Reducing toxicity of 4-1BB costimulation: targeting 4-1BB ligands to the tumor stroma with bi-specific aptamer conjugates

Schrand B.; Berezhnoy A.; Brenneman R.; Williams A.; Levay A.; Gilboa E.

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Reducing toxicity of 4-1BB costimulation: targeting 4-1BB ligands to the tumor stroma with bi-specific aptamer conjugates

机译：降低4-1BB共刺激的毒性：使用双特异性适体偶联物靶向4-1BB配体靶向肿瘤基质

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Systemic administration of immune modulatory antibodies to cancer patients is associated with autoimmune pathologies. We have developed a clinically feasible and broadly applicable approach to limit immune stimulation to disseminated tumor lesions using a bi-specific agonistic 4-1BB oligonucleotide aptamer targeted to a broadly expressed stromal product (e.g., VEGF or osteopontin). The stroma-targeted aptamer conjugates engendered potent antitumor immunity against unrelated tumors and exhibited a superior therapeutic index compared to non-targeted agonistic 4-1BB antibody.

机译：免疫调节抗体对癌症患者的全身给药与自身免疫病理相关。我们已经开发出一种临床上可行且广泛适用的方法，可使用针对广泛表达的基质产物（例如VEGF或骨桥蛋白）的双特异性激动剂4-1BB寡核苷酸适体来限制免疫刺激扩散的肿瘤病变。与非靶向激动剂4-1BB抗体相比，以基质靶向的适体偶联物可产生针对无关肿瘤的有效抗肿瘤免疫力，并显示出更高的治疗指数。

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《Oncoimmunology.》 |2015年第3期|共3页
作者
Schrand B.; Berezhnoy A.; Brenneman R.; Williams A.; Levay A.; Gilboa E.;
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原文格式 PDF
正文语种 eng
中图分类肿瘤学;
关键词
cancer immunotherapy; immune stimulation; autoimmune pathology; 4-1BB; tumor stroma; VEGF; tumor targeting;

机译：癌症免疫疗法;免疫刺激;自身免疫病理;4-1BB;肿瘤基质;VEGF;肿瘤靶向;

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1. Reducing toxicity of 4-1BB costimulation: targeting 4-1BB ligands to the tumor stroma with bi-specific aptamer conjugates [J] . Schrand B., Berezhnoy A., Brenneman R., Oncoimmunology. . 2015,第3期

机译：降低4-1BB共刺激的毒性：使用双特异性适体偶联物靶向4-1BB配体靶向肿瘤基质
2. Targeting 4-1BB Costimulation to the Tumor Stroma with Bispecific Aptamer Conjugates Enhances the Therapeutic Index of Tumor Immunotherapy [J] . Brett Schrand, Alexey Berezhnoy, Randall Brenneman, Cancer immunity . 2014,第9期

机译：靶向4-1BB共刺激对双特异性适体缀合物的肿瘤基质增强了肿瘤免疫治疗的治疗指数。
3. Targeting 4-1BB costimulation to disseminated tumor lesions with bi-specific oligonucleotide aptamers. [J] . Pastor F, Kolonias D, McNamara JO 2nd, Molecular therapy: the journal of the American Society of Gene Therapy . 2011,第10期

机译：使用双特异性寡核苷酸适体将4-1BB共刺激靶向扩散的肿瘤病变。
4. Modulation of Tumor Cytotoxicity and Targeting Selectivity of Nanocarriers via a Dual Ligand Targeting Approach [C] . Justin M. Saul, Ananth V. Annapragada, Ravi V. Bellamkonda Society for Biomaterials Transaction Annual Meeting vol.29 pt.1; 20060426-29; Pittsburgh,PA(US) . 2006

机译：通过双重配体靶向方法调节肿瘤细胞毒性和纳米载体的靶向选择性
5. 4-1BB Costimulation Ameliorates T Cell Exhaustion Induced by Antigen Independent Signaling of Chimeric Antigen Receptors [D] . Long, Adrienne Hart 2015

机译：4-1BB共刺激可改善嵌合抗原受体的抗原独立信号转导所致的T细胞衰竭。
6. Reducing toxicity of 4–1BB costimulation: targeting 4–1BB ligands to the tumor stroma with bi-specific aptamer conjugates [O] . B Schrand, A Berezhnoy, R Brenneman, 2015

机译：降低4–1BB共刺激的毒性：使用双特异性适体偶联物将4–1BB配体靶向肿瘤基质
7. Targeting 4-1BB Costimulation to the Tumor Stroma with Bispecific Aptamer Conjugates Enhances the Therapeutic Index of Tumor Immunotherapy [O] . Brett Schrand, Alexey Berezhnoy, Randall Brenneman, 2014

机译：用双特异性适体缀合物靶向4-1BB的肿瘤基质刺激增强了肿瘤免疫疗法的治疗指数

Reducing toxicity of 4-1BB costimulation: targeting 4-1BB ligands to the tumor stroma with bi-specific aptamer conjugates

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