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甲基化氧嘌呤与小鼠红白血病细胞的分化诱导

Methylated oxypurines and induction of differentiation of murine erythroleukemia cells.

作者信息

Kerr S J

机构信息

Dept. of Biochemistry/Biophysics/Genetics, University of Colorado Health Sciences Center, Denver 80262.

出版信息

Mol Cell Biochem. 1990 Jan 18;92(1):37-44. doi: 10.1007/BF00220717.

Abstract

Murine erythroleukemia cell lines derived from Friend virus infected mice can be induced to differentiate in vitro by numerous agents. Among these compounds are certain naturally occurring purines such as hypoxanthine or 1-methylhypoxanthine. We have extended these studies to other modified oxypurines and have identified some areas of cell regulation with which they may be interacting. Monomethylated derivatives of guanine, hypoxanthine or xanthine are active as inducers of differentiation. Excluding hypoxanthine, the parent oxypurines guanine and xanthine are ineffective in inducing differentiation. The dimethyl- and trimethylxanthine derivatives are also inactive as inducers. The methylated oxypurines are not metabolized to nucleotides by the cell and, therefore, probably do not interact with nucleic acid synthesis directly. We have investigated one cellular process of possible regulatory significance with which they do interact. ADP-ribosylation has been implicated in control of gene expression and differentiation. The methylated oxypurines inhibit this reaction, as measured in permeabilized cells, in the same concentration range at which they are effective as inducers of differentiation. Additionally, 1-methylguanine and 7-methylguanine decrease incorporation of mannose and glucosamine into glycoprotein and into dolichol-oligosaccharide precursors. These effects may be related to cell surface alterations observed during differentiation.

摘要

源自感染弗氏病毒小鼠的鼠红细胞白血病细胞系可被多种因子诱导在体外分化。这些化合物中包括某些天然存在的嘌呤,如次黄嘌呤或1-甲基次黄嘌呤。我们已将这些研究扩展到其他修饰的氧嘌呤,并确定了它们可能相互作用的一些细胞调节区域。鸟嘌呤、次黄嘌呤或黄嘌呤的单甲基化衍生物作为分化诱导剂具有活性。除次黄嘌呤外,母体氧嘌呤鸟嘌呤和黄嘌呤在诱导分化方面无效。二甲基和三甲基黄嘌呤衍生物作为诱导剂也无活性。甲基化的氧嘌呤不会被细胞代谢为核苷酸,因此可能不会直接与核酸合成相互作用。我们研究了它们确实相互作用的一个可能具有调节意义的细胞过程。ADP-核糖基化与基因表达和分化的控制有关。在通透细胞中测定,甲基化的氧嘌呤在与它们作为分化诱导剂有效的相同浓度范围内抑制此反应。此外,1-甲基鸟嘌呤和7-甲基鸟嘌呤减少甘露糖和葡糖胺掺入糖蛋白和二萜醇-寡糖前体中。这些效应可能与分化过程中观察到的细胞表面改变有关。

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