Phase 2 Clinical Trial of Ablation Therapy With Intravesical N-803 In Combination With BCG or Gemcitabine in Participants With Intermediate-Risk Non-Muscle Invasive Papillary Bladder Cancer

This is an open-label, phase 2, randomized study of intravesical N-803 plus BCG (experimental arm A) and intravesical N-803 plus gemcitabine (experimental arm B) in participants who have intermediate-risk Ta/T1 papillary disease. The primary objective of this study is to evaluate the efficacy of these experimental therapies without the need for surgical intervention by CR rate at month 3 or month 6 (for re-inducted participants).

开始日期2025-05-01

申办/合作机构

ImmunityBio, Inc.

NCT06710288

/ Recruiting临床2期

A Phase 2, Open-label, Single-arm Study of Autologous Memory Cytokine Enriched Natural Killer (M-CENK) Adoptive Cell Therapy and N-803 (IL-15 Superagonist) in Combination with Gemcitabine in Participants with Recurrent Platinum-Resistant High-Grade Ovarian Cancer

This is phase 2 single arm study evaluating the safety and preliminary efficacy of M-CENK adoptive cell therapy and fixed dose of N-803 in combination with gemcitabine in participants with platinum-resistant high-grade ovarian cancer (HGOC).Up to 20 participants will receive M-CENK (IV) and N-803 (SC) in combination with gemcitabine (IV).
Participants will undergo an apheresis procedure for the collection of mononuclear cells (MNCs) at least 1 day prior to Cycle 1 for manufacturing of M-CENK. Starting in Cycle 1, participants will receive gemcitabine and starting in Cycle 2 they will also receive M-CENK and N-803, until no additional M-CENK is available or confirmed PD per iRECIST, unless the participant is potentially deriving benefit per Investigator's assessment.
Participants who complete the study treatment or discontinue study treatment will be followed for survival/disease status every 12 weeks (± 2 weeks) for up to 12 months after the last study treatment or until death, lost to follow-up, or withdrawal of consent.

开始日期2025-03-01

申办/合作机构

ImmunityBio, Inc.

NCT05642195

/ Suspended临床1/2期IIT

Phase I/II Evaluation of a Cancer Lysate Vaccine and Montanide(R) ISA-51 VG With or Without the IL-15 Super-Agonist N-803 as Adjuvant Therapy for PD-L1 Negative Non-Small Cell Lung Cancer

Background:
Surgery is the primary treatment for non-small cell lung cancer (NSCLC) that is diagnosed in its earlier stages. But the tumors often return. Radiation and chemotherapy can improve survival in some people who have had surgery for NSCLC, but these treatments also cause serious side effects. A new approach, called immunotherapy, may be a better way to stop NSCLC tumors from coming back.
Objective:
To test a new treatment (H1299 lung cancer cell vaccine combined with the drug N-803) in people who received surgery for NSCLC.
Eligibility:
Adults aged 18 years or older with no sign of disease after surgery for NSCLC.
Design:
Participants will be screened. They will have a physical exam with blood tests. They will have tests of their heart and lung function. They will have imaging scans.
Study treatment will be given in 28-day cycles. Participants will visit the clinic on the first day of each cycle. They will receive 2 treatments at each visit:
The study vaccine is given as 2-4 small shots under the skin of the thigh or arm.
N-803 is given as a shot under the skin of the abdomen.
Treatment will continue for 6 cycles. Blood tests and imaging scans will be repeated throughout the study.
Participants will have a blood test 1 month after receiving the 6th vaccine. Some participants may then resume taking N-803; they may also receive 2 more vaccinations at 3 and 6 months after their previous treatment.
Follow-up visits will continue for up to 5 years.

开始日期2025-02-26

申办/合作机构

National Cancer Institute

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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项与诺格白介素α-因奇西普相关的文献（医药）

2024-12-01·European Urology Oncology

Novel Delivery Systems and Pharmacotherapeutic Approaches for the Treatment of Non–muscle-invasive Bladder Cancer

Review

作者: Daneshmand, Siamak ; Boormans, Joost L ; Guerrero-Ramos, Félix ; Shariat, Shahrokh F ; Vilaseca, Antoni ; Rouprêt, Morgan ; Kamat, Ashish M ; Gontero, Paolo

BACKGROUND AND OBJECTIVE:

Therapeutic options for patients with non-muscle-invasive bladder cancer (NMIBC) have traditionally been limited to intravesical immunotherapy or chemotherapy. A considerable number of new options have been investigated in recent years. Our aim was to review the efficacy and toxicity of novel therapeutic options (results already reported or currently under investigation) for patients with NMIBC.

METHODS:

We assessed the efficacy of various novel therapeutic options by examining key endpoints in diverse settings, including recurrence, progression, overall survival, disease-specific survival, and complete response. We identified the principal advantages and limitations for each option. Safety was predominantly evaluated as the incidence of grade ≥3 adverse events. Our investigation focused on evidence from scientific articles and congress abstracts published in English within the past 5 yr.

KEY FINDINGS AND LIMITATIONS:

To date, pembrolizumab, nadofaragene firadenovec, and the combination of BCG with N-803 have received US Food and Drug administration approval for the treatment of BCG-unresponsive carcinoma in situ of the bladder (with or without papillary tumours). Five phase 3 trials are recruiting BCG-naïve patients with high-risk NMIBC. There is increasing interest in an ablative rather than an adjuvant approach for patients with intermediate-risk NMIBC.

CONCLUSIONS AND CLINICAL IMPLICATIONS:

Novel drugs and device-assisted drug delivery systems are on the verge of changing the treatment of NMIBC. Novel intravesical options seem to have the same efficacy with fewer adverse events in comparison to systemic therapies.

PATIENT SUMMARY:

We reviewed new therapy options for non-muscle-invasive bladder cancer. Two agents (pembrolizumab and nadofaragene firadenovec) have been approved to date. Ongoing trials are assessing direct delivery of drugs in solution into the bladder. This route seems to have similar efficacy and fewer side effects than intravenous immunotherapy.

2024-12-01·EUROPEAN UROLOGY

Bladder-sparing Therapy for Bacillus Calmette-Guérin–unresponsive Non–muscle-invasive Bladder Cancer: International Bladder Cancer Group Recommendations for Optimal Sequencing and Patient Selection

Review

作者: Palou, Joan ; Hensley, Patrick J ; Mariappan, Paramananthan ; Tan, Wei Shen ; Svatek, Robert S ; Ross, Jeffrey S ; Mertens, Laura S ; Guo, Charles C ; Fernández, Mario I ; Bree, Kelly K ; Babjuk, Marko ; Lamm, Donald L ; Horowitz, Amir ; Taoka, Rikiya ; Spiess, Philippe E ; Mir, Carmen ; Buckley, Roger ; O'Donnell, Michael ; Li, Roger ; Kamat, Ashish M ; Pohar, Kamal ; Al-Ahmadie, Hikmat ; Lotan, Yair ; McConkey, David ; Soloway, Mark ; Lerner, Seth P ; Black, Peter C ; Gupta, Shilpa ; Brausi, Maurizio ; Steinberg, Gary

BACKGROUND AND OBJECTIVE:

There has been a recent surge in the development of agents for bacillus Calmette-Guérin-unresponsive (BCG-U) non-muscle-invasive bladder cancer (NMIBC). Critical assessment of these agents and practical recommendations for optimal selection of patients and therapies are urgently needed, especially in the absence of randomized trials on bladder-sparing treatment (BST) options.

METHODS:

A global committee of bladder cancer experts was assembled to develop recommendations on BST for BCG-U NMIBC. Working groups reviewed the literature and developed draft recommendations, which were then voted on by International Bladder Cancer Group (IBCG) members using a modified Delphi process. During a live meeting in August 2023, voting results and supporting evidence were presented, and recommendations were refined on the basis of meeting discussions. Final recommendations achieved >75% agreement during the meeting, and some were further refined via web conferences and e-mail discussions.

KEY FINDINGS AND LIMITATIONS:

There is currently no single optimal agent for patients with BCG-U disease who seek to avoid radical cystectomy (RC). BST selection should be personalized, taking into account individual patient characteristics and preferences, tumor attributes, and efficacy/toxicity data for the agents available. For patients with BCG-U carcinoma in situ (CIS), gemcitabine/docetaxel (GEM/DOCE), nadofaragene firadenovec (NFF), and nogapendekin alfa inbakicept-pmln (NAI) + BCG are recommended; because of its systemic toxicity, pembrolizumab should only be offered after other options are exhausted. For patients with BCG-U papillary-only tumors, GEM/DOCE, NFF, NAI + BCG, single-agent chemotherapy, hyperthermic mitomycin C, and pembrolizumab are recommended. Given the modest efficacy of available options, clinical trial participation is encouraged. For unapproved agents with reported data, IBCG recommendations await the final results of pivotal trials.

CONCLUSIONS AND CLINICAL IMPLICATIONS:

The IBCG consensus recommendations provide practical guidance on BST for BCG-U NMIBC.

2024-12-01·Transplantation and Cellular Therapy

N-803, an IL-15 Superagonist Complex as Maintenance Therapy After Allogeneic Donor Stem Cell Transplant for Acute Myeloid Leukemia or Myelodysplastic Syndrome; A Phase 2 Trial

Article

作者: Juckett, Mark ; Miller, Jeffrey S ; Rashid, Faridullah ; Maakaron, Joseph ; Shanley, Ryan ; Wangen, Rose ; Weisdorf, Daniel ; Merino, Aimee ; Brunstein, Claudio C ; Bachanova, Veronika ; Felices, Martin

Maintenance therapy may improve natural killer (NK) cell surveillance after allogeneic donor hematopoietic cell transplant (HCT) for myeloid malignancies and represents a potential approach to improve cure rates. Interleukin-15 (IL-15) enhances lymphocyte proliferation and antitumor activity. In a prior Phase 1 study of an IL-15 superagonist (N-803) in patients with AML who relapsed after HCT, we observed in vivo expansion of NK cells and antitumor responses. The primary objective of this Phase 2 trial was to determine if post-transplant N-803 could reduce relapse. We administered N-803 (n = 20) (dosed 6 mcg/kg subcutaneously [SQ] at day 60 after HCT to patients with myelodysplastic syndrome [MDS] or acute myeloid leukemia [AML] who were in complete remission [CR]). N-803 treatment was planned weekly, biweekly or every 4 weeks in 2 sequential cohorts. The most common adverse events after administration were self-limited injection sites skin rashes (n = 20). One week after an N-803 dose, we observed enhanced NK cell proliferation and improved antitumor cytotoxicity without inducing immune exhaustion. Five patients who developed acute graft versus host disease (aGVHD) after N-803 responded promptly to steroids and 4 patients developed chronic GVHD. Patients receiving >4 doses of N-803 had a 3-fold decrease in relapse at two years (P = .06). These findings support the safety, immune activation, and potential efficacy of N-803 to prevent relapse of AML/MDS after HSCT.

186

项与诺格白介素α-因奇西普相关的新闻（医药）

2025-02-20

·Pharmaceutical Technology

FDA authorises ImmunityBio’s BCG alternative to treat bladder cancer

The company holds several patents for the composition and use of BCG combined with Anktiva in bladder cancer treatment. Credit: SaiArLawKa2/Shutterstock. ImmunityBio has gained US Food and Drug Administration (FDA) authorisation for an expanded access programme to supply an alternative source of Bacillus Calmette-Guerin (BCG) to treat bladder cancer. The development comes in response to significant supply shortages of Tice BCG [an attenuated, live culture preparation of the BCG strain of Mycobacterium bovis] which have been a major barrier to treatment. In a survey of US urologists by Sermo, more than half reported an inability to treat subjects in the past 12 months due to the lack of access to Tice BCG. The Serum Institute of India-developed alternative BCG (rBCG) source has shown promising outcomes in European clinical trials, demonstrating potent immunogenicity with cluster of differentiation 8+ (CD8+) and CD4+ T cell stimulation and enhanced safety compared to previous BCG strains and formulations. ImmunityBio founder, executive chairman and global chief scientific and medical officer Dr Patrick Soon-Shiong stated: “Our collaboration with the FDA and Serum Institute to ensure a reliable supply of this vital drug for bladder cancer patients underscores ImmunityBio’s commitment to addressing critical access issues that affect so many patients.” In May 2024, ImmunityBio entered an exclusive global agreement with the Serum Institute of India to obtain a supply of the BCG vaccine for all types of cancer. The company holds several patents for the composition and use of BCG combined with Anktiva in bladder cancer treatment. The rBCG vaccine, originally developed as a live vaccine against tuberculosis (TB), has been used since 1921 and administered to more than four billion individuals globally. For non-muscle invasive bladder cancer (NMIBC) patients, BCG has been the standard of care since 1977, inducing an immune response that can lead to cancer clearance. The rBCG has undergone genetic modifications to enhance its immunogenicity and safety. It has completed Phase I/II human trials in Europe as an immunotherapy for NMIBC subjects, showing a safety profile similar to placebo and reduced adverse events.

疫苗免疫疗法上市批准临床研究

2025-02-13

·Business Wire

ImmunityBio Announces UK Medicines and Healthcare Products Regulatory Agency Accepted Marketing Authorization Application for ANKTIVA® for the Treatment of Patients with BCG-unresponsive Non-Muscle Invasive Bladder Cancer Carcinoma In Situ

CULVER CITY, Calif.--( BUSINESS WIRE )--ImmunityBio, Inc. ( NASDAQ: IBRX ), a leading immunity therapy company, today announced the Medicines and Healthcare products Regulatory Agency (MHRA) has validated and accepted the marketing authorization application for ANKTIVA. The MHRA will now begin assessing the marketing authorization application (MAA) for ANKTIVA ® (nogapendekin alfa inbakicept-pmln) in combination with bacillus Calmette-Guérin (BCG) for the treatment of patients with BCG-unresponsive non-muscle invasive bladder cancer (NMIBC) with carcinoma in situ (CIS), with or without papillary tumors. MHRA regulates medicines, medical devices and blood components for transfusion in the UK. “MHRA’s acceptance of our marketing authorization application for the UK comes less than three weeks after the European Medicines Agency accepted for review our MAA for the 30 countries covering the European Union, and just 10 months after FDA approval in the United States,” said Dr. Patrick Soon-Shiong, Founder, Executive Chairman and Global Chief Scientific and Medical Officer of ImmunityBio. “We are determined to reach as many patients as possible with ANKTIVA and BCG and are encouraged by the momentum of our efforts.” About ANKTIVA ® The cytokine interleukin-15 (IL-15) 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 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 drives the activation and proliferation of NK cells with the generation of memory killer T cells that have retained immune memory against these tumor clones. The proliferation of the trifecta of these immune killing cells and the activation of trained immune memory results in immunogenic cell death, inducing a state of equilibrium with durable complete responses. ANKTIVA has improved pharmacokinetic properties, longer persistence in lymphoid tissues, and enhanced anti-tumor activity compared to native, non-complexed IL-15 in-vivo. ANKTIVA was approved by the FDA in 2024 for BCG-unresponsive non-muscle invasive bladder cancer CIS with or without papillary tumors. For more information, visit ImmunityBio.com (Founder’s Vision) and Anktiva.com. About ImmunityBio ImmunityBio is a vertically-integrated biotechnology company developing next-generation therapies and vaccines that bolster the natural immune system to defeat cancers and infectious diseases. The Company’s range of immunotherapy and cell therapy platforms, alone and together, act to drive and sustain an immune response with the goal of creating durable and safe protection against disease. Designated an FDA Breakthrough Therapy, ANKTIVA is the first FDA-approved immunotherapy for non-muscle invasive bladder cancer CIS that activates natural killer cells, T cells, and memory T cells for a long-duration response. The Company is applying its science and platforms to treating cancers, including the development of potential cancer vaccines, as well as developing immunotherapies and cell therapies that we believe sharply reduce or eliminate the need for standard high-dose chemotherapy. These platforms and their associated product candidates are designed to be more effective, accessible, and easily administered than current standards of care in oncology and infectious diseases. For more information, visit ImmunityBio.com (Founder’s Vision) 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, such as statements regarding the anticipated timing of the MHRA’s review of ImmunityBio’s MAA and ultimate decision regarding whether to approve ANKTIVA for the treatment of patients with BCG-unresponsive NMIBC CIS in the territory under its jurisdiction, additional regulatory submissions and timing thereof, global expansion efforts, clinical trial data and potential results to be drawn therefrom, the development of therapeutics for cancer and infectious diseases, potential benefits to patients, potential treatment outcomes for patients, the described mechanism of action and results and contributions therefrom, potential future uses and applications of ANKTIVA and use in cancer vaccines and across multiple tumor types, and ImmunityBio’s approved product and investigational agents as compared to existing treatment options, among others. Statements in this press release that are not statements of historical fact are considered forward-looking statements, which are usually identified by the use of words such as “anticipates,” “believes,” “continues,” “goal,” “could,” “estimates,” “scheduled,” “expects,” “intends,” “may,” “plans,” “potential,” “predicts,” “indicate,” “projects,” “is,” “seeks,” “should,” “will,” “strategy,” and variations of such words or similar expressions. Statements of past performance, efforts, or results of our preclinical and clinical trials, about which inferences or assumptions may be made, can also be forward-looking statements and are not indicative of future performance or results. Forward-looking statements are neither forecasts, promises nor guarantees, and are based on the current beliefs of ImmunityBio’s management as well as assumptions made by and information currently available to ImmunityBio. Such information may be limited or incomplete, and ImmunityBio’s statements should not be read to indicate that it has conducted a thorough inquiry into, or review of, all potentially available relevant information. Such statements reflect the current views of ImmunityBio with respect to future events and are subject to known and unknown risks, including business, regulatory, economic and competitive risks, uncertainties, contingencies and assumptions about ImmunityBio, including, without limitation, (i) risks and uncertainties regarding the MHRA regulatory review process, potential actions required in connection with the same, and whether or not the MHRA will ultimately approve ImmunityBio’s MAA that has been accepted for review, (ii) risks and uncertainties regarding commercial launch execution, success and timing, (iii) risks and uncertainties related to the regulatory submission, filing and review process and the timing thereof, (iv) the ability of ImmunityBio to fund its ongoing and anticipated clinical trials, (v) whether clinical trials will result in registrational pathways, (vi) whether clinical trial data will be accepted by regulatory agencies, (vii) the ability of ImmunityBio to continue its planned preclinical and clinical development of its development programs through itself and/or its investigators, and the timing and success of any such continued preclinical and clinical development, patient enrollment and planned regulatory submissions, (viii) potential delays in product availability and regulatory approvals, (ix) ImmunityBio’s ability to retain and hire key personnel, (x) ImmunityBio’s ability to obtain additional financing to fund its operations and complete the development and commercialization of its various product candidates, (xi) potential product shortages or manufacturing disruptions that may impact the availability and timing of product, (xii) ImmunityBio’s ability to successfully commercialize its approved product and product candidates, (xiii) ImmunityBio’s ability to scale its manufacturing and commercial supply operations for its approved product and future approved products, and (xiv) ImmunityBio’s ability to obtain, maintain, protect, and enforce patent protection and other proprietary rights for its product candidates and technologies. 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 March 19, 2024 and the Company’s Form 10-Q filed with the SEC on November 12, 2024, and in subsequent filings made by ImmunityBio with the SEC, which are available on the SEC’s website at www.sec.gov . 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. Indication and Important Safety Information INDICATION AND USAGE: ANKTIVA is an interleukin-15 (IL-15) receptor agonist indicated with Bacillus Calmette-Guerin (BCG) for the treatment of adult patients with BCG-unresponsive non-muscle invasive bladder cancer (NMIBC) with carcinoma in situ (CIS) with or without papillary tumors. WARNINGS AND PRECAUTIONS: Risk of Metastatic Bladder Cancer with Delayed Cystectomy. Delaying cystectomy can lead to the development of muscle invasive or metastatic bladder cancer, which can be lethal. If patient with CIS do not have a complete response to treatment after a second induction course of ANKTIVA with BCG, reconsider cystectomy. DOSAGE AND ADMINISTRATION: For lntravesical Use Only. Do not administer by subcutaneous or intravenous routes. Instill intravesically only after dilution. Total time from vial puncture to the completion of the intravesical instillation should not exceed 2 hours. USE IN SPECIFIC POPULATIONS: Pregnancy: May cause fetal harm. Advise females of reproductive potential of the potential risk to a fetus and to use effective contraception. ADVERSE REACTIONS: The most common (≥15%) adverse reactions, including laboratory test abnormalities, are increased creatinine, dysuria, hematuria, urinary frequency, micturition urgency, urinary tract infection, increased potassium, musculoskeletal pain, chills and pyrexia. For more information about ANKTIVA, please see the Full Prescribing Information at www.anktiva.com . You are encouraged to report negative side effects of prescription drugs to FDA. Visit www.FDA.gov/medwatch or call 1-800-332-1088. You may also contact lmmunityBio at 1-877-ANKTIVA (1-877-265-8482).

免疫疗法上市批准突破性疗法

2025-01-30

·药智网

强生猛攻膀胱癌

近期，强生宣布已向FDA提交TAR-200的新药申请，用于对卡介苗治疗无反应的高风险非肌层浸润性膀胱癌伴原位癌（可伴或不伴乳头状肿瘤）患者。此前，强生在膀胱癌领域还有一个更大的突破，其泛FGFR抑制剂厄达替尼（Erdafitinib）正式获NMPA批准，用于治疗携带易感型FGFR3基因变异，且既往接受至少一线含抗PD-1或抗PD-L1期间或之后出现疾病进展的手术不可切除的局部晚期或转移性尿路上皮癌（UC）成人患者。长期深耕男性泌尿肿瘤的强生，在前列腺癌领域凭借阿比特龙和阿帕他胺两款重磅产品牢牢占据了前列腺癌市场领先地位。如今，又强势入局膀胱癌领域，有意巩固其泌尿肿瘤霸主地位的野心昭然。 1 新颖的药物形式 TAR-200最初由Taris Biomedical公司开发，强生于2019年底收购了这家公司。该公司致力于开发用于治疗包括膀胱癌在内的泌尿系统疾病的新型药物递送技术，自主研发了TARIS系统。TARIS系统是一种基于硅酮的药物输送装置，可使用微创方法植入体内并从膀胱中取出。这个系统可以将药物直接释放到膀胱肿瘤，评估针对膀胱癌和其他类型癌症患者的新型局部治疗方法。膀胱癌基因容易激活突变，异常基因型的长期积累会导致恶性表型的出现。TARIS系统以一种量身定制的方法提供联合治疗，可以治疗多种膀胱癌类型。 TAR-200是第一个也是唯一个针对膀胱癌的膀胱内药物释放系统，可以通过一根5厘米长的硅胶管，利用其渗透性将化疗药吉西他滨持续、可控地释放到膀胱中，与传统的2小时膀胱灌注时间相比，它可以实现连续几周到几个月向膀胱输送药物。吉西他滨是膀胱癌化疗的首选药物。图片来源：EtudeImpromptu ImpromptuThoughts 作为一种新的膀胱内递送系统，TAR-200能够使肿瘤持续暴露于药物中，并且对比其他化疗或其他药物，TAR-200使肿瘤暴露于药物的总时间更长。同时，TAR-200通过局部给药产生的疗效强大，与标准吉西他滨膀胱内灌注相比，TAR-200的给药剂量明显较低，还不易发生常规化疗导致的患者全身性药物暴露，能够大幅降低毒副作用。此外，比较方便的是，TAR-200易于安装，安装过程仅需3～5分钟，无需麻醉即可完成。这一创新膀胱内药物释放系统的提交，得到了来自2b期SunRISe-1注册研究的数据支持，已在2024 ESMO年会上作为临时口头报告呈现。TAR-200单药治疗显示出83.5%的完全缓解率（CR），并且CR具有高度耐久性，无需重新诱导治疗——在中位随访9个月时，82%的反应者维持了反应。这个数据目前看起来是所有HR-NMIBC在研产品里面单药CR率最高的。 2 竞争进入白热化膀胱癌作为全球高发的恶性肿瘤之一，分为非肌层浸润性膀胱癌（NMIBC，占70%）和肌层浸润性膀胱癌（MIBC，占30%）两大类。非肌层浸润性膀胱癌包括膀胱的原位癌、非浸润性乳头状癌，以及侵犯上皮下结缔的膀胱癌，肌层浸润性膀胱癌是指侵犯浅肌层以上的膀胱癌。 NMIBC是早期阶段膀胱癌，肿瘤的浸润深度尚未超过尿路壁的浅表层。同时，NMIBC也是最常见的膀胱癌类型，约占膀胱肿瘤新发病例的75%。根据弗若斯特沙利文分析，中国NMIBC市场规模在2015-2019年的复合年增长率为14.4%，中国NMIBC市场将继续保持增长，预计于2024年达到26亿元，2030年预计达到88亿元。 NMIBC的标准治疗方式是经尿道膀胱肿瘤切除术（TURBT），微创手术之后临床指南推荐化疗灌注和卡介苗（BCG）膀胱灌注作为辅助治疗，但仍有部分患者对BCG治疗无反应，约50%的患者在5年内发生肿瘤复发。传统上针对复发患者是采用根治性膀胱切除术，但该项手术会使患者失去正常的储尿和排尿功能，严重影响患者的生活质量。因此，对于化疗和BCG无应答NMIBC患者而言，二线治疗的新药研发十分关键。截至目前，全球仅批准三款可用于NMIBC患者的二线疗法，分别是默沙东的K药、Ferring Pharmaceuticals的Adstiladrin和去年4月份刚获得FDA批准的ImmunityBio的Anktiva。不过从其获批适应症上来看，K药以及Adstiladrin仅限于原位癌（CIS），其在NMIBC中占比仅有10%，意味着目前现有获批的二线疗法覆盖的患者群体始终有限。 2024年，可以说是NMIBC治疗领域加速突破的一年。 4月，Anktiva作为ImmunityBio推出的首个基于IL-15的免疫疗法治疗NMIBC，获得了FDA的批准。 8月，UroGen Pharma宣布其丝裂霉素灌注疗法UGN-102已向FDA提交了NDA，用以治疗低级别中等风险非肌层浸润性膀胱癌（LG-IR-NMIBC）患者。试验中，首次使用UGN-102的患者在三个月后，接近80%的人实现了肿瘤完全消失，且12个月后82.3%的患者依然维持无瘤状态。 12月，Protara Therapeutics宣布，其试验性细胞疗法在六个月内对18名对携带高风险原位癌的NMIBC患者的CR率高达72%，在这项积极数据的推动下，公司股价从3.54美元飙升至6.76美元，暴涨119%。同样在12月份，CG Oncology公布了其溶瘤病毒疗法Cretostimogene用于治疗对BCG无应答的高风险NMIBC患者的3期BOND-003试验的主要结果。接受Cretostimogene（CG0070）单药治疗后，近75%的患者在任何时间点达成完全缓解（CR），已计划在2025年下半年向FDA提交上市申请。值得一提的是，2019年，乐普生物获得Cretostimogene（CG0070）中国内地、香港和澳门的开发和商业化权益，目前正在国内开展单药治疗NMIBC临床试验。而国内进展最快的，则是亚虹医药的全球首个进入关键性3期临床试验的NMIBC口服可逆性MetAP2抑制剂APL-1202。在该药物二线NMIBC适应症折戟后，目前正在开展APL-1202另外两项临床试验，分别为APL-1202单药治疗未经治疗的中、危NMIBC的3期临床试验（一线NMIBC适应症）以及APL-1202口服联合PD-1替雷利珠单抗作为MIBC新辅助治疗的2期临床试验。在接二连三的突破性进展之下，NMIBC领域的竞争将愈发激烈。因此对于强生而言，从NMIBC到MIBC深入布局膀胱癌全程化诊疗是其必由之路，目前也初见成效。以TAR-200为例，除了此次提交NDA的单药治疗NMIBC适应症外，强生还设计了一系列研究探索TAR-200单药或联合Cetrelimab（PD-1单抗）治疗NMIBC和MIBC的安全性和有效性，这些研究大都已进行到2/3期，展示出优秀的临床应用前景。此外，强生还有意将厄达替尼拓展到NMIBC领域。厄达替尼虽然在NMIBC患者中显示出了疗效，但全身给药的副作用很大。利用TARIS系统强生如法炮制以膀胱内药物输送系统将厄达替尼在较长时间内、以非常低的剂量持续局部释放到膀胱（TAR-210），完美解决了全身毒性的问题。根据在2024年美国泌尿外科协会年会上报告的一项1期研究的结果显示：TAR-210对具有FGFR基因突变的高风险和中风险非肌层浸润性膀胱癌（NMIBC）患者显示出非常积极的临床活性。在队列1中，90%的患者在12个月时无复发，中位随访时间为8.9个月；在队列3中，31名患者的反应可评估，CR率90%。参考来源 1.https://www.onclive.com/view/fda-approval-sought-for-tar-200-in-bcg-unresponsive-high-risk-nmibc-with-cis. 2.https://www.investor.jnj.com/news/news-details/2025/New-Drug-Application-initiated-with-U.S.-FDA-for-TAR-200-the-first-and-only-intravesical-drug-releasing-system-for-patients-with-BCG-unresponsive-high-risk-non-muscle-invasive-bladder-cancer/default.aspx. 友情推荐：医药行业深度技术内容，点击“博药”查看详情~ 声明：本内容仅用作医药行业信息传播，为作者独立观点，不代表药智网立场。如需转载，请务必注明文章作者和来源。对本文有异议或投诉，请联系maxuelian@yaozh.com。责任编辑 | 史蒂文合作、投稿、转载开白 | 马老师 18323856316（同微信）阅读原文，是受欢迎的文章哦

临床结果并购临床2期

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
非肌层浸润性膀胱肿瘤	美国	Altor BioScience Corp.	2024-04-22

未上市

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适应症	最高研发状态	国家/地区	公司	日期
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
铂耐药性卵巢癌	临床2期	美国	ImmunityBio, Inc.	2025-03-01
复发性铂耐药性卵巢癌	临床2期	美国	ImmunityBio, Inc.	2025-03-01
前列腺癌	临床2期	-	ImmunityBio, Inc.	2025-01-31
胶质母细胞瘤	临床2期	美国	ImmunityBio, Inc.	2024-08-07
头颈癌转移	临床2期	美国	ImmunityBio, Inc.	2024-02-16
复发性头颈癌	临床2期	美国	ImmunityBio, Inc.	2024-02-16
复发性头颈部鳞状细胞癌	临床2期	美国	ImmunityBio, Inc.	2024-02-16
转移性头颈部鳞状细胞癌	临床2期	美国	ImmunityBio, Inc.	2024-02-16

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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


NCT03563157 (CTgov)	临床1/2期	转移性结直肠癌	2	SBRT+Aldoxorubicin Hydrochloride+GI-6301+GI-4000+ETBX-061+Cetuximab+ETBX-051+Leucovorin+ETBX-011+5-Fluorouracil+ALT-803+ETBX-021+nab-paclitaxel+CYCLOPHOSPHAMIDE+Avelumab+haNK+GI-6207+Regorafenib+Oxaliplatin+Capecitabine (NANT Colorectal Cancer (CRC) Vaccine)	齋網選憲網廠蓋壓鑰憲(淵糧鹽網遞襯願壓憲鑰) = 齋壓獵鹹鹹壓獵選齋壓淵窪網鹽範壓繭鏇構襯 (構艱醖構製齋壓膚夢選, 淵網鬱鑰築憲簾夢願膚 ~ 憲鬱夢築積願網鑰鬱獵) 更多	-	2024-12-11
				Regorafenib (Regorafenib)	齋選鹽鹽艱觸繭壓襯鹹(選獵淵鹹壓鏇鏇夢繭膚) = 淵鹹鏇餘蓋鑰襯襯餘艱鹽獵夢齋鏇築繭齋醖願 (願範願窪顧築膚觸艱淵, 顧觸選網夢膚鏇膚繭醖 ~ 網範願製鑰壓觸襯顧衊) 更多
NCT02099539 (CTgov)	临床1期	复发性多发性骨髓瘤 \| 难治性多发性骨髓瘤	19	N-803 (Cohort 1: N-803 - IV 1 ug/kg)	選衊顧窪鏇壓積衊遞構(範廠簾憲艱襯憲繭艱衊) = 夢膚廠獵餘簾膚夢衊積願壓築鏇網壓齋簾憲築 (齋淵襯餘齋淵窪鹹膚願, 艱遞繭糧醖鹹壓繭範遞 ~ 築選艱膚夢選齋衊廠鑰) 更多	-	2024-09-26
				N-803 (Cohort 2: N-803 - IV 3 ug/kg)	選衊顧窪鏇壓積衊遞構(範廠簾憲艱襯憲繭艱衊) = 獵鑰鬱窪製網鹹繭鏇艱願壓築鏇網壓齋簾憲築 (齋淵襯餘齋淵窪鹹膚願, 獵壓獵獵鬱窪鏇糧艱積 ~ 夢窪積衊窪壓遞網膚構) 更多
NCT03493945 (QuEST1, ESMO2024)	临床1/2期	去势抵抗性前列腺癌 dMMR \| pMMR	25	BNVax + BA + Anktiva	選淵選願選顧觸淵願襯(糧淵繭範鏇鹹願選壓鏇) = 觸鬱顧壓構構鏇網襯襯糧蓋鏇膚遞膚範獵觸艱 (遞夢憲遞顧構艱築選遞, 39.9 ~ 83.9) 更多	积极	2024-09-15
NCT03228667 (QUILT 3.055, WCLC2024) 人工标引	临床2期	非小细胞肺癌二线 \| 末线 \| 三线 PDL1+	86	Anktiva 15mcg/knivolumabvolupembrolizumab	網膚艱窪糧鹹壓膚齋夢(範顧願遞構網夢鑰醖鹽) = injection site reaction 78 (91%), fatigue 46 (53%), chills 36 (42%). 積壓壓遞衊醖齋襯廠鏇 (網淵窪構齋餘觸鏇製觸 )	积极	2024-09-08
				Anktiva + CPI (nivolumab or pembrolizumab)pembrolizumab) (failure of CPI + 3rd line)
NCT04385849 (CTgov)	临床1期	新型冠状病毒感染	1	N-803 (Experimental Arm)	顧簾艱鹹簾糧餘鹹衊觸(窪衊夢鏇積憲膚淵鏇鏇) = 憲鬱願醖構鹽積糧獵築製衊鹽膚蓋顧鬱蓋構網 (壓網遞選膚鹹觸壓壓壓, 鹽膚膚鹹繭衊網獵壓襯 ~ 艱構構願蓋觸選製積繭) 更多	-	2024-09-05
				Saline (Placebo Arm)	顧簾艱鹹簾糧餘鹹衊觸(窪衊夢鏇積憲膚淵鏇鏇) = 願糧糧製製範簾鏇糧願製衊鹽膚蓋顧鬱蓋構網 (壓網遞選膚鹹觸壓壓壓, 壓鬱繭構窪遞艱壓築夢 ~ 鏇製蓋觸窪獵範醖範夢) 更多
NCT03853317 (QUILT-3.063, CTgov)	临床2期	转移性Merkel细胞癌 \| 梅克尔细胞癌	9	N-803+Avelumab+haNK™	糧鏇醖顧選構鑰鬱餘製(簾願網遞衊願鹹鏇鏇膚) = 選憲襯膚壓衊鏇蓋憲壓範遞願醖鹽鏇鬱膚艱選 (鹹壓構鑰襯糧顧觸鹹鏇, 鹽夢窪鬱夢範繭艱蓋襯 ~ 淵夢窪鹹壓鹽觸願製鬱) 更多	-	2024-08-09
NCT03127098 (CTgov)	临床1/2期	肺癌 \| 卵巢癌 \| 结肠癌 ... 更多	3	ALT-803+ETBX-011	壓鏇鬱觸鏇積醖選積膚(鏇築鑰糧襯顧夢蓋糧繭) = 構鏇餘餘網襯齋廠糧構糧獵積鬱選觸窪鹽鹽鏇 (窪淵鬱遞網壓選鬱窪壓, 製憲夢願夢窪選醖鹽壓 ~ 夢餘廠淵淵積夢選顧鏇) 更多	-	2024-08-06
NCT02384954 (CTgov)	临床1/2期	难治性惰性非霍奇金淋巴瘤 \| 惰性B细胞非霍奇金淋巴瘤	43	N-803+Rituximab (Phase 1 Cohort 1: N-803 - IV 1 ug/kg)	繭夢夢憲膚鏇鏇範齋製(顧願顧觸蓋窪鏇醖築衊) = 齋獵簾網簾壓艱襯製範夢餘齋鹹構蓋繭觸夢淵 (糧憲選膚齋鹽積糧醖願, 艱壓鏇鏇顧窪鹽觸糧糧 ~ 選醖齋獵積蓋選廠積鏇) 更多	-	2024-07-03
				N-803+Rituximab (Phase 1 Cohort 2: N-803 - IV 3 ug/kg)	繭夢夢憲膚鏇鏇範齋製(顧願顧觸蓋窪鏇醖築衊) = 廠繭膚範鏇鏇繭糧廠範夢餘齋鹹構蓋繭觸夢淵 (糧憲選膚齋鹽積糧醖願, 鹹簾遞選餘鹽構醖窪鏇 ~ 觸衊淵積鑰廠夢築願鏇) 更多
NCT02138734 \| NCT03022825 (Pubmed \| Future Oncol)	N/A	非肌层浸润性膀胱肿瘤	-	N-803 plus BCG	衊衊構選憲鏇鏇糧憲製(襯窪齋構醖築艱構齋鹹) = 鹽齋網壓範齋繭顧鏇簾簾築廠獵鹹鹽糧繭網獵 (壓簾顧鏇鏇襯廠齋憲願 )	积极	2024-07-02
				BCG	衊衊構選憲鏇鏇糧憲製(襯窪齋構醖築艱構齋鹹) = 製觸壓簾鑰製夢簾網壓簾築廠獵鹹鹽糧繭網獵 (壓簾顧鏇鏇襯廠齋憲願 )
NCT03136406 (QUILT-3.039, CTgov)	临床1/2期	胰腺癌	3	avelumab+ALT-803+GI-4000+Nab-paclitaxel+cyclophosphamide+Bevacizumab+Leucovorin+ETBX-011+Oxaliplatin+5-Fluorouracil+Capecitabine	鹹醖構膚衊糧廠獵獵鏇(淵構衊膚選鹹蓋夢鹹獵) = 網醖蓋衊廠鬱鹹壓窪醖簾築積餘選鹹蓋衊顧廠 (夢鑰鹽糧範餘鬱齋淵製, 鬱鏇壓糧構壓觸構選餘 ~ 簾壓範糧膚顧顧觸醖鏇) 更多	-	2024-06-11