Combined immunostimulatory monoclonal antibodies extend survival in an aggressive transgenic hepatocellular carcinoma mouse model

Morales-KastresanaA.; SanmamedM.F.; RodriguezI.; PalazonA.; Martinez-ForeroI.; LabianoS.; Hervas-StubbsS.; SangroB.; OchoaC.; RouzautA.; AzpilikuetaA.; Bola?osE.; Jure-KunkelM.; GütgemannI.; MeleroI.

首页> 外文期刊>Clinical cancer research: an official journal of the American Association for Cancer Research >Combined immunostimulatory monoclonal antibodies extend survival in an aggressive transgenic hepatocellular carcinoma mouse model

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Combined immunostimulatory monoclonal antibodies extend survival in an aggressive transgenic hepatocellular carcinoma mouse model

机译：联合免疫刺激单克隆抗体在侵袭性转基因肝细胞癌小鼠模型中延伸存活

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Purpose: Immunostimulatory monoclonal antibodies (ISmAb) that unleash antitumor immune responses are showing efficacy in cancer clinical trials. Anti-B7-H1 (PD-L1) monoclonal antibodies (mAb) block a critical inhibitory pathway in T cells, whereas anti-CD137 and OX40 mAbs provide T-cell costimulation. A combination of these ISmAbs (anti-CD137 + anti-OX40 + anti-B7-H1) was tested using a transgenic mouse model of multifocal and rapidly progressing hepatocellular carcinoma, in which c-myc drives transformation and cytosolic ovalbumin (OVA) is expressed in tumor cells as a model antigen. Experimental Design: Flow-cytometry and immunohistochemistry were used to quantify tumorinfiltrating lymphocytes (TIL) elicited by treatment and assess their activation status and cytolytic potential. Tolerance induction and its prevention/reversal by treatment with the combination of ISmAbs were revealed by in vivo killing assays. Results: The triple combination of ISmAbs extended survival of mice bearing hepatocellular carcinomas in a CD8-dependent fashion and synergized with adoptive T-cell therapy using activated OVA-specific TCR-transgenic OT-1 and OT-2 lymphocytes. Mice undergoing therapy showed clear increases in tumor infiltration by activated and blastic CD8+ and CD4+ T lymphocytes containing perforin/granzyme B and expressing the ISmAb-targeted receptors on their surface. The triple combination of ISmAbs did not result in enhanced OVA-specific cytotoxic T lymphocyte (CTL) activity but other antigens expressed by cell lines derived from such hepatocellular carcinomas were recognized by endogenous TILs. Adoptively transferred OVA-specific OT-1 lymphocytes into tumor-bearing mice were rendered tolerant, unless given the triple mAb therapy. Conclusion: Extension of survival and dense T-cell infiltrates emphasize the translational potential of combinational immunotherapy strategies for hepatocellular carcinoma.

机译：目的：免疫刺激单克隆抗体（ISMAB）释放抗肿瘤免疫应答在癌症临床试验中显示出疗效。抗B7-H1（PD-L1）单克隆抗体（MAB）阻断T细胞中的临界抑制途径，而抗CD137和OX40 MAb提供T细胞的刺激。使用多灶性小鼠模型测试这些ISMABs（抗CD137 +抗OX40 +抗B7-H1）的组合，并迅速进展肝细胞癌，其中C-MYC驱动变换和细胞溶质卵磷蛋白（OVA）表示在肿瘤细胞作为模型抗原。实验设计：流动细胞术和免疫组化用于量化通过处理引发的肿瘤滤虫淋巴细胞（TIL），评估其活化状态和细胞溶解潜力。通过体内杀伤测定揭示了通过与ISMAB组合的治疗进行耐受性诱导及其预防/逆转。结果：Ismabs三重组合在CD8依赖性时装中携带肝细胞癌携带肝细胞癌的小鼠存活，并通过使用活化的OVA特异性TCR转基因OT-1和OT-2淋巴细胞来协同效应。接受治疗的小鼠通过含有穿孔素/颗粒酶B的活化和爆炸性CD8 +和CD4 + T淋巴细胞的肿瘤渗透和CD4 + T淋巴细胞呈显然增加，并在其表面上表达ISMAB靶向受体。 Ismabs的三重组合未导致增强的卵子特异性细胞毒性T淋巴细胞（CTL）活性，但是通过内源直线识别出由这些肝细胞癌的细胞系表达的其他抗原。除非给予三重MAB疗法，否则将普通的转移的OVA特异性OT-1淋巴细胞含有耐受性的肿瘤小鼠。结论：延长存活和致密T细胞渗透强调肝细胞癌组合免疫疗法策略的平移潜力。

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《Clinical cancer research: an official journal of the American Association for Cancer Research 》 |2013年第22期| 共12页
作者
Morales-KastresanaA.; SanmamedM.F.; RodriguezI.; PalazonA.; Martinez-ForeroI.; LabianoS.; Hervas-StubbsS.; SangroB.; OchoaC.; RouzautA.; AzpilikuetaA.; Bola?osE.; Jure-KunkelM.; GütgemannI.; MeleroI.;
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Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Department of Oncology Clinica Universidad de Navarra Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Liver Unit Clínica Universidad de Navarra Centro de Investigacion Biomedica en Red de;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

Oncology Drug Discovery Division Bristol-Myers Squibb Lawrenceville NJ United States;

Department of Pathology University of Bonn Bonn Germany;

Centro de Investigacion Medica Aplicada (CIMA) Universidad de Navarra 55 31008 Pamplona Spain;

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专利

1. Combined immunostimulatory monoclonal antibodies extend survival in an aggressive transgenic hepatocellular carcinoma mouse model [J] . Morales-KastresanaA., SanmamedM.F., RodriguezI., Clinical cancer research: an official journal of the American Association for Cancer Research . 2013 ,第22期

机译：联合免疫刺激单克隆抗体在侵袭性转基因肝细胞癌小鼠模型中延伸存活
2. Targeting vascular endothelial growth factor with the monoclonal antibody bevacizumab inhibits human hepatocellular carcinoma cells growing in an orthotopic mouse model. [J] . Finn RS, Bentley G, Britten CD, Liver international : . 2009 ,第2期

机译：用单克隆抗体贝伐单抗靶向血管内皮生长因子可抑制在原位小鼠模型中生长的人肝癌细胞。
3. Combined serum and tissue proteomic study applied to a c-Myc transgenic mouse model of hepatocellular carcinoma identified novel disease regulated proteins suitable for diagnosis and therapeutic intervention strategies [J] . Ritorto M.S., Borlak J. Journal of proteome research . 2011 ,第7期

机译：血清和组织蛋白质组学联合研究应用于肝细胞癌c-Myc转基因小鼠模型，确定了适用于诊断和治疗干预策略的新型疾病调控蛋白
4. An Envelop-Type Gene Nanocomplex with Encapsulated Monoclonal Antibodies for Target Therapy of Hepatocellular Carcinoma [C] . Wang Jinlei, Shen Jie, Hu Qinglian, World biomaterials congress . 2012

机译：信封型基因纳米复合物与封装的单克隆抗体对肝细胞癌的靶向治疗
5. New therapeutics for hepatocellular carcinoma using the C3HeB/FeJ mouse model [D] . Zavadil, Jessica Ann. 2016

机译：使用C3HEB / FEJ小鼠模型的肝细胞癌新治疗方法
6. Therapeutic activity of a combination of immunostimulatory monoclonal antibodies (anti-B7-H1 CD137 and OX40) on a c-myc-driven spontaneous transgenic model of hepatocellular carcinoma [O] . Aizea Morales-Kastresana, Sanmamed F Miguel, Inmaculada Rodriguez, 2013

机译：免疫刺激性单克隆抗体（抗B7-H1CD137和OX40）组合对c-myc驱动的肝细胞癌自发转基因模型的治疗活性
7. Combined Immunostimulatory Monoclonal Antibodies Extend Survival in an Aggressive Transgenic Hepatocellular Carcinoma Mouse Model [O] . Aizea Morales-Kastresana, Miguel F. Sanmamed, Inmaculada Rodriguez, 2013

机译：联合免疫刺激单克隆抗体在侵袭性转基因肝细胞癌小鼠模型中延伸存活

Combined immunostimulatory monoclonal antibodies extend survival in an aggressive transgenic hepatocellular carcinoma mouse model

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