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2025-05-08

申办/合作机构

National Cancer Institute

NCT06161545

/ Not yet recruiting临床2期IIT

A Phase II Sequential Window of Opportunity Trial of Pembrolizumab + N-803 Alone or in Combination With PD-L1 t-haNK Cells for Resectable Head and Neck Squamous Cell Carcinoma

Background:
Squamous cell carcinoma is a type of cancer that can cause tumors on the head and neck (HNSCC). Even with treatment, less than 50% of people with certain types of HNSCC survive for 5 years.
Objective:
To test a new drug treatment (N-803 and pembrolizumab, with or without PD-L1 t-haNK cells) in people with HNSCC. These drugs may help the immune system to fight cancer.
Eligibility:
People aged 18 years and older who have HNSCC that is not linked to human papillomavirus infection. They must not yet have received any treatment and be scheduled for surgery to remove the tumors.
Design:
Participants will be screened. They will have a physical exam with blood and urine tests. They will have imaging scans and a test of their heart function. They will have a biopsy: A sample of tissue will be removed from the tumor.
Pembrolizumab is given through a tube attached to a needle inserted into a vein in the arm (intravenous infusion). N-803 is injected under the skin of the abdomen. All participants will receive these 2 treatments on day 1. They will have follow-up visits on days 8 and 15.
Some participants will also receive PD-L1 t-haNK cells by intravenous infusion. These are cells that attack cancer cells. These participants will receive this treatment on days 1, 5, 8, 12, and 15.
All participants will have a clinic visit on day 21. They will have a second biopsy.
Follow-up visits will occur on days 49 and 105. Visits will continue by phone or email every 9 weeks for 2 years....

开始日期2025-05-08

申办/合作机构

National Cancer Institute

NCT06829823

/ Not yet recruiting临床2期

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.

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）

2025-03-10·ONCOLOGIST

Recurrent pancreatic cancer treated with N-803 and PD-L1 t-haNK followed by an EGFR-targeted nanocell drug conjugate

Article

作者: Brahmbhatt, Himanshu ; Nangia, Chaitali ; Seery, Tara ; Sender, Lennie ; Spilman, Patricia ; Moini, Katayoun ; MacDiarmid, Jennifer ; Soon-Shiong, Patrick

Abstract:

Multimodal temporal therapy orchestrated to leverage immunotherapy, tumor-targeted chemotherapy, and natural killer (NK) cell therapy may provide an opportunity to induce immunogenic cell death for tumor response and increased survival in patients with recurrent cancer. The interleukin-15 (IL-15) superagonist N-803, an enhancer of NK cells, CD4 + T cells, cytotoxic CD8 + T cells, and memory T-cell activity, combined with off-the-shelf PD-L1-targeted high-affinity NK (PD-L1 t-haNK) cells represent novel immunotherapies designed to overcome an immunosuppressive tumor microenvironment (TME). The epidermal growth factor receptor-targeted antibody-nanocell conjugate E-EDV-D682 provides tumor-targeted chemotherapy in the form of its anthracycline metabolite PNU159682 (nemorubicin) cargo and is currently being studied in combination with immunomodulatory EDVs delivering the adjuvant α-galactosyl ceramide (GC). Here, we report the compassionate use treatment of this combination in a patient with recurrent, metastatic pancreatic cancer (mPC) after 3 lines of therapy. Under the initial single-patient Investigational New Drug (spIND) protocol, the patient received N-803, PD-L1 t-haNK cells, and the albumin doxorubicin conjugate aldoxorubicin for ~27 months. The patient’s disease became stable on this regimen, and a transient complete response was observed by ~14 months of therapy. Due to progression, a second spIND protocol was designed whereby the patient received E-EDV-D682 plus EDV-GC for more than 24 months, which resulted in stable disease and the patient’s continued survival at the time this report was written. The patient’s extended survival despite the dire prognosis associated with recurrent mPC points to the merits of this temporal combination regimen in overcoming immuno-chemo resistance with enhanced immune activity required for tumor response and extended survival.

2025-02-01·Annals of Medicine and Surgery

Transforming non-muscle invasive bladder cancer (NMIBC) treatment: FDA approval of Anktiva in combination with BCG

作者: Mukhtar, Sameen ; Pokhrel, Prakriti ; Khattak, Aimal Alam ; Javed, Ahmed

2025-02-01·European Urology Oncology

Unmet Need in Non–muscle-invasive Bladder Cancer Failing Bacillus Calmette-Guérin Therapy: A Systematic Review and Cost-effectiveness Analyses from the International Bladder Cancer Group

Review

作者: Burger, Maximilian ; D'Andrea, David ; Masson-Lecomte, Alexandra ; Kamat, Ashish ; Mostafid, Hugh ; Shariat, Shahrokh ; Gontero, Paolo ; Rouprêt, Morgan

BACKGROUND AND OBJECTIVE:

Non-muscle-invasive bladder cancer (NMIBC) poses a significant clinical challenge, particularly when failing bacillus Calmette-Guérin (BCG) therapy, necessitating alternative treatments. Despite radical cystectomy being the recommended treatment, many patients are unfit or unwilling to undergo this invasive procedure, highlighting the need for effective bladder-sparing therapies. This review aims to summarize and report the evidence on the efficacy and to estimate the costs of bladder-preserving strategies used in NMIBC recurrence after failure of intravesical BCG therapy.

METHODS:

We systematically searched online databases for prospective studies investigating intravesical therapy, systemic therapy, or combination of both in patients treated previously with BCG. Owing to significant heterogeneity across the studies, a meta-analysis was inappropriate. A sensitivity analysis was performed in an exploratory manner. We used a decision-analytic Markov model to compare novel U.S. Food and Drug Administration-approved treatments with a 2-yr time horizon.

KEY FINDINGS AND LIMITATIONS:

A total of 57 studies published between 1998 and 2024, with 68 unique study arms and consisting of 2589 patients, were identified. The 3-mo overall response rate (ORR) across all studies, complete response rate (CRR) in concomitant carcinoma in situ (CIS) or CIS only disease, and recurrence-free rate (RFR) in papillary disease were estimated to be 52.4% (95% confidence interval [CI]: 45.4-59.2), 52.8% (95% CI: 42.9-62.6), and 26.4% (95% CI: 13.3-45.6), respectively. The 12-mo ORR, CRR, and RFR were estimated to be 78% (95% CI: 52.9-91.8), 27.8% (95% CI: 21.3-35.4), and 25.4% (95% CI: 18.2-34.2), respectively. The progression rate was estimated to be 13% (95% CI: 9-18.2). The mean proportion of patients treated with radical cystectomy was estimated to be 24.7 (range 0-85.7). The reported toxicity grades were overall mild, with a median of 3.4% (range 0-33.3%) participants experiencing a dose limiting toxicity. Compared with using radical cystectomy to treat patients failing BCG therapy, at a willingness-to-pay threshold of 100 000 USD, nadofaragene firadenovec was cost effective, with an incremental cost-effectiveness ratio (ICER) of 10 014 USD per quality-adjusted life year (QALY), while nogapendekin alfa inbakicept was less cost effective than nadofaragene firadenovec (ICER of 44 602 USD per QALY). Pembrolizumab, which dominated, was both less costly and more effective than the other strategies.

CONCLUSIONS AND CLINICAL IMPLICATIONS:

Salvage bladder-sparing therapies show a response rate of around 50% at 3 mo in patients with NMIBC failing BCG. However, long-term data are heterogeneous. Nevertheless, recently developed agents show promising tumor control activity. In the rapidly evolving landscape of urothelial cancer, some of these treatment strategies might be cost effective and improve patients' quality of life. The findings of our review highlight the need for novel, more effective therapeutic strategies.

PATIENT SUMMARY:

In this study, we reviewed the evidence on the efficacy of bladder-preserving strategies used in patients with bladder cancer recurrence after failing bacillus Calmette-Guérin (BCG) therapy. We found that these strategies show a response rate of around 50% at 3 mo. However, long-term data are heterogeneous. Nevertheless, recently developed agents show promising tumor control activity. In the rapidly evolving landscape of urothelial cancer, some of these treatment strategies might be cost effective and improve patients' quality of life.

209

项与诺格白介素α-因奇西普相关的新闻（医药）

2025-04-23

·小药说药

CD16a生物学与ADCC作用

-01-引言抗体依赖性细胞介导的细胞毒性（ADCC）是一种有效的细胞毒性机制，主要通过自然杀伤（NK）细胞介导。当特异性抗体结合到靶向细胞膜上以后，免疫细胞通过该反应诱导细胞死亡。这是抗体限制和控制感染的几种主要机制之一。抗体和免疫细胞的相互作用通过一个受体家族发生：Fc受体（FcR）。在人类中，IgG的FcR家族（FcγR）由6个受体组成：FcγRI/CD64、FcγRIIa/CD32a、FcγRIIb/CD32b、FcγRIIc/CD32c、FcγRIIIa/CD16a和FcγRIIIb/CD16b，其中CD16a主要负责触发NK细胞介导的ADCC。因此，对CD16a作用机制的了解，有助于我们通过改善单克隆抗体或NK细胞来增强肿瘤免疫治疗药物的ADCC作用。-02-一、ADCC的作用机制NK细胞是一种天然的淋巴细胞，能够非常有效地破坏应激细胞，如病毒感染或肿瘤转化细胞。通常情况下，ADCC效应主要通过结合FCR的抗体激活NK细胞，NK细胞膜上最具特征的FcR就是FcγRIII（CD16），其中NK细胞主要表达CD16a，而CD16b仅限于中性粒细胞。人类NK细胞分为两个主要亚群：CD56bright和CD56dim。CD56brightNK细胞是强有力的细胞因子产生者，但缺乏CD16a；而CD56dim具有高度的细胞毒性，表达D16a。当通过CD16a识别IgG调理的靶点时，NK细胞就会释放不同的细胞毒性分子，从而引发靶细胞的死亡。这种机制依赖于免疫突触的形成和含有穿孔素和颗粒酶的溶解颗粒的脱颗粒。除了脱颗粒外，NK细胞还可以通过将靶死亡受体（如DR4、DR5或Fas）与其死亡受体配体（如FasL和TRAIL）结合来清除靶细胞。-03- 二、CD16a的生物学CD16a是一种跨膜受体，具有短的C-ter胞质尾，并具有两个细胞外Ig样结构域。它的细胞内部分不具有任何信号成分，因此，为了传递信号，它需要两条带有免疫受体酪氨酸基激活基序（ITAM）的信号链。CD16a与IgG的CH2以1:1的方式相互作用，其中CH2上的N297位的 N-聚糖链在这种相互作用中也起着关键作用。因此，不仅氨基酸序列，其聚糖组成都可以极大地影响CD16a对Fc的亲和力，从而影响ADCC的效力。CD16a在其细胞质尾部不具有任何ITAM结构域，因此需要两条含有ITAM结构域的细胞内链串联的帮助，CD3ζ和FcϵRIγ。CD16a结合后，属于Src家族的激酶Lck被激活，并磷酸化CD3ζ和/或FcϵRIγ的ITAM结构域。磷酸化的ITAM允许来自Syk家族的激酶招募和磷酸化，例如Syk和ZAP-70，它们反过来负责后续的信号传导。在它们的底物中，PI3K是高度相关的，因为它将PIP2转化为PIP3，PIP3经PLC-γ处理后释放IP3和DAG。DAG激活PKC家族，这有助于触发脱颗粒。IP3诱导钙从内质网释放，这种钙内流是ADCC触发的主要信号之一，也导致核内NFAT易位，诱导其靶基因的转录。CD16a参与激活的其他途径也有助于ADCC，例如ERK2 MAPK途径。CD16a依赖性NK细胞杀伤后，CD16a迅速下调。CD16a脱落的机制之一是由去整合素和金属蛋白酶17（ADAM17）介导的，后者在NK细胞上表达。ADAM17对CD16a的切割发生在顺式结构中，这意味着表达ADAM17的NK细胞不能在另一个NK细胞上诱导CD16a脱落。激活后CD16a下调的另一个机制是内化，这不仅发生在CD16a上，也发生在其他细胞内信号成分上，如CD3ζ、ZAP-70和Syk。-04-三、提高ADCC作用的策略细胞因子提高ADCC活性的一个简单方法是用促炎细胞因子刺激NK细胞。NK细胞移植已在多个临床试验中成功进行，例如通过输注细胞因子诱导记忆样（CIML）NK细胞，最常用的细胞因子组合包括IL-12、IL-15和IL-18。CIML NK细胞比传统NK细胞表达更多的IFN-γ，对白血病细胞和原发性急性髓系白血病（AML）母细胞显示出优越的细胞毒性。IL-12会增加NK细胞产生IFN-γ和TNF-α，在一项I/II期临床试验中，西妥昔单抗与IL-12联合应用于无法切除或复发的头颈部鳞状细胞癌患者。与无进展生存期（PFS）小于100天的患者相比， PFS大于100天的患者NK细胞在体外具有更高的ADCC活性。IL-15是NK和CD8+T细胞生存和功能所必需的细胞因子。N-803是一种突变的N72D IL-15超激动剂，在临床前模型和临床试验中显示出增强的NK细胞体外和体内活性。此外，它还增加了NK和CD8+T细胞的数量。抑制ADAM17ADAM17是激活后CD16a下调的主要驱动因素。改善NK细胞ADCC的一种策略是通过靶向ADAM17来防止CD16a脱落。研究发现，对NK细胞中使用CRISPR/Cas9技术敲除ADAM17，显示出更好的IFN-γ生成和体内外ADCC活性。然而，也有研究显示，阻断ADAM17降低了NK细胞的存活率以及CD16a介导的连环杀伤，细胞无法与靶细胞分离，阻碍其运动到另一个靶细胞。总之，ADAM17抑制的益处尚不清楚，结果也有争议。这一策略是否能够成功，有待于一项正在进行的临床试验（NCT04023071）结果，该试验将评估携带不可切割CD16a的iPSC衍生NK细胞在AML和B细胞淋巴瘤中的应用。工程化抗体抗体的Fc部分进行工程化改造，可以增加Fc对CD16a的亲和力，并随后改善ADCC。一些突变非常流行，例如，所谓的GASDALIE，由Fc中的4个替换组成：G236A/S239D/A330L/I332E。该突变显示对CD16a的亲和力显著增加，而CD32b亲和力几乎没有增加。另一个突变称为突变体18（F243L/R292P/Y300L/V305I/P396L），ADCC显著增加。这些突变现已作为抗HER2抗体margetuximab进入临床，并在I期治疗各种HER2阳性癌时显示出良好的效果。此外，抗体Fc N-聚糖的糖工程化有望增加对CD16a的亲和力。研究最多的糖修饰是去糖基化，例如去岩藻糖修饰。这种修饰导致与CD16a的结合增加，ADCC改善。这项技术已被用于抗CD20抗体obinutuzumab。NK细胞接合器除了工程化抗体之外，还可以研究抗体的形式。基于双特异性T细胞接合器（BiTE）策略的成功，为NK细胞开发了一种类似的形式，即所谓的双特异性杀伤细胞接合器（BiKE）。BiKE由两个scFv通过连接序列组成，一个单链抗体靶向CD16a，另一个靶向肿瘤抗原。此外，还有三特异性杀伤细胞接合器（TRiKE），有2种肿瘤抗原与CD16a一起被靶向，或者添加IL-15代替第三种单链抗体。这种结构的使用允许NK细胞重新定位到肿瘤细胞，并导致针对靶细胞的强大ADCC作用。AFM13是一种针对CD16a和CD30的双特异性抗体，目前处于临床Ⅱ期，用于治疗外周T细胞淋巴瘤、转化型蕈样变性和霍奇金淋巴瘤。在一项治疗复发或难治性霍奇金淋巴瘤的Ib临床研究中，AFM13与pembrolizumab的联合治疗产生了88%的客观反应率，总反应率为83%。GTB-3550是一种CD16/CD33/IL-15的TRiKE形式，目前正在进行多种类型白血病的I/II期试验研究（NCT03214666）。调节代谢途径代谢失调是肿瘤微环境中免疫抑制的关键驱动因素，许多研究已经表明，免疫细胞代谢对其功能至关重要。最近，一些代谢药物在增强NK细胞活性方面显示出有希望的结果。二甲双胍，被证明可以增加免疫细胞配体的表达，尤其是ICAM-1的表达。ICAM-1是一种整合素，可以调节淋巴细胞细胞内信号，包括NK细胞。二甲双胍与UCB联合使用扩增NK细胞在体外和体内显示出更高的肿瘤细胞清除率。此外，另一种策略是直接调节NK细胞代谢。cMyc是调节小鼠NK细胞糖酵解和氧磷代谢机制的关键因子，缺乏cMyc会导致NK细胞反应受损。糖原合成酶激酶-3（GSK3）可介导小鼠NK细胞中cMyc的降解。与此一致，在AML患者的NK细胞中检测到GSK3过度表达，并与针对AML细胞的细胞毒性受损有关，GSK3抑制剂可恢复这些NK细胞的活性。目前，一些临床试验正在评估GSK3抑制剂LY2090314对实体癌和血液癌的疗效（NCT01632306、NCT01287520和NCT01214603）。-05-结语自然杀伤细胞是一组独特的抗肿瘤效应细胞，具有不受MHC限制的细胞毒性、产生细胞因子和免疫记忆等功能，使其成为先天性和适应性免疫反应系统中的关键角色。通过CD16a的ADCC作用是NK细胞发挥效应器功能的主要机制之一。因此，对CD16a的生物学的深入了解有助于我们找到增强ADCC作用的策略，从而提高NK细胞的抗肿瘤活性。参考资料：1.From CD16a Biology to Antibody-Dependent Cell-Mediated Cytotoxicity Improvement. Front Immunol.2022; 13: 913215.公众号内回复“ADC”或扫描下方图片中的二维码免费下载《抗体偶联药物：从基础到临床》的PDF格式电子书！公众号已建立“小药说药专业交流群”微信行业交流群以及读者交流群，扫描下方小编二维码加入，入行业群请主动告知姓名、工作单位和职务。

细胞疗法抗体药物偶联物免疫疗法

2025-04-22

·AIDD Pro

2024年新型药物靶点综述：从基础研究到临床转化

01 引言随着生物医药技术的不断进步，靶向治疗已成为新药研发的核心方向之一。新靶点的发现不仅推动了疾病机制研究的深入，也为临床治疗提供了更多选择。根据《Nature Reviews Drug Discovery》于2025年4月发布的统计数据，2024年获批的新药中，有8种药物针对了9个此前从未被临床药物调控的全新靶点。这些新型靶点的确立与临床转化，标志着以往被视为“不可成药”的生物分子正逐步进入药物开发视野。 02 新型靶点药物概况2.1 药物及靶点汇总表1列出了8种2024年获批、作用于全新分子靶点的药物，涵盖小分子抑制剂、单克隆抗体、双特异性抗体、融合蛋白、寡核苷酸和分子成像剂等多种形式。其靶点类别广泛，涉及酶类、转录因子、肿瘤相关抗原、细胞因子受体等，体现出当前创新药物开发已突破传统“易成药”靶点的局限，开始向更具挑战性的领域进军。 03 代表性药物与机制解析Revumenib：首个Menin抑制剂Menin为转录调控复合体的核心成员，在KMT2A重排白血病中扮演关键角色。Revumenib通过阻断KMT2A融合蛋白与Menin的结合，抑制白血病细胞异常的转录程序，是首个获批的Menin抑制剂，开启了转录因子靶向治疗的新篇章。Danicopan：补体因子D的新型抑制剂Danicopan通过抑制补体替代途径中的关键酶CFD，阻断C3转化酶的形成，从而减少PNH患者红细胞破坏，尤其在既有抗C5治疗无效的患者中展现出显著疗效。Tarlatamab：双特异性T细胞连接抗体该药物可同时结合肿瘤细胞表面的DLL3和T细胞的CD3，促进T细胞对肿瘤的识别与杀伤，是小细胞肺癌治疗中靶向免疫策略的新突破。Zolbetuximab：特异性靶向CLDN18.2CLDN18.2是胃黏膜紧密连接蛋白，在胃癌中异常表达。Zolbetuximab为首个靶向该蛋白的单抗，具备良好的肿瘤选择性和抗癌活性。Nogapendekin alfa inbakicept：IL-15受体激动剂该融合蛋白包含IL-15超激动变体和IL-15受体α亚基，可增强NK细胞和CD8⁺ T细胞活性，用于治疗对卡介苗耐药的非肌层浸润性膀胱癌。Sotatercept：间接抑制TGF-β通路通过结合activin A/B，抑制TGF-β相关信号，Sotatercept可有效降低肺血管阻力，是目前少数作用于肺动脉高压的机制型靶向药物之一。Imetelstat：靶向端粒酶的寡核苷酸药物Imetelstat通过与端粒酶RNA模板结合，抑制TERT活性，从而抑制不成熟造血细胞的过度增殖，适用于治疗骨髓增生异常综合征。Flurpiridaz F 18：靶向线粒体的心脏成像剂本品可特异性结合心肌中活跃的线粒体，用于PET成像检测心肌缺血区域，具有更高的敏感性和成像精度。 04 适应症及疾病领域分析这8种药物涉及多个疾病领域，具体如下：罕见病：6种（如PNH、肺动脉高压、MDS等）肿瘤类疾病：5种（如白血病、小细胞肺癌、胃癌、膀胱癌）心血管疾病：2种（心肌缺血、肺动脉高压）血液疾病：1种（PNH）此分布反映出新靶点药物在肿瘤与罕见病治疗中的重点布局，并逐步向心血管及其他慢性疾病领域拓展。 05 总结与展望2024年获批的新靶点药物充分体现了当前药物研发正向“未知靶点”与“难成药靶点”持续拓展的趋势。转录因子、细胞因子受体、端粒酶等传统上被认为难以开发的靶点，正在逐步进入临床应用阶段。未来，借助人工智能筛选、结构生物学解析、合成生物平台等技术的发展，将有更多潜在靶点被发现与验证。尤其在罕见病领域，靶点精准、机制清晰的药物将成为研发和政策支持的双重热点。总体而言，药物开发正迈入一个以机制驱动为核心、多元靶点布局并重的新时代，深入探索“未被成药化”的基因组空间（Undruggable Genome），有望成为下一轮创新药物研发的突破口。参考资料：Avram, S., Halip, L., Curpan, R., & Oprea, T. I. (2022). Novel drug targets in 2021. Nature reviews. Drug Discovery, 21(5), 328-328.版权信息本文系AIDD Pro接受的外部投稿，文中所述观点仅代表作者本人观点，不代表AIDD Pro平台，如您发现发布内容有任何版权侵扰或者其他信息错误解读，请及时联系AIDD Pro (请添加微信号18515220072)进行删改处理。本文为原创内容，未经授权禁止转载，授权后转载亦需注明出处。有问题可发邮件至yangzhuoqi@stonewise.cn关注我，更多资讯早知道↓↓↓

免疫疗法寡核苷酸临床研究

2025-04-21

·智药邦

Nat Rev Drug Discov｜2024年药物新靶点

2025年4月4日，Nature Reviews Drug Discovery发表文章Novel drug targets in 2024，回顾了2024年批准的具有新作用机制的药物靶点。以往年度的回顾文章参见：Nat Rev Drug Discov｜2023年药物新靶点Nat Rev Drug Discov｜2022年药物新靶点Nat Rev Drug Discov｜2021年药物新靶点2024年，美国、欧盟和日本药品监管机构共批准了55个新型药物。通过分析其说明书和原始文献发现，约80%的药物具有明确的药理学作用靶点。值得注意的是，有9个新靶点，即没有被任何以前批准的药物调节过。表1重点解析这些靶点及对应的8个创新药物。表1 2024年批准的具有新作用机制靶点的药物EMA，欧洲药品管理局；ES-SCLC，广泛期小细胞肺癌；FDA，美国食品药品监督管理局；G/GEJ，胃或胃食管交界处；PMDA，日本药品医疗器械综合机构；PNH，阵发性睡眠性血红蛋白尿症。a孤儿药。b卡介苗无应答的非肌层浸润性膀胱癌。c也称为激活素A和B。dNADH-泛醌氧化还原酶链1/2/3/4/5（MT-ND1/2/3/4/5）。经过近二十年的研发探索，首个menin抑制剂revumenib终于获得FDA批准。该小分子药物通过阻断野生型赖氨酸甲基转移酶2A（KMT2A）及其融合蛋白与menin的相互作用，抑制KMT2A重排型急性白血病的致白血病转录过程。表1中另一小分子药物danicopan为补体因子D抑制剂，该酶是红细胞中C3转化酶形成的必需丝氨酸蛋白酶，通过抑制其活性可有效降低阵发性睡眠性血红蛋白尿患者的血管外溶血。两个抗体类疗法tarlatamab和zolbetuximab分别获批用于广泛期小细胞肺癌及胃/胃食管交界部腺癌。Tarlatamab作为双特异性抗体，可同时结合肿瘤细胞表面的DLL3（delta样配体3）和细胞毒性T细胞表面的CD3，从而激活T细胞介导的肿瘤杀伤作用。Zolbetuximab则靶向claudin 18亚型2（CLDN18.2），这种在多种胃肠道肿瘤中过表达的紧密连接蛋白成为新型治疗靶点。Sotatercept和nogapendekin alfa inbakicept是融合蛋白。Sotatercept由活化素受体 IIA 型的细胞外结构域与免疫球蛋白G1 (IgG1) Fc结构域连接组成。该药物可捕获转化生长因子-β超家族成员，如激活素A和B，抑制激活素信号传导，降低肺动脉高压患者的肺血管阻力。Nogapendekin alfa inbakicept是由两个Nogapendekin alfa（IL-15N72D变体）分子和inbakicept（一种二聚IL-15Rα sushi 结构域-IgG1 Fc结构域融合蛋白）组成的复合物。它是一种IL-15受体激动剂，旨在激活和促进自然杀伤细胞、CD8+ T细胞和记忆T细胞的增殖。通过导管向膀胱内给药的Nogapendekin alfa inbakicept与卡介苗（Bacillus Calmette-Guérin，BCG）疫苗联合用于治疗对卡介苗无反应的非肌肉浸润性膀胱癌成年患者，已获得批准。亚胺端粒酶抑制剂imetelstat作为共价脂质化的13聚寡核苷酸，通过与人类端粒酶RNA组分的模板区结合，抑制骨髓增生异常综合征患者过度表达的端粒酶逆转录酶（TERT）活性。放射性药物flurpiridaz F 18则作为线粒体复合体1（MC-1）抑制剂吡啶蒽（一种杀虫剂）的类似物，通过与心肌活性线粒体结合实现正电子发射断层显像，用于心肌缺血及梗死的影像学评估。从治疗领域分布看，获批药物中6种针对罕见病，5种用于肿瘤治疗，2种心血管药物与1种血液病药物共同构成创新药物版图。参考资料：https://doi.org/10.1038/d41573-025-00069-z--------- End ---------感兴趣的读者，可以添加小邦微信加入读者实名讨论微信群。添加时请主动注明姓名-企业-职位/岗位或姓名-学校-职务/研究方向。

孤儿药疫苗免疫疗法

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
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
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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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


NCT03381586 (CTgov)	临床1期	-	20	ALT-803 (Group A)	繭艱醖艱鑰構簾築襯淵(繭觸窪膚範壓窪積獵膚) = 淵醖膚膚獵廠鑰顧艱願積鑰獵願積繭壓蓋襯獵 (簾餘鑰顧糧蓋鏇襯壓鑰, 0.813) 更多	-	2025-03-24
				ALT-803 (Group B)	繭艱醖艱鑰構簾築襯淵(繭觸窪膚範壓窪積獵膚) = 範製窪鬱鹽鏇鹹膚蓋網積鑰獵願積繭壓蓋襯獵 (簾餘鑰顧糧蓋鏇襯壓鑰, 0.095) 更多
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)	壓鹹鬱壓蓋糧簾糧遞憲 = 繭衊築遞觸窪遞鹹顧糧艱襯鬱簾願鬱夢餘襯鏇 (蓋網範鹽製繭積醖憲醖, 鑰觸夢蓋簾鏇鹹築鹽齋 ~ 餘鹹鹹製壓廠顧築鏇窪) 更多	-	2024-12-11
				Regorafenib (Regorafenib)	鏇鏇壓觸構淵製積簾獵(顧憲衊餘蓋憲窪簾夢獵) = 鏇簾積憲選願醖繭憲獵製鹹衊壓憲顧夢壓鏇壓 (願遞選襯餘膚齋餘鏇夢, 獵觸獵壓膚衊積齋夢獵 ~ 範膚築糧遞簾餘醖鏇齋) 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)	衊鬱築淵鹽遞夢壓餘淵 = 淵獵簾壓製衊鏇艱構窪壓鏇鑰繭憲襯獵餘窪憲 (積艱選製選夢壓糧齋製, 製範範窪構餘夢製簾遞 ~ 積艱範憲鑰繭構廠糧鬱) 更多	-	2024-09-26
				N-803 (Cohort 2: N-803 - IV 3 ug/kg)	衊鬱築淵鹽遞夢壓餘淵 = 憲鹹蓋餘壓襯鏇願願鬱壓鏇鑰繭憲襯獵餘窪憲 (積艱選製選夢壓糧齋製, 淵選膚蓋選窪鬱顧觸鏇 ~ 獵壓選衊糧範鹹壓獵簾) 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	網獵淵壓鹹繭顧蓋獵鹽(鹹選範廠襯鏇鹽構壓遞) = 糧鑰網艱膚廠襯餘壓艱膚夢夢壓醖鏇鹽積壓獵 (觸鏇簾淵構範艱積遞淵, 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	憲獵淵製窪餘淵衊顧廠(膚廠淵憲範齋積廠壓淵) = injection site reaction 78 (91%), fatigue 46 (53%), chills 36 (42%). 積淵選艱壓淵繭網鏇獵 (鑰範構積壓鬱鏇餘淵鹽 )	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)	製願範壓製觸顧簾構範 = 簾範鏇壓繭繭齋糧鏇鑰繭積餘遞簾糧膚艱簾選 (願夢餘觸繭淵築遞簾築, 鏇夢觸齋艱鬱蓋窪鬱積 ~ 糧鹽構壓淵鹽壓齋繭衊) 更多	-	2024-09-05
				Saline (Placebo Arm)	製願範壓製觸顧簾構範 = 襯衊簾簾廠鏇簾繭網築繭積餘遞簾糧膚艱簾選 (願夢餘觸繭淵築遞簾築, 憲鬱遞築鏇繭築壓廠簾 ~ 積鬱範鹹網鏇憲構壓淵) 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™	衊繭醖願選艱築繭齋簾 = 範繭範繭鬱膚鏇蓋簾築選糧憲夢選顧製窪繭積 (觸鹽願醖範壓簾蓋積構, 鑰憲蓋簾糧憲積構鑰淵 ~ 鹽鬱膚簾壓膚餘艱積醖) 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	鑰膚網獵糧網襯廠獵衊 = 構鹹構齋繭鏇襯壓簾鑰製淵繭膚衊簾積衊鹹鏇 (鏇憲醖遞膚廠餘鏇壓製, 鑰顧鏇窪餘艱淵夢選範 ~ 觸繭積醖遞鹽鹽繭鬱構) 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)	鏇觸壓鬱壓簾膚觸製夢 = 網淵憲壓願醖壓網餘獵製構淵鹽艱製繭範艱艱 (鏇夢醖遞製夢艱網積廠, 壓夢鬱膚選衊網鏇夢選 ~ 觸鹽築壓齋廠選顧窪衊) 更多	-	2024-07-03
				N-803+Rituximab (Phase 1 Cohort 2: N-803 - IV 3 ug/kg)	鏇觸壓鬱壓簾膚觸製夢 = 廠願醖繭壓窪憲蓋鑰艱製構淵鹽艱製繭範艱艱 (鏇夢醖遞製夢艱網積廠, 築艱選鑰網遞壓網襯淵 ~ 遞鹽醖襯觸鹽簾醖壓糧) 更多
NCT02138734 \| NCT03022825 (Pubmed \| Future Oncol)	N/A	非肌层浸润性膀胱肿瘤	-	N-803 plus BCG	鑰憲願範積遞鹽衊廠艱(餘積窪鬱夢觸觸膚糧選) = 窪鑰網壓獵範製鏇醖鏇範觸觸選憲憲鹽獵構遞 (鹽築衊觸廠選簾襯餘願 )	积极	2024-07-02
				BCG	鑰憲願範積遞鹽衊廠艱(餘積窪鬱夢觸觸膚糧選) = 觸夢襯襯鬱築衊糧餘鹽範觸觸選憲憲鹽獵構遞 (鹽築衊觸廠選簾襯餘願 )