A Phase 1b/2a, Double-blind, Placebo-controlled, Three Arm, Randomized Study Evaluating a Single Intravenous Push Followed by a Continuous Infusion of Certepetide Over 4 Hours When Added to Standard of Care (SoC) Versus Two Intravenous Pushes of Certepetide When Added to SoC, Versus SoC Alone in Subjects With Previously Untreated Metastatic Pancreatic Ductal Adenocarcinoma (FORTIFIDE)

The goal of this clinical trial is to test a new drug plus standard treatment compared with standard treatment alone in people with metastatic pancreatic ductal adenocarcinoma.
The main questions it aims to answer are:
* is the new drug plus standard treatment safe and tolerable
* is the new drug plus standard treatment more effective than standard treatment
Participants will:
* Visit the clinic three times every 28 days for treatment and tests
* Have CT or MRI scans every 8 weeks while on treatment

开始日期2030-01-01

申办/合作机构

Lisata Therapeutics, Inc.

NCT07365306

/ Not yet recruiting临床2期IIT

A Phase 2 Study of Epcoritamab-R-GemOx With Consolidative ASCT and Additional Epcoritamab in Relapsed/Refractory Transplant-Eligible DLBCL

This phase II trial tests how well epcoritamab in combination with rituximab, gemcitabine and oxaliplatin (R-GemOx) works as treatment given after the cancer has not responded to other treatments (salvage therapy) before autologous stem cell transplant in treating patients with diffuse large B-cell lymphoma (DLBCL) that has come back after a period of improvement (relapsed) or that does not respond to treatment (refractory). Epcoritamab is a so-called bispecific antibody, a molecule that can bind simultaneously to two different receptors (proteins present on the cell surface). Epcoritamab binds to a receptor called CD3 with one part of the antibody and to a receptor called CD20 with another part of the antibody. CD3 is expressed on T cells, which are important cells of the immune system that help the body fight cancers and infections. CD20 is expressed on the surface of DLBCL cells. By simultaneous binding to CD3 and CD20, epcoritamab brings T cells and DLBCL cells close together and activates the T cells to kill the lymphoma cells. Rituximab is a so-called monoclonal antibody, a molecule that binds to a single receptor. Like epcoritamab, rituximab binds to CD20. After binding to CD20, rituximab activates the immune system to kill the lymphoma cell through several different mechanisms. Gemcitabine is a chemotherapy drug that blocks the cells from making DNA and may kill cancer cells. Oxaliplatin is in a class of medications called platinum-containing antineoplastic agents. It damages the cell's DNA and may kill cancer cells. Giving epcoritamab-R-GemOx as therapy before an autologous stem cell transplant may help kill cancer cells in the body and help make room in the patient's bone marrow for new blood-forming cells (stem cells) to grow.

开始日期2026-12-30

申办/合作机构

City of Hope National Medical Center

[+1]

NCT07275216

/ Not yet recruiting临床2期IIT

Phase 2 Study of Pembrolizumab With Chemotherapy in Frail Patients With Newly Diagnosed Classical Hodgkin Lymphoma

This phase II trial tests how well pembrolizumab in addition to chemotherapy (gemcitabine, brentuximab vedotin, and dacarbazine) works in treating frail patients with newly diagnosed Hodgkin lymphoma who aren't candidates for standard anthracycline-based treatment. Immunotherapy with monoclonal antibodies, such as pembrolizumab, may help the body's immune system attack the cancer, and may interfere with the ability of cancer cells to grow and spread. Gemcitabine is a chemotherapy drug that blocks the cells from making deoxyribonucleic acid (DNA) and may kill cancer cells. Brentuximab vedotin is in a class of medications called antibody-drug conjugates. It is made of a monoclonal antibody called brentuximab that is linked to a cytotoxic agent called vedotin. Brentuximab attaches to CD30 positive lymphoma cells in a targeted way and delivers vedotin to kill them. Dacarbazine is in a class of medications called alkylating agents. It works by damaging the cell's DNA and may kill cancer cells and slow down or stop cancer growth. Pembrolizumab in combination chemotherapy may be a safe and effective alternative treatment option for frail patients with Hodgkin lymphoma who can't receive standard anthracycline-based treatment.

开始日期2026-07-01

申办/合作机构

City of Hope National Medical Center

[+1]

100 项与盐酸吉西他滨相关的临床结果

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100 项与盐酸吉西他滨相关的转化医学

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100 项与盐酸吉西他滨相关的专利（医药）

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11,963

项与盐酸吉西他滨相关的文献（医药）

2026-12-31·JOURNAL OF MEDICAL ECONOMICS

Budget impact model of nadofaragene firadenovec for the treatment of high-risk non-muscle-invasive bladder cancer that is unresponsive to Bacillus Calmette-Guérin immunotherapy

Article

作者: Ye, Dongni ; Yang, Min ; Chai, Xinglei ; Moradi, Ashton ; Zhao, Angela ; Lotan, Yair

AIMS:

To estimate the budget impact of adopting nadofaragene firadenovec for the treatment of adults with high-risk, Bacillus Calmette-Guérin (BCG)-unresponsive non-muscle-invasive bladder cancer (NMIBC) with carcinoma in situ with or without papillary tumors (CIS ± Ta/T1) from a US third-party payer's perspective.

METHODS:

A budget impact model was developed to compare total healthcare costs under two scenarios: (1) with nadofaragene firadenovec included in the treatment mix, and (2) without it. The model simulated a hypothetical US health plan covering one million members over a 3-year time horizon. Costs assessed included drug acquisition and administration, surveillance and disease management, cystectomy, and treatment-related adverse events (AEs). Base-case inputs were informed by trial data, published literature, and real-world evidence. Scenario analyses explored alternative population definitions, epidemiology and clinical inputs; one-way sensitivity analyses tested parameter uncertainty.

RESULTS:

In the base-case, the estimated per-member-per-month (PMPM) budget impact of adopting nadofaragene firadenovec ranged from $0.0010 in Year 1 to $0.0084 in Year 3. Increased drug and administration costs were partially offset by cost savings from reduced disease progression, fewer cystectomies, and lower AE rates. Scenario analyses demonstrated that even examining a broader population including papillary disease-only patients, the budget impact remained modest ($0.0064-$0.0548 PMPM from Years 1-3). Sensitivity analyses confirmed that results were most influenced by uptake rate, drug cost, and target population size.

LIMITATIONS:

Key limitations include reliance on projected market shares for nadofaragene firadenovec, omission of recently approved treatments (nogapendekin alfa inbakicept-pmln and TAR-200) due to the lack of publicly available market share data, and assumptions to derive clinical outcomes for certain treatments due to lack of reported data.

CONCLUSIONS:

Despite its higher acquisition cost, the inclusion of nadofaragene firadenovec resulted in a minimal budget impact as bladder-sparing option for patients with BCG-unresponsive NMIBC with CIS ± Ta/T1.

2026-02-24·CURRENT TOPICS IN MEDICINAL CHEMISTRY

An Expedition of FDA-Approved Anticancer Drugs in 2024: Synthetic Routes, Mechanisms of Action, and Clinical Indications.

Article

作者: Kurmi, Balak Das ; Priya, Sakshi ; Soni, Reena ; Cherian, Issac V ; Kasana, Shivani ; Islam, Md Mustahidul ; Das, Km Supriya ; Patel, Preeti

The year 2024 witnessed significant advancements in cancer therapy, with the U.S. Food and Drug Administration (FDA) approving 56 anticancer drugs for various malignancies. These approvals encompass 36 organic small molecules and 20 macromolecular monoclonal antibody conjugates, each with distinct mechanisms of action targeting key oncogenic pathways. Among the small molecules, kinase inhibitors such as Ribociclib, Imatinib Mesylate, and Nilotinib Hydrochloride Dihydrate modulate critical signaling cascades, while antimetabolites like Fluorouracil and Pemetrexed Disodium disrupt nucleotide biosynthesis. Other classes include DNA-damaging agents (Mitomycin, Gemcitabine Hydrochloride), immune modulators (Pomalidomide, Lenalidomide), and hormonal antagonists (Abiraterone Acetate, Erleada). The macromolecular therapeutics primarily consist of monoclonal antibody-based agents, such as Keytruda, Tecentriq, and Imfinzi, which enhance immune checkpoint inhibition, and antibody-drug conjugates like Enhertu and Elahere, which deliver cytotoxic payloads with high specificity. This review systematically examines the chemical synthesis, mechanisms of action, and therapeutic indications of these FDAapproved agents, emphasizing their role in improving patient outcomes. By analyzing their structural frameworks and biological targets, we aim to provide insights into current trends in anticancer drug development and potential future directions.

2026-01-01·MOLECULAR BIOTECHNOLOGY

Exploring the Effects of Opioid-Related Drugs on the Clinical Outcome of Prostate Cancer Patients Via Integrated Bioinformatics Analysis

Article

作者: Zhang, Yunxuan ; Cao, Qi ; Miao, Qi ; Liu, Yuenan ; Zhang, Xiaoping ; Chen, Kailei

Opioids are the primary regimens for perioperative analgesia with controversial effects on oncological survival. The underlying mechanism remains unexplored. This study developed survival-related gene co-expression networks based on RNA-seq and clinical characteristics from TCGA cohort. Two survival-related networks were identified, and drug-induced transcriptional profiles were predicted. Immune cell infiltration algorithm, least absolute shrinkage and selection operator (LASSO) regression, and cox proportional models were executed to explore the correlation between opioid-related drugs and prostate cancer patient prognosis. The opioid receptor agonists, represented by tramadol, were evidenced for anti-survival effects on prostate cancer by facilitating the DNA replication and cell cycle, and immune cell infiltration. Conversely, opioid receptor antagonists showed pro-survival effects. A novel prognostic model containing CNIH2, MCCC1, and Gleason scores was established and validated in two independent cohorts. This study revealed opioids' effect on prostate cancer progression, and provided a novel model to predict these regulations in clinical outcomes.

1,320

项与盐酸吉西他滨相关的新闻（医药）

2026-03-20

·医脉通消化系统肿瘤

临研情报局｜研值在线！春启新程：3月肝胆胰肿瘤领域创新疗法蓄势待发，破局之路曙光初现

3月份新启动肝胆胰肿瘤领域临床研究最新动态火热出炉！速戳【临研情报局】获取独家情报，先登科研最前沿！肝癌情报A NCT号 NCT07463248 研究分期 II期研究方案 PULSAR+粪便微生物移植纳入人数 64 最近更新时间 2026-03-11 ( 研究亮点 ) 个性化放疗；点击获取情报研究标题：Building Evidence for Ablative Internal Radiation Therapy in Localized HCC Beyond the Up-To-7 Criteria (BEAT-UT7) 中文标题：为超出 Up-to-7 标准的局部 HCC 消融性内部放射治疗建立证据（BEAT-UT7）研究别名：BEAT-UT7 主要研究终点：据mRECIST评估的ORR 发起机构：首尔大学医院研究状态：尚未招募更新时间：2025-01-14 主要完成时间：2027-12-31 预计完成时间：2029-12-31 点击获取情报研究标题：PULSAR Combined With Fecal Microbiota Transplantation for Advanced Hepatocellular Carcinoma Progressing After First-Line Targeted-Immunotherapy 中文标题：PULSAR联合粪便微生物移植治疗一线靶向-免疫治疗后进展的晚期肝细胞癌的研究主要研究终点：PFS 发起机构：华西医院研究状态：尚未招募研究开始时间：2026-03-05 主要完成时间：2028-01-31 预计完成时间：2029-01-31 情报B NCT07422753 NCT号 II期研究分期 TACE+信迪利单抗+贝伐珠单抗+伊匹木单抗N01 研究方案 36 纳入人数 2026-02-20 最近更新时间 ( 研究亮点 ) 靶免联合；局部联合系统治疗；点击获取情报研究标题：Continuation of First-line Therapy with Radiotherapy Versus Early Switch to Second-line Therapy in Oligoprogressive HCC 中文标题：在寡进展性 HCC 中继续一线治疗放疗对比早期转为二线治疗研究别名：SDZLEC2025-025-02 主要研究终点：PFS 发起机构：山东省肿瘤医院研究状态：招募中更新时间：2025-03-11 主要完成时间：2027-03-15 预计完成时间：2028-03-15 点击获取情报研究标题：A Prospective, Randomized Study of TACE Combined With Sintilimab, Bevacizumab, and Ipilimumab N01 Treating Advanced HCC 中文标题：TACE联合信迪利单抗、贝伐珠单抗及伊匹木单抗N01治疗晚期肝细胞癌的前瞻性、随机对照研究主要研究终点：ORR 发起机构：浙江大学医学院附属第二医院研究状态：尚未招募研究开始时间：2026-03 主要完成时间：2027-03 预计完成时间：2029-03 情报C NCT号 NCT07413354 研究分期 II期研究方案替雷利珠单抗+槐耳颗粒纳入人数 94 最近更新时间 2026-02-17 ( 研究亮点 ) 中西医结合；点击获取情报研究标题：Building Evidence for Ablative Internal Radiation Therapy in Localized HCC Beyond the Up-To-7 Criteria (BEAT-UT7) 中文标题：为超出 Up-to-7 标准的局部 HCC 消融性内部放射治疗建立证据（BEAT-UT7）研究别名：BEAT-UT7 主要研究终点：据mRECIST评估的ORR 发起机构：首尔大学医院研究状态：尚未招募更新时间：2025-01-14 主要完成时间：2027-12-31 预计完成时间：2029-12-31 点击获取情报研究标题：Tislelizumab Combined With Huaier Granule as First-line Treatment for Unresectable Hepatocellular Carcinoma 中文标题：替雷利珠单抗联合槐耳颗粒作为不可切除肝细胞癌一线治疗的研究主要研究终点：ORR 发起机构：同济医院研究状态：正在招募研究开始时间：2026-03-01 主要完成时间：2027-03-31 预计完成时间：2027-12-30 情报D NCT07392866 NCT号 II/III期研究分期 SH006+贝伐珠单抗+化疗 vs. SH006+贝伐珠单抗 vs. SH006+化疗 vs. 瑞戈非尼研究方案 120 纳入人数 2026-02-09 最近更新时间 ( 研究亮点 ) TIGIT/PD-L1双特异性抗体；点击获取情报研究标题：Continuation of First-line Therapy with Radiotherapy Versus Early Switch to Second-line Therapy in Oligoprogressive HCC 中文标题：在寡进展性 HCC 中继续一线治疗放疗对比早期转为二线治疗研究别名：SDZLEC2025-025-02 主要研究终点：PFS 发起机构：山东省肿瘤医院研究状态：招募中更新时间：2025-03-11 主要完成时间：2027-03-15 预计完成时间：2028-03-15 点击获取情报研究标题：A Clinical Study of SH006 Injection in Combination Therapy Versus Regorafenib in the Treatment of Advanced Hepatocellular Carcinoma 中文标题：SH006注射液联合治疗对比瑞戈非尼治疗晚期肝细胞癌的临床研究主要研究终点：PFS、AEs（II期）、OS（III期）发起机构：南京圣和药业股份有限公司研究状态：尚未招募研究开始时间：2026-03-01 主要完成时间：2030-03-01 预计完成时间：2030-03-01 情报E NCT号 NCT07291076 研究分期 I/II期研究方案 Pumitamig±伊匹木单抗纳入人数 129 最近更新时间 2026-03-04 ( 研究亮点 ) PD-L1/VEGF-A双特异性抗体；点击获取情报研究标题：A Prospective Study of Cadonilimab or PD-1 Inhibitor in Hepatocellular Carcinoma After Radical Surgery with High Risk of Recurrence 中文标题：Cadonilimab 或 PD-1 抑制剂治疗复发风险高的根治性肝细胞癌的前瞻性研究研究别名：PREVENT-3 主要研究终点：PFS 发起机构：广西医科大学研究状态：尚未招募更新时间：2025-03-06 主要完成时间：2025-12-31 预计完成时间：2025-12-31 点击获取情报研究标题：A Study to Evaluate the Safety and Tolerability of Pumitamig Alone or In Combination With Ipilimumab in Participants With First-Line Advanced or Unresectable Hepatocellular Carcinoma (HCC) (ROSETTA HCC-206) 中文标题：评估Pumitamig单药或联合伊匹木单抗治疗一线晚期或不可切除肝细胞癌（HCC）安全性与耐受性的研究（ROSETTA HCC-206）主要研究终点：AEs、DLT、肿瘤缓解发起机构：Bristol-Myers Squibb 研究状态：正在招募研究开始时间：2026-03-31 主要完成时间：2029-10-15 预计完成时间：2031-10-14 胆道癌情报F NCT07450976 NCT号 II期研究分期 SHR-A1904 研究方案 151 纳入人数 2026-03-12 最近更新时间 ( 研究亮点 ) CLDN18.2 ADC；点击获取情报研究标题：A Study of SHR-A1904 in Previous Systemic Treatment Failed Biliary Tract Cancer 中文标题：SHR-A1904用于既往系统性治疗失败的胆管癌患者的临床研究主要研究终点：ORR 发起机构：苏州盛迪亚生物医药有限公司研究状态：尚未招募研究开始时间：2026-03 主要完成时间：2030-12 预计完成时间：2030-12 胰腺癌情报G NCT号 NCT07469956 研究分期 II期研究方案 Surufatinib+特瑞普利单抗+mFOLFIRINOX 纳入人数 30 最近更新时间 2026-03-13 ( 研究亮点 ) 降期转化；三联方案；点击获取情报研究标题：Surufatinib Plus mFOLFIRINOX and PD-1 Inhibitor as the Neoadjuvant Therapy for High-risk or Borderline Resectable Pancreatic Cancer 中文标题：Surufatinib联合mFOLFIRINOX方案及PD-1抑制剂用于高危或交界可切除胰腺癌的新辅助治疗主要研究终点：EFS 发起机构：中山大学研究状态：尚未招募研究开始时间：2026-03-31 主要完成时间：2028-01-31 预计完成时间：2029-01-31 情报H NCT07450859 NCT号 II期研究分期 BT5528 研究方案 39 纳入人数 2026-03-05 最近更新时间 ( 研究亮点 ) 靶向EphA2的双环肽偶联毒素药物；点击获取情报研究标题：A Study of BT5528 in Patients With Metastatic Pancreatic Ductal Adenocarcinoma (PDAC) 中文标题：BT5528在转移性胰腺导管腺癌患者中的研究主要研究终点：ORR 发起机构：BicycleTx Limited 研究状态：正在招募研究开始时间：2026-03 主要完成时间：2029-03 预计完成时间：2029-05 情报I NCT号 NCT07444541 研究分期 I/II期研究方案 ANO31905+纳米颗粒白蛋白结合紫杉醇+吉西他滨纳入人数 84 最近更新时间 2026-03-03 ( 研究亮点 ) CLDN18.2靶向ADC；点击获取情报研究标题：A Prospective Study of Cadonilimab or PD-1 Inhibitor in Hepatocellular Carcinoma After Radical Surgery with High Risk of Recurrence 中文标题：Cadonilimab 或 PD-1 抑制剂治疗复发风险高的根治性肝细胞癌的前瞻性研究研究别名：PREVENT-3 主要研究终点：PFS 发起机构：广西医科大学研究状态：尚未招募更新时间：2025-03-06 主要完成时间：2025-12-31 预计完成时间：2025-12-31 点击获取情报研究标题：ANO31905 in Combination With Chemotherapy for CLDN18.2-Positive Locally Advanced Unresectable or Metastatic Pancreatic Cancer 中文标题：ANO31905联合化疗治疗CLDN18.2阳性局部晚期不可切除或转移性胰腺癌的研究主要研究终点：DLT 发起机构：Anova Innovation Limited 研究状态：尚未招募研究开始时间：2026-03 主要完成时间：2027-08 预计完成时间：2028-12 情报J NCT07214298 NCT号 I/II期研究分期 Pegcetacoplan+改良FOLFIRINOX 研究方案 35 纳入人数 2026-02-06 最近更新时间 ( 研究亮点 ) C3靶向抑制剂；点击获取情报研究标题：Pegcetacoplan in Combination With Modified FOLFIRINOX for the Treatment of Metastatic Pancreatic Ductal Adenocarcinoma 中文标题：Pegcetacoplan联合改良FOLFIRINOX方案治疗转移性胰腺导管腺癌的研究主要研究终点：AE（I期）、PFS（II期）发起机构：Roswell Park Cancer Institute 研究状态：正在招募研究开始时间：2026-03-01 主要完成时间：2027-10-01 预计完成时间：2028-10-01 情报K NCT号 NCT06904378 研究分期 I/II期研究方案 ONT01+吉西他滨+白蛋白结合型紫杉醇纳入人数 61 最近更新时间 2026-02-17 ( 研究亮点 ) 新型药物；点击获取情报研究标题：A Prospective Study of Cadonilimab or PD-1 Inhibitor in Hepatocellular Carcinoma After Radical Surgery with High Risk of Recurrence 中文标题：Cadonilimab 或 PD-1 抑制剂治疗复发风险高的根治性肝细胞癌的前瞻性研究研究别名：PREVENT-3 主要研究终点：PFS 发起机构：广西医科大学研究状态：尚未招募更新时间：2025-03-06 主要完成时间：2025-12-31 预计完成时间：2025-12-31 点击获取情报研究标题：ONT01 and Gemcitabine/Nab-paclitaxel as Second Line Therapy for Metastatic Pancreatic Ductal Adenocarcinoma 中文标题：ONT01联合吉西他滨/白蛋白紫杉醇作为转移性胰腺导管腺癌二线治疗的研究主要研究终点：RP2D、DLTs 发起机构：Washington University School of Medicine 研究状态：尚未招募研究开始时间：2026-03-31 主要完成时间：2028-09-30 预计完成时间：2029-09-30 情报解读三月，肝胆胰肿瘤领域迎来多项重要研究进展。肝癌领域，局部联合系统治疗模式持续优化，PULSAR联合粪便微生物移植探索克服靶向-免疫耐药新机制；TACE联合信迪利单抗、贝伐珠单抗及伊匹木单抗的方案、替雷利珠单抗联合槐耳颗粒的中西医结合策略、以及SH006注射液联合方案对比瑞戈非尼的头对头研究，均体现了治疗策略的多元化探索；Pumitamig±伊匹木单抗用于一线治疗的研究则探索了免疫治疗2.0时代的新方向。胆道癌领域，SHR-A1904用于系统性治疗失败患者的研究为后线治疗带来新希望。在胰腺癌领域，新辅助治疗探索持续深入，索凡替尼联合mFOLFIRINOX及PD-1抑制剂用于高危或交界可切除胰腺癌的研究有望优化手术转化策略；针对转移性患者，BT5528、ANO31905等新型靶向药物联合化疗的研究相继启动，Pegcetacoplan联合改良FOLFIRINOX、ONT01联合吉西他滨/白蛋白紫杉醇等创新组合为后线治疗提供了新思路。期待这些研究能够早日公布结果，为肝胆胰肿瘤患者带来更多生存获益。撰写：Aurora 审核：Aurora 排版：Aurora 执行：Aurora 医脉通是专业的在线医生平台，“感知世界医学脉搏，助力中国临床决策”是平台的使命。医脉通旗下拥有「临床指南」「用药参考」「医学文献王」「医知源」「e研通」「e脉播」等系列产品，全面满足医学工作者临床决策、获取新知及提升科研效率等方面的需求。本平台旨在为医疗卫生专业人士传递更多医学信息。本平台发布的内容，不能以任何方式取代专业的医疗指导，也不应被视为诊疗建议。如该等信息被用于了解医学信息以外的目的，本平台不承担相关责任。本平台对发布的内容，并不代表同意其描述和观点。若涉及版权问题，烦请权利人与我们联系，我们将尽快处理。

放射疗法临床2期临床结果

2026-03-20

·药康生物GemPharmatech

自发肿瘤模型：肿瘤研究的“天然利器”

自发肿瘤模型区别于诱导模型和移植瘤模型，凭借其独特的生物学特性，成为肿瘤研究中不可替代的工具。其核心优势集中体现在四点：完整肿瘤微环境（TME）：保留肿瘤与周围基质、免疫细胞的天然相互作用，更贴近临床肿瘤发生发展的真实场景，为肿瘤微环境相关研究（如CAF、TAM调控）提供精准载体。精准模拟转移与复发：可自然发生肿瘤转移与复发过程，是研究肿瘤侵袭转移机制、评估长期治疗响应的理想模型。特异性靶基因突变：模型携带明确的原癌基因（KRAS、MYC等）或抑癌基因（p53、APC等）突变，精准匹配人类肿瘤基因特征。原代细胞可提取：为后续体外机制研究、细胞系构建提供充足的优质样本。药康生物作为专注于实验动物模型研发与技术服务的国家高新技术企业，长期致力于自发肿瘤模型的系统构建与应用研究。公司已建立覆盖常见肿瘤类型的自发模型资源库，为肿瘤发生机制解析、药物筛选及临床前药效评价提供关键技术支撑。自发肿瘤模型及应用胰腺癌 1. B6-KPC小鼠：先构建B6-KP小鼠模型，然后B6-KP和Pdx1-Cre配繁获得B6-KPC，KPC小鼠在10周龄时可发展为胰腺导管癌。图1. B6-KPC构建策略图图2. B6-KPC病理检测图如图2所示，B6-KPC 8-10周龄表现为腺泡-导管化生及胰腺上皮内瘤变( PanIN )，12-16周龄发生浸润性胰腺导管腺癌。 2. mPA-KPC模型：为破解传统KPC模型成瘤慢、监测难的痛点，建立mPA-KPC及其荧光标记细胞系，可实现肿瘤生长动力学精准追溯，为体内药效评估提供可靠工具。图3. C57BL/6接种PA-KPC细胞系后抗肿瘤药物药效数据图3结果显示，联合用药方案可实现最高77.74%的肿瘤生长抑制（TGI），助力提升药效验证准确性。图4. C57BL/6接种mPA-KPC-Luciferase细胞系后药物治疗的肿瘤负荷影像图图4结果显示，Gemcitabine+anti-CD40 药物联用具有更好的抗肿瘤效果。乳腺癌 1. FVB-MMTV-PyMT模型：通过MMTV驱动多瘤病毒中间T抗原（PyMT）癌基因在乳腺中高表达，诱发乳腺上皮细胞中PyMT基因的表达失控，进而诱发细胞的恶性增殖，导致乳腺癌发生。图5. MMTV-PyMT病理检测图图5A显示，雌鼠6周龄发展为乳腺癌，并出现肺、卵巢及唾液腺转移；图5B显示，雄鼠6周龄部分发展为乳腺癌，并出现唾液腺转移。 2. FVB-MMTV-PyMT应用于药物药效筛选图6. MMTV-PyMT药效数据（合作验证数据）第三方合作数据显示，PD-L1抑制剂、CTLA-4抑制剂、小分子酪氨酸激酶抑制剂Lapatinib及小分子酪氨酸激酶抑制剂Palbociclib均展现显著抗肿瘤效果，为药物筛选提供有力支撑。肠癌 APC-min小鼠：基于APC抑癌基因突变构建，对自发性肠道腺瘤高度易感，可通过高脂饮食调控加速肿瘤发生，清晰模拟结直肠癌发病机制，为肠道肿瘤预防与治疗研究提供优质载体，助力缩短研究周期。图7. APC-min病理检测图正常饮食下APC-min 16周龄可见明显腺瘤，高脂饮食下8周龄可见明显腺瘤，如图7所示，APC-min小鼠癌细胞呈菜花样腺管排列，黏膜层及肌层可见大量炎性细胞浸润，结肠中可以发现炎性细胞浸润，肌层纤维组织增生。图8. APC-min肠道腺瘤情况如图8所示，正常饮食腺瘤总数0-30不等，高脂饮食的腺瘤总数10-50个。药康生物自发肿瘤模型资源除以上常用模型，药康生物同时拥有肝脏、肺部等多类自发肿瘤模型，并不断完善模型矩阵，全方位覆盖更多研究场景。作者：汪丹丹审核：Gemma 编辑：Zoe 扫描左侧二维码有任何技术交流可咨询小吉哟~ 关于药康生物江苏集萃药康生物科技股份有限公司（科创板代码：688046）是一家专注于实验动物小鼠模型研发、生产及非临床研究服务的国家级高新技术企业，同时是科技部认定的国家遗传工程小鼠资源库共建单位。依托CRISPR/Cas9、ES打靶等在内的基因编辑技术，公司建立了国际一流的基因修饰动物模型研发平台，拥有近3万种自主知识产权的基因工程小鼠模型品系，其中包括基因敲除/条件性敲除小鼠品系（"斑点鼠计划"）、药靶基因人源化模型、复杂疾病模型、系列免疫缺陷小鼠品系、无菌小鼠品系以及用于抗体药物发现的NeoMab®全人源抗体转基因小鼠，为全球科研机构、CRO公司及医药企业提供全面的模型资源支持。公司提供从基因编辑定制（包括转基因TG、基因敲除KO、基因敲入KI及点突变PM等）、模型繁育到功能药效分析的全流程一站式服务，服务范围涵盖肿瘤、自身免疫性疾病、代谢心血管疾病、神经退行性疾病、感染性疾病及罕见病等重点疾病领域，具体包括靶点验证、药效学评价和非GLP安全性评价等临床前研究。药康生物致力于成为全球实验动物模型领域的领导者，通过持续深化基因编辑技术的创新应用和资源整合，为生命科学研究和生物医药产业提供高质量的动物模型和技术服务，推动人类健康事业发展。点赞收藏分享

2026-03-20

·BioSpace

Relmada Therapeutics Reports Fourth Quarter and Full Year 2025 Results and Provides Business Update

Positive 12-month Phase 2 data for NDV-01 in non-muscle invasive bladder cancer (NMIBC) demonstrated a 95% complete response (CR) rate at any time and a durable 76% CR rate at 12 months, with favorable safety profile Completed an oversubscribed $160 million PIPE financing led by leading healthcare investors in March 2026, strengthens balance sheet to support NDV-01 Phase 3 development On track to initiate Phase 3 RESCUE registrational program in second line (2L) BCG-unresponsive and adjuvant intermediate-risk NMIBC in mid-2026 Cash balance of $93.0 million as of December 31, 2025, plus gross proceeds of $160 million from March 2026 PIPE expected to fund operations through 2029, including completion of the NDV-01 RESCUE program Management to host a conference call and webcast today at 4:30 PM ET CORAL GABLES, Fla., March 19, 2026 (GLOBE NEWSWIRE) -- Relmada Therapeutics, Inc. (Nasdaq: RLMD, “Relmada” or the “Company”), a clinical-stage biotechnology company advancing innovative therapies for oncology and central nervous system disorders, today reported audited financial results for the fourth quarter and full year ended December 31, 2025 and provided a corporate update highlighting significant progress across its pipeline. “This has truly been a transformational year for Relmada, marked by significant progress with our lead program NDV-01,” said Sergio Traversa, Chief Executive Officer of Relmada Therapeutics. “Our recently reported 12-month data for NDV-01 demonstrated durable complete responses with a favorable safety profile, reinforcing the program’s potential to become a best-in-class therapy for patients with non-muscle invasive bladder cancer. With a successful $160 million PIPE financing and regulatory alignment with the FDA on two registrational pathways, we believe that we are well positioned to advance NDV-01 into the Phase 3 RESCUE program in mid-2026. Our team is now focused on executing this plan and initiating the RESCUE registrational program as we work to bring NDV-01 to patients as efficiently as possible.” “NDV-01’s compelling efficacy, durability, and favorable safety profile, combined with operational ease-of-use are the cornerstone of its differentiated product pro best-in-class potential,” said Raj S. Pruthi, MD, Chief Medical Officer-Oncology of Relmada Therapeutics . “We continue to be encouraged by the high response rates and durable clinical benefit observed through 12 months, including in the BCG-unresponsive population, alongside a favorable safety pro no ≥ Grade 3 treatment-related adverse events and no treatment-related discontinuations. Our clinical program builds on the urologic oncology community’s comfort with conventional Gem/Doce’s efficacy and safety pro a sustained release product that could provide physicians and patients with a streamlined, less than 5-minute in-office procedure. These results reinforce our confidence as we advance NDV-01 into the Phase 3 RESCUE registrational program in mid-2026.” Highlights of the 12-month follow-up data from the ongoing Phase 2 study of NDV-01: In the 12-month follow-up of the Phase 2a study (March 9, 2026 Company press release) treatment with NDV-01 produced: Durable 76% complete response (CR) rate at 12 months with 95% CR rate at any time in high-risk NMIBC BCG-unresponsive patients achieved an 80% CR rate at 12 months and 94% CR rate at any time No patient had progression to muscle-invasive disease, and no patient underwent a radical cystectomy Favorable overall tolerability – no ≥ Grade 3 treatment-related adverse events and no treatment-related discontinuations or dose interruptions. Phase 3 RESCUE Registrational Pathways: As previously disclosed in the Company’s January 12, 2026 regulatory update, Relmada has received written feedback from the U.S. Food and Drug Administration (FDA) confirming alignment on two registrational development pathways for NDV-01, including study design, patient populations and primary endpoints. Registrational Pathway 1 – An open label randomized controlled trial in intermediate-risk NMIBC of adjuvant therapy following TURBT (NDV-01 vs. observation). There are no approved treatments for adjuvant intermediate risk NMIBC, which we estimate affect ~75,000 patients/year in the U.S. The primary endpoint of the study is disease free survival (DFS). Registration Pathway 2 – A single-arm trial in second line (2L) BCG-unresponsive NMIBC with carcinoma in situ (CIS) patients who are currently refractory to approved or developmental therapies. Patients with BCG-unresponsive NMIBC with CIS who fail first line (1L) therapies, which we estimate to affect ~5,000 patients/year in the U.S., have few, if any, effective treatment alternatives to radical cystectomy. The primary endpoint of the study is complete response (CR) rate at any time. Expected Upcoming Relmada Milestones: NDV-01 United States IND clearance – Mid-2026 NDV-01 Phase 3 RESCUE Program initiation – Mid-2026 Sepranolone Phase 2 initiation in Prader-Willi syndrome – Mid-2026 Initial 3-month NDV-01 data from Phase 3 2L BCG-unresponsive study expected by YE 2026 Financial Results Fourth Quarter 2025 Financial Results Research and development expense for the three months ended December 31, 2025, totaled $8.1 million, compared to $11.0 million for the three months ended December 31, 2024, a decrease of $2.9 million. The decrease was primarily driven by a decrease in study costs associated with the completion of two Phase 3 trials for REL-1017, partially offset by increased costs related to the start-up the Phase 3 NDV-01 trials and Phase 2b sepranolone study and additional R&D personnel. General and administrative expense for the three months ended December 31, 2025, totaled $12.3 million compared to $8.1 million for the three months ended December 31, 2024, an increase of approximately $4.2 million. The increase was primarily driven by an increase in compensation costs partially offset by a decrease in stock based compensation costs. Net cash used in operating activities for the three months ended December 31, 2025, totaled $14.6 million compared to $8.8 million for the three months ended December 31, 2024. The net loss for the three months ended December 31, 2025, was $19.9 million, or $0.27 per basic and diluted share, compared with a net loss of $18.6 million, or $0.62 per basic and diluted share, for the three months ended December 31, 2024. Twelve Month Ended December 31, 2025 Financial Results Research and development (R&D) expense for the 12 months ended December 31, 2025, totaled $26.9 million, compared to $46.2 million for the 12 months ended December 31, 2024, a decrease of $19.3 million. The decrease was primarily driven by a decrease in study costs associated with completion and conclusion of two Phase 3 trials for REL-1017, partially offset by increased costs related to the acquisition of NDV-01 and sepranolone, as well as the start-up of the Phase 3 NDV-01 trials and Phase 2b sepranolone study. General and administrative (G&A) expense for the 12 months ended December 31, 2025, totaled $32.2 million compared to $37.7 million for the 12 months ended December 31, 2024, a decrease of approximately $5.5 million. The decrease was primarily driven by a decrease in stock-based compensation expense and lower professional fees, partially offset by an increase in personnel-related costs. Net cash used in operating activities for the 12 months ended December 31, 2025, totaled $45.8 million compared to $51.8 million for the 12 months ended December 31, 2024. The net loss for the 12 months ended December 31, 2025, was $57.4 million, or $1.45 per basic and diluted share, compared with a net loss of $80.0 million, or $2.65 per basic and diluted share, for the 12 months ended December 31, 2024. The Company’s cash balance of $93.0 million in cash, cash equivalents, and short-term investments, includes net proceeds of approximately $94 million from an underwritten stock offering announced November 5, 2025. This compares to cash, cash equivalents, and short-term investments of approximately $44.9 million at December 31, 2024. On March 9, 2026, the Company announced a private financing with gross proceeds of $160 million. This financing, along with the cash, cash equivalents, and short-term investments as of December 31, 2025, is expected to provide sufficient resources to fund Company operations through 2029, including completion of the Phase 3 NDV-01 RESCUE program. The Company had 104,890,223 shares outstanding, as of March 16, 2026 Conference Call and Webcast Information: Relmada will host a conference call and webcast today at 4:30 PM ET to discuss recent business progress and financial results. Conference Call and Webcast Information: Date: Thursday, March 19, 2026 at 4:30 PM ET Participant Dial-in (US): 1-877-407-0792 Participant Dial-in (International): 1-201-689-8263 Webcast Access: Click Here A replay of the webcast will be available in the Investors section of the Relmada website at . About NDV-01 NDV-01 is a sustained-release, intravesical formulation of gemcitabine and docetaxel (Gem/Doce), in development for the treatment of non-muscle invasive bladder cancer. It is designed to enable Gem/Doce bladder retention and gradual drug release over 10 days. The formulation creates a soft matrix that enhances local exposure while minimizing systemic toxicity. The NDV-01 formulation is ready to use, convenient to administer in-office in less than 5 minutes and does not require anesthesia or specialized equipment. It is protected by patents through 2038. About the Phase 2 Study The Phase 2 study (NCT06663137) is an open-label, single-arm, single-center study evaluating the safety and efficacy of NDV-01 in patients with high-grade non-muscle invasive bladder cancer (HG-NMIBC). Patients are treated with NDV-01 in a biweekly induction phase, followed by monthly maintenance for up to one year, with regular assessments via cystoscopy, cytology, and biopsy, as indicated. The primary efficacy endpoints are safety and complete response rate (CRR) at 12 months, and secondary efficacy endpoints are duration of response (DOR) and event free survival (EFS). About NMIBC NMIBC represents 75-80% of all bladder cancer cases and is associated with high recurrence (50 – 80% over 5 years). With over 744,000 prevalent cases in the U.S. and limited treatment options, the market opportunity is significant. High-grade BCG-unresponsive disease represents one of the most difficult-to-treat NMIBC subtypes, with limited bladder-sparing options. Intermediate-risk NMIBC in the adjuvant setting has no currently approved therapies. NDV-01 has the potential to serve as a frontline or salvage therapy and could be applicable across multiple NMIBC subtypes. About Sepranolone and GABA Modulation Sepranolone, a synthetic isoallopregnanolone, selectively modulates GABA A receptors by antagonizing allopregnanolone (ALLO), without disrupting GABA signaling. It targets disorders linked to excess GABAergic activity such as Prader-Willi syndrome, Tourette syndrome, and Obsessive-Compulsive Disorder (OCD). More than 335 patients have been treated with sepranolone in clinical trials to date, with an excellent safety profile. About Prader-Willi Syndrome (PWS) PWS is a rare genetic disorder caused by chromosomal deletions on chromosome 15, leading to neurodevelopmental and behavioral complications. Global prevalence is estimated to be 350,000-400,000 patients. Current treatments address symptoms but do not modify the underlying neurobehavioral pathology. About Relmada Therapeutics, Inc. Relmada Therapeutics is a clinical-stage biotechnology company focused on developing transformative therapies for oncology and central nervous system conditions. Its lead candidates, NDV-01 and sepranolone, are advancing through mid-stage clinical development with the potential to address significant unmet needs. For more information, visit Forward-Looking Statements: The Private Securities Litigation Reform Act of 1995 provides a safe harbor for forward-looking statements made by us or on our behalf. This press release contains statements which constitute “forward-looking statements” within the meaning of Section 27A of the Securities Act of 1933 and Section 21E of the Securities Exchange Act of 1934. Any statement that is not historical in nature is a forward-looking statement and may be identified by the use of words and phrases such as “if”, “may”, “expects”, “anticipates”, “believes”, “will”, “will likely result”, “will continue”, “plans to”, “potential”, “promising”, and similar expressions. These statements are based on management’s current expectations and beliefs and are subject to a number of risks, uncertainties and assumptions that could cause actual results to differ materially from those described in the forward-looking statements, including potential for Relmada’s product candidates to progress, including the potential for Phase 2 NDV-01 data to continue to deliver positive results supporting further development, potential for clinical trials to deliver statistically and/or clinically significant evidence of efficacy and/or safety, failure of interim or top-line results to accurately reflect the complete results of the trial, failure of planned or ongoing preclinical and clinical studies to demonstrate expected results, potential failure to continue to secure FDA agreement on the regulatory path for NDV-01 and/or sepranolone, or that future NDV-01 and/or sepranolone clinical results will be acceptable to the FDA, failure to secure adequate NDV-01 and/or sepranolone drug supply, the Company’s cash runway and sufficiency of the Company’s cash resources and uncertainties inherent in estimating the Company’s cash runway, future expenses and other financial results, including its ability to fund future operations, including clinical trials, and the other risk factors described under the heading “Risk Factors” set forth in the Company’s reports filed with the SEC from time to time. No forward-looking statement can be guaranteed, and actual results may differ materially from those projected. Relmada undertakes no obligation to publicly update any forward-looking statement, whether as a result of new information, future events, or otherwise. Readers are cautioned that it is not possible to predict or identify all the risks, uncertainties and other factors that may affect future results and that the risks described herein are not a complete list. Investor Contact: Brian Ritchie LifeSci Advisors britchie@lifesciadvisors.com Media Inquiries: Corporate Communications media@relmada.com Relmada Therapeutics, Inc. Condensed Consolidated Balance Sheets (Audited) As of As of December 31, December 31, 2025 2024 Assets Current assets: Cash and cash equivalents $ 3,496,540 $ 3,857,026 Short-term investments 89,509,710 41,052,356 Prepaid expenses 977,721 886,461 Total current assets 93,983,971 45,795,843 Other assets 19,500 21,975 Total assets $ 94,003,471 $ 45,817,818 Liabilities and Stockholders’ Equity Current liabilities: Accounts payable $ 1,568,944 $ 4,130,563 Accrued expenses 4,861,583 6,160,827 Total current liabilities 6,430,527 10,291,390 Stock appreciation rights 1,060,931 4,467 Total liabilities 7,491,458 10,295,857 Commitments and Contingencies (Note 10) Stockholders’ Equity: Preferred stock, $0.001 par value, 200,000,000 shares authorized, none issued and outstanding - - Class A convertible preferred stock, $0.001 par value, 3,500,000 shares authorized, none issued and outstanding - - Common stock, $0.001 par value, 150,000,000 shares authorized, 73,333,622 and 30,174,202 shares issued and outstanding, respectively 73,333 30,174 Additional paid-in capital 784,705,878 676,373,822 Accumulated deficit (698,267,198 ) (640,882,035 ) Total stockholders’ equity 86,512,013 35,521,961 Total liabilities and stockholders’ equity $ 94,003,471 $ 45,817,818 Relmada Therapeutics, Inc. Condensed Consolidated Statements of Operations (Audited) 2025 2024 Operating expenses: Research and development $ 26,879,146 $ 46,175,512 General and administrative 32,221,054 37,715,524 Total operating expenses 59,100,200 83,891,036 Loss from operations (59,100,200 ) (83,891,036 ) Other income (expenses): Interest/investment income, net 1,395,989 3,530,021 Realized (loss) gain on short-term investments (79,207 ) 374,926 Unrealized gain on short-term investments 398,255 6,735 Total other income (expenses), net 1,715,037 3,911,682 Net loss $ (57,385,163 ) $ (79,979,354 ) Net loss per common share – basic and diluted $ (1.45 ) $ (2.65 ) Weighted average number of common shares outstanding – basic and diluted 39,479,694 30,163,751 Relmada Therapeutics, Inc. Condensed Consolidated Statements of Stockholders’ Equity (Audited) Common Stock Additional Paid-in Accumulated Balance – December 31, 2023 30,099,203 $ 30,099 $ 646,229,824 $ (560,902,681 ) $ 85,357,242 Stock-based compensation expense - - 30,184,414 - 30,184,414 Net proceeds from cash exercise option 74,999 75 246,672 - 246,747 ATM fees - - (287,088 ) - (287,088 ) Net loss - - - (79,979,354 ) (79,979,354 ) Balance – December 31, 2024 30,174,202 30,174 676,373,822 (640,882,035 ) 35,521,961 Stock-based compensation expense - - 13,905,181 - 13,905,181 Issuance of restricted common stock 3,017,420 3,017 902,209 - 905,226 Net proceeds from cash exercise options 40,142,000 40,142 93,597,687 - 93,637,829 ATM fees - - (73,021 ) - (73,021 ) Net loss - - - (57,385,163 ) (57,385,163 ) Balance – December 31, 2025 73,333,622 $ 73,333 $ 784,705,878 $ (698,267,198 ) $ 86,512,013 Relmada Therapeutics, Inc. Condensed Consolidated Statements of Cash Flows (Audited) 2025 2024 Cash flows from operating activities Net loss $ (57,385,163 ) $ (79,979,354 ) Adjustments to reconcile net loss to net cash used in operating activities: Stock-based compensation 13,905,181 30,184,414 Stock appreciation rights compensation 1,056,464 4,467 Issuance of restricted common stock 905,226 - Realized (gain) loss on short-term investments 79,207 (374,926 ) Unrealized gain on short-term investments (398,255 ) (6,735 ) Change in operating assets and liabilities: Prepaid expenses and other assets (88,785 ) 319,746 Accounts payable (2,561,619 ) 624,554 Accrued expenses (1,299,244 ) (2,527,964 ) Net cash used in operating activities (45,786,988 ) (51,755,798 ) Cash flows from investing activities Purchase of short-term investments (83,828,576 ) (12,079,628 ) Sale of short-term investments 35,690,270 63,641,225 Net cash (used in)/provided by investing activities (48,138,306 ) 51,561,597 Cash flows from financing activities Proceeds from issuance of common stock, net 93,637,829 - Payment of ATM fees (73,021 ) (287,088 ) Proceeds from options exercised for common stock - 246,747 Net cash provided by/(used in) financing activities 93,564,808 (40,341 ) Net decrease in cash and cash equivalents (360,486 ) (234,542 ) Cash and cash equivalents at beginning of the year 3,857,026 4,091,568 Cash and cash equivalents at end of the year $ 3,496,540 $ 3,857,026

临床2期临床结果临床3期财报

100 项与盐酸吉西他滨相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D01155	盐酸吉西他滨	L01BC05	DB00441

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
非肌层浸润性膀胱肿瘤	美国	Janssen Biotech, Inc.	2025-09-09
局部晚期非小细胞肺癌	澳大利亚	Sandoz Pty Ltd.	2008-12-02
局部晚期胰腺腺癌	澳大利亚	Sandoz Pty Ltd.	2008-12-02
转移性非小细胞肺癌	澳大利亚	Sandoz Pty Ltd.	2008-12-02
转移性胰腺腺癌	澳大利亚	Sandoz Pty Ltd.	2008-12-02
复发性卵巢癌	澳大利亚	Sandoz Pty Ltd.	2008-12-02
尿路上皮癌	日本	Eli Lilly & Co.	2008-11-25
膀胱癌	巴西	Libbs Farmacêutica Ltda.	2008-05-26
胆道癌	日本	Eli Lilly & Co.	2001-08-31
淋巴瘤	日本	Eli Lilly & Co.	2001-08-31
卵巢癌	日本	Eli Lilly & Co.	2001-08-31
乳腺癌	美国	Eli Lilly & Co.	1996-05-15
转移性乳腺癌	美国	Eli Lilly & Co.	1996-05-15
非小细胞肺癌	美国	Eli Lilly & Co.	1996-05-15
胰腺腺癌	美国	Eli Lilly & Co.	1996-05-15
胰腺癌	美国	Eli Lilly & Co.	1996-05-15

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
晚期胆道癌	临床3期	中国台湾	因华生技制药股份有限公司	2025-07-01
复发性膀胱癌	临床3期	美国	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	中国	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	日本	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	阿根廷	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	比利时	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	巴西	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	法国	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	德国	Janssen Research & Development LLC	2024-04-09
复发性膀胱癌	临床3期	意大利	Janssen Research & Development LLC	2024-04-09

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临床结果

适应症

分期

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


ESMO_SRC2026	N/A	平滑肌肉瘤二线	108	Trabectedin	積鏇蓋窪膚醖鏇顧構餘(網夢鑰蓋範鹹鹹壓顧齋) = 網鹹鹹襯衊醖鹹壓衊遞鬱遞願構觸衊壓窪網顧 (選願願壓鹽淵衊繭獵鑰, 5.5 ~ 15.2) 更多	积极	2026-03-09
				gemcitabine-based chemotherapy	積鏇蓋窪膚醖鏇顧構餘(網夢鑰蓋範鹹鹹壓顧齋) = 膚膚窪選鏇願鹹顧鏇鹽鬱遞願構觸衊壓窪網顧 (選願願壓鹽淵衊繭獵鑰, 3.8 ~ 6.4) 更多
ESMO_SRC2026	N/A	软骨肉瘤	10	Gemcitabine 1000 mg/m2 plus Oxaliplatin 100 mg/m2	積窪壓鏇醖憲築簾選蓋(鏇鏇選鬱願憲鹹膚積鬱) = Treatment was generally well tolerated, with limited grade 3 toxicity and one case of grade 5 thrombotic microangiopathy-associated to gemcitabine 選範鹽鑰獵簾衊憲窪顧 (壓餘窪構選鏇積觸願餘 )	积极	2026-03-09
ESMO_SRC2026	N/A	平滑肌肉瘤	336	Gemcitabine combined with docetaxel	壓艱憲願壓壓製淵選餘(夢齋繭艱網糧淵膚獵獵) = 窪衊獵鑰鏇餘觸構願鹹蓋夢願遞構製選壓糧襯 (範蓋構選繭願繭蓋壓蓋 ) 更多	积极	2026-03-09
ESMO_SRC2026	N/A	血管周围上皮样细胞肿瘤	3	sirolimus + exemestane + gemcitabine	獵鏇觸糧顧遞範簾膚壓(膚獵鹽膚衊淵鏇製糧鹹) = 蓋遞顧鬱醖鏇艱鏇餘鑰遞夢顧膚鹹獵鬱願淵構 (鬱範遞選積鹹鏇壓鬱餘 ) 更多	积极	2026-03-09
ASCO_GU2026	N/A	非肌层浸润性膀胱肿瘤	133	BCG	襯觸醖襯網網構範鏇廠(選齋餘衊膚襯範窪願選) = 艱餘觸選顧夢願醖繭醖壓襯顧餘糧顧襯蓋膚鏇 (製膚齋壓鏇簾鏇艱餘鹽 ) 更多	不佳	2026-02-26
				sequential gemcitabine and docetaxel (Gem/Doce)	襯觸醖襯網網構範鏇廠(選齋餘衊膚襯範窪願選) = 壓艱積艱糧廠範觸願鹹壓襯顧餘糧顧襯蓋膚鏇 (製膚齋壓鏇簾鏇艱餘鹽 ) 更多
NCT04179162 (ALLIANCE A032303, ASCO_GU2026)	临床1/2期	复发性膀胱癌	52	Gemcitabine + BCG	積鬱築鏇顧構鹽艱構艱(選積窪廠齋壓鏇鑰窪觸) = 夢齋構鹹繭顧構鏇積膚憲衊鑰齋齋壓蓋願糧範 (願鏇範範鬱憲蓋淵鏇淵 ) 更多	积极	2026-02-26
ASCO_GU2026	N/A	肌层浸润性膀胱癌新辅助	517	Gemcitabine 800 mg/m2	艱遞範網膚網築鬱積願(簾淵鏇鑰觸鹹鹹積簾製): P-Value = 0.012 更多	积极	2026-02-26
				Gemcitabine 1000 mg/m2
ASCO_GU2026	N/A	肌层浸润性膀胱癌	98	Cisplatin	膚淵鬱齋網網製網膚願(觸觸廠齋選艱鹹窪構願) = 醖鑰鹽醖獵蓋夢糧積選膚齋廠齋醖壓觸選繭顧 (鏇襯範糧簾糧網憲觸襯 ) 更多	积极	2026-02-26
				5-FU+MMC	膚淵鬱齋網網製網膚願(觸觸廠齋選艱鹹窪構願) = 鬱壓鹹範獵夢簾襯製獵膚齋廠齋醖壓觸選繭顧 (鏇襯範糧簾糧網憲觸襯 ) 更多
NCT04628767 (EA8192, ASCO_GU2026)	临床2期	肾盂和输尿管尿路上皮癌新辅助	30	Gemcitabine/Durvalumab	鑰鹽觸鑰鹹膚選窪鬱夢(夢鏇遞構襯窪餘鬱鑰獵) = 鹽範衊糧廠糧糧壓襯鬱膚製簾衊構範鹽憲構窪 (製構鹽憲願構齋糧憲選, 3.0 ~ 25.2) 更多	积极	2026-02-26
NCT03366766 (CTgov)	临床2期	非小细胞肺癌Ⅰ期 \| 可切除非小细胞肺癌 \| 非小细胞肺癌IIIA期 ... 更多	14	Nivolumab+cisplatin+Pemetrexed Disodium (Cohort I (Nivolumab, Cisplatin, Pemetrexed Disodium))	範糧夢鑰糧顧繭餘鑰衊 = 觸艱築顧遞憲醖遞蓋窪膚積淵鬱憲窪淵鑰獵選 (醖蓋衊醖鹽鏇膚網襯鑰, 壓壓構範壓鏇鹹餘夢製 ~ 淵願壓餘壓餘顧願範觸) 更多	-	2026-02-20
				nivolumab+Gemcitabine Hydrochloride (Cohort I (Nivolumab, Cisplatin, Gemcitabine Hydrochloride))	鑰簾蓋願範膚鹽遞醖繭 = 齋簾築壓夢繭積鬱蓋膚壓鑰製網餘艱築糧窪齋 (夢夢夢獵鹽積醖鏇顧膚, 醖顧繭範鹽選膚遞遞網 ~ 壓餘鑰觸鬱簾鹽選夢膚)