预约演示

更新于：2026-03-19

Atezolizumab

阿替利珠单抗

更新于：2026-03-19

概要

基本信息

药物类型

单克隆抗体

别名

Anti-PDL-1-Genentech/Roche、Atezolizumab (Genetical Recombination)、Atezolizumab (genetical recombination) (JAN)

+ [11]

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

肿瘤免疫系统疾病消化系统疾病+ [10]

在研适应症

结外NK-T细胞淋巴瘤晚期非小细胞肺癌乳腺癌+ [179]

非在研适应症

大肠腺癌肺腺癌晚期胆管癌+ [110]

原研机构

Genentech, Inc.

Universitair Medisch Centrum Groningen

在研机构

F. Hoffmann-La Roche Ltd.

Nykode Therapeutics ASAHoffmann-La Roche, Inc.

+ [26]

非在研机构

SanofiReplimune, Inc.

Basilea Pharmaceutica AG

+ [10]

权益机构

NeoImmuneTech, Inc.

Harpoon Therapeutics, Inc.Novocure, Inc.

+ [26]

最高研发阶段批准上市

首次获批日期

美国 (2016-05-18),

尿路上皮癌

最高研发阶段(中国)批准上市

特殊审评突破性疗法 (美国)、加速批准 (美国)、孤儿药 (美国)、优先审评 (中国)、附条件批准 (中国)、孤儿药 (日本)、优先审评 (澳大利亚)、孤儿药 (澳大利亚)、快速通道 (美国)

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结构/序列

Sequence Code 122091L

来源: *****

Sequence Code 4720027H

来源: *****

关联

883

项与阿替利珠单抗相关的临床试验

NCT07322341

/ Not yet recruiting临床2期IIT

A Phase 2 Trial of SX-682 and Atezolizumab in Patients With Advanced NSCLC Who Progressed on Prior Chemotherapy and Immune Checkpoint Inhibitor (ICI) Therapy

This phase II trial tests how well SX-682 and atezolizumab works for the treatment of non-small cell lung cancer (NSCLC) that may have spread from where it first started to nearby tissue, lymph nodes, or distant parts of the body (advanced) or that has spread from where it first started (primary site) to other places in the body (metastatic), and has come back after a period of improvement (recurrent). SX-682 blocks proteins that may be able to stimulate the immune system to kill and eliminate tumor cells. Immunotherapy with monoclonal antibodies, such as atezolizumab, may help the body's immune system attack the cancer, and may interfere with the ability of tumor cells to grow and spread. Giving SX-682 and atezolizumab may be effective for the treatment of advanced or metastatic, recurrent NSCLC.

开始日期2026-06-01

申办/合作机构

University of Washington

[+3]

NCT07472517

/ Not yet recruiting临床3期

DAREON ® -Lung-1: A Phase III Multi-center, Open-label, Randomised Trial of Intravenous Obrixtamig in Combination With Atezolizumab, Carboplatin, and Etoposide vs. Atezolizumab, Carboplatin, and Etoposide as First-line Treatment in Patients With Extensive-stage Small Cell Lung Cancer

This study is open to adults with advanced small cell lung cancer (SCLC). The purpose of this study is to find out if a study medicine called obrixtamig plus standard treatment (atezolizumab, carboplatin, and etoposide) improves survival when compared to standard treatment alone. Obrixtamig is an antibody-like molecule that may help the immune system fight cancer. Another purpose of the study is to test a medical device being developed to measure levels of the tumour marker DLL3.
Participants are put into 2 groups randomly, which means by chance. One group receives obrixtamig and standard treatment. The other group receives standard treatment without obrixtamig. All treatments are given as infusions into a vein.
Participants are in the study for up to 3 years. During this time, they visit the study site regularly. Participants in the group receiving obrixtamig stay overnight at the study site following the first 2 obrixtamig treatments. At the visits, doctors check the size of the tumour(s). The results are compared between the 2 groups to see whether the treatment works. The doctors also regularly check participants' health and take note of any unwanted effects.

开始日期2026-04-10

申办/合作机构

Boehringer Ingelheim GmbH

NCT07388524

/ Not yet recruiting临床3期IIT

Evaluating Adjuvant Atezolizumab or Atezolizumab and Hyaluronidase-TQJS to Prevent Recurrence in Stage I Non-Small Cell Lung Cancer (NSCLC): A Randomized Phase III Trial (AASI-NSCLC)

This phase III trial compares the effect of atezolizumab (or atezolizumab and recombinant human hyaluronidase) to standard observation for preventing cancer return after surgery (recurrence) in patients who have undergone a complete surgical removal (resection) of stage I non-small cell lung cancer (NSCLC). Patients who have undergone resection for lung cancer are typically followed by observation or active surveillance, which involves closely watching a patient's condition but not giving treatment unless there are changes in test results. During active surveillance, patients are given certain exams and tests done on a regular schedule. Immunotherapy with monoclonal antibodies, such as atezolizumab, may help the body's immune system attack the cancer, and may interfere with the ability of tumor cells to grow and spread. Atezolizumab and recombinant human hyaluronidase is a formulation of atezolizumab combined with an enzyme called hyaluronidase, which helps increase tissue absorption of the drug. Giving atezolizumab or atezolizumab and recombinant human hyaluronidase after resection may be effective for preventing NSCLC recurrence, and may be a better approach to treating patients with stage I NSCLC than the usual observation approach.

开始日期2026-04-09

申办/合作机构

National Cancer Institute

100 项与阿替利珠单抗相关的临床结果

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100 项与阿替利珠单抗相关的转化医学

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100 项与阿替利珠单抗相关的专利（医药）

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3,994

项与阿替利珠单抗相关的文献（医药）

2026-05-01·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Efficacy of immune checkpoint inhibitors in the first line therapy of non-squamous non-small cell lung cancer: A systematic review and network meta-analysis

Review

作者: Mironenko, Olga ; Fedyanin, Mikhail ; Zhukov, Nikolai ; Sapozhnikov, Kirill ; Sableva, Natalia ; Tolkacheva, Daria ; Moiseenko, Fedor ; Lazarev, Andrei

AIM:

By 2026, several PD-1/PD-L1 antibodies were approved by FDA, EMA and non-EU Eastern European countries for the first-line therapy in advanced non-squamous non-small cell lung cancer (nsNSCLC) without EGFR mutations or ALK alterations. This study aimed to compare overall (OS) and progression-free (PFS) survival among anti-PD-1/PD-L1-containing regimens and to evaluate the immunotherapy effect modification due to PD-L1 expression.

METHODS:

A systematic search in MEDLINE and Embase on December 23, 2025 identified 15 Phase III randomized clinical trials involving adults with advanced nsNSCLC treated with therapies containing prespecified anti-PD-1/PD-L1 agents. Bayesian multilevel network meta-regressions with M-splines were estimated for OS and PFS, incorporating covariates for PD-L1 expression (TPS <1% versus ≥1%) and its interaction with the treatment class (anti-PD-1/PD-L1-based regimens versus chemotherapy ± bevacizumab).

RESULTS:

Regardless of PD-L1 expression, treatments with the highest probability of being the best (SUCRA) by OS are prolgolimab + chemotherapy, pembrolizumab + chemotherapy and cemiplimab + chemotherapy (SUCRA 0.80-0.94), by PFS nivolumab + bevacizumab + chemotherapy and atezolizumab + bevacizumab + chemotherapy (SUCRA 0.91-0.96). The hazard ratio for the interaction between PD-L1-negative status and anti-PD-1/PD-L1-containing therapy was 1.09 (95% CrI, 0.95-1.25) for OS and 1.41 (95% CrI, 1.16-1.71) for PFS.

CONCLUSION:

For advanced nsNSCLC patients, irrespective of PD-L1 expression, prolgolimab, pembrolizumab or cemiplimab, each combined with chemotherapy, are most efficacious by OS; nivolumab or atezolizumab combined with bevacizumab and chemotherapy demonstrate the highest PFS. PD-L1 expression does not modify the effect of examined immunotherapy options on OS, though the opposite is true for PFS.

2026-05-01·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Viral hepatitis and immunotherapy outcome in advanced hepatocellular carcinoma: A comprehensive umbrella review of 15 meta-analyses

Review

作者: Dottorini, Lorenzo ; De Giorgi, Annamaria ; Tomasello, Gianluca ; Colombo, Silvia ; Ghidini, Michele ; Petrelli, Fausto ; Ghilardi, Mara ; Carcano, Giulio

BACKGROUND:

First-line systemic therapy for unresectable/advanced hepatocellular carcinoma (HCC) now prioritizes immune checkpoint inhibitor (ICI)-based combinations, but whether viral hepatitis etiology modifies benefit remains clinically uncertain.

OBJECTIVE:

To synthesize meta-analytic evidence for first-line systemic therapy in unresectable/advanced HCC, assessing hepatitis B (HBV), hepatitis C (HCV), and nonviral etiology as effect modifiers. This umbrella review uniquely quantifies overlap across meta-analyses and applies credibility grading to clarify the strength of evidence for etiology-stratified outcomes.

DESIGN:

Umbrella-style systematic review of systematic reviews with pairwise meta-analyses (network meta-analyses excluded). PubMed/MEDLINE, EMBASE, and the Cochrane Library were searched from inception to 1 December 2025. Pooled hazard ratios (HRs) for overall survival (OS) and progression-free survival (PFS), etiology-stratified/interaction analyses were extracted, and overlap was quantified using corrected covered area (CCA).

RESULTS:

Fifteen meta-analyses/quantitative syntheses (2021-2025) were included. Across phase III RCT meta-analyses, immune-based combinations improved OS and PFS versus sorafenib/lenvatinib (ICI+targeted therapy: OS HR 0.71, 95% CI 0.62-0.82; PFS HR 0.62, 95% CI 0.54-0.71; PD-(L)1 inhibitor+antiangiogenic therapy: OS HR 0.69, 95% CI 0.53-0.89; PFS HR 0.60, 95% CI 0.53-0.67). In etiology-stratified PD-(L)1 inhibitor+antiangiogenic RCT meta-analyses, OS benefit was larger in HBV (HR 0.64, 0.55-0.74) than in nonviral etiology (HR 0.91, 0.75-1.11); a predictor meta-analysis supported effect modification (interaction P = 0.02 for OS; P < 0.01 for PFS). Real-world head-to-head meta-analyses comparing atezolizumab-bevacizumab versus lenvatinib were inconsistent. Overlap across meta-analyses was very high (CCA 44.4% among RCT meta-analyses; 52.4% among real-world syntheses).

CONCLUSION:

ICI-based combinations are effective first-line therapy for unresectable/advanced HCC. Viral hepatitis status, particularly HBV, may be associated with larger relative benefit than nonviral etiology, but subgroup and real-world findings require cautious interpretation. This synthesis clarifies the strength and limitations of current evidence and identifies priority areas for prospective validation, with direct implications for treatment selection as nonviral HCC becomes more prevalent.

2026-04-01·LUNG CANCER

Real-world comparative effectiveness of atezolizumab versus durvalumab for extensive-stage small-cell lung cancer

Article

作者: Yamamoto, Ryo ; Sakaguchi, Tadashi ; Koshio, Jun ; Takigami, Ayako ; Maemondo, Makoto ; Sugawara, Shunichi ; Hara, Shuichiro ; Aiba, Tomoiki ; Sakashita, Hiroyuki ; Tominaga, Shinichiro ; Ando, Yumi

BACKGROUND:

Both atezolizumab and durvalumab combined with platinum-etoposide have become standard first-line treatments for extensive-stage small-cell lung cancer (ES-SCLC), yet head-to-head real-world comparative data remain scarce.

METHODS:

We conducted a multicenter retrospective cohort study of 234 patients with ES-SCLC treated with atezolizumab plus platinum-etoposide (AEP; n = 126) or durvalumab plus platinum-etoposide (DEP; n = 108) across five Japanese institutions between 2016 and 2023. Progression-free survival (PFS) and overall survival (OS) were compared using Kaplan-Meier and overlap-weighted Cox models. Safety, a cost-effectiveness (cost-minimization) analysis based on restricted mean survival time-derived quality-adjusted life years (QALYs), and second-line treatment outcomes were also evaluated.

RESULTS:

Median PFS was 5.0 months for AEP and 5.1 months for DEP (hazard ratio [HR] 0.96; 95% CI, 0.73-1.26), and median OS was 12.0 and 12.1 months for AEP and DEP, respectively (HR 0.94; 95% CI, 0.68-1.31). Safety profiles were broadly equivalent between groups. Economic analysis showed nearly identical QALYs (1.002 vs 1.011) but lower total direct medical cost for AEP (¥4.14 million vs ¥4.88 million). Among 128 patients receiving second-line chemotherapy, those with platinum-sensitive relapse had significantly longer OS than those with platinum-refractory relapse, regardless of regimen.

CONCLUSIONS:

In real-world practice, AEP and DEP demonstrated equivalent efficacy and safety as first-line treatment for ES-SCLC. Given its lower cost with comparable QALYs, AEP may represent the more cost-minimizing option. The prognostic distinction between sensitive and refractory relapse remains clinically relevant after chemoimmunotherapy.

3,142

项与阿替利珠单抗相关的新闻（医药）

2026-03-19

·BioSpace

Oncolytics Biotech® to Present New Mechanistic and Translational Data Supporting Pelareorep as an Immune-Priming Backbone at AACR 2026

Pelareorep treatment drives coordinated immune activation and tertiary lymphoid structure formation Translational data suggest potential to boost response to immunotherapy and targeted therapy in RAS-driven tumors Pelareorep’s ability to engage the innate and adaptive immune system results in doubling or nearly tripling response rates in breast and gastrointestinal cancers SAN DIEGO, March 19, 2026 (GLOBE NEWSWIRE) -- Oncolytics Biotech ® Inc. (Nasdaq: ONCY) (“Oncolytics” or the “Company”), a clinical-stage immunotherapy company developing pelareorep, today announced two abstracts across distinct tumor types were accepted for presentation at the American Association for Cancer Research (“AACR”) Annual Meeting 2026, at the San Diego Convention Center from April 17-22, 2026. Pelareorep is an investigational, systemically delivered immunotherapy that has been shown to activate innate immune-sensing pathways via double‑stranded RNA signaling, driving interferon production, dendritic cell activation, and cytotoxic T‑cell priming. “These new translational findings strengthen our understanding of pelareorep as a systemic immune‑priming agent that reshapes the tumor microenvironment,” said Jared Kelly, Chief Executive Officer of Oncolytics. “The coordinated immune activation and tertiary lymphoid structure formation we are observing support pelareorep as a foundational backbone for combination therapy across multiple tumor types, including RAS-driven cancers. RAS mutations are especially prevalent in deadly cancers, including roughly 95% of pancreatic cancers and 45% of colorectal cancers. As we advance registrational programs in gastrointestinal cancers, we believe pelareorep will enhance immunotherapy activity and potentially help patients who did not respond initially.” Biomarker data from cohort 1 of the Phase 1/2 GOBLET trial in advanced pancreatic cancer suggest pelareorep plus atezolizumab and gemcitabine/nab-paclitaxel can shift tumors toward a more immune-active state. Patients with an immune activation signature after four weeks were more likely to achieve durable clinical benefit, supporting a potential biomarker. Pancreatic cancer continues to pose a significant unmet clinical need, with approximately 510,000 new cases reported globally each year. 1 Additionally, new first-of-its-kind data from AWARE-1 show pelareorep can drive coordinated anti-tumor immune responses, including tertiary lymphoid structure (“TLS”) formation, helping make immunologically cold tumors more susceptible to immunotherapy. This could include patients who have failed checkpoint inhibitors, representing a significant portion of the patient population and a meaningful unmet need in oncology. Pelareorep has also been shown to stimulate RAS-specific T-cell clones in gastrointestinal cancers, which may enhance its ability to target RAS-mutated tumor cells. The Company will present more data on this topic at an upcoming scientific meeting. Together, the data support pelareorep as a novel immune‑priming strategy capable of enhancing the activity of multiple therapeutic classes, including checkpoint inhibitors, targeted therapies, chemotherapy, and emerging immuno‑oncology modalities. Abstract: Pelareorep combined with atezolizumab and chemotherapy shows immune conversion activity in advanced pancreatic cancer: Biomarker results of cohort 1 of the GOBLET trial New biomarker data from cohort 1 of the Phase 1/2 GOBLET study demonstrated that pelareorep in combination with atezolizumab, gemcitabine, and nab-paclitaxel led to meaningful immune activation in patients with metastatic pancreatic ductal adenocarcinoma (“mPDAC”). An exploratory analysis integrating routine serum markers, a 172-protein circulating panel, selected T-cell receptor sequencing, and clinical outcomes found early on-treatment changes showed increases in adaptive immune and cytotoxicity-associated proteins, including interferon signaling and CD8+/NK-related markers, alongside decreases in tumor/stroma-associated proteins. A 14-protein signature linked to oncolytic activity stratified patients at Week 4 into ‘hot’ vs. ‘cold’ immune phenotypes relative to baseline. Patients demonstrating immune activation signatures experienced longer median progression-free survival (7.5 months) compared with patients who did not exhibit similar immune responses (5.6 months). As previously reported, the combination of pelareorep, atezolizumab, gemcitabine, and nab-paclitaxel demonstrated a 62% objective response rate in first-line mPDAC patients, more than double the response rates historically observed with chemotherapy alone. Abstract: Imaging mass cytometry of pelareorep treated early breast cancer samples reveals developing tertiary lymphoid structures AWARE-1 is a window-of-opportunity study evaluating the effects of pelareorep in early-stage breast cancer. In biopsies from Cohort 2 (n=8), cellular neighborhood analysis identified immune-cell clusters, including cytotoxic T cells, dendritic cells, T helper cells, activated T helper cells, B cells, differentiated B cells, and M2 macrophages. Interactions between these cells developed into TLS in select patients. TLS function as localized immune hubs that facilitate antigen presentation, T‑cell activation, and sustained anti‑tumor immune responses. Published studies link TLS formation with improved responses to immunotherapy. These findings support pelareorep’s potential to expand cytotoxic T cells, activate dendritic cells, and promote TLS formation, helping to convert immunologically ‘cold’ tumors into immune-responsive ‘hot’ tumors. About GOBLET The GOBLET ( G astrointestinal tum O rs exploring the treatment com B inations with the oncolytic reovirus pe L ar E orep and an T i-PD-L1) study is a phase 1/2 multiple indication study in advanced or metastatic gastrointestinal tumors. The study is being conducted at 17 centers in Germany and is being managed by AIO-Studien-gGmbH. The co-primary endpoints of the study are objective response rate and/or disease control rate and safety. Key secondary and exploratory endpoints include additional efficacy assessments and evaluation of potential biomarkers. The study comprises five treatment groups: Pelareorep in combination with atezolizumab, gemcitabine, and nab-paclitaxel in 1 st line advanced/metastatic pancreatic cancer patients; Pelareorep in combination with atezolizumab in 1 st line MSI (microsatellite instability)-high metastatic colorectal cancer patients; Pelareorep in combination with atezolizumab and TAS-102 in 3 rd line metastatic colorectal cancer patients Pelareorep in combination with atezolizumab in 2 nd line advanced and unresectable anal cancer patients; and Pelareorep in combination with mFOLFIRINOX with and without atezolizumab in newly diagnosed metastatic PDAC patients. About AIO AIO-Studien-gGmbH (AIO) emerged from the study center of the medical oncology working group within the German Cancer Society (DKG). AIO operates with a non-profit purpose of promoting science and research with a focus on medical oncology. Since its foundation, AIO has become a successful sponsor and study management company and has established itself both nationally and internationally. About AWARE-1 AWARE-1 was an open-label window-of-opportunity study in early-stage breast cancer. The study combined pelareorep, without or with atezolizumab, and standard of care therapy according to breast cancer subtype. Tumor tissue was collected from patients as part of their initial breast cancer diagnosis, again on day three following initial treatment, and finally at three weeks following treatment, on the day their tumor is surgically resected. Key objectives of the study were to confirm that pelareorep is acting as a novel immunotherapy, to evaluate potential synergy between pelareorep and checkpoint blockade, and to collect biomarker data. The primary endpoint of the translational study was overall CelTIL score (a measurement of cellularity and tumor-infiltrating lymphocytes that is associated with favorable clinical outcomes). Secondary endpoints for the study included safety and tumor and blood-based biomarkers. The combination of pelareorep, letrozole, and atezolizumab resulted in 60% of patients experiencing 30% or greater increases in their CelTIL score. Reference Leiphrakpam PD, Chowdhury S, Zhang M, et al. Trends in the Global Incidence of Pancreatic Cancer and a Brief Review of its Histologic and Molecular Subtypes. J Gastrointest Cancer. 2025 Feb 24;56(1):71. About Oncolytics Biotech Inc. Oncolytics is a clinical-stage biotechnology company developing pelareorep, an investigational intravenously delivered double-stranded RNA immunotherapeutic agent. Pelareorep has demonstrated encouraging results in multiple first-line pancreatic cancer studies, two randomized Phase 2 studies in metastatic breast cancer, and early-phase studies in anal and colorectal cancer. It is designed to induce anti-cancer immune responses by converting immunologically “cold” tumors “hot” through the activation of innate and adaptive immune responses. The Company is advancing pelareorep in combination with chemotherapy and/or checkpoint inhibitors in metastatic gastrointestinal cancers, where pelareorep has received Fast Track designation from the FDA for colorectal and pancreatic cancer. Oncolytics is actively pursuing strategic partnerships to accelerate development and maximize commercial impact. For more about Oncolytics, please visit: or follow the Company on social media on LinkedIn and on X @ oncolytics . Tecentriq ® (atezolizumab) is a registered trademark of Genentech, a member of the Roche Group. Forward-looking statements This press release contains forward-looking statements, within the meaning of Section 21E of the U.S. Securities Exchange Act of 1934, as amended, and forward-looking information under applicable Canadian securities laws (such forward-looking statements and forward-looking information are collectively referred to herein as “forward-looking statements”). Forward-looking statements contained in this press release include statements regarding beliefs as to the potential, registration, mechanism of action and benefits of pelareorep as a cancer therapeutic; the Company’s goals, strategies, and objectives; expectations around the timing of the AACR Annual Meeting 2026; expectations as to the content and potential opportunities associated with the findings from the various studies expected to be presented via abstracts in the future; expectations around the design, milestones, anticipated timelines and expected outcomes for current and future studies; anticipated timelines and objectives for future meetings with regulatory bodies, including the FDA; and its belief in the clinical promise of pelareorep in anal, colorectal, pancreatic and other gastrointestinal cancers as well as breast cancer. In any forward-looking statement in which Oncolytics expresses an expectation or belief as to future results, such expectations or beliefs are expressed in good faith and are believed to have a reasonable basis, but there can be no assurance that the statement or expectation or belief will be achieved. These statements involve known and unknown risks and uncertainties that may cause actual results to differ materially from those anticipated. These risks include, but are not limited to, regulatory outcomes, trial execution, financial resources, access to capital markets, and market dynamics. Please refer to Oncolytics’ public filings with securities regulators in the United States and Canada for more information. The Company assumes no obligation to update forward-looking statements, except as required by law. Company Contact Jon Patton Director of IR & Communication jpatton@oncolytics.ca

临床结果免疫疗法快速通道临床2期AACR会议

2026-03-18

·药队长知识百科

日本肝癌防控凭什么出圈？揭秘全球标杆的核心密码

日本在肝癌防控工作上收获了令世界瞩目的成果，其国内肝癌的发病率与死亡率均呈现出持续降低的态势，患者5年生存率更是大幅提高，达到了42.2%。日本在肝癌防控领域所取得的出色成绩，使其毫无争议地成为了全球该领域的标杆性国家。对日本在肝癌防控方面的成功经验进行深入剖析可知，其关键在于构建起了一个科学合理、高效运转的防控体系。该体系以预防作为根本立足点，将早期诊断与及时治疗作为关键要点，把综合治疗作为重要支撑，进而构建起了全方位、多层次的肝癌防控网络。这一体系的建立与推行，为日本的肝癌防控工作提供了稳固的保障与有力的支持。图源：kaiserpermanente.org 依据世界卫生组织（WHO）发布的报告以及多项国际研究数据，均能证实日本在病毒性肝炎防控方面成效斐然。具体来看，日本乙肝表面抗原（HBsAg）的流行率仅为0.2% - 0.3%，大幅低于全球平均水平。近些年来，日本政府通过推行国家层面的肝炎防控行动计划、大力推行肝炎筛查项目、为患者提供治疗费用补助等一系列措施，进一步减轻了肝炎带来的疾病负担，为肝癌防控筑牢了坚实根基。当下，日本在肝癌防控领域的表现得到了国际社会的广泛认同，被看作是“全球典范”。这一成就主要得益于以下三项具有重要战略意义的关键举措： 01 科学完备的早期筛查体系日本自20世纪90年代起就构建了全国性的肝癌防控体系，把甲胎蛋白（AFP）、异常凝血酶原（DCP/PIVKA - II）、AFP - L3%这三项血清学指标纳入医保报销范畴，并与超声检查等影像学诊断技术有效结合，形成了科学完备的筛查方案。针对不同风险程度的人群，日本制定了个性化的筛查策略。对于一般高危人群，每6个月开展一次血清学联合检测与超声检查；对于极高危人群，将筛查间隔缩短至3 - 4个月。这一精准的筛查策略成效显著，使得超过68%的肝癌病例能够在早期就被及时察觉，极大地提高了患者接受根治性治疗的可能性，显著改善了患者的生存预后。图源：drugtargetreview.com 02 具备全球前沿的治疗技术在微创技术领域，日本医疗机构普遍运用腹腔镜手术、达芬奇机器人手术等先进微创手段。这些技术具备创伤微小、术中出血量低、住院时长短、术后恢复迅速等优点。以日本顺天堂医院为例，该院借助达芬奇机器人手术系统以及腹腔镜手术技术，有效减轻了肝癌患者的手术创伤，加速了术后恢复进程，整体治疗效果得到显著提升。日本学者开展的一项针对378例早期肝癌患者（巴塞罗那肝癌分期0 - A期）的回顾性研究显示：接受腹腔镜手术的患者，5年总生存率达到75.8%；5年无复发生存率超过70%。另一项针对巴塞罗那B期（中期）肝癌的研究表明：采用腹腔镜切除术，术后并发症发生率约为14.3%，住院时间约9天，总生存率方面，1年为89.1%，3年为70.4%，5年为58.4%，均优于开腹手术。在质子治疗方面，日本拥有24家专业的质子治疗机构，数量居世界前列。临床数据表明，对于无法手术的肝癌患者，质子治疗的3年局部无进展生存率与总生存率分别高达95.2%和86.4%，同时对正常肝组织的损伤大幅降低。值得一提的是，对于体积超过10cm的巨块型肝癌，质子治疗后的2年局部控制率达87%，且治疗过程中未出现任何3级及以上严重毒性反应。即便对于80岁及以上的肝癌患者，质子治疗同样能取得较好效果。日本筑波大学附属医院质子治疗中心的临床实践显示，该中心收治的所有80岁以上肝癌患者，接受质子治疗后，3年总体生存率达62%，这一结果明显优于传统放疗效果。与传统放疗相比，质子治疗可使正常肝组织受到的照射剂量降低70%，放射性肝病的发生率从22.3%降至2.3%，提高了治疗的安全性。在药物治疗方面，日本在肝癌新药研发与应用上处于国际领先水平。免疫治疗药物（如阿替利珠单抗、贝伐珠单抗）及多种靶向治疗药物（如索拉非尼、乐伐替尼、瑞戈非尼、卡博替尼、贝伐珠单抗和雷莫芦单抗等）均率先在日本获批。同时，日本医疗机构十分重视药物副作用的管理，通过精细化的用药指导，提升了患者的治疗耐受性和生活质量。以阿替利珠单抗联合贝伐珠单抗（T + A方案）为例，一项涵盖日本患者的国际多中心研究显示：该方案用于晚期肝癌患者时，中位总生存期可达18.2个月，客观缓解率达25.3%。基于这些数据，日本厚生劳动省（MHLW）已批准该方案用于晚期肝癌患者的一线治疗。另外，该方案在HCV相关肝癌患者中展现出更优的免疫激活效应，主要原因是HCV感染患者PD - L1表达水平较高，对PD - L1抑制剂的治疗反应更佳。图源：oncologynews.com 03 全程营养支持与多学科协同在营养管理层面，日本医疗机构组建了专业的营养师团队，依据每位患者的具体病情状况，量身定制个性化饮食方案。这些方案着重补充支链氨基酸、优质蛋白等关键营养元素，切实改善了患者的肝功能以及肌肉流失状况。营养干预涵盖以下几个关键环节：全方位营养评估与动态监测日本医疗机构会安排专业营养师对患者展开系统评估，涵盖身体成分分析、肝功能指标检测、代谢状态评估等方面，以此精准把握患者的个体化营养需求。例如，针对肝硬化合并肝癌患者，会特别重视支链氨基酸的补充，以改善肌肉流失和肝功能情况。术前，通过口服营养补充剂或肠内营养手段改善患者的营养状态；术后，依据恢复情况调整饮食方案，鼓励患者尽早经口进食，必要时采用肠内或肠外营养支持；对于放化疗引发的胃肠道反应，为患者提供易消化的食物，并搭配营养制剂，维持营养均衡。图源：healthcare-in-europe.com 个性化的饮食定制方案根据患者的具体病情（如肝功能分级、肿瘤分期）、身体状况以及治疗副作用来制定饮食方案。例如，对于存在腹水的患者，严格限制钠盐摄入；对于食欲不振的患者，采取少食多餐的进食方式。在多学科协作方面，日本医疗机构构建了固定的MDT（多学科诊疗）团队工作机制，确保复杂病例能够获得最优化的综合治疗方案。例如，对于不可切除的肝癌，采用TACE联合PD - 1抑制剂（如帕博利珠单抗） + 仑伐替尼的综合治疗策略，患者的中位无进展生存期（PFS）可达14.6个月，相较于单纯TACE治疗延长了4.6个月。在随访制度方面，要求患者在术后3年内必须定期复查。具体安排为每3个月进行一次全面检查，检查项目包括增强CT扫描、肿瘤标志物检测等多项指标，确保能够及时发现并处理可能的复发或转移情况。综上所述，日本在肝癌治疗领域取得的显著成效以及较高的患者生存率，关键在于构建了一个完整、高效的“早期诊断 - 精准治疗 - 全程管理”三位一体的闭环医疗体系。这一体系不仅为日本国民的健康提供了坚实保障，也为全球肝癌防控工作树立了典范，值得各国学习与借鉴。参考来源： [1]HBV“Viral Elimination” in the Asia-Pacific region:Current status and challenges.Clin Liver Dis (Hoboken) 2024. [2]肝癌三项(AFP、AFP-L3%、DCP)与GALAD、类GALAD模型临床应用专家共识[J].检验医学,2023. [3]Perioperative and long-term survival outcomes of laparoscopic versus laparotomic hepatectomy for BCLC stages 0-A hepatocellular carcinoma patients associated with or without microvascular invasion:a multicenter,propensity score matching analysis. [4]Comparison of outcomes between laparoscopic vs.open liver resection for intermediate stage hepatocellular carcinoma [5]Phase II Study of Hypofractionated Proton Beam Therapy for Hepatocellular Carcinoma. Front Oncol.2020. [6]Atezolizumab plus bevacizumab in unresectable hepatocellular carcinoma.New England Journal of Medicine,2020. [7]Transarterial chemoembolization combined with atezolizumab plus bevacizumab in advanced hepatocellular carcinoma:A real-world study from Japan.ASCO,2025. 免责声明：本公众号内容仅作交流参考使用，不作为诊断及医疗依据，专业医学问题请咨询专业人士或专业医疗机构。 “药队长”积极链接日本前沿医疗资源，为意向赴日就医患者提供日本知名医生远程联合会诊（MDT）、赴日就医、赴日体检等一站式解决方案。如果您想了解更多肝癌的治疗内容，或有意向前往日本寻求专家诊治的，可以长按识别下方二维码免费咨询药队长微信客服。

2026-03-18

·生物药大时代

小细胞肺癌新希望！DLL3/CD3双抗三联疗法进入III期试验

声明：因水平有限，错误不可避免，或有些信息非最及时，欢迎留言指出。本文仅作医疗健康相关药物介绍，非治疗方案推荐（若涉及）;本文不构成任何投资建议。近日，勃林格殷格翰宣布其DLL3/CD3 双抗 obrixtamig 联合免疫治疗和化疗的三联疗法正式启动全球 III 期临床试验（DAREON-Lung-1），有望为小细胞肺癌（SCLC）这一 “难治性肿瘤” 带来全新治疗标准。小细胞肺癌：被遗忘的 “难治性肿瘤” 小细胞肺癌是一种侵袭性极强的神经内分泌肿瘤，约占肺癌总数的 15%，每年全球新发患者超过 20 万例。由于其具有生长速度快、早期易转移、对化疗敏感但易复发的特点，患者的预后极差 ——5 年生存率仅为 7%-10%，广泛期患者的中位生存期不足 18 个月，甚至短于许多晚期实体瘤。过去 40 年，小细胞肺癌的治疗进展缓慢。20 世纪 80 年代，依托泊苷联合化疗成为一线标准治疗，将中位生存期从 3 个月延长至 10 个月；2018 年，免疫检查点抑制剂联合化疗获批，将中位生存期提升至 15-18 个月，但这一突破并未改变小细胞肺癌的 “难治” 本质：超过 80% 的患者会在治疗后 1 年内复发，复发后缺乏有效治疗手段，二线治疗的客观缓解率仅为 20%-30%，中位生存期不足 6 个月。此外，小细胞肺癌患者的生活质量普遍低下，化疗带来的恶心、呕吐、脱发等不良反应严重影响患者日常活动，而肿瘤的快速进展会导致呼吸困难、胸痛、体重下降等症状，许多患者在确诊后半年内就会失去自理能力。因此，小细胞肺癌被称为 “被遗忘的肿瘤”，亟需创新治疗手段。 DLL3 靶点：小细胞肺癌的精准治疗突破口 DLL3（Delta-like ligand 3）是 Notch 信号通路的配体，在胚胎发育过程中发挥重要作用，但在正常成人组织中几乎不表达。然而，超过 80% 的小细胞肺癌患者的肿瘤细胞表面高表达 DLL3，这为精准治疗提供了理想的靶点 —— 靶向 DLL3 的药物可以特异性杀伤肿瘤细胞，而不损伤正常组织。 DLL3 在小细胞肺癌中的作用机制早已被揭示：它通过激活 Notch 信号通路，促进肿瘤细胞的增殖、侵袭和转移，同时抑制肿瘤细胞的分化。因此，抑制 DLL3 的功能可以阻断肿瘤细胞的生长，甚至诱导其凋亡。与其他靶点不同，DLL3 在小细胞肺癌中的表达高度特异，这意味着靶向 DLL3 的药物脱靶毒性低，安全性更好。近年来，DLL3 成为小细胞肺癌研发的热点，全球已有十余款 DLL3 靶向药物进入临床阶段，包括双特异性抗体、抗体偶联药物（ADC）、CAR-T 细胞治疗等。其中，双特异性抗体是最有潜力的方向之一，通过同时结合 DLL3 和 T 细胞表面的 CD3 受体，直接激活 T 细胞产生肿瘤裂解作用，无需依赖 MHC 分子，能更有效地杀伤肿瘤细胞。 obrixtamig：从靶点发现到 III 期临床的突破 obrixtamig 是勃林格殷格翰开发的DLL3/CD3 双特异性 T 细胞衔接器（TCE），其研发历程始于 2018 年。当时，勃林格殷格翰的科研团队通过分析大量小细胞肺癌患者的肿瘤样本，发现 DLL3 在超过 80% 的患者中高表达，且与患者的不良预后相关。基于这一发现，团队决定开发靶向 DLL3 的双特异性抗体。在临床前研究中，obrixtamig 展现出强大的抗肿瘤活性：在小细胞肺癌小鼠模型中，单药治疗可使肿瘤体积缩小 90% 以上，中位生存期延长 2 倍；联合化疗时，肿瘤完全缓解率达 60%，且无明显毒性。这些结果让勃林格殷格翰迅速推进 obrixtamig 进入临床阶段。 2022 年，obrixtamig 的 I 期临床试验启动，针对复发 / 难治性小细胞肺癌患者。初步数据显示，obrixtamig 的客观缓解率达 40%，其中 2 例患者实现完全缓解，且安全性良好，3 级以上不良反应率仅为 25%。这一结果超出了行业预期，因为当时同类 DLL3 双抗的客观缓解率仅为 20%-30%。 2024 年，obrixtamig 的 II 期临床试验结果在 ASCO 年会上公布，进一步验证了其疗效和安全性：针对复发 / 难治性小细胞肺癌患者，obrixtamig 联合化疗的未确认客观缓解率（ORR）达 70%，其中 1 例患者实现完全缓解，15 例患者达部分缓解；疾病控制率（DCR）达 87%。在随访超过 13 周的患者中，确认 ORR 达 69%，中位缓解持续时间尚未达到，而传统化疗的中位缓解持续时间仅为 3-4 个月。安全性方面，在剂量爬坡阶段，未达到最大耐受剂量（MTD）。无患者因治疗相关AE而停用Obrixtamig。细胞因子释放综合征（CRS）发生率为48%，所有病例均为低级别（1-2级）；治疗相关神经毒性（包括ICANS）发生率为8%，均为肌痉挛（1级）。全球 III 期试验：挑战现有治疗标准近日启动的 DAREON-Lung-1 试验是一项随机、开放标签、多中心的 III 期研究，计划在全球入组 670 例广泛期小细胞肺癌（ES-SCLC）患者，随机分为两组：一组接受 obrixtamig 联合 atezolizumab（PD-L1 抑制剂）、卡铂和依托泊苷的三联疗法，另一组仅接受标准的免疫联合化疗方案。试验的主要终点是总生存期（OS）和无进展生存期（PFS），次要终点包括客观缓解率（ORR）、缓解持续时间（DoR）、疾病控制率（DCR）和安全性。预计 2028 年 9 月公布初步结果，若试验成功，obrixtamig 有望成为小细胞肺癌一线治疗的新标准。与现有标准治疗相比，obrixtamig 三联疗法具有三大优势：精准靶向：obrixtamig 特异性结合 DLL3 阳性的肿瘤细胞，直接激活 T 细胞产生肿瘤裂解作用，弥补了免疫检查点抑制剂对免疫抑制肿瘤的无效性；协同效应：obrixtamig 与免疫检查点抑制剂、化疗联合使用时，可产生协同抗肿瘤作用，进一步增强疗效；安全性可控：obrixtamig 的神经毒性发生率低，与现有治疗联合使用时不会显著增加不良反应。勃林格殷格翰全球研发负责人表示：“obrixtamig 的临床数据显示出显著的抗肿瘤活性，我们相信三联疗法能为 SCLC 患者带来新的希望。此次 III 期试验是小细胞肺癌治疗的重要里程碑，我们将全力以赴推进试验，尽快为患者带来新疗法。”五、全球小细胞肺癌管线：obrixtamig 的差异化优势在 obrixtamig 之前，全球已有多款 DLL3 靶向药物进入临床阶段，其中最著名的是安进的塔拉妥单抗（Tarlatamab），这是全球首个获批的 DLL3/CD3 双抗，2024 年获 FDA 加速批准用于复发 / 难治性小细胞肺癌，客观缓解率达 34%，中位总生存期达 13.6个月。国内药企恒瑞医药的SHR‑7787目前在中国处于 II 期临床阶段，用于评估中/后线实体瘤（包括 SCLC）患者的安全性和疗效。信达生物的IBI115刚完成临床申报并计划进入 I 期试验。除了双特异性抗体，DLL3 靶点的 ADC 药物也在快速发展，如阿斯利康的 MEDI7243、默沙东的 MK-6072 等。这些 ADC 药物通过将细胞毒载荷与抗 DLL3 抗体结合，特异性杀伤肿瘤细胞，客观缓解率达 30%-40%，但与 obrixtamig 联合化疗的 70% 客观缓解率相比，仍有差距。此外，小细胞肺癌治疗的其他方向也在推进，如免疫检查点抑制剂联合 PARP 抑制剂、溶瘤病毒疗法、CAR-T 细胞治疗等，但这些疗法大多处于早期临床阶段，疗效尚未得到验证。因此，obrixtamig 是目前最有可能改变小细胞肺癌治疗格局的药物。对勃林格殷格翰而言，obrixtamig 的成功将进一步巩固其在肿瘤领域的地位。勃林格殷格翰近年来持续加大肿瘤研发投入，已拥有包括 obrixtamig、抗 CTLA-4 单抗、ADC 药物等在内的丰富管线。obrixtamig 的获批将为勃林格殷格翰带来新的业绩增长点，同时提升其在全球肿瘤市场的竞争力。结语当我结束这篇分析时，心中涌动着暖流——因为我知道，对于成千上万正在与小细胞肺癌抗争的患者和家属来说，Obrixtamig进入III期临床试验不仅仅是一条行业新闻，更是一束实实在在的希望之光。从科学原理的突破，到临床数据的验证，再到全球III期研究的启动，我们见证了一场精心设计的“攻防战”。展望未来，随着创新疗法的不断涌现，小细胞肺癌这一长期笼罩在“治疗荒漠”中的疾病，终将迎来自己的“绿洲时代”。 END 官方建群啦！生物药大时代组建了抗体药、疫苗、核酸药物等多个相关领域的实名制微信交流群，扫描下方二维码即可入群！

免疫疗法细胞疗法抗体药物偶联物临床3期临床2期

100 项与阿替利珠单抗相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D10773	阿替利珠单抗	L01XC32	DB11595

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
结外NK-T细胞淋巴瘤	日本	Chugai Pharmaceutical Co., Ltd.	2025-09-19
晚期非小细胞肺癌	欧盟	Roche Registration GmbH	2024-07-25
晚期非小细胞肺癌	冰岛	Roche Registration GmbH	2024-07-25
晚期非小细胞肺癌	列支敦士登	Roche Registration GmbH	2024-07-25
晚期非小细胞肺癌	挪威	Roche Registration GmbH	2024-07-25
乳腺癌	加拿大	F. Hoffmann-La Roche Ltd.	2024-03-13
肺泡软组织肉瘤	美国	Genentech, Inc.	2022-12-09
PD-L1阳性非小细胞肺癌	日本	Chugai Pharmaceutical Co., Ltd.	2022-05-26
BRAF V600 突变阳性黑色素瘤	美国	Genentech, Inc.	2020-07-30
PD-L1阳性三阴性乳腺癌	日本	Chugai Pharmaceutical Co., Ltd.	2018-01-19
晚期肝细胞癌	欧盟	Roche Registration GmbH	2017-09-20
晚期肝细胞癌	冰岛	Roche Registration GmbH	2017-09-20
晚期肝细胞癌	列支敦士登	Roche Registration GmbH	2017-09-20
晚期肝细胞癌	挪威	Roche Registration GmbH	2017-09-20
晚期三阴性乳腺癌	欧盟	Roche Registration GmbH	2017-09-20
晚期三阴性乳腺癌	冰岛	Roche Registration GmbH	2017-09-20
晚期三阴性乳腺癌	列支敦士登	Roche Registration GmbH	2017-09-20
晚期三阴性乳腺癌	挪威	Roche Registration GmbH	2017-09-20
广泛期小细胞肺癌	欧盟	Roche Registration GmbH	2017-09-20
广泛期小细胞肺癌	冰岛	Roche Registration GmbH	2017-09-20

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	日本	Chugai Pharmaceutical Co., Ltd.	2026-01-28
膀胱癌	申请上市	中国	Roche Holding AG	2019-02-25
淋巴组织增生性疾病	临床3期	英国	Hoffmann-La Roche Ltd.	2023-10-25
黑色素瘤	临床3期	英国	Hoffmann-La Roche Ltd.	2023-10-25
MSI-H 癌症	临床3期	英国	Hoffmann-La Roche Ltd.	2023-10-25
Turcot综合征	临床3期	英国	Hoffmann-La Roche Ltd.	2023-10-25
转移性胰腺导管腺癌	临床3期	匈牙利	NovoCure GmbH	2023-03-30
转移性胰腺腺癌	临床3期	匈牙利	NovoCure GmbH	2023-03-30
肝转移	临床3期	比利时	-	2021-03-29
原发性恶性肝肿瘤	临床3期	比利时	-	2021-03-29

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临床结果

适应症

分期

评价

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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


IMbrave150 (AACR2026)	N/A	晚期肝细胞癌一线	3,948	Atezolizumab + Bevacizumab	簾積選餘艱觸鏇廠糧夢(鬱淵製憲選夢觸築憲鹽) = The risk of developing predefined adverse events was similar between regimens with nonsignificant RD 積淵鑰選窪獵範選襯壓 (蓋窪繭鑰餘鹽膚壓積鑰 ) 更多	积极	2026-04-21
				Nivolumab + Ipilimumab
GOBLET (AACR2026)	临床1/2期	胰腺癌一线 RAS upregulated	13	Pelareorep + Atezolizumab + Gemcitabine/nab-paclitaxel	壓衊鏇醖鏇鏇積簾鹹艱(鑰鬱廠襯鹹選淵願鑰艱) = 構餘簾淵壓襯壓壓壓繭構艱廠襯鑰簾遞淵選製 (糧鹽繭願醖襯鏇願蓋糧 ) 更多	积极	2026-04-21
AACR2026	N/A	转移性非小细胞肺癌一线	11,758	Atezolizumab	衊齋艱憲淵艱選積壓繭(齋艱鏇壓簾鏇夢窪顧範) = 簾夢襯壓製蓋願廠製鏇構範築築積範窪衊築壓 (獵襯積醖鑰鏇齋網顧醖 ) 更多	不佳	2026-04-21
				Pembrolizumab	衊齋艱憲淵艱選積壓繭(齋艱鏇壓簾鏇夢窪顧範) = 鑰鏇壓鬱構齋顧遞淵鹽構範築築積範窪衊築壓 (獵襯積醖鑰鏇齋網顧醖 ) 更多
AACR2026	临床2期	PD-L1阳性肺癌 PD-L1 positive	41	SBRT + Atezolizumab + Tiragolumab	蓋窪範廠鏇積蓋齋鏇餘(網簾壓積衊繭醖製鹹蓋) = 築壓鑰鹹蓋鏇壓糧構鏇鹹艱鏇遞積鹹觸簾淵醖 (觸積壓憲築艱衊製顧鹹, 6.0 ~ NR) 更多	积极	2026-04-20
				SBRT + Atezolizumab + Tiragolumab (PD-L1 high (> 50%))	蓋窪範廠鏇積蓋齋鏇餘(網簾壓積衊繭醖製鹹蓋) = 鬱築鬱觸簾齋築餘齋醖鹹艱鏇遞積鹹觸簾淵醖 (觸積壓憲築艱衊製顧鹹 )
IMforte (AACR2026)	临床3期	广泛期小细胞肺癌维持	452	Lurbinectedin plus atezolizumab	遞醖襯壓淵積夢觸顧鹽(醖築衊窪糧窪鑰構鬱糧) = 遞願淵築憲顧網繭網網遞鏇襯鹹蓋壓憲網鏇願 (襯網獵壓繭齋憲範鹽壓 ) 更多	积极	2026-04-20
				Durvalumab	遞醖襯壓淵積夢觸顧鹽(醖築衊窪糧窪鑰構鬱糧) = 艱鑰壓築蓋襯網選鹽膚遞鏇襯鹹蓋壓憲網鏇願 (襯網獵壓繭齋憲範鹽壓 ) 更多
NCT04902040 (CTgov)	临床1/2期	皮肤黑色素瘤 \| 晚期恶性实体瘤 \| 晚期肾细胞癌 ... 更多	19	Plinabulin+Pembrolizumab+RTX (Phase 1b: RTX + Plinabulin (30 mg/m2, Q3W) + Pembrolizumab (200 mg, Q3W))	範鬱製壓觸醖壓夢蓋積 = 鹹壓繭糧築鑰糧鑰夢襯壓繭窪範廠構蓋蓋遞膚 (範窪遞膚鏇鑰衊衊糧廠, 繭鬱觸夢醖顧願願鏇憲 ~ 餘壓壓鹹鬱簾壓範夢鏇) 更多	-	2026-03-18
				Nivolumab+Plinabulin+RTX (Phase 1b: RTX + Plinabulin (30 mg/m2, Q4W) + Nivolumab (240 mg, Q2W))	範鬱製壓觸醖壓夢蓋積 = 窪獵襯鏇願襯鑰願觸積壓繭窪範廠構蓋蓋遞膚 (範窪遞膚鏇鑰衊衊糧廠, 築膚蓋齋願獵糧鹹艱襯 ~ 選糧糧衊壓醖獵鹹醖鹹) 更多
NCT04832854 (SKYSCRAPER05 \| SKYSCRAPER-05, CTgov)	临床2期	非小细胞肺癌 \| 局部晚期非小细胞肺癌	50	platinum+atezolizumab+tiragolumab (Cohort A: PD-L1 High)	窪築構鏇構齋鹽窪襯積 = 積窪膚積齋壓鏇廠膚鬱齋鑰鏇糧願鹹齋獵憲選 (蓋餘繭壓觸艱齋築獵壓, 壓襯蓋鹹廠鏇蓋網膚膚 ~ 憲齋繭範選鬱憲襯艱衊) 更多	-	2026-03-11
				platinum+atezolizumab+tiragolumab (Cohort B: PD-L1 All Comers)	窪築構鏇構齋鹽窪襯積 = 觸繭選遞願鹹觸範網願齋鑰鏇糧願鹹齋獵憲選 (蓋餘繭壓觸艱齋築獵壓, 積積艱鹹構鹽遞獵膚選 ~ 鹹襯襯簾網繭構顧窪鏇) 更多
NCT03811002 (NRG Oncology/Alliance LU005, Pubmed \| J Clin Oncol)	临床3期	局限期小细胞肺癌	398	Concurrent chemoradiation + concurrent and adjuvant atezolizumab	淵齋憲鑰築選膚願鏇壓(壓鹽顧製簾蓋醖簾壓襯) = 鏇膚襯壓廠鬱遞簾醖壓衊鏇顧壓窪膚鏇鑰餘膚 (窪憲鹹壓膚鹽膚範獵願, 28.5 ~ 44.7) 更多	不佳	2026-03-10
				Concurrent chemoradiation alone	淵齋憲鑰築選膚願鏇壓(壓鹽顧製簾蓋醖簾壓襯) = 糧廠遞壓鑰觸鹽範壓艱衊鏇顧壓窪膚鏇鑰餘膚 (窪憲鹹壓膚鹽膚範獵願, 28.1 ~ 42.5) 更多
NCT04624399 (ABACUS-2, ASCO_GU2026)	临床2期	肾盂和输尿管尿路上皮癌新辅助 ctDNA \| utDNA	27	Atezolizumab	願構築醖繭壓鹽築鬱繭(製獵鏇淵積糧選膚觸壓) = 網糧蓋顧齋繭簾鑰齋積衊範選淵鑰範憲鹹簾夢 (糧齋壓遞鏇觸願積範選 ) 更多	积极	2026-02-26
NCT04660344 (IMvigor011, ASCO_GU2026)	临床3期	肌层浸润性膀胱癌辅助	379	atezolizumab (pts who cleared ctDNA at C3 or C5)	鏇鬱夢鏇餘壓淵遞醖餘(憲淵繭簾鏇願願廠鬱醖) = 鹹鬱醖鑰艱鹽遞淵願糧蓋壓製構範網簾糧衊鬱 (網襯繭醖築衊憲選鹽鏇 ) 更多	积极	2026-02-26
				placebo (pts who cleared ctDNA at C3 or C5)	鏇鬱夢鏇餘壓淵遞醖餘(憲淵繭簾鏇願願廠鬱醖) = 構齋繭鹽獵觸夢壓構願蓋壓製構範網簾糧衊鬱 (網襯繭醖築衊憲選鹽鏇 ) 更多