Open-Label, Single-Arm Phase 2 Study Of Nogapendekin Alfa Inbakicept, PD-L1 T-HaNK, And Bevacizumab And Randomized Phase 2B Study Of Nogapendekin Alfa Inbakicept, Bevacizumab, And Tumor Treatment Fields With Or Without PD-L1 T-HaNK In Participants With Recurrent Or Progressive Glioblastoma

This Phase 2a/2 study evaluates the safety, tolerability, and efficacy of neoadjuvant and adjuvant NAI, hAd5-HPV vaccine (IBRX-042), and nab-paclitaxel in participants with locally advanced HPV-positive oropharyngeal squamous cell carcinoma (OPSCC). The study includes a Phase 2a safety lead-in followed by a randomized Phase 2 comparison of a de-intensified experimental chemoradiation approach versus standard-of-care chemoradiation.

开始日期2026-07-22

申办/合作机构

ImmunityBio, Inc.

NCT07578558

/ Not yet recruiting临床2期

Phase 2, Randomized, Open-Label Clinical Trial Evaluating Nogapendekin Alfa Inbakicept in Combination With Standard of Care Versus Standard of Care Alone in Critically Ill Adults With Sepsis and Persistent Lymphopenia

This is a Phase 2, randomized, open-label study evaluating the safety and efficacy of nogapendekin alfa inbakicept (NAI, ANKTIVA®) in combination with standard of care versus standard of care alone in critically ill adults with sepsis and persistent lymphopenia. The study aims to determine whether NAI can improve 28-day mortality by addressing the immunosuppressive phase of sepsis characterized by persistent lymphopenia (absolute lymphocyte count <1,000 cells/µL). Participants will be randomized 1:1 to receive either NAI 1.2 mg subcutaneous injection on Days 3 (or earlier if ALC <700 cells/µL), Day 14, and potentially Day 21 if ALC remains <1,000 cells/µL, plus standard of care, or standard of care alone. The study will enroll approximately 50 participants (25 per arm) with persistent lymphopenia.

开始日期2026-07-06

申办/合作机构

ImmunityBio, Inc.

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2026-06-30

申办/合作机构

Washington University School of Medicine

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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-因奇西普相关的转化医学

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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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385

项与诺格白介素α-因奇西普相关的文献（医药）

2026-12-31·Emerging Microbes & Infections

Neuraminidase-inhibiting antibodies boosted by H1N1pdm infection cross-react differently with H5N1 of clades 2.3.4.4b and 2.3.2.1a

Article

作者: Aziz, Dinah Binte ; Tan, Yee-Joo ; Chan, Yee Teng ; Liew, Kong Yen ; Tambyah, Paul ; Tan, Chee Wah

Antibodies against neuraminidase (NA) are an independent correlate of protection and the antigenic relatedness between H1N1pdm and H5N1 NAs suggests that seasonal influenza infection may provide cross-reactive immunity. In this study, recent H1N1pdm infection elicited modest NA-inhibiting (NAI) antibody responses against contemporary A/Victoria/4897/2022 (H1N1pdm) but strong responses against older A/California/7/2009 (H1N1pdm). Convalescent sera exhibited significantly higher cross-reactive NAI against clade 2.3.4.4b H5N1 (A/Texas/37/2024) than non-flu A patients, whereas H3N2 infection did not elicit such cross-reactivity. NAI titres were comparable between N1-California and N1-Texas but lower against N1-Victoria, indicating greater antigenic similarity between N1-California and N1-Texas. This was supported by stronger inhibition of N1-Texas by N1-California sheep antiserum compared with N1-Victoria sheep antiserum. Surprisingly, H1N1pdm-infected patients exhibited very low NAI against clade 2.3.2.1a H5N1 (N1-Bangladesh; GMT of 171 vs GMT 1159 for N1-Texas). Mouse antisera demonstrated reduced reciprocal inhibition between N1-Texas and N1-Bangladesh, consistent with their antigenic divergence. When four residues in N1-Bangladesh were substituted with their corresponding residues in N1-Texas, N1-Bangladesh antiserum showed reduced NAI, while N1-Texas antisera showed increased inhibition compared with wild-type N1-Bangladesh. This suggests that these amino acid differences are partially responsible for their antigenic divergence. Importantly, longitudinal analysis revealed that boosted cross-reactive NAI responses waned by day 90 post-infection, highlighting their limited durability. Together, these findings demonstrate that seasonal H1N1pdm infection can transiently boost cross-reactive NAI antibodies against clade 2.3.4.4b H5N1, but antigenic divergence in clade 2.3.2.1a limits cross-reactivity. As such, the impact of pre-existing antibody during an H5N1 outbreak is dependent on the infecting clade.

2026-06-01·CRITICAL REVIEWS IN ONCOLOGY HEMATOLOGY

Advances in intravesical therapy for non-muscle-invasive bladder cancer

Review

作者: Tang, Yanfeng ; Zeng, Hao ; Zhu, Qiyu ; Xu, Chenhao ; Chen, Junru ; Liu, Haoyang ; Wang, Ling

Non-muscle-invasive bladder cancer (NMIBC) accounts for roughly 75% of newly diagnosed bladder cancer and associates with high risk of recurrence and progression. Intravesical therapy remains the cornerstone of NMIBC management following transurethral resection of bladder tumor (TURBT). For low-risk NMIBC, immediate single instillation of chemotherapy after TURBT effectively reduces recurrence. Intermediate-risk patients could benefit from either intravesical chemotherapy or Bacillus Calmette-Guérin (BCG) instillation, with emerging therapies such as UGN-102 chemoablation showing promise. For high/very high-risk NMIBC, full-dose, 3-year BCG instillation remains the standard of care, However, global BCG shortages and treatment failures have prompted the need for alternative strategies. Optimization of BCG regimens, such as two induction courses, may preserve efficacy while improving feasibility. Moreover, alternative agents such as sequential gemcitabine and docetaxel instillation have demonstrated favorable outcomes in both BCG-naïve and BCG-unresponsive patients. For those with BCG failure, a number of novel therapies are under active investigation. Gene therapy (nadofaragene firadenovec), oncolytic viral therapy (CG0070), interleukin-15 superagonist (Nogapendekin alfa-inbakicept), and innovative drug delivery systems (TAR-200) have shown encouraging clinical potential in this population. This review provides an overview of current intravesical treatment strategies for NMIBC across different risk groups and highlights promising new approaches aimed at overcoming the limitations of BCG therapy.

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.

393

项与诺格白介素α-因奇西普相关的新闻（医药）

2026-06-05

·BioSpace

ImmunityBio Presents New Clinical and Comparative Data Across Lung and Bladder Cancer at ASCO 2026

Presentations highlight ANKTIVA®-based approaches in non-small cell lung cancer (NSCLC) and non-muscle invasive bladder cancer (NMIBC) CULVER CITY, Calif.--(BUSINESS WIRE)--ImmunityBio, Inc. ( NASDAQ: IBRX ), a commercial-stage immunotherapy company, today announced two poster presentations and one online publication at the American Society of Clinical Oncology (ASCO) Annual Meeting, taking place May 29-June 2, 2026, in Chicago. The presentations span two randomized Phase 3 trials in advanced NSCLC and a matched adjusted indirect comparison (MAIC) in BCG unresponsive non-muscle invasive bladder cancer (NMIBC), and collectively evaluate ANKTIVA ® (nogapendekin alfa inbakicept-pmln), the company’s IL-15 receptor agonist immunotherapy designed to activate natural killer (NK) cells, CD4+ and CD8+ T cells, and memory T cells, across multiple solid tumor indications. “ASCO provides an important opportunity to share emerging clinical and translational data that continue to deepen our understanding of how ANKTIVA-based immunotherapy may restore immune function and rescue or reinvigorate the response to checkpoint inhibitors,” said Dr. Patrick Soon-Shiong, Founder, Executive Chairman, and Global Chief Scientific and Medical Officer of ImmunityBio. “ANKTIVA is the first FDA-approved immunotherapy designed to stimulate NK cells, CD4+ and CD8+ T cells, and memory T cells, which are the very immune cells that are depleted in patients with lymphopenia and that are critical to mounting an effective anti-tumor response. Growing long-term survival data across bladder, lung and other solid tumors are beginning to put in focus a compelling hypothesis: that restoring immune competence and addressing lymphopenia may be as a fundamental to cancer care as targeting the tumor itself. These findings reinforce our conviction that the future of immunotherapy lies in activating and amplifying the immune system, not suppressing it.” Presentation highlights include: ASCO 2026 Annual Meeting Poster Presentations - Sunday, May 31st (9am-12pm) Poster Title: Phase 3 trial ResQ201A of nogapendekin alfa inbakicept (NAI) plus tislelizumab and docetaxel vs. docetaxel monotherapy for advanced or metastatic NSCLC resistant to ICI therapy Poster Board: 455am Abstract: #TPS8671 Presenter: Andreas Saltos (Affiliation: Moffitt) Poster Title: Efficacy outcomes in first line (1L) non–small cell lung cancer (NSCLC) with maintenance of immune competence: QUILT‑2.023 randomized phase 3 study of IL‑15R agonist nogapendekin alfa inbakicept (NAI) with checkpoint inhibitor (CPI) ± chemotherapy Poster Board: 378 Abstract: #8588 Presenter: John Wrangle (Affiliation: MUSC) Online Publication Only Abstract Title: A matched adjusted indirect comparison (MAIC) of NAI+BCG & pembrolizumab in patients with BCG unresponsive NMIBC with CIS ± papillary disease – Will be published on at 5:00 PM EDT on May 21, 2026 About ANKTIVA ® (nogapendekin alfa inbakicept-pmln) The interleukin-15 (IL-15) cytokine plays a crucial role in the immune system by affecting the development, maintenance, and function of key immune cells—NK and CD8+ killer T cells—that are involved in killing cancer cells. By activating NK cells, ANKTIVA ® overcomes the tumor escape phase of clones resistant to T cells and restores memory T cell activity with resultant prolonged duration of complete response. ANKTIVA® is a first-in-class IL-15 receptor agonist IgG1 fusion complex, consisting of an IL-15 mutant (IL-15N72D) fused with an IL-15 receptor alpha, which binds with high affinity to IL-15 receptors on NK, CD4+, and CD8+ T cells. This fusion complex of ANKTIVA ® mimics the natural biological properties of the membrane-bound IL-15 receptor alpha, delivering IL-15 by dendritic cells and driving the activation and proliferation of NK cells with the generation of memory killer T cells that have retained immune memory against these tumor clones. About ImmunityBio ImmunityBio, Inc. is a biotechnology company focused on innovating, developing, and commercializing next-generation immunotherapies designed to activate the patient’s immune system and deliver durable protection against cancer and infectious diseases. Our approach harnesses both the adaptive and innate immune systems with the goal of restoring immune function and generating lasting immunological memory in patients. At the core of our strategy is the Cancer BioShield ™ platform, which is designed to stimulate critical lymphocytes, including natural killer (NK) cells, cytotoxic T cells, and memory T cells via our proprietary IL-15 receptor superagonist, ANKTIVA ® (nogapendekin alfa inbakicept). Our Cancer BioShield platform is anchored by this antibody-cytokine fusion protein and is complemented by a portfolio that includes adenovirus-vectored vaccines, allogeneic (off-the-shelf) and autologous NK-cell therapies, and additional immunomodulators intended to promote immunogenic cell death and support durable immune responses while potentially reducing reliance on high-dose chemo-radiation therapy. For more information, visit ImmunityBio.com and connect with us on X (Twitter), Facebook , LinkedIn , and Instagram . Forward-Looking Statements This press release contains forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995, including statements regarding the clinical development of ANKTIVA® (nogapendekin alfa inbakicept-pmln), the potential benefits of ANKTIVA-based immunotherapy in non-small cell lung cancer (NSCLC) and non-muscle invasive bladder cancer (NMIBC), future regulatory submissions and approvals, commercialization plans and market potential, and the company's strategic vision for restoring immune competence in cancer patients. These forward-looking statements are based on ImmunityBio's current expectations and beliefs and are subject to uncertainties and factors that could cause actual results to differ materially from those expressed or implied by such statements. Such risks and uncertainties include, but are not limited to: the risk that clinical trials may not demonstrate adequate safety and efficacy to support regulatory approval or may be delayed or terminated; the risk that regulatory authorities may not approve ANKTIVA for additional indications or may impose restrictions on its use; the risk that the company may not successfully commercialize ANKTIVA or achieve market acceptance; competition from other therapies; manufacturing and supply chain risks; intellectual property risks; and the company's ability to obtain additional funding to support its operations. More details about these and other risks that may impact ImmunityBio’s business are described under the heading “Risk Factors” in the Company’s Form 10-K filed with the U.S. Securities and Exchange Commission (SEC) on February 23, 2026 as well as its Form 10-Q filed with the SEC on May 7, 2026, and in subsequent filings made by ImmunityBio with the SEC, which are available on the SEC’s website at . ImmunityBio cautions you not to place undue reliance on any forward-looking statements, which speak only as of the date hereof. ImmunityBio does not undertake any duty to update any forward-looking statement or other information in this press release, except to the extent required by law. Contacts ImmunityBio Contacts: Investors Hemanth Ramaprakash, PhD, MBA ImmunityBio, Inc. +1 858-746-9289 Hemanth.Ramaprakash@ImmunityBio.com Media Sarah Singleton ImmunityBio, Inc. +1 415-290-8045 Sarah.Singleton@ImmunityBio.com

2026-05-29

·PRNewswire

The $13 Million Company Teaching the Immune System to Hunt Cancer

Issued on behalf of GT Biopharma, Inc. (NASDAQ: GTBP) Three drugs in human trials. A platform licensed from one of the world's top cancer-research universities. A market cap smaller than a Manhattan apartment. For investors willing to look where almost no one is looking, GT Biopharma is the kind of asymmetric setup that biotech is built on. NEW YORK, May 29, 2026 /PRNewswire/ -- USA News Group Market Commentary - Start with the number that makes everyone do a double take. As of mid-May 2026, GT Biopharma (NASDAQ: GTBP) carried a market capitalization of roughly $13 million. Thirteen million. That is not a typo, and it is not a shell company. It is a clinical-stage immuno-oncology company with three separate drug candidates already dosing patients in human trials, a technology platform exclusively licensed from the University of Minnesota, and a scientific approach that the largest names in cancer immunotherapy are spending billions to pursue. See the full GT Biopharma investor breakdown at USA News Group → That gap — between what the company is doing in the clinic and what the market is paying for it — is the entire story. Whether it closes, and in which direction, is the question every investor reading this should be weighing right now. The idea: don't build a new weapon, sharpen the one you already have Most cancer therapies try to bolt something new onto the body — a manufactured cell, a synthetic antibody, a toxic payload. GT Biopharma's approach is different, and once you understand it, it's hard to forget. The human immune system already contains a class of cells whose entire job is to find and destroy abnormal cells: natural killer cells, or NK cells. They are the immune system's first responders, patrolling the body and killing threats without needing to be "trained" first. The problem in cancer is that tumors learn to hide from them. GT Biopharma's platform, called TriKE® — short for Tri-specific Killer Engager — is designed to drag those NK cells directly onto the tumor and switch them on. A TriKE molecule is engineered with three parts joined together. One arm grabs the NK cell by a receptor called CD16. A second arm grabs the cancer cell by a marker on its surface. And in the middle sits a molecule called IL-15, which acts like a shot of adrenaline, keeping the NK cell alive and multiplying once it's locked onto its target. The result, in concept, is elegant: you take the body's existing assassins, handcuff them to the tumor, and tell them to get to work. The platform was developed at the University of Minnesota, and GT Biopharma holds an exclusive worldwide license to develop and commercialize therapies based on it. This is not a science project the company dreamed up in isolation — it's institutional research that GTBP has the rights to turn into medicine. Why now: three shots on goal, all live What changed in 2026 is that GT Biopharma stopped being a one-drug story. As of this spring, the company has advanced three TriKE candidates into the clinic — a milestone its leadership rightly calls a turning point. Track every clinical milestone on the GTBP catalyst timeline → The lead program is GTB-3650, aimed at relapsed or refractory CD33-positive blood cancers — specifically acute myeloid leukemia (AML) and high-risk myelodysplastic syndrome (MDS), two of the most treatment-resistant cancers in oncology. It is the first TriKE built on camelid nanobody technology — antibody fragments derived from the same family as llamas and alpacas, prized for being small, stable, and able to penetrate tissue. The Phase 1 dose-escalation trial began enrolling in early 2025 and has moved methodically upward through its dose cohorts. As of the company's Q1 2026 report in May, Cohort 4 enrollment was complete with eight patients treated across the first four cohorts — and, critically, the earlier safety reviews advanced without the dose-limiting toxicities that derail so many early trials. The study can escalate through up to seven cohorts, and management has guided to a meaningful data update in the second half of 2026. The newest program is where the ambition becomes obvious. In May 2026, GT Biopharma dosed the first patient in the Phase 1 trial of GTB-5550, a TriKE targeting a protein called B7-H3. Here is why that matters: B7-H3 is expressed on a huge range of solid tumors, and in metastatic castration-resistant prostate cancer it appears in over 90% of tumors. The trial begins with a prostate-cancer-focused dose escalation, then expands into a "basket" across as many as seven solid tumor types — prostate, ovarian, breast, head and neck, non-small cell lung, pancreatic, and bladder. In the company's own framing, the solid-tumor patient population GTB-5550 targets is "orders of magnitude larger" than the blood-cancer population of its lead drug. And GTB-5550 uses subcutaneous dosing — a simple injection rather than an infusion — which the company describes as more patient-friendly, a quiet but real commercial advantage if the drug works. Three programs. Two cancers as different as liquid and solid tumors. One underlying platform. That is the shape of a company trying to prove a technology, not just a single molecule. The market it's chasing is enormous The backdrop here is not subtle. The global oncology market is projected to nearly double from roughly $139 billion in 2025 to about $268 billion by 2034. Solid tumors alone represent a market estimated in the hundreds of billions of dollars, and B7-H3 — GTB-5550's target — shows up across many of the most common and lethal of them. NK-cell-directed immunotherapy has become one of the most closely watched frontiers in the entire sector, precisely because it offers the prospect of harnessing the immune system with potentially fewer of the brutal side effects of conventional treatment. Why NK-cell therapy is biotech's hottest frontier — read the deep dive → When a tiny company is pointed at a market that large, the math of asymmetry takes over. It does not require GT Biopharma to win the whole field. It requires only that one of its three shots connects — and that the market eventually notices a company priced near $13 million is playing in an arena measured in the hundreds of billions. How GT Biopharma stacks up against its NK-cell peers The most useful way to understand GTBP's positioning is to look at the company it keeps. NK-cell and immune-engager therapy is a crowded, well-funded field — and the contrast in scale is the entire investment argument. ImmunityBio (NASDAQ: IBRX) is the proof of concept that NK-cell immunotherapy can reach the market. Its NK-activating therapy ANKTIVA is FDA-approved for bladder cancer, the company reported roughly $44 million in product revenue in Q1 2026 and held some $381 million in cash, and it is now scaling NK-cell manufacturing to billions of cells per batch. ImmunityBio is what NK-cell success looks like at commercial scale — and a reminder of the valuation gap a clinical-stage peer could theoretically narrow if its data delivers. Fate Therapeutics (NASDAQ: FATE) is the deep-pocketed platform play, engineering off-the-shelf NK and CAR-T cell therapies from induced pluripotent stem cells, with roughly $175 million in cash and a runway management has guided into 2028. Fate illustrates how richly the market will fund an NK/cell-therapy platform it believes in — a striking counterpoint to GTBP's microcap valuation. Nkarta (NASDAQ: NKTX) is the engineered-NK-cell specialist, advancing its platform into autoimmune disease and backed by a market capitalization and cash position orders of magnitude above GT Biopharma's. Nkarta shows that NK-cell companies can command substantial valuations well before commercialization, on the strength of platform potential alone. Artiva Biotherapeutics (NASDAQ: ARTV) rounds out the set as the allogeneic, off-the-shelf NK-cell developer whose lead candidate AlloNK is heading toward a Phase 3 registrational trial in refractory rheumatoid arthritis in 2026. Artiva demonstrates how far and how fast an NK-cell program can advance through the clinic — the kind of trajectory GTBP investors are betting its TriKE platform can follow. Set GT Biopharma beside those four names and the picture sharpens. They are pursuing variations of the same fundamental thesis — unleash NK cells against disease — and the market has assigned them valuations ranging from the hundreds of millions into the billions. GT Biopharma, with three candidates already in the clinic, sits near $13 million. Either the market has correctly priced a struggling microcap, or it has badly overlooked a platform company in the same arena as far larger peers. That is the bet, stated plainly. The risks, stated honestly No serious investor case is complete without the other side of the ledger, and GT Biopharma's is real. This is a clinical-stage company with no approved products and no product revenue. Its cash balance was approximately $9 million at the end of Q1 2026, which management expects to fund operations only through the fourth quarter of 2026 — meaning additional financing, likely dilutive to existing shareholders, is a near-certainty rather than a possibility. The stock trades well under a dollar and far below its 52-week high, and a Roth Capital analyst, while maintaining a Buy rating, cut the price target to $3 from $8 earlier this year. Phase 1 trials are designed to test safety, not to prove a drug works; the encouraging absence of dose-limiting toxicities and the early signs of NK-cell activation are genuinely positive, but they are not efficacy. Most drugs that enter Phase 1 never reach the market. And the very peers that make GTBP look cheap are also formidable competitors with vastly greater resources. In short: this is a high-risk, binary-outcome situation. It is exactly the kind of company that can multiply many times over on a single strong data readout — and exactly the kind that can be forced into painful dilution or worse if the data disappoints or the financing window closes. Both outcomes are live. The bottom line GT Biopharma is a study in asymmetry. On one side: a roughly $13 million valuation, a sub-dollar stock, a thin cash runway, and all the risk that comes with clinical-stage biotech. On the other: three drugs dosing patients, a platform licensed from a top-tier research university, a mechanism the biggest players in immuno-oncology are validating with their own R&D budgets, and a pair of catalysts — GTB-3650 data and GTB-5550 progress — both expected in the second half of 2026. That is the setup. A company priced for failure, sitting on a platform built for something much larger, with hard data events on the calendar in a matter of months. For investors who understand that the biggest biotech returns come from the names the market has written off just before it's forced to reconsider, GT Biopharma is a story worth watching very closely between now and year-end. Get the full GTBP investor profile, pipeline, and catalyst calendar at USA News Group → CONTACT: USA News Group [email protected] 604-265-2873 Sources: GT Biopharma, Inc., "GT Biopharma Announces First Patient Dosed in Phase 1 Trial of GTB-5550, a B7-H3-Targeted Natural Killer (NK) Cell Engager for Solid Tumors," GlobeNewswire, May 14, 2026. GT Biopharma, Inc., "GT Biopharma Reports First Quarter 2026 Financial Results," May 15, 2026 (Cohort 4 complete, 8 patients across first four cohorts; ~$9M cash to Q4 2026; 2H 2026 updates). GT Biopharma, Inc., IND submission / pipeline overview — TriKE mechanism (camelid anti-CD16 / scFv anti-CD33 / IL-15), GTB-3650 dose-escalation design (up to 7 cohorts, ~14 patients), GTB-5550 design and B7-H3 >90% in mCRPC; gtbiopharma.com product pipeline. Roth Capital analyst note (Jonathan Aschoff), price target revised to $3 (Buy), 2026. Global Market Insights Inc. oncology market size ($139.4B 2025 → $268.3B 2034); Data Bridge Market Research solid-tumor market context. ImmunityBio (NASDAQ: IBRX) Q1 2026 results and NK-cell manufacturing release, 2026. Fate Therapeutics (NASDAQ: FATE) Q1 2026 results (runway into 2028), May 13, 2026. Nkarta (NASDAQ: NKTX) corporate/clinical disclosure, 2026. Artiva Biotherapeutics (NASDAQ: ARTV) corporate disclosure / AlloNK Phase 3 plan, 2026. 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 digital media distribution 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. 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 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. USA News Group is a wholly-owned subsidiary of Market IQ Media Group, Inc. ("MIQ"). This article is being distributed by USA News Group on behalf of MIQ. MIQ has been paid a fee for GT Biopharma, Inc. advertising and digital media from Creative Direct Marketing Group ("CDMG"). There may be 3rd parties who may have shares of GT Biopharma, 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 article or email as the basis for any investment decision. The owner/operator of MIQ currently owns shares of GT Biopharma, Inc. that were purchased in the open market and reserves the right to buy and sell, and will buy and sell shares of GT Biopharma, 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 disseminated by MIQ has been reviewed and approved on behalf of GT Biopharma, Inc. by CDMG; this is a digital media distribution. 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 article 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 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. 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免疫疗法临床1期引进/卖出上市批准细胞疗法

2026-05-27

·国际干细胞与免疫细胞研究

15个月持续完全缓解！无化疗门诊CAR-NK暴击淋巴瘤，顶刊数据全面围剿脑瘤、肺癌等

点击蓝字关注我们据“AJMC”相关报道，现成异基因CAR-NK细胞疗法联合利妥昔单抗，可在不使用化疗的前提下，帮助华氏淋巴瘤患者实现长期病情缓解，一例CR长达15个月，且后续未再进行其他治疗。该疗法是首款无需化疗、无需淋巴细胞清除的CAR-NK方案。所有治疗均可在门诊完成。疗法同时靶向CD19与CD20靶点，抗肿瘤效果显著；其起效快、疗效持久的特点，也契合当下肿瘤限时治疗的发展方向，为癌症患者带来新的希望与选择！ ▲截图源自“AJMC” 门诊式CAR-NK免疫疗法亮剑难治性淋巴瘤，一例CR长达15个月本文开篇提到的这项QUILT-106（NCT06334991）临床研究，采用可表达高亲和力CD16受体的基因工程CD19特异性CAR-NK细胞，依托双重作用机制联合利妥昔单抗，显著提升抗肿瘤活性。研究针对治疗手段匮乏、经标准靶向及抗体治疗后复发耐药的罕见B细胞恶性肿瘤——华氏非霍奇金淋巴瘤，精准解决临床治疗难题。该疗法支持门诊全程施治，无需化疗及淋巴细胞清除预处理，有效规避传统治疗毒副作用。试验统一给药方案为21天一个疗程，共4个疗程，累计输注8剂CAR-NK细胞与6剂利妥昔单抗，治疗全程无需额外辅助干预，并在完成2个疗程后开展疗效评估。长期随访数据显示：两例难治性患者均获得持久完全缓解（CR）。其中多发淋巴瘤骨病灶患者，完全缓解状态已维持7个月，疗效可通过PET扫描直观验证（详见下图）；骨髓肿瘤浸润率达95%的重度受累患者，仅4剂联合治疗即实现骨髓形态学完全缓解，完成全部疗程且无后续治疗干预的情况下，缓解时长已达15个月并持续保持。 ▲图源“Nat Med”，版权归原作者所有，如无意中侵犯了知识产权，请联系我们删除本研究首次证实，无化疗、无预处理的门诊式异基因CD19 CAR-NK联合利妥昔单抗方案，为血液肿瘤领域带来新的曙光！ CAR-NK联合疗法重创胶质母细胞瘤，82.6%患者获得持续生存获益一项Ⅱ期QUILT-3.078临床试验，评估了ANKTIVA®联合PD-L1 t-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临床效果。ⅡB期试验采用1:1随机分组设计，对照组采用ANKTIVA+贝伐珠单抗+肿瘤电场疗法，试验组在此基础上新增PD-L1 t-haNK联合治疗。本次研究整体纳入23例经常规手术、放疗、替莫唑胺化疗后疾病进展的复发/进展性患者。结果显示：23例患者中19例存活，生存获益比例达82.6%。其中14例可评估患者构成疗效分析队列，累计接受139剂联合免疫治疗，目前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，请联系我们删除影像学结果直观证实，代表性患者接受CAR-NK联合治疗后，肿瘤病灶显著缩小。 ▲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 CCCR-NK92疗法，助肺癌病灶显著缩小全球知名期刊《Cell Transplantation（细胞移植）》刊发过一个振奋的临床案例，证实改良型CAR-NK疗法——CCCR-NK92，对晚期非小细胞肺癌具备明确治疗活性。本次案例为一名69岁晚期非小细胞肺癌女性患者，基因检测提示T790突变、Exon-19缺失突变，合并颅内转移，既往经吉非替尼、奥西替尼靶向治疗及头部放疗后病情仍进展。患者因担忧化疗副作用拒绝常规化疗，最终符合入组条件，参与CCCR-NK92疗法治疗晚期非小细胞肺癌的Ⅱ期临床试验（NCT03656705）。结果显示：患者完成3个周期CAR-NK治疗后，影像学复查显示病灶明显缩小：气管前-后腔静脉间质区淋巴结由11.3mm缩减至8.55mm，左肺包裹性胸腔积液由46.22mm缩减至33.59mm（详见下图），充分验证了该疗法对晚期肺癌的干预价值。 ▲图源“Sage Journals”，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 CD19 CAR-NK疗法强效对抗白血病，治疗30天病灶完全消退《新英格兰医学杂志》刊发MD安德森癌症中心重磅临床研究（NCT03056339），证实靶向CD19的CAR-NK细胞疗法，对CD19阳性恶性肿瘤具备优异的治疗效果，临床数据极具突破性。研究中一例发生Richter转化的慢性淋巴细胞白血病患者，经CAR-NK细胞输注治疗后成效显著。结果显示：输注30天后PET-CT复查显示，高级别淋巴瘤病灶完全消退，氟脱氧葡萄糖摄取转为阴性。患者虽初期存在血细胞减少、骨髓残留病灶等问题，但最终成功实现完全缓解（CR），充分彰显了CD19 CAR-NK疗法强效、持久的抗肿瘤能力。 ▼5号患者在CAR-NK细胞治疗前后的FDG PET-CT、PET-CT对比 ▲图源“N Engl J Med”，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 CAR工程的出现引领了细胞治疗领域的变革，经CAR修饰后的NK细胞，能更加精准的对抗肿瘤细胞，CAR-NK细胞在临床研究中具有广阔的应用前景，在治疗血液肿瘤及部分实体瘤中，展现了令人惊艳的初步疗效及安全性。如果您对目前的治疗方案存疑，或想寻求CAR-NK细胞、NK细胞、CAR-T细胞获国内外其他抗癌新技术的帮助，可扫文末二维码，将治疗经历、近期病理报告等，提交至国际干细胞与免疫细胞研究医学部，进行初步评估或申请国内外抗癌专家会诊。参考资料 [1]Zhang X,et al.Cytokine release syndrome after modified CAR-NK therapy in an advanced non-small cell lung cancer patient: a case report[J]. Cell Transplantation, 2022, 31: 09636897221094244. https://journals.sagepub.com/doi/full/10.1177/09636897221094244 [2]Liu E,et al.Thompson P, Basar R, Nassif Kerbauy L, Overman B, Thall P, Kaplan M, Nandivada V, Kaur I, Nunez Cortes A, Cao K, Daher M, Hosing C, Cohen EN, Kebriaei P, Mehta R, Neelapu S, Nieto Y, Wang M, Wierda W, Keating M, Champlin R, Shpall EJ, Rezvani K. Use of CAR-Transduced Natural Killer Cells in CD19-Positive Lymphoid Tumors. N Engl J Med. 2020 Feb 6;382(6):545-553. [3]https://www.ajmc.com/view/long-term-cr-seen-with-allo-car-nk-cell-therapy-plus-rituximab-in-waldenstrom-nhl [4]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

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
D12888	-	-	-

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
转移性非小细胞肺癌	沙特阿拉伯	ImmunityBio, Inc.	2026-04-21
原位癌	欧盟	ImmunityBio, Inc.	2026-02-16
原位癌	冰岛	ImmunityBio, Inc.	2026-02-16
原位癌	列支敦士登	ImmunityBio, Inc.	2026-02-16
原位癌	挪威	ImmunityBio, Inc.	2026-02-16
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,

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适应症	最高研发状态	国家/地区	公司	日期
社区获得性肺炎	临床3期	-	ImmunityBio, Inc.	2026-04-15
急性呼吸窘迫综合征	临床3期	-	ImmunityBio, Inc.	2026-04-15
脓毒症	临床3期	-	ImmunityBio, Inc.	2026-04-15
脓毒性休克	临床3期	-	ImmunityBio, Inc.	2026-04-15
肺癌	临床3期	美国	ImmunityBio, Inc.	2022-07-27
晚期非小细胞肺癌	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
HPV阳性的口咽鳞状细胞癌	临床2期	-	ImmunityBio, Inc.	2026-07-22
HPV16阳性口咽癌	临床2期	-	ImmunityBio, Inc.	2026-07-22
复发性胶质母细胞瘤	临床2期	-	ImmunityBio, Inc.	2026-07-22

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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


NCT02782546 (CTgov)	临床2期	急性髓性白血病 \| 难治性急性髓细胞白血病	60	G-CSF+ALT-803+Tacrolimus+mycophenolate mofetil+CIML NK cell infusion (Recipient)	淵糧願醖壓蓋簾積顧獵 = 膚憲製獵襯觸糧選鹹遞齋築積廠鏇鏇憲鏇製構 (觸鏇簾膚壓淵鑰廠觸鬱, 鹹壓積壓遞蓋簾簾壓範 ~ 蓋獵膚醖艱遞艱廠艱網) 更多	-	2026-06-01
				Leukapheresis (Donor)	積糧網鬱範襯艱窪築糧(襯壓築壓齋觸廠願選壓) = 蓋憲醖觸膚鑰鏇壓範簾鏇襯夢鹽壓壓網憲願簾 (艱遞淵襯鏇淵夢廠壓夢, 繭夢網齋膚鑰夢鏇憲願 ~ 獵壓夢餘衊鏇衊選廠觸) 更多
NCT03022825 (QUILT-3.032, ASCO2026)	临床3期	非肌层浸润性膀胱肿瘤	173	nogapendekin alfa inbakicept-pmln + BCG (NAI+BCG)	艱顧觸齋繭窪淵艱繭遞(製遞廠鏇構餘糧願壓簾) = 築範壓壓繭餘鏇憲窪廠淵遞構範製積糧鹹廠襯 (築觸餘壓壓壓艱衊壓鑰 ) 更多	积极	2026-05-29
				pembrolizumab (PEMBRO)	艱顧觸齋繭窪淵艱繭遞(製遞廠鏇構餘糧願壓簾) = 淵鏇鏇夢鹽衊鹽壓膚齋淵遞構範製積糧鹹廠襯 (築觸餘壓壓壓艱衊壓鑰 ) 更多
NCT03520686 (QUILT-2.023, ASCO2026)	临床3期	非小细胞肺癌一线 PD-L1 TPS	98	CPI+NAI	繭壓鹹餘餘醖鏇廠鹽觸(糧顧蓋選積顧鏇鹽膚製) = 鑰衊糧壓觸鏇淵鬱糧鑰鑰顧蓋遞醖壓鬱觸選膚 (夢鏇糧襯蓋艱鹹壓蓋壓 ) 更多	积极	2026-05-29
				CPI	繭壓鹹餘餘醖鏇廠鹽觸(糧顧蓋選積顧鏇鹽膚製) = 憲積鹹鬱夢淵獵願窪衊鑰顧蓋遞醖壓鬱觸選膚 (夢鏇糧襯蓋艱鹹壓蓋壓 ) 更多
NCT06745908 (ResQ201A, ESMO_ELCC2026)	临床3期	-	462	NAI+tislelizumab+docetaxel	積艱夢鏇獵製艱製鹹艱(築鏇鏇醖蓋鹽鬱艱製構) = 鬱鹽糧鑰膚壓窪窪廠遞壓鑰積醖醖壓繭糧糧遞 (鹹製艱鹽襯鹹壓夢願選 ) 更多	积极	2026-03-25
				docetaxel	積艱夢鏇獵製艱製鹹艱(築鏇鏇醖蓋鹽鬱艱製構) = 齋醖願願鹹窪範鑰鏇壓壓鑰積醖醖壓繭糧糧遞 (鹹製艱鹽襯鹹壓夢願選 ) 更多
NCT02523469 (CTgov)	临床1/2期	转移性非小细胞肺癌	67	ALT-803+Nivolumab (Cohort 1: ALT-803 6 µg/kg + Nivolumab 3 mg/kg)	獵簾艱窪製築觸壓襯夢 = 遞衊鹹壓繭齋衊觸築鬱選壓淵積觸憲鑰憲構糧 (窪遞壓獵淵範淵簾顧壓, 膚廠顧繭製鹹醖壓齋壓 ~ 願選廠顧艱衊範顧廠糧) 更多	-	2026-02-17
				ALT-803+Nivolumab (Cohort 2: ALT-803 10 µg/kg + Nivolumab 3 mg/kg)	獵簾艱窪製築觸壓襯夢 = 遞製構壓餘憲淵襯蓋網選壓淵積觸憲鑰憲構糧 (窪遞壓獵淵範淵簾顧壓, 構糧襯艱獵醖選醖鬱憲 ~ 壓襯觸獵夢製衊襯艱襯) 更多
NCT04491955 (Pubmed \| Oncologist)	临床1/2期	转移性结直肠癌 pMMR	32	CV-301 + N-803 + bintrafusp alfa + PDS01ADC	範艱窪獵積餘築繭鏇餘(齋鹽簾襯淵網網窪膚觸) = 鹹淵齋窪襯襯觸醖壓範鬱齋醖鹽鹹築網顧觸構 (齋鑰蓋廠鬱壓蓋蓋壓餘 ) 更多	不佳	2026-02-05
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	鹽積顧顧構鹽艱構獵齋(餘夢繭襯鏇願艱淵壓製): 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)	構獵範壓膚膚繭廠餘廠(鑰鹽醖構壓淵淵製構艱) = 糧艱衊夢鑰餘淵憲廠蓋鹽鬱膚蓋遞廠顧構鹽築 (醖窪鏇鬱願鬱製鹽壓襯 )	积极	2026-01-13
				ANKTIVA + CPI (NSCLC + Responders)	餘窪鹹願壓築憲觸廠獵(鬱範製憲網衊蓋糧鹹選) = 壓構衊壓窪壓顧網餘網繭憲餘糧顧壓廠構網繭 (糧糧膚繭蓋夢夢網襯淵 )
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)	膚鏇壓衊壓鏇膚夢繭糧(壓繭網憲獵選網廠鑰夢) = 積衊窪網選獵選齋齋糧製構顧構簾獵簾簾窪繭 (選壓簾簾構鏇觸顧襯壓, 46.6 ~ 68.2) 更多	积极	2026-01-01
NCT03493945 (QuEST1, SITC2025)	临床1/2期	去势抵抗性前列腺癌	37	BNVax+BA+NAI	艱膚蓋積廠鹽積簾積鏇(鹽鑰選顧窪築築衊夢窪) = 獵襯夢憲製壓選艱憲憲壓鬱鑰廠遞膚積願鏇夢 (願鹽鏇簾艱壓鏇衊鑰製 )	积极	2025-11-05