This early phase I trial tests the safety and how well N-803 works in treating patients with synovial sarcoma (SS) or myxoid/round cell liposarcoma (MRCL) that is growing, spreading, or getting worse (progressive) after being treated with adoptive cellular therapy (ACT) using T-cell receptor therapy (T-CRT). Synovial sarcoma is a rare, slow-growing cancer that affects the soft tissues, like muscles or ligaments near the joints. Myxoid/round cell liposarcoma is a rare type of soft tissue sarcoma cancer that originates from fat cells usually in the arms and legs. N-803 is a type of immunotherapy-a treatment that helps patients' own immune system fight cancer, and it is made up of a natural protein called interleukin-15 (IL-15) that is important for growing and activating immune cells. Studies have shown that patients can progress after initially responding to TCR-T, so this trial will use N-803 to stimulate rare persisting cells (cells that survive treatment and cause treatment failure and disease relapse) to make them work better at attacking the cancer. Adoptive cell therapy is a type of therapy that uses a patient's own immune cells to fight cancer. T-cell receptor therapy is a type of ACT that can recognize better recognize and bind to protein in cancer cells. Giving N-803 may be safe and tolerable in patients with SS or MRCL.

开始日期2026-09-02

申办/合作机构

Northwestern University

[+1]

NCT07355205

/ Not yet recruiting临床2期IIT

A Phase II, Single-Center, Open-Label Study of First-Line Ipilimumab Plus Nivolumab and Nogapendekin Alfa Inbakicept (N-803) in Patients With Stage IV or Recurrent Non-Small Cell Lung Cancer (FLINN)

This is an open-label, single center, one cohort, non-randomized, phase II study. The aim of the study is to evaluate the efficacy and safety of the combination of nivolumab and ipilimumab with nogapendekin alfa inbakicept in patients with stage IV or recurrent non-small cell lung cancer (NSCLC). It is hypothesized that the study treatment will be safe and well tolerated and will improve progression-free survival when compared to a historical study which treated advanced NSCLC patients with nivolumab plus ipilimumab. Patients will be treated in cycles lasting 6 weeks with two to three different chemotherapy drugs to up to 24 months.

开始日期2026-03-31

申办/合作机构

Washington University School of Medicine

[+2]

NCT07217496

/ Not yet recruiting临床1期IIT

Phase Ib Trial Combining N-803 and Pembrolizumab With Shorter Duration of Enfortumab Vedotin in Treatment-Naïve Patients With Metastatic Urothelial Carcinoma

This phase Ib trial will investigate the effect of N-803 in combination with pembrolizumab and enfortumab vedotin in treating participants with urothelial cancer that has spread to nearby tissue or lymph nodes (locally advanced) or that has spread from where it first started (primary site) to other places in the body (metastatic).

开始日期2026-02-15

申办/合作机构

The University of California, San Francisco

[+1]

100 项与诺格白介素α-因奇西普相关的临床结果

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100 项与诺格白介素α-因奇西普相关的专利（医药）

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332

项与诺格白介素α-因奇西普相关的文献（医药）

2026-05-01·Biomaterials advances

A novel ROS switcher potentiates the type-I photodynamic effect of sodium zinc chlorophyllin against Pseudomonas aeruginosa in diabetic wounds

Article

作者: Yuan, Cai ; Wang, Guodong ; Chen, Hongjie ; Huang, Mingdong ; Wu, Lusheng

Skin wound infections present a serious threat to human health, with bacterial infections in diabetic wounds being particularly challenging due to impaired healing. Gram-negative bacteria are common pathogens in diabetic wound infections and often exhibit high resistance to conventional treatments, necessitating prolonged and costly therapies. Photodynamic antibacterial therapy (PACT) is regarded as a non-invasive and effective approach, with minimal risk of inducing resistance. Sodium zinc chlorophyllin (ZnChl), a water-soluble metalloporphyrin photosensitizer, offers multiple advantages such as low cost, high safety, and the ability to promote wound healing. However, its bactericidal efficacy against Gram-negative bacteria is limited under the hypoxic conditions typically found in diabetic wounds. Herein, we report a strategy to develop an efficient chlorophyll-based photosensitizer operating via an oxygen-independent Type I mechanism by combining ZnChl with inorganic salts (NaI, KBr, or KI). This approach significantly improved antibacterial performance, particularly with NaI or KI. Upon 630 nm light irradiation, low concentrations of KI (5 mM) markedly enhanced the bactericidal effect of ZnChl (50 μM), reducing the survival of three Gram-negative bacterial strains by 3 logs (99.9%). Interestingly, we further discovered that KI acts as a "reactive oxygen species (ROS) converter," shifting the photodynamic mechanism of ZnChl from a mixed Type I/Type II mode to a dominant Type I mechanism, generating highly reactive hydroxyl radicals (OH). Moreover, the ZnChl-KI combination demonstrated significant therapeutic efficacy in treating Pseudomonas aeruginosa-infected diabetic wounds without inducing apparent toxicity in rats. This work provides a foundation for developing efficient and economical Type I photosensitizers for the treatment of bacterial infections in diabetic wounds.

2026-02-01·JOURNAL OF UROLOGY

Letter: Prolonged Progression-Free Survival, Disease-Free Survival, and Cystectomy Avoidance With IL-15 Receptor Lymphocyte–Stimulating Agent NAI Plus Bacillus Calmette-Guérin in Bacillus Calmette-Guérin–Unresponsive Papillary-Only Nonmuscle-Invasive Bladder Cancer

Letter

作者: Yu, Zekai ; Huang, Shiye ; Zhuang, Ziye ; Feng, Yubin ; Zhou, Shuqing

2026-01-01·JOURNAL OF UROLOGY

Prolonged Progression-Free Survival, Disease-Free Survival, and Cystectomy Avoidance With IL-15 Receptor Lymphocyte–Stimulating Agent NAI Plus Bacillus Calmette-Guérin in Bacillus Calmette-Guérin–Unresponsive Papillary-Only Nonmuscle-Invasive Bladder Cancer

Article

作者: Huang, Megan ; Kaminetsky, Jed ; Trabulsi, Edouard J. ; Chamie, Karim ; Bjurlin, Marc ; Sender, Lennie ; Jalkut, Mark W. ; Gonzalgo, Mark L. ; Cowan, Barrett E. ; Guru, Khurshid ; Spilman, Patricia ; Sexton, Wade J. ; Corcoran, Anthony ; Trainer, Andrew F. ; Cher, Michael L. ; Koo, Alec S. ; Shah, Mihir S. ; Chang, Sam S. ; Bassett, Jeffrey C. ; Kramolowsky, Eugene ; Drusbosky, Leylah M. ; Reddy, Sandeep ; Goldfischer, Evan ; Brown, Bruce ; Agarwal, Piyush Kumar ; Kaffenberger, Samuel D. ; Bhar, Paul ; Soon-Shiong, Patrick ; Tikhonenkov, Sergei N. ; Clark, William ; David, Richard

PURPOSE:

In QUILT-3.032, the efficacy of interleukin-15 receptor agonist, nogapendekin alfa inbakicept (NAI), in combination with bacillus Calmette-Guérin (BCG) for BCG-unresponsive high-grade papillary-only nonmuscle-invasive bladder cancer was assessed. In this study, we report the 36-month follow-up among participants with BCG-unresponsive papillary disease (cohort B).

MATERIALS AND METHODS:

NCT03022825 is an open-label, multicenter study of patients with BCG-unresponsive high-grade Ta/T1 papillary nonmuscle-invasive bladder cancer who received 400 μg NAI plus 50 mg BCG intravesically weekly for 6 consecutive weeks. The primary end point is disease-free survival (DFS) at 12 months. Progression-free survival (PFS), disease-specific survival (DSS), and cystectomy avoidance were assessed. Treatment-related adverse events were assessed.

RESULTS:

At July 15, 2024, data cutoff, the DFS rates at 12, 24, and 36 months were 58.2% (95% CI: 46.6, 68.2), 52.1% (95% CI: 40.3, 62.7), and 38.2% (95% CI: 25.6, 50.6), respectively. The PFS rates at 12 and 36 months were 94.9% (95% CI: 86.9, 98.0) and 83.1% (95% CI: 69.5, 91.0). The DSS rates at 12 and 36 months were 98.7% (95% CI: 91.4, 99.8) and 96.0% (95% CI: 88.2, 98.7). The median DSS has not been reached. Cystectomy avoidance rates at 12 and 36 months were 92.2% (95% CI: 83.4, 96.4) and 81.8% (95% CI: 68.1, 90.1), with median time to cystectomy not reached. Most treatment-related adverse events were grade 1 to 2 (61%) with 3% grade 3 and no grade 4 to 5.

CONCLUSIONS:

The 12-month and 36-month DFS, PFS, DSS, and cystectomy avoidance rates demonstrate the effectiveness and safety of NAI plus BCG in the management of BCG-unresponsive papillary disease.

TRIAL REGISTRATION:

ClinicalTrials.gov Identifier: NCT03022825.

307

项与诺格白介素α-因奇西普相关的新闻（医药）

16 小时之前

·国际干细胞与免疫细胞研究

CAR-NK联合疗法撕掉脑瘤难治标签，82.6%患者实现长期持续生存

点击蓝字关注我们胶质母细胞瘤预后较差，患者五年生存率不足10%。历经数十年药物研发，其临床疗效仍未取得显著突破。其核心治疗难题在于：药物研发与药物在人脑内的作用机制研究存在脱节；同时，标准治疗所致淋巴细胞减少、低绝对淋巴细胞计数（ALC）对总生存期的不良影响，长期被学界忽略。 2026年1月23日，ImmunityBio发布QUILT 3.078研究（NCT06061809）Ⅱ期临床最新数据，该研究创新性的采用无化疗免疫治疗方案（即CAR-NK疗法+ANKTIVA®联合治疗），直击胶质母细胞瘤既往治疗的核心痛点，填补了免疫相关治疗探索的空白，为这一难治性恶性肿瘤的临床研究与治疗实践开辟了全新路径。随着研究的持续深入与后续大规模临床试验的开展，胶质母细胞瘤的治疗格局有望被彻底改写，更多患者将迎来切实的生存获益！ ▲截图源自“immunitybio” 胶质母细胞瘤临床现状与免疫治疗核心痛点胶质母细胞瘤（GBM）是成人最常见的侵袭性原发性恶性脑肿瘤。即便接受手术、放疗联合替莫唑胺化疗的标准综合治疗，患者预后仍极差：初诊中位总生存期 14～16 个月，复发后中位生存期仅 6～9 个月，五年生存率＜10%，现有治疗方案局限性显著。治疗相关免疫抑制，尤其是淋巴细胞减少，是长期被学界忽视的关键问题。多项研究证实，基线或标准治疗后绝对淋巴细胞计数（ALC）降低，与患者生存期缩短独立相关，且与肿瘤负荷、切除程度无关。放疗、烷化剂化疗可引发循环淋巴细胞持续性减少，损伤抗肿瘤免疫监视功能，限制后续治疗疗效。临床分析进一步表明，放化疗后持续性淋巴细胞减少与总生存期缩短相关，淋巴细胞数量的维持或恢复则提示预后更佳。学界逐步确认，免疫功能是胶质母细胞瘤患者生存的关键生物学决定因素，修复淋巴细胞数量的疗法对长期病情控制至关重要。同时，胶质母细胞瘤被重新定义为兼具局部侵袭性与全身免疫衰竭的疾病，为免疫重建联合肿瘤靶向的治疗策略提供了理论支撑。 CAR-NK联合疗法暴击胶质母细胞瘤，82.6%患者实现持续生存获益 QUILT-3.078为II期临床试验，旨在评估ANKTIVA®联合PD-L1t-haNK、贝伐珠单抗及肿瘤电场疗法，治疗复发性胶质母细胞瘤的疗效。研究同步开展随机化IIB期扩展试验，以验证疗效持久性。IIB期试验按1:1随机分组，两组分别接受ANKTIVA+贝伐珠单抗+肿瘤电场疗法、以及在此基础上联合PD-L1t-haNK的方案，研究药物每两周给药一次。IIB期扩展队列目标入组20例，目前已入组8例，后续将进一步评估总生存期、疗效持久性及免疫生物标志物。此外，18例复发性GBM患者通过单例患者IND（spIND）接受该方案治疗，其中7例为一线治疗。研究共纳入23例经手术、放疗、替莫唑胺化疗标准治疗后进展的复发/进展性GBM患者。结果显示：23例患者中19例存活（82.6%），14例患者具备可评估临床数据，构成疗效分析队列，累计接受139剂联合免疫治疗，患者中位总生存期尚未达到（详见下图）。 ▲图源“immunitybio”，版权归原作者所有，如无意中侵犯了知识产权，请联系我们删除下图展示了两例代表性患者，在接受CAR-NK联合治疗前后的影像学对比，可见肿瘤显著缩小。 ▲图源“immunitybio”，版权归原作者所有，如无意中侵犯了知识产权，请联系我们删除小编寄语近年来，脑瘤的治疗已经取得了长足的进展，逆转了晚期患者的生存期，除了上面整理的内容，还有更多的新药/新技术正在研发中。如果您对现有治疗方案不满意，或想了解脑瘤更多抗癌新药/新技术的更多讯息，可扫文末二维码，将治疗经历、近期病理检查报告、出院小结等，提交至国际干细胞与免疫细胞研究医学部，进行初步评估。参考资料 [1]https://immunitybio.com/immunitybio-reports-median-overall-survival-not-yet-reached-and-lymphopenia-reversed-in-recurrent-glioblastoma-patients-receiving-anktiva-plus-car-nk-chemo-free-therapy/ 本文为“国际干细胞与免疫细胞研究”原创，转载需授权干细胞与免疫细胞研究入群免费领取抗癌细胞资讯｜新技术｜新药研发｜权威专家资料求分享求收藏求点击求在看

2026-01-28

·PRNewswire

Late-Stage Breakthroughs: How 2026's Top Clinical Platforms Are Redefining Cancer Treatment

Issued on behalf of Oncolytics Biotech Inc. VANCOUVER, BC., Jan. 28, 2026 /PRNewswire/ -- USANewsGroup.com News Commentary – As the global oncology clinical trials market surges toward a projected $25.61 billion valuation by 2035[1], a structural rotation is favoring 'registration-ready' platforms that demonstrate exceptional efficacy and pivotal-trial alignment with 2026's evolving FDA regulatory frameworks[2]. Investors are increasingly prioritizing late-stage and newly commercial companies poised for rapid maturation as sector fundamentals strengthen. This structural shift creates a window for Oncolytics Biotech Inc. (NASDAQ: ONCY), BioNTech (NASDAQ: BNTX), MAIA Biotechnology (NYSE-A: MAIA), Acrivon Therapeutics (NASDAQ: ACRV), and ImmunityBio (NASDAQ: IBRX). With 2026 set to be a banner year for M&A as buyers facing patent cliffs compete for a limited pool of late-stage assets[3], companies demonstrating disciplined pivotal execution and FDA alignment command asymmetric upside in an environment where executive infrastructure determines valuation floors. Oncolytics Biotech Inc. (NASDAQ: ONCY) is strengthening its operational and clinical leadership as it advances pelareorep toward multiple registration-directed programs in gastrointestinal cancers. The company recently announced the appointments of John McAdory as Executive Vice President of Strategy and Operations and Yujun Wu as Vice President, Head of Biostatistics, bringing deep expertise in late-stage oncology trial execution and regulatory strategy. McAdory joins from CG Oncology, where he served as Vice President of Clinical Operations leading late-stage development programs for oncolytic virus therapies. Wu arrives from Morphic Therapeutic, where he headed Biostatistics through the company's acquisition by Eli Lilly, and previously led statistical strategy for multiple Phase 3 oncology programs at Takeda. Both executives bring direct experience navigating complex registration trials and global regulatory interactions. "John's background running complex, late-stage oncology trials makes him exceptionally well-suited to lead Oncolytics' next phase of execution," said Jared Kelly, CEO of Oncolytics Biotech. "As we progress toward pivotal and registration-enabling studies in anal, pancreatic, and colorectal cancers, his experience will be critical to ensuring disciplined execution, speed, and regulatory alignment." These appointments complete a transformative executive team buildout following Kelly's promotion to CEO last year and the addition of Chief Business Officer Andrew Aromando. They were both crucial contributors to Ambrx Biopharma's $2 billion acquisition by Johnson & Johnson. Oncolytics also recently expanded its Scientific Advisory Board with globally recognized experts from Memorial Sloan Kettering Cancer Center and MD Anderson Cancer Center, positioning the company for accelerated clinical development across multiple indications. The company recently announced breakthrough efficacy data showing pelareorep achieved a 33% objective response rate in second-line KRAS-mutant microsatellite stable metastatic colorectal cancer patients when combined with standard chemotherapy. This triples the historical 6-11% response rate for chemotherapy alone in this difficult-to-treat patient population. The company is also advancing pelareorep toward potential accelerated approval in anal cancer after reporting third-line data that achieved a 29% objective response rate, nearly tripling historical benchmarks in a setting with no FDA-approved treatment options. The median duration of response reached approximately 17 months. Second-line or later results were equally compelling, with pelareorep achieving a 30% response rate, more than doubling the 13.8% benchmark for the only FDA-approved immunotherapy in this setting. The median duration of response of 15.5 months compared to 9.5 months for standard care demonstrates pelareorep's ability to deliver durable clinical benefit in patients with limited treatment options. Oncolytics has also secured FDA alignment on its Phase 3 study design for pelareorep in first-line metastatic pancreatic cancer, positioning it to launch the only immunotherapy registration trial currently planned for this disease. This regulatory milestone clears the path for initiating a pivotal study in one of oncology's most challenging therapeutic areas. CONTINUED… Read this and more news for Oncolytics Biotech at: In other recent industry developments and happenings in the market include: BioNTech (NASDAQ: BNTX) received FDA Fast Track designation for BNT113, an investigational mRNA cancer immunotherapy, for the treatment of patients with human papillomavirus type 16 positive head and neck squamous cell carcinoma (HNSCC) expressing PD-L1. The designation was granted based on preliminary safety and efficacy data from the ongoing pivotal Phase 2/3 AHEAD-MERIT clinical trial evaluating BNT113 in combination with pembrolizumab versus pembrolizumab monotherapy as first-line treatment in patients with unresectable recurrent or metastatic HPV16+ HNSCC expressing PD-L1, a cancer type with limited treatment options where patients experience median overall survival of 20.7 months under current standard of care. Head and neck squamous cell carcinoma is the seventh most common cancer type worldwide with increasing global incidence, with about one third of cases being HPV-positive and approximately 90% of oropharyngeal cancers driven by HPV16. BNT113 is designed to induce HPV16-specific anti-tumor immune responses by encoding the E6 and E7 proteins of HPV16 that are frequently found in HPV16+ solid tumors, with the FDA Fast Track designation enabling more frequent engagement with the FDA to support development and expedite regulatory review of this novel HPV-targeted chemotherapy-free treatment option. MAIA Biotechnology (NYSE-A: MAIA) advanced ateganosine into pivotal development with high probability of technical success based on exceptional efficacy data in third-line non-small cell lung cancer. The telomere-targeting agent secured FDA Fast Track designation and represents the first and only direct telomere-targeting anticancer therapy in clinical development, targeting an estimated $50+ billion global immunotherapy market. " MAIA's strong clinical execution in 2025 delivered exceptional efficacy data for ateganosine sequenced with a checkpoint inhibitor, including disease control, response rates, and survival data well above standard of care benchmarks," said Vlad Vitoc, M.D., founder and CEO of MAIA. "The results clearly differentiate our novel telomere-targeting science and support the U.S. FDA's Fast Track designation granted in 2025, positioning ateganosine for potential eligibility under the Accelerated Approval and Priority Review regulatory pathways." The company advanced concurrent Phase 3 and Phase 2 expansion trials targeting potential early commercial approval within 18 to 24 months. MAIA Biotechnology received a $2.3 million NIH grant supporting U.S. patient enrollment and is advancing second-generation molecules into Phase 1 development with enhanced expected efficacy. Acrivon Therapeutics (NASDAQ: ACRV) announced positive data from its ACR-368 Phase 2b registrational-intent trial showing 39% overall response rate in endometrial cancer with 52% confirmed response rate in serous subtype patients with up to two prior lines of therapy. The company submitted EU Clinical Trial Application for Arm 3 enrollment across more than 20 European sites in four major countries, with enrollment completion expected in Q4 2026. "We are pleased with tangible progress accelerating across multiple high-value opportunities," said Peter Blume-Jensen, M.D., Ph.D., CEO of Acrivon. "We are particularly excited by the observation from our ongoing ACR-368 Phase 2 trial that subjects with serous endometrial cancer with up to two prior lines of therapy are showing over 50% confirmed response rate. This provides an attractive opportunity for rapid Arm 3 enrollment without the need for a pretreatment biopsy, both in the US and more than 20 newly selected sites in major EU countries." Acrivon Therapeutics has submitted a Phase 3 confirmatory protocol to the FDA for ACR-368 combined with anti-PD-1 therapy in frontline endometrial cancer based on strong preclinical synergy data. The company also reported initial ACR-2316 Phase 1 data showing tumor shrinkage in endometrial cancer, SCLC and squamous NSCLC, with ACR-6840 nominated as its next CDK11 inhibitor development candidate. ImmunityBio (NASDAQ: IBRX) announced that it recently held a Type B End-of-Phase meeting with the U.S. FDA regarding the Company's supplemental Biologics License Application for ANKTIVA plus Bacillus Calmette-Guérin in BCG-unresponsive non-muscle invasive bladder cancer (NMIBC) with papillary tumors. The Company presented more than five years of follow-up data demonstrating durable disease-specific survival of approximately 96% at 36 months with median survival not yet reached even with five years of follow-up, high rates of cystectomy avoidance of 92% and 82% at one and three years respectively, and a safety profile consistent with the currently approved indication in CIS disease with or without papillary tumors. "We appreciate the FDA's collaboration throughout this process and remain fully committed to delivering this much-needed therapy to patients who currently have no approved alternatives when standard of care fails," said Richard Adcock, President and CEO of ImmunityBio. "We have completed the assembly and analysis of the requested additional information and will submit it within the next 30 days for the Agency's review." Based on discussions with the FDA, the Agency recommended that the Company provide certain additional information for its consideration to support a potential resubmission of the sBLA initially submitted in 2025 for the papillary indication, with this additional information not contemplating the initiation or design of a new clinical trial. ImmunityBio commercially launched ANKTIVA for NMIBC CIS with or without papillary tumors in the United States and has since expanded approvals to the United Kingdom and Saudi Arabia, with conditional approval in the European Union. Source: CONTACT: USA NEWS GROUP [email protected] (604) 265-2873 DISCLAIMER: Nothing in this publication should be considered as personalized financial advice. We are not licensed under securities laws to address your particular financial situation. No communication by our employees to you should be deemed as personalized financial advice. Please consult a licensed financial advisor before making any investment decision. This is a paid advertisement and is neither an offer nor recommendation to buy or sell any security. We hold no investment licenses and are thus neither licensed nor qualified to provide investment advice. The content in this report or email is not provided to any individual with a view toward their individual circumstances. USA News Group is a wholly-owned subsidiary of Market IQ Media Group, Inc. ("MIQ"). MIQ has been paid a fee for Oncolytics Biotech Inc. advertising and digital media from the company directly. There may be 3rd parties who may have shares of Oncolytics Biotech Inc., and may liquidate their shares which could have a negative effect on the price of the stock. This compensation constitutes a conflict of interest as to our ability to remain objective in our communication regarding the profiled company. Because of this conflict, individuals are strongly encouraged to not use this publication as the basis for any investment decision. The owner/operator of MIQ own shares of Oncolytics Biotech Inc. which were purchased in the open market, and reserve the right to buy and sell, and will buy and sell shares of Oncolytics Biotech Inc. at any time without any further notice commencing immediately and ongoing. We also expect further compensation as an ongoing digital media effort to increase visibility for the company, no further notice will be given, but let this disclaimer serve as notice that all material, including this article, which is disseminated by MIQ has been approved by Oncolytics Biotech Inc.; this is a paid advertisement, we currently own shares of Oncolytics Biotech Inc. and will buy and sell shares of the company in the open market, or through private placements, and/or other investment vehicles. While all information is believed to be reliable, it is not guaranteed by us to be accurate. Individuals should assume that all information contained in our newsletter is not trustworthy unless verified by their own independent research. Also, because events and circumstances frequently do not occur as expected, there will likely be differences between the any predictions and actual results. Always consult a licensed investment professional before making any investment decision. Be extremely careful, investing in securities carries a high degree of risk; you may likely lose some or all of the investment. SOURCES CITED: Logo: 21% more press release views with Request a Demo

临床3期临床结果临床2期临床1期免疫疗法

2026-01-27

·药研网

全球首创IL-15免疫疗法N-803国内申报临床

1月23日，CDE官网公示，ImmunityBio公司申报的原研药“N-803（nogapendekin alfa inbakicept）”临床试验申请获受理。 N-803（商品名 Anktiva®）是一种First-in-Class IL-15受体激动剂融合蛋白，通过激活CD8+ T细胞和NK细胞，增强机体抗肿瘤免疫应答。与部分细胞因子类药物不同，Anktiva 不会刺激免疫抑制性的 Treg 细胞，在免疫激活与安全性之间形成差异化优势。日前，ImmunityBio公布了QUILT-3.078临床2期研究的最新数据，该研究正在评估由IL-15超级激动剂Anktiva（nogapendekin alfa inbakicept）与CAR-NK细胞疗法联合的无化疗免疫治疗方案，用于治疗二线复发或进展的胶质母细胞瘤（GBM）患者，同时也涵盖通过单例患者IND（spINDs）接受治疗的1线至3线患者。截至2026年1月22日，研究已入组23例在接受标准治疗（包括手术、放疗及替莫唑胺化疗）后出现复发或进展的GBM患者，其中19例仍然存活。该研究的主要终点为总生存期（OS），截至数据更新时，中位总生存期尚未达到，显示该组合方案在延长患者生存方面释放出积极信号。 Anktiva 最早于2024 年4 月在美国获批上市，用于与BCG联合治疗对BCG无应答的非肌层浸润性膀胱癌(NMIBC)。作为近30年来获批的第三款肿瘤免疫治疗细胞因子药物，Anktiva代表了细胞因子疗法领域的重要突破。 2025年，ANKTIVA全年净产品收入约为1.13亿美元，同比增长700%，取得亮眼业绩。目前，该药正在开展覆盖膀胱癌、肺癌、胶质母细胞瘤等多项临床。 2026年1月16 日，ImmunityBio 宣布，其原研药 Anktiva® 获得沙特食品药品监督管理局（SFDA）批准上市，共涉及两项适应症： 1）与免疫治疗联合，用于既往标准治疗失败的转移性非小细胞肺癌（NSCLC）成人患者。值得注意的是，该适应症以“有条件批准”形式通过，后续仍需开展确认性临床试验以进一步验证其长期疗效。值得注意的是，SFDA 是全球首个在 NSCLC 适应症上对 Anktiva 给予有条件批准的监管机构。 2）与卡介苗（BCG）联合，用于治疗高风险、BCG 无应答的非肌层浸润性膀胱癌（NMIBC，伴原位癌 CIS）。在给药方式上，Anktiva 在NSCLC适应症中采用皮下注射，而在 NMIBC 中则通过膀胱灌注进行局部给药，体现了不同肿瘤类型下的差异化用药策略。 IL-15靶点进展 IL-15被认为是肿瘤免疫治疗的潜力靶点，目前全球监管机构仅批准一款IL-15靶向药Anktiva，还有多款在研IL-15靶向药，如下表。其中NKTR-255进展较快，其治疗弥漫性大B细胞淋巴瘤的临床试验已进入2/3期阶段。国内药企中，恒瑞医药的SHR-1501、奥赛康的ASKG315、博际生物的BJ-001、智翔金泰的GR2301等同样值得关注。去年7月，智翔金泰的 IL-15 单抗 GR2301 注射液获得 CDE 临床受理，用于白癜风治疗，填补了国内该靶点单抗在临床阶段的空白。全球部分在研 IL-15 靶向药物（药研网整理 | 数据来源：新药情报库） End 声明：本公众号所有发文章(包括原创及转载文章)系出于传递更多信息之目的，且注明来源和作者。本公众号欢迎分享朋友圈或大群，谢绝媒体或机构未经授权以任何形式转载至其他平台。转载/商务/投稿 | 联系微信15618157102（sum_Gmi）商务合作稿件征集点击了解详情往期回顾一文读懂抗体：结构、分类与ADCC/ ADCP/ CDC机制 BCG 2025行业回顾：创新药与中国的加速崛起

100 项与诺格白介素α-因奇西普相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
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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
非肌层浸润性膀胱尿路上皮癌	沙特阿拉伯	ImmunityBio, Inc.	2026-01-14
淋巴细胞减少	美国	ImmunityBio, Inc.	2025-06-02
非肌层浸润性膀胱肿瘤	美国	Altor BioScience Corp.	2024-04-22

未上市

10 条进展最快的记录,

后查看更多信息

适应症	最高研发状态	国家/地区	公司	日期
晚期非小细胞肺癌	临床3期	美国	ImmunityBio, Inc.	2018-05-18
转移性非小细胞肺癌	临床3期	美国	ImmunityBio, Inc.	2018-05-18
膀胱癌	临床3期	美国	ImmunityBio, Inc.	2017-06-02
复发性非小细胞肺癌	临床2期	美国	ImmunityBio, Inc.	2026-03-31
新冠肺炎后遗症	临床2期	美国	ImmunityBio, Inc.	2025-09-04
前列腺腺癌	临床2期	-	ImmunityBio, Inc.	2025-05-15
铂耐药性卵巢癌	临床2期	美国	ImmunityBio, Inc.	2024-11-06
复发性铂耐药性卵巢癌	临床2期	美国	ImmunityBio, Inc.	2024-11-06
多形性胶质母细胞瘤	临床2期	美国	ImmunityBio, Inc.	2024-08-07
胶质母细胞瘤，IDH野生型	临床2期	美国	ImmunityBio, Inc.	2024-08-07

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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


NCT03520686 (QUILT-2.023, Company_Website) 人工标引	临床3期	转移性非小细胞肺癌 \| 晚期非小细胞肺癌一线	-	ANKTIVA + CPI	襯鹹壓鏇顧蓋襯衊築顧(觸醖鬱構築顧獵鬱蓋憲): P-Value = 0.0065	积极	2026-01-13
				CPI
NCT03228667 (QUILT-3.055, Company_Website) 人工标引	临床2期	非小细胞肺癌二线	-	ANKTIVA + CPI (NSCLC)	淵醖構鹹築簾鏇廠繭襯(鹹築簾顧築壓築鹹憲獵) = 餘餘製襯範遞構憲範獵積選範壓襯艱繭築廠齋 (淵蓋窪膚膚糧糧積獵窪 )	积极	2026-01-13
				ANKTIVA + CPI (NSCLC + Responders)	網淵壓夢夢範鹹觸簾築(簾鏇簾獵廠窪觸膚網餘) = 網壓獵鹽糧鬱艱築窪糧壓鏇構襯夢範窪觸醖窪 (鏇壓簾製製繭顧築築壓 )
NCT04491955 (Pubmed \| Oncologist)	临床1/2期	转移性结直肠癌 pMMR	32	CV-301 + N-803 + bintrafusp alfa + PDS01ADC	廠簾廠夢蓋網製繭鹹獵(繭積積獵範選網顧鑰遞) = 顧網餘衊顧鬱襯憲範觸繭襯鑰觸觸齋網顧遞餘 (醖鬱廠廠範繭壓淵觸簾 ) 更多	不佳	2026-01-10
NCT03493945 (QuEST1, SITC2025)	临床1/2期	去势抵抗性前列腺癌	37	BNVax+BA+NAI	鬱獵鏇繭淵壓築範膚糧(餘蓋選遞窪壓壓淵構壓) = 網膚憲繭鬱願窪觸艱積壓鏇憲積範顧網膚選膚 (糧製襯顧鹽窪繭餘網獵 )	积极	2025-11-05
NCT03022825 (QUILT-3.032, Pubmed \| J Urol)	临床2期	-	54	NAI plus BCG (BCG-unresponsive high-grade Ta/T1 papillary nonmuscle-invasive bladder cancer)	鹽簾鹹膚壓築鏇網簾糧(觸網繭範鬱醖廠顧壓觸) = 顧鬱獵鹽鏇膚糧願衊鹽膚壓齋鬱糧壓夢鬱淵範 (鑰鹹蓋範憲鬱膚遞醖簾, 46.6 ~ 68.2) 更多	积极	2025-11-03
NEWS 人工标引	N/A	复发性胶质母细胞瘤	5	Anktiva	鏇憲網顧淵觸顧構鏇襯(憲餘淵遞鑰鬱衊襯鑰鏇) = 艱襯憲襯衊壓憲艱鬱製餘鑰獵願獵願鏇觸觸襯 (顧蓋蓋膚選顧獵製憲襯 )	积极	2025-08-29
NCT03493945 (QuEST1, CTgov)	临床1/2期	局部晚期恶性实体瘤 \| 晚期恶性实体瘤	59	castration+M7824+BN-Brachyury (Phase IIA Dose Expansion (Dose Exp.), Cohort 2, Arm 2.1A)	鹹繭襯鏇醖醖鑰選構範 = 蓋製壓願夢淵淵蓋範蓋築鬱糧遞鏇構膚齋築糧 (齋齋壓鏇簾衊築蓋醖鹽, 醖齋觸窪糧餘衊餘醖繭 ~ 襯廠製糧網膚襯窪範鏇) 更多	-	2025-06-08
				N-803+M7824+BN-Brachyury (All Participants in Phase IIA Dose Expansion and Phase IIB Dose Expansion)	鹹繭襯鏇醖醖鑰選構範 = 積範壓淵餘顧顧積簾糧築鬱糧遞鏇構膚齋築糧 (齋齋壓鏇簾衊築蓋醖鹽, 糧蓋廠糧憲網製積觸蓋 ~ 壓鹽獵願糧醖簾願築製) 更多
NCT04390399 (QUILT-88, ASCO2025)	临床2期	转移性胰腺癌 ALC \| CA19-9	84	N-803 and PD-L1 t-haNK chemo-immunotherapy	衊鑰獵蓋鏇夢築網網糧(鬱蓋鏇壓網憲積鏇憲齋) = Grade 3 or higher TEAEs occurred in 95% of patients and were largely chemotherapy-associated 蓋觸艱醖簾淵選醖鏇廠 (廠選壓鏇獵遞壓鏇遞憲 )	积极	2025-05-30
				Low-dose SBRT and low-dose chemotherapy
NCT03022825 (QUILT-3.032, Company_Website \| Literature) 人工标引	临床2/3期	非肌层浸润性膀胱肿瘤	180	ANKTIVA®ANKTIVA® plus BCG (CIS with or without Papillary)	壓窪選鑰夢簾觸鏇餘膚(齋繭鑰膚衊構顧顧積顧) = 壓製壓繭鏇壓鑰網艱鑰獵廠蓋顧觸膚齋襯簾齋 (願糧壓積餘網願鏇鹽鹹 ) 更多	积极	2025-04-28
				ANKTIVA® Plus BCG (Papillary without CIS)	糧餘鏇積積餘製齋鑰繭(獵顧襯蓋膚餘鏇獵鏇網) = 觸鏇蓋鏇構築鹽鑰窪淵積選餘鏇蓋淵艱膚遞簾 (願鹽繭簾憲糧齋襯築繭 ) 更多
NCT03381586 (CTgov)	临床1期	-	20	ALT-803 (Group A)	餘糧顧艱鹽獵構夢廠鑰(壓製積鏇鏇築鑰餘餘鬱) = 獵獵鹽獵網蓋醖餘選膚構顧淵鹹襯襯齋獵積膚 (築艱範鏇壓積艱願醖選, 0.813) 更多	-	2025-03-24
				ALT-803 (Group B)	餘糧顧艱鹽獵構夢廠鑰(壓製積鏇鏇築鑰餘餘鬱) = 願願淵醖醖鑰壓鏇獵構構顧淵鹹襯襯齋獵積膚 (築艱範鏇壓積艱願醖選, 0.095) 更多