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神经节苷脂GM3(NeuAc)和GM3(NeuGc)在小鼠、大鼠和人源骨髓瘤及杂交瘤中的表达

Expression of gangliosides GM3 (NeuAc) and GM3 (NeuGc) in myelomas and hybridomas of mouse, rat, and human origin.

作者信息

Müthing J, Steuer H, Peter-Katalinić J, Marx U, Bethke U, Neumann U, Lehmann J

机构信息

Institut für Zellkulturtechnik der Universität, Bielefeld, Germany.

出版信息

J Biochem. 1994 Jul;116(1):64-73. doi: 10.1093/oxfordjournals.jbchem.a124504.

Abstract

In this study gangliosides from various myelomas and hybridomas of mouse, rat, and human origin were characterized by thin-layer and high-performance liquid chromatography, immunological methods (overlay technique) and fast atom bombardment mass spectrometry. Exclusively GM3 substituted with C24:1- and C16:0-fatty acid, was found in all B cell-derived cell lines. C18 sphingosine was the single long chain base in each GM3 ceramide portion. The mouse myeloma (NS-1) and all hybridomas, obtained by fusion of mouse, rat, or human B lymphocytes with murine myelomas, showed high GM3 (NeuGc) content (> 75%) and low GM3 (NeuAc) expression. Absolute amounts of GM3 ranged from 0.2 up to 0.8 mg x 10(-9) cells. Normally, human cells do not express NeuGc, and an Epstein-Barr virus-transformed human B lymphocyte line analyzed in this study retained this sialylation status, expressing exclusively GM3 (NeuAc) (100%). The fusion of human B lymphocytes with mouse myelomas led to high GM3 (NeuGc) expression (average about 85%) in all mouse/human heterohybridomas examined. Our results indicate the chromosomal gene "transfer" and/or the activation of enzymes involved in NeuGc-biosynthesis due to the somatic cell fusion process, which might explain the mouse dominance in the manifestation of the NeuGc-phenotype in hybridomas of human origin.

摘要

在本研究中,通过薄层色谱法、高效液相色谱法、免疫方法(覆盖技术)和快原子轰击质谱法对来自小鼠、大鼠和人类的各种骨髓瘤及杂交瘤中的神经节苷脂进行了表征。在所有B细胞来源的细胞系中,仅发现了被C24:1 - 和C16:0 - 脂肪酸取代的GM3。C18鞘氨醇是每个GM3神经酰胺部分中的单一长链碱基。小鼠骨髓瘤(NS - 1)以及通过小鼠、大鼠或人类B淋巴细胞与小鼠骨髓瘤融合获得的所有杂交瘤,均显示出高GM3(NeuGc)含量(> 75%)和低GM3(NeuAc)表达。GM3的绝对含量范围为0.2至0.8 mg×10⁻⁹个细胞。正常情况下,人类细胞不表达NeuGc,本研究中分析的一株爱泼斯坦 - 巴尔病毒转化的人类B淋巴细胞系保持了这种唾液酸化状态,仅表达GM3(NeuAc)(100%)。人类B淋巴细胞与小鼠骨髓瘤的融合导致在所检测的所有小鼠/人类异种杂交瘤中均出现高GM3(NeuGc)表达(平均约85%)。我们的结果表明,由于体细胞融合过程,可能发生了染色体基因“转移”和/或参与NeuGc生物合成的酶的激活,这可能解释了在人类来源的杂交瘤中NeuGc表型表现上小鼠占主导地位的现象。

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