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.

NCT06498648

/ Suspended临床1/2期IIT

Phase I/II Study to Evaluate the Feasibility and Efficacy of Sequential Abemaciclib and Gemcitabine Treatment in Patients With Retinoblastoma (Rb)+ Sarcomas

This phase I/II trial tests the side effects and best dose of abemaciclib when added to gemcitabine and compares the effectiveness of that treatment to the usual treatment of gemcitabine with docetaxel for the treatment of patients with soft tissue sarcoma that may have spread from where it first started to nearby tissue, lymph nodes, or distant parts of the body (advanced) or that has spread from where it first started (primary site) to other places in the body (metastatic) (phase 1) or patients with leiomyosarcoma or dedifferentiated liposarcoma (phase 2). Abemaciclib is in a class of medications called kinase inhibitors. It works by blocking the action of an abnormal protein that signals tumor cells to multiply. This helps slow or stop the spread of tumor cells. Gemcitabine is a chemotherapy drug that blocks the cells from making deoxyribonucleic acid and may kill tumor cells. Docetaxel is in a class of medications called taxanes. It stops cancer cells from growing and dividing and may kill them. Giving abemaciclib with gemcitabine may be safe and effective when compared to treatment with gemcitabine and docetaxel for patients with advanced or metastatic soft tissue sarcoma or leiomyosarcoma or dedifferentiated liposarcoma.

开始日期2026-10-14

申办/合作机构

National Cancer Institute

NCT06822010

/ Not yet recruiting临床2期IIT

A Phase II Trial of SeqUential GeMcitabine and MITomycin Treatment for Favorable High-Risk Upper Urinary Tract Urothelial Carcinoma (SUMMIT)

This Phase II clinical trial, titled "A Phase II Trial of Sequential Gemcitabine and Mitomycin Treatment for Favorable High-Risk Upper Urinary Tract Urothelial Carcinoma (SUMMIT)," aims to evaluate the safety and effectiveness of a combination chemotherapy treatment for patients with favorable papillary high-grade upper tract urothelial carcinoma (UTUC). The study focuses on sequential administration of two drugs, gemcitabine and Jelmyto (a gel-based form of mitomycin), to potentially preserve kidney function and avoid nephroureterectomy (kidney removal), which is the current standard of care for participants with non-endoscopically resectable tumors.

开始日期2026-06-01

申办/合作机构

Rutgers State University of New Jersey

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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14,862

项与盐酸吉西他滨相关的文献（医药）

2025-11-01·CURRENT OPINION IN UROLOGY

Novel intravesical delivery systems for nonmuscle invasive bladder cancer

Review

作者: Ramos, Felix-Guerrero ; Xylinas, Evanguelos ; Katzendorn, Olga ; Pradere, Benjamin ; Khene, Zine Eddine ; Uleri, Alessandro

Purpose of review:

Nonmuscle invasive bladder cancer (NMIBC) represents approximately 75% of bladder cancer cases at diagnosis and poses a significant management challenge due to high recurrence rates and risk for progression. Conventional intravesical therapies face limitations including suboptimal drug delivery, mucosal exposure time and significant adverse events. This review provides a timely assessment of novel intravesical delivery systems developed to overcome these limitations and improve oncological outcomes for patients with NMIBC.

Recent findings:

Several innovative delivery systems show promising results. Hyperthermic intravesical chemotherapy (HIVEC) demonstrates its efficacy in selected high-risk NMIBC. Intravesical drug-releasing systems (iDRS) like TAR-200 showed complete response rates up to 84% in BCG-unresponsive disease, while TAR-210 shows promise for FGFR-altered NMIBC. UGN-102, a reverse thermal gel containing mitomycin C, achieves 65–79% complete response rates in low-grade intermediate-risk NMIBC. Oncofid-P-B, combining paclitaxel with hyaluronic acid, demonstrates efficacy in BCG-unresponsive CIS.

Summary:

Novel intravesical delivery systems show to enhance drug retention, improve tissue penetration, and potentially reduce adverse events. While traditional chemotherapy or BCG remain the gold-standard adjuvant treatments for NMIBC, these novel approaches offer promising alternatives for selected patients pending on ongoing clinical validation.

2025-10-10·JOURNAL OF CLINICAL ONCOLOGY

Erratum: TAR-200 for Bacillus Calmette-Guérin–Unresponsive High-Risk Non–Muscle-Invasive Bladder Cancer: Results From the Phase IIb SunRISe-1 Study

Article

作者: Jacob, Joseph M. ; Casco, Nelson Canales ; Cahn, David ; Stromberg, Katharine ; Necchi, Andrea ; Pieczonka, Christopher M. ; Daneshmand, Siamak ; Lotan, Yair ; Cutie, Christopher J. ; Martin, Jason ; Kawahara, Takashi ; Shukla, Abhijit ; Bertzos, Kristi ; Bögemann, Martin ; Murray, Katie S. ; Zainfeld, Daniel ; Hampras, Shalaka ; Xylinas, Evanguelos ; Guerrero-Ramos, Felix ; Sweiti, Hussein ; Spiegelhalder, Philipp ; Van der Heijden, Michiel S. ; Simone, Giuseppe

2025-10-03·Expert Opinion On Drug Safety

Signal mining and gender differences analysis of adverse events in NMIBC treatment with gemcitabine and BCG bladder instillation based on the FAERS database

Article

作者: Wang, Jia-Hao ; Wang, Ben ; Wang, Li ; Xia, Long ; Jiang, Bing-Lei ; Zhu, Ping-Yu ; Liu, Ying ; Yang, Lin ; Bao, Er-Hao

OBJECTIVE:

To explore safety differences and perform a gender-based analysis of adverse events related to gemcitabine and Bacillus Calmette-Guérin (BCG) vaccine using the U.S. FDA Adverse Event Reporting System (FAERS) database.

METHODS:

Using the Reporting Odds Ratio (ROR) and Proportional Reporting Ratio (PRR) methods, adverse events associated with gemcitabine and BCG were mined from FAERS database reports spanning from Q1 2004 to Q3 2023.

RESULTS:

The study extracted 37,855 reports with gemcitabine and 5,455 reports with BCG as the primary suspected drugs. Adverse events were more prevalent in males (male-to-female ratio: gemcitabine 1.10, BCG 4.25). Differences in high-frequency adverse events among the top 20 signals were detected for both drugs. Both drugs affected similar organ systems, including potential pulmonary, ocular, and renal toxicity, with gemcitabine showing a broader range of adverse events. Gender analysis revealed fewer adverse reactions to gemcitabine in females, while males had fewer adverse reactions to BCG.

CONCLUSION:

Differences in high-frequency adverse events between gemcitabine and BCG, including some not listed on drug labels, were observed. Both drugs affect similar organ systems, with gemcitabine showing a broader range of adverse events. Gender differences in adverse events were notable.

1,096

项与盐酸吉西他滨相关的新闻（医药）

2025-11-17

·临床试验信息资讯

一项评估注射用华卟啉钠光动力疗法联合吉西他滨与顺铂化疗在伴有胆道梗阻的晚期肝外胆管癌患者中初步疗效和安全性的IIa期临床研究

基本信息登记号 CTR20254544 试验状态进行中申请人联系人郑燕飞首次公示信息日期 2025-11-13 申请人名称青龙高科技股份有限公司公示的试验信息一、题目和背景信息登记号 CTR20254544 相关登记号 CTR20150690,CTR20150725,CTR20200598,CTR20221271,CTR20222704 药物名称注射用华卟啉钠曾用名: 药物类型化学药物临床申请受理号企业选择不公示适应症胆管癌试验专业题目一项评估注射用华卟啉钠光动力疗法联合吉西他滨与顺铂化疗在伴有胆道梗阻的晚期肝外胆管癌患者中初步疗效和安全性的多中心、开放、IIa期临床研究试验通俗题目华卟啉钠-PDT联合GC化疗治疗伴胆道梗阻晚期肝外胆管癌的IIa期临床研究试验方案编号 GS101-BTC-II-1 方案最新版本号 V1.0 版本日期: 2025-07-18 方案是否为联合用药否二、申请人信息申请人名称 1 联系人姓名郑燕飞联系人座机 021-68066188 联系人手机号 18154303405 联系人Email yanfei.zheng@shgsmed.com 联系人邮政地址上海市-上海市-上海市浦东新区凌霄花路266号联系人邮编 201206 三、临床试验信息 1、试验目的主要目的：初步评价华卟啉钠光动力疗法（PDT）联合吉西他滨与顺铂（GC方案）化疗在伴有胆道梗阻的晚期肝外胆管癌患者中的有效性；次要目的：初步评价华卟啉钠光动力疗法（PDT）联合吉西他滨和顺铂（GC方案）化疗在伴有胆道梗阻的晚期肝外胆管癌患者中的安全性和耐受性；探索性目的：探索注射用华卟啉钠单次给药后在伴有胆道梗阻的晚期肝外胆管癌患者体内的药代动力学及代谢特征； 2、试验设计试验分类安全性和有效性试验分期 II期设计类型单臂试验随机化非随机化盲法开放试验范围国内试验 3、受试者信息年龄 18岁(最小年龄)至无上限 (最大年龄) 健康受试者无入选标准 1 1.所有受试者或其法定代理人必须在开始任何筛选程序之前自愿书面签署伦理委员会批准的知情同意书； 2 年龄≥18周岁，性别不限； 3 经组织学或细胞学证实的，不可手术或不愿意接受手术的局部进展期或复发转移的晚期肝外胆管腺癌患者； 4 复发转移阶段未接受过系统治疗； 5 肝外胆管存在梗阻病灶，且依据实体瘤疗效评价标准/RECIST 1.1胆管外至少存在一处可测量病灶； 6 ECOG体能状态评分为0或1分的受试者； 7 预期生存期≥3个月的受试者； 8 受试者有足够的器官和骨髓功能，满足以下实验室检查标准：？骨髓功能：绝对中性粒细胞数（ANC）≥1.5 × 109/L（1500/mm3）；血小板≥100 × 109/L（1 × 105/mm3）；血红蛋白≥9.0 g/dL（筛选期实验室检查前14天内未使用过GCS-F、EPO或输血等针对骨髓抑制的治疗）；？肾功能：肌酐清除率（Ccr）≥50 mL/min（使用Cockcroft-Gault公式计算，详见附录4）；？凝血功能：国际标准化比值（INR）≤1.5 × ULN，活化部分凝血活酶时间（APTT）≤1.5 × ULN；？心脏彩超：左室射血分数（LVEF）≥50%；？12导联心电图：Fridericia法校正的QT间期（QTcF）<470 msec； 9 从先前所有治疗中恢复，毒性反应降至1级或1级以下者； 10 育龄期女性及所有男性受试者必须同意在试验期间及最后一次使用华卟啉钠后6个月内使用高效避孕方法（采取避孕套、避孕海绵、避孕凝胶、避孕膜、宫内节育器、口服或者注射用的避孕药、皮下埋植剂等），且育龄期女性在试验药物给药前≤7天内的妊娠检测结果必须为阴性。排除标准 1 壶腹部癌患者； 2 已知对华卟啉钠或其他光敏类药物过敏者； 3 弥漫性肝转移或肝肿瘤负荷超过50%肝体积者； 4 已知存在或疑似脑转移、脑膜转移或脊髓压迫者(包括无症状和得到充分治疗者)； 5 试验药物给药前4周内参与其他任何药物临床试验或其他干预性临床试验的受试者，但参与观察性（非干预性）临床研究或已处于干预性研究随访期的受试者除外； 6 之前接受过光敏剂或光动力治疗者； 7 肝外胆管有不可移除的支架植入者； 8 既往接受过免疫治疗（包括但不限于各种抗PD-1单抗、抗PD-L单抗、抗CTLA-4单抗等）、吉西他滨或顺铂治疗的患者； 9 试验药物给药前4周内接受过大手术者； 10 试验药物给药前14天内使用了具有免疫调节作用或抗肿瘤作用的中药； 11 处于恶液质状态，或预计无法耐受光动力治疗的晚期胆管癌受试者； 12 Bismuth IV型肝门部胆管癌患者； 13 不适合ERCP或内窥镜检查者； 14 试验药物治疗期间需要联合任何其他抗肿瘤治疗的受试者，包括GC方案以外的其他化疗、放疗、免疫疗法、生物制剂治疗等； 15 首次给予研究药物前5年内曾诊断为任何其它恶性肿瘤，但既往已治愈的任何类型原位癌、微小或低危甲状腺乳头状癌以及痊愈的皮肤基底细胞癌或鳞状皮肤细胞癌等除外； 16 既往接受过同种异体器官移植，或已知有自体或异体造血干细胞移植史； 17 华卟啉钠首次给药前4周内存在有临床意义（恶性/癌性，或中大量）的胸腔积液、腹腔积液、心包积液，但通过影像学检查发现仅有少量积液（未接受过处理）的受试者可以入组； 18 伴有急性炎症（尤其是腐蚀性炎症）或有临床意义的活动性感染者； 19 丙型肝炎病毒（HCV）RNA阳性、梅毒活动期或人类免疫缺陷病毒（HIV）抗体检查结果中任意一种或几种呈阳性，或活动性乙肝受试者（定义为HBV DNA≥2000 IU/mL或者HBV DNA≥104拷贝数）； 20 具有临床意义的心血管疾病或状况，包括但不限于： a)首次给药前6个月内发生的心肌梗死； b)首次给药前 3个月内发生的未控制的心绞痛； c)既往或目前存在有临床意义的室性心律失常（例如，室性心动过速、心室颤动、尖端扭转型室性心动过速等）或其他≥2级持续心律失常（根据NCI-CTCAE v5.0）； d)既往或目前存在充血性心力衰竭[纽约心脏协会(NYHA) 3 级或 4 级（附录5）]； e)完全左束支传导阻滞或完全右束支传导阻滞合并有左前分支传导阻滞（双束支传导阻滞）； f)合并长QT综合征或已证实有长QT综合征家族史；已知合并使用延长QT间期药物； g)心动过缓，筛选期 ECG 显示心率 < 45 次/分； h)低血压，表现为筛选期收缩压≤86 毫米汞柱（mmHg）；未控制的高血压，受试者接受规范降压治疗，筛选期收缩压> 160mmHg 和/或舒张压≥100 mmHg； 21 首次给药前 6 个月内发生过脑血管事件（包括出血性、缺血性、短暂性脑缺血发作）、颅脑手术及不明原因的意识丧失； 22 合并严重的既存疾病，如间质性肺病、静息时发生的或需要吸氧治疗的重度呼吸困难、哮喘发作期或呼吸功能衰竭导致不能平卧、活动性或慢性肝病、重度肝功能受损[巴塞罗那分期(Child-Pugh)C级]、继发于肝功能不全的出血性疾病、肝性脑病等、癫痫或可能诱发癫痫的疾病、需要全身免疫治疗[包括免疫抑制剂等，如抗 TNF 单克隆抗体，糖皮质激素(允许鼻吸入、局部外用)]的疾病；合并肾上腺功能障碍病史； 23 首次给药前 6 个月内发生血栓栓塞性疾病； 24 患有不受控精神疾病/社会情况、预计将限制其对研究要求的遵守或损害受试者书面签署知情同意书的能力； 25 已知有精神类药物滥用或吸毒史； 26 妊娠期或哺乳期女性； 27 首次给药前4周内接种活疫苗； 28 经研究者判断具有不适合参加本试验的其他原因。 4、试验分组试验药序号名称用法 1 中文通用名:注射用华卟啉钠英文通用名:Sinoporphyrin Sodium ForInjection商品名称:NA 剂型:冻干粉针剂规格:10mg/瓶用法用量:0.2mg/kg用药时程:单次给药 2 中文通用名:注射用盐酸吉西他滨英文通用名:Gemeitabine Hydrochloride for Injection商品名称:注射用盐酸吉西他滨剂型:注射剂规格:1.0g用法用量:1000mg/㎡用药时程:21天1个给药周期，D1和D8给药 3 中文通用名:注射用顺铂（冻干型）英文通用名:NA商品名称:注射用顺铂（冻干型）剂型:注射剂规格:20mg用法用量:25mg/㎡用药时程:21天1个给药周期，D1和D8给药对照药序号名称用法暂未填写此信息 5、终点指标主要终点指标及评价时间序号指标评价时间终点指标选择 1 生存期（OS）：6个月OS率 6个月有效性指标+安全性指标次要终点指标及评价时间序号指标评价时间终点指标选择 1 次要终点包括安全性指标（不良事件、实验室/心电图/生命体征/体格检查异常）及疗效指标（ORR、DCR、PFS、DoR、生存率、至化疗/黄疸复发时间）。 24个月有效性指标+安全性指标 6、数据安全监查委员会（DMC）无 7、是否购买保险有四、研究者信息 1、主要研究者信息 1 姓名周军学位博士职称主任医师电话 133 6615 2815 Email joelbmu@126.com 邮政地址北京市-北京市-北京市海淀区阜成路52号邮编 100142 单位名称北京肿瘤医院 2、各参加机构信息序号机构名称主要研究者省（州）城市 1 北京肿瘤医院周军北京市北京市 2 西安交通大学第一附属医院耿智敏陕西省西安市 3 中山大学附属第一医院殷晓煜广东省广州市 4 四川大学华西医院李富宇四川省成都市五、伦理委员会信息序号名称审查结论批准日期/备案日期 1 北京肿瘤医院同意 2025-09-29 六、试验状态信息 1、试验状态进行中（尚未招募） 2、试验人数目标入组人数国内: 30 ；已入组人数国内: 登记人暂未填写该信息；实际入组总人数国内: 登记人暂未填写该信息； 3、受试者招募及试验完成日期第一例受试者签署知情同意书日期国内：登记人暂未填写该信息；第一例受试者入组日期国内：登记人暂未填写该信息；试验完成日期国内：登记人暂未填写该信息；七、临床试验结果摘要序号版本号版本日期暂未填写此信息

2025-11-17

·搜狐新闻

2025 CSCO |【胆道肿瘤专场】聚焦精准与规范，共谋胆道肿瘤诊疗新未来

2025年9月10日~14日，由中国临床肿瘤学会（CSCO）和北京市希思科临床肿瘤学研究基金会共同主办的第28届CSCO学术年会在山东济南盛大开幕，本届年会以“规范诊疗，创新引领”为主题，汇聚全球肿瘤领域知名专家学者，分享前沿研究成果与临床经验，促进学术交流与合作，通过肿瘤学继续教育推动临床诊疗规范的普及。胆道肿瘤专场作为大会重要组成部分，特邀顶尖专家学者参与，通过专题报告、共识解读和临床研究分享，全方位展现胆道肿瘤领域的最新成果与发展方向，为推动中国胆道肿瘤的规范化、精准化与国际化进程注入强劲动力。开场致辞海军军医大学第三附属医院沈锋教授、陆军军医大学西南医院梁后杰教授对本届CSCO年会的召开表示热烈祝贺，并对与会专家同道的到来致以诚挚欢迎。他们强调，本次胆道肿瘤专场凝聚了国内顶尖学术力量，旨在共商诊疗新策略、共谋规范新未来，期待通过高水平的交流互鉴，进一步推动我国胆道恶性肿瘤（BTC）领域的创新与协同发展，预祝大会圆满成功。Session 1 围术期治疗本环节由复旦大学附属华山医院钦伦秀教授、上海交通大学医学院附属仁济医院王理伟教授共同主持。西安交通大学第一附属医院吴胤瑛教授以《从HER2视角看胆管癌的精准治疗策略》为题进行分享。HER2扩增或突变主要发生在胆囊癌和肝外胆管癌，且与胆管癌预后不良相关，HER2扩增患者复发及死亡风险更高。报告指出，需优化精准靶向治疗策略，包括联合治疗、探索化疗角色、靶向治疗前移等，还需探索耐药机制，如HER2基因突变、蛋白表达异质性等，可通过联合治疗、研发新型HER2靶向药物、应用个体化治疗策略及液体活检实时监测等手段克服耐药，此外还涉及ADC到细胞免疫治疗等新型药物研发。华中科技大学同济医学院附属协和医院马虹教授围绕《精准放疗在BTC新辅助治疗中进展》展开精彩分享。马虹教授围绕BTC新辅助治疗中放疗的作用展开，探讨了放疗在新辅助/转化治疗策略中的可行性及实施的精准性，分析了放疗在新辅助治疗中的作用及争议，还涉及新辅助治疗的精准化实施，包括依据肿瘤特性选择放疗方式及剂量、建立临床评价体系辅助治疗决策等，强调新兴影像学、基因组学检测的必要性，以及基于肿瘤特征选择放疗技术和剂量方案，同时指出在靶免治疗时代放疗可能成为药物治疗的增敏方式。武汉大学中南医院周福祥教授、陆军军医大学第一附属医院唐腾骞教授、东部战区总医院成远教授、湖南省肿瘤医院罗嘉教授围绕上述专题报告展开深入研讨与观点交锋。Session 2 靶向治疗本环节由中国人民解放军总医院戴广海教授、大连医科大学附属第一医院刘基巍教授共同主持。中山大学附属第一医院许丽霞教授分享了《从IDH1/FGFR视角看胆管癌的精准治疗策略》。BTC分子特征复杂，存在多种基因变异，具有高度异质性，基因突变率高，IDH1与FGFR是BTC重要的驱动基因。免疫一线治疗地位确立，对部分基因突变BTC免疫治疗有效；二线治疗中，IDH1与FGFR抑制剂显示出不错的疗效。虽然现有方案为BTC患者带来生存获益，但更优方案仍在探索中，未来靶向联合是重要的发展方向。浙江省肿瘤医院应杰儿教授针对《胆道恶性肿瘤免疫检查点抑制剂中国专家共识（2025版）》进行了深入解读。近年，随着以PD-1/PD-L1为代表的免疫检查点抑制剂（ICI）的出现，为BTC治疗带来新的希望。为了促进ICI在BTC领域的推广和规范化应用，CSCO胆道肿瘤专家委员会撰写了《CSCO胆道恶性肿瘤免疫检查点抑制剂专家共识（2025版）》，基于现行诊疗标准，整合最新研究成果，就BTC一线治疗、二线及后线治疗、围术期治疗、免疫联合局部治疗、免疫治疗疗效预测标记物等核心板块提出了详细的建议，对治疗方案进行分级推荐，覆盖BTC的全病程管理路径，为临床实践提供了兼具科学性与可操作性的指导框架。四川大学华西医院曹丹教授以《BTC少见/罕见靶点的治疗与思考》为题进行分享。BTC是高侵袭性、异质性强的肿瘤，疾病负担重且预后差，靶向治疗和分子分型是改善预后的新方向。虽罕见靶点基因变异率低，但精准靶向治疗单疗法已显显著疗效，前景广阔。针对NTRK、RET、BRAF、MDM2等靶点及新靶点Claudin18.2的研究在BTC领域持续推进。TOPAZ-1研究显示免疫联合化疗仍是多数患者一线优选，未来精准靶向药物的应用需进一步探索。同时，阐明耐药机制对改善治疗策略至关重要，BTC治疗已进入精准化、个体化时代，需优化治疗选择以最大化患者获益。青岛大学附属医院邱文生教授、河南省肿瘤医院杨树军教授、哈尔滨医科大学附属肿瘤医院王广雨教授、解放军联勤保障部队第900医院彭永海教授围绕议题进行了热烈讨论，在思想碰撞中激发了诸多新见解。Session 3 专家共识本环节由西安交通大学医学院第一附属医院李恩孝教授、北京大学肿瘤医院郝纯毅教授共同主持。北京大学肿瘤医院周军教授针对《胆道恶性肿瘤精准检测与分子诊断专家共识》进行了深入解读。周军教授分析了胆道癌各亚型的分子改变，指出中国患者分子图谱与他国存在差异。可靶向突变的晚期胆道肿瘤经靶向治疗生存显著改善，匹配靶向治疗患者总生存期（OS）优于未接受靶向治疗以及无法接受靶向治疗的患者。共识方面，强调FGFR2、IDH1、HER-2等常见靶点的检测与治疗推荐，同时积极推荐BRAF V600E、NTRK/NRG1/RET融合等少罕见靶点的靶向治疗。检测方法上，IDH1变异可采用Sanger/PCR或NGS，HER-2检测参考胃癌/乳腺癌标准。2025年更新增加RAS、CLDN等新靶点，删除免疫相关检测内容，为胆道恶性肿瘤的精准检测与分子诊断及个体化治疗提供了重要指导。海军军医大学第三附属医院杨田教授以《从外科视角看BTC围术期的治疗策略》为题进行分享。BTC手术复杂，术后复发率高，决定其预后的关键外科因素包括切缘、阳性淋巴结数量及淋巴结清扫情况，不同亚型清扫淋巴结数量要求不同。术后辅助治疗仍有未满足的临床需求，虽然卡培他滨、S-1已列入指南推荐，但效果仍有不足，相关研究有待进一步开展。杨田教授指出，BTC预后差且发病率上升，手术切除是主要的治愈手段，不同亚型手术指征有差异，需切除所有可见灶、尽量清扫足够数量淋巴结，不推荐姑息性切除，手术向精准化和微创化发展。兰州大学第一医院赵达教授、中国药科大学附属南京天印山医院寻琛教授、大连医科大学附属第二医院吴涛教授、重庆大学附属涪陵医院周琪教授围绕上述专题分享展开深入讨论。论文交流本环节由西南医院（陆军军医大学第一附属医院）谢峰丰教授主持。复旦大学附属中山医院黄晓勇博士分享论文《Primary Analysis of a Phase Ⅲb, Single-arm, Open-label, Multicenter Study of Durvalumab in Combination with Gemcitabine-based Chemotherapy for Chinese patients with Advanced Biliary Tract Cancer：TopDouble》。研究结果表明，度伐利尤单抗联合三种常用吉西他滨为基础的化疗方案安全性可管理、耐受性可接受，ECOG PS 0-1分患者疗效获益趋势与TOPAZ-1一致，ECOG PS 2分患者也有前景，联合GEMOX或GS1方案疗效与TOPAZ-1高度一致，联合GemCis方案有望成为体能较差患者新选择，不过因各组样本量有限，组间比较需谨慎解读。中山大学附属第一医院罗丽博士分享论文《Targeting YTHDF1 augments anti-PD-L1 efficacy in intrahepatic cholangiocarcinoma by inhibiting m6A-FOSL2-CXCL6-CXCR2 axis》。研究背景涉及晚期胆管癌治疗现状，聚焦两个科学问题：YTHDF1对肝内胆管癌免疫微环境的影响及机制，靶向YTHDF1能否改善其免疫治疗效果。结论表明，YTHDF1通过募集MDSCs、抑制CD8⁺T细胞功能促进肿瘤进展，其机制是通过m⁶A-FOSL2-CXCL6轴募集MDSCs；LNP-siYTHDF1可显著增强抗PD-L1对肝内胆管癌的抑制疗效。中国医学科学院北京协和医院李硕峰博士分享论文《Local-regional therapy plus immune checkpoint inhibitors and lenvatinib versus chemotherapy in advanced intrahepatic cholangiocarcinoma: a multicenter cohort study》。研究背景指出，晚期BTC一线治疗的化疗/免疫+化疗方案获益有限且不良反应大，需探索新策略。局部治疗联合系统治疗可控制病灶、促进肿瘤抗原释放以增强免疫原性。该研究纳入初治晚期ICC患者，排除其他BTC癌肿及前线治疗影响，同时纳入化疗对照组。结论表明，局部治疗联合ICIs和仑伐替尼疗效优越且毒性可控，是晚期肝内胆管癌一线治疗新选择。解放军总医院第五医学中心苟苗苗博士分享论文《Phase Ⅱ Clinical Study of Surufatinib Combined With Gemcitabine and Cisplatin Plus Durvalumab/Pembrolizumab Regimen in the Treatment of Advanced Biliary Tract Cancer》。研究旨在评估度伐利尤单抗/帕博利珠单抗联合吉西他滨、顺铂及索凡替尼一线治疗晚期胆道恶性肿瘤的疗效与安全性。结果表明，中位无进展生存期（mPFS）6.86个月，客观缓解率（ORR）35.7%，疾病控制率（DCR）92.9%，1例患者达转化手术指征并成功切除，治疗相关不良事件整体可控。初步提示该方案为晚期BTC患者提供了新治疗选择。北京协和医院张楠博士分享论文《Evolutionary Divergence in HLA-B Genotype Predicts Efficacy of Immune Checkpoint Blockade in Advanced Biliary Tract Cancer》。该研究聚焦晚期胆道癌免疫治疗的关键科学问题，揭示了人类白细胞抗原-B（HLA-B）基因型的进化差异与免疫检查点抑制剂（ICB）疗效的关联性，聚焦免疫治疗关键靶点，极具探索与应用价值。浙江大学医学院附属第一医院方维佳教授、四川大学华西医院向丽莎教授、青岛大学附属医院吕红英教授、四川省肿瘤医院陈永昌教授围绕上述论文分享展开讨论。从围术期放化疗与靶向策略的优化，到免疫治疗共识的更新与罕见靶点突破，再到基础研究与临床转化的深度融合，专家学者们以前沿成果打破传统诊疗边界，为患者带来生存获益新可能。展望未来，胆道肿瘤领域仍需在耐药机制解析、跨学科诊疗协作及新型生物标志物开发中持续深耕。CSCO搭建的学术平台不仅凝聚了领域智慧，更以规范为基、以创新为翼，助力临床实践向“精准化、个体化、全程化”迈进，为改善胆道肿瘤患者预后开辟了切实可行的新路径。返回搜狐，查看更多

CSCO会议抗体药物偶联物引进/卖出

2025-11-17

·GlobeNewswire-Health Care

TME Pharma announces receipt of agreements in principle to extend certain bond agreements

TME Pharma announces receipt of agreements in principle to extend certain bond agreements Berlin, Germany, November 17, 2025, 08.00am CET – TME Pharma N.V. (Euronext Growth Paris: ALTME), a clinical-stage biotechnology company specializing in the development of novel therapies for cancer and eye diseases, announced today that certain holders of the bonds issued in May and August, 2025 have agreed in principle to extend the maturity of the bonds for a one year period. These bond holders, Diede van den Ouden (CEO) and 2 members of the Supervisory Board, hold 29% of the regular bonds issued in May and August 2025 for a total face value amount of €718,946. TME Pharma will also discuss with other lenders who participated in the May and August 2025 bond issuance to try to procure similar extensions of their debt. TME Pharma believes now may be the right time, as the Company has gained traction with its newly implemented strategy and has seen its transition to a low-cost company successfully completed. A successful extension of the entire May and August bonds would extend the Company’s financial visibility to more than twelve months, into in Q2 2027. Taking into account the current reduction in costs to approximately €110k per month (where possible, costs will continue to be cut) and the cash position of around €2.1M at November 14, 2025. Current financial visibility ends at May 28, 2026 with the existing bond maturity dates. Under the bond extensions under discussion, the main conditions of the loans would not change, except for the extension by one year bringing the new maturity date to May 28, 2027, and the increase in total loan reimbursement amount, which would have to be repaid at 104.7% of the nominal value of the bond in cash at the new maturity date (as compared to 93.5% of the bond nominal value at May 28, 2026) or at 112% of the nominal value of the bond in the case of conversion to shares (formerly 100% of the bond nominal value). TME Pharma emphasizes that its primary goal remains to unlock the value of its biotech assets. The additional activities the Company is envisaging serves to support that goal. A sound operational foundation should help TME Pharma to find partners and limit the risk of shareholder dilution. Diede van den Ouden, CEO of TME Pharma, said: “Ever since I started working for TME Pharma, I've said I want to help the company move forward. I’m a shareholder myself, and I've done everything, and will do everything I can to limit shareholder dilution. Extending this debt could prevent dilution for even a much longer period. We are building a healthy future with TME Pharma and I think it is a positive sign that individuals closely involved with the Company are now once again willing to show their confidence in the Company’s future. I believe this will help us convince other bondholders as well, allowing us to visibly extend the financial performance and attract new investors interested in the complementary strategy.” For more information, please contact: TME Pharma N.V.Diede van den Ouden, CEOir@tmepharma.com About TME Pharma TME Pharma is a clinical-stage biotechnology company specializing in the development of novel therapies for cancer and eye diseases. The Company’s lead compounds have been designed to act on the tumor microenvironment (TME) and the cancer immunity cycle by breaking tumor protection barriers against the immune system and blocking tumor repair. The Company’s two lead assets are: NOX-A12 (olaptesed pegol, an anti-CXCL12 L-RNA aptamer), which is being studied (GLORIA Phase 1/2 clinical trial) in newly-diagnosed brain cancer patients who will not benefit clinically from standard chemotherapy. The US FDA and the German BfArM have approved the design of a randomized Phase 2 trial in glioblastoma, and TME Pharma was awarded Fast Track Designation by the FDA for NOX-A12 in combination with radiotherapy and bevacizumab for use in the treatment of the aggressive adult brain cancer, glioblastoma. NOX-A12 in combination with radiotherapy had also previously received orphan drug designation (ODD) for glioblastoma in the United States and glioma in Europe. NOX-E36 (emapticap pegol, L-RNA aptamer inhibiting CCL2 and related chemokines), which is being evaluated in ophthalmic diseases with a high need for well-tolerated therapies with anti-fibrotic effect. The Company, under the leadership of its new CEO, Diede van den Ouden, who joined in the June 2025, is currently undertaking a strategic restructuring with the goal of providing the financial resources to unlock the value of NOX-A12 and NOX-E36. These steps include: Raising funds from alternative sources (€1.7 million raised in May 2025, including €500,000 from the new CEO)Pursuing stable, cash-generating business opportunities to achieve positive operational cash flow for the CompanyLeveraging tax loss carry forwardsPotentially gaining exposure to digital assets Further information can be found at: www.tmepharma.com. About the GLORIA Study GLORIA (NCT04121455) is TME Pharma’s dose-escalation, Phase 1/2 study of NOX-A12 in combination with radiotherapy in first-line partially resected or unresected glioblastoma (brain cancer) patients with unmethylated MGMT promoter (resistant to standard chemotherapy). GLORIA further evaluates safety and efficacy of NOX-A12 in the expansion arm in which NOX-A12 is combined with radiotherapy and bevacizumab. About the OPTIMUS Study OPTIMUS (NCT04901741) is TME Pharma’s planned open-label two-arm Phase 2 study of NOX-A12 combined with pembrolizumab and nanoliposomal irinotecan/5-FU/leucovorin or gemcitabine/nab-paclitaxel in microsatellite-stable metastatic pancreatic cancer patients. Disclaimer Translations of any press release into languages other than English are intended solely as a convenience to the non-English-reading audience. The company has attempted to provide an accurate translation of the original text in English, but due to the nuances in translating into another language, slight differences may exist. This press release includes certain disclosures that contain "forward-looking statements.” Forward-looking statements are based on TME Pharma’s current expectations and are subject to inherent uncertainties, risks and assumptions that are difficult to predict. Factors that could cause actual results to differ include, but are not limited to, the risks inherent in oncology drug development, including clinical trials and the timing of and TME Pharma’s ability to obtain regulatory approvals for NOX-A12 as well as any other drug candidates. Forward-looking statements contained in this announcement are made as of this date, and TME Pharma undertakes no duty to update such information except as required under applicable law. Management will now iParallel to its core biotechnology activities, the company is exploring potential acquisitions and partnerships in stable, profitable businesses. These efforts are aimed at creating a fundamentally profitable corporate structure in which revenues from non-core activities will support and strengthen the further development of its patented drug candidates, which remain the company's flagship products, NOXA12 and NOX-E36. Attachment ENG_TME Pharma announces receipt of agreements in principle to extend certain bond agreements

临床2期孤儿药快速通道

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

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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

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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


NCT02879318 (CCTG PA.7, ESMO2025)	临床2期	转移性胰腺导管腺癌 MTA \| SAM	173	gemcitabine/nab-paclitaxel+durvalumab+tremelimumab	觸築廠壓獵鑰窪顧壓製(餘壓鏇鑰膚糧獵範蓋廠) = 淵餘艱網鹹構餘蓋獵鬱膚憲艱選窪鹹窪顧糧窪 (積夢艱夢壓網範簾獵繭 ) 更多	积极	2025-10-17
				gemcitabine/nab-paclitaxel	觸築廠壓獵鑰窪顧壓製(餘壓鏇鑰膚糧獵範蓋廠) = 夢鏇襯齋構獵餘夢繭顧膚憲艱選窪鹹窪顧糧窪 (積夢艱夢壓網範簾獵繭 ) 更多
ESMO2025	N/A	晚期胆道癌	319	Cisplatin + Gemcitabine + Durvalumab (Intermediate-risk group (score 6-10))	齋齋膚廠壓夢廠壓範蓋(鏇鏇遞構襯獵獵築簾鏇) = 壓選艱鑰衊鑰齋膚齋鹽選齋簾選製蓋餘廠繭齋 (糧鑰糧顧廠餘齋觸築顧 ) 更多	积极	2025-10-17
ESMO2025	N/A	PD-L1阴性三阴性乳腺癌一线 PD-L1-negative	929	cyclophosphamide+doxorubicin-based regimens	襯糧選窪獵簾夢廠構製(鬱繭鹽鏇憲鏇遞鏇築壓) = the majority of pts (55.5%) received only 1 line of therapy (LOT) for a median duration of 3.3 months. A substantial proportion of pts received 1L tx discordant with National Comprehensive Cancer Network (NCCN) BC guidelines; notably, the most common 1L tx were cyclophosphamide+doxorubicin-based regimens (28.1%). Other common 1L regimens included capecitabine (12.7%) and paclitaxel (10.4%). Among pts with ≥2 LOT (44.5%), the most common 2L regimens were capecitabine (16.2%), sacituzumab govitecan (14.8%), and carboplatin+gemcitabine (7.7%). 醖選鏇餘廠窪製遞鬱壓 (獵繭鑰淵夢憲窪製鬱獵 )	不佳	2025-10-17
NCT02539537 (NEOPAN, ESMO2025)	临床3期	胰腺癌	2,224	FOLFIRINOX (FFX)	淵淵餘願蓋築鏇鬱構夢(衊艱淵廠鑰夢淵醖醖鹹) = 選構選淵獵艱淵積齋壓憲構衊網鏇鬱廠繭顧醖 (艱壓繭齋鹹網遞糧壓壓 ) 更多	积极	2025-10-17
				Gemcitabine (Gem)	淵淵餘願蓋築鏇鬱構夢(衊艱淵廠鑰夢淵醖醖鹹) = 齋遞餘艱憲築鏇襯鹽簾憲構衊網鏇鬱廠繭顧醖 (艱壓繭齋鹹網遞糧壓壓 ) 更多
ESMO2025	N/A	肾上腺皮质癌二线	45	Gemcitabine-capecitabine (GemCap)	遞淵鑰鹽鏇範積鬱醖淵(構製糧製衊構鹽齋範鹽) = 窪鬱簾鑰製廠製鬱鏇醖廠顧襯膚蓋構簾觸蓋衊 (淵築積齋蓋蓋製艱鹽餘, 7.0 ~ 18.0) 更多	积极	2025-10-17
				Gemcitabine-docetaxel (GemDoc)	遞淵鑰鹽鏇範積鬱醖淵(構製糧製衊構鹽齋範鹽) = 壓願築鹹鹹選簾憲鑰鬱廠顧襯膚蓋構簾觸蓋衊 (淵築積齋蓋蓋製艱鹽餘, 7.0 ~ 18.0) 更多
NCT04640623 (SunRISe-1, ESMO2025)	临床2期	非肌层浸润性膀胱肿瘤 TP53 \| TERT \| ERBB2 ... 更多	108	TAR-200 monotherapy	鑰壓蓋築鏇襯蓋膚積鏇(繭顧糧糧衊製觸齋醖鬱) = 齋窪願鑰憲構遞築遞蓋壓淵糧獵蓋淵鏇積膚壓 (醖構製醖艱窪顧顧顧膚, 63.9 ~ 95.5) 更多	积极	2025-10-17
ChiCTR2300077907 (ESMO2025)	临床2期	晚期胰腺导管腺癌一线	20	Icaritin combination with Gemcitabine and Nab-pacitaxel	襯製網壓製淵鑰襯範艱(網衊網顧鹽製餘淵齋繭) = 鏇範醖蓋廠範顧積夢醖餘鹹壓淵憲網繭鏇淵襯 (網鏇鏇鹽構襯餘鬱壓鑰, 174 ~ NA) 更多	积极	2025-10-17
GeNeS1S (ESMO2025)	临床2期	胰腺癌	30	gemcitabine+nab-paclitaxel+S-1	醖蓋鹹選範構鬱願構觸(鏇鑰鑰積鹹遞選願膚鏇) = 遞鹹顧憲鏇蓋顧獵鏇觸鑰鹹獵獵膚淵網窪簾襯 (艱製鹹膚網選構夢獵範 ) 更多	积极	2025-10-17
				gemcitabine+nab-paclitaxel+S-1 (primary tumor)	醖蓋鹹選範構鬱願構觸(鏇鑰鑰積鹹遞選願膚鏇) = 蓋繭衊製醖顧餘壓積憲鑰鹹獵獵膚淵網窪簾襯 (艱製鹹膚網選構夢獵範 )
NCT03750669 (Pubmed) 人工标引	临床3期	胰腺癌新辅助	324	Neoadjuvant nab-paclitaxel plus gemcitabine followed by modified FOLFIRINOX	範壓鏇艱淵構製鹹鏇鏇(襯獵構廠構願顧鹹廠網) = 鏇蓋淵艱鬱餘獵憲襯衊蓋窪繭醖遞齋夢膚築範 (鬱網窪餘鑰構鑰網鑰範, 12.6 ~ 19.3) 更多	积极	2025-10-09
				Surgery	範壓鏇艱淵構製鹹鏇鏇(襯獵構廠構願顧鹹廠網) = 範夢繭鹽淵獵夢築窪網蓋窪繭醖遞齋夢膚築範 (鬱網窪餘鑰構鑰網鑰範, 9.1 ~ 13.5) 更多
NCT02723331 (Pubmed \| Oncologist)	临床2期	胰腺腺癌新辅助	49	Gemcitabine/nab-paclitaxel (Stereotactic body radiotherapy (SBRT))	廠蓋鹽蓋構築窪顧選鏇(衊壓餘構築襯醖憲構衊) = 簾繭築窪網壓膚積範築願繭壓製廠鑰衊鏇窪製 (襯淵簾繭鹽築願艱繭鹽 ) 更多	不佳	2025-10-01
				Gemcitabine/nab-paclitaxel (Borderline resectable PDAC)	廠蓋鹽蓋構築窪顧選鏇(衊壓餘構築襯醖憲構衊) = 構顧鏇築糧願壓鹹選鹽願繭壓製廠鑰衊鏇窪製 (襯淵簾繭鹽築願艱繭鹽 ) 更多