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.

NCT04910386

/ Not yet recruiting临床2期

A Randomized, Open-Label, Multicenter Phase 2 Study of Envafolimab in Combination With Gemcitabine Plus Cisplatin Versus Gemcitabine Plus Cisplatin as the First-line Treatment in Patients With Locally Advanced or Metastatic Biliary Tract Cancers

This is a Randomized, Open-Label, Multicenter Phase 2 Study to access the efficacy and safety of Envafolimab in Combination with Gemcitabine Plus Cisplatin Versus Gemcitabine Plus Cisplatin as the First-line Treatment in Patients with Locally Advanced or Metastatic Biliary Tract Cancers

开始日期2027-06-01

申办/合作机构

四川思路康瑞药业有限公司

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

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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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13,197

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.

2026-03-01·Oncology and Therapy

Neoadjuvant Therapy in Cisplatin-Ineligible Muscle-Invasive Bladder Cancer: Recent Progress, Challenges, and Future Directions in the Era of TAR-200 and Enfortumab Vedotin Plus Pembrolizumab

Review

作者: Buonerba, Carlo ; Di Lorenzo, Giuseppe ; Di Maio, Massimo

Cisplatin-based neoadjuvant chemotherapy (NAC) followed by radical cystectomy remains the standard of care for patients with nonmetastatic muscle-invasive bladder cancer (MIBC) who are eligible for cisplatin. However, many patients cannot receive cisplatin because of renal dysfunction, frailty, neuropathy, ototoxicity, or comorbidities, leaving an unmet need for effective cisplatin-free perioperative options. Single-arm phase 2 studies of neoadjuvant immune checkpoint inhibitors (ICIs) have shown encouraging pathologic complete response (pCR) rates in patients who are ineligible for cisplatin or who decline it, and randomized survival evidence has only recently begun to mature. Two conceptually distinct cisplatin-free paradigms are now shaping the field: (1) systemic intensification with perioperative enfortumab vedotin plus pembrolizumab, an antibody-drug conjugate (ADC) plus programmed death 1 (PD-1) inhibitor regimen supported by phase 3 data; and (2) bladder-centered intensification with TAR-200 (intravesical sustained-release gemcitabine) combined with systemic PD-1 blockade, which has demonstrated promising pathologic activity in early-phase studies but remains investigational in MIBC. This narrative review summarizes the evolving perioperative evidence base across traditional NAC, neoadjuvant ICI monotherapy, ADC-ICI combinations, and locoregional drug delivery approaches; highlights key interpretive challenges including heterogeneous trial populations and endpoints and the limitations of cross-trial comparisons; and discusses future directions such as response-adapted escalation and de-escalation strategies using circulating tumor DNA and urinary tumor DNA. We present a conceptual framework for future prospective trials evaluating how systemic and bladder-centered strategies might be selected and sequenced, rather than definitive guidance for routine clinical practice.

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.

1,366

项与盐酸吉西他滨相关的新闻（医药）

2026-04-16

·ioncology

CSCO BC大咖对话丨郝春芳、陈占红教授：Trop-2 ADC改写《CSCO BC指南》，晚期TNBC进入ADC一线治疗时代

点击上方蓝字关注我们编者按：三阴性乳腺癌（TNBC）因其异质性高、侵袭性强、预后差，被成为“最凶险”的乳腺癌亚型。在传统化疗治疗获益有限且毒副作用大的背景下，新型Trop-2 ADC戈沙妥珠单抗（Sacituzumab Govitecan，SG）的ASCENT（含“攀登、上升”之意）系列研究取得了突破性进展，为晚期TNBC一线治疗提供了更优治疗方案。在《中国临床肿瘤学会（CSCO）乳腺癌诊疗指南》（以下简称《CSCO BC指南》或指南）中，SG单药或联合免疫治疗已成功跻身晚期TNBC一线治疗推荐。《肿瘤瞭望》特邀天津医科大学肿瘤医院郝春芳教授、浙江省肿瘤医院陈占红教授解读治疗更新如下。聚焦· 晚期TNBC的临床治疗痛点《肿瘤瞭望》：三阴性乳腺癌（TNBC）始终是乳腺癌诊疗领域的难点，晚期患者的生存预后更是面临严峻挑战。能否请您谈谈当前晚期 TNBC 的整体诊疗现状，以及一线治疗中仍存在哪些亟待解决的临床痛点与未被满足的需求？陈占红教授浙江省肿瘤医院 TNBC 约占全部乳腺癌的 15%-20%[1]，由于具有高异质性、缺乏明确治疗靶点、疾病进展快、复发转移风险高等特征，TNBC始终是乳腺癌诊疗领域中预后最差的亚型，也是临床攻坚的重点与难点。当前晚期 TNBC 的一线诊疗，仍面临着疗效与安全性的双重瓶颈，以及大量未被满足的临床需求。在传统治疗层面，既往晚期 TNBC 一线治疗长期以紫杉类联合铂类的化疗方案为核心，其中位无进展生存期（PFS）仅 6-9 个月，且化疗相关不良反应发生率高，约 45% 的患者因毒性导致治疗停药，患者治疗耐受性与依从性均受到严重影响[2-3]。近年来，免疫治疗、PARP 抑制剂等精准治疗方案的问世，虽为部分晚期 TNBC 患者带来了明确的生存获益，但其临床应用仍存在显著的人群覆盖局限：PD-1/L1免疫检查点抑制剂治疗的获益人群主要集中于 PD-L1 表达阳性的患者，且现有方案的生存改善效果仍存在明显的提升空间；PARP 抑制剂则仅适用于携带 gBRCA1/2 突变的特定人群，此类突变在 TNBC 患者中整体发生率较低，临床中绝大多数患者仍无法从这类精准靶向方案中获益。由于治疗有限，临床中有近三分之一转移性 TNBC 患者止步于一线治疗，无法接受后续二线治疗。因此，临床亟需能够覆盖全人群、高效低毒、可显著延长患者生存且耐受性良好的一线治疗方案，突破现有治疗的疗效天花板，改善患者整体生存预后。共享· 新型Trop-2 ADC的“攀升”之路《肿瘤瞭望》：过去一年，Trop-2 ADC的一系列进展引领TNBC一线治疗变革，以SG为代表的ASCENT-04 和 ASCENT-03 两项重磅研究结果在国际大会发布并见刊《NEJM》。您如何看待这两项研究的价值？郝春芳教授天津医科大学肿瘤医院 2025年晚期TNBC领域迎来重要的突破性研究进展，其中ASCENT-03[4]、ASCENT-04[5]研究是尤其引人瞩目的两项研究。这两项全球多中心临床研究均聚焦于晚期TNBC一线治疗。ASCENT-04 研究主要针对PD-L1阳性的适合免疫治疗的晚期TNBC患者，分别使用SG或传统化疗联合免疫检查点抑制剂的一线治疗。研究数据显示，SG 联合帕博利珠单抗可延长患者中位 PFS （11.2 vs 7.8个月），较传统化疗联合免疫方案显著降低 35% 的疾病进展或死亡风险（HR 0.65，95%CI：0.51-0.84；P＜0.001）；同时显著增加肿瘤缓解深度与持续时间，完全缓解（CR）率接近翻倍（13% vs 8%）；目前该研究OS尚不成熟，在一线治疗进展后，化疗联合帕博利珠单抗组继续治疗人群中有81%的患者接受了SG二线治疗，在此背景下，OS仍展现出获益趋势，SG联合帕博利珠单抗组较对照组降低了11%的死亡风险（HR 0.89）。在安全性方面，联合方案未新增额外毒副作用，治疗停药率仅为化疗对照组的三分之一。ASCENT-04研究为 PD-L1 阳性的晚期TNBC患者一线治疗提供了新选择。 ASCENT-03 研究恰好与ASCENT-04研究形成互补，主要针对PD-L1阴性和不适合免疫治疗的 mTNBC 人群，使用SG单药或传统化疗。研究结果显示，SG 单药治疗的中位 PFS 达 9.7 个月，较传统化疗（6.9个月）延长 2.8 个月，疾病进展或死亡风险显著降低 38%，所有关键亚组均显示一致获益；在82%的TPC组患者疾病进展后选择SG作为二线治疗的情况下，SG 组相较于TPC组仍延长PFS2达 4.2 个月（18.2 vs 14.0 个月），降低二次进展或死亡风险达 30%（HR 0.7，95% CI：0.55～0.90），和ASCENT-04研究一样，ASCENT-03研究也尚未成熟，正在观察随访中。在安全性方面，SG的表现与既往一致，安全可耐受。在试验设计上，两项研究充分体现了对患者全程治疗获益的重视，由于目前SG已经获批了TNBC二线治疗适应症，故两项研究在充分考虑对照组获益的基础上，均采用了交叉（cross-over）设计，允许对照组二线阶段接受 SG 治疗，这一设计既坚守了临床试验的伦理底线，也传递出了为患者规划全程治疗获益的诊疗理念。见证· SG改写国内外权威指南《肿瘤瞭望》：随外各大权威乳腺癌指南均就此做了重要更新。能否请您梳理盘点一下，目前国内外指南对SG 在晚期 TNBC 一线治疗中的推荐情况，以及这些指南更新背后的临床意义？陈占红教授浙江省肿瘤医院正如刚刚郝春芳教授所分享的， ASCENT-03、ASCENT-04 两项全球多中心 III 期研究为SG在TNBC的一线治疗提供了坚实的循证医学证据。基于此，2026版《CSCO BC指南》推荐：对于紫杉类敏感的晚期TNBC患者：新增SG单药为II级推荐（1B类证据）；解救免疫治疗方面新增SG＋PD-1抑制剂为II级推荐（1B类证据）。对于紫杉类失败的晚期TNBC患者：SG单药升级为I级推荐（1B类证据）；解救免疫治疗方面新增SG＋PD-1抑制剂为II级推荐（1B类证据）。上述推荐不仅能满足晚期 TNBC 患者疗效提升的治疗需求，还能全面覆盖晚期TNBC患者，同时具备充分的临床实践可行性，全面确立了 SG 在晚期 TNBC 治疗中的核心权威地位。 △2026版《CSCO BC指南》mTNBC解救化疗推荐 △2026版《CSCO BC指南》mTNBC解救免疫治疗推荐与此同时，2026版《CBCS指南精要版》[6]也将SG 作为当前唯一纳入晚期 TNBC 一线治疗推荐的 ADC 药物。指南建议，PD-L1阳性TNBC的一线治疗，SG联合帕博利珠单抗为“可选”方案；一般人群或未检测到治疗靶点的TNBC一线治疗，SG单药也为“可选”方案。在国际指南层面，《NCCN 乳腺癌指南2026 v2版》[7]建议，对于PD-L1 CPS≥10的TNBC一线治疗，SG联合帕博利珠单抗为1类证据，优先推荐；对于PD-L1 CPS＜10且无BRCA1/2突变的TNBC一线治疗，SG单药同样为1类证据，优先推荐。国内外权威指南的同步推荐，主要源于 SG 扎实的全人群获益证据，使更多TNBC患者获益的得到提升，有力推动了晚期 TNBC 一线治疗水平提升。展望· 夯实ADC一线治疗的中国证据《肿瘤瞭望》：国内外指南对于SG的推荐助力晚期 TNBC 全面迈入 ADC时代。展望未来，您对 SG在乳腺癌领域的临床应用与发展有哪些期待？郝春芳教授天津医科大学肿瘤医院基于多项III期研究结果，国内外权威指南迅速将其纳入晚期TNBC一线治疗推荐，标志着该领域正式迈入ADC治疗优选时代。此突破性进展改变了现有治疗格局，对未来治疗影响深远。期待SG相关一线治疗适应症能够尽快在国内获批，造福中国晚期TNBC患者。全球多中心的ASCENT-03、04研究中，对于既往接受过免疫治疗但未耐药的患者，后续治疗情况不清楚。鉴于诸多未满足的临床需求，中国已开展ASCENT-C04研究。该全国多中心研究聚焦中国人群。鉴于国内已有CPS≥1获批的PD-1单抗治疗，该研究将适合免疫治疗人群界定为CPS≥1，联合免疫治疗药物为特瑞普利单抗，且允许既往接受过免疫治疗的患者一线再应用。我们期待该研究能产生针对中国人群的高质量循证证据，为本土临床实践提供更具针对性的用药指导。总之，SG正在全面布局TNBC领域，期待着更多临床研究的开花结果，最终实现乳腺癌患者生存时长与生活质量的双重提升，推动乳腺癌的稳步迈向治愈。参考文献上下滑动查看更多内容 [1] Camorani S, Fedele M, Zannetti A, Cerchia L. TNBC Challenge: Oligonucleotide Aptamers for New Imaging and Therapy Modalities. Pharmaceuticals (Basel).2018;11(4):123. Published 2018 Nov 13. [2] Yardley DA, Coleman R, Conte P, et al. nab-Paclitaxel plus carboplatin or gemcitabine versus gemcitabine plus carboplatin as first-line treatment of patients with triple-negative metastatic breast cancer: results from the tnAcity trial. Ann Oncol. 2018;29(8):1763-1770. [3] Wang B, Sun T, Zhao Y, et al. A randomized phase 3 trial of Gemcitabine or Nab-paclitaxel combined with cisPlatin as first-line treatment in patients with metastatic triple-negative breast cancer. Nat Commun. 2022;13(1):4025. Published 2022 Jul 12. [4] Cortés J, Punie K, Barrios C, et al. Sacituzumab Govitecan in Untreated, Advanced Triple-Negative Breast Cancer. N Engl J Med. 2025;393(19):1912-1925. [5] Tolaney SM, de Azambuja E, Kalinsky K, et al. Sacituzumab Govitecan plus Pembrolizumab for Advanced Triple-Negative Breast Cancer. N Engl J Med. 2026;394(4):354-366. [6] 《中国抗癌协会与中华医学会肿瘤学分会乳腺癌诊治指南与规范》编纂秘书处. 中国抗癌协会与中华医学会肿瘤学分会乳腺癌诊治指南与规范（2026年版精要本）. 2025.12.20. [7] NCCN. NCCN Guidelines Version2. 2026 Invassive Breast Cancer. Available at [2026.03.03] https://www.nccn.org/professionals/physician_gls/pdf/breast.pdf 郝春芳教授医学博士、硕士生导师天津市肿瘤医院空港医院乳腺内科科主任中国临床肿瘤学会乳腺癌专家委员会委员中国抗癌协会乳腺癌专业委员会委员中国抗癌协会肿瘤防治科普专业委员会委员中国女医师协会乳腺专委会常务委员北京癌症防治学会乳腺癌青年委员会副主任委员北京癌症防治学会乳腺癌个体化诊疗及MDT专委会常务委员北京乳腺病防治学会健康管理专业委员会常务委员天津市药理学会肿瘤药理专委会委员陈占红教授主任医师、硕士生导师浙江省肿瘤医院乳腺内科副主任兼病区主任国家抗肿瘤药物临床应用检测专家委员会乳腺癌组专家中国抗癌协会整合肿瘤心脏病学分会常务委员中国女医师协会乳腺专业委员会常务委员中国健康促进基金会乳腺疾病专家委员会常务委员中国临床肿瘤学会乳腺癌专家委员会委员/CSCO-BC指南编委中国医师协会肿瘤医师分会第二届委员会乳腺癌学组委员浙江省抗癌协会肿瘤心脏病学专业委员会主任委员浙江省数理医学学会乳腺肿瘤诊疗专业委员会主任委员浙江省数理医学学会乳腺临床试验专业委员会候任主任委员浙江省免疫学会肿瘤免疫与生物治疗专业委员会副主任委员浙江省预防医学会第一届生殖疾病预防与控制专业委员会副主任委员浙江省抗癌协会乳腺癌专业委员会常务委员（来源：《肿瘤瞭望》编辑部）声明凡署名原创的文章版权属《肿瘤瞭望》所有，欢迎分享、转载。本文仅供医疗卫生专业人士了解最新医药资讯参考使用，不代表本平台观点。该等信息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，如果该信息被用于资讯以外的目的，本站及作者不承担相关责任。

2026-04-16

·BioSpace

TME Pharma Announces Publication of NOX-A12 “Triple Therapy” Phase 1/2 Expansion Arm A Findings from GLORIA trial in Nature Communications

TME Pharma Announces Publication of NOX-A12 “Triple Therapy” Phase 1/2 Expansion Arm A Findings from GLORIA trial in Nature Communications Berlin, Germany , April 16, 2026, 08.00am CET – TME Pharma N.V. (Euronext Growth Paris: ALTME), a clinical-stage biotechnology company specializing in the development of novel therapies for braincancer and eye diseases, is pleased to announce a Nature Communications article on the results from the Phase 1/2 expansion Arm A cohort of the GLORIA trial testing NOX-A12 + radiotherapy + anti-VEGF “triple therapy” in glioblastoma patients. The article in the scientific peer-reviewed high-impact journal, Nature Communications, describes results of the expansion cohort Arm A in TME Pharma’s Phase 1/2 GLORIA trial. In this arm, chemotherapy-resistant (MGMT unmethylated) glioblastoma patients with residual tumor after surgery received NOX-A12 + radiotherapy + anti-VEGF (bevacizumab) “Triple Therapy”. The authors noted that overall survival (OS) of patients receiving NOX-A12 Triple Therapy significantly outperformed two different cohorts of similar patients external to the trial who received standard of care treatment, and further noted that due to the conservative trial design, the study “likely underestimates survival compared with most contemporary trials.” As already disclosed in the March 5, 2024 press release, the GLORIA trial has been amended to allow inclusion of 100 additional patients in a randomized, controlled Phase 2 part of the trial composed of 5 additional arms (Expansion Group Arms D through H) to assess three different doses of NOX-A12 in the Triple Therapy, one dose of NOX-A12 + radiotherapy and standard of care. It is planned to initiate this Phase 2 part of the trial once appropriate partnerships are in place. The findings described in the publication demonstrate the potential and value of TME Pharma’s NOX-A12 asset. TME Pharma remains confident in its strategy to search for a strategic partner to outlicense NOX-A12with the goal of bringing NOX-A12 to market authorization. As communicated on January 5, 2026, TME Pharma continues its active discussions with potential partners for the NOX-A12 program. As indicated in its press release of March 9, 2026, TME Pharma’s financial runway now extends to Q2-2027, providing the company with the flexibility to identify the optimal partnership for NOX-A12. Diede van den Ouden, CEO of TME Pharma , said: "We are encouraged by the publication in Nature Communications, which underscore the scientific validity of our approach. We remain fully committed to bringing NOX-A12 to success and believe that a strategic partnership is the optimal path forward. With our extended cash runway, we are well-positioned to continue our negotiations with potential partners." The full article can be found for reading through the TME Pharma website. Through the TME Pharma website > Scientific Approach > Scientific Publications and on the landing page. For more information, please contact: TME Pharma N.V. Diede van den Ouden, CEO ir@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 Company Leveraging tax loss carry forwards Potentially gaining exposure to digital assets Further information can be found at: . 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 Publication of NOX-A12 “Triple Therapy” Phase 1_2 Expansion Arm A Findings from GLORIA trial in Nature Communications

临床2期快速通道孤儿药临床结果

2026-04-16

·allsci.com

Partner Therapeutics seeking third indication for Bizengri in NRG1 fusion-positive cholangiocarcinoma

Partner Therapeutics submitted a supplemental Biologics License Application (sBLA) to the US FDA on April 14, 2026 for Bizengri (zenocutuzumab-zbco), seeking approval for adults with advanced unresectable or metastatic cholangiocarcinoma harboring an NRG1 gene fusion. The filing marks the first regulatory submission for Bizengri in this bile duct malignancy with the aim of adding a third indication to the molecule’s existing accelerated approvals in NRG1 fusion-positive non-small cell lung cancer and pancreatic adenocarcinoma. The sBLA seeks approval without restriction to a specific line of therapy, the company said. The filing is supported by data from the eNRGy study, a basket trial evaluating zenocutuzumab-zbco across NRG1 fusion-positive solid tumors. No priority review or accelerated pathway designation was disclosed in the announcement, and the company did not provide a projected PDUFA date. Bizengri’s cholangiocarcinoma data The cholangiocarcinoma cohort of the eNRGy study generated an overall response rate of 36.8% (95% CI: 16.3, 61.6%) and a median duration of response of 12.9 months, as assessed by blinded independent central review. No patients in that cohort discontinued therapy due to adverse events, the company said. The mechanism underlying the filing differs from all currently approved CCA therapies: zenocutuzumab-zbco is a bispecific antibody that simultaneously blocks HER2/HER3 heterodimerization and NRG1 fusion interactions with HER3, disrupting downstream signaling driven by NRG1 chimeric ligands rather than the chimeric receptors targeted by FGFR inhibitors such as pemigatinib and futibatinib. NRG1 fusions are estimated to occur in fewer than 2% of cholangiocarcinoma cases, and the source material states that no approved therapies currently target this molecular subgroup in the disease. The rarity of the alteration creates a diagnostic challenge: unlike NTRK, RET, or FGFR fusions, NRG1 fusions produce chimeric ligands that are frequently missed by DNA-only next-generation sequencing panels and require tissue-based RNA testing for reliable detection. Partner Therapeutics noted this in its announcement, with Chief Development Officer Pritesh Gandhi stating that RNA testing is essential to ensure patients with NRG1-driven tumors are identified. NCCN guidelines The filing arrives alongside a notable guideline development. The National Comprehensive Cancer Network added zenocutuzumab-zbco to its oncology clinical practice guidelines for biliary tract cancers as a Category 2A subsequent-line therapy and as a Category 2B recommendation for front-line treatment of NRG1 fusion-positive cholangiocarcinoma — the latter positioning preceding any formal regulatory approval for the indication. Dr. James Cleary of Dana-Farber Cancer Institute, commenting in the release, described NRG1 gene fusions as an actionable biomarker in this disease and said the eNRGy data suggest targeted inhibition with zenocutuzumab may represent a meaningful treatment approach. The cholangiocarcinoma treatment landscape has undergone substantial change since 2020, when pemigatinib became the first targeted therapy approved in the disease. Ivosidenib followed in 2021 for IDH1-mutant CCA, futibatinib in 2022 for FGFR2 fusion-positive intrahepatic disease, and durvalumab in combination with gemcitabine and cisplatin was approved the same year for first-line biliary tract cancer regardless of biomarker status. Pembrolizumab combined with gemcitabine and cisplatin received approval in 2023 for the same unselected population. Despite this expansion, the molecular subgroup defined by NRG1 fusions has remained without a specifically labeled therapy, and the eNRGy data represent the primary clinical evidence base for this population in CCA. The sBLA adds to a field where accelerated approval pathways have played a central role, and where the durability of those approvals has varied. Infigratinib, an FGFR1–3 inhibitor that received accelerated approval in 2021 for FGFR2 fusion-positive CCA, was voluntarily withdrawn in 2024 after a confirmatory trial failed to verify clinical benefit — a precedent that underscores the regulatory risk associated with response-rate-based submissions in this disease. The eNRGy cholangiocarcinoma cohort was small, as is typical for trials enrolling rare fusion-defined populations, and the 95% confidence interval for the reported ORR is correspondingly wide. Bizengri’s existing accelerated approvals in NSCLC and pancreatic adenocarcinoma were also granted based on overall response rate and duration of response, with continued approval in those indications contingent on confirmatory trial data. The cholangiocarcinoma sBLA follows the same evidentiary model. Partner Therapeutics holds exclusive US rights to develop and commercialize zenocutuzumab-zbco under an agreement with Merus B.V., a wholly owned subsidiary of Genmab. Leave a Reply Cancel reply Your email address will not be published. Required fields are marked * Comment * Name * Email * Website

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

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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	2026-05-01
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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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT05498220 (CTgov)	临床2期	复发性弥漫性大B细胞淋巴瘤	5	Hyaluronidase+Polatuzumab vedotin+GCSF+Gemcitabine+cisplatin+Dexamethasone+Rituximab+PV	顧襯範顧蓋積構齋衊築 = 鹹蓋窪範壓網獵膚餘製觸鹹壓鹹齋襯網積齋憲 (獵製網夢蓋醖夢襯夢廠, 繭鏇構齋構壓積膚積鬱 ~ 憲網鹹齋壓襯衊鏇顧遞) 更多	-	2026-04-16
ESMO_SRC2026	N/A	平滑肌肉瘤	336	Gemcitabine combined with docetaxel	顧壓糧蓋憲遞築簾繭淵(顧構觸鏇遞範繭壓壓願) = 選願糧淵鬱蓋壓願願繭襯簾壓選積簾觸鹽膚膚 (齋鹽鑰夢製鹽衊餘鏇獵 ) 更多	积极	2026-03-09
ESMO_SRC2026	N/A	平滑肌肉瘤二线	108	Trabectedin	鑰夢廠蓋憲鹽蓋觸衊壓(餘網願齋選廠餘繭簾範) = 鬱積構鬱糧憲簾鏇壓醖鑰遞鏇築願膚艱衊鑰窪 (遞鹹選衊壓簾顧糧製鏇, 5.5 ~ 15.2) 更多	积极	2026-03-09
ESMO_SRC2026	N/A	平滑肌肉瘤二线	108	gemcitabine-based chemotherapy	鑰夢廠蓋憲鹽蓋觸衊壓(餘網願齋選廠餘繭簾範) = 願鹹網蓋鬱築築網顧憲鑰遞鏇築願膚艱衊鑰窪 (遞鹹選衊壓簾顧糧製鏇, 3.8 ~ 6.4) 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	鹹構膚繭鬱鬱艱鹽簾膚(簾構積鏇鏇鏇淵窪蓋觸) = 膚遞鹽廠夢繭淵齋鹹夢顧蓋積壓遞願糧糧積範 (製襯艱壓範鹹鏇築繭蓋 ) 更多	积极	2026-03-09
ESMO_SRC2026	N/A	软骨肉瘤	10	Gemcitabine 1000 mg/m2 plus Oxaliplatin 100 mg/m2	願構膚顧齋築蓋願鹹繭(膚選構顧範膚鑰襯蓋積) = Treatment was generally well tolerated, with limited grade 3 toxicity and one case of grade 5 thrombotic microangiopathy-associated to gemcitabine 範簾夢鏇醖廠衊鏇襯膚 (鏇膚願衊餘簾齋廠壓遞 )	积极	2026-03-09
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	觸廠憲鏇窪繭襯衊範網(廠壓觸衊構糧範夢淵積) = 夢窪鹽廠鹹觸鏇鏇遞鏇鬱餘齋鏇鹽壓遞鏇簾積 (廠糧窪鏇願選鬱襯夢遞, 3.0 ~ 25.2) 更多	积极	2026-02-26
ASCO_GU2026	N/A	非肌层浸润性膀胱肿瘤	133	BCG	構襯壓衊齋網餘糧醖積(鏇選選蓋糧糧鏇範夢夢) = 網鬱鑰膚繭繭衊築鏇觸範衊獵構壓積積鏇鬱觸 (壓窪醖顧膚憲鹽憲願鹽 ) 更多	不佳	2026-02-26
ASCO_GU2026	N/A	非肌层浸润性膀胱肿瘤	133	sequential gemcitabine and docetaxel (Gem/Doce)	構襯壓衊齋網餘糧醖積(鏇選選蓋糧糧鏇範夢夢) = 願衊壓選簾淵蓋糧繭醖範衊獵構壓積積鏇鬱觸 (壓窪醖顧膚憲鹽憲願鹽 ) 更多	不佳	2026-02-26
ASCO_GU2026	N/A	肌层浸润性膀胱癌新辅助	517	Gemcitabine 800 mg/m2	顧簾選鑰壓廠鏇淵餘糧(艱壓鬱鑰遞範餘選蓋鹹): P-Value = 0.012 更多	积极	2026-02-26
ASCO_GU2026	N/A	肌层浸润性膀胱癌新辅助	517	Gemcitabine 1000 mg/m2	顧簾選鑰壓廠鏇淵餘糧(艱壓鬱鑰遞範餘選蓋鹹): P-Value = 0.012 更多	积极	2026-02-26
NCT04179162 (ALLIANCE A032303, ASCO_GU2026)	临床1/2期	复发性膀胱癌	52	Gemcitabine + BCG	壓淵襯膚顧淵構窪繭鏇(願憲簾齋繭願廠鬱顧願) = 鏇繭窪餘窪簾簾餘蓋廠衊膚齋範窪蓋鑰窪糧淵 (醖鑰蓋夢糧獵艱襯醖艱 ) 更多	积极	2026-02-26
ASCO_GU2026	N/A	肌层浸润性膀胱癌	98	Cisplatin	蓋鑰憲願廠夢鹹遞醖夢(夢窪築醖鏇窪壓憲艱壓) = 築蓋壓範鑰廠夢艱衊蓋齋衊網築廠廠襯餘壓膚 (蓋齋繭艱築艱醖淵築蓋 ) 更多	积极	2026-02-26
ASCO_GU2026	N/A	肌层浸润性膀胱癌	98	5-FU+MMC	蓋鑰憲願廠夢鹹遞醖夢(夢窪築醖鏇窪壓憲艱壓) = 鏇廠糧窪觸襯醖觸鏇襯齋衊網築廠廠襯餘壓膚 (蓋齋繭艱築艱醖淵築蓋 ) 更多	积极	2026-02-26