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Genetically Engineered Cell-Derived Nanoparticles for Targeted Breast Cancer Immunotherapy

机译:基因工程型细胞衍生的纳米颗粒用于靶向乳腺癌免疫疗法

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摘要

Exosomes are nanosized membranous vesicles secreted by a variety of cells. Due to their unique and pharmacologically important properties, cell-derived exosome nanoparticles have drawn significant interest for drug development. By genetically modifying exosomes with two distinct types of surface-displayed monoclonal antibodies, we have developed an exosome platform termed synthetic multivalent antibodies retargeted exosome (SMART-Exo) for controlling cellular immunity. Here, we apply this approach to human epidermal growth factor receptor 2 (HER2)-expressing breast cancer by engineering exosomes through genetic display of both anti-human CD3 and anti-human HER2 antibodies, resulting in SMART-Exos dually targeting T cell CD3 and breast cancer-associated HER2 receptors. By redirecting and activating cytotoxic T cells toward attacking HER2-expressing breast cancer cells, the designed SMART-Exos exhibited highly potent and specific anti-tumor activity both in vitro and in vivo. This work demonstrates preclinical feasibility of utilizing endogenous exosomes for targeted breast cancer immunotherapy and the SMART-Exos as a broadly applicable platform technology for the development of next-generation immuno-nanomedicines.
机译:外泌体是由多种细胞分泌的纳米膜囊泡。由于它们独特而药理学上重要的性质,细胞衍生的外渗纳米粒子对药物发育产生了显着的兴趣。通过遗传修饰具有两种不同类型的表面显示的单克隆抗体的外泌体,我们开发出一种鼻孔平台,其称为用于控制细胞免疫的外泌体(Smart-EXO)。在此,我们通过抗人CD3和抗人类HER2抗体的遗传显示,将这种方法应用于人表皮生长因子受体2(HER2) - 通过工程外来进行乳腺癌,导致智能外部靶向T细胞CD3和乳腺癌相关的Her2受体。通过重定向和激活细胞毒性T细胞攻击攻击Her2表达Her2表达的乳腺癌细胞,设计的智能外壳在体外和体内表现出高度有效和特异性的抗肿瘤活性。这项工作展示了利用具有靶向乳腺癌免疫疗法的内源外泌体和智能外部的临床前可行性,作为广泛适用的平台技术,用于开发下一代免疫纳米胺。

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