预约演示

更新于：2026-04-03

Atezolizumab

阿替利珠单抗

更新于：2026-04-03

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+ [145]

非在研适应症

大肠腺癌肺腺癌晚期胆管癌+ [104]

原研机构

Genentech, Inc.

Universitair Medisch Centrum Groningen

在研机构

Roche Registration GmbHRoche Pharma AG

罗氏（中国）投资有限公司

+ [22]

非在研机构

Kymab Ltd.

Sanofi

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

884

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]

NCT07059494

/ Recruiting临床4期IIT

A Feasibility Clinical Trial of Atezolizumab and Bevacizumab in Combination With Y^90 Radioembolization for Patients With Hepatocellular Carcinoma (HCC) for Liver Transplantation

A single institution, single arm, two-cohort feasibility trial to evaluate the combination of locoregional Y^90 therapy with systemic atezolizumab and bevacizumab, in participants presenting with hepatocellular carcinoma (HCC) 1) within Milan Criteria (MC) with AFP ≥ 400 ng/ml as a means of bridge therapy prior to transplant, 2) beyond the Milan Criteria (MC) (within USCF DS criteria and all comers), as a means of downstaging prior to liver transplantation.

开始日期2026-06-01

申办/合作机构

Icahn School of Medicine at Mount Sinai

[+1]

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

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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4,077

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·ALIMENTARY PHARMACOLOGY & THERAPEUTICS

Clinical Trial: Early Nivolumab Addition to Regorafenib in Patients With Hepatocellular Carcinoma in Second‐Line (The GOING Trial)

Article

作者: José Luis Lledo ; Àngels Kateb ; Marta Fortuny ; Sergio Muñoz-Martínez ; Andrés Castaño-García ; Gemma Iserte ; Neus Llarch ; Maria Reig ; Loreto Boix ; María Varela ; Christie Perelló ; Ana Matilla ; Jordi Bruix ; Antonio Guerrero ; Ferran Torres ; Jordi Rimola ; Esther Samper ; Mercedes Iñarrairaegui ; Ángeles García-Criado ; José Rios-Guillermo ; Gema Domenech ; Marco Sanduzzi-Zamparelli ; Laura Carrión ; Beatriz Mínguez ; Laura Márquez

ABSTRACT:

Background & Aims:

Highly effective second‐line treatments for hepatocellular carcinoma remain an unmet need. The GOING investigator‐initiated Phase I/IIa trial evaluated regorafenib plus nivolumab ( add‐on ) in patients who progressed on sorafenib (Cohort‐A) or discontinued atezolizumab‐bevacizumab (Cohort‐B).

Methods:

Patients received regorafenib for two 28‐day cycles, adding nivolumab in cycle 3, until unacceptable adverse events, symptomatic progression, withdrawal or death. Primary endpoint was safety. Secondary endpoints included overall survival, time to progression, post‐progression survival, objective response rate and incidence of new‐extrahepatic‐spread.

Results:

Of 85 patients screened, 67 were enrolled (75.5% BCLC‐C). All experienced adverse events and 9% led to discontinuation. Severe treatment‐related adverse events occurred in 28.4% overall, 32.1% in Cohort‐A, and 14.3% in Cohort‐B. Median overall survival was 20.0 (95% CI 11–37) months, with 40.6% survival at 36 months. In Cohort‐A, median overall survival was 25 (95% CI 14–39) months with 45% survival at 36 months, while Cohort‐B median overall survival was 8 (95% CI 4–NE) months with 28.6% survival at 24 months. Objective response rate was 16.4%; median time to progression and post‐progression survival were 5 (95% CI 4–9) months and 14 (95% CI 8–33) months. Intrahepatic growth was the most common progression pattern, followed by new‐extrahepatic‐spread.

Conclusions:

The add‐on strategy of regorafenib plus nivolumab in second‐line had manageable safety and significant clinical activity with a noteworthy median overall survival of 20 months. Among those progressing on sorafenib, 45% were alive at 3 years. These findings support further evaluation with mechanism‐guided trials after progression on immunotherapy.

Trial Registration:

EudraCT number: 2019‐003108‐10; https://www.clinicaltrialsregister.eu

3,213

项与阿替利珠单抗相关的新闻（医药）

2026-04-02

·美通社

再鼎医药宣布达成全球临床研究合作及供应协议，以评估创新性DLL3抗体药物偶联物Zocilurtatug Pelitecan与双特异性T细胞衔接器的联合治疗

与安进合作探索靶向 DLL3 的 ADC 药物 zocilurtatug pelitecan 联合 IMDELLTRA ® 的临床潜力安进将申办并执行一项全球 1b 期研究；再鼎医药保留 zocilurtatug pelitecan 的完整所有权上海和马萨诸塞州剑桥 2026年4月2日 /美通社/ -- 再鼎医药有限公司（纳斯达克代码：ZLAB；香港联交所股份代号：9688）今日宣布与安进公司（纳斯达克代码：AMGN）达成一项全球临床研究合作，旨在评估再鼎医药处于临床阶段的靶向delta样配体3（DLL3）的抗体药物偶联物（ADC）zocilurtatug pelitecan（zoci，前称ZL-1310）联合安进IMDELLTRA ® （tarlatamab-dlle），一款靶向DLL3的双特异性T细胞衔接器（BiTE ® ）疗法，用于治疗广泛期小细胞肺癌（ES-SCLC）患者。作为该合作协议的一部分，安进将申办一项全球1b期研究，评估zoci联合IMDELLTRA ® 在ES-SCLC患者中的安全性和有效性。再鼎医药将保留zoci的完整所有权，并将向安进提供临床研究用药。再鼎医药总裁、全球研发负责人Rafael G. Amado博士表示："这种双靶向联合策略有望提升全身及颅内治疗的缓解率和缓解程度，应对耐药机制，并为小细胞肺癌患者开辟新的治疗范式。这两种疗法利用了互补的作用机制——我们的ADC将强效的细胞毒性载荷直接递送至表达DLL3的肿瘤细胞，而T细胞衔接器则旨在通过结合同一抗原激活T细胞，引发抗肿瘤免疫应答。" Zoci是靶向DLL3的 ADC，用于小细胞肺癌的治疗。再鼎医药已在2025年EORTC-NCI-AACR（ENA）大会和2025年美国临床肿瘤学会（ASCO）年会上公布了zoci的1/2期临床研究数据，数据显示zoci在经过多药治疗的小细胞肺癌（SCLC）患者中实现了高缓解率，展示了显著的颅内活性且可耐受的安全性。安进的IMDELLTRA ® 已获得FDA批准，目前在美国上市，用于治疗既往接受含铂化疗后出现疾病进展的ES-SCLC成人患者。请参阅IMDELLTRA ® 包括黑框警告在内的完整处方信息。关于 Zocilurtatug Pelitecan (zoci, 前称 ZL-1310) Zoci是再鼎医药全球肿瘤研发管线中一款靶向DLL3的新型ADC。DLL3是一种在多个神经内分泌癌症中过度表达的抗原，是小细胞肺癌（SCLC）已验证的治疗靶点，通常与不良临床预后相关。Zoci包含人源化抗DLL3单克隆抗体，该抗体与新型喜树碱衍生物（一种拓扑异构酶1抑制剂）连接作为其有效载荷。此分子的设计来源于新型ADC技术平台TMALIN ® 。该平台能够利用肿瘤微环境克服第一代ADC疗法遇到的相关挑战（包括脱靶载荷的毒性）。 Zoci正在进行全球临床开发，涉及以下三项临床研究方案：DLLEVATE研究——一项随机三期关键性研究，旨在进一步评估zoci对比研究者选择的单药化疗用于复发性ES-SCLC患者中的安全性和有效性；一项评估zoci用于包括肺外神经内分泌癌的特定实体瘤中的1b/2期研究；以及一项评估zoci单药及联合免疫检查点抑制剂阿替利珠单抗用于ES-SCLC的1a/1b期研究。 Zoci的安全性特征及明确的全身性和颅内的疗效，支持其有望作为ES-SCLC一线联合方案的基石，用以降低化疗的毒性负担。Zoci已获得美国FDA授予的治疗SCLC的孤儿药资格认定和快速通道资格认定。关于小细胞肺癌（ SCLC ）小细胞肺癌是最具侵袭性和致命的实体肿瘤之一，每年全球约250万被诊断为肺癌的患者中，大约有15%属于小细胞肺癌 [1,2] 。其中，约三分之二的小细胞肺癌患者在确诊时已经处于广泛期 [3] 。该阶段复发率高且预后差。ES-SCLC患者预后尤为严峻：初始治疗后中位总生存期仅约12个月 [4] ，五年总生存率约5-10% [5] 。一旦患者使用含铂化疗后出现疾病进展，可用的治疗选择曾经十分有限。IMDELLTRA ® 是首款靶向DLL3的双特异性T细胞衔接器疗法，在上述患者中已验证具有总生存期获益。Zocilurtatug Pelitecan与IMDELLTRA ® 的联合用药方案有望在此优势基础上，进一步改善有效性，同时保持可控的安全性 [6] 。 References: [1] J Thorac Oncol. 2023 Jan;18(1):31-46; Lung Cancer Foundation of America. [2] WHO Globocan 2022. [3] Sabari JK, et al. Nat Rev Clin Oncol. 2017;14:549-561. [4] Phase 3 IMpower133 (atezolizumab) and CASPIAN study (durvalumab). [5] National Cancer Institute. www.cancer.gov . Accessed October 15, 2024. [6] Mountzios et al, NEJM 2025 关于再鼎医药再鼎医药（纳斯达克股票代码：ZLAB；香港联交所股份代号：9688）是一家以研发为基础、处于商业化阶段的创新型生物制药公司，总部位于中国和美国。我们致力于通过创新产品的发现、开发和商业化解决肿瘤、免疫、神经科学和感染性疾病领域未被满足的巨大医疗需求。我们的目标是利用我们的能力和资源为人类健康带来积极影响。有关再鼎医药的更多信息，请访问 www.zailaboratory.com 或关注 https://x.com/ZaiLab_Global 。再鼎医药前瞻性声明本新闻稿包含关于再鼎医药未来预期、计划和展望的前瞻性陈述，包括但不限于与我们开发和商业化包括zocilurtatug pelitecan在内的新一代抗体药物偶联物（ADC）相关的前景和计划，zocilurtatug pelitecan的潜在获益，以及小细胞肺癌和其他神经内分泌癌的潜在疗法有关的陈述。这些前瞻性陈述可能包含诸如"旨在"、"预计"、"认为"、"可能"、"估计"、"预期"、"预测"、"目标"、"打算"、"或许"、"计划"、"可能的"、"潜在"、"将会"、"将要"等词语以及其他类似表述。此类陈述构成《1995年美国私人证券诉讼改革法案》所定义的前瞻性陈述。前瞻性陈述并非历史事实的陈述，亦非对未来表现的担保或保证。前瞻性陈述基于我们截至本新闻稿发布之日的预期和假设，并且受到固有不确定性、风险以及可能与前瞻性陈述所预期的情况存在重大差异的情势变更的影响。实际结果可能受各种重要因素的影响而与前瞻性陈述所示存在重大差异，该等因素包括但不限于：(1)我们成功商业化自身已获批上市产品并从中产生收入的能力；(2)我们为自身的运营和业务活动获取资金的能力；(3)我们候选产品的临床开发和临床前开发的结果；(4)相关监管机构对我们的候选产品作出审批决定的内容和时间；(5)与在中国营商有关的风险；和(6)我们向美国证券交易委员会（SEC）提交的最新年报和季报以及其他报告中指出的其他因素。我们预计后续事件和发展将导致我们的预期和假设改变，但除法律要求之外，不论是出于新信息、未来事件或其他原因，我们均无义务更新或修订任何前瞻性陈述。该等前瞻性陈述不应被视为我们在本新闻稿发布之日后任何日期的意见而加以信赖。如需查阅公司向SEC提交的文件，请访问公司网站 www.zailaboratory.com 和SEC网站 www.SEC.gov 。

2026-04-02

·小药说药

抗体在癌症治疗中的应用：机制、进展与未来展望

-01- 引言在过去的一个世纪里，已经开发出化疗和放疗等强效治疗方法来治疗癌症。不幸的是，这些方法通常缺乏足够的选择性，无法在避免不可耐受毒性的情况下使用足以根除癌细胞的高剂量。单克隆抗体能够提供显著扩大治疗窗口所需的高特异性水平，一些抗体甚至能够区分仅相差一个氨基酸或一个翻译后修饰的两个抗原。几项关键技术的发展使得抗体能够用于治疗目的。首先，20世纪70年代开发的杂交瘤系统允许生产和筛选针对人类抗原的高特异性小鼠单克隆抗体。其次，将人抗体恒定区移植到小鼠抗体可变区的能力产生了具有更好治疗效果和更少不良反应的嵌合抗体。第三，20世纪90年代转基因小鼠模型和噬菌体展示系统的使用使得能够生成针对癌症靶点的全人源抗体。随着这些技术进步和临床需求的增加，过去二十五年见证了基于抗体的新疗法的爆炸式增长。自1997年以来，已有超过五十种用于肿瘤学应用的基于抗体的治疗剂获得美国食品和药物管理局（FDA）和欧洲药品管理局（EMA）的批准。除了基于抗体的治疗剂外，抗体片段还用于生成用于T细胞工程的嵌合抗原受体。 -02- 一、抗体生成一系列技术被用于识别靶向肿瘤抗原的治疗性单克隆抗体或抗体片段。这些技术包括用靶抗原免疫啮齿动物、噬菌体或酵母展示等展示技术、从人和转基因小鼠中进行单B细胞克隆，以及从骆驼科动物中识别单域抗体。具有临床实用性的抗体的进一步开发涉及抗体工程，使其逐渐与人类免疫系统更加兼容。嵌合和人源化抗体单克隆抗体传统上是通过使用1975年Cesar Milstein和Georges Kohler开发的杂交瘤技术生产的。在此过程中，用特定抗原免疫后，从小鼠脾脏或淋巴结中分离B细胞，然后与骨髓瘤细胞系（如Sp2/0）融合，形成称为杂交瘤细胞系的杂交细胞。通常通过酶联免疫吸附测定筛选蛋白质结合，通过流式细胞术筛选细胞结合来筛选杂交瘤克隆。杂交瘤技术稳健且经济高效地产生了一系列小鼠单克隆抗体。然而，注入人体的小鼠抗体会产生人抗鼠抗体免疫反应，限制了其疗效并增加了不良反应。因此，大多数获得监管批准的小鼠抗体后来都被撤市。Blinatumomab是一种使用两个小鼠来源的单链可变片段格式且缺乏Fc片段的双特异性T细胞衔接器，是唯一在临床得到广泛采用的鼠源抗体。为了减少患者免疫反应的诱导，将小鼠抗体的恒定区替换为其人源对应部分以产生嵌合抗体。利妥昔单抗和西妥昔单抗是最早产生的嵌合抗体之一，通过将小鼠抗体2B8和225的可变区连接到人免疫球蛋白G1重链和人κ轻链恒定区而生成。然而，具有鼠源可变区的嵌合抗体仍可被识别为外来物，导致可能清除治疗性抗体的人抗嵌合抗体免疫反应。这可能会限制嵌合抗体的重复应用并阻碍其临床开发。为了进一步减少不必要的免疫反应，通过20世纪80年代开发的称为“人源化”的过程增加了小鼠单克隆抗体的人源含量。人源化涉及仅将小鼠抗体的互补决定区移植到人抗体的框架区。曲妥珠单抗是最早开发的人源化抗体之一，通过将小鼠HER2抗体mumAb4D5的CDR移植到人抗体框架中而开发，类似的策略被用于开发奥比妥珠单抗、帕博利珠单抗和阿特珠单抗。除了小鼠杂交瘤技术外，还开发了兔杂交瘤用于生产针对肿瘤抗原（如间皮素）的兔单克隆抗体。CDR移植方法已被用于人源化兔单克隆抗体，例如针对间皮素的YP218，用于临床开发。监管机构批准的大多数治疗性抗体都是使用杂交瘤方法生成，然后工程化为嵌合或人源化形式，并广泛用于癌症治疗。人源抗体借助20世纪90年代开发的两项技术，即人抗体噬菌体展示和人抗体表达转基因小鼠模型，实现了生成全人源抗体的最后一步。为了生成产生人源抗体的转基因小鼠，将人Ig基因座或可变区插入小鼠基因组，同时破坏小鼠Ig基因。从用靶抗原免疫的小鼠中分离B细胞用于单B细胞克隆和测序。转基因小鼠平台XenoMouse、VelocImmune和HuMab产生了九种获批的靶向癌症的人源抗体：达雷妥尤单抗、伊匹木单抗、纳武利尤单抗、奥法木单抗、帕尼单抗、度伐利尤单抗、西米普利单抗、替索妥单抗和瑞拉利单抗。这些抗体成功的临床开发导致了多个转基因小鼠平台的迅速兴起，例如KyMouse、OmniRat、H2L2 Mouse、Trianni Mouse和RenMab。展示技术为人源抗体开发提供了替代平台。使用噬菌体展示，可以从多样性超过10¹⁰的大型文库中分离人scFv或Fab片段。噬菌体展示技术通常使用M13丝状噬菌体来表达与噬菌体pIII外壳蛋白融合的抗体片段，如scFv。用固定在微孔板或珠子上的靶抗原筛选噬菌体文库。洗去非特异性噬菌体结合物，收获剩余的特异性结合物用于下一轮筛选。通常需要三到五轮筛选来分离特异性结合物。这个过程称为噬菌体淘选，它模拟了体外的免疫选择。使用下一代测序的新方法有助于快速识别稀有结合物。 Dyax的噬菌体展示系统产生了三种获得监管批准的全人源抗体：雷莫西单抗、奈西妥珠单抗和阿维鲁单抗。此外，由Dyax、Cambridge Antibody Technology、MorphoSys等公司产生的多种噬菌体展示来源的人源抗体目前正在进行临床试验。转基因小鼠和噬菌体展示技术都有其独特的优势。通常，转基因小鼠平台倾向于产生具有更理想生物物理特性和在临床试验中表现更好的抗体，而噬菌体展示允许选择靶向特定表位的抗体。除了噬菌体展示外，细胞表面展示、核糖体展示和mRNA展示技术也已用于抗体生成。酵母和哺乳动物细胞表面展示允许在真核细胞表面表达重组抗体片段。这使得能够通过流式细胞术分离抗原特异性细胞并发现高亲和力结合物。比较嵌合、人源化和人源抗体嵌合、人源化或全人源抗体生产的目标是减少针对抗体的免疫反应，这种反应带有重复给药导致中和和不良反应的风险。对各种抗体疗法进行的大型人类临床试验分析显示，使用嵌合、人源化和人源抗体时，免疫原性逐渐下降。然而，该研究未检验较低的免疫原性是否会导致更优的肿瘤消退或患者生存期。几种FDA和EMA批准的嵌合、人源化和人源抗体靶向常见的癌症抗原，如CD20、HER2和EGFR，尽管表位不同且结合特性不同。比较靶向CD20、HER2和EGFR的抗体的III期临床试验已证明相似的总生存期和相似的治疗相关停药率，表明治疗效果相当。然而，显著的HAMA免疫反应阻碍了靶向双唾液酸神经节苷脂GD2的小鼠抗体的开发，并且在自身免疫性疾病患者中使用利妥昔单抗观察到了强烈的HACA免疫反应。对HACA免疫反应的担忧，加上简化人源化和人源抗体生成的技术进步，增加了这两种格式的利用。进入当前临床试验的抗体要么是人源化产品，要么是全人源产品，并且根据之前的试验结果，人源化和人源抗体在患者中往往表现出相似的治疗效果。 -03- 二、抗体疗法的不同形式根据其结构和功能机制，抗体疗法可分为三大主要格式：单特异性抗体、双特异性抗体以及与载荷偶联的抗体。单特异性抗体格式单特异性抗体格式涉及结合靶抗原的全长免疫球蛋白。在五种免疫球蛋白同种型中，只有IgG与新生儿Fc受体结合，导致半衰期较长。靶向癌症的抗体利用IgG同种型来利用这种延长的半衰期，并且通常每21天给药一次。大多数FDA和EMA批准的抗体以及开发中的抗体都使用单特异性IgG抗体格式。IgG抗体以四种亚类存在，大多数治疗性抗体使用IgG1亚类。单特异性抗体格式的靶抗原是细胞表面蛋白，主要是实体瘤中过表达的生长因子受体。对于血液系统恶性肿瘤，抗体通常靶向由不同免疫细胞亚群表达的细胞表面糖蛋白。作用机制：抗体与癌细胞结合通过多种机制导致癌细胞死亡。直接阻断来自生长因子的生存信号和阻断血管生成导致肿瘤血供破坏是这些抗体导致实体瘤消退的两个主要机制。相比之下，血液系统恶性肿瘤中靶向的CD标记物通常在促进癌细胞存活方面没有实质性作用，相反，抗体通过募集和激活免疫效应细胞来诱导细胞毒性。每个IgG抗体亚类赋予抗体不同的效应功能。IgG1亚类Fc段与巨噬细胞和自然杀伤细胞表达的激活Fcγ受体具有强亲和力。FcγR结合导致巨噬细胞和NK细胞介导的抗体依赖性细胞毒性和抗体依赖性细胞吞噬作用，直接杀死癌细胞。最早获得FDA批准的两种抗体是靶向恶性B细胞表达的CD20的利妥昔单抗和靶向乳腺癌细胞过表达的HER2的曲妥珠单抗，这两种抗体都使用常见的IgG1同种型。IgG1诱导ADCC和ADCP的能力最终导致癌细胞死亡，并且可以通过Fc工程进一步增强。IgG1亚类还结合补体蛋白C1q，通过补体依赖性细胞毒性导致癌细胞死亡。目前，市售的单克隆抗体主要由IgG1组成。除了效应功能外，IgG亚类的选择还基于结构稳定性、循环半衰期、制造和监管批准经验、缺乏免疫原性或意外副作用，以及公司开发组合中特定IgG亚类的可用性。单特异性抗体Fc工程化：大多数IgG1抗体效应功能由Fc结构域介导。数十年的研究增加了我们对Fc结构域与不同Fc受体相互作用的理解，并帮助设计了具有理想效应功能的抗体。在临床前研究中显示活性增加的常见Fc结构域修饰包括去岩藻糖基化或关键残基的氨基酸取代，两者都导致增强的ADCC和ADCP。免疫检查点抑制剂在过去十年中，一类完全不同的靶向免疫细胞调节检查点的单特异性抗体显示出显著的临床疗效。目前有11种FDA和EMA批准的免疫检查点抑制抗体正用于治疗超过二十种不同类型的癌症，包括肺癌、黑色素瘤、肾细胞癌、头颈部鳞状细胞癌，预计未来还会有更多此类抑制抗体获得批准。免疫检查点抑制剂在大多数癌症类型中显示出20-30%的反应率。然而，某些恶性肿瘤，如霍奇金淋巴瘤和皮肤癌、微卫星不稳定性高癌症、PDL1表达升高的癌症、或高突变负荷的癌症，以及一些与病毒相关的癌症，反应率显著更高。作用机制：免疫检查点阻断抗体抑制负向调节T细胞的通路，从而重振细胞毒性T细胞以杀死癌细胞。在临床试验中正在研究的超过20个免疫检查点中，治疗性抗体已获得FDA或EMA批准的三个蛋白质或通路是CTLA4、PD1-PDL1和LAG3。CTLA4、PD1和LAG3的表达在T细胞刺激后被诱导，其主要目的是限制T细胞活化的程度。 PD1阻断抗体是迄今为止使用最广泛的免疫检查点抑制剂。七种获批的PD1阻断抗体和两种目前正在进行临床试验的抗体使用IgG4格式，与IgG1同种型相比，该格式不能有效激活补体级联反应且Fc受体结合较弱。因此，IgG4格式可能保护表达PD1的效应T细胞免于被ADCC或CDC意外杀死。类似的IgG4格式也用于靶向LAG3的抗体瑞拉利单抗。所有IgG4抗体都携带S228P突变以防止Fab臂交换。免疫检查点抑制剂毒性：免疫检查点阻断抗体通过一般免疫激活介导癌细胞杀伤，这有时可能会错误地针对健康组织。免疫检查点抑制抗体具有非常独特的不良反应谱，称为免疫相关不良事件。这些irAE包括各种表现，包括皮肤、胃肠道、肝脏、内分泌、肺部、神经和心脏事件。虽然不常见，但偶尔可能因免疫检查点抑制而产生严重且可能致命的毒性。在许多情况下，需要使用糖皮质激素、肿瘤坏死因子拮抗剂、霉酚酸酯或其他免疫调节剂进行临时免疫抑制来控制irAE。双特异性抗体格式第二种格式包括多样化的双特异性抗体类别。与单特异性抗体不同，双特异性抗体结合两种不同的抗原或表位。抗原可以位于同一靶细胞上或不同细胞上。靶向两种不同细胞的双特异性抗体大多是T细胞衔接器，将癌细胞与效应T细胞交联；因此，它们被称为T细胞衔接器。交联后，效应T细胞被激活，通过释放细胞毒性颗粒和淋巴因子杀死结合的靶癌细胞。另一类双特异性抗体参与同一靶细胞表达的两种不同抗原，例如两种不同的生长因子受体。此类双特异性抗体通过阻断靶生长因子受体的增殖信号以及激活针对癌细胞的NK细胞和巨噬细胞来杀死靶细胞。双特异性T细胞衔接器：博纳吐单抗在2014年获得监管批准，导致了此类基于抗体的治疗剂的爆炸性增长。原型TCE双特异性博纳吐单抗是一种小的54 kDa融合蛋白，大小约为IgG抗体的三分之一。博纳吐单抗由双特异性抗体所需的最基本元件组成；一个靶向癌症的scFv通过甘氨酸-丝氨酸肽连接子与一个结合T细胞的scFv连接。博纳吐单抗通过抗CD19 scFv结合B细胞，同时通过抗CD3 scFv连接并激活T细胞，导致B细胞死亡。博纳吐单抗在一系列B细胞恶性肿瘤中显示出活性，并获得批准用于治疗B细胞前体急性淋巴细胞白血病。博纳吐单抗的基本设计被后续获得监管批准的TCE双特异性抗体所采用。制药公司通常对使用独特架构和方法组装双特异性抗体的独特TCE格式进行商标注册。常见格式包括双特异性T细胞衔接器、Duobody、DART和Xmab，博纳吐单抗使用BiTE格式。Tebentafusp是一种独特的TCE双特异性格式，名为ImmTAC，它将靶向黑色素瘤细胞表达的gp100-HLA-A02复合物的亲和力增强的TCR与抗CD3 scFv连接起来。Tebentafusp在转移性葡萄膜黑色素瘤患者中显示出优越的总生存期，于2022年获得批准。在过去2年中，六种靶向血液系统恶性肿瘤的新双特异性抗体获得监管批准。这些包括teclistamab和elranatamab、talquetamab用于多发性骨髓瘤，以及mosunetuzumab、epcoritamab和glofitamab用于B细胞淋巴瘤。然而，TCE双特异性抗体在实体瘤中的批准滞后。然而，针对实体恶性肿瘤的TCE双特异性抗体临床试验激增，为这一策略将扩大其应用范围带来了希望。最近关于TCE双特异性抗体靶向DLL3在小细胞肺癌中的阳性I期试验报告令人鼓舞，表明实体瘤障碍将被打破。靶向同一细胞上不同抗原的双特异性抗体：双特异性抗体也被设计为结合靶癌细胞上的两种不同抗原或表位，而不参与效应T细胞。它们的抗癌作用是通过阻断两个增殖信号通路介导的，从而最大化抗肿瘤活性。除了其受体阻断活性外，这些双特异性抗体还可以被工程化以包含功能性的IgG1 Fc结构域，使它们能够通过非T细胞基础的免疫效应通路（如ADCC、ADCP和CDC）杀死癌细胞。阿米万他单抗是第一个靶向癌细胞表达的EGFR和MET的受体阻断双特异性抗体，并获得监管批准用于治疗具有外显子20插入突变的非小细胞肺癌。阿米万他单抗比单受体结合抗体的组合更有效地阻断驱动肺癌亚群的EGFR和MET通路信号传导。此外，阿米万他单抗的IgG1 Fc结构域被工程化为具有低岩藻糖水平，这增强了FcγRIIIa结合和NK细胞介导的ADCC。类似的双特异性设计被扎尼达他单抗采用，该抗体用每个Fab臂结合两个不同的HER2表位。这些臂靶向HER2亚结构域2和亚结构域4，分别是帕妥珠单抗和曲妥珠单抗的结合位点，这两种靶向HER2的抗体被批准用于治疗HER2+乳腺癌。临床前研究表明，与曲妥珠单抗、帕妥珠单抗或曲妥珠单抗和帕妥珠单抗的组合相比，扎尼达他单抗增强了HER2聚集、受体下调并增加了CDC介导的HER2+癌细胞杀伤。在一项I期试验中，扎尼达他单抗在一系列HER2+实体瘤中显示出鼓舞人心的活性。双特异性抗体毒性：TCE双特异性抗体具有相似的不良反应，因为它们使用通过T细胞活化杀死靶细胞的共同抗癌机制。毒性水平与携带TCE双特异性抗体靶点的细胞的总身体负担有些相关。TCE双特异性抗体诱导以发热、不同程度的缺氧、低血压和偶尔多器官衰竭为特征的全身性炎症，统称为细胞因子释放综合征。神经毒性是与TCE双特异性抗体相关的另一种独特不良反应，表现为意识模糊和震颤，以及言语和行为的改变。CRS和神经毒性的病理生理学不完全清楚，可能与细胞因子水平升高有关。接受TCE双特异性抗体治疗的患者需要密切监测，并可能需要使用糖皮质激素或抗细胞因子药物（如IL-6中和抗体托珠单抗）进行免疫抑制。此外，已经实施了几种策略来预防或减少CRS和神经毒性，包括逐渐上调TCE双特异性抗体剂量、预防性使用糖皮质激素，以及在开始TCE双特异性抗体治疗前使用化疗减少肿瘤负荷。受体阻断双特异性抗体不能激活T细胞，因此不会诱导通常在TCE双特异性抗体中观察到的CRS或神经毒性。受体阻断双特异性抗体与单特异性抗体对应物的不良反应相似，例如阿米万他单抗引起的皮疹以及扎尼达他单抗引起的心力衰竭。偶联抗体形式第三种主要格式涉及与毒性载荷连接的抗体，例如细胞毒性药物、细菌或植物毒素，或放射性同位素，这增强了抗体杀死癌细胞的能力。在该组中，ADC是迄今为止使用最广泛的格式，而毒素偶联和放射性同位素偶联抗体尚未被广泛采用。抗体药物偶联物：ADC是通过将肿瘤靶向抗体与细胞毒性药物连接而构建的。ADC分子与细胞表面抗原的结合导致其内化，随后在细胞内释放细胞毒性药物。这使得细胞毒性药物能够选择性地递送至癌细胞，同时保留大部分健康组织。ADC的关键组成部分包括肿瘤靶向抗体、细胞毒性药物和连接抗体与细胞毒性药物的连接子。ADC的成功取决于这些关键组成部分的最佳选择，以及用于将连接子连接到抗体的偶联方法，这通常决定了药物抗体比。大多数ADC使用人源化或人源IgG1作为肿瘤靶向抗体。如上所述，使用IgG1的流行是由于其约21天的长血浆半衰期，以及其结合Fc受体导致通过ADCC和ADCP增强靶细胞杀伤的能力。两种ADC，吉妥珠单抗和奥英妥珠单抗，使用IgG4，其对FcγRII和FcγRIII的亲和力较低，从而限制了ADCP，同时可能由于通过Fc受体非特异性摄取ADC进入免疫细胞减少而降低毒性。大多数连接子将细胞毒性药物连接到IgG1抗体骨架上的随机赖氨酸或半胱氨酸残基。有效的连接子最大限度地减少细胞毒性药物在血流中的早期释放，同时促进活性药物在优选靶向位置的受控释放。连接子大致分为可裂解和不可裂解。多数ADC中使用可裂解连接子，例如肽连接子、腙连接子、二硫键连接子或CL2A连接子。为药物连接开发的第一个连接子之一是使用腙键的可裂解连接子。该连接子用于将抗肿瘤抗生素卡奇霉素连接到ADC吉妥珠单抗和奥英妥珠单抗。腙键被设计为在靶细胞溶酶体内的酸性条件下分解以释放卡奇霉素。然而，腙键可以在血浆中发生水解，导致药物分子意外释放，引起全身毒性。第二种可裂解连接子是肽连接子，需要溶酶体内组织蛋白酶B介导的选择性裂解。四种ADC使用mc-VC-PABC二肽连接子，该连接子由Seagen首次开发用于生成ADC Brentuximab，该ADC使用与微管抑制剂单甲基澳瑞他汀E连接的靶向CD30的抗体。Brentuximab联合化疗在几种不同淋巴瘤亚型的患者中显示出显著疗效，被认为是霍奇金淋巴瘤和CD30+外周T细胞淋巴瘤的标准一线治疗。Brentuximab的成功导致了mc-VC-PABC二肽连接子的广泛采用。Seagen与罗氏、安斯泰来和Genmab合作，使用mc-VC-PABC二肽连接子分别开发靶向CD79B、nectin-4和TF的ADC。第三种可裂解连接子是二硫键连接子，其中连接子裂解由细胞内高浓度的谷胱甘肽介导。具有二硫键连接子的ADC包括mirvetuximab，该药在卵巢癌患者的III期试验中显示出生存获益。与可裂解连接子相比，不可裂解连接子对各种分解机制具有抵抗力。载荷在靶细胞溶酶体内抗体降解后释放。两种ADC，曲妥珠单抗美坦新和belantamab mafodotin，使用不可裂解连接子进行药物连接。临床前研究表明，由于不可裂解连接子的血浆稳定性增加，对非靶细胞的毒性较低。然而，可裂解和不可裂解连接子尚未在临床试验中进行直接比较，一种相对于另一种的优势仍不清楚。肿瘤细胞杀伤过程由连接到肿瘤靶向抗体的细胞毒性药物执行。该药物通常是一种具有高细胞杀伤效力的小分子，通过三种机制之一诱导细胞死亡：直接DNA损伤、破坏微管网络或抑制拓扑异构酶活性。目前使用的药物具有广泛不同的IC₅₀，从5 nM到5 pM。然而，ADC的效力取决于药物的IC₅₀和DAR。因此，具有高效力PBD载荷和相对较低DAR的loncastuximab tesirine与具有较低效力载荷Dxd但相对较高DAR的曲妥珠单抗德鲁替康都能够在几种体内模型中诱导完全肿瘤消退。具有高DAR和新型连接子设计的ADC的益处也在临床试验中观察到。曲妥珠单抗美坦新和曲妥珠单抗德鲁替康共享相同的靶向HER2抗体。然而，曲妥珠单抗美坦新携带通过不可裂解连接子连接的微管抑制剂DM1，而曲妥珠单抗德鲁替康利用通过可裂解连接子连接的药物Dxd。在比较两种ADC的III期试验中，曲妥珠单抗德鲁替康显示出更高的反应率和总生存期。此外，曲妥珠单抗德鲁替康延长了表达低水平HER2的乳腺癌患者的生存期，使其成为第一个对HER2低乳腺癌有效的ADC。最近，fam-trastuzumab deruxtecan在一系列具有高HER2表达的实体瘤中显示出肿瘤消退，并获得了首个FDA批准的肿瘤不可知HER2导向疗法。 ADC毒性：ADC被认为是靶向药物，比传统细胞毒性化疗耐受性更好。然而，大多数患者在使用ADC时会出现某种形式的毒性。大多数ADC共有的毒性包括输注反应、血细胞减少、感染、肝酶升高、胃肠道症状和胚胎-胎儿毒性。某些毒性与特定载荷的使用有关，例如微管抑制剂引起的周围神经病变和卡奇霉素引起的肝毒性。其他毒性在靶向共同抗原的ADC中普遍存在。例如，靶向HER2的ADC可引起心力衰竭并介导间质性肺病。抗体-毒素偶联物或免疫毒素：免疫毒素有两个组成部分，一个靶向抗体或抗体的Fv，以及一个通常来自细菌或植物毒素的细胞毒性蛋白质。靶向抗体或Fv结合靶细胞，允许选择性递送毒素。毒素来自细菌，如假单胞菌外毒素A和白喉毒素，或来自植物，如蓖麻毒素。理论上，任何用于生成ADC的靶向抗体都可用于免疫毒素。然而，尽管过去几年有12种ADC获批，但只有一种免疫毒素莫昔妥莫单抗帕苏多托获得FDA和EMA批准用于治疗毛细胞白血病。莫昔妥莫单抗是一种融合蛋白，将CD22结合的Fv与截短的假单胞菌外毒素A组合，由美国国家癌症研究所的I. Pastan开发。进入靶细胞后，PE38毒素与延伸因子2结合并阻断蛋白质合成。莫昔妥莫单抗在毛细胞白血病患者的临床试验中显示出41%的高完全缓解率，并于2018年获得监管批准。然而，由于临床使用率低，莫昔妥莫单抗的生产于2023年停止。莫昔妥莫单抗和其他研究中的免疫毒素面临若干挑战，包括导致治疗效果丧失的高免疫原性，以及导致毛细血管渗漏综合征和溶血性尿毒症综合征等毒性的狭窄治疗窗。莫昔妥莫单抗采用率低也可能是因为给药的复杂性，包括毒性预防、治疗前和治疗后水化、需要安全监测以避免不良反应以及毛细胞白血病替代疗法的可用性。尽管过去有几项临床试验评估了靶向BCMA、间皮素和其他癌症相关抗原的免疫毒素的疗效，但目前没有一种处于监管审查阶段，也没有预计在不久的将来获得批准。抗体-放射性同位素偶联物：抗体-放射性同位素偶联物由与放射性同位素连接的靶向抗体组成。放射性同位素发射α粒子或β粒子，导致靶细胞中的DNA链断裂，从而导致细胞死亡。抗体-放射性同位素偶联物不需要内化即可诱导细胞死亡，这提供了相对于ADC和免疫毒素的独特优势，包括旁观者效应。α粒子是大的带正电粒子，由两个质子和两个中子组成，有效范围相对较短。相比之下，β粒子是小的带负电电子，有效范围更长，但DNA损伤能量较低。β粒子发射体的例子包括碘-131、镥-177和钇-90。两种FDA和/或EMA批准的抗体-放射性同位素偶联物，⁹⁰Y-替伊莫单抗和¹³¹I-托西莫单抗，将β粒子发射放射性核素连接到靶向CD20的抗体上，用于治疗B细胞淋巴瘤。⁹⁰Y-替伊莫单抗和¹³¹I-托西莫单抗在临床试验中显示出65-80%的总体反应率和20-30%的完全反应率。两项研究都观察到一些可预测的治疗相关不良反应，包括健康骨髓暴露于辐射导致的长期和严重血细胞减少、¹³¹I-托西莫单抗中放射性碘导致的甲状腺功能减退，以及继发性恶性肿瘤，如骨髓增生异常综合征和白血病。尽管反应率高，但这些药物并未实现广泛的临床应用，2012年只有75名患者接受了¹³¹I-托西莫单抗。结果，¹³¹I-托西莫单抗于2013年自愿撤市。⁹⁰Y-替伊莫单抗仍可用于复发或难治性低级别B细胞淋巴瘤患者，但报告表明只有少数患者接受这种治疗。批准数量有限和临床采用率低可能是因为需要多学科团队来开发和在临床部署这些分子。很少有中心具备这种能力，因此，抗体-放射性同位素偶联物的使用落后于ADC。 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三、挑战与未来展望肿瘤学药物开发是一个艰巨的过程，成功率为3-7%。缺乏针对肿瘤学基于抗体的治疗剂成功率的具体数据，但进入I期试验的治疗性抗体中约有18%会进入药物上市阶段。这些低数字反映了药物开发过程中遇到的许多障碍。治疗性抗体开发是一项资源密集的多步骤操作。它需要生成针对靶抗原的多种抗体，然后选择少数具有理想结合和生物物理特性的先导候选物。然后使用小鼠模型在体内测试先导抗体的疗效，使用非人灵长类动物测试毒性和药代动力学，然后进行首次人体临床试验。多种在小鼠模型中显示出有前景疗效的抗体由于在非人灵长类动物或首次人体试验中的毒性而未能进入临床开发。尽管存在这些障碍，但一些抗体正在显示出鼓舞人心的临床前和临床数据，并可能在未来几年改变患者护理。新靶点：实体瘤占新发癌症患者的大多数。很大比例的实体瘤患者出现需要全身治疗的转移性疾病，而这很少能治愈。因此，转移性肺癌、结肠癌、胰腺癌、乳腺癌、前列腺癌、肝癌和胆管癌共同导致了大多数癌症死亡。然而，与血液系统恶性肿瘤相比，针对实体瘤的抗体开发滞后，主要是由于缺乏可靶向的抗原。不同的淋巴瘤亚型约占所有癌症死亡的3%，但有五个肿瘤抗原被治疗性抗体靶向。相比之下，导致约21%癌症死亡的肺癌只有一个可靶向的肿瘤抗原。此外，胰腺癌、前列腺癌和脑癌完全缺乏FDA和/或EMA批准的治疗性抗体。这种差异主要是因为淋巴瘤和骨髓瘤起源于正常的B细胞，后者表达独特的可靶向抗原。此外，根除正常B细胞不会导致不可耐受的后果。不幸的是，靶抗原发现在实体瘤中产生的线索很少。因此，新靶点的识别可能需要涉及对大量患者样本进行单细胞测序，以寻找在癌症和正常组织中差异表达的抗原。此外，最近的临床试验显示，靶向claudins、HER3、FGFR2B、DLL3、CTGF和STEAP1的抗体显示出令人鼓舞的结果。最后，规避缺乏肿瘤特异性抗原的一种创新方法是组合靶向多种抗原。大多数癌症缺乏在健康组织中不存在的真正特异性抗原的表达。因此，靶向仅在肿瘤中共表达而在健康组织中不共表达的抗原组合可能提供可行的治疗途径。利用需要两个或三个靶点激活细胞毒性机制的布尔逻辑AND门的临床前研究已证明肿瘤消退，但它们尚未在临床试验中进行测试。一些细胞表面蛋白聚糖，如硫酸软骨素和硫酸乙酰肝素，是癌症和其他人类疾病中信号通路的重要调节剂。硫酸软骨素蛋白聚糖已被证明可促进肿瘤血管化并调节与肿瘤生长相关的信号转导通路，并且在多种癌症类型中表达。Glypicans是糖基磷脂酰肌醇锚定的细胞表面HSPG。几种glypicans如GPC1、GPC2和GPC3在癌症中过表达，表明它们是潜在的肿瘤相关抗原。针对GPC1、GPC2和GPC3的抗体和CAR T细胞已分别开发用于治疗胰腺癌、神经母细胞瘤和肝癌。肿瘤特异性抗原：目前大多数获批的基于抗体的治疗剂靶向肿瘤相关抗原或组织特异性抗原。肿瘤相关抗原，如HER2，由癌细胞过表达，但也由一部分正常组织表达，尽管水平较低。癌症和正常组织之间表达水平的差异提供了治疗窗口。组织特异性抗原，如CD20，在癌细胞和正常细胞中以相似的水平表达。靶向此类组织特异性抗原的疗法旨在消除正常细胞和癌细胞，因为正常B细胞的耗竭在临床上是可耐受的。靶向CD19、CD20、CD38和BCMA的B细胞谱系癌症疗法代表了最成功的组织特异性治疗性抗体实例。肿瘤特异性抗原的主要例子是新抗原，这些是由MHC分子呈递的突变肽。突变肽是携带氨基酸变化的蛋白质的短蛋白水解产物，这些变化源于突变，这是癌细胞的标志。来自突变癌症驱动基因（如BRAF、RAS、PIK3CA、TP53和异柠檬酸脱氢酶）的公共新抗原提供了对癌细胞极为独特的靶点，可用于造福患者。这些公共新抗原目前正被双特异性抗体靶向，并在临床前研究中显示出针对携带TP53和RAS突变的癌症的令人鼓舞的活性。细胞内抗原：抗体无法穿透细胞膜，因此只能靶向细胞表面抗原。细胞内抗原可以与MHC分子结合呈递在细胞表面，使其可靶向。通过这种方式，tebentafusp靶向细胞内抗原gp100，该抗原在黑色素瘤中过表达，并与HLA-A*02:01结合呈递在细胞表面。现在正在开发抗体以靶向类似癌症特异性过表达的细胞内蛋白，如hTERT、MUC1、NY-ESO1、TARP、p53、WT1和PRAME，其中靶向PRAME在临床试验中显示出令人鼓舞的初步结果。肿瘤微环境中的抗原：癌症在复杂的免疫细胞、成纤维细胞和细胞外基质混合物中发展，这被称为肿瘤微环境。目前的研究正在检查肿瘤微环境中免疫细胞的作用，如肿瘤相关巨噬细胞、树突状细胞和髓源性抑制细胞，这些细胞已知会驱动对免疫检查点抑制剂的耐药性。因此，耗竭或阻断这些免疫抑制细胞的功能可能使肿瘤对免疫检查点抑制剂敏感。早期临床试验证明了通过靶向CSF1R、TREM1和TREM2进行抗体介导的TAM抑制的安全性和可行性。临床前研究还表明，使用激动性CD40单克隆抗体增强肿瘤微环境中树突状细胞的功能可以增强T细胞介导的肿瘤消退。所有对抗肿瘤微环境内免疫抑制状态的抗体目前正在II/III期试验中进行测试，这将决定它们的最终效用。靶向低密度抗原：目前批准的ADC和双特异性抗体靶向相对丰富的抗原，如CD19、CD20和BCMA，每个癌细胞约有1,000至50,000个拷贝。靶向新抗原的主要挑战源于它们在癌细胞表面的低丰度，一些细胞表达1-10个靶抗原拷贝。除了新抗原外，有效靶向肿瘤相关或组织特异性抗原也可能受到其可变细胞表面密度的影响。此外，治疗压力也可以选择具有低靶抗原表达的癌细胞克隆。临床前研究表明，双特异性抗体能够杀死每个细胞表达低至1-10个抗原的癌细胞，而ADC需要1,000个或以上的拷贝才能杀死细胞。未修饰的全长抗体可能需要更高的靶抗原表达。靶向此类低密度抗原仍然是一个挑战，优化的抗体工程正在使其在临床前研究中有效靶向个位数水平的新抗原成为可能。新型免疫检查点抑制剂：伊匹木单抗在2011年的批准迎来了免疫治疗时代。免疫检查点阻断剂具有前所未有的能力，可以在一些复发性实体瘤患者中诱导长期缓解，这导致了一系列临床试验的激增。FDA和EMA已批准11种不同版本的靶向CTLA4、PD1和PDL1的抗体，用于超过20种癌症类型的超过65种不同适应症。在CTLA4、PD1和PDL1靶向取得初步成功后，一系列额外的免疫检查点被探索，以诱导一系列癌症类型的缓解。除了在黑色素瘤中靶向LAG3的瑞拉利单抗外，其他所有药物尚未在III期试验中证明获得监管批准所需的治疗活性。类似地，阻断CD47的巨噬细胞检查点抑制剂magrolimab在早期试验中显示出令人鼓舞的活性，但由于缺乏疗效，在MDS和AML患者中的III期试验被终止。目前新型免疫检查点阻断剂的表现低于预期，导致制药行业将重点放在PD1-PDL1领域。新型抗体格式：所有全长治疗性抗体都使用IgG同种型。临床前研究和早期试验正在探索五聚体IgM格式，与IgG格式中的两个结合位点相比，它具有十个抗原结合位点。与靶向相同表位的IgG抗体相比，这提供了更高的结合亲合力。一个例子是IGM-8444，一种高亲合力五聚体IgM激动抗体，靶向死亡受体5，该抗体已在小鼠模型中显示出肿瘤消退，并已进入I期试验。新型双特异性格式：TCE双特异性格式通过提高疗效同时减少不良反应而不断发展。目前有超过200种双特异性抗体处于临床开发阶段，其中大多数使用TCE方法靶向实体瘤。Glofitamab和xaluritamig在临床试验中均显示出疗效，并共享独特的2:1 T细胞衔接双特异性格式，具有对靶点的二价结合和对CD3的单价结合。与传统的1:1靶点与CD3结合设计相比，这种格式可能提供更高的肿瘤细胞杀伤能力。IgM格式TCE双特异性抗体由于使用五聚体IgM而具有更令人印象深刻的10:1靶点与CD3结合比。高靶点与CD3结合比设计允许高亲合力靶点结合，可能产生更高的靶点细胞毒性，同时减少细胞因子分泌。Imvotamab的I期试验已证明在晚期B细胞恶性肿瘤患者中具有几个完全缓解。双特异性免疫检查点阻断剂：双特异性格式也被用于同时抑制两个免疫检查点，以增强T细胞活化，超越两种单特异性免疫检查点阻断剂组合所能达到的效果。靶向PD1xLAG3、PD1xCTLA4和PDL1xCTLA4的双特异性免疫检查点阻断剂在早期临床试验中显示出令人鼓舞的疗效。虽然最初的双特异性免疫检查点阻断剂组专注于抑制临床已确立的免疫检查点，但临床前研究正在调查类似的双特异性免疫检查点阻断剂是否可以通过靶向新型免疫受体来诱导抗肿瘤免疫。三特异性抗体：三特异性抗体具有同时与三种不同抗原相互作用的能力。这种功能使三特异性抗体能够与两种不同的癌症相关抗原相互作用，同时在B细胞恶性肿瘤的背景下使用第三个结合域与细胞毒性T细胞结合。这种创新方法有助于减轻由于单一抗原丢失而引起的治疗耐药性，因为癌细胞必须同时下调两种抗原以逃避杀伤。或者，三特异性抗体被设计为与两个T细胞受体相互作用，从而向癌细胞传递更有效的激活信号。纳米抗体：可能导致抗体工程重要范式变化的一个研究领域是单域抗体的开发。纳米抗体主要来源于骆驼科重链抗体，体积小，易于生产，稳定，并且能够穿透肿瘤或病毒抗原中的隐藏位点。纳米抗体通常从骆驼科来源的噬菌体展示文库中分离，最近也从转基因小鼠中分离。纳米抗体具有长的CDR3环，可以穿透抗原表面的空腔。第一个基于纳米抗体的靶向BCMA的CAR T细胞已获得FDA批准，并且与基于抗体的CAR T细胞相比显示出更高的疗效。靶向CD19或CD20和HER2的纳米抗体来源药物目前正在淋巴瘤和乳腺癌患者的临床试验中进行测试。纳米抗体是否会提供比当前基于抗体的药物更高的疗效仍有待观察。可激活抗体：肿瘤微环境通常表现出较低的pH，含有活性蛋白酶酶，并具有正常组织缺乏的特定抗原组合。这些独特的特性被用来选择性地靶向癌细胞，使用可激活抗体，这些抗体根据环境条件的变化获得或失去功能。在抗体序列的某些位置添加组氨酸残基使其能够与靶抗原进行pH依赖性结合。具有这种掩蔽机制的抗体通常被称为前体药物疗法，正被用于改善PDL1、CTLA4、EGFR、CD166和CD71在一系列实体瘤和血液系统恶性肿瘤中的靶向。新型偶联抗体：调节连接子设计和增加DAR可能会增强治疗益处。例如，具有高DAR的靶向细胞表面糖蛋白TROP2的ADC是第一个改善三阴性乳腺癌患者生存期的ADC。第一三共开发的创新四肽连接子用于曲妥珠单抗德鲁替康，掩盖了载荷DXd的疏水性，并允许均匀连接大量药物，同时保持良好的药代动力学并最大限度地减少药物在血浆中的过早释放。这种连接子-载荷组合现在正被几种接近批准或处于临床试验阶段的ADC采用。最后，新型药物载荷，如蛋白质降解剂、RNA聚合酶抑制剂、BCL-xL抑制剂、Toll样受体激动剂和干扰素基因刺激剂激动剂，预计将通过使用新型杀伤机制来改进ADC。免疫毒素偶联物：免疫毒素的一个明显限制是抗毒素免疫反应的产生，这会缩短半衰期并降低疗效。目前的工作重点是去除被宿主免疫细胞识别的表位，以降低假单胞菌外毒素的免疫原性。这种修饰的免疫毒素可能会提高疗效，并允许免疫毒素靶向一系列恶性肿瘤。白介素-毒素偶联物的生成是该领域的另一项发展，并利用了癌细胞中白介素受体的过表达。Tagraxofusp是一种靶向IL3RA的细胞毒素，由IL-3与白喉毒素融合而成，在母细胞性浆细胞样树突状细胞肿瘤患者中显示出有效性。类似地，denileukin diftitox是一种IL-2R靶向细胞毒素，由IL-2与白喉毒素融合而成，在皮肤T细胞淋巴瘤患者中有效。然而，这些IL-毒素偶联物不被视为基于抗体的药物，因为它们使用受体配体而非scFv进行肿瘤靶向。放射性同位素偶联物：在基于小分子和肽的放射性同位素偶联物在实体瘤中取得成功后，人们对放射性同位素偶联物重新产生了一些兴趣。将镥-177与结合前列腺特异性膜抗原的小分子或与结合生长抑素受体的肽类似物偶联，分别在前列腺癌和神经内分泌肿瘤患者中显示出显著的肿瘤消退，从而获得FDA批准。此类肿瘤靶向小分子-放射性同位素或肽-放射性同位素偶联物的行为类似于抗体-放射性同位素偶联物，但具有不同的结构和药代动力学。 -05- 结语总之，基于抗体的治疗剂因其抗体与靶点结合所能提供的精确水平而在肿瘤学领域具有巨大前景。主要挑战仍然存在，但新靶点和各种新颖的设计和工程策略有望为许多这些挑战提供解决方案。获得监管批准的更有效的基于抗体的治疗剂的爆炸式增长可能会延续过去二十五年显示的趋势。参考文献： Cancer therapy with antibodies. Nat Rev Cancer. 2024 Jun;24(6):399-426. 公众号已建立“小药说药专业交流群”微信行业交流群以及读者交流群，扫描下方小编二维码加入，入行业群请主动告知姓名、工作单位和职务。

2026-04-02

·BioSpace

Adagene Reports Full Year 2025 Financial Results and Provides Corporate Update

In 2025, muzastotug showed 29% confirmed overall response rate (ORR) among 21 patients with MSS CRC in the 20 mg/kg dose cohorts Median overall survival (OS) for the 10 mg/kg cohorts was 19.4 months, with a median follow-up of 17.8 months 4% overall discontinuation rate, no dose limiting toxicities, and no Grade 4 or 5 treatment-related adverse events (TRAEs) across 67 patients in all dose cohorts supports improved tolerability pro muzastotug Randomized Phase 2 trial enrollment ahead of plan, with potential updates in 2026 and results expected in 1H 2027; registration trial expected to begin once optimal dose regimen has been established Cash and cash equivalents of $74.5 million as of December 31, 2025, plus proceeds raised from the ATM Offering in 2026 year-to-date, anticipated to provide cash runway into early 2028 SAN DIEGO, Calif. and SUZHOU, China, April 01, 2026 (GLOBE NEWSWIRE) -- Adagene Inc. (“Adagene”) (Nasdaq: ADAG), a platform-driven, clinical-stage biotechnology company transforming the discovery and development of novel anti-body-based therapies, today reported financial results for the full year 2025 and provided corporate updates. “Our clinical data for muzastotug plus pembrolizumab consistently demonstrate potent, dose-dependent efficacy,” said Peter Luo, Ph.D., Chairman and President of R&D at Adagene. “The 10 mg/kg data reported at ASCO have now matured into the classic long survival tail of CTLA-4 inhibition. By significantly mitigating severe toxicities, patients remain on therapy longer, allowing CTLA-4-mediated intratumoral Treg depletion, alongside PD-1-mediated reinvigoration and CTLA-4-mediated priming of effector T cells, to drive durable disease control. Importantly, these data provide a clear, de-risked read-through to the 20 mg/kg dose, which already shows an encouraging 29% ORR with median duration of response not yet reached. “Supported by Fast Track Designation and FDA alignment under Project Optimus, we are on track to finalize the optimal combination dose regimen for a potential MSS colorectal cancer registrational trial. The expanded therapeutic window also helps to establish muzastotug as a foundational combination backbone. At AACR, we will showcase this potential with data from triplet regimens—combining with fruquintinib in 3L+ MSS CRC, alongside results from the Morpheus Liver study evaluating a triplet of muzastotug, atezolizumab, and bevacizumab versus atezolizumab and bevacizumab alone in first-line HCC. These readouts underscore our ability to safely unlock deeper responses in hard-to-treat tumors.” 2026 OBJECTIVES & CASH RUNWAY INTO EARLY 2028 Data update from the ongoing Phase 1b/2 study of muzastotug in combination with Merck’s (known as MSD outside of the United States and Canada) anti-PD-1 therapy, KEYTRUDA ® (pembrolizumab) in 3L+ MSS CRC, including 41 patients in the 10 mg/kg cohorts and 26 patients in the 20 mg/kg cohorts Complete enrollment of the ongoing randomized Phase 2 dose-optimization study with muzastotug, which is being conducted in alignment with FDA Project Optimus, and designed to allow dose regimen selection for Phase 3. Provide preliminary clinical data, including pathological responses, to inform future development from investigator-initiated Phase 2 trial for neoadjuvant muzastotug + pembrolizumab in colorectal cancer. Provide initial clinical data from a new cohort of patients in the ongoing Phase 1b/2 study of muzastotug + pembrolizumab in combination with standard of care (fruquintinib) in MSS CRC patients. Share results of the clinical trial collaboration with Roche, which evaluates muzastotug in triplet combination with atezolizumab and bevacizumab in first-line treatment of locally advanced or metastatic hepatocellular carcinoma (HCC; liver cancer). Establish additional collaboration/licensing agreements. With cash and cash equivalents of $74.5 million as of December 31, 2025, plus proceeds raised from the ATM Offering in 2026 year-to-date, Company expects a cash runway extending into early 2028. PIPELINE HIGHLIGHTS ADG126- Phase 1b/2 data: As presented at ASCO 2025, muzastotug showed 29% (6/21) confirmed overall response rate (ORR) in the combined 20 mg/kg dose cohorts. Among 41 patients in the combined 10mg/kg dose cohorts, median overall survival (mOS) was 19.4 months with a 17.8-month median follow-up, which compares favorably to 11-12 month mOS from fruquintinib Phase 3 trials in the same population 1 Across 67 patients in all cohorts, a low 4% overall discontinuation rate, no dose limiting toxicities, and no Grade 4 or 5 treatment-related adverse events (TRAEs); Grade 3 TRAEs were 15% in the 10 mg/kg cohorts and 27% in the 20 mg/kg cohorts, which were generally transient and manageable. Updated data demonstrate the durability of response and further support the optimized therapeutic index pro muzastotug, which overcomes well-known dose-limiting toxicities of other CTLA-4 inhibitors at 10-20-fold higher doses 2 , to provide potentially improved efficacy. Randomized Phase 2 trial enrollment ongoing, with results expected in 1H 2027; registration trial expected to begin once optimal dose regimen has been established AMERICAN ASSOCIATION FOR CANCER RESEARCH 2026 PRESENTATIONS The following abstracts have been selected for presentation at AACR 2026: 1) Title: Ph1b evaluation of ADG126 (muzastotug, an anti-CTLA-4 masking antibody) pembrolizumab (Pembro) IO doublet in combination with fruquintinib (Fruq) in advanced and metastatic microsatellite stable colorectal cancer This poster will provide initial clinical data from a new cohort of patients in the ongoing Phase 1b/2 study of muzastotug + pembrolizumab in combination with standard of care (fruquintinib) in MSS CRC patients. 2) Title: Results from the phase 1b/2 Morpheus Liver study in patients with unresectable locally advanced or metastatic hepatocellular carcinoma (HCC): Muzastotug (ADG126: masked anti-CTLA-4 Ab) combination arm This poster will share results of the clinical trial collaboration with Roche, which evaluates muzastotug in triplet combination with atezolizumab and bevacizumab in first-line treatment of liver cancer. 3) Title: Preclinical characterization of XB404, a masked anti-ROR1/2 antibody-drug conjugate Partner Exelixis will present preclinical data from antibody-drug conjugate, XB404, built with Adagene’s SAFEbody masking technology and designed to deliver a cytotoxic payload to ROR1/2-expressing tumors while minimizing on-target, off-tumor side effects. ONGOING COLLABORATIONS Sanofi: Invested up to $25 million to support muzastotug’s randomized Phase 2 study. Separately, Adagene will supply Sanofi with muzastotug to evaluate the safety, efficacy, pharmacokinetics and biomarker data in combination with Sanofi’s SAR445877 (PD-1 x IL-15 fusion protein) in over 100 patients in a Phase 1/2 clinical trial in advanced solid tumors. Sanofi also exercised its option for a third SAFEbody® discovery program. Third Arc Bio: Partnered to develop two masked CD3 T cell engagers, expanding SAFEbody® into next-generation T cell therapies. Exelixis: Advanced a third masked ADC against a solid tumor target, building on the 2021 collaboration. ConjugateBio: Collaborated on bispecific ADCs using Adagene-derived antibody, further demonstrating scalable platform potential. Roche: Roche is sponsoring and conducting a phase 1b/2 multi-national trial to evaluate ADG126 in a triple combination with atezolizumab and bevacizumab in first-line hepatocellular carcinoma (HCC). FINANCIAL HIGHLIGHTS Cash and Cash Equivalents: Cash and cash equivalents were US$74.5 million as of December 31, 2025, compared to US$85.2 million as of December 31, 2024. Total borrowings from commercial banks in China (denominated in RMB) decreased to US$6.1 million as of December 31, 2025 from US$18.2 million as of December 31, 2024. The associated loan proceeds were primarily used to pay for the company’s R&D activities in China. Net Revenue: Net revenue was US$7.7 million for the year ended December 31, 2025, compared to US$0.1 million in 2024. The increase of approximately 7,333% reflects net revenue recognized upon fulfillment of certain performance obligations associated with the collaboration and technology licensing agreements with Sanofi, ConjugateBio and Third Arc Bio, respectively. Research and Development (R&D) Expenses: R&D expenses were US$22.0 million for the year ended December 31, 2025, compared to US$28.8 million in 2024. The decrease of approximately 23% in R&D expenses reflects clinical focus on and prioritization of the company’s masked, anti-CTLA-4 SAFEbody ADG126. Administrative Expenses: Administrative expenses were US$7.1 million for the year ended December 31, 2025, compared to US$7.3 million in 2024. The decrease was mainly a result of cost-control measures. Net Loss: Net loss attributable to Adagene Inc.’s shareholders was US$17.6 million for the year ended December 31, 2025, compared to US$33.4 million in 2024. Ordinary Shares Outstanding: As of December 31, 2025, there were 59,231,993 ordinary shares issued and outstanding. Each American depository share, or ADS, represents one and one quarter (1.25) ordinary shares of the company. Non-GAAP Net Loss: Non-GAAP net loss, which is defined as net loss attributable to ordinary shareholders for the period after excluding share-based compensation expenses, was US$13.9 million for the year ended December 31, 2025, compared to US$28.5 million in 2024. Please refer to the section in this press release titled “Reconciliation of GAAP and Non-GAAP Results” for details. Non-GAAP Financial Measures: The company uses non-GAAP net loss and non-GAAP net loss per ordinary shares for the year, which are non-GAAP financial measures, in evaluating its operating results and for financial and operational decision-making purposes. The company believes that non-GAAP net loss and non-GAAP net loss per ordinary shares for the year help identify underlying trends in the company’s business that could otherwise be distorted by the effect of certain expenses that the company includes in its loss for the year. The company believes that non-GAAP net loss and non-GAAP net loss per ordinary shares for the year provide useful information about its results of operations, enhances the overall understanding of its past performance and future prospects and allows for greater visibility with respect to key metrics used by its management in its financial and operational decision-making. Non-GAAP net loss and non-GAAP net loss per ordinary shares for the year should not be considered in isolation or construed as an alternative to operating profit, loss for the year or any other measure of performance or as an indicator of its operating performance. Investors are encouraged to review non-GAAP net loss and non-GAAP net loss per ordinary shares for the year and the reconciliation to their most directly comparable GAAP measures. Non-GAAP net loss and non-GAAP net loss per ordinary shares for the year here may not be comparable to similarly titled measures presented by other companies. Other companies may calculate similarly titled measures differently, limiting their usefulness as comparative measures to the company’s data. The company encourages investors and others to review its financial information in its entirety and not rely on a single financial measure. Non-GAAP net loss and non-GAAP net loss per ordinary shares for the year represent net loss attributable to ordinary shareholders for the year excluding share-based compensation expenses. Share-based compensation expense is a non-cash expense arising from the grant of stock-based awards to employees. The company believes that the exclusion of share-based compensation expenses from the net loss in the Reconciliation of GAAP and Non-GAAP Results assists management and investors in making meaningful period-to-period comparisons in the company's operating performance or peer group comparisons because (i) the amount of share-based compensation expenses in any specific period may not directly correlate to the company’s underlying performance, (ii) such expenses can vary significantly between periods as a result of the timing of grants of new stock-based awards, and (iii) other companies may use different forms of employee compensation or different valuation methodologies for their share-based compensation. Please see the “Reconciliation of GAAP and Non-GAAP Results” included in this press release for a full reconciliation of non-GAAP net loss and non-GAAP net loss per ordinary shares for the year to net loss attributable to ordinary shareholders for the year/period. 1 Qin S, Xu RH, Shen L, Et Al. Subgroup Analysis By Liver Metastasis In The FRESCO Trial Comparing Fruquintinib Versus Placebo Plus Best Supportive Care In Chinese Patients With Metastatic Colorectal Cancer. Onco Targets Ther. 2021;14:4439-; Garcia-Carbonero R, Dasari NA, Eng C, et al. 520P Efficacy and safety of fruquintinib in patients with refractory metastatic colorectal cancer with and without liver metastasis: A subgroup analysis of the phase III FRESCO-2 trial. Ann Onc 2024;35:S439 2 (i) CheckMate 511 (Phase IIIb/IV): This study compared nivolumab 3 mg/kg plus ipilimumab 1 mg/kg Q3W × 4 versus the standard nivolumab 1 mg/kg plus ipilimumab 3 mg/kg Q3W × 4 in patients with advanced melanoma. The trial demonstrated similar efficacy with a significantly lower incidence of Grade 3–5 treatment-related adverse events (34% vs. 48%); and (ii) Lebbé C, et al. (2019). Evaluation of two dosing regimens for nivolumab in combination with ipilimumab in patients with advanced melanoma: Results from the Phase IIIb/IV CheckMate 511 trial. Journal of Clinical Oncology, 37(11):867–875. About Adagene Adagene Inc. (Nasdaq: ADAG) is a platform-driven, clinical-stage biotechnology company committed to transforming the discovery and development of novel antibody-based cancer immunotherapies. Adagene combines computational biology and artificial intelligence to design novel antibodies that address globally unmet patient needs. The company has forged strategic collaborations with reputable global partners that leverage its SAFEbody precision masking technology in multiple approaches at the vanguard of science. Powered by its proprietary Dynamic Precision Library (DPL) platform, composed of NEObody™, SAFEbody, and POWERbody™ technologies, Adagene’s highly differentiated pipeline features novel immunotherapy programs. The company’s SAFEbody technology is designed to address safety and tolerability challenges associated with many antibody therapeutics by using precision masking technology to shield the binding domain of the biologic therapy. Through activation in the tumor microenvironment, this allows for tumor-specific targeting of antibodies, while minimizing on-target off-tumor toxicity in healthy tissues. Adagene’s lead clinical program, muzastotug (ADG126), is a masked, anti-CTLA-4 SAFEbody with FDA Fast Track designation that targets a unique epitope of CTLA-4 in regulatory T cells (Tregs) in the tumor microenvironment. Muzastotug is currently in Phase 1b/2 and Phase 2 clinical studies in combination with anti-PD-1 therapy, particularly focused on microsatellite stable (MSS) metastatic colorectal cancer (CRC). Validated by ongoing clinical research, the SAFEbody platform can be applied to a wide variety of antibody-based therapeutic modalities, including Fc empowered antibodies, antibody-drug conjugates, and bi/multi-specific T-cell engagers. For more information, please visit: Follow Adagene on WeChat, LinkedIn and X. SAFEbody® is a registered trademark in the United States, China, Australia, Japan, Singapore, and the European Union. KEYTRUDA® is a registered trademark of Merck Sharp & Dohme LLC, a subsidiary of Merck & Co., Inc., Rahway, NJ, USA.. Safe Harbor Statement This press release contains forward-looking statements, including statements regarding certain clinical results of ADG126, the potential implications of clinical data for patients, and Adagene’s advancement of, and anticipated preclinical activities, clinical development, regulatory milestones, and commercialization of its product candidates. Actual results may differ materially from those indicated in the forward-looking statements as a result of various important factors, including but not limited to Adagene’s ability to demonstrate the safety and efficacy of its drug candidates; the clinical results for its drug candidates, which may not support further development or regulatory approval; the content and timing of decisions made by the relevant regulatory authorities regarding regulatory approval of Adagene’s drug candidates; Adagene’s ability to achieve commercial success for its drug candidates, if approved; Adagene’s ability to obtain and maintain protection of intellectual property for its technology and drugs; Adagene’s reliance on third parties to conduct drug development, manufacturing and other services; Adagene’s limited operating history and Adagene’s ability to obtain additional funding for operations and to complete the development and commercialization of its drug candidates; Adagene’s ability to enter into additional collaboration agreements beyond its existing strategic partnerships or collaborations, and the impact of the COVID-19 pandemic on Adagene’s clinical development, commercial and other operations, as well as those risks more fully discussed in the “Risk Factors” section in Adagene’s filings with the U.S. Securities and Exchange Commission. All forward-looking statements are based on information currently available to Adagene, and Adagene undertakes no obligation to publicly update or revise any forward-looking statements, whether as a result of new information, future events or otherwise, except as may be required by law. Investor Contacts: Raymond Tam Raymond_tam@adagene.com Corey Davis LifeSci Advisors cdavis@lifesciadvisors.com Media: Lindsay Rocco Elixir Health Public Relations 1-862-596-1304 lrocco@elixirhealthpr.com Unaudited Consolidated Balance Sheets December 31, 2024 December 31, 2025 US$ US$ ASSETS Current assets: Cash and cash equivalents 85,194,502 74,523,782 Amounts due from related parties 8,309 17,349 Prepayments and other current assets 2,575,194 2,834,034 Total current assets 87,778,005 77,375,165 Property, equipment and software, net 1,125,389 717,374 Operating lease right-of-use assets 283,645 145,535 Other non-current assets 81,386 25,223 TOTAL ASSETS 89,268,425 78,263,297 LIABILITIES AND SHAREHOLDERS’ EQUITY Current liabilities: Accounts payable 4,241,773 2,884,507 Contract liabilities — 3,462,683 Amounts due to related parties 13,187,966 10,347,200 Accruals and other current liabilities 2,816,038 2,790,794 Income tax payable 5,265 410,198 Warrant liabilities — 205,146 Short-term borrowings 4,868,956 4,268,154 Current portion of long-term borrowings 12,923,599 711,359 Current portion of operating lease liabilities 141,341 92,055 Total current liabilities 38,184,938 25,172,096 Long-term borrowings 417,339 1,138,174 Operating lease liabilities 142,304 53,480 TOTAL LIABILITIES 38,744,581 26,363,750 Commitments and contingencies Mezzanine equity: Series A non-voting contingently redeemable convertible preferred shares (par value of US$0.0001 per share; nil authorized, issued and outstanding as of December 31, 2024; and 1,062,500 shares authorized, issued and outstanding as of December 31, 2025) — 16,550,000 Total mezzanine equity — 16,550,000 Shareholders’ equity: Ordinary shares (par value of US$0.0001 per share; 640,000,000 shares authorized, and 58,886,944 shares issued and outstanding as of December 31, 2024; and 640,000,000 shares authorized, and 59,231,993 shares issued and outstanding as of December 31, 2025) 5,889 5,923 Additional paid-in capital 362,220,445 366,043,455 Accumulated other comprehensive loss (526,903 ) (1,914,831 ) Accumulated deficit (311,175,587 ) (328,785,000 ) Total shareholders’ equity 50,523,844 35,349,547 TOTAL LIABILITIES, MEZZANINE EQUITY AND SHAREHOLDERS’ EQUITY 89,268,425 78,263,297 Unaudited Consolidated Statements of Comprehensive Loss For the Year Ended December 31, 2024 For the Year Ended December 31, 2025 US$ US$ Revenues Licensing and collaboration revenue 103,204 7,670,902 Operating expenses and income Research and development expenses (28,781,412 ) (22,033,573 ) Including external related parties (1,943,523 ) (1,580,387 ) Administrative expenses (7,273,335 ) (7,075,624 ) Loss from operations (35,951,543 ) (21,438,295 ) Interest and investment income 3,801,345 2,303,990 Interest expense (851,874 ) (463,132 ) Other income, net 466,620 323,988 Foreign exchange gain (loss), net (906,212 ) 1,318,235 Change in fair value of warrant liabilities — 47,941 Loss before income tax (33,441,664 ) (17,907,273 ) Income tax benefit 17,553 297,860 Net loss attributable to Adagene Inc.’s shareholders (33,424,111 ) (17,609,413 ) Other comprehensive income (loss) Foreign currency translation adjustments, net of nil tax 1,273,185 (1,387,928 ) Total comprehensive loss attributable to Adagene Inc.’s shareholders (32,150,926 ) (18,997,341 ) Net loss attributable to Adagene Inc.’s shareholders (33,424,111 ) (17,609,413 ) Net loss attributable to ordinary shareholders (33,424,111 ) (17,609,413 ) Weighted average number of ordinary shares used in per share calculation: —Basic 56,287,903 59,006,129 —Diluted 56,287,903 59,006,129 Net loss per ordinary share —Basic (0.59 ) (0.30 ) —Diluted (0.59 ) (0.30 ) Reconciliation of GAAP and Non-GAAP Results For the Year Ended December 31, 2024 For the Year Ended December 31, 2025 US$ US$ GAAP net loss attributable to ordinary shareholders (33,424,111 ) (17,609,413 ) Add back: Share-based compensation expenses 4,909,573 3,741,548 Non-GAAP net loss (28,514,538 ) (13,867,865 ) Weighted average number of ordinary shares used in per share calculation: —Basic 56,287,903 59,006,129 —Diluted 56,287,903 59,006,129 Non-GAAP net loss per ordinary share —Basic (0.51 ) (0.24 ) —Diluted (0.51 ) (0.24 )

临床结果临床2期快速通道

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
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
局部晚期乳腺癌	临床3期	澳大利亚	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

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


GOBLET (AACR2026)	临床1/2期	胰腺癌一线 RAS upregulated	13	Pelareorep + Atezolizumab + Gemcitabine/nab-paclitaxel	艱淵願網襯範廠鏇鏇鹽(顧顧築鏇鏇遞願壓鑰淵) = 願餘觸衊網夢獵淵鑰簾糧衊願蓋網簾鹽餘衊遞 (遞鑰顧繭鏇壓蓋繭淵鹽 ) 更多	积极	2026-04-21
AACR2026	N/A	转移性非小细胞肺癌一线	11,758	Atezolizumab	鑰齋憲鹽醖憲積鬱鹽築(膚鏇鏇壓構選遞糧壓醖) = 壓鹽繭築窪餘糧積獵鹹衊積醖鹹構憲製襯蓋構 (構齋衊糧夢襯鑰範鹹觸 ) 更多	不佳	2026-04-21
				Pembrolizumab	鑰齋憲鹽醖憲積鬱鹽築(膚鏇鏇壓構選遞糧壓醖) = 壓繭範築築憲夢醖淵糧衊積醖鹹構憲製襯蓋構 (構齋衊糧夢襯鑰範鹹觸 ) 更多
IMbrave150 (AACR2026)	N/A	晚期肝细胞癌一线	3,948	Atezolizumab + Bevacizumab	築壓鏇憲網鑰積繭構夢(願鬱顧糧醖鏇顧製顧鹽) = The risk of developing predefined adverse events was similar between regimens with nonsignificant RD 蓋觸觸鹽窪鑰壓範繭選 (網餘網餘鹽範遞夢衊鬱 ) 更多	积极	2026-04-21
				Nivolumab + Ipilimumab
AACR2026	临床2期	PD-L1阳性肺癌 PD-L1 positive	41	SBRT + Atezolizumab + Tiragolumab	醖鬱願夢齋積範廠鏇衊(壓繭顧積願憲艱夢構鏇) = 憲醖顧齋齋餘廠鬱鹹網艱醖壓網淵蓋糧積襯願 (襯鏇憲蓋鬱鏇餘遞齋網, 6.0 ~ NR) 更多	积极	2026-04-20
				SBRT + Atezolizumab + Tiragolumab (PD-L1 high (> 50%))	醖鬱願夢齋積範廠鏇衊(壓繭顧積願憲艱夢構鏇) = 觸鏇簾鏇餘糧鏇選蓋範艱醖壓網淵蓋糧積襯願 (襯鏇憲蓋鬱鏇餘遞齋網 )
IMforte (AACR2026)	临床3期	广泛期小细胞肺癌维持	452	Lurbinectedin plus atezolizumab	遞構選繭鏇窪獵鏇鹽糧(簾網廠衊糧積觸憲齋窪) = 選蓋窪糧艱餘齋蓋齋衊糧顧網繭蓋衊窪獵鏇壓 (艱糧構繭衊願憲獵壓壓 ) 更多	积极	2026-04-20
				Durvalumab	遞構選繭鏇窪獵鏇鹽糧(簾網廠衊糧積觸憲齋窪) = 築壓鹹鏇範範製衊積衊糧顧網繭蓋衊窪獵鏇壓 (艱糧構繭衊願憲獵壓壓 ) 更多
NCT03483012 (Pubmed \| Breast Cancer Res Treat)	临床2期	三阴性乳腺癌 \| 脑转移瘤 ER Negative \| PR Negative \| HER2 Negative	6	Atezolizumab (Stereotactic Radiosurgery)	獵膚壓廠鹽願醖繭憲觸(憲憲遞積醖積襯鏇襯壓) = 鬱襯願範鑰選範餘繭簾醖簾醖衊製夢鑰構襯範 (壓膚鏇壓鑰願顧壓簾顧, 0.95 ~ NA) 更多	不佳	2026-04-01
NCT04637594 (IMAGINE, CTgov)	临床3期	膀胱尿路上皮癌 \| 转移性尿道尿路上皮癌 \| 局部晚期尿路上皮癌 ... 更多	3	Nivolumab+Avelumab+Atezolizumab+Pembrolizumab+Durvalumab (Arm A (Immune Checkpoint Inhibitor))	淵鏇範鹽獵願衊顧鑰餘 = 網鏇網構糧糧憲獵製鑰齋糧窪選網鹹蓋鹽獵鹽 (餘網餘窪壓鏇蓋鑰顧積, 廠選構鹽鑰窪餘鹽窪艱 ~ 積鹽膚齋願壓窪夢壓艱) 更多	-	2026-03-20
				Nivolumab+Avelumab+Atezolizumab+Pembrolizumab+Durvalumab (Arm B (Immune Checkpoint Inhibitor))	淵鏇範鹽獵願衊顧鑰餘 = 蓋鏇願積餘廠繭齋顧選齋糧窪選網鹹蓋鹽獵鹽 (餘網餘窪壓鏇蓋鑰顧積, 窪鹽襯糧願淵壓積鑰鑰 ~ 鑰鏇簾壓餘積膚製窪膚) 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))	齋獵淵積衊觸構網鹹獵 = 範鹹夢製願蓋夢鏇築夢網艱襯壓繭鬱製鏇簾獵 (簾構觸襯鬱範廠構壓糧, 鏇衊糧餘衊淵餘願餘獵 ~ 淵獵齋觸醖選網簾糧膚) 更多	-	2026-03-18
				Nivolumab+Plinabulin+RTX (Phase 1b: RTX + Plinabulin (30 mg/m2, Q4W) + Nivolumab (240 mg, Q2W))	齋獵淵積衊觸構網鹹獵 = 積築鏇鹽範鹽艱網膚築網艱襯壓繭鬱製鏇簾獵 (簾構觸襯鬱範廠構壓糧, 鹹襯構壓夢範鏇窪醖製 ~ 衊鏇廠網淵製範窪鹽衊) 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)	憲鏇衊糧醖積糧鹹餘繭 = 衊網蓋繭鹽遞廠製築艱願艱築積齋淵糧網製淵 (鹹獵鹽蓋鏇鹹廠齋顧範, 獵衊餘壓壓齋齋製蓋築 ~ 製選窪獵醖範觸鬱觸蓋) 更多	-	2026-03-11
				platinum+atezolizumab+tiragolumab (Cohort B: PD-L1 All Comers)	憲鏇衊糧醖積糧鹹餘繭 = 憲範膚顧製構窪憲顧襯願艱築積齋淵糧網製淵 (鹹獵鹽蓋鏇鹹廠齋顧範, 積製淵築築鑰簾鏇壓衊 ~ 蓋憲願繭廠壓餘鹽膚繭) 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	範願膚鬱糧製簾衊襯範(選積糧鹽餘鏇廠鏇襯襯) = 鬱衊構膚鏇齋願範繭觸鑰積廠窪鹹範鏇製膚淵 (鏇憲繭餘繭製獵衊淵糧, 28.5 ~ 44.7) 更多	不佳	2026-03-10
				Concurrent chemoradiation alone	範願膚鬱糧製簾衊襯範(選積糧鹽餘鏇廠鏇襯襯) = 壓製遞鹹網衊廠構顧衊鑰積廠窪鹹範鏇製膚淵 (鏇憲繭餘繭製獵衊淵糧, 28.1 ~ 42.5) 更多