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Synthetic integrin-binding immune stimulators target cancer cells and prevent tumor formation

机译:合成整联蛋白结合免疫刺激剂靶向癌细胞并防止肿瘤形成

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Immuno-oncology approaches mainly utilize monoclonal antibodies or protein-based scaffolds that bind with high affinity to cancer cells and can generate an immune response. Peptides can also bind with high affinity to cancer cells and are intermediate in size between antibodies and small molecules. They are also synthetically accessible and therefore easily modified to optimize their stability, binding affinity and selectivity. Here we describe the design of immune system engagers (ISErs), a novel class of synthetic peptide-based compounds that bind specifically to cancer cells and stimulate the immune system. A prototype, Y9, targets integrin α3, which is overexpressed on several cancer cells, and activates the immune system via a formyl methionine-containing effector peptide. Injection of Y9 leads to immune cell infiltration into tissue and prevents tumor formation in a guinea pig model. The anti-tumor activity and synthetic accessibility of Y9 illustrate that ISErs could be applied to a wide variety of targets and diseases.
机译:免疫肿瘤学方法主要利用与癌细胞具有高亲和力的单克隆抗体或基于蛋白质的支架,并可以产生免疫反应。肽还可以与癌细胞高亲和力结合,并且大小介于抗体和小分子之间。它们也可通过合成途径获得,因此易于修饰以优化其稳定性,结合亲和力和选择性。在这里,我们描述了免疫系统接合剂(ISErs)的设计,这是一类新型的基于合成肽的化合物,可特异性结合癌细胞并刺激免疫系统。 Y9原型针对整合素α3,整合素α3在几种癌细胞中过表达,并通过含甲硫甲硫氨酸的效应肽激活免疫系统。注射Y9导致免疫细胞浸润到组织中并防止在豚鼠模型中形成肿瘤。 Y9的抗肿瘤活性和合成可及性说明ISErs可应用于多种靶标和疾病。

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