iadademstat Combined With Immune Checkpoint Inhibition Maintenance After Initial Chemoimmunotherapy in Patients With Extensive-Stage Small Cell Lung Cancer

This phase I/II trial tests the safety, side effects, and best dose of iadademstat when given together with atezolizumab or durvalumab, and studies the effect of the combination in treating patients with small cell lung cancer that has spread outside of the lung in which it began or to other parts of the body (extensive stage) who initially received standard of care chemotherapy and immunotherapy. Iadademstat may stop the growth of tumor cells by blocking some of the enzymes needed for cell growth. Immunotherapy with monoclonal antibodies, such as atezolizumab or durvalumab, may help the body's immune system attack the cancer, and may interfere with the ability of tumor cells to grow and spread. Adding iadademstat to either atezolizumab or durvalumab may be able to stabilize cancer for longer than atezolizumab or durvalumab alone in treating patients with extensive stage small cell lung cancer.

开始日期2025-08-17

申办/合作机构

National Cancer Institute

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2025-06-01

申办/合作机构

The Case Comprehensive Cancer Center

NCT06274879

/ Not yet recruiting临床2期

Safety of Biliary Intraductal Radiofrequency Ablation in Patients With Unresectable Extrahepatic Biliary Tract Cancer Undergoing Standard of Care Chemo-immune Checkpoint Inhibitor -Therapy: a Phase II, Multicenter, Randomized and Controlled

The goal of this clinical trial is to provide evidence for the general tolerability of radiofrequency ablation (bRFA) in patients with unresectable bile duct cancer undergoing systemic palliative treatment consisting of chemotherapy (gemcitabine and cisplatin) plus durvalumab (immune-checkpoint-inhibitor, ICI). The main question it aims to answer is whether it is safe to combine chemotherapy (gemcitabine and cisplatin) and immunotherapy (durvalumab) - CICI therapy.
Participants will be assigned to either the control group or the experimental group. In the control group, the standard of care consists of endoscopy with stent placement in the bile duct and CICI, whereas in the experimental group, bRFA will be performed in addition to the standard of care. Participants will be followed up for 6 months, during the follow-up, the stage of the tumor, blood examination, the duration of the stent from the insertion until its failure, adverse events and quality of life will be examined.
Researchers will compare the standard of care alone to the experimental group to see if the additional bRFA procedure causes higher or no difference in adverse events rate.

开始日期2025-06-01

申办/合作机构

Insel Gruppe AG

[+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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1,935

项与度伐利尤单抗相关的文献（医药）

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.

2025-02-01·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Cardiotoxicity associated with immune checkpoint inhibitors: Systematic review and meta-analysis

Review

作者: Carollo, Anna ; Provenzani, Alessio ; Cutaia, Sofia ; Novara, Maria Eugenia ; Piazza, Lavinia ; Rizzo, Sergio ; Di Martino, Enrica

BACKGROUND AND AIMS:

The aim of this systematic review was to assess the risk of cardiac toxicity in patients undergoing approved PD-1 (nivolumab, pembrolizumab, cemiplimab, dostarlimab), PD-L1 (atezolizumab, avelumab, durvalumab), and CTLA-4 (ipilimumab) inhibitors.

RESULTS:

Among a total of 2272 articles, 11 phase II and III clinical trials included: 5463 patients and 175 cardiac adverse events. The most common cardiac disorder was atrial fibrillation (12 %), while cardiac arrest and cardiac failure (6 %) led to death in three cases. Overall, ICI treatment increased the risk of cardiotoxicity compared with control groups (RR=1.62, 95 %-CI= 1.18-2.24, p-value=0.0033; OR=1.71, 95 %-CI= 1.20-2.42, p-value=0.0027).

CONCLUSIONS:

This study proved that the recognition of frequency and severity of all grade cardiotoxicity associated with ICIs is still underestimated. Thus, a systematic cardiological screening becomes necessary, in order to intercept the potential cardiological complications beforehand and optimize the outcomes of the respective treatment with PD-1, PD-L1 and CTLA-4 inhibitors.

2025-02-01·RADIOTHERAPY AND ONCOLOGY

Association of the time of day of chemoradiotherapy and durvalumab with tumor control in lung cancer

Article

作者: McMillan, Matthew T ; Gelblum, Daphna Y ; Simone, Charles B ; Wu, Abraham J ; Shaverdian, Narek ; Schoenfeld, Adam J ; Iyengar, Puneeth ; Shepherd, Annemarie ; Chaft, Jamie E ; Gomez, Daniel R ; Cooper, Alissa J

BACKGROUND/PURPOSE:

The circadian clock governs the expression of genes related to immunity and DNA repair. We investigated whether the time of day of radiotherapy and/or systemic therapy infusions (chemotherapy or anti-PD-L1) are associated with disease control and survival in locally advanced non-small cell lung cancer (LA-NSCLC).

MATERIALS/METHODS:

178 consecutive patients with inoperable LA-NSCLC who received definitive chemoradiotherapy followed by durvalumab between 5/2017-8/2022 were reviewed. Outcomes evaluated included progression-free survival (PFS), distant metastasis-free survival (DMFS), locoregional control (LRC), and overall survival (OS).

RESULTS:

At a median follow up of 48.0 mo from durvalumab initiation, median PFS and OS were 26.2 mo and 50.0 mo, respectively. Median LRC and DMFS were not reached and 41.0 mo, respectively. Receiving > 50 % (N = 23) versus ≤ 50 % (N = 155) of radiotherapy treatments within 3 h of sunset was associated with younger age; otherwise, there were no other differences between cohorts. There were no significant differences in characteristics between patients who received > 50 % (N = 23) versus ≤ 50 % (N = 155) of durvalumab infusions within 3 h of sunset. On multivariable analysis, receiving > 50 % of radiotherapy treatments within 3 h of sunset was independently associated with reduced risk for progression (HR 0.39, p = 0.017) and distant metastasis (HR 0.27, p = 0.007); conversely, receiving > 50 % of durvalumab infusions within 3 h of sunset was independently associated with increased risk for distant metastasis (HR 2.13, p = 0.025). The timing of chemotherapy was not associated with disease outcomes.

CONCLUSION:

The time of day of radiotherapy and durvalumab infusion may be associated with disease control in LA-NSCLC, and the optimal time of treatment depends on the treatment modality.

2,019

项与度伐利尤单抗相关的新闻（医药）

2025-01-21

·ir.nanobiotix.com

NANOBIOTIX Announces First Patient Dosed in a New Randomized Phase 2 Study Evaluating JNJ-1900 (NBTXR3) for Patients With Stage 3 Unresectable Non-Small Cell Lung Cancer

PARIS and CAMBRIDGE, Mass., Jan. 21, 2025 (GLOBE NEWSWIRE) -- NANOBIOTIX (Euronext: NANO –– NASDAQ: NBTX – the ‘‘Company’’), a late-clinical stage biotechnology company pioneering nanoparticle-based therapeutic approaches to expand treatment possibilities for patients with cancer and other major diseases, today announced that the first patient has been dosed in the CONVERGE study, a Phase 2 randomized controlled clinical trial evaluating potential first-in-class radioenhancer JNJ-1900 (NBTXR3) for the treatment of patients with Stage 3 unresectable non-small cell lung cancer receiving standard of care chemoradiation followed by consolidation durvalumab (NCT06667908). CONVERGE is sponsored by Janssen Pharmaceutica NV, a Johnson & Johnson Company, under a global license agreement. “We believe the true value of JNJ-1900 (NBTXR3) is driven by its potential to address the unmet needs of the millions of patients each year who receive radiotherapy as part of their treatment,” said Laurent Levy, Nanobiotix Chief Executive Officer and Chairman of the Executive Board. “With a clear path to potential registration in head and neck cancer established through NANORAY-312, the first patient dosed in the CONVERGE study in non-small cell lung cancer brings us another step closer to delivering for the large number of patients JNJ-1900 (NBTXR3) is designed to serve.” About NBTXR3 (JNJ-1900) NBTXR3 is a novel, potentially first-in-class oncology product composed of functionalized hafnium oxide nanoparticles that is administered via one-time intratumoral injection and activated by radiotherapy. Its proof-of-concept was achieved in soft tissue sarcomas for which the product received a European CE mark in 2019. The product candidate’s physical mechanism of action (MoA) is designed to induce significant tumor cell death in the injected tumor when activated by radiotherapy, subsequently triggering adaptive immune response and long-term anti-cancer memory. Given the physical MoA, Nanobiotix believes that NBTXR3 could be scalable across any solid tumor that can be treated with radiotherapy and across any therapeutic combination, particularly immune checkpoint inhibitors. Radiotherapy-activated NBTXR3 is being evaluated across multiple solid tumor indications as a single agent or in combination with anti-PD-1 immune checkpoint inhibitors, including in NANORAY-312—a global, randomized Phase 3 study in locally advanced head and neck squamous cell cancers. In February 2020, the United States Food and Drug Administration granted regulatory Fast Track designation for the investigation of NBTXR3 activated by radiation therapy, with or without cetuximab, for the treatment of patients with locally advanced HNSCC who are not eligible for platinum-based chemotherapy—the same population being evaluated in the Phase 3 study. Given the Company’s focus areas, and balanced against the scalable potential of NBTXR3, Nanobiotix has engaged in a collaboration strategy to expand development of the product candidate in parallel with its priority development pathways. Pursuant to this strategy, in 2019 Nanobiotix entered into a broad, comprehensive clinical research collaboration with The University of Texas MD Anderson Cancer Center to sponsor several Phase 1 and Phase 2 studies evaluating NBTXR3 across tumor types and therapeutic combinations. In 2023, Nanobiotix announced a license agreement for the global co-development and commercialization of NBTXR3 with Janssen Pharmaceutica NV, a Johnson & Johnson Company. 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 umbrella patents 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 Disclaimer This 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 24, 2024 under “Item 3.D. Risk Factors”, in Nanobiotix’s 2023 universal registration document filed with the AMF on April 24, 2024, in Nanobiotix’ 2024 semi-annual report under the caption “Supplemental Risk Factor” filed with the SEC on Form 6-K and with AMF on September 18 2024, and subsequent filings Nanobiotix makes with the SEC from time to time which are available on the SEC’s website at www.sec.gov. 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

临床2期引进/卖出临床3期快速通道

2025-01-20

·GlobeNewswire-Health Care

AIM ImmunoTech Highlights Key 2024 Achievements and Outlines Upcoming 2025-26 Value-Driving Milestones

– Continued execution across Ampligen® (rintatolimod) clinical development programs in areas with critical unmet needs, especially in the high-value pancreatic cancer and Long-COVID spaces – Expected milestones over the course of the next 18 months provide significant value-driving opportunities, including some trials being partially funded by the National Cancer Institute, AstraZeneca and Merck Jan. 15, 2025 -- AIM ImmunoTech Inc. (NYSE American: AIM) (“AIM” or the “Company”) today highlighted key clinical, regulatory and corporate milestones achieved over 2024 and outlined its expected upcoming milestones. “It is clear that 2024 was a foundational year for AIM on the clinical, regulatory and corporate fronts. Without a doubt, our team continued to drive our strategy forward and deliver results. We believe this progress has positioned AIM for an exciting 2025 and the opportunity to drive value for our stockholders,” stated Thomas K. Equels, Chief Executive Officer of AIM ImmunoTech. “Looking ahead, we believe we are poised for an exciting 2025 with a number of key milestones expected over the next 18 months across important clinical trials addressing major unmet medical needs. Certain of these trials are being funded in part by major oncology interests such as the National Cancer Institute, AstraZeneca and Merck, which we believe emphasizes their great potential to change lives for the better. Our team is committed to the seamless execution of our clinical development programs and, if successful, we believe each holds the potential to drive significant value in the near and long term.” Metastatic Pancreatic Ductal Adenocarcinoma Program Commenced enrollment and dosing in DURIPANC Phase 1b/2 study combining Ampligen with AstraZeneca’s anti-PD-L1 immune checkpoint inhibitor Imfinzi® (durvalumab) for the treatment of late-stage pancreatic cancer; Announced that the first dose level was generally well-tolerated in the DURIPANC Phase 1b/2 study of Ampligen and Imfinzi as a combination therapy for late-stage pancreatic cancer; and Reported positive preliminary data from Phase 1b/2 study of Ampligen and Imfinzi as a combination therapy for late-stage pancreatic cancer. Phase 2 Locally Advanced Pancreatic Adenocarcinoma Program Received authorization from the Erasmus Medical Center Ethics Committee to open a European site for the ongoing Phase 2 study (“AMP-270”) of Ampligen as a therapy for locally advanced pancreatic cancer; and Announced the publication of new positive data analysis from a long-term Early Access Program studying Ampligen for the treatment of advanced pancreatic ductal adenocarcinoma. The Company sought FDA guidance on expansion of inclusion criteria and treatment arms, and then subsequently amended the study protocol. The study is recruiting patients. These adjustments are also expected to result in substantial reductions in clinical costs. Phase 2 Recurrent Ovarian Cancer Program Reported positive top-line, protocol-planned interim report data from the study of Ampligen combined with pembrolizumab for the treatment of recurrent ovarian cancer. Phase 2 Post-COVID Conditions Program Reported positive topline results from the Company’s Phase 2 study evaluating the efficacy and safety of Ampligen as a potential therapeutic for people with the post-COVID condition of fatigue (“AMP-518”); and Reported an analysis of the AMP-518 clinical trial, based upon statistically significant data, which supports the Company’s belief in Ampligen as a potential therapeutic for people with the moderate-to-severe post-COVID-19 condition of fatigue, and that this would be the likely subject population for AIM’s planned follow-up clinical trial. Further, the Company was also granted two important patents covering Ampligen for the treatment of: Endometriosis, a painful chronic condition that affects nearly 10% of women of reproductive age, or approximately 6.5 million women in the United States. This patent was granted in the United States. The Post-COVID Condition of Fatigue. This method and compositions patent was granted in the Netherlands. Additionally, AIM successfully completed cGMP manufacturing of 9,042 clinical vials of Ampligen. The Company announced the publication of new pre-clinical data of Ampligen as part of a combinational therapy in the treatment of melanoma. Metastatic Pancreatic Ductal Adenocarcinoma Phase 1b/2 Combining Anti-PD-L1 Immune Checkpoint Inhibitor Durvalumab with TLR-3 Agonist Ampligen in Patients with Metastatic Pancreatic Ductal Adenocarcinoma for Therapy Efficacy (DURIPANC) (NCT05927142); Funded through collaboration of AstraZeneca and Erasmus Medical Center Q1 2025: Complete Phase 1b Early Q2 2025: Launch of Phase 2 Q2/Q3 2026: Last patient enrolled in Phase 2 Locally Advanced Pancreas Cancer (LAPC) Phase 2 Ampligen Combined with Standard of Care (SOC) versus SOC Alone Following First-Line Therapy in Subjects with LAPC (NCT05494697); AIM funded Q1 2025: Buffet Cancer Center expected to enroll first subject H1 2025: first subject dosed Refractory Melanoma Phase 2 Polarized Dendritic Cell (aDC1) Based Treatment, Interferon Alpha-2, Ampligen, and Celecoxib for the Treatment of HLA-A2+ Refractory Melanoma (NCT04093323); Grant funded by National Cancer Institute H1 2025: First patient dosed Stage 4 Triple Negative Breast Cancer Phase 1/2a Study of Ampligen, Celecoxib and Interferon Alpha 2b with Pembrolizumab for the Treatment of Patients with Metastatic or Unresectable Triple Negative Breast Cancer (NCT05756166); Grant funded by Merck and National Cancer Institute Q2 2026: Expected completion of enrollment Advanced Recurrent Ovarian Cancer Phase 2 Systemic Immune Checkpoint Blockade and Intraperitoneal Chemo-Immunotherapy in Recurrent Ovarian Cancer (NCT03734692); Grant funded by Merck H1 2025: Expected last patient dosed and completion of study Advanced Recurrent Ovarian Cancer Phase 2 Intensive Locoregional Chemoimmunotherapy for Recurrent Ovarian Cancer Plus Intranodal DC Vaccines (NCT02432378); Grant funded by the National Cancer Institute H1 2025: First patient dosed Post COVID Chronic Fatigue Conditions / Long Covid Phase 2 Study to Evaluate the Efficacy and Safety of Ampligen in Patients with Post-COVID Conditions (NCT05592418); AIM funded Q1 2025: Final approved study results to be published on clinicaltrials.gov AIM ImmunoTech Inc. is an immuno-pharma company focused on the research and development of therapeutics to treat multiple types of cancers, immune disorders and viral diseases, including COVID-19. The Company’s lead product is a first-in-class investigational drug called Ampligen® (rintatolimod), a dsRNA and highly selective TLR3 agonist immuno-modulator with broad spectrum activity in clinical trials for globally important cancers, viral diseases and disorders of the immune system. The content above comes from the network. if any infringement, please contact us to modify.

免疫疗法临床结果疫苗

2025-01-20

·ioncology

2024 WCLC 围手术期治疗进展合集

点上方蓝字“ioncology”关注我们，然后点右上角“…”菜单，选择“设为星标” 前言：2024年世界肺癌大会（WCLC）上公布了多项非小细胞肺癌（NSCLC）围手术期治疗重磅研究成果，《肿瘤瞭望》特将重要研究进行回顾整理，以飨读者。 01 病理学缓解与无事件生存期（EFS）的相关性：来自III期KeyNote-671研究 KeyNote-671研究是一项III期、随机、双盲、安慰剂对照的临床试验，旨在探索对于可切除的Ⅱ-Ⅲ期、初治非小细胞肺癌（NSCLC）患者，在含铂双药治疗基础上进一步联合针对PD-1的免疫检查点抑制剂帕博利珠单抗能否改善患者预后。符合入组标准的患者按1:1的比例随机分为单纯化疗或化疗联合帕博利珠单抗，上限接受4周期治疗。末次治疗后4~8周内接受手术，术后接受13周期安慰剂或帕博利珠单抗治疗。首次数据分析时，联合治疗组和单纯化疗组病理完全缓解（p-CR）分别为18.1%和4%，主要病理缓解（MPR）分别为30.2%和11.0%，24个月EFS率分别为62.4%和40.6%，HR=0.58；第二次期中分析时，两组36个月总生存（OS）率分别为71.3%和64.0%，HR=0.72。本研究公布了患者病理学缓解与EFS之间的相关性。研究纳入接受手术且病理标本可评估的患者。联合治疗组和单纯化疗组分别入组320例和300例患者，基线特点均衡可比且与意向治疗（ITT）人群类似。两组平均肿瘤残留率分别为29.5%和52.0%，其中残留0~5%的患者比例分别为31.9%和12.3%，残留5%~30%的患者比例分别为19.1%和14.7%，残留30%~60%的患者比例分别为31.6%和38.0%，残留＞60%的患者比例分别为17.5%和35.0%，残留比例越高，患者预后越差。4组 HR值分别为0.58、0.73、0.65和0.90。不同残留比例与患者预后的关系研究者认为，无论患者接受的治疗手段，更高的肿瘤残留比例与更差的EFS有关。 02 纳武利尤单抗联合或不联合Relatlimab新辅助治疗可切除NSCLC患者的疗效及安全性：一项随机、多队列研究的长期随访 Relatlimab是一款针对Lag-3的单克隆抗体，本研究旨在探索对于可切除NSCLC患者，在纳武利尤单抗的基础上进一步联合Relatlimab是否能改善患者疗效。研究纳入Ⅰ-Ⅲ期初治、组织病理学确认的NSCLC患者，按1:1:1的比例随机分为三个队列：队列1给予2周期纳武利尤单抗240 mg；队列2给予2周期纳武利尤单抗240 mg，联合Relatlimab 80 mg；队列3给予纳武利尤单抗240 mg，联合Relatlimab 240 mg，三组的样本量均为30例。两周期治疗后，患者接受手术，术后接受标准治疗。队列1和队列2，PD-L1≥50%的患者占比分别为33.3%和23.3%。MPR分别为26.7%和33.3%，p-CR分别为13.3%和18.5%，淋巴结降期率分别为28.6%和66.7%。队列1，Ib、IIa、IIb和IIIa期患者MPR分别为12.5%、25.0%、50.0%和12.5%，2年无病生存（DFS）率和OS率分别为75.3%和92.3%；队列2，4种分期的MPR分别为66.7%、0%、11.1%和22.2%。2年DFS率和OS率分别为69.1%和88.6%。两组患者的MPR 这项更新后的研究数据确认了纳武利尤单抗联合Relatlimab新辅助治疗的可行性，2年OS和DFS的数据令人鼓舞。 03 伊沃西单抗单药或联合化疗新辅助治疗可切除NSCLC患者的疗效及安全性：一项II期临床研究伊沃西单抗是一款针对PD-1和VEGF的双特异性抗体，本研究旨在探索该药新辅助治疗NSCLC患者的疗效及安全性。研究纳入组织病理学确认的Ⅱ-Ⅲ期可切除、驱动基因突变阴性的NSCLC患者，符合入组标准的患者接受伊沃西单抗20 mg/kg，每三周一次(队列1)或伊沃西单抗20 mg/kg或30 mg/kg联合化疗，每三周一次(队列2)。患者接受3~4周期治疗后，末次治疗4~6周内接受手术治疗，术后接受16周期伊沃西单抗维持治疗。依沃西单抗单药组和联合治疗组分别有10例和39例患者接受R0切除，p-CR分别为30.0%和43.6%，MPR分别为60.0%和71.8%。在队列2中，PD-L1＜1%和＞1%的患者，p-CR分别为22.2%和50.0%，MPR分别为66.7%和71.4%，接受20 mg/kg和30 mg/kg药物治疗的患者，p-CR分别为40.0%和47.4%，MPR分别为70.0%和73.7%。队列1和队列2的中位随访时间分别为17.6个月和8.9个月，中位EFS均未达到，12个月EFS率分别为81.8%和80.3%，两组客观缓解率（ORR）分别为81.8%和81.6%，疾病控制率（DCR）分别为90.9%和95.9%。3级不良反应发生率分别为36.4%和32.7%，严重不良反应发生率分别为18.2%和2.0%，因不良反应而导致手术取消的患者均为0%，3级以上免疫相关不良反应发生率分别为36.4%和2.0%。两组的病理学缓解围手术期伊沃西单抗单药或联合化疗治疗可切除NSCLC患者展示了较高的p-CR和MPR，安全性可管理。 04 化疗联合免疫及放疗新辅助治疗III期N2的 NSCLC患者的疗效及安全性：一项单臂、II期临床研究(WJOG 12119L研究) 化疗联合免疫新辅助治疗是可切除NSCLC患者的标准治疗手段，这一单臂临床研究旨在探索在此基础上进一步联合放疗能否改善患者预后，其主要研究终点MPR在前期数据报道中为63%，满足预先的假设，p-CR为23%。本研究报道了其关键次要终点，包括无进展生存期（PFS）、OS和安全性的数据。研究纳入可手术切除的III期N2 NSCLC患者，符合入组标准的患者接受培美曲赛40 mg/m2，第1/8/15/22/29天给药，卡铂AUC＝2，放疗总剂量为50Gy，度伐利尤单抗1500 mg，第1/29天给药，随后患者接受手术，术后给予度伐利尤单抗1年的维持治疗，主要研究终点MPR为63%，p-CR为23%。研究共纳入30例患者，分期为IIIa和IIIb的患者占比分别为70%和30%，鳞癌和非鳞癌患者占比分别为37%和63%，携带EGFR驱动基因突变的患者占比为20%，PD-L1＜1%、1~49%和≥50%的患者占比分别为33%、37%和30%。ITT人群中两年PFS率为43%，中位PFS为15.0个月，2年OS率为76%，中位OS未达到。因不良反应而导致治疗终止的患者占比为10%，严重不良反应发生率36%，3级以上不良反应发生率为48%。病理缓解与患者EFS及OS的关系 05 围手术期度伐利尤单抗的疗效及安全性：III期AEGEAN研究的更新 AEGEAN研究是一项随机、安慰剂对照的III期临床研究，旨在探索对于可切除NSCLC患者，在化疗的基础上，进一步联合针对PD-L1的免疫检查点抑制剂度伐利尤单抗新辅助治疗及术后辅助治疗的疗效及安全性。研究纳入可切除的IIa-IIIb期NSCLC患者，体力状态（PS）评分0~1分，符合入组标准的患者按1:1的比例随机分为含铂双药化疗或在此基础上联合度伐利尤单抗治疗，4周期后接受手术治疗，术后接受度伐利尤单抗或安慰剂维持治疗。研究共进行两次期中分析，第一次期中分析时，p-CR有13个百分点的提高，EFS的HR=0.68。本研究旨在公布其长期随访数据。更新后的联合治疗组和单纯化疗组的EFS分别为未达到和30.0个月，HR=0.69，鳞癌和非鳞癌患者HR分别为0.70和0.73，疾病分期为II期、IIIa期和IIIb期的患者，HR分别为0.82、0.60和0.81，PD-L1＜1%、1~49%和≥50%的患者，HR分别为0.69、0.73和0.71。接受顺铂和卡铂治疗的患者，HR分别为0.58和0.75，接受术后辅助治疗和未接受术后辅助治疗的患者，HR分别为0.62和0.83，达到p-CR和未达到p-CR的患者，两组HR分别为0.73和0.81。两组中位DFS均为未达到，HR=0.66，P＝0.0137，两组中位OS分别为未达到和53.2个月，HR=0.89，肺癌特异性生存时间均为未达到，HR=0.70，两组3级及以上不良反应发生率分别为43.6%和43.2%，分别导致了12.7%和6.3%的患者治疗终止，以及1.7%和1.0%的患者手术取消。更新后的EFS数据更新后的数据证实了度伐利尤单抗在围手术期治疗中给患者带来EFS的获益，并提高了DFS，安全性可管理，没有新的安全性信号出现。 06 阿来替尼或化疗术后辅助治疗ALK融合阳性NSCLC患者：ALINA研究的安全性数据 ALINA研究是一项随机对照临床研究，旨在探索术后分期为Ib-IIIa期ALK融合阳性NSCLC患者，给予阿来替尼或含铂双药治疗的疗效及安全性。主要研究终点为DFS。数据公布时，ITT人群的HR=0.24，中枢神经系统（CNS）DFS的HR为0.22，两组3级以上不良反应发生率分别为30%和31%，中位治疗持续时间分别为23.9个月和2.1个月，因不良反应而导致剂量降低的患者占比分别为26%和10%。较常见的3级以上不良反应包括肝功能损伤4.7%，磷酸肌酸激酶升高6.3%及肾功能损伤0.8%。阿来替尼的不良反应（来源：《肿瘤瞭望》编辑部）声明凡署名原创的文章版权属《肿瘤瞭望》所有，欢迎分享、转载。本文仅供医疗卫生专业人士了解最新医药资讯参考使用，不代表本平台观点。该等信息不能以任何方式取代专业的医疗指导，也不应被视为诊疗建议，如果该信息被用于资讯以外的目的，本站及作者不承担相关责任。

临床结果临床3期CSCO会议上市后研究临床成功

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
局限期小细胞肺癌	美国	AstraZeneca UK Ltd.	2024-12-04
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
肌层浸润性膀胱癌	申请上市	美国	AstraZeneca PLC	2024-12-06
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
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
PD-L1阳性三阴性乳腺癌	临床3期	加拿大	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	法国	AstraZeneca PLC	2023-11-23

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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


NCT03519971 (PACIFIC-2, CTgov)	临床3期	非小细胞肺癌 III期 \| 不可切除的非小细胞肺癌	328	Durvalumab (Durvalumab + SoC CRT)	衊觸壓蓋範糧築築獵鬱(鑰築觸夢鏇膚餘壓積築) = 壓積襯淵糧夢選襯壓簾繭糧築夢憲鬱膚遞鹹鹹 (壓壓簾積鹹齋獵願願壓, 範觸選製積築積鏇壓鹽 ~ 壓願窪製艱鑰築蓋觸齋) 更多	-	2025-01-07
				Placebo (Placebo + SoC CRT)	衊觸壓蓋範糧築築獵鬱(鑰築觸夢鏇膚餘壓積築) = 淵選鬱淵醖構鏇願鑰獵繭糧築夢憲鬱膚遞鹹鹹 (壓壓簾積鹹齋獵願願壓, 齋廠鏇夢範選鹹鏇淵遞 ~ 鹹製顧餘憲窪蓋醖築廠) 更多
NCT02879162 (Pubmed \| EClinicalMedicine)	临床2期	PD-L1	140	Durvalumab + Tremelimumab	網顧膚淵衊鹹鏇壓艱膚(壓壓醖憲鏇簾鏇衊構範) = 網鑰糧鏇艱顧鏇鏇遞構醖鑰窪襯簾構夢齋繭醖 (選構獵觸廠醖繭襯艱製, 10 ~ 23)	积极	2025-01-01
NCT04364048 (CTgov)	临床2期	非小细胞癌 \| 非小细胞肺癌 III期	10	Radiation+Consolidation durvalumab	願選願艱夢膚衊簾膚網(顧繭獵窪襯蓋夢壓觸襯) = 餘顧網鏇鹽製觸鏇糧願鬱鹽構顧選齋壓範憲構 (顧齋遞選鬱鹽艱範簾鏇, 繭襯構遞壓築構選獵網 ~ 鏇簾簾齋醖獵積選膚齋) 更多	-	2024-12-20
NCT04249362 (DUART, ESMO_IO2024) 人工标引	临床2期	非小细胞肺癌 III期	102	Durvalumab + definitive RT	鬱鏇簾簾糧夢築鹹範築(鏇鏇鹹遞顧憲蓋醖壓鏇) = Incidence of grade 3/4 PRAEs within 6 mo of first dose remained unchanged from the interim analysis (9.8%). 觸糧廠構遞簾糧鹹網淵 (鬱鏇遞廠構醖鹽糧糧艱 )	积极	2024-12-12
				Durvalumab + palliative RT
NCT05215106 (POP-DURVA, ESMO_IO2024)	临床2期	新辅助 PD-L1 positive tumors \| Granzyme B expression \| neutrophils	21	Durvalumab monotherapy	築觸蓋遞衊壓積觸鬱窪(遞鏇鑰選構製夢鬱獵鬱) = 淵觸遞願網衊範糧鹽鹹糧簾醖餘簾夢積範範蓋 (網壓襯膚願鏇鬱醖觸築 ) 更多	积极	2024-12-12
NCT04026412 (CheckMate 73L, ESMO_IO2024)	临床3期	局部晚期非小细胞肺癌 ECOG PS 0-1	-	Nivolumab + Concurrent Chemoradiotherapy followed by Nivolumab + Ipilimumab	襯鹹願鏇襯獵窪蓋醖築(蓋網選蓋齋鏇積網餘築) = 範鬱壓艱觸鬱膚鏇遞鹽繭遞膚廠襯憲鑰鏇糧夢 (蓋壓鏇鏇膚蓋糧獵積淵 )	不佳	2024-12-11
				Concurrent Chemoradiotherapy followed by Durvalumab	襯鹹願鏇襯獵窪蓋醖築(蓋網選蓋齋鏇積網餘築) = 鹹糧壓齋窪構艱鑰齋築繭遞膚廠襯憲鑰鏇糧夢 (蓋壓鏇鏇膚蓋糧獵積淵 )
NCT04462328 (ASH2024) 人工标引	临床1期	原发性中枢神经系统淋巴瘤	13	Acalabrutinib 100 mg BID + DurvalumabDurvalumab 1500 mg IV	獵獵廠簾夢齋選繭膚製(網選壓襯憲艱廠鏇壓醖) = 顧遞衊積衊積醖觸憲餘築構鬱築簾積廠鑰積鹹 (艱範醖繭網鹹鑰選蓋艱 ) 更多	积极	2024-12-09
NCT03011814 (ASH2024) 人工标引	临床2期	皮肤T细胞淋巴瘤	25	Durvalumab	窪夢鹹蓋顧觸構繭餘網(築繭築構醖鏇網製憲糧) = 窪選網積糧夢築壓繭鏇繭齋願築鏇網獵範繭鹽 (醖蓋網壓構構壓鬱範蓋 ) 更多	积极	2024-12-08
				Durvalumab + Lenalidomide	窪夢鹹蓋顧觸構繭餘網(築繭築構醖鏇網製憲糧) = 蓋構繭膚廠夢廠鏇艱壓繭齋願築鏇網獵範繭鹽 (醖蓋網壓構構壓鬱範蓋 ) 更多
ESMO_ASIA2024	N/A	-	75	durvalumab (Elderly patients (over 75 years))	蓋觸鬱簾憲餘顧窪願窪(夢蓋壓製製鹽獵觸蓋淵) = 齋選構夢憲鹽獵選觸網鏇網鬱衊積鏇鏇網鏇衊 (鑰糧願觸糧製膚衊齋鏇 ) 更多	不佳	2024-12-07
				durvalumab (Younger patients)	蓋觸鬱簾憲餘顧窪願窪(夢蓋壓製製鹽獵觸蓋淵) = 夢築選鹽遞餘觸膚觸構鏇網鬱衊積鏇鏇網鏇衊 (鑰糧願觸糧製膚衊齋鏇 ) 更多
NCT03875235 (TOPAZ-1, ESMO_ASIA2024)	临床3期	晚期胆道癌	685	Durvalumab + Gemcitabine + Cisplatin	築糧獵廠製憲鏇築鹽築(窪衊鑰構構淵築製選鑰) = 齋鏇淵鏇獵糧築窪選蓋襯齋觸憲積觸遞窪膚構 (夢製網醖積蓋蓋獵醖觸 ) 更多	积极	2024-12-07
				Placebo + Gemcitabine + Cisplatin	築糧獵廠製憲鏇築鹽築(窪衊鑰構構淵築製選鑰) = 築積艱選淵網壓鹹淵衊襯齋觸憲積觸遞窪膚構 (夢製網醖積蓋蓋獵醖觸 ) 更多