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Redirecting natural killer cells to potentiate adoptive immunotherapy in solid tumors through stabilized Y-type bispecific aptamer

机译:将加强自然杀伤细胞在实体肿瘤过继免疫治疗稳定的引水系统双特异性适配子

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摘要

Modulating interactions between immune effector cells and tumor cells in vivo using a bispecific aptamer (Ap) is a promising strategy for cancer immunotherapy. However, it remains a technical challenge owing to the complex and dynamic internal environment accompanied by severe degradation. Herein, by using a Y-shaped DNA scaffold, a bispecific and stabilized Y-type Ap is designed to redirect natural killer (NK) cells to enhance adoptive immunotherapy of hepatocellular carcinoma (HCC) solid tumors. Y-type Ap is constituted by the HCC-specific Ap TLS11a linked with the CD16-specific Ap through a Y-shaped DNA scaffold. Owing to the rigid structure, Y-type Ap shows high stability in 10% serum for over 72 h and resistance to denaturation by 8 M urea. Additionally, the Y-type Ap exhibits more potent avidity to bind with NK cells and tumor cells both in vitro and in vivo, resulting in higher cytokine secretion and excellent antitumor efficiency. Collectively, this study offers a translational platform for constructing stable bispecific Ap, offering considerable potential to enhance adoptive immunotherapy of solid tumors.
机译:调节免疫效应之间的相互作用使用双特异性细胞和肿瘤细胞体内适配子(美联社)是一种针对癌症的有前途的战略免疫疗法。由于复杂和动态的挑战伴随着严重的内部环境退化。支架、双特异性和稳定引水美联社旨在改变自然杀伤(NK)细胞增强的过继免疫治疗肝细胞癌(HCC)实体肿瘤。引水系统由HCC-specific美联社Ap是构成TLS11a CD16-specific美联社通过一个链接y形DNA支架。结构、引水系统Ap显示高稳定在10%血清了72 h和阻力由8 M尿素变性。引水系统美联社展品贪欲将更有效NK细胞和肿瘤细胞在体外和体内,导致更高的细胞因子的分泌和优秀的抗肿瘤的效率。这项研究提供了一种转化平台构建稳定的双特异性美联社,祭相当大的潜力,增强收养实体肿瘤的免疫治疗。

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