Cancer immunogenic cell death via pyroptosis with CXCR4-targeted nanotoxins in hepatocellular carcinoma.

IF 4.3 3区工程技术 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY

Frontiers in Bioengineering and Biotechnology Pub Date : 2024-11-04 eCollection Date: 2024-01-01 DOI:10.3389/fbioe.2024.1433126

Yingbin Huang, Yihu Li, Rui He, Shuyi Dong, Zheng Zhao, Xingyuan Jiao

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引用次数: 0

Abstract

Introduction: Cytotoxic agents have shown limited benefits in hepatocellular carcinoma (HCC), mediated in part by the lack of targeting. As cell-penetrating peptides (CPPs) are capable of delivering various biologically active molecules into cells, including protein, peptides, small chemo-drugs, and nucleic acid with or without targeting, we developed T22-PE24, a CXCR4-targeted self-assembling cytotoxic nanotoxin, to effectively induce HCC pyroptosis.

Methods: T22 incorporating enhanced green fluorescent protein (EGFP) or PE24 was purified from DE3 bacterial cells and characterized using transmission electron microscopy, the Zetasizer Nano^®, and SEC-HPLC. The internalization effect of T22-EGFP was detected by flow cytometry system (FCS) in CXCR4⁺/LM3(^CXCR4-) HCC cells. The CCK8, lactate dehydrogenase (LDH) release, Western blot, and nude mice HCC models were used to estimate the cell viability of T22-PE24. The complete-immunity HCC tumor-bearing mice model was used to assess the immune response of T22-PE24.

Results: The round shape under transmission electron microscopy, 49.4 nm hydrodynamic diameter, and -33.33 mV zeta potential indicated that T22-PE24 self-assembled into nanoparticles. T22 incorporating EGFP selectively internalized in CXCR4⁺ HCC cells and showed no accumulation in CXCR4-knockout HCC cells. The T22-PE24 nanotoxin induced HCC pyroptosis via the caspase-3/GSDME signaling pathway and suppressed tumor growth in the absence of histological alterations in normal organs. Using the complete-immunity HCC tumor-bearing mice model, we found that T22-PE24 nanotoxin effectively induces the global reprogramming of cell components of the immune tumor microenvironment, leading to enhanced antitumor effects compared to those observed in immunodeficient mice.

Conclusion: Our findings demonstrate the activation of the innate immune response in HCC by inducing pyroptosis with T22-PE24 nanotoxin treatment and support an implementation of this strategy for HCC treatment.

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在肝细胞癌中使用 CXCR4 靶向纳米毒素，通过热解作用使癌症免疫细胞死亡。

简介：细胞毒性药物对肝细胞癌（HCC）的治疗效果有限，部分原因是缺乏靶向性。由于细胞穿透肽（CPPs）能够将各种生物活性分子（包括蛋白质、肽、小化疗药物和核酸）靶向或非靶向地送入细胞，因此我们开发了一种CXCR4靶向的自组装细胞毒性纳米毒素T22-PE24，以有效诱导HCC发生热休克：从DE3细菌细胞中纯化出含有增强型绿色荧光蛋白（EGFP）或PE24的T22，并使用透射电子显微镜、Zetasizer Nano®和SEC-HPLC对其进行表征。流式细胞仪系统（FCS）检测了 T22-EGFP 在 CXCR4+/LM3(CXCR4-) HCC 细胞中的内化效应。利用CCK8、乳酸脱氢酶（LDH）释放、Western blot和裸鼠HCC模型来评估T22-PE24的细胞活力。完全免疫 HCC 肿瘤小鼠模型用于评估 T22-PE24 的免疫反应：结果：透射电子显微镜下T22-PE24呈圆形，流体力学直径为49.4 nm，ZETA电位为-33.33 mV。加入 EGFP 的 T22 在 CXCR4+ HCC 细胞中选择性内化，而在 CXCR4 基因敲除的 HCC 细胞中则无积累。T22-PE24纳米毒素通过caspase-3/GSDME信号通路诱导HCC发生热休克，并抑制肿瘤生长，而正常器官没有组织学改变。利用完全免疫HCC肿瘤小鼠模型，我们发现T22-PE24纳米毒素能有效诱导免疫肿瘤微环境细胞成分的整体重编程，从而导致比在免疫缺陷小鼠中观察到的更强的抗肿瘤效果：我们的研究结果表明，T22-PE24 纳米毒素可通过诱导热蛋白沉积激活 HCC 的先天性免疫反应，并支持将这一策略用于 HCC 治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Frontiers in Bioengineering and Biotechnology Chemical Engineering-Bioengineering

CiteScore

8.30

自引率

5.30%

发文量

2270

审稿时长

12 weeks

期刊介绍： The translation of new discoveries in medicine to clinical routine has never been easy. During the second half of the last century, thanks to the progress in chemistry, biochemistry and pharmacology, we have seen the development and the application of a large number of drugs and devices aimed at the treatment of symptoms, blocking unwanted pathways and, in the case of infectious diseases, fighting the micro-organisms responsible. However, we are facing, today, a dramatic change in the therapeutic approach to pathologies and diseases. Indeed, the challenge of the present and the next decade is to fully restore the physiological status of the diseased organism and to completely regenerate tissue and organs when they are so seriously affected that treatments cannot be limited to the repression of symptoms or to the repair of damage. This is being made possible thanks to the major developments made in basic cell and molecular biology, including stem cell science, growth factor delivery, gene isolation and transfection, the advances in bioengineering and nanotechnology, including development of new biomaterials, biofabrication technologies and use of bioreactors, and the big improvements in diagnostic tools and imaging of cells, tissues and organs. In today`s world, an enhancement of communication between multidisciplinary experts, together with the promotion of joint projects and close collaborations among scientists, engineers, industry people, regulatory agencies and physicians are absolute requirements for the success of any attempt to develop and clinically apply a new biological therapy or an innovative device involving the collective use of biomaterials, cells and/or bioactive molecules. “Frontiers in Bioengineering and Biotechnology” aspires to be a forum for all people involved in the process by bridging the gap too often existing between a discovery in the basic sciences and its clinical application.