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

NCT05870800

/ Recruiting临床2期IIT

Phase II Open-label Trial of Neoadjuvant Immunotherapy (Atezolizumab) in Combination With CAPOX for Resectable Non-metastatic Proficient Mismatch Repair (pMMR) Colon CancER: NICER Study

This is a Phase II open-label trial of neoadjuvant immunochemotherapy with Atezolizumab and CAPOX followed by surgery and potentially adjuvant chemotherapy for patients with localized resectable pMMR adenocarcinoma of the colon with a target accrual of 28 patients. The investigators will explore if appropriately timed neoadjuvant CAPOX with anti-PD-L1 mAb (Atezolizumab) can be administered safely and feasibly, and that this combination will lead to improved clinical response associated with enhanced numbers of immune cells in surgically resected colon tumors. Patients will receive 4 cycles of atezolizumab in combination with 4 cycles of CAPOX (atezolizumab will be administered prior to chemotherapy) before standard of care surgical resection. Following surgery, patients still considered to be at high-risk of recurrence (per SOC guidelines) will receive further adjuvant chemotherapy (mFOLFOX6 or CAPOX), based on the discretion of the treating oncologist/investigator. Circulating tumor DNA (ctDNA) dynamic change status will be analyzed through collection of blood samples throughout different stages of the patient's neoadjuvant treatment regimen (baseline, pre-neoadjuvant therapy, mid-neoadjuvant, post-neoadjuvant therapy, and during postoperative period) as a marker of early read on efficacy.
The end of the study for each patient enrolled will be at the 6 month postoperative visit.
On Study Protocol: Patients will be followed up for an efficacy follow-up phase during the first 6 months after surgery (week 2 & months 3, 6 visits). All assessments beyond the 6 month visit will be performed under standard of care surveillance office visits.
Off Study Protocol: Thereafter they will enter a survival follow-up phase per standard of care protocols. Patients will be seen every 6 months starting at month 12 until month 36. All collection of research-specific assessments including whole blood, stool collection and quality of life questionnaires will be optional beyond the 6 month postop visit (months 12-36).

开始日期2025-06-15

申办/合作机构

Baylor College of Medicine

[+1]

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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4,521

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.

2025-08-01·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.

2025-08-01·ENVIRONMENTAL RESEARCH

Unraveling the hidden pathways: Bioaccumulation and metabolism of atrazine, acetochlor, and metolachlor in aquatic organisms

Article

作者: Guo, Xiaxia ; Zhang, Wenjie ; Zeng, Dongqiang ; Cao, Wenjing ; Chen, Zhaojie ; Li, Xuesheng ; Zhang, Cuifang

Atrazine (ATZ), acetochlor (ACE), and metolachlor (MET) are widely used herbicides whose residues persist in the environment, contributing to the mixed pollution of aquatic ecosystems. However, the mechanisms underlying their environmental behavior and biological effects remain poorly understood. In this study, we systematically investigated the transfer, bioaccumulation, and elimination of ATZ, ACE, and MET in fish (Procypris merus) under single and combined exposure conditions. The results indicate that after exposure in water, ATZ, ACE, and MET extensively accumulate in the muscle tissue of P. merus, accounting for 71 %-84 % of the total pesticide accumulation, making it the primary storage site for these herbicides. Under mixed exposure conditions, the three herbicides exhibited time-dependent synergistic toxic effects. Combined exposure to ATZ, ACE, and MET significantly increased the concentrations of ATZ and ACE in the liver, as well as the K_up and BCF of ACE and MET. During the purification and detoxification phases, the gills exhibited the highest purification rate, nearly twice that of the intestines and liver. The distribution of herbicides in various tissues was positively correlated with hydrophobicity (log Kow) and lipid content. Using UPLC-ESI-QTOF-MS/MS, the metabolites of ATZ, ACE, and MET were identified and analyzed. The three pesticides were primarily metabolized in the lotus carp through dealkylation, hydroxylation, and conjugation with glutathione/glucose. A total of 9 ATZ metabolites, 11 ACE metabolites, and 10 MET metabolites were identified, 19 of which were detected in fish for the first time. rac-MET displayed distinct stereoselective behavior, with the liver preferentially enriching the 1'S, α'R-MET isomer. This study provides a robust dataset for understanding the environmental and dietary risks of the target herbicides associated with residues that persist for prolonged periods.

2,188

项与阿替利珠单抗相关的新闻（医药）

15 小时之前

·小药说药

巨噬细胞肿瘤免疫治疗的研究进展

-01-引言肿瘤相关巨噬细胞（TAM）是免疫抑制细胞和细胞因子网络的核心，在肿瘤免疫逃避中起着至关重要的作用。因此，了解巨噬细胞和其他免疫细胞之间的相互作用以及增强现有抗癌治疗的因素至关重要。TAM在功能上是异质性的，分为两个主要亚群，M1和M2巨噬细胞。M1巨噬细胞是抵抗微生物感染的第一道防线，M1巨噬细胞还保持强大的抗原呈递能力，诱导强烈的Th1反应。相反，M2巨噬细胞在限制免疫反应、诱导血管生成和组织修复方面起着关键作用。因此，M2型TAM的存在与促肿瘤活性相关，而M1型TAM的存在与抗肿瘤活性相关。总之，TAM是产生免疫抑制性TME的关键，并且巨噬细胞与TME中的各种免疫细胞和细胞因子之间的串扰起着不可替代的作用。了解巨噬细胞参与肿瘤免疫逃逸的主要机制和相关靶向治疗，有助于我们改善临床方案，制定克服巨噬细胞相关免疫耐受的潜在新策略。-02-一、调节巨噬细胞吞噬的信号途径CD47/SIRPαCD47是一种广泛分布于正常细胞表面的免疫球蛋白，可通过抑制吞噬作用负调节抗肿瘤免疫，并参与介导细胞增殖、迁移、凋亡和免疫稳态。其主要配体信号调节蛋白α（SIRPα）是一种在髓细胞膜上高表达的跨膜蛋白，其胞外区的N末端可与CD47结合，导致免疫受体酪氨酸抑制基序（ITIM）上的酪氨酸磷酸化，释放“不要吃我”信号，从而抑制巨噬细胞介导的吞噬作用，保护正常细胞免受免疫系统的破坏。研究表明CD47在多种肿瘤中高表达，如恶性血液肿瘤和肝细胞癌（HCC），这也与不良预后相关。给予CD47阻断抗体或靶向灭活CD47基因可显著抑制肿瘤生长。此外，抗CD47治疗还可以改变TME中巨噬细胞的极化状态，诱导TAM转化为抗肿瘤状态。LILRB1/MHCI白细胞免疫球蛋白样受体B（LILRB）在大多数免疫细胞上表达，由细胞外Ig样区、跨膜区和含有ITIM的细胞内区组成。它与主要配体主要组织相容性复合体I（MHCI）结合后可介导免疫细胞激活的负调控。MHCI是由HLAα链和β2-微球蛋白（β2M）形成的复合体，某些肿瘤细胞高表达β2M，其可与巨噬细胞上的LILRB1结合以抑制吞噬作用，导致免疫监视丧失。因此，在肿瘤细胞上MHCI正常或高表达的患者中，靶向MHCI/LILRB1轴的药物可能促进抗肿瘤免疫反应，并与靶向CD47/SIRPα轴的药物发挥协同作用。CD24/Siglec-10CD24，也称为热稳定抗原，是一种高度糖基化的表面蛋白，由糖基磷脂酰肌醇锚定，可与唾液酸结合免疫球蛋白样凝集素-10（Siglec-10）相互作用，以减少感染或肝损伤引起的先天免疫介导的有害炎症。肿瘤细胞高表达CD24，而TAM高表达Siglec-10。与CD24结合后，Siglec-10的ITIM可招募并激活含有SH2结构域的酪氨酸磷酸酶SHP-1或SHP-2，从而阻断巨噬细胞吞噬所需的细胞骨架重排，触发抑制性信号转导级联。“不要吃我”发出CD47、β2M和CD24信号，所有这些信号都涉及基于ITIM的巨噬细胞信号，导致巨噬细胞耐药癌细胞亚群的免疫选择，使肿瘤细胞逃避巨噬细胞的监视和清除。因此，掌握肿瘤细胞表达抗吞噬信号的机制可以更好地预测治疗效果以及靶向治疗。-03- 二、巨噬细胞参与免疫逃避的机制巨噬细胞参与形成抑制性髓系微环境TME中的各种介质参与调节MDSC和单核细胞的募集，并通过不同的信号通路极化巨噬细胞，从而促进免疫抑制髓系微环境的形成。此外，巨噬细胞、MDSC和树突状细胞之间的串扰进一步形成免疫抑制髓系微环境。卵巢癌细胞高表达CD39和CD73，有助于催化细胞外ATP转化为腺苷，腺苷可以招募单核细胞并诱导它们分化为分泌IL-10的TAM。TAM表达CD39和CD73，进一步增加MDSC和TAM的浸润，从而形成一种自我放大机制，促进局部免疫逃逸。肿瘤相关中性粒细胞（TAN）也是免疫抑制髓系微环境的重要组成部分。与巨噬细胞一样，中性粒细胞可以被描述为两个亚群，N1和N2，N1表现出抗肿瘤活性，N2被认为能促进肿瘤转移。在乳腺癌模型中，TAMs分泌的IL-1β诱导γδT细胞释放IL-17以调节G-CSF的释放并促进中性粒细胞的募集以刺激转移，表明TANs在肿瘤进展中与TAMs密切相关。然而，TAN和TAM在肿瘤发生和免疫逃逸中的特异性相互作用机制尚不清楚。巨噬细胞影响Th细胞巨噬细胞和辅助性T细胞之间存在相互调节作用。巨噬细胞依赖TGF-β和IL-10将Th1细胞转化为Th2细胞，以逆转CD8+细胞毒性T细胞和CD4+Th1细胞的抗肿瘤作用，这被认为是一种肿瘤免疫逃逸机制。而Th细胞通过改变巨噬细胞的极化方向影响肿瘤TME。Th1细胞分泌IFN-γ以诱导M1极化，而Th2细胞可分泌IL-4、IL-5和IL-10以促进M2巨噬细胞的生成。此外，Treg表型和功能对免疫抑制性TME发挥重要作用。最近的研究表明，巨噬细胞可以通过各种途径影响Treg的增殖、迁移和功能。首先，TAMs可分泌IL-23，促进Treg的增殖以及IL-10和TGF-β的表达，抑制CTL杀伤肿瘤细胞；其次，巨噬细胞过度表达CCL1，即Treg上表达的CCR8的配体，以吸引Treg进入肿瘤区域；类似地，巨噬细胞分泌CCL22以诱导Treg迁移到卵巢癌的肿瘤区域，抑制T细胞免疫并促进肿瘤生长。巨噬细胞与CAF 的相互作用CAF是TME中最丰富的基质细胞，可释放大量细胞因子，合成和重塑细胞外基质，形成促瘤纤维微环境。CAF可分泌IL-6、M-CSF、MCP-1和基质细胞衍生因子-1，以促进巨噬细胞的浸润和分化。而M2可分泌TGF-β，以促进内皮细胞向间质细胞的转化，并增加CAF的反应性，从而增强癌细胞的侵袭性。巨噬细胞通过PD-1/PD-L1轴介导免疫逃逸TAMs调节肿瘤细胞上PD-L1和CD8+T细胞上PD-1的表达。PD-L1在多种肿瘤组织中高表达，可被TAM衍生的TNF-α上调，并与肿瘤基质中的巨噬细胞浸润呈正相关。在TME中，PD-L1在TAMs上的表达也受到许多因素的影响。IL-27/STAT3轴在淋巴瘤浸润巨噬细胞中诱导PD-L1/2过表达。Progranulin可以通过STAT3途径上调TAMs上的PD-L1，从而促进乳腺癌的免疫逃避。同时，PD-1/PD-L1轴对巨噬细胞功能有着深刻的影响。TAMs上PD-1表达的增加可抑制其吞噬作用，并在结构上作用于mTOR途径，对巨噬细胞的增殖和活化起负调节作用。因此，PD-1/PD-L1阻断也可直接影响巨噬细胞。PD-1/PD-L1阻断剂可促进巨噬细胞的促炎极化，增强效应T细胞的活性，并与其他免疫检查点抑制剂合作限制肿瘤扩散。除了PD-1/PD-L1轴外，一些实验结果表明TAM还可以与其他免疫检查点（如CTLA/CD86轴和TIM3/galectin-9轴）一起诱导免疫逃逸，但仍缺乏确切的证据。巨噬细胞与这些免疫检查点在免疫逃逸中的相互作用值得进一步研究。巨噬细胞有助于形成免疫无反应部位免疫无应答是肿瘤组织逃避免疫监视的重要原因，巨噬细胞可能通过以下机制参与肿瘤组织的免疫豁免。首先，巨噬细胞可以通过聚集CAF到肿瘤区域，CAF沉积纤维胶原、透明质酸、纤维连接蛋白和其他物质，并分泌赖氨酰氧化酶刺激I型胶原交联，从而形成物理屏障。其次，与肿瘤细胞类似，诱导的TAM可表达Fas-L并释放活性可溶性Fas-L，诱导Fas+淋巴细胞凋亡，而CAF可通过MHC-1抗原交叉呈递上调Fas-L和PD-L2，抑制CD8+T细胞的活性，从而形成缺乏淋巴细胞浸润的TME。此外，肿瘤细胞分泌的透明质酸可与巨噬细胞表面的TLR4结合，诱导TAM迁移至肿瘤相关区域，并通过miR935抑制C/EBPβ的表达，促进巨噬细胞向M2表型的分化，从而促进恶性肿瘤细胞逃避免疫监视并“冷却”免疫反应。-04-三、巨噬细胞免疫治疗的临床进展靶向TAM越来越多的证据表明TAM有助于化疗耐药性,以TAM为靶点的单一疗法或联合化疗的治疗方法正在临床前和临床中进行试验。TAM被CSF-1招募到TME中，促进乳腺癌的发展和转移。因此，用单克隆抗体或小分子化合物靶向CSF-1/CSF-1R轴的治疗方法正在试验中。RG7155是一种靶向CSF-1R的单克隆抗体，在一项1期临床试验（NCT01494688）中对7名诊断为弥漫型巨细胞瘤的患者进行治疗，所有患者均出现PR，2名患者出现CR。此外，在RG7155治疗的患者肿瘤活检中，CD68+CD163+巨噬细胞的数量减少，表明TAM向TME的募集减少。靶向CSF-1R、c-Kit和Flt3的酪氨酸激酶抑制剂PLX3397通过使TAM的M2表型去极化来阻断肿瘤进展。PLX3397正在包括黑色素瘤（NCT02071940、NCT02975700）、前列腺癌（NCT0149043）和胶质母细胞瘤（NCT01349036）患者中进行临床试验。其他CSF-1R抑制剂，如ARRY-382（NCT01316822）、BLZ945（NCT02829723）、AMG820（NCT01444404）和IMC-CS4（NCT01346358）也正在各种实体瘤患者中进行测试。除了单药治疗外，针对CSF-1或CSF-1R的抑制剂还与化疗联合进行测试。例如，PLX3397与紫杉醇联合用于晚期实体瘤患者（NCT01525602）；PLX3397与eribulin联合用于乳腺癌患者的试验（NCT01596751）；PLX3397与vemurafenib用于BRAF突变黑色素瘤患者（NCT01826448）；PLX3397联合sirolimus用于晚期肉瘤患者（ NCT02584647）等。此外，TAM的靶向剂和免疫检查点抑制剂的联合应用也在开发中。IMC-CS4与durvalumab或tremelimumab联合用于实体瘤患者的临床试验（NCT02718911）正在进行中。还有PLX3397与pembrolizumab联合用于各种肿瘤患者的1期临床试验（NCT02452424），ARRY-382与pembrolizumab的联合试验（NCT02880371），BLZ945与PDR001（一种针对PD-1的单克隆抗体）的联合试验（NCT02829723），RG7155与atezolizumab的联合试验（NCT02323191），以及AMG820与使用pembrolizumab的联合试验（NCT02713529）。CAR-巨噬细胞直到2020年11月，两个基于CAR-M策略的临床试验已经获得FDA的批准。第一个是来自CARISMA Therapeutics的候选药物CT-0508，它用抗HER2的CAR-M治疗复发/难治性HER2过度表达的肿瘤患者（I期临床试验）。另一个是Maxyte的MCY-M11，它利用mRNA转染PBMC表达靶向间皮素的CAR（包括CAR-M），治疗复发/难治性卵巢癌和腹膜间皮瘤患者，目前正在招募志愿者进行I期临床试验。-05-结语越来越多的研究表明巨噬细胞在肿瘤发展、转移、免疫调节、肿瘤血管形成、TME重塑和癌症治疗反应中起着关键作用。巨噬细胞靶向治疗有望成为肿瘤免疫治疗的下一个前沿，阐明其相互作用模式将有助于对免疫抑制性TME形成更全面的认识，避免免疫反弹，减少肿瘤免疫逃避，促进相关研究的发展。参考资料：1.Next frontier in tumor immunotherapy:macrophage-mediated immune evasion. Biomark Res. 2021; 9: 72.公众号内回复“ADC”或扫描下方图片中的二维码免费下载《抗体偶联药物：从基础到临床》的PDF格式电子书！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。

免疫疗法

2025-05-27

·GlobeNewswire-Health Care

BioNTech to Present Progress Across Diversified Oncology Pipeline at the 2025 ASCO Annual Meeting

MAINZ, Germany, May 27, 2025 -- BioNTech SE (Nasdaq: BNTX, “BioNTech” or “the Company”) will present clinical trial data from select pipeline candidates across the Company’s diversified oncology portfolio at the American Society of Clinical Oncology (“ASCO”) Annual Meeting, to be held in Chicago, IL, from May 30 to June 3, 2025. The data highlight continued progress of the Company’s clinical programs consisting of complementary therapeutic modalities, including mRNA cancer immunotherapies, next-generation immunomodulators, and targeted therapies, including antibody-drug conjugates (“ADCs”). “We believe that the next era of cancer medicine will be defined by the interplay of complementary mechanisms and innovative molecules, unlocking their full potential through synergy. Our data presentations at this year's ASCO Annual Meeting show how we aim to help shape this era,” said Prof. Özlem Türeci, M.D., Co-Founder and Chief Medical Officer at BioNTech. “We will present clinical progress with two of our therapeutic modalities: our next generation immunomodulators, most notably our investigational anti-PD-L1xVEGF-A antibody BNT327, and for one of our ADC programs, which are an important pillar of our combination strategy. These data underline the potential of our assets to improve outcomes for patients.” Highlights of BioNTech’s oncology programs to be presented at ASCO 2025: Three presentations on BNT3271, an investigational anti-PD-L1xVEGF-A antibody, will detail data from ongoing later-stage and potentially registrational clinical trials: An oral presentation will feature the first data from a Phase 2 clinical trial (NCT05918107) of BNT327 in combination with chemotherapy as first-line treatment for patients with unresectable malignant mesothelioma. Malignant mesothelioma is a type of cancer that develops in the tissue that covers the lung or the abdomen. The preliminary data indicated anti-tumor activity and a manageable safety profile. Two posters will detail the ongoing global Phase 3 and Phase 2/3 clinical trials, ROSETTA Lung-01 (NCT06712355) in extensive-stage small cell lung cancer (“ES-SCLC”) and ROSETTA Lung-02 (NCT06712316) in non-small cell lung cancer (“NSCLC”). BNT327 combines the two complementary anti-tumor mechanisms of PD-L1 checkpoint and VEGF-A signaling blockade in the tumor microenvironment, thereby aiming to enhance anti-tumor activity. Data on BNT324/DB-1311, a B7H3-targeted ADC candidate, from an ongoing Phase 1/2 clinical trial (NCT05914116) in patients with heavily pre-treated castration-resistant prostate cancer (“CRPC”) will be presented during an oral session. The data indicated early clinical activity and a manageable safety profile. BNT324/DB-1311 received Fast Track Designation by the U.S. Food & Drug Administration (“FDA”) for this patient population in 2024 and is being developed in collaboration with Duality Biologics (Suzhou) Co. Ltd. (“DualityBio”). Preliminary data on BNT316/ONC-392 (gotistobart), an investigational anti-CTLA-4 antibody, from two ongoing Phase 1/2 clinical trials evaluating the antibody candidate in combination with current standard of care treatments will be presented. Data from the PRESERVE-001 clinical trial (NCT04140526) in patients with advanced melanoma indicated a manageable safety profile and early signs of anti-tumor activity. The data included an analysis of overall survival (“OS”) and an ad-hoc analysis of next-treatment free survival (“NTFS”), a measure for potential long-lasting benefit after initial treatment. Data from the PRESERVE-006 clinical trial (NCT05682443) in patients with metastatic CRPC indicated a manageable safety profile and preliminary efficacy. BNT316/ONC-392 is being developed in collaboration with OncoC4, Inc. (“OncoC4”).Data on BNT142 from an exploratory Phase 1/2 dose finding trial (NCT05262530) in patients with CLDN6-positive advanced solid tumors will be featured in an oral presentation. BNT142 is an investigational lipid nanoparticle-formulated mRNA immunotherapy that encodes a CD3xCDLN6 T cell engager antibody. Preliminary data indicated a manageable safety profile and early signs of clinical activity, supporting scientific proof-of-concept and underscoring the potential of mRNA-encoded bispecific antibodies. BioNTech has established a diversified oncology portfolio to develop novel treatment approaches for patients living with cancer. The Company is advancing its oncology pipeline across multiple solid tumor indications, including more than 20 active Phase 2 and 3 clinical trials with a strategic focus on two pan-tumor priority programs: investigational mRNA cancer immunotherapies and the next-generation immunomodulator candidate BNT327. BioNTech expects multiple data readouts in 2025 and 2026 aimed at supporting its strategy and advancing the Company towards becoming a diversified multi-product oncology company. The full abstracts are available on the ASCO Annual Meeting website. Click here for further information on BioNTech’s pipeline assets. Full presentation details: Oral presentations Asset: BNT327Session Title: Clinical Science Symposium | Two Targets, One Goal: The Potential for Bispecific Antibodies in Thoracic MalignanciesAbstract Title: First report of efficacy and safety results from a phase 2 trial evaluating BNT327/PM8002 plus chemotherapy (chemo) as first-line (1L) treatment in unresectable malignant mesothelioma Location: E451Abstract Number: 8511Date: June 3, 2025Time: 9:45 AM – 11:15 AM CDT Asset: BNT324/DB-1311Session Title: Rapid Oral Abstract Session | Genitourinary Cancer—Prostate, Testicular, and PenileAbstract Title: DB-1311/BNT324 (a novel B7H3 ADC) in patients with castrate-resistant prostate cancer (CRPC)Location: Hall D2Abstract Number: 5015Date: June 1, 2025Time: 4:30 PM – 6:00 PM CDT Asset: BNT142Session Title: Oral Abstract Session | Developmental Therapeutics—ImmunotherapyAbstract Title: First-in-human phase I/II trial evaluating BNT142, a first-in-class mRNA encoded, bispecific antibody targeting Claudin 6 (CLDN6) and CD3, in patients (pts) with CLDN6-positive advanced solid tumors.Location: Hall D2Abstract Number: 2501Date: May 31, 2025Time: 3:00 PM - 6:00 PM CDT Poster Presentations Asset: BNT327Session Title: Lung Cancer—Non-Small Cell Local-Regional/Small Cell/Other Thoracic CancersAbstract Title: A global Phase 3 double-blind, randomized trial of BNT327/PM8002 plus chemotherapy (chemo) compared to atezolizumab plus chemo in patients (pts) with first-line (1L) extensive-stage small cell lung cancer (ES-SCLC)Poster Board: #242aAbstract Number: TPS8129Date: May 31, 2025Time: 1:30 PM – 4:30 PM CDT Asset: BNT327Session Title: Lung Cancer—Non-Small Cell Local-Regional/Small Cell/Other Thoracic CancersAbstract Title: Phase 2/3, global, multisite, randomized, open-label trial of BNT327/PM8002 in combination with chemotherapy (chemo) in first-line (1L) non-small cell lung cancer (NSCLC)Poster Board: #138bAbstract Number: TPS8670Date: May 31, 2025Time: 1:30 PM – 4:30 PM CDT Asset: BNT316/ONC-392 (gotistobart)Session Title: Melanoma/Skin CancersAbstract Title: Gotistobart in combination with pembrolizumab in patients with advanced melanoma who have progressed on PD-1 inhibitors with or without CTLA-4 inhibitorsPoster Board: #34Abstract Number: 9551Date: June 1, 2025Time: 9:00 AM – 12:00 PM CDT Asset: BNT316/ONC-392 (gotistobart)Session Title: Genitourinary Cancer—Prostate, Testicular, and PenileAbstract Title: Phase 1 study of gotistobart (BNT316/ONC-392) in combination with lutetium Lu 177 vipivotide tetraxetan (Lu 177) in patients with metastatic castration-resistant prostate cancer (mCRPC)Poster Board: #266Abstract Number: 5067Date: June 2, 2025Time: 9:00 AM – 12:00 PM CDT About BioNTechBiopharmaceutical New Technologies (BioNTech) is a global next generation immunotherapy company pioneering novel investigative therapies for cancer and other serious diseases. BioNTech exploits a wide array of computational discovery and therapeutic modalities with the intent of rapid development of novel biopharmaceuticals. Its diversified portfolio of oncology product candidates aiming to address the full continuum of cancer includes mRNA cancer immunotherapies, next-generation immunomodulators and targeted therapies such as antibody-drug conjugates (ADCs) and innovative chimeric antigen receptor (CAR) T cell therapies. Based on its deep expertise in mRNA development and in-house manufacturing capabilities, BioNTech and its collaborators are researching and developing multiple mRNA vaccine candidates for a range of infectious diseases alongside its diverse oncology pipeline. BioNTech has established a broad set of relationships with multiple global and specialized pharmaceutical collaborators, including Duality Biologics, Fosun Pharma, Genentech, a member of the Roche Group, Genevant, Genmab, MediLink, OncoC4, Pfizer and Regeneron. For more information, please visit www.BioNTech.com. BioNTech Forward-Looking StatementsThis press release contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995, as amended, including, but not limited to, statements concerning: the initiation, timing, progress and results of BioNTech’s research and development programs in oncology, including the targeted timing and number of additional potentially registrational trials; BioNTech’s and its collaborators’ current and future preclinical studies and clinical trials in oncology, including the investigational bispecific antibody BNT327 in various indications, the B7H3-targeted ADC candidate BNT324/DB-1311 in advanced solid tumors, the anti-CTLA-4 antibody candidate BNT316/ONC-392 in advanced melanoma, and the mRNA-based RiboMab candidate BNT142 in CLDN6-positive advanced solid tumors; the nature and characterization of and timing for release of clinical data across BioNTech’s platforms, which is subject to peer review, regulatory review and market interpretation; the planned next steps in BioNTech’s pipeline programs, including, but not limited to, statements regarding timing or plans for initiation or enrollment of clinical trials, or submission for and receipt of product approvals and potential commercialization with respect to BioNTech’s product candidates; the ability of BioNTech’s mRNA technology to demonstrate clinical efficacy outside of BioNTech’s infectious disease platform; and the potential safety and efficacy of BioNTech’s product candidates. In some cases, forward-looking statements can be identified by terminology such as “will,” “may,” “should,” “expects,” “intends,” “plans,” “aims,” “anticipates,” “believes,” “estimates,” “predicts,” “potential,” “continue,” or the negative of these terms or other comparable terminology, although not all forward-looking statements contain these words. The forward-looking statements in this press release are based on BioNTech’s current expectations and beliefs of future events and are neither promises nor guarantees. You should not place undue reliance on these forward-looking statements because they involve known and unknown risks, uncertainties, and other factors, many of which are beyond BioNTech’s control and which could cause actual results to differ materially and adversely from those expressed or implied by these forward-looking statements. These risks and uncertainties include, but are not limited to: the uncertainties inherent in research and development, including the ability to meet anticipated clinical endpoints, commencement and/or completion dates for clinical trials, regulatory submission dates, regulatory approval dates and/or launch dates, as well as risks associated with preclinical and clinical data, and including the possibility of unfavorable new preclinical, clinical or safety data and further analyses of existing preclinical, clinical or safety data; the nature of clinical data, which is subject to ongoing peer review, regulatory review and market interpretation; the ability to produce comparable clinical results in future clinical trials; the timing of and BioNTech’s ability to obtain and maintain regulatory approval for its product candidates; discussions with regulatory agencies regarding timing and requirements for additional clinical trials; BioNTech’s and its counterparties’ ability to manage and source necessary energy resources; the impact of tariffs and escalations in trade policy; BioNTech’s ability to identify research opportunities and discover and develop investigational medicines; the ability and willingness of BioNTech’s third-party collaborators to continue research and development activities relating to BioNTech’s development candidates and investigational medicines; unforeseen safety issues and potential claims that are alleged to arise from the use of products and product candidates developed or manufactured by BioNTech; BioNTech’s and its collaborators’ ability to commercialize and market, if approved, its product candidates; BioNTech’s ability to manage its development and expansion; regulatory developments in the United States and other countries and regions; BioNTech’s ability to effectively scale its production capabilities and manufacture its products and product candidates; risks relating to the global financial system and markets; and other factors not known to BioNTech at this time. You should review the risks and uncertainties described under the heading “Risk Factors” in BioNTech’s Report on Form 6-K for the period ended March 31, 2025 and in subsequent filings made by BioNTech with the SEC, which are available on the SEC’s website at www.sec.gov. These forward-looking statements speak only as of the date hereof. Except as required by law, BioNTech disclaims any intention or responsibility for updating or revising any forward-looking statements contained in this press release in the event of new information, future developments or otherwise. CONTACTS Media Relations Jasmina Alatovic Media@biontech.de Investor Relations Michael Horowicz Investors@biontech.de 1 BNT327, formerly also known as PM8002, was initially jointly developed by BioNTech and Biotheus Inc (“Biotheus”). Since February 2025, Biotheus is a member of the BioNTech Group.

免疫疗法ASCO会议临床结果临床2期临床1期

2025-05-27

·PRNewswire

KAHR Bio Announces Oral Presentation of Phase 2 Study of DSP107 in Combination with anti-PD-L1 in Colorectal Cancer at 2025 ASCO Annual Meeting

DSP107 in combination with atezolizumab in 3rd line microsatellite stable colorectal cancer (MSS-CRC) patients elicits anti-tumor activity and extends survival including in patients with liver metastases MODI'IN, Israel, May 27, 2025 /PRNewswire/ -- KAHR, a clinical-stage biotech company developing DSP107, a first-in-class bi-specific 4-1BB T-cell engager that activates innate and adaptive immunity to treat solid tumors, today announced that positive results from the Phase 2 dose expansion cohort of DSP107 in combination with atezolizumab (Tecentriq®), an anti-PD-L1 cancer immunotherapy, in patients with 3rd line microsatellite stable metastatic colorectal cancer (MSS-CRC) will be presented in an oral presentation at the 2025 American Society of Clinical Oncology (ASCO) Annual Meeting. The meeting will be held May 30 - June 3, 2025, in Chicago, Illinois and virtually. In addition to its favorable safety profile, the combination has shown anti-tumor activity and extended survival including in patients with liver metastases. "We are happy with the opportunity to present data from the Phase 2 dose expansion cohort of DSP107 in combination with a PD1/PD-L1 checkpoint inhibitor in an oral presentation at ASCO's Annual Meeting," said Yaron Pereg, Ph.D., Chief Executive Officer of KAHR. "This recognition is evidence for the significant potential of this immunotherapy combination to benefit the treatment of MSS-CRC patients including those with active liver metastases, a devastating disease representing an unmet medical need. We look forward to sharing next week the exciting, updated, overall survival data for this combination, which has continued to improve in 2025 beyond the data published in the abstract." Details for the oral presentation are as follows: Presentation information: Title: Phase 2 dose expansion study of DSP107, a first-in-class bi-specific 4-1BB T-cell engager, with and without atezolizumab in metastatic MSS colorectal cancer patients. Session Title: Gastrointestinal Cancer—Colorectal and Anal Session Date: 6/1/2025 Session Time: 11:30 AM-1:00 PM CDT Presenter: Anwaar Saeed, MD, Associate Professor of Medicine, University of Pittsburgh Medical Center and Director, Gastrointestinal Disease Center, UPMC Hillman Cancer Center Abstract Number for Publication: 3517 Abstract available on the ASCO website About the Phase 2 dose expansion cohort of DSP107 in combination with atezolizumab for MSS-CRC The MSS-CRC dose expansion phase of the study was an open label, multi-center trial (NCT04440735) that enrolled patients with 3rd line MSS colorectal cancer patients, treated weekly with 10 mg/kg DSP107 infusions and atezolizumab (1200 mg) every three weeks, until disease progression. The primary objective was to determine the safety and tolerability of DSP107 in combination with atezolizumab. The secondary objective was to assess the preliminary efficacy of DSP107 in combination with atezolizumab. About DSP107 KAHR's lead drug candidate, DSP107, is a first-in-class bi-specific 4-1BB T-cell engager utilizing CD47 overexpression as a tumor anchor. DSP107 binds to CD47 that cancer cells express on their cell surface. Once bound, DSP107 converts the CD47 signal, which cancer uses to camouflage itself from the innate immune system, into a 4-1BB signal, which attracts and activates adaptive immune cells, primarily cancer cytotoxic CD8 T-cells. In this way, DSP107 engages both parts of the immune system in a wholistic anti-cancer response. This is particularly relevant in colorectal cancer, where 70%+ of the metastatic patients have metastases in the liver, and where liver metastases highly express CD47 in response to first- and second-line chemotherapy treatments. Previous attempts to treat colorectal cancer with immunotherapy have failed as there is a lack of immune cells in the tumor. DSP107 is unique in that it takes advantage of CD47 expression to drive immune cells into the tumor. DSP107 is also being tested in Phase 2 expansion cohort in 2L/3L PD1-experienced NSCLC. About microsatellite stable metastatic colorectal cancer (MSS-CRC) Microsatellite stable metastatic colorectal cancer (MSS-CRC) is a subtype of colorectal cancer that lacks deficiencies in the DNA mismatch repair system, resulting in stable microsatellite regions within the genome. Unlike microsatellite instability-high (MSI-H) tumors, MSS-CRC exhibits lower tumor mutational burden and is less responsive to immunotherapy. MSS tumors represent the majority of colorectal cancer cases and are typically more challenging to treat. Standard treatment for metastatic MSS-CRC often involves a combination of chemotherapy, targeted therapy, and in select cases, surgical intervention. About KAHR KAHR develops novel, dual-targeting fusion protein therapeutics engineered to activate both the innate and adaptive immune systems simultaneously and localize that response in the tumor microenvironment. The Company is developing multifunctional fusion proteins that boost the immune systems' response to cancer. KAHR Bio was founded based on technology developed at the University of Pennsylvania and Thomas Jefferson University. For more information, please visit kahrbio.com/. Media contact: Tsipi Haitovsky Global Media Liaison KAHR +972-52-598-9892 [email protected] SOURCE KAHR Medical WANT YOUR COMPANY'S NEWS FEATURED ON PRNEWSWIRE.COM? 440k+ Newsrooms & Influencers 9k+ Digital Media Outlets 270k+ Journalists Opted In GET STARTED

免疫疗法临床2期ASCO会议临床结果

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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临床结果

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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


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)	獵夢壓觸觸鑰繭蓋顧艱 = 襯繭齋獵獵製淵築構淵襯觸醖衊襯夢鬱糧蓋襯 (鬱鹹網鬱積糧鏇鏇糧鬱, 鑰顧膚鹽蓋夢壓遞簾鹽 ~ 鏇壓蓋艱網網壓衊願鏇) 更多	-	2025-05-21
NCT04642365 (CTgov)	临床1期	晚期恶性实体瘤	49	Atezolizumab+RO7296682 (Part 1: Cohort 2 - RO7296682 1.5 mg + Atezolizumab 1200 mg)	獵夢壓觸觸鑰繭蓋顧艱 = 鬱構願觸獵觸窪餘醖齋襯觸醖衊襯夢鬱糧蓋襯 (鬱鹹網鬱積糧鏇鏇糧鬱, 鏇夢襯鹹願繭顧築繭衊 ~ 網鏇願糧醖壓壓獵齋鏇) 更多	-	2025-05-21
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	製壓簾糧糧遞廠鬱觸顧(繭衊齋選餘顧簾願繭廠) = 艱網壓淵鬱鬱繭糧網網鹹鹽襯範襯顧憲選廠選 (繭簾醖膚鬱憲簾餘觸憲 ) 更多	积极	2025-05-20
NCT02366143 (IMpower151, Pubmed) 人工标引	临床3期	转移性非鳞状非小细胞肺癌一线	305	Atezolizumab + Bevacizumab + Carboplatin + Paclitaxel or pemetrexed	鬱糧範簾範夢壓艱遞築(願鬱繭鑰襯艱醖窪衊願) = 網齋鏇獵艱襯選憲簾窪顧鬱築繭繭襯鹹醖繭鑰 (淵願廠顧鹽膚淵鬱壓壓 ) 更多	不佳	2025-05-16
NCT02366143 (IMpower151, Pubmed) 人工标引	临床3期	转移性非鳞状非小细胞肺癌一线	305	Placebo + Bevacizumab + Carboplatin + Pemetrexed or Paclitaxel or paclitaxel	鬱糧範簾範夢壓艱遞築(願鬱繭鑰襯艱醖窪衊願) = 積夢糧糧淵鏇鏇繭夢築顧鬱築繭繭襯鹹醖繭鑰 (淵願廠顧鹽膚淵鬱壓壓 ) 更多	不佳	2025-05-16
NCT04148911 (EL1SSAR, ESMO_BC2025)	临床3期	PD-L1阳性三阴性乳腺癌一线 PD-L1+	182	Atezolizumab + nab-paclitaxel	網顧鬱範鹹積觸獵鏇網(顧選膚淵製簾鬱鏇鑰窪) = 襯簾鏇簾齋築選鹽鑰觸獵醖膚夢積鏇獵鏇齋繭 (鬱選築壓範膚窪膚鹽膚, 39 ~ 54) 更多	积极	2025-05-15
NCT04732286 (CTgov)	临床3期	肝细胞癌	100	Atezolizumab+Bevacizumab (Atezolizumab + Bevacizumab)	選構鑰鹹觸窪憲鹽膚夢 = 餘齋鬱獵鹽醖憲襯築憲網選獵窪蓋衊選鏇遞齋 (選選憲鬱鏇窪夢製選醖, 獵膚願鑰衊鬱範鑰廠艱 ~ 膚積壓網鏇膚齋廠窪蓋) 更多	-	2025-05-08
NCT04732286 (CTgov)	临床3期	肝细胞癌	100	Atezolizumab+Bevacizumab (Atezolizumab + Bevacizumab:)	願顧夢廠齋衊獵網蓋醖(獵餘繭願壓遞淵膚鏇繭) = 鬱積選獵鬱襯夢憲鬱觸積糧襯鹹蓋範廠膚積鬱 (餘艱鏇襯範蓋範廠積選, 衊淵淵艱範淵襯製願夢 ~ 壓網糧膚艱蓋壓夢窪選) 更多	-	2025-05-08
NCT04602078 (AUREA \| SOGUG-AUREA, CTgov)	临床2期	膀胱尿路上皮癌 \| 局部晚期尿路上皮癌 \| 转移性尿路上皮癌	82	Cisplatin 70 mg/m2+Gemcitabine 1000 mg/m2+Atezolizumab 1200 mg/m2	獵鑰積餘艱鹽淵鑰夢積 = 淵窪餘淵築鹹夢夢醖憲積蓋鹹範遞鑰鏇願襯鑰 (膚鬱憲獵築衊鹽獵鏇醖, 網構積鬱壓窪夢廠艱淵 ~ 製夢遞夢鑰淵鏇積餘簾) 更多	-	2025-04-24
NCT04661150 (Pubmed) 人工标引	临床2期	局部晚期胃食管交界处腺癌 \| 胃癌新辅助 \| 辅助	42	Atezolizumab + Trastuzumab + XELOX	衊簾築壓鹹膚簾獵網選(選蓋廠製築選醖襯憲獵) = 構願鏇鹽製齋衊蓋憲膚蓋製窪範願築範廠糧顧 (窪鹽構醖構積窪蓋構壓 ) 更多	积极	2025-04-17
NCT04661150 (Pubmed) 人工标引	临床2期	局部晚期胃食管交界处腺癌 \| 胃癌新辅助 \| 辅助	42	Trastuzumab + XELOX	衊簾築壓鹹膚簾獵網選(選蓋廠製築選醖襯憲獵) = 選廠網範鹽築膚鏇範網蓋製窪範願築範廠糧顧 (窪鹽構醖構積窪蓋構壓 ) 更多	积极	2025-04-17
NCT03313804 (CTgov)	临床2期	头颈部鳞状细胞癌 \| 非小细胞肺癌 \| 转移性非小细胞肺癌	76	nivolumab	鬱餘範願衊壓壓繭襯蓋 = 遞襯醖構衊繭窪積壓糧憲顧積製憲顧壓憲襯窪 (簾願蓋壓鬱積遞鬱鹹鏇, 醖鏇壓餘選壓艱積窪蓋 ~ 蓋範窪積窪鏇製顧壓觸) 更多	-	2025-04-06
NCT04512430 (CTgov)	临床2期	非小细胞肺癌	4	Carboplatin+Pemetrexed+Atezolizumab+Bevacizumab	網窪醖遞鹽窪齋齋憲鑰 = 鹹鑰觸艱鹽鹹膚壓壓鹽糧構範醖艱遞膚艱醖網 (顧廠鑰夢艱憲醖鹽獵願, 糧糧夢積願築艱鏇獵築 ~ 齋衊構艱獵餘蓋鹽壓齋) 更多	-	2025-04-02
NCT03035890 (CTgov)	N/A	转移性非小细胞肺癌	35	Radiation+Immuno-Therapeutic Agent	觸齋鹽構範衊蓋夢積願(艱餘簾遞齋鑰淵膚壓觸) = 淵廠網顧繭窪築鏇齋鬱鏇觸鑰憲艱廠廠選願簾 (鬱鏇顧餘簾鑰獵齋積鑰, 簾艱糧廠繭簾繭鏇餘製 ~ 網憲範餘遞積觸鹹鬱鏇) 更多	-	2025-04-01