预约演示

更新于：2026-03-01

Atezolizumab

阿替利珠单抗

更新于：2026-03-01

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+ [180]

非在研适应症

大肠腺癌肺腺癌晚期胆管癌+ [109]

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

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

登录后查看时间轴

结构/序列

Sequence Code 122091L

来源: *****

Sequence Code 4720027H

来源: *****

关联

880

项与阿替利珠单抗相关的临床试验

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

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2026-03-01

申办/合作机构

University of Washington

[+3]

NCT07407933

/ Not yet recruiting临床1/2期

A Phase Ib/II, Multicenter, Open-Label Study to Evaluate Safety, Efficacy, and Pharmacokinetics of YL201 in Combination With Other Anti-Cancer Therapies in Patients With Advanced Solid Tumors

This is a phase Ib/II, multicenter, open-label study of YL201 combined with atezolizumab. The study will include 2 parts. Part 1 of the study is a dose escalation in participants with previously untreated ES-SCLC to determine the safety and tolerability of YL201 in combination with fixed dose of atezolizumab. The planned dose levels of YL201 are 1.2 mg/kg, 1.6 mg/kg and 2.0 mg/kg. Part 2 consists of a dose optimization stage followed by a dose expansion stage. During the dose optimization stage, participants will be randomized 1:1:1 to receive either YL201 at 1.2 mg/kg,1.6 mg/kg or 2.0 mg/kg Q3W in combination with fixed dose of atezolizumab. The decision to initiate the dose expansion stage in Part 2 and choose one or two of the YL201 dose level(s) will be based on the review of safety, PK, and efficacy from the dose optimization stage. Treatment will continue until disease progression, unacceptable toxicity, or withdraw of consent.

开始日期2026-03-01

申办/合作机构

苏州宜联生物医药有限公司

[+1]

100 项与阿替利珠单抗相关的临床结果

登录后查看更多信息

100 项与阿替利珠单抗相关的转化医学

登录后查看更多信息

100 项与阿替利珠单抗相关的专利（医药）

登录后查看更多信息

4,000

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.

2026-04-01·DEN open

A Case of Obstructive Jaundice due to Bile Duct Tumor Thrombus of Hepatocellular Carcinoma Diagnosed by Peroral Cholangioscopy

Article

作者: Tokumaru, Tomoko ; Endo, Mizuki ; Kinoshita, Keisuke ; Uchida, Takuro ; Murakami, Kazunari ; Okamoto, Kazuhisa ; Saito, Tomoko ; Iwao, Masao ; Kodama, Masaaki ; Arakawa, Mie

Abstract:

While hepatocellular carcinoma (HCC) often invades the portal or hepatic vein to form tumor thrombus, tumor thrombus in the bile duct is rare. In such cases, differentiation from intrahepatic cholangiocarcinoma is difficult, and the tumor often appears as a smooth, yellowish‐white, polypoid mass within the bile duct lumen. We report herein a case of obstructive jaundice due to bile duct tumor thrombus of HCC diagnosed by peroral cholangioscopy (POCS). A 64‐year‐old man presented with epigastralgia and jaundice. Contrast‐enhanced computed tomography revealed an irregular mass with hypoenhancement in liver segment S8, along with dilatation of the right intrahepatic bile duct due to the invading tumor. The hepatic mass was poorly visualized on ultrasound, making percutaneous liver tumor biopsy difficult. POCS was performed after endoscopic retrograde cholangiopancreatography for biopsy of the intrahepatic bile duct tumor thrombus. POCS clearly revealed a smooth, yellowish‐white, polypoid tumor in the right intrahepatic bile duct, and a biopsy of the tumor was performed under POCS. Based on the pathological findings, HCC was diagnosed, and chemotherapy with atezolizumab and bevacizumab was initiated.

2026-04-01·DEN open

A Rare Case of Immune‐related Adverse Events Localized to the Small Intestine

Article

作者: Taguchi, Towako ; Morikawa, Ryo ; Fukuda, Masayoshi ; Okamoto, Ryuichi ; Fujii, Toshimitsu ; Kanaya, Ryosuke ; Nemoto, Yasuhiro ; Ohtsuka, Kazuo ; Yamamoto, Kurara ; Shimizu, Hiromichi

ABSTRACT:

Enterocolitis is a common gastrointestinal manifestation of immune‐related adverse events (irAEs); however, only a few studies have reported on irAE enteritis with localized active inflammation in the small intestine. Here, we report the case of a 74‐year‐old man who developed diarrhea, abdominal pain, and oral intake difficulty and was subsequently hospitalized after receiving atezolizumab for pulmonary adenocarcinoma. Computed tomography and enterocolonoscopy revealed active inflammation in the small intestine but not in the colon, leading to the final diagnosis of irAE enteritis. After initiating prednisolone at a dose of 60 mg/day, his symptoms improved rapidly, and a follow‐up enterocolonoscopy revealed a marked reduction in inflammation. Being a relatively rare gastrointestinal toxicity, irAE enteritis often goes unrecognized due to diagnostic challenges, but can lead to serious AEs such as perforation. Therefore, even if colonoscopy findings are normal, a thorough examination of the small intestine is essential for patients who develop gastrointestinal symptoms while undergoing immune checkpoint inhibitor therapy. We herein report a rare case of irAE enteritis confirmed through endoscopic and pathological examination, which has not been previously reported.

3,068

项与阿替利珠单抗相关的新闻（医药）

2026-02-28

·ioncology

国际视野丨转移性透明细胞肾细胞癌的HIF-2α抑制剂联合治疗策略

点击上方蓝字关注我们编者按：目前晚期肾癌的一线治疗以抗血管和免疫治疗为主，而后线治疗多根据一线治疗方案组成、有效性和安全性进行药物选择。近年来研究显示，HIF-2α抑制剂在后线展现出显著疗效，并且正在探索联合治疗策略。肿瘤瞭望-泌尿时讯特别整理HIF-2α抑制剂相关研究，以飨读者。亮点抢先看 1 大多数散发性转移性透明细胞肾细胞癌（mccRCC）存在VHL失活，导致HIF-2α信号异常激活，而HIF-2α抑制剂，如贝组替凡已展现出临床应用价值。 2 值得注意的是，HIF-2α在血管生成通路中发挥关键作用，这为HIF-2α抑制剂与靶向VEGF的酪氨酸激酶抑制剂（TKI）联合应用奠定了基础。 3 HIF-2α抑制剂（例如贝组替凡和Casdatifan）与TKI的新型联合疗法，展现出良好的疗效，目前正在进行进一步的临床研究。对于mccRCC患者而言，免疫治疗与TKI为患者生存预后带来了质的飞跃。当下，一线双免联合方案（伊匹木单抗与纳武利尤单抗）、免疫联合TKI（如卡博替尼联合纳武利尤单抗、仑伐替尼联合帕博利珠单抗、阿昔替尼联合帕博利珠单抗），均显示了持久且亮眼的疗效。然而，现实的挑战依旧严峻：多数mccRCC患者的预后仍然较差，5年生存率预估仅18%。近期III期临床研究结果表明，对于既往接受过免疫治疗的mccRCC患者，再次使用基于免疫的联合方案，临床疗效并未实现实质性突破。因此，难治性mccRCC的治疗选择目前仍以TKI为主。我们需要具有全新作用机制的新型药物来更好地改善mccRCC预后。 VHL通路：mccRCC治疗的重要靶点 VHL肿瘤抑制基因作为缺氧通路调控的核心枢纽，通过缺氧诱导转录因子（HIF）进行精准调控。一旦VHL缺失，HIF便被激活，进而推动下游参与细胞增殖的基因开启表达程序。尤为值得关注的是，HIF-2α不仅能够上调血管生成生长因子，如VEGFA、PDGFB，还因促红细胞生成素的大量产生，诱发红细胞增多症。尽管VHL的胚系失活是遗传性VHL综合征和VHL相关肾细胞癌的典型特征，但在45%-85%的散发性ccRCC中，导致VHL缺失的体细胞突变同样广泛存在。这也让VHL通路成为mccRCC治疗中极具潜力的独特靶点。贝组替凡：开启HIF-2α抑制剂治疗新篇当前，贝组替凡作为美国食品药品监督管理局（FDA）唯一批准用于治疗VHL相关肿瘤及散发性转移性肾细胞癌的HIF-2α抑制剂，凭借LITESPARK-005试验的亮眼表现，成功突围。这项研究结果表明，相较于依维莫司，贝组替凡显著延长了患者的无进展生存期（PFS）。不过，贝组替凡也存在靶向毒性，贫血、疲乏和缺氧等不良反应需谨慎应对，但与TKI相关的腹泻、高血压等常见不良事件发生率较低。鉴于VHL通路与VEGF介导的血管生成之间千丝万缕的联系，HIF-2α抑制剂与TKI的联合，有望为mccRCC患者开辟更为高效的治疗路径。 △ HIF-2α抑制剂联合TKI临床试验结果（非头对头研究，数据谨慎解读） △ 截至2025年12月，正在进行的HIF-2α抑制剂联合TKI的临床试验结果（非头对头研究，数据谨慎解读）贝组替凡联合TKI：多项研究奏响疗效强音 LITESPARK-003研究：这项II期临床试验聚焦贝组替凡120mg/日联合卡博替尼60mg/日治疗mccRCC的疗效。研究纳入初治患者（队列1）与既往接受过免疫治疗的患者（队列2）。队列1中，联合治疗组的客观缓解率（ORR）高达70%，8%的患者实现完全缓解；队列2中，联合治疗组的ORR为31%。最新数据显示，队列1和队列2的中位无进展生存期（PFS）分别达到30个月和14个月，联合用药常见的3 - 4级不良事件为高血压（12%）、贫血（10%）和疲乏（8%）。 KEYMAKER-U-03研究：是一项I/II期伞式研究，旨在探索多种新型联合疗法在mccRCC中的疗效。其子研究03-B聚焦既往接受过免疫联合TKI治疗的mccRCC患者。中期分析显示，贝组替凡联合仑伐替尼的ORR达47%。 LITESPARK-011研究：这是一项正在进行的随机III期研究，针对既往接受过至多2种疗法（含免疫治疗）的mccRCC患者，旨在对比贝组替凡联合仑伐替尼和卡博替尼单药治疗。2025年10月发布的新闻稿表明，联合疗法在PFS上实现统计学意义的显著改善。除双药联合外，贝组替凡在三药联合方案中的表现同样引人瞩目。KEYMAKER-U-03研究的子研究03-A，针对未经治疗的mccRCC患者，贝组替凡联合仑伐替尼和帕博利珠单抗的治疗方案，疗效结果显示，能够达到78%的ORR（13%为完全缓解）以及32个月中位PFS。不过，该三联疗法导致24%的患者因不良事件终止研究，最常见的各级别不良事件包括贫血（76%）、疲乏（51%）和腹泻（47%）。LITESPARK-012研究正在进一步评估该联合疗法的良好疗效。 Casdatifan联合TKI Casdatifan是一种选择性强效的HIF-2α抑制剂，已在mccRCC治疗领域崭露头角。Casdatifan可显著降低促红细胞生成素水平（一种已验证的HIF-2α抑制剂生物标志物），且呈剂量依赖性，凸显了该药物的独特疗效。单药方案：针对既往接受过治疗的mccRCC患者，Casdatifan单药展现出亮眼疗效，在多线治疗患者队列中，ORR达到25%，且毒性可控。联合治疗探索：ARC-20试验的扩展队列，聚焦Casdatifan联合卡博替尼治疗既往接受过免疫治疗（无论是否联合TKI）的mccRCC患者。中期分析显示，联合用药组的ORR达46%，贫血（59%）和疲乏（56%）为最常见不良事件，仅7%的患者因不良事件减量，4%的患者因Casdatifan导致的低氧血症停药。基于早期研究的出色成果，III期PEAK-1试验顺势启动。该研究将既往接受过免疫治疗的mccRCC患者随机分为两组，分别接受卡博替尼60mg联合Casdatifan 100mg每日一次治疗，或卡博替尼60mg联合安慰剂治疗，主要终点是无进展生存期（PFS），关键次要终点包括OS和ORR。未来方向 HIF-2α抑制剂与TKI的新型联合疗法，已成为mccRCC患者的希望之光，众多可能改写临床实践的临床试验正在进行。但前行之路，仍需破解诸多难题：随着HIF-2α抑制剂及其联合疗法从难治性阶段向早期治疗拓展，后续治疗的最佳顺序尚无定论；接受过贝组替凡或Casdatifan方案后，继续使用其他抑制剂阻断HIF-2α的疗效也未明确。另外，还需要长期不良事件和生活质量数据来权衡这些联合疗法的临床获益和潜在毒性。参考文献上下滑动查看更多内容 [1]. Siegel RL, Kratzer TB, Giaquinto AN, Sung H, Jemal A. Cancer statistics, 2025. CA Cancer J Clin. 2025;75(1):10-45. [2]. Pal SK, Albiges L, Tomczak P, et al. Atezolizumab plus cabozantinib versus cabozantinib monotherapy for patients with renal cell carcinoma after progression with previous immune checkpoint inhibitor treatment (CONTACT-03): a multicentre, randomised, open-label, phase 3 trial. Lancet. 2023;402(10397):185-195. [3]. Choueiri TK, Albiges L, Barthélémy P, et al. Tivozanib plus nivolumab versus tivozanib monotherapy in patients with renal cell carcinoma following an immune checkpoint inhibitor: results of the phase 3 TiNivo-2 study. Lancet. 2024;404(10460):1309-1320. [4]. Cowey CL, Rathmell WK. VHL gene mutations in renal cell carcinoma: role as a biomarker of disease outcome and drug efficacy. Curr Oncol Rep. 2009;11(2):94-101. [5]. Choueiri TK, Kaelin WG Jr. Targeting the HIF2-VEGF axis in renal cell carcinoma. Nat Med. 2020;26(10):1519-1530. [6]. Brauch H, Weirich G, Brieger J, et al. VHL alterations in human clear cell renal cell carcinoma: association with advanced tumor stage and a novel hot spot mutation. Cancer Res. 2000;60(7):1942-1948. [7]. Shenoy N, Pagliaro L. Sequential pathogenesis of metastatic VHL mutant clear cell renal cell carcinoma: putting it together with a translational perspective. Ann Oncol. 2016;27(9):1685-1695. [8]. U.S. Food and Drug Administration. FDA approves belzutifan for cancers associated with von Hippel-Lindau disease. FDA.gov. August 13, 2021. Updated February 1, 2022. Accessed December 17, 2025. https://www.fda.gov/drugs/resources-information-approved-drugs/fda-approves-belzutifan-cancers-associated-von-hippel-lindau-disease. [9]. U.S. Food and Drug Administration. FDA approves belzutifan for advanced renal cell carcinoma. FDA.gov. December 14, 2023. Accessed December 17, 2025. https://www.fda.gov/drugs/resources-information-approved-drugs/fda-approves-belzutifan-advanced-renal-cell-carcinoma. [10]. Jonasch E, Donskov F, Iliopoulos O, et al; MK-6482-004 Investigators. Belzutifan for renal cell carcinoma in von Hippel-Lindau disease. N Engl J Med. 2021;385(22):2036-2046. [11]. Choueiri TK, Powles T, Peltola K, et al; LITESPARK-005 Investigators. Belzutifan versus everolimus for advanced renal-cell carcinoma. N Engl J Med. 2024;391(8):710-721. [12]. Choueiri TK, Merchan JR, Figlin R, et al. Belzutifan plus cabozantinib as first-line treatment for patients with advanced clear-cell renal cell carcinoma (LITESPARK-003): an open-label, single-arm, phase 2 study. Lancet Oncol. 2025;26(1):64-73. [13]. Albiges L, Suarez C, Powles T, et al. KEYMAKER-U03 Substudy 03B: pembrolizumab (pembro) and targeted therapy combinations for advanced clear cell renal cell carcinoma (ccRCC). J Clin Oncol. 2025;43:5s (suppl; abstr 440). [14]. Suarez C, Rojas C, Shin SJ, et al. Novel pembrolizumab-based treatments as first-line therapy in advanced clear-cell renal cell carcinoma: substudy 03A of the open-label, umbrella platform, phase I/II KEYMAKER-U03 trial. Ann Oncol. Published online October 17, 2025. [15]. Choueiri TK, Lee JL, Merchan JR, et al. Casdatifan (Cas) monotherapy in patients (pts) with previously treated clear cell renal cell carcinoma (ccRCC): safety, efficacy and subgroup analysis across multiple doses from ARC-20, a phase 1 open-label study. J Clin Oncol. 2025;43:5s (suppl; abstr 441). [16]. Choueiri TK, Bauer TM, Merchan JR, et al. Updated results from the phase 2 LITESPARK-003 study of belzutifan plus cabozantinib in patients with advanced clear cell renal cell carcinoma (ccRCC). J Clin Oncol. 2025;43:5s (suppl; abstr 549). [17]. Merck. Merck and Eisai announce WELIREG® (belzutifan) plus LENVIMA® (lenvatinib) met primary endpoint of progression-free survival (PFS) in certain previously treated patients with advanced renal cell carcinoma. Merck.com. October 28, 2025. Accessed December 17, 2025. https://www.merck.com/news/merck-and-eisai-announce-welireg-belzutifan-plus-lenvima-lenvatinib-met-primary-endpoint-of-progression-free-survival-pfs-in-certain-previously-treated-patients-with-advanced-renal-c/. [18]. Ghasemi M, Kim JY, Seitz L, et al. Pharmacokinetics, pharmacodynamics and safety of casdatifan, a novel hypoxia-inducible factor-2α inhibitor, in healthy participants. Br J Clin Pharmacol. 2025;91(12):3366-3377. （来源：《肿瘤瞭望-泌尿时讯》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期免疫疗法临床失败抗体药物偶联物

2026-02-27

·Business Wire

Signatera™ MRD Data at ASCO GU Highlights Potential Utility Across GU Cancers, Including for Bladder Preservation

AUSTIN, Texas--(BUSINESS WIRE)--Natera, Inc. (NASDAQ: NTRA), a global leader in cell-free DNA and precision medicine, today announced it will present new data in genitourinary malignancies at the American Society of Clinical Oncology Genitourinary Cancers Symposium (ASCO GU), taking place February 26-28, 2026. Across four oral presentations in muscle-invasive bladder cancer (MIBC), these data reinforce Signatera’s role in identifying patients who benefit from adjuvant immunotherapy, supporting response-adaptive bladder preservation strategies, and refining molecular residual disease (MRD) detection with plasma circulating tumor DNA (ctDNA) and urinary tumor DNA (utDNA). Bladder Preservation: INDIBLADE and RETAIN The INDIBLADE and RETAIN multicenter phase 2 trials demonstrate Signatera’s consistent performance in treatment response monitoring across diverse neoadjuvant regimens in MIBC, with 73-77% of patients demonstrating clearance of ctDNA following therapy and Signatera-negativity showing strong associations with positive outcomes, even with the bladder preserved. INDIBLADE, the findings of which will be published today in Nature Medicine, investigated induction with combination immune checkpoint inhibitors (ICI) followed by chemoradiotherapy as a bladder-sparing strategy in stage II/III MIBC patients. The results show that Signatera status post-ICI was associated with bladder-intact event-free survival (BI-EFS). Specifically, Signatera-negativity at baseline and post-neoadjuvant therapy was linked to an 88.6% and 91% estimated two-year BI-EFS, respectively. RETAIN evaluated a clinical response-adapted approach to identify patients for potential bladder-preservation following neoadjuvant therapy. The findings showed that post-treatment ctDNA clearance or negativity was associated with improved metastasis-free survival (MFS), and that Signatera-negative patients with no clinical or radiographic evidence of disease managed with active surveillance achieved MFS comparable to Signatera-negative patients undergoing cystectomy. In contrast, persistent Signatera-positivity was associated with poor outcomes. Perioperative Care: NIAGARA This phase 3 randomized perioperative study includes the first-ever presentation of utDNA data with clinical correlation. The combination of utDNA and ctDNA status post-neoadjuvant therapy and pre-cystectomy identified the group with the highest 24-month EFS. utDNA-positivity pre-cystectomy was more strongly associated with residual non-invasive disease vs ctDNA-positivity was more strongly associated with residual invasive disease. These data suggest that the combined assessment of utDNA and ctDNA can provide complementary risk stratification benchmarked against pathologic staging, enabling comprehensive identification of residual disease. “As treatment options expand in perioperative and bladder preservation settings, we need tools that help us determine who truly requires additional therapy and who may safely avoid it,” said Michiel van der Heijden, M.D., Ph.D., Netherlands Cancer Institute, principal investigator of INDIBLADE and presenting author of the NIAGARA study. “The data presented at ASCO GU demonstrate that MRD assessment with Signatera has strong correlations with outcomes and the potential to inform these critical treatment decisions.” “Following our milestone PMA submission to the FDA based on IMvigor011, these compelling data presentations reflect our commitment to transforming care across the spectrum of genitourinary malignancies,” said Minetta Liu, M.D., chief medical officer of oncology and early cancer detection at Natera. “The new data suggests a particularly important opportunity for Signatera to optimize clinical decisions around bladder preservation, a major opening to improve patient quality of life.” The full list of presentations at ASCO GU includes: February 27, 8:10 AM PT | Abstract #633 (Oral Presentation) Presenter: Joaquim Bellmunt, M.D. Circulating tumor (ct)DNA-guided adjuvant atezolizumab (atezo) in muscle-invasive bladder cancer (MIBC): Exploratory analysis of ctDNA dynamics in the IMvigor011 trial February 27, 8:10 AM PT | Abstract #632 (Oral Presentation) Presenter: Pooja Ghatalia, M.D. Circulating tumor DNA (ctDNA) to guide response-adapted bladder preservation in muscle invasive bladder cancer (MIBC): Integrated analysis of the RETAIN trials February 27, 11:30 AM PT | Abstract #797 Presenter: Can Aydogdu, M.D. Integrating genomic profiling and circulating tumor DNA monitoring to optimize surveillance strategies in muscle-invasive bladder cancer February 27, 11:30 AM PT | Abstract #831 Presenter: Can Aydogdu, M.D. Association of ctDNA status with upstaging, pathologic outcomes, and genomic alterations in high-risk NMIBC February 27, 2:30 PM PT | Abstract #637 (Oral Presentation) Presenter: Jan-Jaap J. Mellema, M.D. Induction ipilimumab plus nivolumab followed by consolidating chemoradiotherapy as bladder-sparing treatment in stage II/III urothelial carcinoma of the bladder: The phase 2 INDIBLADE trial February 27, 4:00 PM PT | Abstract #636 (Oral Presentation) Presenter: Michiel van der Heijden, M.D., Ph.D. Urinary tumor DNA (utDNA) and circulating tumor DNA (ctDNA) in patients (pts) with muscle-invasive bladder cancer (MIBC) who received perioperative durvalumab (D) in NIAGARA February 28, 7:00 AM PT | Abstract #532 Presenter: Shuchi Gulati, M.D., M.Sc. Association of pre-operative circulating tumor DNA (ctDNA) status with clinicopathologic characteristics in patients (pts) with localized renal cell carcinoma (RCC) February 28, 7:00 AM PT | Abstract #620 Presenter: Dalia Kaakour, M.D., MPH Use of circulating tumor DNA (ctDNA) in the detection of residual disease and recurrence for patients with testicular cancer February 27, 11:30 AM PT | Abstract #860 Presenter: Lingbin Meng, M.D., Ph.D. Use of circulating tumor DNA (ctDNA) in the detection of residual disease and recurrence for patients with testicular cancer February 27, 11:30 AM PT | Abstract #800 Presenter: Tanya Jindal, BS, BA Predictive value of early circulating tumor DNA (ctDNA) response in advanced urothelial carcinoma (aUC) treated with enfortumab vedotin plus pembrolizumab (EVP). February 28, 7:00 AM PT | Abstract #541 Presenter: David F. McDermott, M.D. Circulating tumor DNA (ctDNA) analysis in participants (pts) with advanced clear cell renal cell carcinoma (ccRCC) treated with first-line pembrolizumab (pembro) monotherapy from the phase 2 KEYNOTE-427 study. About Natera Natera™ is a global leader in cell-free DNA and precision medicine, dedicated to oncology, women’s health, and organ health. We aim to make personalized genetic testing and diagnostics part of the standard-of-care to protect health and inform earlier, more targeted interventions that help lead to longer, healthier lives. Natera’s tests are supported by more than 350 peer-reviewed publications that demonstrate excellent performance. Natera operates ISO 13485-certified and CAP-accredited laboratories certified under the Clinical Laboratory Improvement Amendments (CLIA) in Austin, Texas, and San Carlos, California, and through Foresight Diagnostics, its subsidiary, operates an ISO 27001-certified and CAP-accredited laboratory certified under CLIA in Boulder, Colorado. For more information, visit www.natera.com. Forward-Looking Statements All statements other than statements of historical facts contained in this press release are forward-looking statements and are not a representation that Natera’s plans, estimates, or expectations will be achieved. These forward-looking statements represent Natera’s expectations as of the date of this press release, and Natera disclaims any obligation to update the forward-looking statements. These forward-looking statements are subject to known and unknown risks and uncertainties that may cause actual results to differ materially, including with respect to our efforts to develop and commercialize new product offerings, whether the results of clinical or other studies will support the use of our product offerings, the impact of results of such studies, our expectations of the reliability, accuracy, and performance of our tests, or of the benefits of our tests and product offerings to patients, providers, and payers. Additional risks and uncertainties are discussed in greater detail in "Risk Factors" in Natera’s recent filings on Forms 10-K and 10-Q, and in other filings Natera makes with the SEC from time to time. These documents are available at www.natera.com/investors and www.sec.gov.

临床结果临床2期ASCO会议临床3期

2026-02-27

·谈呼吸

一缕青烟后的生死博弈：2025 烟草病学年度进展的临床解读与思考

引言：从 “烟雾病” 到 “烟雾病理” 在呼吸科门诊工作了三十多年，我常常会问患者一个问题：“您知道烟草病学是什么吗？” 大部分人的回应都是摇头。他们熟悉慢阻肺、肺癌、间质性肺病这些疾病，却很难把它们和小小的香烟联系起来。这其实值得我们医生反思 —— 当疾病的治疗被划分成各个专科领域，那些疾病共同的根源往往就被我们忽视了。烟草病学，简单来说，就是专门研究烟草使用对人体健康造成的危害，以及探讨相关防治策略的交叉学科。在 2025 年，中国和国际呼吸领域发布了许多重要的指南与共识，从肺癌筛查到慢阻肺管理，从戒烟干预到免疫治疗等各个方面，都体现出一个清晰的学术方向：回归疾病的根源，进行整体防控。接下来，我将从临床一线的角度出发，对 2025 年度烟草病学的相关进展进行系统梳理和深度解读。希望能给同行们提供一些参考，也为患者朋友们点亮一盏认知的明灯，让大家更清楚地了解这一领域的知识。一、流行病学新图景：烟草烟雾下的 “三驾马车” 1.1 肺癌：中国女性的沉默危机肺癌一直是全球和中国死亡率最高的恶性肿瘤。《中华医学会肺癌临床诊疗指南（2025 版）》的最新数据表明，中国肺癌的发病在性别和地域上有明显差异。特别值得注意的是，中国女性肺癌患者中，不吸烟的比例比西方国家高很多。这说明除了烟草本身，像二手烟、室内空气污染、基因易感性等因素，在中国人群患肺癌的过程中也起着重要作用。但这绝不意味着我们可以小看烟草的危害。研究已经明确显示，吸烟的人患肺癌的风险是不吸烟的人的 10 - 25 倍，而且吸烟的量越大、时间越长，患肺癌的风险就越高。在我的临床工作中，就见过很多 50 - 60 岁的男性患者，他们吸烟史大多超过 30 包年，等确诊肺癌的时候，往往已经到了局部晚期或者发生了远处转移。 1.2 慢阻肺：被低估的 “隐形杀手” 《国家基层慢性阻塞性肺疾病防治及管理实施指南（2025）》指出，中国 40 岁及以上人群中，慢阻肺的患病率高达 13.7%，患者总数差不多有 1 亿人。这个数字真的很惊人，相当于每 10 个中老年人里，就有 1 - 2 个人患有慢阻肺，然而，知道自己患病并且接受规范治疗的人还不到 10%。烟草暴露是导致慢阻肺的首要危险因素。大约 80 - 90% 的慢阻肺死亡都和吸烟有关。2025 年 GOLD 报告特别强调了 “早发现、早干预” 的重要性，建议对于有吸烟史、职业暴露史或者家族史的高危人群，要定期进行肺功能筛查。 1.3 间质性肺疾病：烟草相关纤维化的新认知间质性肺疾病（ILD）是一类比较复杂的疾病，其中特发性肺纤维化（IPF）和吸烟的关系最为紧密。《间质性肺疾病年度进展 2025》提到，吸烟是 IPF 的独立危险因素，吸烟的人患 IPF 的风险是不吸烟的人的 1.6 - 2.3 倍。另外，吸烟还和脱屑性间质性肺炎（DIP）、呼吸性细支气管炎伴间质性肺疾病（RB - ILD）等疾病密切相关。二、肺癌筛查新纪元：LDCT 与戒烟的 “双轮驱动” 2.1 《中国肺癌低剂量 CT 筛查指南（2025 年版）》核心更新 2025 年，中国肺癌筛查指南有了重大更新，核心理念可以总结为 “精准定位、风险分层、综合干预”：高危人群定义更新：年龄要≥50 岁；吸烟史≥20 包年（包括已经戒烟，但戒烟时间不到 15 年的人）；或者有职业暴露史（比如接触石棉、氡、铍、铬、镉、镍、硅、煤烟等）；或者一级亲属中有患肺癌的。筛查策略优化：推荐每年进行 LDCT 筛查；强调利用解剖变异和 AI 辅助诊断；引入风险预测模型，实现个性化的筛查间隔。这次更新和 NCCN 2025、USPSTF 的建议一致，都强调 LDCT 是目前唯一被证实能够降低肺癌死亡率的筛查方法。 2.2 “筛查 + 戒烟”：黄金组合的临床价值《肺癌筛查及肺结节健康管理专家共识（2025 版）》最有前瞻性的一点就是：把戒烟咨询和宣传融入到肺癌筛查的整个过程中。这个理念的改变意义深远。研究发现，参加 LDCT 筛查的吸烟者，他们的戒烟意愿比普通人群要高很多。利用筛查这个机会进行简短的戒烟干预，能让戒烟成功率提高 2 - 3 倍。这很好理解，当患者看到自己肺部有结节或者磨玻璃影的时候，“吸烟有害健康” 就不再是抽象的概念，而是实实在在的恐惧，改变行为的动力自然就大大增加了。在临床实践中，我通常用 “三步法” 来把筛查和戒烟干预结合起来：告知：清楚地向患者解释 CT 检查发现的异常和吸烟之间的关系；建议：强烈建议患者戒烟，告诉他们戒烟是降低肺癌风险最根本、最有效的办法；支持：给患者提供戒烟药物处方，并且做好随访支持。三、慢阻肺管理新策略：从 “治疗” 到 “管理” 的范式转变 3.1 GOLD 2025 核心更新要点 GOLD 2025 报告在之前 ABCD 分组的基础上，又进一步强调了以下内容：心血管风险评估：慢阻肺患者发生心血管事件的风险明显增加，GOLD 2025 首次建议对所有慢阻肺患者进行心血管风险评估，包括做心电图、超声心动图以及检测生物标志物。急性加重管理：急性加重是慢阻肺病程的关键转折点。指南推荐：首选短效支气管扩张剂（SABA/SAMA）；全身使用糖皮质激素（泼尼松 40mg/d，连用 5 天）可以缩短恢复时间；当出现痰量增加、脓痰等典型细菌感染症状时，使用抗生素。稳定期治疗优化：双支气管扩张剂（LABA/LAMA）是症状管理的基础；对于急性加重高风险的患者，推荐添加 ICS（吸入糖皮质激素）；血嗜酸粒细胞计数≥300/μL 是对 ICS 反应良好的预测指标。 3.2 中西医结合的新视角《慢性阻塞性肺疾病中西医结合诊疗指南（2025 版）》为慢阻肺管理提供了具有中国特色的方案：稳定期：通过益肺健脾、补肾固本，配合西医规范治疗；急性加重期：采用清热化痰、宣肺平喘的方法，还能缩短抗生素使用时间；康复期：打太极拳、练八段锦等传统功法，可以改善运动耐量。在临床工作中，我发现中西医结合治疗对于改善患者生活质量、减少急性加重次数，确实有独特的优势，尤其适合老年患者以及有多种合并症的患者群体。 3.3 运动处方：被忽视的 “药物” 《慢性阻塞性肺疾病人群运动处方临床路径》的发布，标志着运动干预从简单的 “建议” 变成了正式的 “处方”。指南推荐：有氧训练：像步行、踏车，每周进行 3 - 5 次，每次 20 - 30 分钟；抗阻训练：进行上下肢肌力训练，每周 2 - 3 次；呼吸肌训练：比如缩唇呼吸、腹式呼吸，每天 2 次。我经常跟住院患者说：“肺康复就像是给肺做‘理疗’，效果不比任何药物差。” 大量的科学证据都证明，肺康复可以改善患者呼吸困难的症状，提高运动耐量，减少再次住院的几率，从成本效益比来看，比任何单一药物治疗都要好。四、间质性肺疾病诊疗进展：精准医学的曙光 4.1 抗纤维化药物：从 “延缓” 到 “希望” 特发性肺纤维化（IPF）曾经被叫做 “不是癌症的癌症”，预后非常差。不过近年来，抗纤维化药物的出现改变了这种情况。尼达尼布与吡非尼酮：两项重要的临床试验（INPULSIS 和 ASCEND）证明，尼达尼布和吡非尼酮可以显著延缓 IPF 患者 FVC（用力肺活量）下降的速度，大概能延缓 50%。2025 年的最新研究还发现，早期开始使用抗纤维化治疗的患者，他们的无进展生存期（PFS）明显延长了。新药研发动态：BI 1015550 是一种新型磷酸二酯酶 4B 抑制剂，II 期临床试验显示它可以改善 IPF 患者的肺功能，III 期临床试验正在进行中。另外，PD - 1/PD - L1 轴也正在成为纤维化肺疾病治疗的潜在新靶点。 4.2 诊断技术的进步《间质性肺疾病年度进展 2025》强调了多学科讨论（MDD）在 ILD 诊断中的核心地位。高分辨率 CT（HRCT）依然是诊断的关键依据，AI 辅助诊断系统的应用也在不断提高诊断的一致性和准确性。对于病因不明确的 ILD，经支气管冷冻肺活检（TBLC）和外科肺活检（SLB）可以提供组织病理学方面的依据。不过，选择活检的时机和方式，需要综合考虑风险和获益，特别是对于年纪大、心肺功能差的患者。五、免疫治疗与靶向治疗：肺癌治疗的革命性突破 5.1 PD - 1/PD - L1 抑制剂：从 “晚期” 到 “早期” 免疫检查点抑制剂彻底改变了晚期非小细胞肺癌（NSCLC）的治疗局面。2025 年多项临床试验有了新的数据更新：晚期 NSCLC 一线治疗：KEYNOTE - 024 的长期随访数据表明，PD - L1 高表达（≥50%）的患者，接受帕博利珠单抗单药治疗，中位总生存期（OS）超过 30 个月，比化疗组要好很多。IMPOWER - 110 研究显示，阿替利珠单抗单药治疗 PD - L1 高表达患者，中位 OS 达到 20.2 个月。围手术期治疗：CheckMate - 816 研究证实，纳武利尤单抗联合化疗用于可切除 NSCLC 的新辅助治疗，病理完全缓解率（pCR）达到 24%，比单纯化疗组显著提高。这一结果开创了免疫治疗应用于早期肺癌的先河。 5.2 安全性管理：不可忽视的另一面免疫相关不良事件是 PD - 1/PD - L1 抑制剂特有的毒性表现。2025 年中国《免疫检查点抑制剂临床应用指南》特别强调：肺炎：发生率大概在 3 - 5%，严重的肺炎可能会危及生命；内分泌毒性：像甲状腺功能异常、垂体炎等；皮肤毒性：皮疹、瘙痒、白癜风样改变等。临床医生必须时刻保持警惕，建立起早识别、早干预的全程管理体系。六、戒烟干预：临床医生最被低估的 “处方” 6.1 戒烟的医学证据戒烟的好处超乎很多人的想象：戒烟 1 年后，冠心病风险降低 50%；戒烟 5 年后，口腔癌、喉癌、食管癌风险降低 50%；戒烟 10 年后，肺癌风险降低约 50%；戒烟 15 年后，心血管疾病风险就和不吸烟的人差不多了。 GOLD 2025 明确指出：“戒烟是唯一被证实可以延缓肺功能下降速度、改善慢阻肺预后的干预措施。” 6.2 临床戒烟干预策略世界卫生组织推荐的 “5A” 法是标准的戒烟流程： Ask（询问）：每次患者就诊都要询问吸烟情况； Advise（建议）：强烈建议患者戒烟； Assess（评估）：评估患者的戒烟意愿； Assist（帮助）：为患者提供戒烟支持和药物； Arrange（安排）：安排随访。药物治疗：尼古丁替代疗法（NRT），比如口香糖、贴片、吸入剂；伐尼克兰，这是一线首选药物，戒烟成功率大概在 30 - 40%；安非他酮，适合伴有抑郁症状的患者。在临床实践中，我常常告诉患者：“戒烟不是靠意志力就能做到的，吸烟成瘾是一种疾病，需要医学帮助。” 把戒烟这件事从单纯的道德层面剥离，让患者明白这是一种需要治疗的疾病，而不是个人品质问题，这是和患者建立治疗联盟的第一步。七、未来展望：从 “疾病治疗” 到 “健康促进” 站在 2025 年这个时间点，回顾烟草病学领域的发展历程，我们可以看到，从 “治疗已经发生的疾病” 到 “预防疾病发生” 的宏大画卷正在徐徐展开。 7.1 精准医学与个体化治疗基因检测、液体活检、人工智能辅助诊断等新技术的应用，正让呼吸系统疾病的诊断和治疗变得更加精准。对于肺癌患者，基于 ctDNA - MRD（循环肿瘤 DNA 微小残留病灶）的适应性治疗策略正在改变传统治疗模式。对于慢阻肺患者，血嗜酸粒细胞计数、炎症因子谱等生物标志物正在为治疗决策提供指导。 7.2 多学科协作（MDT）模式的深化肺癌、慢阻肺、间质性肺疾病都不是单一科室能够独立处理的。呼吸科、胸外科、肿瘤科、影像科、康复科、营养科等多学科协作，已经成为规范化诊疗的标准配置。 7.3 从 “以疾病为中心” 到 “以患者为中心” 无论是《肺癌筛查及肺结节健康管理专家共识（2025 版）》对患者知情同意的重视，还是慢阻肺管理中对患者报告结局（PROs）的关注，都体现了医学人文关怀的回归。治疗的目标不再仅仅是延长患者的生命，还包括提高患者的生活质量，维护患者的尊严。结语：一根香烟的重量在三十多年的临床生涯中，我见过太多因为吸烟而走向生命尽头的患者。他们中有权势显赫的企业家，有教书育人的教师，还有享受天伦之乐的慈祥祖父…… 躺在病床上，他们最常说的一句话就是：“早知道，当初就不该吸烟。” 作为医生，我们面对的不仅仅是疾病本身，更是背后一个个鲜活的生命和完整的家庭。每一次劝导患者戒烟，每一次建议患者进行早期筛查，每一次提供规范化治疗，都是在和死神的博弈中，为患者争取更多生存的机会。烟草病学的研究进展，让我们从科学的角度更深入地了解了烟草烟雾的危害机制，也为我们提供了更多的干预方法。然而，医学的最终价值，不在于发表了多少论文，而在于能够改变多少患者的命运。希望每一位读到这篇文章的读者，无论是医生还是患者，都能成为控烟行动的践行者和传播者。因为，每一根香烟的背后，都承载着生与死的重量。互动话题：各位读者，对于吸烟与这些疾病的关联，您有什么看法或者身边有相关的故事吗？医生朋友们，在临床工作中，您在劝导患者戒烟、进行疾病筛查和治疗方面，有没有什么特别的经验或者遇到过什么困难呢？欢迎在评论区分享交流。新春快乐 2026 New Year 马年吉祥 2026 New Year 免责声明本文为基于当前医学研究与临床指南的科普性文章，旨在提供信息参考，不构成任何具体的医疗建议。所有诊断和治疗决策，请务必咨询并遵从您的主治医生。 2026 转发给需要的家人朋友，一起科学控病！ @关注我，带你用医生的视角看懂呼吸世界！

100 项与阿替利珠单抗相关的药物交易

登录后查看更多信息

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,

后查看更多信息

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,

后查看更多信息

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

登录后查看更多信息

临床结果

适应症

分期

评价

查看全部结果

研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT02530489 (CTgov)	临床2期	三阴性乳腺癌 \| 浸润性乳腺癌	37	Nab-paclitaxel+Atezolizumab	繭夢齋壓衊夢鹹簾夢繭 = 廠選糧築壓淵齋醖鏇鏇餘積繭廠範選顧衊鹹壓 (憲簾繭鹽範齋積範鏇構, 簾齋窪觸艱選願齋壓壓 ~ 糧衊網衊壓窪鬱選繭顧) 更多	-	2026-02-17
NCT05746481 (CTgov)	临床2期	转移性非鳞状非小细胞肺癌 \| 非鳞状非小细胞肺癌 \| 脑转移瘤	3	Carboplatin+Pemetrexed+Atezolizumab+Tiragolumab	範蓋鹹遞範醖築夢積觸 = 夢糧願艱鏇鹽衊繭築築鏇鹹鬱醖憲醖衊淵醖遞 (觸簾網簾簾憲鹽觸艱蓋, 製鑰觸網製鹽醖餘築製 ~ 蓋遞餘遞窪廠選選構築) 更多	-	2026-01-22
NCT05009069 (NEOTERIC, Pubmed \| NEWS \| J Clin Oncol) 人工标引	临床2期	局部晚期直肠癌新辅助	55	Atezolizumab + Tiragolumab	膚蓋艱築衊餘餘醖廠獵(糧觸簾簾廠構膚選艱膚) = 衊遞壓鑰範鹽廠膚簾製顧糧淵齋餘壓夢積淵蓋 (顧繭願艱網繭繭襯蓋觸, 18.6 ~ 55.9) 更多	积极	2026-01-13
				Atezolizumab	膚蓋艱築衊餘餘醖廠獵(糧觸簾簾廠構膚選艱膚) = 衊襯願繭蓋膚遞遞糧築顧糧淵齋餘壓夢積淵蓋 (顧繭願艱網繭繭襯蓋觸, 8.6 ~ 42.3) 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	鹹鑰範範蓋選餘構淵製(簾窪齋憲鏇餘鑰膚憲廠) = 壓鑰鏇衊鬱窪窪獵鑰膚膚鑰夢糧構蓋廠醖廠蓋 (築簾觸膚鑰積鹽網觸醖, 28.5 ~ 44.7) 更多	不佳	2026-01-13
				Concurrent chemoradiation alone	鹹鑰範範蓋選餘構淵製(簾窪齋憲鏇餘鑰膚憲廠) = 廠衊範夢構蓋醖簾鑰繭膚鑰夢糧構蓋廠醖廠蓋 (築簾觸膚鑰積鹽網觸醖, 28.1 ~ 42.5) 更多
NCT07280377 (GOBLET, Company_Website) 人工标引	临床1/2期	肛门肿瘤三线	14	Pelareorep + Atezolizumab	膚製窪衊膚膚壓壓鏇蓋(選選遞餘遞衊蓋鑰選鏇) = 廠餘淵鹹膚獵網膚築鹹遞網夢構遞廠齋壓艱鑰 (顧廠窪築顧製鏇選鏇製 ) 更多	积极	2026-01-12
NCT04770272 (neoMono, CTgov)	临床2期	三阴性乳腺癌	442	Biopsy Arm A+Cyclophosphamide+Carboplatin+Paclitaxel+Atezolizumab 840 MG in 14 ML Injection+epirubicin (Arm A)	積繭襯糧窪遞衊齋膚觸 = 簾醖壓鬱醖襯廠膚鹹積構範簾膚廠齋憲齋夢壓 (齋壓觸顧選鹹鬱鑰壓獵, 夢願網蓋艱構構衊鹹簾 ~ 餘衊膚觸壓膚遞鹹積願) 更多	-	2026-01-12
				Biopsy Arm B+Cyclophosphamide+Carboplatin+Paclitaxel+Atezolizumab 1200 MG in 20 ML Injection+epirubicin (Arm B)	積繭襯糧窪遞衊齋膚觸 = 鑰膚齋襯顧鏇觸夢積繭構範簾膚廠齋憲齋夢壓 (齋壓觸顧選鹹鬱鑰壓獵, 簾窪艱鹹範廠鏇夢憲壓 ~ 選膚齋鬱鹹網餘糧憲衊) 更多
NCT05168163 (ASCO_GI2026)	临床2期	晚期肝细胞癌二线	18	Atezolizumab plus MKI (cabozantinib or lenvatinib)	膚蓋糧憲網艱齋鹹網艱(醖製廠製構齋獵壓觸積) = 夢襯廠衊鑰蓋鏇構憲構廠壓廠繭遞壓鹽積淵夢 (膚簾醖構壓遞襯壓繭壓 ) 更多	积极	2026-01-08
				MKI alone	膚蓋糧憲網艱齋鹹網艱(醖製廠製構齋獵壓觸積) = 蓋壓積餘壓餘獵襯鬱願廠壓廠繭遞壓鹽積淵夢 (膚簾醖構壓遞襯壓繭壓 ) 更多
ASCO_GI2026	N/A	晚期肝细胞癌一线	3,306	Bevacizumab-atezolizumab	獵鹽鏇衊夢遞齋願構艱(餘鏇範願鹹繭蓋襯顧製): HR = 0.873 (95.0% CI, 0.75 ~ 0.935), P-Value = 0.0016	积极	2026-01-08
				Lenvatinib
NCT03784326 (ASCO_GI2026)	临床1/2期	食管腺癌 \| 胃食管交界处腺癌辅助	23	Atezolizumab + Tiragolumab + modified FOLFOX	鬱積網鏇製願淵糧遞窪(餘廠鹽構觸顧鏇鏇淵積) = 鬱壓觸製糧範簾糧網觸襯選網衊簾鬱廠構壓憲 (憲構鬱鹹壓夢鏇壓膚網 ) 更多	积极	2026-01-08
NCT06294548 (ASCO_GI2026)	临床1/2期	晚期肝细胞癌一线	27	Valemetostat tosylate (DS-3201b)BevacizumabAtezolizumab tosylate (DS-3201b) + Valemetostat tosylate (DS-3201b)BevacizumabAtezolizumab + Valemetostat tosylate (DS-3201b)BevacizumabAtezolizumab	憲遞鬱膚艱選餘憲積衊(鬱積廠窪廠窪淵簾夢範) = 積鹹願鑰壓鹽範積窪糧糧顧餘顧築鬱鹹築壓顧 (構網遞遞簾蓋觸廠鑰觸 ) 更多	积极	2026-01-08