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欧洲槲寄生(Viscum album L.)中的毒性凝集素ML I和ML III与人淋巴细胞的差异结合

Differential binding of toxic lectins from Viscum album L., ML I and ML III, to human lymphocytes.

作者信息

Büssing A, Stein G M, Pfüller U, Schietzel M

机构信息

Department of Applied Immunology, Communal Hospital Herdecke, University Witten/Herdecke, Germany.

出版信息

Anticancer Res. 1999 Nov-Dec;19(6B):5095-9.

Abstract

The killing capacity of extracts from Viscum album L., widely used as an adjuvant in complementary cancer therapy, is dependent on the content of toxic proteins, especially the mistletoe lectins (ML). Although one may expect a homogeneous distribution of 'receptors' for these proteins on the cell surface, the sensitivity of cells to the ML-mediated cytotoxicity obviously differs, as the galNAc-binding ML III in contrast to the gal-binding ML I selectively killed CD8+ lymphocytes with a 'memory' phenotype (CD62Llo), while CD19+ B cells remained almost unaffected. B cells hardly bind ML III but did bind the gal-specific ML I. In accordance with these observations, in leukaemic B cells from patients with B chronic lymphocytic leukaemia and the human IgE-secreting myeloma cell line U-266 a strong induction of apoptosis-associated mitochondrial Apo2.7 molecules was observed after treatment with ML I and less effectively by ML III, while in the leukaemic T cell line Molt-4 both ML were strong inductors of apoptosis. In the light of these findings, the possible impact of ML I- and ML III-rich mistletoe extracts in the treatment of B cell neoplasia has to be carefully investigated.

摘要

欧洲槲寄生提取物在辅助癌症综合治疗中广泛应用,其杀伤能力取决于有毒蛋白质的含量,尤其是槲寄生凝集素(ML)。尽管人们可能期望这些蛋白质的“受体”在细胞表面均匀分布,但细胞对ML介导的细胞毒性的敏感性明显不同,因为与半乳糖结合的ML I相比,结合N-乙酰半乳糖胺的ML III选择性地杀死具有“记忆”表型(CD62Llo)的CD8 +淋巴细胞,而CD19 + B细胞几乎不受影响。B细胞几乎不结合ML III,但确实结合半乳糖特异性的ML I。根据这些观察结果,在用ML I处理后,在B慢性淋巴细胞白血病患者的白血病B细胞和人IgE分泌性骨髓瘤细胞系U-266中观察到凋亡相关线粒体Apo2.7分子的强烈诱导,而ML III的诱导作用较弱,而在白血病T细胞系Molt-4中,两种ML都是凋亡的强烈诱导剂。鉴于这些发现,必须仔细研究富含ML I和ML III的槲寄生提取物在B细胞肿瘤治疗中的可能影响。

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