槲寄生（Viscum album L.）发酵提取物在体外诱导内质网应激导致免疫原性细胞死亡的标志物。

IF 3.3 2区医学 Q1 INTEGRATIVE & COMPLEMENTARY MEDICINE

BMC Complementary Medicine and Therapies Pub Date : 2025-05-14 DOI:10.1186/s12906-025-04909-8

Ulrike Weissenstein, Sibylle Tschumi, Bettina Leonhard, Stephan Baumgartner

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引用次数: 0

摘要

背景：免疫逃避是癌症的特征标志。免疫疗法旨在激活和支持人体的免疫系统来识别和对抗肿瘤细胞。诱导免疫原性细胞死亡（ICD）和相关危险信号通路的激活可以增加肿瘤细胞的免疫原性。治疗性ICD刺激激活内质网应激途径和细胞凋亡，导致细胞表达损伤相关分子模式（DAMPs）。本实验旨在探讨槲寄生提取物是否能诱导肿瘤细胞免疫原性死亡。方法：将3株人乳腺癌细胞株（SKBR3、MDA-MB-231、MCF-7、B16F10）和1株小鼠黑色素瘤细胞株（SKBR3、MDA-MB-231、MCF-7、B16F10）分别用发酵后的visum提取物（VAE: Iscador Qu spec.）和紫杉醇或tunicamycin作为阳性对照进行处理。为了研究VAE是否诱导了核素毒性应激，我们采用Western blot方法检测了内质网应激调节因子p-eIF2a、ATF4和CHOP。流式细胞术检测细胞表面暴露的DAMPs（钙网蛋白、热休克蛋白hsp70和hsp90）、细胞凋亡和线粒体活性氧（ROS）诱导情况。采用酶联免疫吸附法和化学发光法分别测定HMGB1和ATP含量。结果：VAE可导致所有肿瘤细胞系eIF2α磷酸化，并增加凋亡前SKBR3乳腺癌和B16F10小鼠黑色素瘤细胞表面钙网蛋白（CRT）暴露量。VAE在所有细胞系中均表现出浓度依赖效应，导致早期凋亡细胞表面三种DAMPs （CRT、hsp70和hsp90）暴露量显著增加。此外，VAE提高了线粒体ROS的产生和ATP的释放。HMGB1释放不受VAE诱导。结论：在这项体外研究中，我们首次证明了槲寄生提取物诱导免疫原性癌细胞死亡替代标志物的潜力。这是研究VAEs促进icd诱导的肿瘤特异性免疫激活的潜力的第一步。

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A fermented Mistletoe (Viscum album L.) extract elicits markers characteristic for immunogenic cell death driven by endoplasmic reticulum stress in vitro.

Background: Immune evasion is a characteristic hallmark of cancer. Immunotherapies aim to activate and support the body's immune system to recognize and fight tumor cells. Induction of immunogenic cell death (ICD) and the associated activation of danger signaling pathways can increase the immunogenicity of tumor cells. Therapeutic ICD stimuli activate endoplasmic reticulum stress pathways and apoptosis leading to the cellular expression of damage-associated molecular patterns (DAMPs). The aim of our in vitro study was to investigate whether mistletoe extracts induce characteristics of immunogenic tumor cell death in cancer cell lines.

Methods: Three human breast cancer cell lines and one murine melanoma cell line (SKBR3, MDA-MB-231, MCF-7, and B16F10) were treated with aqueous, fermented Viscum album extract (VAE: Iscador Qu spec.) and taxol or tunicamycin as positive controls, respectively. To investigate whether VAE induces ribotoxic stress, we measured the ER stress regulators p-eIF2a, ATF4, and CHOP by Western blot. Cell surface exposure of DAMPs (calreticulin, heat shock proteins hsp70 and hsp90), apoptosis and induction of mitochondrial reactive oxygen species (ROS) were assessed by flow cytometry. HMGB1 and ATP were quantified by ELISA and chemiluminescence assay, respectively.

Results: Treatment with VAE resulted in phosphorylation of eIF2α in all cancer cell lines tested and increased calreticulin (CRT) exposure on the surface of pre-apoptotic SKBR3 breast cancer and B16F10 mouse melanoma cells. VAE exerted a concentration-dependent effect in all cell lines, resulting in a significantly increased exposure of three DAMPs (CRT, hsp70 and hsp90) on the surface of early apoptotic cells. Furthermore, VAE elevated mitochondrial ROS production and the release of ATP. HMGB1 release was not induced by VAE.

Conclusions: In this in vitro study, we demonstrated for the first time the potential of a mistletoe extract to induce surrogate markers of immunogenic cancer cell death. This is a primary step in investigating the potential of VAEs to contribute to ICD-induced tumor-specific immune activation.

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