A Phase II, Randomized, Open-label, National, Multicenter Study Evaluating the Efficacy and Safety of the Combination of Atezolizumab and Bevacizumab as Neoadjuvant Plus Adjuvant Treatment in Hepatocellular Carcinoma (ASPIRE)

Study to evaluate the efficacy and safety of the combination of Atezolizumab and Bevacizumab as neoadjuvant plus adjuvant treatment in Hepatocellular Carcinoma.

开始日期2025-11-01

申办/合作机构-

NCT06719973

/ Not yet recruiting临床1期

An Open Label, Multicenter, Phase 1 Study of the PARP1 Inhibitor M9466 in Combination With Carboplatin and Platinum-based Anticancer Therapy (DDRiver 521)

The purpose of this study is to evaluate the safety, tolerability, pharmacokinetics, pharmacodynamic, and preliminary clinical activity of M9466 in combinations with carboplatin in advanced or metastatic refractory solid tumor and with the standard of care (carboplatin, etoposide, and atezolizumab) in treatment-naïve ES-SCLC. The results will support any investigation of carboplatin-based combination anticancer treatments with M9466 as well as the selection of a RP2D of M9466 in combination with carboplatin, etoposide, and atezolizumab for a subsequent ES-SCLC study.

开始日期2025-07-01

申办/合作机构

EMD Serono Research & Development Institute, Inc.

[+1]

NCT06294548

/ Not yet recruiting临床1/2期IIT

A Phase Ib/II, Dose Escalation and Dose Expansion Study of Valemetostat Tosylate (DS-3201b) With Atezolizumab and Bevacizumab in Advanced Hepatocellular Carcinoma (HCC)

This is a phase Ib/II, dose escalation and dose expansion study of valemetostat (DS-3201) with atezolizumab and bevacizumab in patients advanced Hepatocellular carcinoma (HCC) who did not receive prior systemic therapy for advanced HCC.

开始日期2025-06-30

申办/合作机构

The University of Alabama at Birmingham

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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4,553

项与阿替利珠单抗相关的文献（医药）

2025-12-01·CANCER CHEMOTHERAPY AND PHARMACOLOGY

Potential role of endothelial dysfunction in hypertension and proteinuria in patients with hepatocellular carcinoma receiving atezolizumab plus bevacizumab: a pilot prospective observational study

Article

作者: Kudo, Kenzo ; Nihei, Satoru ; Oikawa, Takayoshi ; Saito, Kazuki ; Asaka, Junichi ; Ikeda, Tatsuki ; Asahi, Koichi

PURPOSE:

Bevacizumab, a monoclonal antibody targeting vascular endothelial growth factor (VEGF), is the first-line treatment for patients with unresectable hepatocellular carcinoma (HCC). Its inhibition of VEGF signaling may lead to proteinuria due to endothelial dysfunction but the association between endothelial function and clinical outcomes has not been established. This study aimed to investigate vascular endothelial function in patients with HCC receiving atezolizumab plus bevacizumab, and to assess the correlation between reactive hyperemia index (RHI) and adverse renal outcomes.

METHODS:

This pilot prospective observational study included 20 patients with HCC who received atezolizumab plus bevacizumab. We used reactive hyperemia-peripheral arterial tonometry (RH-PAT) and evaluated vascular endothelial function on the basis of RHI. RHI, blood pressure, and proteinuria were recorded at baseline and at 3 and 6 months after initiation of atezolizumab plus bevacizumab treatment. Statistical analyses were performed to investigate the relationship of RHI to blood pressure and proteinuria.

RESULTS:

Following initiation of atezolizumab plus bevacizumab treatment, systolic blood pressure and urine protein-creatinine ratio increased significantly, and RHI decreased. Patients with borderline or low baseline RHI had a higher incidence of grade ≥ 2 proteinuria than those with normal baseline RHI but not hypertension. A significant inverse correlation was found between RHI and urine protein-creatinine ratio.

CONCLUSION:

Bevacizumab administration may cause endothelial dysfunction in patients with HCC. The vascular endothelial function status before and during atezolizumab plus bevacizumab treatment is associated with the risk of bevacizumab-induced proteinuria.

2025-09-01·CHEMOSPHERE

Optimizing the atrazine degradation in g-C3N4@BiOBr/polyvinylidene fluoride photocatalytic membrane system

Article

作者: Gar Alalm, Mohamed ; Fuoad, Mohram ; Samy, Mahmoud ; Hamdy, Nourhan ; El-Geundi, Mohammad

In this study, g-C₃N₄@BiOBr heterostructure was synthesized at different molar ratios and dispersed into a polyvinylidene fluoride (PVDF) matrix for the photodegradation of atrazine (ATZ, herbicide) under visible light. The investigation of the photocatalytic performance of g-C₃N₄@BiOBr/PVDF membrane under different operating parameters has not been extensively studied in the literature. Thus, this study focused on the optimization of the g-C₃N₄@BiOBr/PVDF membrane degradation system and deep exploration of the degradation mechanism. Various analyses characterized the as-prepared catalysts and membranes, including XRD, TEM, FTIR, EDX, SEM, XPS, and DRS. The g-C₃N₄@BiOBr/PVDF membrane (g-C₃N₄@BiOBr at a mole ratio 1:3) showed the highest photocatalytic activity for ATZ removal among the composite membranes. The response surface methodology (RSM) was used to optimize the operating parameters, exhibiting that pH 3, initial ATZ concentration of 0.5 mg/L, and BiOBr mole ratio of 0.75 were the optimum conditions. The contribution of reactive species to the degradation mechanism was investigated using efficient scavengers, confirming the significant roles of •O₂^- and h⁺ in the reaction process. Furthermore, the as-prepared membrane demonstrated enhanced reusability and stability with an 81 % ATZ removal rate after five cycles. The generated intermediates were identified using liquid chromatography-mass spectroscopy analysis indicating the degradation of ATZ to simpler compounds. The mechanism of the photocatalytic degradation of atrazine by g-C₃N₄@BiOBr/PVDF was further proposed. This study proposes a low-cost, efficient, and stable photocatalytic membrane system that can be executed in real applications.

2025-08-01·WATER RESEARCH

Effects of microplastics on atrazine removal in constructed wetlands: Insight into the response characteristics of microorganisms, enzyme activity, and functional genes

Article

作者: Hu, Zhen ; Wu, Haiming ; Kong, Qiaoping ; Chen, Bo ; Wang, Longmian ; Yuan, Qianyin ; Lian, Jianjun

Constructed wetlands (CWs) technology has been widely used to treat agricultural non-point source pollution. However, knowledge about the impact mechanism and distribution characteristics of microplastics (MPs) on pesticide treatment in CWs is limited. This study employed atrazine (ATZ), a representative pesticide, as a model contaminant, to systematically investigate the impacts of polyethylene microplastics (PE MPs) on the removal of ATZ and nutrients, as well as the enzyme activity and the distribution of functional genes in vertical subsurface-flow CW microcosm. The results showed that compared to the control group (CK), CWs treated with different concentrations of MPs had no significant difference in the removal of ATZ. Moreover, in the second stage (ATZ=400 μg/L), the average removal efficiency of ATZ by CWs containing MPs was slightly higher than that of the CK group. PE MPs reduced the nitrogen removal efficiency of CWs by 1.57 %-3.03 %, but had no significant effect on TP removal. The concentration distribution of PE MPs in the substrate layer exhibited a decreasing trend from top to bottom, and the interception capacity of CWs gradually decreased with time (from 100 % to 97.4 %); When exposed to PE MPs, the activities of enzymes in substrate related to nitrogen metabolism were inhibited; Moreover, the addition of PE MPs in CWs promoted the removal of ATZ by increasing the abundance of ATZ metabolizing bacteria (Hydrogenophaga, Zoogloea, Rhizobium, etc.) and ATZ degradation key genes (atzA and trzN). These results not only provide theoretical support for the practical application of CWs in the treatment of pesticide wastewater, but also provide a theoretical basis for the environmental risk control of pesticide non-point source pollution ecological treatment technology in the presence of MPs.

2,259

项与阿替利珠单抗相关的新闻（医药）

2025-06-13

·摩熵医药

中国临床试验数量再创新高！近六年中国临床试验数据一览

注：本文不构成任何投资意见和建议，以官方/公司公告为准；本文仅作医疗健康相关药物介绍，非治疗方案推荐（若涉及），不代表平台立场。任何文章转载需要得到授权。近年来，中国医药研发领域蓬勃发展，临床试验数量屡创新高。2019至2024年，中国临床试验登记总量从2385项增长至4884项，年复合增长率达15%，新药研发占比过半。化学药和生物制品成为主导力量，肿瘤领域稳居治疗首位，GLP-1R等靶点研发热度显著提升。本文基于摩熵咨询最新发布的《中国临床试验趋势与国际多中心临床展望》研究报告，将梳理近六年中国临床试验的关键数据，为读者展现医药创新的蓬勃态势与未来潜力。012024年中国临床试验登记总量超4800项，新药临床试验占比过半近年来中国新药注册临床试验数量逐年增加，据摩熵医药中国临床试验数据库显示，2019-2024年中国临床试验登记总量由2385项提升至4884项，年复合增长率达15%，其中2023年首次突破4000大关，达4226项，2024年持续增长至4884项，预计将快速突破5000项。按新药临床试验和生物等效性试验（BE试验）分类，2024年新药临床试验数量达2524项，占比约51.68%，BE试验数量为2360项，占比48.32%。截图来源：摩熵咨询《中国临床试验趋势与国际多中心临床展望》报告022024年化学药占55%，生物制品首破千项，中药临床有待突破新药临床试验中，按药物类型化学药、生物制品和中药进行统计，2019-2024年期间化学药临床试验从794项提升至1398项，年复合增长率为12%，生物制品临床试验在2024年首次突破1000项，与化药、生物制品相比，中药临床试验规模尚小。占比来看，我国临床试验以化学药为主，占比保持在55%以上，其次为生物制品，占比约40%。近年各类药物占比情况基本保持一致。截图来源：摩熵咨询《中国临床试验趋势与国际多中心临床展望》报告03临床试验效率稳步提升，Ⅱ期、Ⅲ期临床均超600项，合计占比过半在2024年新药临床试验中，Ⅰ期临床试验首次突破千项，我国新药研发活跃度较高；而Ⅱ期、Ⅲ期临床数量分别达642、654项，临床试验整体效率稳步提升；相比之下，Ⅳ期临床试验规模较小，新药上市后监测力度仍有待提升。占比方面，近年我国Ⅰ期临床试验占比呈下降趋势，2024年占比约40.73%；与此同时，Ⅱ期、Ⅲ期临床则呈现出上升的积极变化，占比分别为25.44%和25.91%。截图来源：摩熵咨询《中国临床试验趋势与国际多中心临床展望》报告04肿瘤为新药研发第一大治疗领域，2024年肿瘤新药临床试验合计超500项2024年化学药新药临床试验主要集中在肿瘤、神经系统、消化与代谢系统以及心血管系统等治疗领域，其中肿瘤领域稳居首位，2024年肿瘤新药临床试验达228项，占比约16.31%。生物制品治疗领域同样以肿瘤为主，达303项，占比约25.06%，其次为消化与代谢系统53项、心血管系统47项。中药新药治疗领域分布与化学药、生物制品略有不同，呼吸系统为第一大治疗领域，占比约14.43%，其次为消化与代谢系统、生殖泌尿、皮肤病等。数据来源：摩熵医药中国临床试验数据05GLP-1R靶点热门度快速提升，2024年临床试验数量达128项，PD-1研发渐趋成熟2024年新药临床热门靶点TOP5依次为GLP-1R、TOP1、HER2、EGFR以及PD-1，其中GLP-1R靶点近年热门程度快速提升，以GLP-1R为靶点的新药临床试验达到128项，代表药物司美格鲁肽、替尔泊肽等获批后在全球市场取得极佳的销售表现。与此同时，PD-1等靶点热度减退，研发趋于成熟，2019-2024年PD-1靶点的新药临床试验合计达402项。数据来源：摩熵医药中国临床试验数据库06前十品种合计开展临床达330项，司美格鲁肽注射液临床试验申办居首司美格鲁肽注射液位居近年新药临床试验申办品种TOP1，该品种合计开展临床试验数量达52项，其中Ⅰ期达20项，Ⅲ期达31项。作为热门研发品种，以司美格鲁肽为代表的GLP-1药物行业竞争预计将持续加剧。此外，贝伐珠单抗（VEGF）、帕博利珠单抗（PD-1）、地舒单抗（RANKL）、阿替利珠单抗（PD-L1）、注射用BL-B01D1（ EGFR/HER3 ）等品种上榜申办品种TOP10。数据来源：摩熵医药中国临床试验数据库07前十内外资企业合计开展28%临床试验，恒瑞医药、阿斯利康斩获榜首从申办企业来看，2019-2024开展新药临床试验的内资药企中，恒瑞医药凭借835项位列榜首，其次为正大天晴（344项）、翰森制药（190项）。排名前十的内资企业合计开展2150项试验，占比约18.52%。外资药企中，阿斯利康位居榜首，近六年在我国开展新药临床试验176项，其次为强生、诺华、默沙东等企业。排名前十的外资企业合计开展1123项试验，占比约9.67%。数据来源：摩熵医药中国临床试验数据库08政策助力中医药研发升温，中药新药获批临床数量持续攀升受益于政策支持，近年来我国中医药领域研发热情持续高涨，中药临床试验申请/获批数量持续攀升。中药创新药、中药改良型新药、古代经典名方中药复方制剂、同名同方药中，前三类属于中药新药。1类中药创新药中，2020-2024年获批临床药品数不断提升，从2020年4款提升至2024年46款，五年合计获批临床数量达149款；2类中药改良型新药中，2020-2023年获批临床药品数稳步攀升，2023年达16款，2024年跌落至12款，五年合计获批临床数量达46款。截图来源：摩熵咨询《中国临床试验趋势与国际多中心临床展望》报告09富马酸伏诺拉生片为BE试验热门品种，齐鲁制药开展BE试验达114项近六年BE试验数量前十品种中，富马酸伏诺拉生片、他达拉非片、达格列净片登记试验数量最多，分别有116项、103项、78项。齐鲁制药、华海药业以及石家庄四药等企业布局的BE试验数量较多，分别有114项、111项、109项。热门品种富马酸伏诺拉生片原研企业为武田，2014年全球首次获批，2019年进入中国市场。国内布局该品种的仿制药企众多，首家过评企业为山东新时代，目前过评企业总计14家。截图来源：摩熵咨询《中国临床试验趋势与国际多中心临床展望》报告小结近六年中国临床试验数量持续增长，2024年突破4800项，新药研发占据主导地位。化学药和生物制品表现突出，肿瘤领域成为研发焦点，GLP-1R靶点异军突起。恒瑞医药、阿斯利康等企业领跑申办榜单，中医药在政策支持下稳步发展。尽管成果显著，但中药临床规模和Ⅳ期试验仍有提升空间。未来，中国医药创新有望在全球舞台上发挥更重要的作用。END本文为原创文章，转载请留言获取授权《中国临床试验趋势与国际多中心临床展望》下期内容预告目录一、百济神州国际化进程加速！本土药企国际多中心临床趋势一览二、创新药大爆发！百济神州、亚盛医药国际多中心临床详解近期将持续更新，敬请期待近期热门资源获取中国临床试验趋势与国际多中心临床展望-2025052024年医药企业综合实力排行榜-202505中国带状疱疹疫苗行业分析报告-2025052023H2-2024H1中国药品分析报告-202504数据透视：中药创新药、经典验方、改良型新药、同名同方的申报、获批、销售情况-2025032024年中国1类新药靶点白皮书-202503中国AI医疗健康企业创新发展百强榜单-202502解码护肤抗衰：消费偏好洞察与市场格局分析-2025022024年FDA批准上市的新药分析报告-202501小分子化药白皮书（上）-2025012024年中国医疗健康投融资全景洞察报告-2025012024年医保谈判及市场分析报告-202501近期更多摩熵咨询热门报告，识别下方二维码领取联系我们，体验摩熵医药更多专业服务会议合作园区服务数据库咨询定制服务媒体合作👆👆👆点击上方图片，即可开启摩熵化学数据查询点击阅读原文，申请摩熵医药企业版免费试用！

临床1期临床2期临床3期

2025-06-13

·复星医药

全球研发｜东南亚市场再拓两国！复星医药子公司复宏汉霖H药汉斯状®新加坡和马来西亚获批上市

近日，复星医药子公司复宏汉霖自主研发的抗PD-1单抗H药汉斯状®（斯鲁利单抗，欧洲商品名：Hetronifly®），分别获得新加坡卫生科学局（HSA）和马来西亚国家药品监管局（NPRA）批准，用于治疗广泛期小细胞肺癌（ES-SCLC），商品名为Zerpidio®。此次获批是继印度尼西亚、柬埔寨、泰国获批后，该产品在东南亚市场的又一重要拓展。H药在东南亚的商业化由印度尼西亚制药公司PT Kalbe Farma Tbk.子公司KGbio负责，该公司被授予H药在东盟十国的部分适应症及疗法的独家开发和商业化权利。突破桎梏，重塑SCLC长生存希望肺癌是全球发病率和死亡率最高的恶性肿瘤，据GLOBOCAN最新数据显示，2022年，东南亚地区肺癌新发病例18.6万，死亡病例16.6万，其中，新加坡和马来西亚的肺癌死亡率高居该国所有癌种首位[1]。小细胞肺癌（SCLC）是肺癌中侵袭性最强的亚型，约占肺癌总数的15%，分为局限期小细胞肺癌（LS-SCLC）和ES-SCLC。据统计，约80%的患者首次确诊已处于广泛期阶段，且临床病情恶化快，总体预后不良[2]。近年来，以PD-1/PD-L1免疫检查点抑制剂为代表的免疫治疗兴起，为SCLC患者带来了更多的治疗选择及生存获益。H药是全球首个获批一线治疗小细胞肺癌的抗PD-1单抗，已在全球30多个国家和地区获批上市，惠及逾11万名患者。此次H药在新加坡和马来西亚获批主要基于ASTRUM-005研究，该研究在全球开设了128个试验中心，入组585例受试者，研究结果于2022年美国临床肿瘤学会（ASCO）年会以口头报告方式首次发布，并于全球四大顶级医学期刊之一的《美国医学会杂志》（JAMA）发表，成为全球首个登上JAMA主刊的SCLC免疫治疗临床研究。在今年ASCO大会上，ASTRUM-005首次公布了4年OS率。长期随访数据（中位随访时间42.4个月）显示斯鲁利单抗组的4年OS率达21.9%，对照组为7.2%，进一步夯实了该方案能为ES-SCLC患者带来显著的长期生存获益。拓展全球，推动更多患者获益2019年，复宏汉霖与KGbio就H药签订独家许可协议，授予其H药在东盟十国的部分适应症及疗法的独家开发和商业化权利。2023年8月，双方深化合作，KGbio获得在沙特阿拉伯、阿联酋、埃及、卡塔尔、约旦、摩洛哥等12个中东和北非地区（MENA）国家针对H药包括ES-SCLC在内的两项适应症进行独家开发和商业化的权益。得益于双方紧密协作，H药的国际化进程持续提速。2023年12月，H药迎来首个海外获批，获得印度尼西亚食品药品监督管理局（BPOM）批准用于治疗ES-SCLC，成为首个于东南亚获批上市的国产抗PD-1单抗。2024年4月和7月，H药相继在柬埔寨和泰国获批治疗ES-SCLC；2025年1月，H药于印度尼西亚和泰国新增获批鳞状非小细胞肺癌（sqNSCLC），东南亚市场影响力进一步扩大。除东南亚市场外，H药的全球化布局也正加速向多区域纵深推进。截至目前，H药已在中国获批用于治疗sqNSCLC、ES-SCLC、食管鳞状细胞癌（ESCC）和非鳞状非小细胞肺癌（nsNSCLC)。2025年2月，H药获欧盟批准用于一线治疗ES-SCLC，成为欧盟首个且唯一获批该适应症的抗PD-1单抗，实现了国产创新药在欧美主流生物药市场的关键突破。目前，公司正在美国开展一项H药对比一线标准治疗阿替利珠单抗用于ES-SCLC的头对头桥接试验，以支持其美国上市申报。此外，H药治疗SCLC已获美国食品和药品监督管理局（FDA）、欧盟委员会（EC）、瑞士药品监督管理局（Swissmedic）授予孤儿药资格，并获韩国食品药品安全部（MFDS）授予用于ES-SCLC孤儿药资格。复宏汉霖始终坚持以患者为中心，未来将继续携手全球合作伙伴，通过创新与合作，为全球患者带来更多优质、可负担的治疗选择。关于复宏汉霖复宏汉霖（2696.HK）是一家国际化的创新生物制药公司，致力于为全球患者提供可负担的高品质生物药，产品覆盖肿瘤、自身免疫疾病、眼科疾病等领域，已有6款产品在中国获批上市，4款产品在国际获批上市，5个上市申请分别获中国药监局、美国FDA和欧盟EMA受理。自2010年成立以来，复宏汉霖已建成一体化生物制药平台，高效及创新的自主核心能力贯穿研发、生产及商业运营全产业链。公司已建立完善高效的全球创新中心，按照国际药品生产质量管理规范（GMP）标准进行生产和质量管控，不断夯实一体化综合生产平台，其中，公司商业化生产基地已相继获得中国、欧盟和美国GMP认证。复宏汉霖前瞻性布局了一个多元化、高质量的产品管线，涵盖约50个分子，并全面推进基于自有抗PD-1单抗H药汉斯状®的肿瘤免疫联合疗法。截至目前，公司已获批上市产品包括国内首个生物类似药汉利康®（利妥昔单抗）、自主研发的中美欧三地获批单抗生物类似药汉曲优®（曲妥珠单抗，美国商品名：HERCESSI™，欧洲商品名：Zercepac®）、汉达远®（阿达木单抗）、汉贝泰®（贝伐珠单抗）、全球首个获批一线治疗小细胞肺癌的抗PD-1单抗汉斯状®（斯鲁利单抗，欧洲商品名：Hetronifly®）以及汉奈佳®（奈拉替尼）。公司亦同步就19个产品在全球范围内开展30多项临床试验，对外授权全面覆盖欧美主流生物药市场和众多新兴市场。Expanding Southeast Asian Presence: Serplulimab Approved in Singapore and MalaysiaRecently, Henlius' self-developed anti-PD-1 monoclonal antibody HANSIZHUANG (serplulimab, trade name: Hetronifly® in Europe) has secured approvals in Singapore and Malaysia through its local license holder, KGbio (a subsidiary of PT Kalbe Farma Tbk.), under the trade name Zerpidio® for the treatment of extensive-stage small cell lung cancer (ES-SCLC). This marks another significant expansion in Southeast Asia following earlier approvals in Indonesia, Cambodia, and Thailand. Under the agreement, serplulimab’s commercialization in Southeast Asia is managed by KGbio, which holds exclusive rights to develop and commercialize the drug for certain indications and therapies across 10 ASEAN countries. SCLC Survival Breakthrough: Renewing Hope for PatientsLung cancer continues to be the malignancy with the highest global incidence and mortality rates. According to the latest GLOBOCAN data, Southeast Asia witnessed approximately 186,000 new lung cancer cases and 166,000 deaths in 2022. Notably, lung cancer mortality ranked highest among all cancer types in both Singapore and Malaysia[1]]. Small cell lung cancer (SCLC), accounting for roughly 15% of all lung cancer cases, stands as one of its most aggressive subtypes. It is classified into limited-stage (LS-SCLC) and ES-SCLC. Statistics indicate that nearly 80% of patients are diagnosed at the extensive stage, with rapid clinical deterioration and poor overall prognosis[2]. In recent years, advances in immunotherapy, particularly PD-1/PD-L1 immune checkpoint inhibitors, have expanded treatment options and improved survival outcomes for SCLC patients.Serplulimab is the world's first anti-PD-1 monoclonal antibody approved for first-line treatment of SCLC, having been approved for marketing in over 30 countries and regions worldwide, benefiting over 110,000 patients. This approval of serplulimab in Singapore and Malaysia is primarily based on the ASTRUM-005 study, which established 128 trial centers globally and enrolled 585 subjects. The study results were first released via oral presentation at the 2022 American Society of Clinical Oncology (ASCO) annual meeting and published in the Journal of the American Medical Association (JAMA), one of the world's four top-tier medical journals, making it the world's first SCLC immunotherapy clinical research published in JAMA's main journal. At this year's ASCO conference, the ASTRUM-005 trial, for the first time, reported the 4-year overall survival (OS) rate. Long-term follow-up data (median follow-up: 42.4 months) showed a 4-year OS rate of 21.9% in the serplulimab-treated group versus 7.2% in the control group, further confirming that this regimen can bring significant long-term survival benefits to ES-SCLC patients.Global Expansion: Helping More Patients WorldwideIn 2019, Henlius entered into an exclusive licensing agreement with KGbio for serplulimab, granting KGbio exclusive rights to develop, register and commercialize serplulimab for certain indications and therapies across 10 ASEAN countries. Building on this partnership, the collaboration expanded in August 2023 with KGbio securing exclusive commercialization rights for two indications – including ES-SCLC – in 12 Middle East and North Africa (MENA) countries, notably Saudi Arabia, UAE, Egypt, Qatar, Jordan, and Morocco. Accelerated by this strategic collaboration, serplulimab's global rollout has achieved significant milestones. In December 2023, serplulimab achieved its first overseas approval, receiving authorization from the Indonesian Food and Drug Administration (BPOM) for the treatment of ES-SCLC. This made it the first China-developed anti-PD-1 monoclonal antibody approved for marketing in Southeast Asia. In April and July 2024, serplulimab was successively approved for the treatment of ES-SCLC in Cambodia and Thailand. In January 2025, serplulimab received additional approvals for squamous non-small cell lung cancer (sqNSCLC) in Indonesia and Thailand, further expanding its influence in the Southeast Asian market.Beyond the Southeast Asia, serplulimab's global deployment is accelerating across multiple key markets. To date, the drug has gained four Chinese approvals for the treatment of sqNSCLC, ES-SCLC, esophageal squamous cell carcinoma (ESCC), and non-squamous non-small cell lung cancer (nsNSCLC). A pivotal milestone was achieved in February 2025 when the European Commission approved serplulimab as first-line therapy for ES-SCLC – making it the first and only anti-PD-1 mAb authorized for this indication in the EU. This authorization represents a landmark breakthrough for China-developed biologics in Western regulated markets. To support US registration, the company is steadily advancing the bridging head-to-head trial in the US to compare serplulimab to standard-of-care atezolizumab (anti-PD-L1 mAb) for the first-line treatment of ES-SCLC. Furthermore, serplulimab has earned Orphan Drug Designations for SCLC from the US FDA, European Commission, and Swissmedic, along with specific designation for ES-SCLC from Korea's Ministry of Food and Drug Safety (MFDS).Henlius remains committed to a patient-centric approach. Moving forward, we will continue to collaborate closely with global partners, leveraging innovation and cooperation, to deliver more high-quality, affordable treatment options to patients worldwide.About HenliusHenlius (2696.HK) is a global biopharmaceutical company with the vision to offer high-quality, affordable and innovative biologic medicines for patients worldwide with a focus on oncology, autoimmune diseases and ophthalmic diseases. Up to date, 6 products have been launched in China, 4 have been approved for marketing in overseas markets, and 5 marketing applications have been accepted for review in China, the U.S. and the EU, respectively. Since its inception in 2010, Henlius has built an integrated biopharmaceutical platform with core capabilities of high-efficiency and innovation embedded throughout the whole product life cycle including R&D, manufacturing and commercialization. It has established global innovation centre and Shanghai-based commercial manufacturing facilities certificated by China, the EU and U.S. GMP.Henlius has pro-actively built a diversified and high-quality product pipeline covering about 50 molecules and has continued to explore immuno-oncology combination therapies with proprietary HANSIZHUANG (anti-PD-1 mAb) as the backbone. To date, the company's launched products include HANLIKANG (rituximab), the first China-developed biosimilar, HANQUYOU (trastuzumab, trade name: HERCESSI™ in the U.S., Zercepac® in Europe), a China-developed mAb biosimilar approved in China, Europe and U.S., HANDAYUAN (adalimumab), HANBEITAI (bevacizumab), HANSIZHUANG (serplulimab, trade name: Hetronifly® in Europe), the world’s first anti-PD-1 mAb for the first-line treatment of SCLC, and HANNAIJIA (neratinib). What’s more, Henlius has conducted over 30 clinical studies for 19 products, expanding its presence in major markets as well as emerging markets.References[1] Bray, F., Laversanne, M., Sung, H., et al. (2024). Global cancer statistics 2022: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries. CA: A Cancer Journal for Clinicians. DOI: 10.3322/caac.21834[2] 中国临床肿瘤学会小细胞肺癌专家委员会, 中国医师协会肿瘤多学科诊疗专业委员会. 小细胞肺癌免疫治疗专家共识（2025版）[J]. 中华肿瘤杂志, 2025, 47(1): 65-75.

2025-06-13

·医学新视点

《柳叶刀》：死亡风险降低27%！联合疗法显著延长肺癌患者生命

近日，IMforte临床3期试验的总生存期结果公布，该试验评估Zepzelca（lurbinectedin）与PD-L1抑制剂Tecentriq（atezolizumab）联合作为广泛期小细胞肺癌（ES-SCLC）成人患者（≥18岁）一线维持疗法的效果。该研究结果同步发表于ASCO和《柳叶刀》。根据此积极结果，该公司已向美国FDA提交了Zepzelca组合疗法用于此类患者群体的监管申请。截图来源：The Lancet分析显示，在中位随访15.0个月时，与Tecentriq单药相较，接受Zepzelca与Tecentriq联合疗法患者的死亡风险降低了27%（HR=0.73，95% CI：0.57-0.95，P=0.0174）。接受Zepzelca组合疗法治疗患者的中位总生存期为13.2个月，而活性对照组患者的中位总生存期为10.6个月。Zepzelca又名PM1183，是一种烷基化药物，可结合DNA内的鸟嘌呤碱基。这触发了一系列级联反应，可影响DNA结合蛋白（包括一些转录因子）的活性，以及DNA修复通路，从而导致细胞周期的破坏和最终的细胞死亡。该疗法在2020年6月获美国FDA加速批准上市，用于治疗接受铂类药物化疗时或化疗后疾病进展的转移性小细胞肺癌成人患者。PD-L1抑制剂Tecentriq已经在美国，欧盟等国家获得批准，可以单独使用，也可以与靶向疗法或化疗联合使用，用于治疗多种癌症类型。推荐阅读NEJM：肺癌靶向治疗新突破！71%患者客观缓解，持续缓解超14个月JCO：无进展生存期几乎翻倍，阿法替尼或改写这类肺癌治疗标准95%肺癌患者持续缓解6个月！中肿张力&方文峰团队研究登《自然-医学》5年存活患者几乎翻倍，死亡风险降低41%！新药为晚期肺癌患者带来持久显著获益参考资料：[1] Lurbinectedin (lurbi) + atezolizumab (atezo) as first-line (1L) maintenance treatment (tx) in patients (pts) with extensive-stage small cell lung cancer (ES-SCLC): Primary results of the phase 3 IMforte trial. Retrieved May 23, 2025 from https://meetings.asco.org/abstracts-presentations/243670[2] IMforte investigators (2025). Efficacy and safety of first-line maintenance therapy with lurbinectedin plus atezolizumab in extensive-stage small-cell lung cancer (IMforte): a randomised, multicentre, open-label, phase 3 trial. The Lancet, DOI: https://doi.org/10.1016/S0140-6736(25)01011-6免责声明：本文仅作信息交流之目的，文中观点不代表药明康德立场，亦不代表药明康德支持或反对文中观点。本文也不是治疗方案推荐。如需获得治疗方案指导，请前往正规医院就诊。版权说明：欢迎个人转发至朋友圈，谢绝媒体或机构未经授权以任何形式转载至其他平台。转载授权请在「药明康德」微信公众号回复“转载”，获取转载须知。分享，点赞，在看，传递医学新知

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
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
广泛期小细胞肺癌	列支敦士登	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
结外NK-T细胞淋巴瘤	申请上市	日本	Chugai Pharmaceutical Co., Ltd.	2024-10-31
1型糖尿病	申请上市	中国	Provention Bio, Inc.	2024-08-28
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	-	2023-10-25
黑色素瘤	临床3期	英国	-	2023-10-25
MSI-H 癌症	临床3期	英国	-	2023-10-25
Turcot综合征	临床3期	英国	-	2023-10-25
肌层浸润性膀胱癌	临床3期	比利时	Hoffmann-La Roche, Inc.	2021-05-03
肌层浸润性膀胱癌	临床3期	中国香港	Hoffmann-La Roche, Inc.	2021-05-03
肌层浸润性膀胱癌	临床3期	墨西哥	Hoffmann-La Roche, Inc.	2021-05-03

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分期

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT03811002 (NRG-LU005, CTgov)	临床3期	局限期小细胞肺癌	544	Intensity-Modulated Radiation Therapy+Etoposide+Carboplatin+cisplatin (Arm I (Chemotherapy, Radiation Therapy))	觸鹹鏇獵餘餘構選鹹襯(鏇夢淵遞膚遞餘鬱範簾) = 鹽艱網憲鏇糧齋鹹憲糧窪衊壓網範獵壓膚繭糧 (繭製艱繭襯廠餘壓憲衊, 齋獵鹽膚衊繭壓窪選選 ~ 鑰膚糧積襯醖顧鬱鏇齋) 更多	-	2025-06-12
				Intensity-Modulated Radiation Therapy+Etoposide+Carboplatin+cisplatin+Atezolizumab (Arm II (Chemotherapy, Radiation Therapy, Atezolizumab))	觸鹹鏇獵餘餘構選鹹襯(鏇夢淵遞膚遞餘鬱範簾) = 膚艱鹽衊築選壓願蓋憲窪衊壓網範獵壓膚繭糧 (繭製艱繭襯廠餘壓憲衊, 鬱製遞淵餘積獵窪繭顧 ~ 觸糧蓋壓膚夢衊衊鏇壓) 更多
NCT02912559 (Alliance A021502; ATOMIC, ASCO2025) 人工标引	临床3期	错配修复缺陷或微高卫星不稳定性结肠癌辅助 Deficient DNA Mismatch Repair (dMMR)	712	atezolizumab + mFOLFOX6	衊艱築壓觸膚憲衊鹹餘(鏇鑰簾襯範餘構淵衊膚) = 鹽壓衊選鬱蓋淵艱壓夢齋淵顧獵壓醖鏇廠遞餘 (鏇憲築淵壓夢壓網壓築, 81.8 ~ 89.9) 更多	积极	2025-05-30
				mFOLFOX6	衊艱築壓觸膚憲衊鹹餘(鏇鑰簾襯範餘構淵衊膚) = 選構獵鏇蓋壓鑰簾願蓋齋淵顧獵壓醖鏇廠遞餘 (鏇憲築淵壓夢壓網壓築, 71.3 ~ 81.0) 更多
NCT05091567 (IMforte, ASCO2025) 人工标引	临床3期	广泛期小细胞肺癌维持 \| 一线	660	Lurbinectedin + Atezolizumab	獵壓願構膚衊築顧餘糧(醖範壓憲憲窪繭壓憲簾) = 網齋蓋齋製鬱選選廠襯築窪壓鏇遞簾顧醖廠糧 (鏇淵網構襯積蓋壓遞遞, 4.2 ~ 5.8) 更多	积极	2025-05-30
				Atezolizumab	獵壓願構膚衊築顧餘糧(醖範壓憲憲窪繭壓憲簾) = 選艱醖積鏇選鬱壓範製築窪壓鏇遞簾顧醖廠糧 (鏇淵網構襯積蓋壓遞遞, 1.6 ~ 2.7) 更多
NCT03554083 (NeoACTIVATE arm C, ASCO2025)	临床2期	新辅助 \| 辅助 TIGIT	34	Atezolizumab 1200mg IV + Tiragolumab 600mg IV	顧積積艱憲築築憲簾願(夢遞窪顧夢鏇願餘廠膚) = 5 patients (14.7%) experienced any grade 3+ AE with 2 (5.9%) at least possibly related to the neoadjuvant regimen 餘顧網夢夢鹽壓網觸繭 (蓋壓夢憲壓範衊顧衊醖 )	积极	2025-05-30
ASCO2025	N/A	晚期肝细胞癌二线	552	Lenvatinib	選膚範衊築積衊齋鬱遞(觸衊淵餘夢願窪遞窪衊) = 構顧範獵艱襯襯衊鏇選齋範選餘鹹繭鏇憲壓鹹 (網衊鹹鹹淵網選鹹製鏇 )	不佳	2025-05-30
				Cabozantinib	選膚範衊築積衊齋鬱遞(觸衊淵餘夢願窪遞窪衊) = 繭簾獵鏇衊選膚壓餘醖齋範選餘鹹繭鏇憲壓鹹 (網衊鹹鹹淵網選鹹製鏇 )
NCT04338269 (CONTACT-03, ASCO2025)	临床3期	晚期肾细胞癌二线	522	Cabozantinib (cabo)	夢繭鹽襯觸獵顧蓋遞壓(範願艱鹽廠糧齋醖齋鏇) = 鏇願窪積壓鬱願遞獵齋鹽構鏇鏇壓鏇壓遞襯製 (網膚範鬱窪廠糧鑰繭願 ) 更多	积极	2025-05-30
				Cabozantinib (cabo) + Atezolizumab (atezo)	夢繭鹽襯觸獵顧蓋遞壓(範願艱鹽廠糧齋醖齋鏇) = 膚觸艱壓憲獵醖願鹹築鹽構鏇鏇壓鏇壓遞襯製 (網膚範鬱窪廠糧鑰繭願 ) 更多
ASCO2025	N/A	不可切除的肝细胞癌一线 Non-Alcoholic Steatohepatitis (NASH)	21	Atezolizumab and Bevacizumab Combination	製襯網憲壓築選鏇製顧(壓餘構憲繭鹽齋獵衊製) = 57.1% 觸願夢獵遞築壓廠鏇齋 (獵鹹糧顧觸夢製範餘築 ) 更多	不佳	2025-05-30
NCT03108131 (CTgov)	临床2期	腺癌 \| 肝转移 \| 肿瘤转移 ... 更多	49	Cobimetinib+atezolizumab+5FU	襯觸範繭壓簾網膚襯膚 = 鬱遞鑰餘繭顧窪願壓淵衊艱鬱糧網窪範範醖衊 (襯艱醖鑰壓淵積壓窪鑰, 襯遞鹹膚糧願醖醖網觸 ~ 顧簾壓廠鏇簾壓鑰顧鏇) 更多	-	2025-05-28
NCT04642365 (CTgov)	临床1期	晚期恶性实体瘤	49	Atezolizumab+RO7296682 (Part 1: Cohort 1 - RO7296682 0.3 mg + Atezolizumab 1200 mg)	繭積窪獵窪遞衊鏇範夢 = 窪鹹築壓築遞壓選餘夢淵蓋衊廠餘觸選衊構憲 (製廠壓憲簾廠遞觸鹹簾, 簾鑰製廠鬱積繭願膚壓 ~ 窪壓廠淵範蓋獵衊廠壓) 更多	-	2025-05-21
				Atezolizumab+RO7296682 (Part 1: Cohort 2 - RO7296682 1.5 mg + Atezolizumab 1200 mg)	繭積窪獵窪遞衊鏇範夢 = 糧廠繭鹹顧襯餘簾壓蓋淵蓋衊廠餘觸選衊構憲 (製廠壓憲簾廠遞觸鹹簾, 淵簾願鏇壓蓋醖窪製選 ~ 淵夢觸簾襯窪獵壓願觸) 更多
NCT04730999 (CeLEBrATE, NEWS) 人工标引	临床2期	广泛期小细胞肺癌一线	48	阿替利珠单抗+贝伐单抗+卡铂+依托泊苷	餘鬱範淵憲艱鹽鹽顧艱(網鏇網網顧選艱襯範艱) = 築構觸築範齋窪壓壓襯積夢願簾壓鏇淵餘夢淵 (夢壓製糧鹹淵夢壓壓壓 ) 更多	积极	2025-05-20