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首页> 外文期刊>Brain pathology >Recent advances in the biochemistry of sphingolipidoses.
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Recent advances in the biochemistry of sphingolipidoses.

机译:鞘脂糖生物化学的最新进展。

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Glycosphingolipids are ubiquitous membrane components of eukaryotic cells. They participate in various cell recognition events and can regulate enzymes and receptors within the plasma membrane. Sphingolipidoses are due to an impaired lysosomal digestion of these substances. Glycosphingolipids are degraded by the action of exohydrolases, which are supported, in the case of glycosphingolipids with short oligosaccharide chains, by sphingolipid activator proteins. Five sphingolipid activator proteins are known so far, the GM2-activator and the SAPs, SAP-A to D (also called saposins). Degradation of glycosphingolipids requires endocytic membrane flow of plasma membrane derived glycosphingolipids into the lysosomes. Recent research focused on the topology of this process and on the mechanism and physiological function of sphingolipid activator proteins. Limited knowledge is available about enzymology and topology of glycosphingolipid biosynthesis. Recently, intermediates of this metabolic pathway have been identified as novel signalling molecules. Inhibition of glycosphingolipid biosynthesis has been shown to be beneficial in the animal model of Tay-Sachs disease. Mice with disrupted genes for lysosomal hydrolases and activator proteins are useful models for known human diseases and are valuable tools for the study of glycosphingolipid metabolism, the pathogenesis of sphingolipidoses and novel therapeutic approaches.
机译:糖鞘脂是真核细胞的普遍存在的膜成分。它们参与各种细胞识别事件,并可以调节质膜内的酶和受体。鞘脂糖是由于这些物质的溶酶体消化受损。糖鞘脂通过胞外水解酶的作用而降解,在具有短寡糖链的糖鞘脂的情况下,鞘糖脂激活蛋白支持。迄今为止已知五个鞘脂激活蛋白,GM2-激活蛋白和SAP,SAP-A至D(也称为鞘脂激活蛋白)。糖鞘脂的降解需要胞质膜衍生的糖鞘脂的内吞膜流进入溶酶体。最近的研究集中于该过程的拓扑结构以及鞘脂激活蛋白的机制和生理功能。关于糖鞘脂生物合成的酶学和拓扑学的知识有限。最近,该代谢途径的中间体已被鉴定为新型信号分子。在Tay-Sachs病的动物模型中,抑制鞘糖脂的生物合成是有益的。具有溶酶体水解酶和激活蛋白的基因被破坏的小鼠是已知人类疾病的有用模型,并且是研究糖鞘脂代谢,鞘脂的发病机理和新治疗方法的有价值的工具。

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