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氧化石墨烯通过上调颗粒酶 B 的表达激活 B 细胞:其免疫调节特性和抗癌活性的单细胞水平证据。

Graphene oxide activates B cells with upregulation of granzyme B expression: evidence at the single-cell level for its immune-modulatory properties and anticancer activity.

机构信息

Department of Chemistry and Pharmacy University of Sassari, Sassari, Italy.

Department of Immunology, Cancer Program, Sidra Medicine, Education City, Doha, Qatar.

出版信息

Nanoscale. 2022 Jan 6;14(2):333-349. doi: 10.1039/d1nr04355b.

Abstract

We recently found by single-cell mass cytometry that human B cells internalize graphene oxide (GO). The functional impact of such uptake on B cells remains unexplored. Here, we disclosed the effects of GO and amino-functionalized GO (GONH) interacting with human B cells and at the protein and gene expression levels. Moreover, our study considered three different subpopulations of B cells and their functionality in terms of: (i) cytokine production, (ii) activation markers, (iii) killing activity towards cancer cells. Single-cell mass cytometry screening revealed the higher impact of GO on cell viability towards naïve, memory, and plasma B cell subsets. Different cytokines such as granzyme B (GrB) and activation markers, like CD69, CD80, CD138, and CD38, were differently regulated by GONH compared to GO, supporting possible diverse B cell activation paths. Moreover, co-culture experiments also suggest the functional ability of both GOs to activate B cells and therefore enhance the toxicity towards HeLa cancer cell line. Complete transcriptomic analysis on a B cell line highlighted the distinctive GO and GONH elicited responses, inducing pathways such as B cell receptor and CD40 signaling pathways, key players for GrB secretion. B cells were regularly left behind the scenes in graphene biological studies; our results may open new horizons in the development of GO-based immune-modulatory strategies having B cell as main actors.

摘要

我们最近通过单细胞质谱流式细胞术发现,人类 B 细胞内吞氧化石墨烯(GO)。这种摄取对 B 细胞的功能影响尚未得到探索。在这里,我们揭示了 GO 和氨基功能化 GO(GONH)与人 B 细胞相互作用的蛋白质和基因表达水平上的影响。此外,我们的研究考虑了 B 细胞的三个不同亚群及其功能,包括:(i)细胞因子产生,(ii)激活标志物,(iii)对癌细胞的杀伤活性。单细胞质谱流式细胞术筛选显示,GO 对幼稚、记忆和浆细胞 B 细胞亚群的细胞活力影响更大。与 GO 相比,GONH 对不同的细胞因子(如颗粒酶 B(GrB)和激活标志物,如 CD69、CD80、CD138 和 CD38)的调节不同,这支持了可能的不同 B 细胞激活途径。此外,共培养实验还表明,两种 GO 都具有激活 B 细胞的功能,从而增强对 HeLa 癌细胞系的毒性。B 细胞系的全转录组分析突出了 GO 和 GONH 引发的不同反应,诱导了 B 细胞受体和 CD40 信号通路等途径,这些途径是 GrB 分泌的关键。在石墨烯生物学研究中,B 细胞通常被置于幕后;我们的结果可能为以 B 细胞为主要作用物的基于 GO 的免疫调节策略的发展开辟新的前景。

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