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溶酶体靶向 DNA 纳米器件选择性靶向巨噬细胞以减弱肿瘤。

A lysosome-targeted DNA nanodevice selectively targets macrophages to attenuate tumours.

机构信息

Committee on Cancer Biology, The University of Chicago, Chicago, IL, USA.

Ben May Department for Cancer Research, The University of Chicago, Chicago, IL, USA.

出版信息

Nat Nanotechnol. 2021 Dec;16(12):1394-1402. doi: 10.1038/s41565-021-00988-z. Epub 2021 Nov 11.

Abstract

Activating CD8 T cells by antigen cross-presentation is remarkably effective at eliminating tumours. Although this function is traditionally attributed to dendritic cells, tumour-associated macrophages (TAMs) can also cross-present antigens. TAMs are the most abundant tumour-infiltrating leukocyte. Yet, TAMs have not been leveraged to activate CD8 T cells because mechanisms that modulate their ability to cross-present antigens are incompletely understood. Here we show that TAMs harbour hyperactive cysteine protease activity in their lysosomes, which impedes antigen cross-presentation, thereby preventing CD8 T cell activation. We developed a DNA nanodevice (E64-DNA) that targets the lysosomes of TAMs in mice. E64-DNA inhibits the population of cysteine proteases that is present specifically inside the lysosomes of TAMs, improves their ability to cross-present antigens and attenuates tumour growth via CD8 T cells. When combined with cyclophosphamide, E64-DNA showed sustained tumour regression in a triple-negative-breast-cancer model. Our studies demonstrate that DNA nanodevices can be targeted with organelle-level precision to reprogram macrophages and achieve immunomodulation in vivo.

摘要

通过抗原交叉呈递激活 CD8 T 细胞在消除肿瘤方面非常有效。尽管这种功能传统上归因于树突状细胞,但肿瘤相关巨噬细胞(TAMs)也可以交叉呈递抗原。TAMs 是最丰富的肿瘤浸润白细胞。然而,由于调节其抗原交叉呈递能力的机制尚未完全了解,因此尚未利用 TAMs 来激活 CD8 T 细胞。在这里,我们表明 TAMs 溶酶体中存在过度活跃的半胱氨酸蛋白酶活性,这会阻碍抗原交叉呈递,从而阻止 CD8 T 细胞的激活。我们开发了一种 DNA 纳米器件(E64-DNA),可在小鼠中靶向 TAMs 的溶酶体。E64-DNA 抑制了 TAMs 溶酶体中特异性存在的半胱氨酸蛋白酶群体,提高了它们交叉呈递抗原的能力,并通过 CD8 T 细胞减弱肿瘤生长。当与环磷酰胺联合使用时,E64-DNA 在三阴性乳腺癌模型中显示出持续的肿瘤消退。我们的研究表明,DNA 纳米器件可以针对细胞器水平进行精确靶向,以重新编程巨噬细胞并在体内实现免疫调节。

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