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β-干扰素对培养的人胶质瘤细胞的生长抑制作用不依赖于神经节苷脂组成的变化。

Growth inhibition of cultured human glioma cells by beta-interferon is not dependent on changes in ganglioside composition.

作者信息

Yates A J, Markowitz D L, Stephens R E, Pearl D K, Whisler R L

机构信息

Department of Pathology, College of Medicine, Ohio State University, Columbus 43210.

出版信息

J Neuropathol Exp Neurol. 1988 Mar;47(2):119-27. doi: 10.1097/00005072-198803000-00004.

Abstract

This investigation tested the hypothesis that the growth inhibiting effects of human beta-interferon on cultured human glioma cells involves changes in the ganglioside composition of these cells. Four cell lines derived from human malignant gliomas (12-18, U-251 MG, I29-A, 7-24) and two lines from human fetal brain (CHI, CHII) were cultured in the presence and in the absence of human beta-interferon (HuIFN-beta), 1,000 units per ml medium for three days before harvesting. Human beta-interferon had an inhibitory effect on growth of glioma but not fetal brain cells. Total ganglioside sialic acid for all cell lines ranged between 3.5 and 13.8 micrograms/10(7) cells (0.6-3.9 micrograms/mg protein). No distinct difference in the amount of total ganglioside per cell was observed between neoplastic and non-neoplastic cells, but the latter had more ganglioside per mg total protein. All cell lines displayed different patterns of gangliosides determined by high performance thin layer chromatography, but there was no distinct difference between glioma and fetal brain cells. Human beta-interferon increased the total amount of ganglioside per cell in one fetal brain and two glioma lines, but on a protein basis in only one glioma cell line (I29-A); HuIFN-beta had only minor effects on ganglioside patterns. There was a slight shift towards a greater proportion of structurally simpler gangliosides in both fetal brain and two glioma cell lines exposed to HuIFN-beta, but the reverse occurred in glioma U-251 MG. None of these changes strongly correlated with the degree of growth inhibition due to HuIFN-beta.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

本研究检验了以下假设

人β-干扰素对培养的人胶质瘤细胞的生长抑制作用涉及这些细胞神经节苷脂组成的变化。从人恶性胶质瘤中获得的4种细胞系(12 - 18、U - 251 MG、I29 - A、7 - 24)和来自人胎脑的2种细胞系(CHI、CHII),在添加和不添加人β-干扰素(HuIFN-β,每毫升培养基1000单位)的情况下培养三天后收获。人β-干扰素对胶质瘤细胞生长有抑制作用,但对胎脑细胞无此作用。所有细胞系的总神经节苷脂唾液酸含量在3.5至13.8微克/10⁷个细胞(0.6 - 3.9微克/毫克蛋白)之间。肿瘤细胞和非肿瘤细胞每细胞的总神经节苷脂量未观察到明显差异,但后者每毫克总蛋白的神经节苷脂含量更高。通过高效薄层色谱法测定,所有细胞系均呈现不同的神经节苷脂模式,但胶质瘤细胞和胎脑细胞之间无明显差异。人β-干扰素增加了一个胎脑细胞系和两个胶质瘤细胞系中每细胞的神经节苷脂总量,但仅在一个胶质瘤细胞系(I29 - A)中基于蛋白含量有增加;HuIFN-β对神经节苷脂模式的影响较小。在暴露于HuIFN-β的胎脑细胞系和两个胶质瘤细胞系中,均有向结构更简单的神经节苷脂比例更高的方向轻微转变,但在胶质瘤U - 251 MG细胞系中则相反。这些变化均与HuIFN-β引起的生长抑制程度无强烈相关性。(摘要截选至250字)

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