预约演示

更新于：2026-05-28

Atezolizumab

阿替利珠单抗

更新于：2026-05-28

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+ [147]

非在研适应症

大肠腺癌晚期胆管癌晚期胆道癌+ [104]

原研机构

Genentech, Inc.

Universitair Medisch Centrum Groningen

在研机构

Hoffmann-La Roche, Inc.

罗氏（中国）投资有限公司

Roche Diagnostics GmbH

+ [22]

非在研机构

Sanofi

Kymab Ltd.

Pfizer Inc.

+ [11]

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

888

项与阿替利珠单抗相关的临床试验

NCT07170592

/ Not yet recruiting临床1期

A Phase 1 Study of OTS-412 (Recombinant Oncolytic Vaccinia Virus) in Combination With Hydroxyurea or Hydroxyurea/Atezolizumab in Treatment-refractory Solid Tumor Patients

This clinical trial aims to determine whether the administration of the investigational drug OTS-412, OTS-412 in combination with hydroxyurea or hydroxyurea/atezolizumab is safe and effective for patients with various types of cancer.

开始日期2027-01-01

申办/合作机构

Bionoxx, Inc.

NCT07545954

/ Not yet recruiting临床1期IIT

A Pilot Study of DSP-0390 in Combination With Atezolizumab as Maintenance Therapy for Extensive Stage Small Cell Lung Cancer

This is a single center pilot, phase Ib study with a safety lead-in evaluating the safety and preliminary efficacy of the EBP inhibitor DSP-0390 in combination with atezolizumab in patients with extensive stage small cell lung cancer (ES-SCLC) whose disease has not progressed after initial induction therapy with platinum-based chemotherapy and anti-PD-L1 immunotherapy (atezolizumab or durvalumab per treating physician's discretion). This trial is testing the hypothesis that inhibition of de novo cholesterol synthesis by DSP-0390 when used in combination with atezolizumab in the maintenance therapy of patients with ES-SCLC will be tolerable.

开始日期2026-07-31

申办/合作机构

Washington University School of Medicine

[+1]

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2026-06-05

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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4,411

项与阿替利珠单抗相关的文献（医药）

2026-12-31·JOURNAL OF MEDICAL ECONOMICS

Cost-effectiveness analysis of atezolizumab and bevacizumab as first-line systemic therapy in unresectable hepatocellular carcinoma in Malaysia

Article

作者: Chaiyakunapruk, Nathorn ; Patikorn, Chanthawat ; Sulaiman Shah, Audi Adawiah ; Wong, Yoke Fui ; Mohamed, Rosmawati

AIM:

This study aims to evaluate the cost-effectiveness of atezolizumab plus bevacizumab as first-line systemic therapy for unresectable hepatocellular carcinoma (uHCC) in Malaysia, compared with the current standard treatments in the Malaysian Ministry of Health (MOH) to inform public healthcare decision‑making.

MATERIALS AND METHODS:

A cost-effectiveness analysis was conducted from the MOH perspective, following the national pharmacoeconomic guidelines (2019). The study compared atezolizumab plus bevacizumab with sorafenib and lenvatinib, respectively, using a partitioned survival model to project health outcomes and costs over a lifetime horizon. Clinical efficacy data were sourced from published trials and network meta-analyses. Cost inputs reflected local healthcare resource use and prices, using 2024 Malaysian Ringgit values inflated via the Consumer Price Index for Health. Costs and outcomes were discounted at 3% annually. Deterministic and probabilistic sensitivity analyses were performed to assess the impact of key parameter uncertainties on the results.

RESULTS:

Atezolizumab plus bevacizumab provided the highest quality-adjusted life years (QALYs) and life years compared to sorafenib and lenvatinib. Sorafenib was dominated by lenvatinib due to lower QALYs and higher costs and excluded from further analysis. Compared to lenvatinib, atezolizumab plus bevacizumab yielded 0.873 additional QALYs and RM 44,863 additional cost, resulting in an incremental cost-effectiveness ratio (ICER) of RM 51,399 per QALY gained (∼0.906 GDP/capita at Malaysia's 2024 GDP/capita RM 56,734).

CONCLUSIONS:

Atezolizumab plus bevacizumab is cost-effective compared to lenvatinib and sorafenib across willingness-to-pay (WTP) values of one to three times Malaysia's GDP per capita. These findings provide evidence to inform public health policy that expanding funding and adoption of atezolizumab plus bevacizumab is likely to improve health outcomes cost-effectively.

2026-09-01·COMPARATIVE BIOCHEMISTRY AND PHYSIOLOGY C-TOXICOLOGY & PHARMACOLOGY

Toxic effects of acute atrazine exposure on the physiological functions and transcriptional levels in non-targeted marine invertebrates (Chlamys nobilis)

Article

作者: Sun, Jing ; Zheng, Huaiping ; Liu, Yaoting ; Yan, Beiyu ; Lin, Qing ; Wang, Weili ; Zhang, Hongkuan

Atrazine (ATZ), the second most widely used pesticide globally, poses potential risks to non-target aquatic organisms. However, its toxicological impacts on the economically valuable Chlamys nobilis remain unknown. This study investigates the toxicological effects of ATZ on the economically important C. nobilis. We assessed tissue integrity, physiological functions, and transcriptional profiles following ATZ exposure. Mortality in C. nobilis was observed to be time- and dose-dependent. Gill tissue damage was first noted at 5 μg/L ATZ, with severity increasing at higher concentrations. Superoxide dismutase (SOD) and catalase (CAT) activities were significantly elevated at 5 μg/L and 50 μg/L compared to controls but declined at 500 μg/L (P < 0.05). Glutathione S-transferase (GST) activity increased in all exposed groups except at 500 μg/L, peaking at 5 μg/L (P < 0.05). Malondialdehyde (MDA) levels rose significantly at 0.5 μg/L and further increased with higher ATZ concentrations (P < 0.05). RNA-seq analysis revealed 167 and 282 differentially expressed genes (DEGs) at 0.5 μg/L and 50 μg/L, respectively, enriched in pathways related to the endocrine, sensory, and digestive systems. Our findings highlight the toxic effects of ATZ on C. nobilis and contribute to the environmental risk assessment of this pesticide.

2026-08-01·WATER RESEARCH

Breaking the activity-stability trade-off of zero-valent iron for robust peracetic acid activation: The synergistic role of S/N Co-doping

Article

作者: He, Chuan-Shu ; Yang, Qing ; Xiong, Zhao-Kun ; Zhang, Yu ; Xing, Dan-Ying ; Lai, Bo

The practical application of pristine zero-valent iron (ZVI) is often hindered by sluggish interfacial electron transfer and rapid passivation. Herein, we simultaneously enhanced catalytic activity and anti-aging performance via a "Promotion and Protection" material design strategy, synthesizing a robust sulfur/nitrogen co-doped ZVI (S/N-ZVI) catalyst via one-step mechanochemistry. The S/N-ZVI/peracetic acid (PAA) system showed markedly enhanced kinetics for atrazine degradation, with a pseudo-first-order rate constant (k_obs) 66.4 times that of pristine ZVI. Remarkably, the catalyst retained over 89 % of its efficiency after 10 months of natural aging, demonstrating exceptional robustness. Density functional theory (DFT) calculations reveal that the "Promotion" effect stems from an electronic structure modulation: S/N doping induces a distinct upshift of the Fe d-band center and a significant reduction in work function, thereby substantially enhancing the intrinsic outward electron flux. Simultaneously, the "Protection" mechanism is enabled by a quasi-hydrophobic shell that repels environmental moisture and oxygen. Furthermore, S/N doping modulates the evolution of corrosion products, ensuring the formation of a permeable oxide layer that maintains long-term electron transport channels. Electron Paramagnetic Resonance (EPR) and quenching experiments reveal that despite the generation of multiple reactive species, hydroxyl radicals (•OH) are the dominated species driving ATZ degradation. Bench-scale reactor tests and toxicity predictions further validate the system's scalability and ecological safety. This work provides a distinct strategy for designing metastable iron-based materials with sustained reactivity.

3,478

项与阿替利珠单抗相关的新闻（医药）

9 小时之前

·PRNewswire

Florida Cancer Specialists & Research Institute Advances the Future of Cancer Care

32 Abstracts and Presentations Showcase Cutting-Edge Research at the 2026 ASCO® Annual Meeting 2026 ASCO® Annual Meeting abstracts featuring FCS research: 1073, 1094, 1530, 2629, 3013, 3078, 3088, 3146, 4213, 5511, 5565, 5580, 6062, 7023, 7029, 7532, 7565, 9564, e13044, e16400, TPS11202, TPS2668, TPS2680, TPS3155, TPS3160, TPS3167, TPS3179, TPS5139, TPS5628, TPS5647, TPS8134, TPS8136 FORT MYERS, Fla., May 28, 2026 /PRNewswire/ -- Findings from 32 abstracts and presentations conducted at Florida Cancer Specialists & Research Institute, LLC (FCS) are among the groundbreaking scientific advances in cancer care that will be featured as oncology professionals from around the world gather this week at the 2026 American Society of Clinical Oncology (ASCO®) Annual Meeting in Chicago. Continue Reading Florida Cancer Specialists & Research Institute (FCS) will present findings from 32 abstracts and presentations at the 2026 ASCO® Annual Meeting, showcasing innovative clinical trials, targeted therapies and precision oncology research led by FCS physicians and researchers across Florida. Thirteen physicians and leaders from the statewide practice will present the outcomes of early and late-phase clinical trials performed at FCS Phase 1 Drug Development Units and clinics throughout Florida. Research conducted at FCS is made possible through valuable relationships with Sarah Cannon Research Institute (SCRI), one of the world's leading oncology research organizations conducting community-based clinical trials, Paradigm Health, an AI-enabled clinical trial matching and recruitment platform, and other independent clinical trial programs. FCS Assistant Managing Physician, David Wenk, MD, said, "Our extensive research program is a defining strength of FCS and a vital part of our mission to provide patients with convenient access to world-class cancer care close to home." "The research being presented highlights both innovative treatment strategies and cutting-edge targeted therapies," said FCS Director of Drug Development Manish R. Patel, MD. "Through our ongoing clinical research efforts, we are generating new scientific insights that are advancing precision oncology for patients with a wide range of cancers, including rare and advanced disease." The following FCS principal investigators are first authors on ten abstracts that will be presented throughout the meeting: Lucio Gordan, MD, FCS president & managing physician, Ashley Hernandez, Amanda Warner and Christian Okitondo Patient characteristics, treatment patterns, social determinants of health, and safety in patients prescribed nivolumab and hyaluronidase-nvhy by early adopters. Lowell Hart, MD (Retired) (RW) post-progression outcomes after first-line (1L) treatment with ribociclib + an aromatase inhibitor (AI) vs AI alone in US patients with hormone receptor-positive/human epidermal growth factor receptor 2-negative (HR+/HER2–) metastatic breast cancer (MBC). Maen Hussein, MD, FCS director of value-based care and Kristin Boykin, FCS senior director, pharmacy operations Evaluating the impact of a statewide intervention on multiple myeloma bispecific T-cell engaging antibody (BsAb) therapy uptake in Florida (FL). Management of chemotherapy-induced adverse events in patients with metastatic pancreatic ductal adenocarcinoma: A US-based modified Delphi consensus. Bradley Monk, MD, FACOG, FACS A pragmatic, hybrid observational study evaluating the effectiveness of trastuzumab deruxtecan (T-DXd) in patients with human epidermal growth factor receptor 2 (HER2) immunohistochemistry (IHC) 3+ solid tumors: DESTINY-PanTumor04. Efficacy prediction for progression-free survival (PFS) and overall survival (OS) by genomic instability score (GIS) cutoffs in patients (pts) with advanced ovarian cancer (aOC): Post hoc results from the phase 3 PRIMA/ENGOT-OV26/GOG-3012 trial. Manish R. Patel, MD A phase 1/2, first-in-human study of AVZO-021, a selective cyclin-dependent kinase 2 inhibitor (CDK2i), as monotherapy and in combination for patients with advanced solid tumors, including hormone receptor–positive (HR+)/human epidermal growth factor receptor 2–negative (HER2−) breast cancer (BC) and cyclin E1 (CCNE1)–amplified solid tumors: Updated safety and efficacy results. A phase 1, first-in-human study of DS9051, a novel targeted protein degradation molecule, in patients with advanced/metastatic adrenocortical carcinoma (ACC) or metastatic castration-resistant prostate cancer (mCRPC). Judy Wang, MD, FCS associate director of drug development, Sarasota Drug Development Unit A first-in-human study of ATX-295, an oral inhibitor of KIF18A, in patients with advanced or metastatic solid tumors, including ovarian cancer. Judy Wang, MD and Cesar Augusto Perez, MD, FCS director of drug development, SCRI at Lake Nona Drug Development Unit Phase 1 dose escalation of CTX-8371, a novel PD-1×PD-L1 bispecific antibody, in patients with advanced malignancies post checkpoint inhibition. The following FCS principal investigators have co-authored 22 additional abstracts and publications of research results and other clinical findings featured throughout the annual meeting: Lucio N. Gordan, MD Real-world patient characteristics, outcomes, and resource utilization of chimeric antigen receptor (CAR) T cell therapy across Foundation for the Accreditation of Cellular Therapy (FACT) and non-FACT treatment centers in large B-cell lymphoma (LBCL).* Lowell Hart, MD (Retired) (RW) post-progression outcomes following first-line (1L) ribociclib (RIB) + aromatase inhibitor (AI) versus AI alone in African American and low socio-economic status (SES) patients with hormone receptor-positive/human epidermal growth factor receptor 2-negative (HR+/HER2–) metastatic breast cancer (MBC) in US. Maen Hussein, MD, FCS medical director, value-based care TIGOS-LS, an open-label, randomized study of BMS-986489 (atigotatug + nivolumab fixed-dose combination) vs durvalumab as consolidation therapy following chemoradiotherapy in limited-stage small-cell lung cancer. Bradley Monk, MD TroFuse-036/GOG-3123/ENGOT-cx22: A 2-part, phase 3, randomized study of sacituzumab tirumotecan (sac-TMT) + pembrolizumab (pembro) ± bevacizumab (bev) vs standard of care (SoC) as first-line maintenance therapy for PD-L1–positive cervical cancer. Overall survival for patients with pre-treated platinum-resistant ovarian cancer receiving gotistobart in combination with pembrolizumab. Puxitatug samrotecan (AZD8205) vs chemotherapy in patients with B7‑H4–selected advanced/metastatic endometrial cancer: The phase 3 randomized Bluestar‑Endometrial01 (BE01)/GOG-3110/ENGOT-EN28 trial. Manish R. Patel, MD A phase 1, first-in-human study of OP-3136, a novel oral selective KAT6A/B inhibitor, as monotherapy in advanced solid tumors and in combination with endocrine therapy in ER+, HER2− advanced breast cancer (ABC): Preliminary results. A randomized, open-label, phase 3 study of ZL-1310, a DLL3 antibody-drug conjugate (ADC), compared to investigator's choice therapy in participants with relapsed small cell lung cancer (DLLEVATE). BNT326-01: A Phase 1b/2 trial of BNT326/YL202 (HER3 ADC) as monotherapy and in combination with pumitamig (anti-PD-L1 × VEGF bsAb) in patients with advanced solid tumors. Farnesyl transferase inhibitor (FTI) darlifarnib (KO-2806) in combination with adagrasib in KRAS G12C mutated (mut) advanced solid tumors: Preliminary results from the FIT-001 phase 1 first-in-human trial. A phase 3 randomized, open-label study of pasritamig (JNJ-78278343), a T-cell engager targeting human kallikrein-2, with docetaxel versus docetaxel for metastatic castration-resistant prostate cancer. Intismeran autogene to induce de novo neoantigen-specific T cells as adjuvant therapy in melanoma. Shachar Peles, MD, FCS director of cell therapy Fixed-duration subcutaneous (SC) mosunetuzumab (Mosun) in elderly/unfit patients with previously untreated diffuse large B-cell lymphoma (DLBCL): Interim analysis and patient-reported outcomes (PROs) from the phase 2 MorningSun study Ivor Percent, MD Post-hoc efficacy and biomarker analysis of elraglusib plus gemcitabine/nab-paclitaxel versus chemotherapy alone in metastatic pancreatic ductal adenocarcinoma. Cesar Augusto Perez, MD First-in-human study of BG-C9074 (B7-H4–targeting ADC) in advanced solid tumors: Dose escalation and safety expansion. BMS-986504 in patients (pts) with advanced solid tumors with homozygous MTAP deletion (MTAP-del): Exploratory pharmacodynamic (PD) and biomarker analyses from CA240-0007. A phase 1/2, first-in-human, open-label, dose-escalation and -expansion study of TAK-188, a novel antibody-drug conjugate (ADC) targeting CCR8+ regulatory T cells, in adult patients with locally advanced or metastatic solid tumors. A phase 1/2 study of the next-generation nectin-4–targeting antibody-drug conjugate CRB-701 (SYS6002) in patients with recurrent or metastatic head and neck squamous cell carcinoma. Phase I, multicenter, first-in-human (FIH) global study of SIM0505, an anti-CDH6 (CDH6) antibody-drug conjugate (ADC) in patients with advanced solid tumors. First-in-human phase 1a/1b study of LB-LR1109, an anti-LILRB1 monoclonal antibody, as monotherapy in advanced solid tumors and in combination with atezolizumab in advanced NSCLC. Judy Wang, MD A phase 1, first-in-human study of DS5361, a small-molecule, nonsense-mediated mRNA decay (NMD) inhibitor in patients with advanced/metastatic solid tumors (parts 1 and 2). Syed Zafar, MD Durable clinical benefit with B-cell maturation antigen (BCMA)–directed therapy, belantamab mafodotin plus pomalidomide and dexamethasone (BPd) in relapsed/refractory multiple myeloma (RRMM): DREAMM‑8 long‑term responder (LTR) analysis. FCS Chief Executive Officer Ryan Ciarrocchi said, "The ASCO® Annual Meeting highlights the most significant cancer research from around the world, and FCS is proud to once again be recognized among the leaders helping to shape the future of cancer care." All abstracts and presentations are available to view at ASCO® 2026 Annual Meeting. The American Society of Clinical Oncology (ASCO®) represents nearly 50,000 physicians and oncology professionals representing 150 countries who care for people living with all forms of cancer. ASCO® works to conquer cancer through research, education, policy and promotion of high quality and equitable patient care. About Florida Cancer Specialists & Research Institute, LLC: ( FLCancer.com ) For more than 40 years, Florida Cancer Specialists & Research Institute (FCS) has embraced innovation to deliver world-class care and drive the dramatic transformation of oncology care through its robust clinical research program. FCS provides patients with access to a wide range of clinical trials, positioning it as a leader in research among private oncology practices in Florida and across the country. Through its robust clinical research program with Sarah Cannon Research Institute (SCRI) and a suite of independent site management programs, with advanced clinical trial matching technology, FCS offers patients innovative therapies close to home. Each year, FCS conducts more than 180 active clinical trials that directly elevate patient care and accelerate progress in oncology. Many of the cancer drugs approved by the FDA in the U.S over the past decade were accessible to patients at FCS through clinical trial participation before receiving approval. Our outstanding team of highly trained and dedicated physicians is committed to delivering tailored treatment plans that make the best use of cutting-edge precision oncology advancements to enhance patient outcomes. SOURCE Florida Cancer Specialists & Research Institute 21% more press release views with Request a Demo

临床1期ASCO会议临床3期临床结果细胞疗法

21 小时之前

·BioSpace

Opinion: The real potential of PD-(L)1×VEGF bispecifics may be outside lung cancer

iStock, selvanegra PD-(L)1×VEGF bispecifics have emerged as a closely watched new class in immuno-oncology, with multiple candidates advancing through trials in lung cancer. But the potential of these drugs may be highest in cancers where angiogenesis and immune escape are tightly intertwined. The next wave of immuno-oncology innovation may not come from entirely new mechanisms but from smarter combinations engineered into a single molecule. A case in point: PD-(L)1×VEGF bispecific antibodies. Once viewed as gradual extensions of existing checkpoint and anti-angiogenic therapies, these assets have rapidly become one of the hottest platforms in biopharma, resulting in significant deal-making. High-value deals such as Akeso’s out-licensing of ivonescimab to Summit Therapeutics (up to $5 billion), Bristol Myers Squibb’s $11.1 billion partnership with BioNTech for pumitamig (BNT327), Pfizer’s multi-billion-dollar deal for SSGJ-707 and Merck’s early bet on LaNova’s LM-229 (MK-2010) collectively signal that this class of bispecifics is being treated as a potential next-generation immuno-oncology platform. As consultants at Lifescience Dynamics who work closely with clients in biopharma, we believe that while the lion’s share of clinical trials on these candidates have so far explored their use in lung cancer, other cancers may be more fruitful indications for this class. These antibodies target both immune checkpoints and angiogenesis—the formation of new blood vessels to provide nutrients and oxygen to cancer cells, enabling their growth and spread. Thus, in cancers where these processes are intertwined, such as hepatocellular carcinoma, PD-(L)1×VEGF bispecifics could be a one-two punch that knocks down these hard-to-treat malignancies. A nuanced success story Lung cancer has emerged as the frontrunner indication for the most advanced PD-(L)1×VEGF bispecifics. Early-stage studies, particularly those reported in China, have yielded high response rates and encouraging progression-free survival data. However, as larger, late-stage trials read out, the picture is proving more nuanced than investment trends alone might suggest. In first-line squamous non-small cell lung cancer (NSCLC), the China-only Phase 3 HARMONi-6 study reported a clear progression-free survival advantage for ivonescimab plus chemotherapy (11.1 months) compared with the anti-PD-1 tislelizumab plus chemotherapy (6.9 months), with improvements seen across PD-L1 subgroups. Safety was broadly comparable between arms, and the relatively low rate of severe bleeding events (1.9%) is notable given the hemorrhage concerns associated with anti-VEGF therapies in this patient population. These findings, alongside the progression-free survival (PFS) benefit seen in the HARMONi-2 study of ivonescimab vs. pembrolizumab (anti-PD-1) in first-line PD-L1-positive NSCLC, suggest a degree of consistency for these agents in delivering PFS gains. Based on the positive data, China’s National Medical Products Administration has accepted the supplemental NDA for the ivonescimab regimen, having already approved the HARMONi-2 regimen. However, global regulators, including the FDA and the European Medicines Agency, typically look for a more robust overall survival benefit before considering approval. For now, the absence of a clear statistically significant overall survival signal from HARMONi-6 introduces an element of caution. A similar pattern has emerged in the global Phase 3 HARMONi trial in previously-treated patients with EGFR-mutant NSCLC where ivonescimab plus chemotherapy delivered a strong PFS improvement versus chemotherapy alone, yet overall survival results have been harder to interpret. That said, in January, Summit announced that the FDA has accepted its Biologics License Application (BLA) for ivonescimab plus chemotherapy, with an action date of November 14. More recently, Summit’s’ disclosure that ivonescimab failed to reach a statistical bar for PFS in the Phase 3 HARMONi-3 trial in first-line NSCLC at an early interim analysis was met with some disappointment from analysts, with the company’s shares trading nearly 26% down at market close on Friday, May 1. Meanwhile, Merck’s PD-1 x VEGF bispecific, MK-2010, generated an unconfirmed ORR of 55% as a first-line treatment for NSCLC, which some analysts appeared to interpret as competitive but undifferentiated from the data already seen with ivonescimab. Taken together, the results to date suggest that while PD-(L)1×VEGF bispecifics may deliver robust PFS gains and deeper responses in lung cancer, a clean globally consistent overall survival win has not yet been demonstrated. In the competitive lung cancer landscape, which is saturated with immuno-oncology, chemotherapy and antibody-drug conjugate (ADC) combinations, incremental PFS benefits without an unambiguous overall survival advantage may not reshape standards of care in the clinic. Normalizing vasculature could be a differentiator So why are many companies and investors still writing multibillion-dollar checks for this asset class? Mechanistically, colocalizing checkpoint blockade and VEGF inhibition in a single molecule has the potential to normalize tumor vasculature, relieve VEGF-driven immunosuppression and potentially use lower systemic VEGF exposure more effectively than separate anti-PD-(L)1 plus bevacizumab (anti-VEGF) combinations. While lung cancers may have been the lead indications for PD(L)-1×VEGF bispecifics initially, several companies are starting to investigate the class in Phase 3 studies in other indications, both within and outside of China. PD(L)-1×VEGF antibodies are now being investigated in Phase 3 studies in first-line colorectal, biliary tract, pancreatic and triple-negative breast cancers in China. Elsewhere, Pfizer and BioNTech/BMS appear to have the most advanced programs for PF-08634404 and pumitamig, respectively, with three currently listed non-lung Phase 3 trials for each. In addition, Pfizer’s PF-08634404 is currently being investigated in a Phase 1/2 study in hepatocellular carcinoma, an angiogenesis-heavy tumor. Notably, as of publication, none of the key assets in this class are in Phase 3 clinical development for hepatocellular carcinoma. The success of atezolizumab (anti-PD-L1) plus bevacizumab (anti-VEGF) as a frontline standard in unresectable hepatocellular carcinoma established a clear mechanistic precedent supporting PD-(L)1×VEGF bispecifics in this indication and offers one of the most derisked paths forward for this asset class outside of lung cancer. For R&D leaders and investors, the implications are straightforward. While lung cancer may still be treated as a validation arena, the performance of PD(L)-1×VEGF bispecific antibodies in this space should not be viewed as the sole value driver. Displacing entrenched regimens of chemotherapy plus immuno-oncology in lung cancers will likely require a decisive global overall survival win in a head-to-head study against standard of care. Indication selection should therefore be more biology-led, prioritizing highly VEGF-dependent tumors where angiogenesis and immune escape are tightly intertwined. Moreover, China-origin data, while invaluable, must be confirmed in multi-regional populations before being assumed to translate into global practice-changing impact. The emerging potential of this asset class may therefore be more nuanced than what the headline deal news flow would suggest. While PD-(L)1×VEGF bispecifics may still potentially secure their first approvals in lung cancer, their highest value could lie in tumors where immune and vascular biology are inseparable and where the bar set by first-generation immuno-oncology combinations is eminently beatable.

临床3期临床结果免疫疗法引进/卖出申请上市

2026-05-27

·蛋白质AI笔记

PD-1抗体药十年：从"神药"叙事到理性认知一份全景数据分析

很早以前就一直关注PD1抗体药，今天加播一篇，大家耐心阅读，定有收货。 2018年，James Allison和Tasuku Honjo因为发现PD-1和CTLA-4这两个免疫检查点拿了诺贝尔生理学或医学奖。那一年，Keytruda全球卖了72亿美元。到了2025年，这个数字变成了约295亿美元——一款药，超过了很多国家的GDP。但今年已经是2026年了。PD-1这个赛道不是新闻了。当我们说"免疫治疗"的时候，谈论的已经不是"有没有用"，而是"在谁身上有用""为什么多数人没用""下一代是什么"。我想用数据，而不是信念，把这些问题理一遍。 PD-1到底是什么——用一句话讲清楚免疫系统里有一类细胞叫T细胞，它们是杀肿瘤的核心力量。但T细胞身上有一个"刹车"——PD-1受体。肿瘤细胞进化出了一个狡猾的策略：在表面大量表达PD-L1蛋白，去踩T细胞的这个刹车。正常细胞也有PD-L1，但量很少。肿瘤细胞把它变成了自己的"隐身衣"——本来T细胞应该攻击癌细胞的，被踩了刹车就不动了。 PD-1抑制剂就是把这个刹车拆掉。它的结构是一个抗体，能精确结合到PD-1或者PD-L1上，堵住两者之间的接触面。刹车拆了，T细胞就可以重新识别和杀死肿瘤。它不是传统意义上"攻击肿瘤的药"——它是"训练免疫系统的药"。这是关键区别，也是所有优势和劣势的根源。中国26款免疫检查点抑制剂：一个拥挤的市场截至2026年初，中国已经获批上市26款免疫检查点抑制剂。 PD-1抑制剂（12个，竞争最激烈的赛道）：国外（2个）：纳武利尤单抗/O药（BMS）、帕博利珠单抗/K药（默沙东）国产（10个）：特瑞普利单抗（君实）、信迪利单抗（信达）、卡瑞利珠单抗（恒瑞）、替雷利珠单抗（百济）、派安普利单抗（正大天晴/康方）、赛帕利单抗（誉衡）、斯鲁利单抗（复宏汉霖）、普特利单抗（乐普）、恩朗苏拜单抗（石药）、菲诺利单抗（神州细胞） PD-L1抑制剂（8个）：度伐利尤单抗/I药（AZ）、阿替利珠单抗/T药（罗氏）、恩沃利单抗（康宁杰瑞）、舒格利单抗（基石）、索卡佐利单抗（李氏）、贝莫苏拜单抗（正大天晴）、阿得贝利单抗（恒瑞）、塔戈利单抗（科伦博泰） CTLA-4抑制剂（2个）：伊匹木单抗（BMS）为核心双特异性抗体（4个）：卡度尼利单抗/PD-1×CTLA-4（康方）、依沃西单抗/PD-1×VEGF（康方）、艾帕洛利托沃瑞利单抗/PD-1×CTLA-4（齐鲁）等 26款药，听起来很多。但其中13款国产PD-1/PD-L1已经挤进了国家医保。价格从最初的几十万一年，降到了医保报销后患者自付几千到一万多一年。一个曾被称为"天价抗癌药"的品类，现在变成了标准的治疗方案。这个转变本身就很值得想——一个市场的供给端从两个药变成二十多个药，到底意味的不是暴利，而是可及性。 PD-1 vs 化疗：数据告诉你差距有多大我们来看数字。以下数据来自2024-2025年发表的系统综述和III期临床试验：非小细胞肺癌（NSCLC），中国患者荟萃分析，11项III期RCT，3712例： PD-1+化疗 vs 单独化疗： - 总生存期HR 0.65（95% CI 0.60-0.72），意味着死亡风险降低35% - 无进展生存期HR 0.49——疾病进展风险降低超过一半 - 客观缓解率提升60% - 5年总生存率：联合方案约20% vs 化疗约7% 食管癌，7项RCT网络荟萃分析，4363例：OS HR 0.69，死亡风险降低31%。对食管鳞癌——中国最高发的食管癌类型——尤其显著。胃癌/胃食管交界癌，6项III期RCT，6294例：信迪利单抗+化疗的OS获益在各药物中排名第一，替雷利珠单抗和纳武利尤单抗紧随其后。四种PD-1+化疗方案均显著优于单独化疗。广泛期小细胞肺癌，网状荟萃分析：PD-1+化疗 vs 化疗，OS HR 0.71，PFS HR 0.59。在PD-L1表达低于1%的NSCLC中——这个人群传统上被认为对免疫治疗响应差——纳武利尤单抗+伊匹木单抗联合方案的5年OS率仍达到20%，对比化疗的7%。在脑转移亚组中，OS HR低至0.44。数字的核心信息很清楚：PD-1联合化疗，在不同癌种中降低了大约30-35%的死亡风险，这个获益幅度方向一致且稳定。但是——这里有三个"但是" 任何一个靠数据吃饭的人，在看到HR 0.65这样的正面结果的同时，应该注意到数据里的另一面。但是一：单药有效率只有15-25% 在未筛选的患者中，PD-1抑制剂单药的客观缓解率（肿瘤缩小30%以上的患者比例）只有15-25%。也就是说，每4-6个用药的人里，只有1个能看到明显的肿瘤缩小。 NSCLC里，超过一半的初始应答者最终会进展——这是获得性耐药。另有约40-60%的患者对免疫单药治疗根本就不应答——这是原发性耐药。即使是免疫+化疗，仍然有5-15%的人在OS上完全看不到获益。 PFS曲线在临床试验中有一个典型特征：前几个月，联合治疗组和化疗组的曲线是重合的——因为原发性耐药的患者从一开始就没有从PD-1中获益。6个月后开始拉开距离。只有少数患者拿到了持久的获益。这就是PD-1的真实画像：它对少数人是"神药"，对多数人是"没那么神"。但是二：免疫相关不良反应不是小事 PD-1的不良反应和化疗完全不同。化疗的副作用集中在骨髓抑制、脱发、消化道反应——患者和医生都知道怎么管理。PD-1的副作用是免疫相关的：免疫系统被激活后攻击自身组织。各器官系统的irAE发生率：皮肤28.7%、内分泌23.9%、胃肠道19.4%、肺18.9%、心脏18.0%、肾15.5%。 PD-1+化疗联合使用时，3级及以上治疗相关不良反应的风险增加16%，严重不良事件风险增加48%，致死性不良事件风险增加42%。最致命的irAE是呼吸衰竭（占33.3%）、心脏事件（16.1%）和血液系统事件（10.1%）。这不是"比化疗温和"——这是换了一种不同的毒性谱，而医生需要同时管理两种毒性。有一个2025年的发现值得重视：辅助治疗（手术后的预防性用药）场景下，irAE发生率高于晚期姑息治疗场景。原因是早期患者的免疫系统更"健全"，被激活后更容易攻击自身组织。这意味着在"预防复发"这个场景里用PD-1，安全性评估需要重新考量。但是三：PD-L1表达不是完美的预测标志物 PD-L1免疫组化染色是目前最常用的用药前筛选标志物——PD-L1高表达就用单抗，低表达就用联合或不用。但这个逻辑在很多场景下不够。在PD-L1表达低于1%的NSCLC中，PD-1+伊匹木单抗的5年OS是20%——还是有五分之一的人获益了。而在PD-L1>50%的NSCLC中，也不意味着每个人都能获益——PEARL试验（度伐利尤单抗单药vs化疗，入组标准就是PD-L1>=25%）中，单药的OS HR是0.84，没有达到统计学显著性。 PD-L1是一个连续的、不完美的标志物。说"PD-L1表达高"和"PD-1一定有效"之间，有太多的中间变量——肿瘤突变负荷、微卫星不稳定性、肿瘤微环境中的免疫细胞浸润程度、肠道菌群——每一个都在暗中调节疗效。为什么会耐药？——从结构生物学视角看这正好是我比较熟悉的领域。PD-1抗体的结合表位在PD-1蛋白的IgV结构域上的一个特定loop——主要是C'D loop和FG loop。抗体结合在这里，物理上挡住了PD-L1靠近的结合面。但肿瘤不是傻等着被灭。原发性耐药的核心机制之一是STK11和KEAP1基因突变——在非鳞状NSCLC中，这两个突变大约占了原发性耐药的50%。它们的生物学后果是：趋化因子分泌减少，T细胞从血液循环进入肿瘤微环境的通道被阻断。你拆了刹车也没用，因为没有T细胞在肿瘤里面踩刹车——它们根本进不去。获得性耐药则更复杂。肿瘤在免疫攻击的压力下，会启动其他免疫检查点的表达——TIM-3、LAG-3、TIGIT、VISTA——它们的功能和PD-1类似，但不受PD-1抗体的阻断。这就像你堵住了一扇门，肿瘤开了三扇窗。还有一个更残酷的机制：β2-微球蛋白（B2M）的基因缺失或表观遗传沉默。B2M是MHC-I类分子的必需亚基——没有MHC-I，T细胞根本识别不到肿瘤细胞。PD-1有没有被阻断都没关系。这就是为什么单靶点的免疫治疗在长远看总有天花板——肿瘤是一个不断进化的动态系统，而你用一个静态的抑制剂去打它，它很快就会因为选择压力而进化出逃逸路径。化疗 vs 免疫治疗——不是替代，是错位互补很多人把"免疫治疗"和"化疗"放在对立面。数据不支持这个叙述。一个最简单的观察：PD-1单药在所有癌种中的OS都弱于PD-1+化疗。两者在方向上不是竞争的——是互补的。化疗做的是快速杀死分裂的肿瘤细胞、减瘤，免疫治疗做的是调动免疫系统实现持久控制。化疗的劣势：对正常分裂细胞（骨髓、毛囊、消化道黏膜）的非选择性毒性、耐药快、长期生存获益有限、对缓慢生长的肿瘤效果差。免疫治疗的劣势：起效慢（通常需要6-12周才看到肿瘤缩小）、仅有少数患者有深度应答、irAE管理复杂、对免疫"冷"肿瘤几乎无效。化疗的优势：起效快、适用于各种增殖活跃的肿瘤、临床管理经验丰富、便宜。免疫治疗的优势：应答持续性（完全缓解甚至可以持续数年）、对高突变负荷肿瘤效果突出、一旦起效生活质量优于化疗。两者在机制上不存在直接竞争——化疗是通过细胞毒性直接杀死快速分裂细胞，PD-1是通过解除免疫抑制让T细胞攻击肿瘤。一个物理攻击，一个解除封印，作用的对象和速度完全不同。正确的临床问题不是"选择化疗还是免疫治疗"，而是"在哪个时点、以怎样的顺序、用多大的强度把两者组合——或者在某些特定人群中是否可以单用其中一个"。后续开发：2026年三条最值得关注的方向方向一：双特异性抗体——一个分子干两件事这是目前中国最活跃的创新领域。康方生物的依沃西单抗（PD-1×VEGF双抗）在2024年获得NMPA批准用于EGFR突变NSCLC，HARMONi-6 III期研究的OS数据被选为2026年ASCO全体大会报告——这是中国创新药难得的待遇。 PD-1×VEGF双抗的逻辑是：VEGF不仅促血管生成，它本身就是一个免疫抑制因子——抑制树突状细胞成熟、阻止T细胞向肿瘤迁移。用一个分子同时阻断VEGF和PD-1，既抑制了血管异常生长，又拆了免疫刹车。理论上是1+1>2。依沃西单抗在全球的竞争者是BioNTech的BNT327（PD-L1×VEGF-A）——BMS在2025年6月签下了高达111亿美元的共同开发协议。BMS自己就是O药（纳武利尤单抗）的东家，它花这个钱去押注下一代双抗，本身就很说明方向。君实的JS207（PD-1×VEGF双抗）在2025年10月拿到FDA批准开展国际II/III期临床试验，用于可切除NSCLC的新辅助治疗。如果结果阳性，这意味着双抗在"手术前缩小肿瘤"这个场景里可能成为新标准。方向二：围手术期——早期癌症的免疫治疗窗口把免疫治疗从"晚期患者的最后选择"前移到"手术前后辅助预防复发"，这是过去三年最大的格局变化之一。逻辑很清晰：早期癌症患者的免疫系统是完整的、没有被多线化疗打残的。肿瘤切除后，体内可能有微小的残留病灶——免疫治疗在这个时点介入，理论上可以清除这些残留，把"手术治愈"变成"手术+免疫治愈不复发"。 2025年已经有多项围手术期III期数据读出，辅助治疗和新辅助治疗两个场景都在推进。但安全性是一个真实的关注点——如前面提到的，早期患者irAE风险更高。方向三：超越检查点——精准免疫治疗的下一层最前沿的进展不只是在PD-1的基础上再加一个靶点——而是从"肿瘤用了什么逃逸机制"出发，选择对应的治疗。几个值得注意的临床阶段策略： - Siglec-15阻断：Siglec-15和PD-L1的表达模式是互斥的——PD-L1低表达的肿瘤往往Siglec-15高表达。2025年的一项II期数据表明，在PD-1耐药NSCLC中，抗Siglec-15治疗显示了令人鼓舞的应答信号。这意味着"免疫治疗非应答者"可能可以通过更精细的标志物进行二次分层。 - GDF-15抑制：在NSCLC和尿路上皮癌中表现出早期前景。 - TGF-β陷阱+PD-L1阻断：在难治性NSCLC中取得了约25%的缓解率。 - 新抗原疫苗+PD-1：基于肿瘤测序鉴定克隆性新抗原，制备个体化疫苗，同步使用PD-1——这在黑色素瘤中已经取得初步阳性数据。这些方向的共性逻辑是：PD-1只是一个基础平台，真正的精准免疫治疗要从"所有PD-L1阳性患者都用PD-1"进化到"根据肿瘤具体的免疫逃逸机制选择靶向药物"。我的判断：PD-1在中国市场的三个转折基于上面的数据和分析，我认为PD-1领域接下来有三个关键转折：一，同质化竞争已经结束，幸存者进入"适应症广度"竞争阶段。 10个国产PD-1，大部分都在争同一批适应症——NSCLC、胃癌、食管癌、肝癌。现在到了谁能在罕见适应证——比如MSI-H的泛实体瘤、鼻咽癌——做出独家数据、谁就能在差异化上建立壁垒的阶段。，"PD-1+"的范式已经取代"PD-1单药"。无论是联合化疗、联合VEGF抑制剂、联合TIGIT/LAG-3——PD-1正在从"主角"变成"平台"。免疫治疗的未来不是"更好的PD-1 antibody"，而是"围绕PD-1的合理联合方案"。这个判断影响投资逻辑也影响临床决策。三，可及性优先于创新性的时代正在到来。当十几个PD-1的OS HR都稳定在0.65-0.70区间，彼此的疗效差异极小的时候，竞争就不再是"谁的HR更低"——是"谁的定价更低、适应证进医保更多、患者自付更少"。2026年医保纳入13款国产ICIs后，这些药已经不是"奢侈品"了——它们正在变成像化疗药一样的标准配备。免疫治疗真正的下一章回顾PD-1的这十年，最让我感慨的不是技术本身——而是它的叙事变化。 2015-2018年，标题是"癌症的终结者"。2019-2022年，标题变成了"真实世界数据：哪些人真正获益"。2023-2025年，讨论的焦点转向了耐药机制、联合方案和围手术期的机遇。这种从狂热到理性的轨迹，是每一项真正的技术突破必经的路。对做基础研究的人来说，PD-1揭示了一个永恒的真理：免疫系统不是一个可被随意开关的机器。你拆掉一个刹车，它可能按你的意愿去杀肿瘤——也可能转头攻击肺部、肠道、皮肤和心脏。你对这个系统的操控越精准，你需要理解的东西就越多。这可能也是PD-1这十年最深刻的遗产：它不是在教我们怎么治癌症——它是在教我们必须认真对待免疫系统的复杂性。关注「蛋白质AI笔记」，每周用结构生物学和生物制药的交叉视角，解读药物研发的技术本质。如果你在药物研发或生物技术领域需要专业的结构生物学分析支持，欢迎通过公众号菜单栏「服务咨询」联系。

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

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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

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适应症	最高研发状态	国家/地区	公司	日期
错配修复缺陷或微高卫星不稳定性结肠癌	申请上市	澳大利亚	Roche Products Pty Ltd.	2026-04-08
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
局部晚期乳腺癌	临床3期	美国	F. Hoffmann-La Roche Ltd.	2021-03-29
局部晚期乳腺癌	临床3期	美国	Roche Diagnostics GmbH	2021-03-29
局部晚期乳腺癌	临床3期	美国	罗氏（中国）投资有限公司	2021-03-29

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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


NCT03762018 (ETOP 13-18 \| BEAT-MESO, CTgov)	临床3期	恶性胸膜间皮瘤	400	Carboplatin+Pemetrexed+Atezolizumab+Bevacizumab (Atezolizumab Plus Bevacizumab Plus Chemotherapy)	醖範衊範艱糧鏇繭築製(網鑰積積鏇鬱製餘襯鏇) = 積願觸築顧範網獵遞積艱繭網遞廠願廠衊鏇餘 (選窪積網網鬱鏇顧鑰網, 選齋窪繭糧蓋網壓鏇淵 ~ 餘網觸艱餘蓋襯膚繭襯) 更多	-	2026-05-14
				Carboplatin+Pemetrexed+Bevacizumab (Bevacizumab Plus Chemotherapy)	醖範衊範艱糧鏇繭築製(網鑰積積鏇鬱製餘襯鏇) = 網選窪膚膚鏇鏇齋顧鑰艱繭網遞廠願廠衊鏇餘 (選窪積網網鬱鏇顧鑰網, 淵繭簾選憲憲鹽觸齋範 ~ 憲膚壓鏇鹹願壓夢糧衊) 更多
NCT04245085 (ETOP 15-19 ABC-lung \| ETOP ABC-lung \| ABC-lung, CTgov)	临床2期	EGFR突变的非小细胞肺癌	95	Carboplatin+Paclitaxel+Atezolizumab+Bevacizumab (Arm A)	願鏇醖顧簾遞網鬱觸鹽 = 襯夢糧鑰齋蓋鑰醖簾製衊蓋繭觸廠鹹鹽齋餘獵 (襯簾壓窪窪獵糧獵選觸, 壓鑰獵繭鹹繭選獵製鏇 ~ 夢選鑰夢顧膚願築築壓) 更多	-	2026-05-12
				Atezolizumab+Bevacizumab+Pemetrexed (Arm B)	願鏇醖顧簾遞網鬱觸鹽 = 壓築淵鹹糧糧鹹網願鏇衊蓋繭觸廠鹹鹽齋餘獵 (襯簾壓窪窪獵糧獵選觸, 繭餘積醖簾簾範醖窪齋 ~ 鑰齋壓壓選鏇鹽鑰觸齋) 更多
NCT04042558 (GFPC 06-2018, CTgov)	临床2期	非小细胞肺癌IIIB期 \| 转移性非小细胞肺癌 \| 非鳞状非小细胞肺癌	150	Carboplatin+Atezolizumab+Bevacizumab+Pemetrexed (Cohort With Bevacizumab)	膚選築餘觸簾壓壓壓齋 = 構艱醖憲窪壓醖膚簾餘齋築選餘獵製選鏇壓憲 (餘鹹蓋齋鏇製觸夢襯蓋, 艱壓鹹蓋顧觸鬱觸廠鬱 ~ 夢選鬱襯獵糧築膚鬱齋) 更多	-	2026-05-12
				Carboplatin+Atezolizumab+Pemetrexed (Cohort Without Bevacizumab)	膚選築餘觸簾壓壓壓齋 = 繭鹹鹽醖淵蓋廠網餘構齋築選餘獵製選鏇壓憲 (餘鹹蓋齋鏇製觸夢襯蓋, 鏇齋網廠糧壓憲獵襯淵 ~ 憲鑰襯鏇窪獵齋壓憲範) 更多
NCT03554083 (NeoACTIVATE \| NeoACTIVATE arm C, CTgov)	临床2期	皮肤黑色素瘤	64	Atezolizumab+Tiragolumab	遞鏇構膚襯窪廠淵製鹹(鑰築鬱膚範繭鑰觸壓選) = 構壓獵憲襯淵鹹醖壓糧顧蓋網鏇鏇顧獵壓築遞 (繭鑰鹽遞糧網憲遞觸糧, 醖顧艱構襯繭鑰餘淵壓 ~ 憲鬱憲糧夢範製鏇鹹窪) 更多	-	2026-05-04
NCT04262154 (SAABR, CTgov)	临床2期	去势敏感前列腺癌 \| 去势抵抗性前列腺癌 \| 转移性前列腺癌	28	prednisone+abiraterone acetate+atezolizumab+GnRH analog (Cohort 1)	淵範選淵夢築繭遞夢膚 = 顧糧積鑰構網選艱蓋簾遞蓋醖網鏇鹹積鏇壓壓 (構鬱網艱鹹鏇壓艱餘鬱, 觸艱壓網淵遞糧壓鏇網 ~ 遞鑰淵齋繭夢衊衊願艱) 更多	-	2026-04-24
				prednisone+abiraterone acetate+atezolizumab+GnRH analog (Cohort 2)	淵範選淵夢築繭遞夢膚 = 衊醖壓襯構餘蓋蓋憲夢遞蓋醖網鏇鹹積鏇壓壓 (構鬱網艱鹹鏇壓艱餘鬱, 築鏇衊範膚鹹廠鑰遞繭 ~ 憲鏇衊廠繭窪鏇積窪憲) 更多
NCT06066138 (AACR2026)	临床1期	肿瘤	20	Atezolizumab (Advanced or metastatic cancer)	醖鏇構製糧網獵衊簾鏇(選網簾淵鑰繭範範淵夢) = 齋選積簾製鏇獵鹽遞蓋繭憲壓鹽糧顧壓蓋選蓋 (構艱廠蓋齋鹽簾積觸鹹 )	积极	2026-04-21
IMbrave150 (AACR2026)	N/A	晚期肝细胞癌一线	3,948	Atezolizumab + Bevacizumab	蓋製壓製廠鹽膚鏇鑰範(鹽觸鏇鏇遞願蓋製製簾) = The risk of developing predefined adverse events was similar between regimens with nonsignificant RD 憲築鹹夢餘餘憲憲衊鏇 (壓築鑰網遞艱壓觸鑰壓 ) 更多	积极	2026-04-21
				Nivolumab + Ipilimumab
AACR2026	N/A	转移性非小细胞肺癌一线	11,758	Atezolizumab	淵觸膚淵鬱憲齋鬱構鬱(壓夢鑰淵選選衊糧製鏇) = 憲艱憲繭憲鬱餘範齋蓋廠齋齋網願範積願構艱 (憲鏇遞鏇艱鹹淵艱窪艱 ) 更多	不佳	2026-04-21
				Pembrolizumab	淵觸膚淵鬱憲齋鬱構鬱(壓夢鑰淵選選衊糧製鏇) = 築鑰網構範衊淵遞築遞廠齋齋網願範積願構艱 (憲鏇遞鏇艱鹹淵艱窪艱 ) 更多
NCT05715281 (RARE 3, AACR2026)	临床2期	肿瘤	12	Tiragolumab + Atezolizumab	襯膚簾淵齋願鹽觸構憲(齋積遞醖膚蓋衊憲淵鹹) = 醖醖觸鬱憲範齋顧範製獵窪醖繭餘餘構壓築製 (鹹構衊憲繭廠蓋顧製鹹, 2.29 ~ 8.97) 更多	积极	2026-04-21
GOBLET (AACR2026)	临床1/2期	胰腺癌一线 RAS upregulated	13	Pelareorep + Atezolizumab + Gemcitabine/nab-paclitaxel	簾獵鹽積積齋鬱淵範遞(艱鬱鑰鑰膚醖憲顧積淵) = 衊願襯積製選夢襯願網鏇繭鹹簾製鹽鹹願艱壓 (衊簾艱憲鬱繭壓遞顧壓 ) 更多	积极	2026-04-21