This phase II trial tests the impact of biomarkers in predicting initial treatment (first-line) PD1 or PD-L1 (PD[L]-1)-based immunotherapy response and in selecting second-line treatment in patients with stage IIIB-IV non-small cell lung cancer (NSCLC). Response and survival rates in advanced stage NSCLC, unlike other cancers, rely on response to first-line therapy. Immunotherapy with PD(L)1-based therapy, may induce changes in body's immune system and may interfere with the ability of tumor cells to grow and spread. While immunotherapy has improved survival rate, the prognosis remains poor with most patients receiving chemotherapy after immunotherapy. Many types of tumors tend to lose cells or release different types of cellular products including their deoxyribonucleic acid (DNA) which is referred to as circulating tumor DNA (ctDNA) into the bloodstream before changes can be seen on scans. Health care providers can measure the level of ctDNA in blood or other bodily fluids to determine which patients are at higher risk for disease progression or relapse. The first part of this trial, studying samples of blood and tissue in the laboratory from patients receiving immunotherapy may help doctors learn more about the effects PD(L)1-based therapy on cells. It may also help doctors understand how well patients respond to treatment and may help develop new individualized treatment strategies. The second part of this trial also tests the effect of second-line immunotherapy, such as tremelimumab and durvalumab or adagrasib and bevacizumab, in treating patients with NSCLC with specific genetic mutations that is growing, spreading or getting worse (progressive). Tremelimumab is a monoclonal antibody that may interfere with the ability of tumor cells to grow and spread. A monoclonal antibody is a type of protein that can bind to certain targets in the body, such as molecules that cause the body to make an immune response (antigens). Immunotherapy with monoclonal antibodies, such as durvalumab, may help the body's immune system attack the tumor, and may interfere with the ability of tumor cells to grow and spread. Adagrasib, a type of targeted therapy, may stop the growth of tumor cells by blocking a protein needed for tumor cell growth and may kill them. Bevacizumab is in a class of medications called antiangiogenic agents. It works by stopping the formation of blood vessels that bring oxygen and nutrients to tumor. This may slow the growth and spread of tumor. Giving second-line immunotherapy, tremelimumab and durvalumab or adagrasib with bevacizumab, may be safe, tolerable, and/or effective in treating patients with stage IIIB/IV NSCLC with specific genetic mutations.

开始日期2026-09-21

申办/合作机构

City of Hope National Medical Center

[+1]

NCT05403723

/ Suspended临床1期IIT

A Phase 1b Trial of Adaptive Stereotactic Body Radiotherapy in Combination With Durvalumab (MEDI4736), Platinum, and Etoposide in Extensive Stage Small Cell Lung Cancer

This is trial studying the safety of adaptive stereotactic body radiotherapy (SBRT) combined with durvalumab immunotherapy, platinum chemotherapy, and etoposide chemotherapy in platinum refractory extensive stage small cell lung cancer (SCLC).

开始日期2026-06-30

申办/合作机构

University of Maryland Baltimore

[+1]

NCT05253131

/ Not yet recruiting临床2期IIT

Phase 1/2 Trial of the MEK Inhibitor Selumetinib and Bromodomain Inhibitor ZEN-3694 With Durvalumab (MEDI4736), a PD-L1 Antibody for Sarcomas Including Malignant Peripheral Nerve Sheath Tumors

A multi-institutional open-label phase 1/2 trial of selumetinib in combination with ZEN-3694 and durvalumab in refractory/unresectable sarcomas including MPNST. The phase 1 portion will be separated in two parts and will be open to all patients with refractory/relapsed sarcomas. The phase 2 portion will be for patients with refractory/unresectable NF1-associated MPNST.

开始日期2026-05-15

申办/合作机构

The University of Alabama at Birmingham

[+1]

100 项与度伐利尤单抗相关的临床结果

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100 项与度伐利尤单抗相关的转化医学

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100 项与度伐利尤单抗相关的专利（医药）

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1,979

项与度伐利尤单抗相关的文献（医药）

2026-03-01·LUNG CANCER

Durvalumab-containing treatment for recurrent or metastatic pulmonary sarcomatoid carcinoma: A pooled post hoc analysis of two KCSG phase II trials

Article

作者: Kim, Tae Min ; Kim, Yu Jung ; Kim, Dong-Wan ; Lee, Gyeong-Won ; Keam, Bhumsuk ; Kim, Miso ; Kim, Dong Hyun ; Kim, Joo-Hang ; Ahn, Mi Sun ; Hong, Sook-Hee ; Kim, Jin-Soo ; Kim, Se Hyun ; Shin, Seong Hoon ; Youk, Jeonghwan

INTRODUCTION:

Pulmonary sarcomatoid carcinoma (PSC) is a rare cancer characterized by a high programmed death-ligand 1 (PD-L1) expression, suggesting a potential therapeutic benefit from immune checkpoint inhibitors. We investigated the efficacy of durvalumab-containing combination therapy and explored potential predictive biomarkers in patients with recurrent or metastatic (R/M) PSC.

METHOD:

In this pooled post hoc analysis, data were integrated from two prospective phase II trials (NCT03022500 and NCT04224337) wherein durvalumab-containing combination therapies were evaluated in patients with R/M PSC. PD-L1 expression was assessed using 22C3 or SP263 assays, and circulating lymphocyte subsets were analyzed using flow cytometry.

RESULTS:

Overall, 33 patients were included, of whom 66.7 % had a PD-L1 tumor proportion score (TPS) ≥ 1 % and 45.5 % had a TPS ≥ 50 %. The overall response rate was 33.3 % (95 % confidence interval [CI], 18.0 %-51.8 %), and the disease control rate was 72.7 % (95 % CI, 54.5 %-86.7 %). The median progression-free survival and overall survival were 5.4 (95 % CI, 2.8-9.4) and 15.7 (95 % CI, 11.3-not estimated) months, respectively. PD-L1 expression was not associated with the response or survival outcomes. Patients who achieved disease control exhibited a higher proportion of circulating CD8⁺ T cells (mean, 28.5 % vs. 20.3 %, P = 0.083) and a lower CD4⁺/CD8⁺ ratio (median, 1.4 vs. 1.7, P = 0.048) than did those with progressive disease.

CONCLUSION:

Durvalumab-containing combination therapy showed promising efficacy in patients with R/M PSC, irrespective of PD-L1 expression. A lower CD4⁺/CD8⁺ ratio may be associated with favorable disease control.

2026-03-01·JOURNAL OF CLINICAL ONCOLOGY

Adjuvant Durvalumab in Completely Resected Early-Stage Non–Small Cell Lung Cancer

Article

作者: Bradbury, Penelope A. ; Greillier, Laurent ; Catino, Annamaria ; Dziadziuszko, Rafal ; Domine, Manuel ; Wu, Yi-Long ; Westeel, Virginie ; Goss, Glenwood D. ; Ding, Keyue ; Molinier, Olivier ; Whittom, Renaud ; Massutí, Bartomeu ; Dingemans, Anne-Marie C. ; McLachlan, Sue-Anne ; Nakagawa, Kazuhiko ; Morin, Franck ; Toffart, Anne-Claire ; Nadal, Ernest ; Kang, Jin Hyoung ; Darling, Gail E. ; Mitsudomi, Tetsuya ; O'Callaghan, Christopher J. ; Audigier-Valette, Clarisse ; Sugawara, Shunichi ; Yamamoto, Nobuyuki ; Stockler, Martin R. ; Okada, Morihito ; Perrone, Francesco

PURPOSE:

Adjuvant immunotherapy improved patient outcomes in two trials in completely resected non–small cell lung cancer (NSCLC), but with conflicting primary end point results. The Canadian Cancer Trials Group BR.31 trial evaluated adjuvant durvalumab in completely resected early-stage NSCLC.

METHODS:

Following resection of stage IB (≥4 cm) to IIIA NSCLC (American Joint Committee on Cancer 7th Edition) and optional adjuvant chemotherapy, patients were randomly assigned 2:1 to durvalumab 20 mg/kg or placebo 20 mg/kg once every 4 weeks for 12 cycles. Random assignment was stratified by stage, extent of nodal dissection, tumor cell (TC) PD-L1 expression, adjuvant chemotherapy use, and center. The primary end point was investigator-assessed disease-free survival (DFS). Secondary outcomes included overall survival (OS), adverse events, and quality of life. The primary analysis was in the subgroup with cancers that had a PD-L1 TC expression ≥25%, no common activating EGFR mutations ( EGFR –), and no ALK gene rearrangements ( ALK –). Secondary analyses in hierarchical order included DFS in the subgroup whose tumors were EGFR–/ALK– with PD-L1 TC ≥1%, followed by all patients whose tumors were EGFR–/ALK–, followed by OS in the same primary and secondary subgroups in the same hierarchical order.

RESULTS:

Of 1,415 patients randomly assigned, 1,219 (86%) had EGFR–/ALK– tumors: 815 randomly assigned to durvalumab and 404 to placebo. With a median follow-up of 60 months, there were no differences in DFS between patients assigned durvalumab (316) versus placebo (161) in the primary population (stratified hazard ratio [HR], 0.93 [95% CI, 0.71 to 1.25]; P = .64) or in the secondary populations. Grade 3 to 4 adverse events were higher in durvalumab-treated patients (D = 26% v P = 20%).

CONCLUSION:

Adjuvant durvalumab following complete resection was not associated with improvement in DFS compared with placebo in EGFR –/ ALK – NSCLC, regardless of PD-L1 status.

2026-03-01·Case reports in women's health

Recurrent endometrial carcinoma with immune-mediated thrombocytopenia following durvalumab: A case report

Article

作者: Sakakibara, Ami ; Shirane, Terumi ; Sakai, Tomomi ; Nagai, Shimpei ; Hattori, Yoshihisa ; Kurahashi, Takashi ; Hino, Makiko ; Fujioka, Yoko

The use of immune checkpoint inhibitors (ICIs) has expanded the therapeutic landscape for advanced or recurrent endometrial carcinoma. Durvalumab-a programmed death-ligand 1 (PD-L1) inhibitor-demonstrated clinical benefit in the 2023 DUO-E trial when combined with carboplatin and paclitaxel. Immune thrombocytopenia (ITP) is an uncommon but potentially life-threatening immune-related adverse event (irAE). A 73-year-old woman with recurrent endometrial carcinoma developed severe ITP after three cycles of paclitaxel, carboplatin, and durvalumab. Fourteen days after cycle 3 she presented with pyelonephritis, bacteremia, and acute disseminated intravascular coagulation (DIC). Despite infection control, her platelet count declined to 1 × 10³/μL, with epistaxis, hematuria, and melena. Suspecting ITP as an irAE, intravenous immunoglobulin (IVIG 10 g/day × 5 days) and high-dose intravenous prednisolone (1 mg/kg/day) were administered. Platelet counts improved gradually to 85 × 10³/μL by hospital day 32, and she was discharged on a steroid taper. This appears to be the first Japanese report of durvalumab-associated ITP in endometrial carcinoma. Clinicians should maintain a high index of suspicion for ITP when unexpected thrombocytopenia or bleeding occurs during durvalumab therapy and initiate prompt treatment.

2,411

项与度伐利尤单抗相关的新闻（医药）

2026-02-27

·Business Wire

Signatera™ MRD Data at ASCO GU Highlights Potential Utility Across GU Cancers, Including for Bladder Preservation

AUSTIN, Texas--(BUSINESS WIRE)--Natera, Inc. (NASDAQ: NTRA), a global leader in cell-free DNA and precision medicine, today announced it will present new data in genitourinary malignancies at the American Society of Clinical Oncology Genitourinary Cancers Symposium (ASCO GU), taking place February 26-28, 2026. Across four oral presentations in muscle-invasive bladder cancer (MIBC), these data reinforce Signatera’s role in identifying patients who benefit from adjuvant immunotherapy, supporting response-adaptive bladder preservation strategies, and refining molecular residual disease (MRD) detection with plasma circulating tumor DNA (ctDNA) and urinary tumor DNA (utDNA). Bladder Preservation: INDIBLADE and RETAIN The INDIBLADE and RETAIN multicenter phase 2 trials demonstrate Signatera’s consistent performance in treatment response monitoring across diverse neoadjuvant regimens in MIBC, with 73-77% of patients demonstrating clearance of ctDNA following therapy and Signatera-negativity showing strong associations with positive outcomes, even with the bladder preserved. INDIBLADE, the findings of which will be published today in Nature Medicine, investigated induction with combination immune checkpoint inhibitors (ICI) followed by chemoradiotherapy as a bladder-sparing strategy in stage II/III MIBC patients. The results show that Signatera status post-ICI was associated with bladder-intact event-free survival (BI-EFS). Specifically, Signatera-negativity at baseline and post-neoadjuvant therapy was linked to an 88.6% and 91% estimated two-year BI-EFS, respectively. RETAIN evaluated a clinical response-adapted approach to identify patients for potential bladder-preservation following neoadjuvant therapy. The findings showed that post-treatment ctDNA clearance or negativity was associated with improved metastasis-free survival (MFS), and that Signatera-negative patients with no clinical or radiographic evidence of disease managed with active surveillance achieved MFS comparable to Signatera-negative patients undergoing cystectomy. In contrast, persistent Signatera-positivity was associated with poor outcomes. Perioperative Care: NIAGARA This phase 3 randomized perioperative study includes the first-ever presentation of utDNA data with clinical correlation. The combination of utDNA and ctDNA status post-neoadjuvant therapy and pre-cystectomy identified the group with the highest 24-month EFS. utDNA-positivity pre-cystectomy was more strongly associated with residual non-invasive disease vs ctDNA-positivity was more strongly associated with residual invasive disease. These data suggest that the combined assessment of utDNA and ctDNA can provide complementary risk stratification benchmarked against pathologic staging, enabling comprehensive identification of residual disease. “As treatment options expand in perioperative and bladder preservation settings, we need tools that help us determine who truly requires additional therapy and who may safely avoid it,” said Michiel van der Heijden, M.D., Ph.D., Netherlands Cancer Institute, principal investigator of INDIBLADE and presenting author of the NIAGARA study. “The data presented at ASCO GU demonstrate that MRD assessment with Signatera has strong correlations with outcomes and the potential to inform these critical treatment decisions.” “Following our milestone PMA submission to the FDA based on IMvigor011, these compelling data presentations reflect our commitment to transforming care across the spectrum of genitourinary malignancies,” said Minetta Liu, M.D., chief medical officer of oncology and early cancer detection at Natera. “The new data suggests a particularly important opportunity for Signatera to optimize clinical decisions around bladder preservation, a major opening to improve patient quality of life.” The full list of presentations at ASCO GU includes: February 27, 8:10 AM PT | Abstract #633 (Oral Presentation) Presenter: Joaquim Bellmunt, M.D. Circulating tumor (ct)DNA-guided adjuvant atezolizumab (atezo) in muscle-invasive bladder cancer (MIBC): Exploratory analysis of ctDNA dynamics in the IMvigor011 trial February 27, 8:10 AM PT | Abstract #632 (Oral Presentation) Presenter: Pooja Ghatalia, M.D. Circulating tumor DNA (ctDNA) to guide response-adapted bladder preservation in muscle invasive bladder cancer (MIBC): Integrated analysis of the RETAIN trials February 27, 11:30 AM PT | Abstract #797 Presenter: Can Aydogdu, M.D. Integrating genomic profiling and circulating tumor DNA monitoring to optimize surveillance strategies in muscle-invasive bladder cancer February 27, 11:30 AM PT | Abstract #831 Presenter: Can Aydogdu, M.D. Association of ctDNA status with upstaging, pathologic outcomes, and genomic alterations in high-risk NMIBC February 27, 2:30 PM PT | Abstract #637 (Oral Presentation) Presenter: Jan-Jaap J. Mellema, M.D. Induction ipilimumab plus nivolumab followed by consolidating chemoradiotherapy as bladder-sparing treatment in stage II/III urothelial carcinoma of the bladder: The phase 2 INDIBLADE trial February 27, 4:00 PM PT | Abstract #636 (Oral Presentation) Presenter: Michiel van der Heijden, M.D., Ph.D. Urinary tumor DNA (utDNA) and circulating tumor DNA (ctDNA) in patients (pts) with muscle-invasive bladder cancer (MIBC) who received perioperative durvalumab (D) in NIAGARA February 28, 7:00 AM PT | Abstract #532 Presenter: Shuchi Gulati, M.D., M.Sc. Association of pre-operative circulating tumor DNA (ctDNA) status with clinicopathologic characteristics in patients (pts) with localized renal cell carcinoma (RCC) February 28, 7:00 AM PT | Abstract #620 Presenter: Dalia Kaakour, M.D., MPH Use of circulating tumor DNA (ctDNA) in the detection of residual disease and recurrence for patients with testicular cancer February 27, 11:30 AM PT | Abstract #860 Presenter: Lingbin Meng, M.D., Ph.D. Use of circulating tumor DNA (ctDNA) in the detection of residual disease and recurrence for patients with testicular cancer February 27, 11:30 AM PT | Abstract #800 Presenter: Tanya Jindal, BS, BA Predictive value of early circulating tumor DNA (ctDNA) response in advanced urothelial carcinoma (aUC) treated with enfortumab vedotin plus pembrolizumab (EVP). February 28, 7:00 AM PT | Abstract #541 Presenter: David F. McDermott, M.D. Circulating tumor DNA (ctDNA) analysis in participants (pts) with advanced clear cell renal cell carcinoma (ccRCC) treated with first-line pembrolizumab (pembro) monotherapy from the phase 2 KEYNOTE-427 study. About Natera Natera™ is a global leader in cell-free DNA and precision medicine, dedicated to oncology, women’s health, and organ health. We aim to make personalized genetic testing and diagnostics part of the standard-of-care to protect health and inform earlier, more targeted interventions that help lead to longer, healthier lives. Natera’s tests are supported by more than 350 peer-reviewed publications that demonstrate excellent performance. Natera operates ISO 13485-certified and CAP-accredited laboratories certified under the Clinical Laboratory Improvement Amendments (CLIA) in Austin, Texas, and San Carlos, California, and through Foresight Diagnostics, its subsidiary, operates an ISO 27001-certified and CAP-accredited laboratory certified under CLIA in Boulder, Colorado. For more information, visit www.natera.com. Forward-Looking Statements All statements other than statements of historical facts contained in this press release are forward-looking statements and are not a representation that Natera’s plans, estimates, or expectations will be achieved. These forward-looking statements represent Natera’s expectations as of the date of this press release, and Natera disclaims any obligation to update the forward-looking statements. These forward-looking statements are subject to known and unknown risks and uncertainties that may cause actual results to differ materially, including with respect to our efforts to develop and commercialize new product offerings, whether the results of clinical or other studies will support the use of our product offerings, the impact of results of such studies, our expectations of the reliability, accuracy, and performance of our tests, or of the benefits of our tests and product offerings to patients, providers, and payers. Additional risks and uncertainties are discussed in greater detail in "Risk Factors" in Natera’s recent filings on Forms 10-K and 10-Q, and in other filings Natera makes with the SEC from time to time. These documents are available at www.natera.com/investors and www.sec.gov.

临床结果临床2期ASCO会议临床3期

2026-02-27

·FiercePharma

Padcev-Keytruda combo aces another bladder cancer trial as MIBC landscape becomes more complex

The Padcev-Keytruda combination looks poised to move into another earlier-stage bladder cancer setting, reporting a 35% reduction in the risk of death in the Keynote-B15 trial. The combination of Padcev and Keytruda has once again delivered strong results, this time significantly improving overall survival (OS) for patients with cisplatin-eligible muscle-invasive bladder cancer (MIBC). Yet questions remain about its impact on practice due to a changing treatment landscape.Results from the Keynote-B15 (EV-304) trial showed a major 47% reduction in patients’ risk of tumor recurrence, disease worsening or death for the Padcev-Keytruda combination compared with neoadjuvant cisplatin-based chemotherapy alone.Presented at the American Society of Clinical Oncology (ASCO) Genitourinary Cancers Symposium, the data also showed that using Padcev and Keytruda both before and after surgical removal of patients’ bladders lowered their risk of death by 35% compared with presurgical chemotherapy.The statistically significant OS number was gleaned during an interim analysis, when the majority of patients in both arms were still alive, study presenter Matthew Galsky, M.D., from the Mount Sinai Tisch Cancer Center, told reporters during a press briefing. As of a data cutoff on Oct. 27, 2025, 83% of patients in the perioperative combo arm, versus 75.4% of those in the control arm, were alive. “The Keynote-B15 study marks an exciting development in establishing a potential new treatment option and standard of care for these patients,” Kevin Kelly, an ASCO expert in genitourinary cancer from Thomas Jefferson University, said in a statement. Merck & Co. sponsored the study and offered Keytruda, while Pfizer and Astellas contributed Padcev, an antibody-drug conjugate. The trial win in cisplatin-eligible patients with MIBC follows a similarly positive readout from the Keynote-905 (EV-303) study, which showed the Padcev-Keytruda combo can improve survival in cisplatin-ineligible patients, leading to a groundbreaking FDA approval in November 2025.However, unlike the conclusiveness of the combo’s prowess in that previous trial, the latest triumph comes with some questions as the treatment landscape in bladder cancer has gotten more complicated—both in early-stage and metastatic settings—since the Keynote-B15 study started in 2021. By Galsky’s estimate, eligibility for cisplatin divides MIBC patients roughly 50-50. Among the uncertainties, clinicians are left wondering whether the trial’s neoadjuvant chemo-only control arm remains a relevant comparator. As Kelly noted, the study’s control arm lacked an adjuvant therapy. In August 2021, merely four months after Keynote-B15’s launch, the FDA approved Bristol Myers Squibb’s Opdivo for the adjuvant treatment of bladder cancer patients who are at high risk of recurrence after undergoing radical resection.More recently, the FDA last year blessed AstraZeneca’s Imfinzi as perioperative regimen in MIBC.Opdivo adjuvant therapy has not shown an OS benefit in bladder cancer, Galsky, who’s also the lead author of the CheckMate-274 trial that supported Opdivo’s adjuvant nod, noted during the press briefing. Last year, Galsky presented updated long-term follow-up data from the BMS trial. While OS data remained immature, adjuvant Opdivo was linked to a favorable trend toward a 27% death-risk reduction versus placebo in MIBC patients.Besides, Opdivo’s indication only covers a subset of patients at high risk of recurrence after surgery, he pointed out.As for Imfinzi, Galsky cautioned against making a cross-trial comparison, but he still pointed to some differences in the two regimens’ effect sizes. For example, on the secondary endpoint of rate of pathological complete response (pCR), which measures the absence of cancer in the resected tumor tissues, the Padcev-Keytruda cocktail reached 55.8%, versus 32.5% for the control arm in the current Keynote-B15 trial. In the Niagra trial, the Imfinzi regimen recorded a 33.8% pCR rate, versus 25.8% in the comparison group. The Niagra perioperative regimen was the first immunotherapy to deliver a survival win against cisplatin chemo for MIBC patients, showing a death-risk reduction of 25%. The regimen includes Imfinzi and cisplatin-based chemo before surgery followed by Imfinzi alone post-surgery. The Padcev-Keytruda combo foregoes any systemic chemo, leading to fewer hematological toxicities such as neutropenia, anemia and thrombocytopenia despite higher rates of skin reactions, diarrhea and hair loss, according to the Keynote-B15 results. To further complicate clinicians’ treatment decisions, Padcev-Keytruda has become the new standard of care in first-line metastatic bladder cancer, raising the possibility that some physicians might reserve the combo as an option for patients who eventually progress rather than using it upfront in early-stage MIBC.Despite this reluctance, it’s better to give patients the best treatment upfront, which improves long-term outcomes, Catherine Pietanza, M.D., vice president of global clinical development at Merck Research Laboratories, argued.Patients who receive Padcev-Keytruda as a perioperative treatment for MIBC would have to look for a different regimen if their cancer progresses to advanced disease, she acknowledged in an interview with Fierce Pharma. But that won’t be problem for all bladder cancer patients considering the PD-1/ADC combo, because only about 25% of bladder cancer patients are diagnosed at the MIBC stage, whereas the majority are first diagnosed with metastatic disease.“Having [Padcev-Keytruda] treatments in both the perioperative setting and the first-line setting allows patients to have both available to them, whether they are diagnosed in early-stage or in the metastatic setting,” Pietanza said.In another potential advantage over AZ’s Niagra regimen, as Pietanza noted, the twin triumphs of Keynote-905 and now Keynote-B15 mean that the combo, if approved in cisplatin-eligible patients, would simplify treatment for doctors as they wouldn’t have to think about whether a patient is eligible for cisplatin.There’s also the perennial question of whether all patients need treatment both before and after surgery. Galsky acknowledged that the field doesn’t have an answer to this because researchers have only recently started to think about treatment de-escalation. He raised circulating tumor DNA as a powerful tool that may be incorporated in future trials to identify patients for personalized treatment escalation.

临床结果上市批准ASCO会议

2026-02-27

·今日头条

“协同突破——肺癌全程诊疗研讨会”天津站圆满落幕

深入探讨肺癌从早期到晚期的全程管理策略，为临床实践的精准化指明方向。 2025年10月25日，“协同突破——肺癌全程诊疗研讨会”在天津成功召开。本次大会由天津市胸科医院彭海鹰教授与首都医科大学附属北京安贞医院游宾教授共同担任主席，并汇聚了十余位肺癌领域的顶尖专家。会议聚焦晚期非小细胞肺癌（NSCLC）一线治疗、耐药机制破解、辅助治疗时长优化、Ⅲ期不可切除患者治疗策略以及抗体偶联药物（ADC）最新突破等前沿议题，展开了深度交流与思维碰撞，为与会者搭建了一个高水平的前沿学术对话平台。 EGFR突变晚期NSCLC治疗策略优化：从一线联合到耐药应对首都医科大学附属北京友谊医院林芳教授以“一线联合治疗引领EGFR突变晚期NSCLC向更长生存迈进”为题，分享了EGFR突变晚期NSCLC的一线治疗进展。林芳教授指出，肿瘤细胞可通过不同的进化途径抵抗EGFR-TKI的疗效，而联合治疗可同时杀伤对药物敏感的肿瘤细胞和耐药肿瘤细胞，并阻断耐药细胞的形成。目前，针对EGFR突变NSCLC晚期的一线联合治疗正在广泛探索中。例如FLAURA2研究（奥希替尼联合含铂化疗）、AENEAS2研究（阿美替尼联合化疗）、MARIPOSA研究（兰泽替尼联合埃万妥单抗）等[1-3]。面对EGFR-TKI治疗后不可避免的耐药难题，天津医科大学总医院刘夏教授带来了“EGFR-TKI进展后MET扩增NSCLC治疗新方向”的精彩报告。MET扩增是贯穿1-3代TKI耐药的重要旁路机制，发生率超20%。针对此类耐药人群，精准检测是治疗的前提。目前临床推荐采用FISH作为MET扩增检测的金标准，同时，组织NGS也可作为有效补充。在治疗策略方面，Ⅲ期SACHI研究评估了双靶联合策略[4]。此外，MARIPOSA-2研究显示，埃万妥单抗联合化疗在EGFR-TKI耐药后的具有较好的疗效[5]；HARMONi-A研究则证实依沃西单抗联合化疗可为EGFR-TKI治疗进展患者带来生存获益[6]；此外，IMpower150和ORIENT-31研究也评估了免疫联合抗血管及化疗的四药模式在此类人群中的治疗潜力[7,8]。沧州市中心医院万善志教授分享的一例晚期EGFR L858R突变肺腺癌患者的治疗历程。该患者初诊时即伴有肺内多发转移、大量胸腔积液及广泛骨转移，肿瘤负荷高。在明确基因分型后，一线即采用奥希替尼联合培美曲塞+卡铂的FLAURA2方案。治疗2周期后复查，患者胸闷气短症状显著缓解，影像学评估达部分缓解（PR）。在完成4周期含铂化疗后，顺利进入维持治疗阶段，目前无进展生存期（PFS）已超过15个月，且未出现严重不良反应。在专题讨论环节中，与会专家聚焦两大临床关键问题，分享了各自的观点。针对一线EGFR-TKI联合化疗，锦州医科大学附属第三医院何东宁教授强调，需筛选优势人群（如L858R突变、脑转移、高肿瘤负荷）进行联合治疗。天津医科大学肿瘤医院鲁蒙教授指出，肿瘤异质性是推动联合治疗探索的根本原因。山西省晋城人民医院马文途教授分享了两例联合治疗案例，并提出了在维持治疗阶段如何平衡疗效与患者依从性的现实思考。万善志教授认为，对于年轻、耐受性好、治疗意愿强的患者，一线采用联合方案能带来快速且深度的缓解。对于MET扩增的预后意义与双靶治疗时机，彭海鹰教授指出，MET扩增是明确的不良预后因素。对于明确MET扩增者，应积极考虑双靶联合。何东宁教授从辩证角度分析认为，MET扩增从生物学行为上是预后差的标志，但从治疗角度看，它为患者提供了一个明确的、可干预的靶点。鲁蒙教授提出，在临床中应仔细审阅基因拷贝数的具体数值，对于检测阴性但临床高度怀疑的患者，可考虑再次组织活检。 Ⅲ期不可切除NSCLC诊疗精进：MDT引领下的个体化策略探索中国医科大学附属第一医院孙艳彬教授对“EGFR突变NSCLC靶向辅助治疗时长变迁及全程管理策略”进行了系统梳理。他从早期辅助治疗2年模式的探索与局限讲起，深入分析了为何需要更长的治疗时长。在EVIDENCE研究中[9]，经埃克替尼治疗2年，EGFR突变Ⅱ-ⅢA期患者的中位无病生存期（DFS）较化疗组显著延长（47.0个月vs 22.1个月，HR=0.36，95%CI 0.24-0.55，P<0.0001），但DFS获益未转化为总生存期（OS）获益（HR=0.91, 95% Cl 0.42-1.94）。而在ADAURA研究中[10]，经3年的辅助靶向治疗，ⅠB-ⅢA期患者的5年OS率可达到88%，死亡风险较安慰剂组降低51%（HR=0.49，95.03% Cl：0.33-0.73，P<0.001）。ARTS研究是一项随机、双盲、安慰剂对照的III期临床研究[11]，旨在评估阿美替尼对比安慰剂用于EGFR敏感突变II-IIIB期（T3N2M0）NSCLC完全切除术后辅助治疗的疗效和安全性。研究结果显示，阿美替尼组 vs 安慰剂组的中位DFS分别为未达到 vs 19.4个月（HR=0.17；P<0.0001）。阿美替尼组 vs 安慰剂组的研究者评估的2年DFS率分别为90.2% vs 44.4%，疾病进展或死亡风险降低83%。此外，随着治疗时间的延长，不良反应管理、患者依从性及生活质量维护成为影响疗效的关键因素。在术后随访方面，应结合影像学、肿瘤标志物及分子监测等手段，实施个体化、风险适应的随访策略，从而早期识别复发、优化长期结局。邯郸中心医院季艳霞教授围绕“Ⅲ期不可切除NSCLC治疗策略”这一主题，系统讨论了该疾病阶段的异质性及其对临床决策的影响。Ⅲ期NSCLC因其在疾病分期、淋巴结转移状态及可切除性界定上存在高度异质性，治疗策略的制定尤为复杂。对于Ⅲ期不可切除NSCLC，PACIFIC研究采用了同步放化疗后进行免疫巩固治疗。然而，PACIFIC研究亚组分析显示[12]，免疫巩固治疗在EGFR突变人群中的疗效有限。这一治疗瓶颈进一步推动了精准治疗的发展。LAURA研究证实[13]，在EGFR突变Ⅲ期不可切患者同步放化疗后，采用第三代EGFR-TKI进行靶向巩固治疗的中位PFS达到39.1个月，患者疾病进展或死亡风险降低84%（HR=0.16，P<0.001）。Ⅲ期POLESTAR研究进一步验证了“CRT后靶向维持”策略在EGFR突变Ⅲ期不可切除NSCLC中的可行性[14]。该研究评估了阿美替尼对比安慰剂作为根治性放化疗后维持治疗的疗效和安全性，结果显示，相较于安慰剂组，阿美替尼组显著延长了中位PFS（30.4个月 vs. 3.8个月，HR=0.2，P＜0.0001）。未来，深化多学科协作、依托生物标志物探索个体化治疗路径，将是进一步改善患者预后的关键方向。徐涛教授以“ADC在非小细胞肺癌治疗中的创新与突破”为题，系统回顾了肺癌治疗从化疗、靶向、免疫到ADC时代的发展历程，指出ADC凭借“精准靶向、高效杀伤及旁观者效应”等独特优势，已成为新的抗肿瘤手段。DESTINY-Lung02研究显示[15]，德曲妥珠单抗（T-DXd）治疗HER2突变NSCLC的确认ORR达到了51%，中位PFS和中位OS分别为10个月和19个月。此外，瑞康曲妥珠单抗在HORIZON-Lung研究中也显示出了优于传统二线治疗的疗效[16]，中位PFS达到了11.5个月。针对TROP2靶点的ADC在EGFR-TKI经治人群中均展现出较好的疗效，其中芦康沙妥珠单抗中位PFS达到了6.9个月[17],Teliso-V在c-MET高表达、EGFR野生型患者中ORR达34.6%[18]。在本场会议的多学科（MDT）讨论环节中，多位专家围绕Ⅲ期不可切除NSCLC的诊疗策略、ADC药物发展等关键议题展开了深入交流。游宾教授强调了MDT协作在Ⅲ期不可切除患者诊疗中的核心价值。刘夏教授认为，部分不可切除患者经MDT评估后仍可能从手术中获益。何东宁教授进一步指出，MDT对确保Ⅲ期NSCLC患者规范化诊疗至关重要。关于ADC药物发展前景，鲁蒙教授和马文途教授一致认为其在后线治疗中潜力较好，马文途教授进一步强调需通过生物标志物细化获益人群。总结大会进入尾声，彭海鹰教授进行了总结致辞。本次会议全面涵盖肺癌靶向治疗、耐药后探索、辅助治疗及MDT模式等关键议题。相信随着新药研发和理念更新，肺癌治疗将更加个体化精准化，为患者带来更长生存和更好生活质量。审批编号：CN-179040 有效期至：2026-03-27 声明：本材料由阿斯利康提供，仅供医疗卫生专业人士进行医学科学交流，不用于推广目的。参考文献： [1] Planchard D, et al. Osimertinib with or without Chemotherapy in EGFR-Mutated Advanced NSCLC. N Engl J Med. 2023;389(21):1935-1948. [2] Lu S, et al. Aumolertinib with or without chemotherapy as first line treatment in locally advanced or metastatic NSCLC with sensitizing EGFR mutations (AENEAS2). Cancer Res. 85;(8_Supplement_2):CT053. [3] Cho BC, et al. Amivantamab plus Lazertinib in Previously Untreated EGFR-Mutated Advanced NSCLC. N Engl J Med. 2024;391(13):1189-1200. [4] Lu S, et al. Savolitinib (Savo) combined with osimertinib (osi) versus chemotherapy (chemo) in EGFR-mutant (EGFRm) and MET-amplification (METamp) advanced NSCLC after disease progression (PD) on EGFR tyrosine kinase inhibitor (TKI): Results from a randomized phase 3 SACHI study. J Clin Oncol. 2025;43(17_suppl):LBA8505. [5] Passaro A, et al. Amivantamab plus chemotherapy with and without lazertinib in EGFR-mutated advanced NSCLC after disease progression on osimertinib: primary results from the phase III MARIPOSA-2 study. Ann Oncol. 2024;35(1):77-90. [6] Fang J, et al. Ivonescimab Plus Chemotherapy in Non-Small Cell Lung Cancer With EGFR Variant: A Randomized Clinical Trial. JAMA. 2024;331(22):1898-1909. [7] Socinski MA, et al. Atezolizumab for First-Line Treatment of Metastatic Nonsquamous NSCLC. N Engl J Med. 2018;378(24):2288-2301. [8] Lu S, et al. Sintilimab plus bevacizumab biosimilar IBI305 and chemotherapy for patients with EGFR-mutated non-squamous non-small-cell lung cancer who progressed on EGFR tyrosine-kinase inhibitor therapy (ORIENT-31): first interim results from a randomised, double-blind, multicentre, phase 3 trial. Lancet Oncol. 2022;23(9):1167-1179. [9] He J, et al. Icotinib versus chemotherapy as adjuvant treatment for stage II-IIIA EGFR-mutant non-small-cell lung cancer (EVIDENCE): a randomised, open-label, phase 3 trial. Lancet Respir Med. 2021;9(9):1021-1029. [10] Tsuboi M, et al. Overall Survival with Osimertinib in Resected EGFR-Mutated NSCLC. N Engl J Med. 2023;389(2):137-147. [11] Zhang L, et al. Aumolertinib as adjuvant therapy in resected EGFR-mutated non-small-cell lung cancer (ARTS): a double-blind, multicentre, randomised, controlled, phase 3 trial. Lancet Oncol. 2026;27(2):159-168. [12] Antonia SJ, et al. Durvalumab after Chemoradiotherapy in Stage III Non-Small-Cell Lung Cancer. N Engl J Med. 2017;377(20):1919-1929. [13] Lu S, et al. Osimertinib after Chemoradiotherapy in Stage III EGFR-Mutated NSCLC. N Engl J Med. 2024;391(7):585-597. [14] Meng X, et al. Aumolertinib Maintenance after Chemoradiotherapy in Stage III Non-Small-Cell Lung Cancer: Interim Results of the Phase III Study (POLESTAR). J Thorac Oncol. 2024;19(10):S6-S7. [15] Goto K, et al. Trastuzumab Deruxtecan in Patients With HER2-Mutant Metastatic Non-Small-Cell Lung Cancer: Primary Results From the Randomized, Phase II DESTINY-Lung02 Trial. J Clin Oncol. 2023;41(31):4852-4863. [16] Lu S, et al. HORIZON-Lung: A Phase II Study of Trastuzumab Rezetecan (SHR-A1811) in Patients with HER2-Mutated Advanced Non-Small Cell Lung Cancer. Presented at: American Association for Cancer Research (AACR) Annual Meeting; April 25-30, 2025. [17] Fang W, et al. Sacituzumab tirumotecan versus docetaxel for previously treated EGFR-mutated advanced non-small cell lung cancer: multicentre, open label, randomised controlled trial. BMJ. 2025;389:e085680. Published 2025 Jun 5. [18] Camidge DR, Bar J, Horinouchi H, et al. Telisotuzumab Vedotin Monotherapy in Patients With Previously Treated c-Met Protein-Overexpressing Advanced Nonsquamous EGFR-Wildtype Non-Small Cell Lung Cancer in the Phase II LUMINOSITY Trial. J Clin Oncol. 2024;42(25):3000-3011. *“医学界”力求所发表内容专业、可靠，但不对内容的准确性做出承诺；请相关各方在采用或以此作为决策依据时另行核查。

100 项与度伐利尤单抗相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D10808	度伐利尤单抗	L01XC28	DB11714

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
早期胃癌	美国	AstraZeneca PLC	2025-11-25
胃食管交界处癌	美国	AstraZeneca PLC	2025-11-25
局部晚期胃癌	美国	AstraZeneca PLC	2025-11-25
不可切除的非小细胞肺癌	中国	AstraZeneca UK Ltd.	2025-11-18
肌层浸润性膀胱癌	美国	AstraZeneca UK Ltd.	2025-03-28
子宫癌	日本	阿斯利康制药有限公司	2024-11-22
晚期子宫内膜癌	欧盟	AstraZeneca AB	2024-08-15
晚期子宫内膜癌	冰岛	AstraZeneca AB	2024-08-15
晚期子宫内膜癌	列支敦士登	AstraZeneca AB	2024-08-15
晚期子宫内膜癌	挪威	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	欧盟	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	冰岛	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	列支敦士登	AstraZeneca AB	2024-08-15
复发性子宫内膜癌	挪威	AstraZeneca AB	2024-08-15
可切除非小细胞肺癌	英国	AstraZeneca PLC	2024-07-09
晚期胆道癌	美国	AstraZeneca UK Ltd.	2024-06-14
错配修复缺陷子宫内膜癌	美国	AstraZeneca UK Ltd.	2024-06-14
非小细胞肺癌 III期	美国	AstraZeneca UK Ltd.	2024-06-14
晚期肝细胞癌	欧盟	AstraZeneca AB	2023-04-14
晚期肝细胞癌	冰岛	AstraZeneca AB	2023-04-14

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
胃食管交界处腺癌	申请上市	澳大利亚	AstraZeneca Pty Ltd.	2025-06-11
胃癌	申请上市	澳大利亚	AstraZeneca Pty Ltd.	2025-06-11
ALK阳性非小细胞肺癌	申请上市	中国	AstraZeneca AB	2025-02-21
EGFR突变的非小细胞肺癌	申请上市	中国	AstraZeneca UK Ltd.	2025-02-21
卵巢上皮癌	申请上市	中国	AstraZeneca UK Ltd.	2024-08-16
PD-L1阳性三阴性乳腺癌	临床3期	美国	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	中国	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	日本	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	阿根廷	AstraZeneca PLC	2023-11-23
PD-L1阳性三阴性乳腺癌	临床3期	澳大利亚	AstraZeneca PLC	2023-11-23

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临床结果

适应症

分期

评价

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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


NCT04945720 (DurHope, CTgov)	临床2期	晚期肝细胞癌 \| 门静脉血栓形成	30	FOLFOX+leucovorin+Durvalumab+oxaliplatin+fluorouracil	鹽製築壓艱鏇窪鏇網鏇 = 簾範構獵築構獵遞遞觸積築簾繭製壓衊範窪鬱 (鏇獵選衊簾鹽憲積淵淵, 簾簾夢糧遞遞鑰觸襯廠 ~ 餘壓構廠鑰襯齋願製餘) 更多	-	2026-02-25
NCT03874325 (Pubmed \| Breast Cancer Res Treat)	临床2期	HR阳性乳腺癌新辅助 HR+ \| HER2-	17	Durvalumab + Aromatase Inhibitors (HR+/HER2-negative breast cancer + Postmenopausal)	夢憲衊衊壓積遞鑰製網(廠獵廠遞簾鑰鹽範選衊) = Treatment was well tolerated, with most adverse events being grade 1-2. 艱獵蓋觸衊齋艱選齋鑰 (衊齋製遞觸遞糧糧鏇齋 )	不佳	2026-02-01
IMbrave150 (ASCO_GI2026)	临床2/3期	晚期肝细胞癌一线	1,064	Tremelimumab + Durvalumab	壓顧製積顧艱鹹簾壓廠(糧淵繭製積獵廠構糧構) = 願鬱鹽憲壓壓艱衊窪獵築範築襯網廠積壓築餘 (遞觸觸鬱糧範膚餘網蓋 ) 更多	积极	2026-01-08
				Atezolizumab + Bevacizumab	壓顧製積顧艱鹹簾壓廠(糧淵繭製積獵廠構糧構) = 衊網壓鹹願顧簾淵餘鏇築範築襯網廠積壓築餘 (遞觸觸鬱糧範膚餘網蓋 ) 更多
NCT02962063 (ASCO_GI2026)	临床2期	食管腺癌	20	Durvalumab + Tremelimumab + PET-directed chemoradiation	網獵襯蓋壓鹹襯願網積(醖鬱築鏇選醖觸網膚選) = 築鑰憲觸築憲醖獵艱壓淵繭鑰遞鑰範廠膚壓顧 (鏇鹹醖觸築範網廠簾衊 ) 更多	积极	2026-01-08
				Durvalumab + Tremelimumab + PET-directed chemoradiation (resected Pts)	網獵襯蓋壓鹹襯願網積(醖鬱築鏇選醖觸網膚選) = 範網淵鏇構艱蓋觸夢範淵繭鑰遞鑰範廠膚壓顧 (鏇鹹醖觸築範網廠簾衊 )
TOPAZ-1 (ASCO_GI2026)	临床3期	晚期胆管癌一线	874	Gemcitabine + cisplatin + durvalumab	壓膚願願憲淵鏇遞遞鑰(齋糧選憲壓廠鹽艱積艱) = 鑰製醖繭觸獵糧糧鑰鹹窪窪繭廠觸醖築構鑰齋 (淵醖艱齋製糧糧遞夢艱 ) 更多	相似	2026-01-08
				Gemcitabine + cisplatin + pembrolizumab	壓膚願願憲淵鏇遞遞鑰(齋糧選憲壓廠鹽艱積艱) = 積獵齋齋廠鹹齋壓網艱窪窪繭廠觸醖築構鑰齋 (淵醖艱齋製糧糧遞夢艱 ) 更多
TPAZ-1 (ASCO_GI2026)	临床3期	晚期胆管癌一线	3,373	Gemcitabine plus cisplatin plus durvalumab	構齋夢餘鑰製蓋淵觸膚(鏇齋選窪積構積齋鑰鏇): HR = 0.6 (95.0% CI, 0.55 ~ 0.66), P-Value = < 0.001 更多	积极	2026-01-08
				Gemcitabine plus cisplatin plus pembrolizumab
ASCO_GI2026	N/A	晚期肝细胞癌一线	3,306	Bevacizumab-atezolizumab	淵積衊積網鏇範壓鹹餘(膚憲廠範糧構壓膚製鹹): HR = 0.873 (95.0% CI, 0.75 ~ 0.935), P-Value = 0.0016	积极	2026-01-08
				Lenvatinib
NCT05733598 (RP2-003, ASCO_GI2026)	临床2期	晚期胆道癌 \| 晚期肝细胞癌二线 \| 一线	60	RP2 + Atezolizumab + Bevacizumab	蓋製構衊獵鹽鏇壓製襯(夢夢艱選範襯積衊繭顧) = 襯齋網夢願築鹹鑰製顧選壓淵願襯製鑰壓衊襯 (夢範蓋糧蓋網觸衊糧選 )	积极	2026-01-08
				RP2 + Durvalumab	蓋製構衊獵鹽鏇壓製襯(夢齋衊製觸廠淵蓋構襯) = 糧遞窪衊選糧醖壓積範鹹獵積鹽夢網鬱繭遞艱 (艱範衊齋鏇艱繭構憲糧 )
ASCO_GI2026	N/A	胆道癌一线	148	gemcitabine + cisplatin + immune checkpoint inhibitor	憲網構醖鏇齋鏇積廠齋(鑰艱願願夢艱夢鬱憲夢) = 淵廠鏇鏇糧鏇鑰鹹醖鏇鹹願選願範簾選構願範 (積鏇淵鑰構糧鏇憲顧鹹, 10.6 ~ 16.4) 更多	积极	2026-01-08
				gemcitabine + cisplatin + S-1	憲網構醖鏇齋鏇積廠齋(鑰艱願願夢艱夢鬱憲夢) = 構遞選齋範鏇膚醖鬱齋鹹願選願範簾選構願範 (積鏇淵鑰構糧鏇憲顧鹹, 8.5 ~ 13.5) 更多
NCT04592913 (MATTERHORN, ASCO_GI2026)	临床3期	胃食管交界处腺癌辅助 \| 新辅助	948	durvalumab + FLOT	簾獵鑰製淵繭蓋糧艱艱(膚鬱遞窪選淵積觸壓襯) = 齋選繭範壓選餘廠醖衊網廠網網顧簾壓醖衊遞 (膚憲憲壓窪膚簾艱淵鏇 ) 更多	积极	2026-01-08
				placebo + FLOT	簾獵鑰製淵繭蓋糧艱艱(膚鬱遞窪選淵積觸壓襯) = 鑰願鬱鏇艱夢齋構顧觸網廠網網顧簾壓醖衊遞 (膚憲憲壓窪膚簾艱淵鏇 ) 更多