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用欧洲槲寄生处理的人淋巴细胞中的细胞凋亡诱导是由槲寄生凝集素介导的。

Induction of apoptosis in human lymphocytes treated with Viscum album L. is mediated by the mistletoe lectins.

作者信息

Büssing A, Suzart K, Bergmann J, Pfüller U, Schietzel M, Schweizer K

机构信息

Krebsforschung Herdecke, Department of Applied Immunology, University Witten/Herdecke, Germany.

出版信息

Cancer Lett. 1996 Jan 19;99(1):59-72. doi: 10.1016/0304-3835(95)04038-2.

Abstract

Viscum album L. (VAL) is a phytopreparation used in adjuvant cancer therapy with both immunostimulatory and DNA stabilizing properties at low drug concentrations and cytostatic/cytotoxic properties at higher concentrations. The present work examines the cytotoxic effects of VAL extracts produced from mistletoes grown on different host trees and of purified toxic proteins from VAL, such as the D-galactose-specific lectin I (ML I), the N-acetyl-D-galactosamine-specific ML II and ML III, and crude viscotoxins towards cultured human lymphocytes. The decrease in the number of cultured lymphocytes and blast cells treated with whole plant extracts from VAL was host tree-specific. Nevertheless, there was no close correlation to the content of MLs or viscotoxins. Using the purified proteins, it became obvious that the cell killing was mediated by the induction of apoptosis, as measured by the appearance of a hypodiploid DNA peak using flow cytometry. ML III was the most effective to induce apoptosis, followed by ML II and ML I, while the viscotoxins and oligosaccharides from VAL did not. By measuring the surface expression of IL-2R alpha chains, transferrin receptors and APO-1/Fas molecules on non-apoptotic T cells, no significant changes were observed at low ML concentrations (1 ng/ml), but their decrease at higher ones. Our findings suggest that there might be at least two different ways of cell killing operative in VAL-mediated cytotoxicity: (a) the typical apoptotic cell death with the appearance of hypo-diploid nuclei, and (b) a direct or indirect killing by damaging the cell membrane with subsequent influx of Ca2+ and of the DNA intercalating dye propidium iodide and cell shrinkage. These effects might not be exclusive, as they probably occur simultaneously.

摘要

槲寄生(Viscum album L.,VAL)是一种用于癌症辅助治疗的植物制剂,在低药物浓度下具有免疫刺激和DNA稳定特性,在较高浓度下具有细胞抑制/细胞毒性特性。本研究考察了生长在不同宿主树上的槲寄生所产生的VAL提取物,以及VAL中的纯化毒性蛋白,如D-半乳糖特异性凝集素I(ML I)、N-乙酰-D-半乳糖胺特异性ML II和ML III,还有粗制槲寄生毒素对培养的人淋巴细胞的细胞毒性作用。用VAL全株提取物处理后,培养的淋巴细胞和母细胞数量的减少具有宿主树特异性。然而,这与MLs或槲寄生毒素的含量没有密切相关性。使用纯化蛋白后发现,细胞杀伤是由凋亡诱导介导的,通过流式细胞术检测到亚二倍体DNA峰的出现来衡量。ML III诱导凋亡的效果最显著,其次是ML II和ML I,而VAL中的槲寄生毒素和寡糖则没有这种作用。通过测量非凋亡T细胞上IL-2Rα链、转铁蛋白受体和APO-1/Fas分子的表面表达,在低ML浓度(1 ng/ml)下未观察到显著变化,但在较高浓度下其表达下降。我们的研究结果表明,在VAL介导的细胞毒性中可能至少有两种不同的细胞杀伤方式:(a)出现亚二倍体核的典型凋亡性细胞死亡,以及(b)通过损伤细胞膜,随后Ca2+内流、DNA嵌入染料碘化丙啶内流和细胞收缩导致的直接或间接杀伤。这些效应可能并非相互排斥,因为它们可能同时发生。

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