An International, Randomized, Double-Blind, Controlled Phase II Study of Rindopepimut/GM-CSF with Adjuvant Temozolomide in Patients with Newly Diagnosed, Surgically Resected, EGFRvIII-positive Glioblastoma - Irradiance

开始日期2013-01-11

申办/合作机构

Celldex Therapeutics, Inc.

NCT01498328

/ Completed临床2期

A Phase II Study of Rindopepimut/GM-CSF in Patients With Relapsed EGFRvIII-Positive Glioblastoma

The purpose of this research study is to find out whether adding an experimental vaccine called rindopepimut (also known as CDX-110) to the commonly used drug bevacizumab can improve progression free survival (slowing the growth of tumors) of patients with relapsed EGFRvIII positive glioblastoma.

开始日期2011-12-01

申办/合作机构

Celldex Therapeutics, Inc.

NCT01480479

/ Completed临床3期

An International, Randomized, Double-Blind, Controlled Study of Rindopepimut/GM-CSF With Adjuvant Temozolomide in Patients With Newly Diagnosed, Surgically Resected, EGFRvIII-positive Glioblastoma

This 2-arm, randomized, phase III study will investigate the efficacy and safety of the addition of rindopepimut (an experimental cancer vaccine that may act to promote anti-cancer effects in patients who have tumors that express the EGFRvIII protein) to the current standard of care (temozolomide) in patients with recently diagnosed glioblastoma, a type of brain cancer.
All patients will be administered temozolomide, the standard treatment for glioblastoma. Half the patients will be randomly assigned to receive rindopepimut and half the patients will be randomly assigned to receive a control called keyhole limpet hemocyanin.
Patients will be treated in a blinded fashion (neither the patient or the doctor will know which arm of the study the patient is on). Patients will be treated until disease progression or intolerance to therapy and all patients will be followed for survival.

开始日期2011-11-01

申办/合作机构

Celldex Therapeutics, Inc.

100 项与 Rindopepimut 相关的临床结果

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100 项与 Rindopepimut 相关的转化医学

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100 项与 Rindopepimut 相关的专利（医药）

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项与 Rindopepimut 相关的文献（医药）

2024-06-01·Cancer Medicine

Targeted agents in patients with progressive glioblastoma—A systematic meta‐analysis of randomized clinical trials

Review

作者: Seliger‐Behme, Corinna ; Agkatsev, Sarina ; Scherm, Angelika ; Kessler, Tobias ; Leitzmann, Michael F. ; Ippen, Franziska Maria ; Baurecht, Hansjörg ; Hau, Peter ; Wick, Wolfgang ; Knüttel, Helge

Abstract:

Background:

Glioblastoma (GB) is the most common malignant primary brain tumor in adults and is associated with a poor prognosis. Current treatment guidelines outline the standard of care for patients with newly diagnosed GB; however, there is currently no well‐established consensus for the treatment of progressive GB. With this systematic meta‐analysis of recently published randomized controlled trials (RCTs), we aim to establish evidence on targeted agents in the treatment of patients with progressive GB.

Material and Methods:

We conducted searches across the Cochrane Library, Pubmed, MEDLINE (Ovid), ClinicalTrials.gov, WHO‘s International Clinical Trials Registry Platform and Google Scholar, encompassing the time span from 1954 to 2022, aiming to identify RCTs evaluating targeted therapies in patients with progressive GB. In order to perform a random‐effects meta‐analysis, we extracted hazard ratios (HRs) of overall survival (OS) and progression‐free survival (PFS).

Results:

We included 16 RCTs (n = 3025 patients) in the systematic meta‐analysis. Formally, regorafenib (RR 0.50; 95% CI 0.33–0.75), Depatux‐M + TMZ (RR 0.66; 95% CI 0.47–0.93) and rindopepimut + bevacizumab (RR 0.53; 95% CI 0.32–0.88) were associated with an improved OS compared to the control arm. The combination of bevacizumab + CCNU (RR = 0.49; 95% CI 0.35–0.69) and regorafenib (RR 0.65; 95% CI 0.44–0.95) were formally associated with improved PFS.

Conclusions:

The aim of this systematic meta‐analysis was to establish evidence for the use of targeted therapies in progressive GB. While some studies demonstrated benefits for OS and/or PFS, those results have to be interpreted with caution as most studies had major methodological weaknesses, including potential differences in sample size, trial design, or the initial distribution of prognostic factors.

2023-01-01·Advances in Experimental Medicine and Biology

Immunotherapy as a New Therapeutic Approach for Brain and Spinal Cord Tumors

Article

作者: Medikonda, Ravi ; Pant, Ayush ; Lim, Michael

Historically, the central nervous system (CNS) was considered an immune-privileged organ. However, recent studies have shown that the immune system plays a significant role in the CNS. Thus, there is renewed interest in applying cancer immunotherapy to CNS malignancies with the hope of generating a robust anti-tumor immune response and creating long-lasting immunity in patients. There has been some work with non-specific immunotherapy such as IL-2 for brain metastasis. Unfortunately, the results from non-specific immunotherapy studies were lackluster, so the focus has shifted to more specific CNS immunotherapies including cancer vaccines, immune checkpoint inhibitors, oncolytic virus therapy, and chimeric antigen receptor (CAR) T cell therapy. With respect to cancer vaccines, rindopepimut has been well-studied in glioblastoma (GBM) patients with the EGFRvIII mutation, with early results from phase II trials showing possible efficacy in carefully selected GBM patients. Other antigen-specific CNS tumor vaccines are still in the early stages. Immune checkpoint inhibitors are amongst the most promising and widely studied CNS immunotherapy strategies. Anti-PD-1 showed promising results in many non-CNS solid tumors, however, results from early clinical trials show poor efficacy for anti-PD-1 in GBM patients. Anti-PD-1 is also under investigation for CNS metastasis and showed some efficacy in non-small cell lung cancer and renal cell carcinoma patients. Anti-PD-1 is under early stage investigation for other CNS tumors such as chordoma. Oncolytic virus therapy is the strategy of infecting tumor cells with a virus that in turn triggers an innate immune response leading to tumor cell lysis. Oncolytic viruses currently under investigation include several adenovirus-based therapies and a herpes simplex virus-based therapy. Phase I studies have demonstrated the safety of oncolytic virus therapies in GBM patients. Current studies are evaluating the efficacy of these therapies both alone and in combination with other immunotherapy approaches such as checkpoint inhibition in patients with CNS tumors. CAR T cell therapy is a newer immunotherapy approach. CAR T cell therapies, directed against EGFRvIII mutation and HER-2 mutation, demonstrate an acceptable safety profile, although there is no conclusive evidence of the survival benefit of these therapies in early trials. Studies are currently underway to determine optimal tumor-specific antigen selection and modality of administration for CAR T cell therapy. Overall, the prognosis is generally poor for patients with CNS malignancies. The promising results of cancer immunotherapy for non-CNS tumors have created significant interest in applying these therapies for CNS malignancies. Preliminary results have not demonstrated robust efficacy for CNS immunotherapy. However, it is important to keep in mind that the field is still in its infancy and many clinical trials are still early-phase. Several, clinical trials are currently underway to further explore the role of immunotherapy for CNS malignancies.

2022-04-01·World neurosurgery4区 · 医学

Efficacy and Safety of Bevacizumab Combined with Other Therapeutic Regimens for Treatment of Recurrent Glioblastoma: A Network Meta-analysis

4区 · 医学

Article

作者: Tong, Chen ; Qian, Han ; Zhengyao, Zuo ; Fengqun, Mu ; Xiaozhuo, Liu ; Qing, Wang ; Mei, Li ; Mingming, Fan ; Dongpo, Su

BACKGROUND:

Despite the fact that bevacizumab (Bev) has been approved to treat recurrent glioblastoma, patients have failed to demonstrate a significant overall survival (OS) advantage. In recent years, the advent of more Bev combination regimens seems to bring new hope for patients; nevertheless, there is still a lack of intuitive comparison among these therapies.

OBJECTIVE:

To explore the efficacy and safety of various Bev combination regimens in patients with recurrent glioblastoma and to further explore the differences in the efficacy of each treatment in randomized controlled trials (RCTs) and nonrandomized controlled trials (non-RCTs).

METHODS:

We comprehensively searched the PubMed, Cochrane Library, and OVID databases for relevant RCTs and non-RCTs of Bev in combined regimens for recurrent glioblastoma. The Cochrane quality assessment method was used to assess the quality of RCTs, and the Newcastle-Ottawa scale was used to assess the quality of non-RCTs. Excel software was used to extract data from the literature, and a network meta-analysis was performed using RevMan 5.3 and Stata 16 statistical software.

RESULTS:

In patients with recurrent glioblastoma, the 6-month OS of patients receiving bevacizumab combination therapy was ranked from high to low as follows: Bev + rindopepimut, Bev + lomustine (CCNU), CCNU, tumor treating fields + Bev, Bev, Bev + irinotecan (Iri), Bev + temozolomide (TMZ), Bev + vorinostat, Bev + onartuzumab, Bev + dasatinib, Bev + carboplatin, Bev + trebananib, Bev + VB-111, TMZ, PCV, VB-111, and carboplatin. The 6-month progression-free survival from high to low was ranked as follows: Bev + CCNU, Bev + rindopepimut, Bev + dasatinib, Bev + vorinostat, Bev, Bev + Iri, Bev + TMZ, CCNU, Bev + carboplatin, TMZ, Bev + VB-111, PCV, Bev + trebananib, carboplatin, and VB-111. We compared the total incidence of serious adverse events (≥3) and found that Bev + vorinostat and Bev + trebananib were safer than Bev, while other regimens were not as safe as Bev. A descriptive analysis showed that Bev + rindopepimut also appeared to be safer than Bev. In subgroup analysis, among RCTs, Bev + CCNU therapy had the highest 6-month OS and 6-month progression-free survival. Among non-RCTs, Bev + Iri therapy showed the highest 6-month OS and good 6-month progression-free survival.

CONCLUSIONS:

Both Bev + CCNU and Bev + rindopepimut could be considered as effective therapies for treating the recurrent glioblastoma according to the network meta-analysis results. Among them, Bev + rindopepimut therapy seems to be safer and more effective. Moreover, we found that Bev + Iri also appeared to be an effective therapy in a retrospective study.

项与 Rindopepimut 相关的新闻（医药）

2024-06-03

·同写意

癌症疫苗百年沉浮：希望、遇冷、触底、重塑

同写意20岁庆！中国医药创新未来之路！“意”同创新，穿越周期，赢得未来。7月中旬，苏州金鸡湖畔，让我们与“新药写意人”一起为中国医药创新“同写意”！ “登上月球和治愈癌症，你觉得哪个更容易实现？” 在上世纪中期美国媒体的一次民调中，被问到这个问题的美国人给出惊人的一致答案：癌症可能治愈，登上月球是不可能的。岁月无情地打了他们的脸。时至今日，阿波罗号飞船已经登月几十年，人类却依旧奋斗在治愈癌症的征途中。当然，如今人类对抗癌症的手段越来越多，PD-1、ADC、CAR-T等技术路线均有突破性的疗效，但却依然距离“治愈”目标很远，科学家们仍然希望继续扩展工具箱，来实现这个夙愿。单纯从理论角度出发，癌症疫苗可能是最合适的工具：通过利用肿瘤细胞相关抗原，来唤醒人体针对癌症的免疫系统。然而现实却十分残酷，肿瘤疫苗的研究的从未中断过，但却并未有人真正突破。第一款癌症疫苗因疗效一般、价格昂贵而淡出市场。此后，Celldex的Rintega、Argos的rocapuldencel-T、和Agenus的Prophage G-200等多款癌症疫苗也先后在临床试验中以失败告终。难道癌症疫苗真的只是科学家们的南柯一梦？或许我们并不应该如此悲观，经过长时间的努力，人类已经距离癌症疫苗的成功研发越来越近。 1 癌症疫苗：一上来就是逆风局疫苗是人类在医学领域里最伟大的发明。每当一款疫苗被研发出来，就意味着某些疾病将被击败，甚至永久性地从人类生活中消失。基于疫苗强大的功效，科学家们开始将疫苗的应用领域逐渐扩大，甚至开始尝试治疗癌症。最广为人知的预防性癌症疫苗就是当下爆火的HPV疫苗。高危型人乳头瘤病毒（HPV）持续感染是导致宫颈癌的主要原因，通过接种HPV疫苗可有效预防HPV持续感染及相关宫颈病变，是宫颈癌一级预防的主要措施。不过只有约15%的癌症是由病毒引起，更多的癌症则是由于基因突变产生。对于这类癌症，就需要治疗疫苗发挥作用。目前，大多数药企的主攻方向也都是市场更广阔的治疗疫苗。追根溯源，人类对癌症疫苗的探索，已有百年历史。早在1893年，癌症免疫治疗之父William B. Coley发现了化脓性链球菌所分泌的丹毒毒素能够引起肉瘤晚期患者的肿瘤消退，奠定了肿瘤疫苗的研究开端。此后的百年时间中，癌症疫苗发展并不顺利，直至二十一世纪才有所突破。2007年，治疗前列腺癌的疫苗Provenge，以13：4的压倒性优势获得了FDA顾问委员会的支持，站在获批上市的边缘。但令人意想不到的是，这四张反对票的力量出其不意地强大。反对者表示，Provenge虽然改善了患者生存率，但肿瘤大小并没有显著变化，疗效乏善可陈，顶多也只是在安全性上大概率治不死患者。图：Provenge作用原理，来源：天风证券这样的说法并不是毫无根据，虽然打着癌症疫苗这个新概念，但Provenge的临床数据着实不算亮眼。Provenge的确没有带来颠覆性的疗效，比起对照组仅仅将患者的总体生存期延长4.1个月。反对者指责投赞成票的人，在癌症药物这档子事上压根一窍不通，才会轻易被这种刺激免疫系统治疗癌症的古老概念诱骗。迫于形势和舆论压力，FDA只能宣布Provenge投票作废，并要求提供更多临床数据支持。当年，《华尔街日报》将此次事件称为癌症免疫疗法史上的“黑色星期三”，癌症疫苗的发展也一夜回到解放前。经过反复斡旋，Provenge还是在2010年通过了FDA的批准，开创了癌症免疫治疗新时代。可事情的发展并没有想象中的顺利，经历重重阻碍成功问世的Provenge，不仅没给这个领域带来希望反倒是狠狠破了一盆冷水：Provenge临床效果一般，每疗程定价却高达9.9万美元。图：Provenge与小分子药物对比，来源：天风证券作为对照，在2011年和2012年上市的阿比特龙和恩杂鲁胺，同样治疗疗前列腺癌效果却都比Provenge数据更好。在这样的情况下，患者选择用脚投票，最终“跨时代疗法”Provenge以惨淡销售收场，其背后的研发公司Dendreon也落得破产结局。从那之后，再未有任何一款癌症治疗疫苗成功上市。这么多年过去了，不禁有投资者心生疑问，阻碍癌症疫苗发展的绊脚石究竟是什么呢？ 2 问题的七寸究竟在哪里？癌症疫苗的原理不算复杂。正常情况下，免疫系统会发现并杀死人体的入侵者。但是癌细胞异常狡猾，它并不属于入侵者，而且可以伪装成良民，逃过免疫细胞的火眼金睛。从机制上看，癌症疫苗的总体思路是让一个人的免疫系统可以精准区分肿瘤细胞和正常细胞，通过将肿瘤抗原以核酸、蛋白多肽等形式导入患者体内，来刺激患者体内自身免疫系统的反应从而对肿瘤细胞进行清除。一剂癌症疫苗，由肿瘤抗原、制剂、免疫佐剂和运载工具四部分组成。不同癌症患者的肿瘤细胞突变不同，所以癌症疫苗需对个体的肿瘤细胞进行基因测序以识别靶标，进行个性化定制。靶标通常是肿瘤细胞中出现的突变蛋白，也就是肿瘤抗原，这是癌症疫苗研发过程中的第一个难点。肿瘤抗原被注射到患者体内后，会激活机体免疫系统杀灭肿瘤细胞的特异性免疫反应。理想的情况下，癌症疫苗所选用的抗原应该存在于所有癌细胞中，并且是癌细胞存活所必需的，但在正常细胞中不存在，所以能更有效地激发人体的免疫反应。但想要找到完美的肿瘤抗原并不容易。因为肿瘤相关抗原是一种自身抗原，患者对这些抗原可能已经有中枢耐受，这导致免疫系统难以对其产生强烈的免疫反应。并且，肿瘤相关抗原在正常细胞中也有存在，这就导致在免疫系统受到刺激后，正常细胞可能也会被误伤。可以说，这类被称为肿瘤相关抗原（TAA）的蛋白并非理想抗原。也是因此，据此研发的大部分肿瘤疫苗，不仅达不到理想的治疗效果，还会出现较大的不良反应。同时，肿瘤微环境也是影响因素之一。免疫抑制细胞的存在，让肿瘤微环境具备免疫抑制效果，保护肿瘤免受免疫攻击，影响癌症疫苗的效果。想提高疫苗的治疗效果，就得想效应免疫细胞克服肿瘤微环境内的多重抑制网络和激活障碍。此外，适合的体外评估模型、临床研究终点的设计、癌症疫苗的生产等方方面面都充满着未知的挑战。言而总之，治疗性癌症疫苗想要成功，需要从确定肿瘤抗原、克服免疫抑制肿瘤微环境等角度共同入手。 3 破晓的曙光陷入技术瓶颈多年后，癌症疫苗终迎破晓曙光：新型肿瘤抗原正在进入科学家视野。新型抗原通常由肿瘤细胞基因组突变产生，仅存在于肿瘤细胞。由于正常细胞不会产生和表达新抗原，所以能更有效地激发人体的免疫反应。 2021年的时候，发表在国际顶级《Nature medicine》上的文章披露，NeoVax新型抗原疫苗用于治疗黑色素瘤患者，可以有效的控制肿瘤生长的免疫反应持续了长达四年。同时，新冠疫情爆发， mRNA 疫苗迅速得到广泛应用，使得 mRNA 在生产策略、递送系统、抗肿瘤免疫策略等多方面取得进展，也加速了癌症疫苗的实际落地速度。由默沙东与Moderna联合开发的皮肤癌疫苗mRNA-4157，就是根据每位患者肿瘤独特的DNA序列突变特征通过算法设计而成，包含编码最多34种新抗原的单一合成mRNA分子。当将此疫苗注入患者体内时，这些RNA所携带的新抗原序列会被翻译成蛋白质，并通过体内的抗原呈递，刺激产生T细胞抗肿瘤反应。针对肿瘤微环境中的免疫抑制的问题，癌症疫苗与其他免疫疗法的协同，或许会给出解决方案。比如mRNA疫苗与PD-1的联用，就是如此。在临床试验中，这一组合已经展示出了潜力。在ASCO年会当中，默沙东与Moderna公布了mRNA-4157与K药联合，在157位经手术切除高风险黑色素瘤患者中的疗效与安全性数据。图：mRNA-4157联合K药数据，来源：东北证券与单独使用K药相比，降低肿瘤产生远处转移或死亡的风险达65%。根据临床2b期试验KEYNOTE-942的数据，FDA授予mRNA-4157与Keytruda组合突破性疗法认定，作为辅助疗法用以治疗完全切除后的高风险黑色素瘤患者。 2023年底，Moderna首席执行官接受采访时曾表示，“Moderna针对黑色素瘤的mRNA癌症疫苗可能在两年内上市，这将是抗击这种最严重形式皮肤癌的里程碑式的一步。”看来，经过几十年的缓慢进展，肿瘤疫苗的钟摆终于又荡到了成功的边缘。更多优质内容，欢迎关注↓↓↓

疫苗细胞疗法免疫疗法抗体药物偶联物信使RNA

2022-06-01

·药时代

2项癌症疫苗新进展，问题来了：T细胞的最佳搭档是哪位？NK细胞 or B细胞？

癌症是一种由肿瘤细胞不受控制，异常生长造成的疾病，其核心在于肿瘤细胞逃避了人体的免疫系统，从而无限增殖造成的。近百年来，科学家们都在研究如何通过激活免疫系统，达到治疗肿瘤的目的，从而让患者获益。大多数癌症免疫疗法主要依靠T细胞来抑制肿瘤。但在两项新的研究中，丹娜-法伯癌症研究所（Dana-Farber）和斯坦福大学的科学家发现了新的免疫肿瘤学方法，表明利用免疫系统的其他组成部分可以达到更好的抗肿瘤效果。2022年5月25日，发表在《Nature》杂志的一项研究中，由Dana-Farber领导的团队开发了一种癌症疫苗，该疫苗靶向T细胞和自然杀伤（NK）细胞，采取双管齐下的攻击方式，防止肿瘤细胞逃避免疫系统的攻击。此外，近期发表于《Science Immunology》上的另一项研究中，斯坦福大学的一个团队发现，将Dynavax的疫苗佐剂加入Dragonfly Therapeutics研发的白细胞介素-12 （IL-12）药物中，并将其直接注射到肿瘤中，由于B细胞和T细胞之间存在的密切联系，该方法可以激活B细胞并诱导全身抗肿瘤反应。两个团队都表示，他们的方法是具有潜力的癌症治疗方法，可以增强抗肿瘤反应并防止患者癌症复发。什么是癌症疫苗？1890年，科学家发现可以通过外源刺激免疫反应，使肿瘤消退，这也成为了癌症治疗疫苗的理论基石。但由于缺乏对肿瘤抗原的深入了解，癌症疫苗发展缓慢。肿瘤细胞具有极强的反击能力，它们在肿瘤边缘形成了强大的保护层，使很多肿瘤疫苗或转输到体内的T细胞不能发挥抑制肿瘤的功能。医学界对癌症疫苗的研究从未中断，但效果都不理想，Celldex的Rintega、Argos的rocapuldencel-T、和Agenus的Prophage G-200均先后在临床试验中以失败告终。除了HPV疫苗是知名的预防性癌症疫苗外，2010年，FDA批准了全球首个也是目前唯一一款癌症治疗疫苗Provenge（sipuleucel-T），用于治疗晚期前列腺癌。这种疫苗第一次实现了利用患者自身的免疫系统攻击癌细胞的设想。但由于Provenge效果一般，价格却不便宜，其研发公司Dendreon最终也以破产告终。目前，癌症疫苗中疗效及预防复发效果较为突出的是树突状细胞疫苗和个性化新抗原疫苗等，树突状细胞（DCs）能提呈肿瘤蛋白给适应性免疫细胞（如T细胞），帮助激活T细胞免疫反应进而攻击肿瘤细胞。DC疫苗的主要优势之一是，其不存在HLA不匹配的风险。在德国、日本也有树突状细胞疫苗用于临床辅助治疗多种癌症，如肺癌、肝癌、肾癌、乳腺癌、皮肤癌等，这是癌症患者治疗的新希望。肿瘤免疫治疗的机理是什么？肿瘤免疫治疗通过调控免疫系统来达到控制肿瘤的目的，所以肿瘤免疫治疗的直接作用目标是免疫细胞而不是肿瘤细胞。肿瘤免疫治疗的目的是恢复或增强免疫细胞识别和清除肿瘤细胞的能力，其治疗效果取决于诱导出的免疫细胞清除肿瘤细胞的能力。免疫反应有两种类型：固有免疫反应和适应性免疫反应。前者反应快，不具有抗原特异性；后者反应较慢，对抗原具有特异性，并具有记忆功能，是保护性免疫疫苗的理论基础。巨噬细胞和自然杀伤细胞（NK细胞）是两种主要的能杀伤肿瘤的固有免疫细胞。适应性免疫细胞主要包括T细胞和B细胞。肿瘤细胞与正常细胞不同，它们表达独特的肿瘤抗原，这些肿瘤抗原能被T细胞识别而引发免疫反应。肿瘤抗原是包埋在MHC分子内的，而不是直接表达在肿瘤细胞表面。MHC提呈的抗原被T细胞表达的T细胞受体识别。一个T细胞只能表达一种T细胞受体并且只能识别一种抗原。与T细胞不同，B细胞不直接杀死肿瘤细胞，而是产生攻击分子（又叫抗体）。这些抗体能够捕捉目标抗原，一种抗体只能和一种抗原结合。一旦抗体与抗原结合，它们要么阻断这个靶分子的功能，要么引导其他免疫细胞（如巨噬细胞和自然杀伤细胞）杀死表达抗原的靶细胞，这一过程称为抗体依赖的细胞介导的细胞毒性作用（ADCC）。在肿瘤治疗中，特别是血液肿瘤中，ADCC起着关键作用。1T细胞+NK细胞，通用型疫苗癌症疫苗的工作原理是诱导T细胞对肿瘤细胞表面的特定抗原产生反应。但肿瘤细胞可以发展出各种各样的机制来干扰抗原向T细胞呈递，从而隐藏自己不被免疫系统识别。更重要的是，每个个体的肿瘤抗原可能是不同的，因此很难设计出一款可以同时治疗很多患者的通用型癌症疫苗。Dana-Farber的科学家们在Kai Wucherpfennig医学博士的带领下，针对两种表面蛋白：MICA和MICB进行了疫苗的研发。主要组织相容性复合体（MHC）相关蛋白A和B（MICA/MICB）属于应激蛋白。MHC的主要功能是将抗原“呈现”在细胞表面，供合适的T细胞识别。MHC可测量细胞内是否有肿瘤抗原，因此该指标在许多实体瘤上高水平表达。在DNA损伤等应激条件下，这些蛋白质的表达可能会增加。然后它们结合并激活T细胞和NK细胞，从而清除异常细胞。但是肿瘤细胞可以通过切断MICA和MICB，使其脱落，从而逃脱这种免疫反应。新的疫苗诱导抗体抑制肿瘤细胞MICA/MICB脱落到无法检测到的水平，并将不同群体的T细胞和NK细胞招募到小鼠的肿瘤中。此种疫苗可同时调动T细胞和NK细胞，从而对肿瘤细胞起到杀伤作用，还能避开肿瘤细胞的免疫逃逸机制。该疫苗进入了临床试验的哪个阶段？在此项临床研究中，研究人员在小鼠中进行体内试验来检验疫苗的作用。这款抗癌疫苗MICB-vax（针对MICB α3结构域设计的疫苗）在控制表达MICB/MICA的黑色素瘤细胞和淋巴瘤细胞方面显示出显著功效。更为惊喜的是，MICB-vax疫苗还可有效抑制肿瘤转移、预防肿瘤复发。在侵袭性黑色素瘤的小鼠模型中，MICB疫苗显著缩小了肿瘤，在某些情况下甚至根除了肿瘤，而对照组小鼠则出现了主要肿瘤的生长。该团队还在患有黑色素瘤的小鼠身上测试了这种疫苗，这些小鼠对目前的免疫疗法具有耐药性，但在接受该疫苗治疗后效果良好。50%至75%的小鼠在疫苗治疗后100天以上保持无瘤状态。进一步的分析表明，为有效控制肿瘤，T细胞和NK细胞都是不可或缺的。基于在小鼠体内试验的积极疗效以及在猴子体内试验的一些免疫原性和安全性结果，Dana-Farber的科学家们表示，他们目前正计划对这种疫苗进行首次人体试验。研究人员在《Nature》杂志的研究中写道，这种疫苗“也可能与局部放疗相结合，因为DNA损伤会增强癌细胞的MICA/MICB表达”。值得一提的是，由于表达MICA/MICB是肿瘤普遍的特点，因此针对此靶点的疫苗具有通用型，不用针对每位患者进行个性化定制，此研究使通用型抗癌疫苗的研发迈出了重要一步。2B细胞的意外发现，局部+远端同时治疗从传统的细胞毒化疗药物、小分子抑制剂、到免疫检查点抑制剂治疗，肿瘤治疗的方法呈爆发式发展。这些进展同时也伴随着新的毒性和疾病。免疫相关不良事件最常累及的器官是胃肠道、皮肤和内分泌系统。与传统的化疗相比，肿瘤免疫治疗有着特殊的不良反应谱。免疫治疗相关不良反应的早期识别和治疗是患者管理的重要环节。白细胞介素12（IL-12）是由P35和P40亚基组成的异源二聚体，是诱导细胞免疫的主要细胞因子之一。在肿瘤微环境中，IL-12刺激活化的T细胞和自然杀伤细胞（NK）释放毒杀性的酶类或分泌效应细胞因子如IFNγ，这些效应分子对于肿瘤的清除至关重要。IL-12可以激活免疫细胞的细胞因子，被认为是一种有效的抗肿瘤药物，但毒性一直是限制IL-12临床应用的主要原因。斯坦福大学的研究团队尝试将Dragonfly Therapeutics改良的IL-12药物以低剂量方案注射到肿瘤局部，同时利用其治疗潜力以降低毒性。根据2020年签署的一项协议，百时美施贵宝（Bristol Myers Squibb）已经授权Dragonfly公司的IL-12候选药物（编号为DF6002或BMS-9896415）用于癌症治疗。研发团队有什么新发现？在他们的研究中，由医学博士Ronald Levy领导的斯坦福团队意外发现，在接受局部免疫治疗后，B细胞竟然还能有助于远处肿瘤的缩小。斯坦福大学的科学家进一步添加了Dynavax公司的疫苗佐剂CpG SD-101作为刺激，以实现更有效的T细胞免疫反应。在淋巴瘤、结肠癌、三阴性乳腺癌和黑素瘤的多个小鼠模型中，联合治疗实现了局部和远处肿瘤控制，并显著提高了动物的生存率。虽然这种治疗是为了增强T细胞介导的反应，但科学家们惊奇地发现，B细胞在这种全身反应中也是必不可少的。研究小组发现，在联合治疗之前和治疗期间，用抗CD20抗体清除B细胞可以消除全身效应。在进一步研究了B细胞的行为后，研究小组发现B细胞产生了肿瘤特异性抗体。在第一个肿瘤附近的淋巴结中，它们将肿瘤抗原呈递给T细胞。这些处理过的T细胞随后移动到远处的肿瘤并杀死它们。斯坦福大学团队在研究中写道，“我们的数据表明，在未来， B细胞在其他形式的肿瘤免疫治疗中的作用应该被研究。提供B细胞刺激的药物可以加入到T细胞刺激的方法中，以增强免疫治疗方案的效力和特异性。”3结语了解免疫系统及其肿瘤治疗中的作用有助于开发早期抗肿瘤疫苗。疫苗能够刺激宿主产生免疫力对抗肿瘤，而且方便在门诊使用且毒性更小。但是，缺乏理想的抗原以及疗效较差是目前抗肿瘤疫苗研发的主要瓶颈。理想的抗肿瘤疫苗必须克服肿瘤细胞产生的免疫耐受。随着人类对免疫系统作用机制的进一步了解，对癌症疫苗的研发也会取得更多的突破，相信不远的将来，癌症或许不再是人类无法攻克的疾病。参考资料：https://www.fiercebiotech.com/research/novel-cancer-vaccines-dana-farber-and-stanford-look-beyond-t-cells-better-fight-tumors《通用型癌症疫苗获重大突破！同时激活T细胞和NK细胞，有望治疗多种癌症！》《癌症疫苗30年，为什么就是研发不出来？》其他公开资料。版权声明/免责声明本文为原创文章，版权归拥有者。仅供感兴趣的个人谨慎参考，非商用，非医用、非投资用。欢迎朋友们批评指正！衷心感谢！文中图片、视频为授权正版作品，或来自微信公共图片库，或取自网络根据CC0协议使用，版权归拥有者。任何问题，请与我们联系（电话：13651980212。微信：27674131。邮箱：contact@drugtimes.cn）。衷心感谢！推荐阅读寒冬之下，逆势前行！2021年度中国最佳「生物医药领域投资案例」TOP10出炉，这些公司有何特别之处？生物经济来临，如何应对挑战，穿越AI制药产业新周期？受美国预摘牌影响的14家中国药企之股价、市值分析 | 药时代出海系列中国新药出海，传奇再现！全球新，中国创！本维莫德终获FDA批准！恒瑞喜讯频传！。。。| 药时代出海系列2022 ASCO 各领域口头报告一览（附：731页ASCO 会议摘要）【诚聘付费专家】电话咨询主题：抑郁症、肺鳞癌、黑色素瘤、糖尿病、肥胖新药研发之竞争格局与潜在机遇Fierce Biotech裁员盘点：生物技术行业正向着“小而精”的趋势发展药时代BD项目 | 高亲和力、高效能CD24靶向单克隆抗体斑秃患者的福音！JAK抑制剂CTP-543的III期临床试验取得阳性结果！维昇药业首个关键3期临床试验达到主要终点点击这里，帮您找到理想的合作伙伴！

疫苗免疫疗法信使RNA抗体细胞疗法

2016-12-07

·BioSpace

BioPharm Executive: So Long 2016 (and Good Riddance?)

December 14, 2016 By Karl Thiel for BioSpace.com Many of us will be glad to see the end of 2016, a year that was marked by terrorism both domestic and international, a string of celebrity deaths, a new disease scourge (Zika became the new Ebola), and a whole lot of political turmoil that made for some tense Thanksgiving table conversations. Here in our little corner of the world, there was plenty of volatility too. So without further delay, let’s count down this year’s wholly subjective list of the year’s top 10 biotech trends and events. #10: Brexit. The U.K.'s decision to exit the European Union will likely have some broad-reaching and long-lasting effects, most of which are yet to be felt. In the short term, the move has been on balance positive for U.K.'s pharma sector—for a simple reason. A historically weak pound sterling is helping companies like GlaxoSmithKline and AstraZeneca boost dollar-denominated profits. Rumors initially swirled that both these pharma giants would pull up roots and leave the U.K., but that doesn’t appear to be the case, at least for now. Longer term, it remains to be seen if some of the bigger fears—failure to attract or retain top talent, securing investment, and keeping favorable trade deals—come to fruition. #9: Sharply declining approvals. Both 2014 and 2015 were tough acts to follow. There were 45 novel drugs approved last year; 41 the year before. As I write, there have only been 19 novel drugs approved in 2016—putting this on track to be the worst year since 2007. This isn’t necessarily the FDA’s fault—they can only approve the applications these receive…and some would argue that the agency has, if anything, been overly lenient in granting approvals this year. #8: Lots of big clinical failures. While 2016 has certainly had its bright spots, the year has been more notable for high-pro failures than for its successes. There’s BioMarin’s drisapersen, Celldex Therapeutics’ Rintega, Eli Lilly’s solenuzumab, Alnylam’s Revusiran, Clovis Oncology’s rociletinib, and Bristol Myers-Squibb’s Opdivo in lung cancer. Juno Therapeutics has run into some serious, perhaps program-ending difficulties with JCAR-015. Gilead has had a bad run of luck with almost everything it touched this year, from GS-5745 (in ulcerative colitis) to simtuzumab to eleclazine to Zydelig (in first-line cancer applications). Bluebird Bio went from hot to not after turning out disappointing early results in its sickle cell programs. There have been some great achievements (see below)—but it’s hard to counter-balance this depressing list. #7: The drug price debate continues, then stops, then starts up again. Drug companies always make juicy political targets, so it’s no surprise that the heat stayed high all during this election year. It’s been a debate long on rhetoric and short on substance, with the main result being that companies grew more eager to get in price increases before the music stopped. Some, of course, were a little more ham-fisted about than others (cough, Mylan ). Pharma investors breathed a sigh of relief after the election of Donald Trump (see point #1 below), but that sense of resolution may have come too early. Also, don’t forget about some of the most visible faces of price-gouging— Valeant subsidiary Philidor and its CEO have had criminal charges filed against them, and there may be more to come. Martin Shkreli is guaranteed to be back in the news in 2017, since that’s when his criminal fraud trial is likely to take place. #6: M&A slowed to a comparative crawl. 2015 was a record-breaking year for biopharma M&A, with some $330 billion in deals, even after you factor out the $183 billion Pfizer - Allergan link-up that never happened. Few expected this year to match that sum, but fewer still expected the totals to drop so sharply. The final tallies won’t be in until the New Year, but 2016 was recently running under $100 billion in pharma and biotech M&A. Will a flood of repatriated cash, courtesy of a new Trump tax policy, change the calculus in 2017? I have my doubts (and not only because it will take a while to change the tax code, even with a willing Congress). But it wouldn’t be surprising to see the pace pick up at least a little next year. #5: Market meltdown. The “Trump bump” to the stock market—and the biotech market in particular—was nice for investors while it lasted. Even at its best, it did little to erase what happened in the opening weeks of 2016. As we stand now, the Nasdaq Biotech Index, up less than 2 percent since the election. It is down over 20 percent year-to-date. A number of other points in this list help explain why. #4: The (controversial) rise of antisense. Antisense has been kicking around since the 1980s without much commercial success. While that technically continued to be true this year, it’s about to change. Spinraza, the antisense drug for spinal muscular atrophy developed by Ionis Pharma and Biogen , produced strong enough results in a study of infantile onset spinal muscular atrophy that the trial was stopped early. Since then, robust signals have been seen in patients with later-onset disease. And the drug reportedly has a reasonably clean safety pro since side effects and safety concerns have dogged some other antisense drugs. Then there’s Sarepta’s eteplirsen, trade-named Exondys 51, approved to treat Duchenne muscular dystrophy is a specific subset of patients. The decision to approve was controversial and, according to some, undermined the credibility of the FDA. Certainly it remains unclear whether the drug’s miniscule effect on dystrophin production will create a meaningful change in the course of the disease. But that probably won’t stop it from racking up hundreds of millions of dollars in sales. #3: CAR-T meltdown? Cancer immunotherapy has been so hot over the past few years that some pundits have bemoaned a lack of research dollars going elsewhere. CAR-T seems like an obvious next step—a way to program T-cells to attack specific cancers. And early clinical results have shown astounding success, producing apparent cures in leukemia. But the therapy has turned out to be quite dangerous in some situations, dousing another fire that burned so bright for biotech in 2015. That’s been particularly true for Juno Therapeutics , which has put its pivotal trial of JCAR-015 on clinical hold twice. Novartis , once arguably the leader in the area, seemingly stepped back from CAR-T this past summer, dissolving its dedicated unit, bringing programs back into the larger organization and perhaps putting less emphasis on the technology (though they continue to push forward). Kite Pharma is the beneficiary of these developments, yet investors are regarding the company warily. The stock is down sharply for the year and well off its 52-week high even as it files for its first approval. Call it another case of hype waking up to reality: CAR-T remains a very promising technology, but it’s still unclear how effective it will be outside of blood cancers, and how it will be used even in leukemias, where oncologists will have to weigh up robust results against serious potential risks. #2: CRISPR goes public. At the start of the year, there were zero pure-play companies in the CRISPR space. Now there are three— Editas Medicine , Intellia Therapeutics , and CRISPR Therapeutics —not to mention a bunch more companies dabbling in the space. But these companies—which have had a mixed-at-best reception with investors—are only the tip of the iceberg, held back in part by complex and acrimonious intellectual property disputes. CRISPR has exploded around the world, with the University of Pennsylvania planning a seeming Hail Mary pass into clinical trials thanks to funding from the Parker Institute, only to be beaten to the punch by Sichuan University in China. Even without clinical trials, the technology is making all sorts of experiments possible—even if some raise safety or ethical issues. By this time next year, perhaps we’ll all have access to giant CRISPR beagles . #1: Trump elected president. This election upset takes the number one spot. But what it means for the biotech sector (or anything else) remains unclear. Trump has certainly been known to spout anti-science rhetoric and anti-vaxxer drivel. He’s said he wants to cut drug prices, using mechanisms like reimportation and direct Medicare negotiation. But then he went mum on those topics. And then he started up again, so who knows? He has said he wants to streamline FDA and get medicines to people more quickly, pushing a popular political hot button. But does that mean a bigger FDA budget, laxer standards, or something else? It seems likely, based on both his rhetoric and his choice of Rep. Tom Price (R-Ga.) as Secretary of Health and Human Services , that he plans to make good on his promise to repeal and replace Obamacare. Yet how will that play out? The Affordable Care Act has generally been popular with drug companies, because it has given them millions of new customers. But it has also come with new regulatory burdens, like requirements to compile and submit data to Patient Centered Outcomes Research Institutes. What is simply repealed and what is replaced will have a big impact on companies. Here’s another irony: One interesting impact of Obamacare is that it gives the president fairly broad authority to enact price controls when Medicare grows at a certain level beyond inflation—as it is expected to do in 2017 for the first time since the law was passed. So biopharma companies who’ve thus far seen the most favorable side of the law may be saved from its restrictions just before the hammer comes down—if Trump and Congress do indeed repeal. But maybe Trump will decide he likes the authority in the current law. However it goes down, it’s going to be an interesting 2017. - Karl Thiel Read the BioPharm Executive online newsletter December 14, 2016. Sign-up for the free monthly subscription to the BioPharm Executive Related Jobs VP, Clinical Development Director, Genomics VP, Clinical Development Director of Operations VP, Sales Director, Biostatistics View More Jobs

上市批准免疫疗法

100 项与 Rindopepimut 相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D09660	Rindopepimut	-	DB05374

研发状态

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
胶质母细胞瘤	临床3期	美国	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	澳大利亚	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	奥地利	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	比利时	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	巴西	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	加拿大	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	哥伦比亚	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	捷克	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	法国	Celldex Therapeutics, Inc.	2011-11-01
胶质母细胞瘤	临床3期	德国	Celldex Therapeutics, Inc.	2011-11-01

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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


NCT01498328 (ReACT, Pubmed \| Clin Cancer Res) 人工标引	临床2期	EGFR突变胶质母细胞瘤 EGFR Positive	73	bevacizumab+Rindopepimut	鏇簾網糧窪糧餘蓋遞憲(廠製廠觸憲淵鑰鬱鑰鬱) = 齋築積鏇鑰願壓鹽窪鹽廠製製鹹鑰膚顧窪衊窪 (繭窪製網艱鑰觸觸衊壓 ) 更多	积极	2020-04-01
				bevacizumab+keyhole limpet hemocyanin	鏇簾網糧窪糧餘蓋遞憲(廠製廠觸憲淵鑰鬱鑰鬱) = 鑰鏇夢鬱齋願選窪獵廠廠製製鹹鑰膚顧窪衊窪 (繭窪製網艱鑰觸觸衊壓 ) 更多
ACT IV (SNO2016)	临床3期	EGFR突变胶质母细胞瘤 EGFRvIII+	745	Rindopepimut	繭獵齋艱糧鹽壓糧鏇鹹(顧醖衊築憲構襯築鹹齋) = 廠淵鑰鑰築顧範構鹽繭網築艱艱鹽觸鹽糧遞淵 (鹹遞壓顧製廠齋簾淵蓋 ) 更多	不佳	2016-11-07
				Rindopepimut (Control (KLH))	繭獵齋艱糧鹽壓糧鏇鹹(顧醖衊築憲構襯築鹹齋) = 餘醖窪網獵選積膚選齋網築艱艱鹽觸鹽糧遞淵 (鹹遞壓顧製廠齋簾淵蓋 ) 更多
NCT01498328 (ReACT, ASCO2015)	临床2期	复发性胶质母细胞瘤	72	Rindopepimut plus bevacizumab	鹹艱鹹衊鹹鏇築艱鬱齋(憲觸繭襯選積繭蓋選選) = 齋淵遞壓蓋蓋鑰鹽憲醖範糧範壓壓夢壓衊壓壓 (願夢製廠襯淵網製衊淵 ) 更多	积极	2015-05-20
				Control (KLH) plus bevacizumab	鹹艱鹹衊鹹鏇築艱鬱齋(憲觸繭襯選積繭蓋選選) = 製製積襯簾廠繭膚遞壓範糧範壓壓夢壓衊壓壓 (願夢製廠襯淵網製衊淵 ) 更多
NCT01498328 (REACT, ASCO2012)	临床2期	复发性胶质母细胞瘤	127	Rindopepimut plus bevacizumab	膚遞壓願願鑰蓋襯願獵(廠獵窪襯範製鬱鬱壓膚) = 襯憲醖鏇鏇淵衊夢蓋膚蓋觸鬱齋範製餘範襯壓 (鑰窪窪蓋艱襯齋艱艱構 ) 更多	-	2012-05-20
				Control injection (low-dose KLH)	膚遞壓願願鑰蓋襯願獵(廠獵窪襯範製鬱鬱壓膚) = 憲膚廠製廠網選鹽夢淵蓋觸鬱齋範製餘範襯壓 (鑰窪窪蓋艱襯齋艱艱構 ) 更多
NCT00458601 (ACT III, ASCO2010)	临床2期	胶质母细胞瘤	81	PF-04948568	鹹襯淵醖醖網餘艱築餘(製積製衊願簾窪襯網艱) = 壓鹽蓋獵簾夢淵糧夢襯簾鑰鑰夢蓋觸顧遞壓廠 (淵鏇餘窪襯艱襯製顧齋, [53.5 ~ 83.4])	-	2010-05-20
ASCO2008	临床2期	多形性胶质母细胞瘤	21	EGFRvIII-specific peptide vaccine (CDX-110)	鏇繭齋鏇構繭願壓夢鏇(積鹹襯廠壓遞鑰蓋壓觸) = 窪艱襯廠鏇構遞製窪餘願積蓋壓範選獵襯繭憲 (廠窪廠廠鏇構顧鏇願願 ) 更多	-	2008-05-20