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磷脂酶诱导的多萜醇磷酸甘露糖合酶活性调节。

Phospholipase-induced modulation of dolichyl-phosphomannose synthase activity.

作者信息

Jensen J W, Schutzbach J S

机构信息

Department of Microbiology, University of Alabama, Birmingham 35294.

出版信息

Biochemistry. 1989 Jan 24;28(2):851-5. doi: 10.1021/bi00428a066.

Abstract

Rat liver dolichyl-phosphomannose synthase is optimally active when the enzyme is reconstituted with lipids that prefer a nonlamellar macroscopic organization in isolation, such as phosphatidylethanolamine (PE), but the enzyme is only negligibly active in the presence of lipids that normally form stable bilayers, such as phosphatidylcholine (PC) [Jensen, J.W., & Schutzbach, J.S. (1985) Eur. J. Biochem. 153, 41-48]. We now report that the activity of the synthase can be modulated by incorporating diacylglycerol and lysophosphatidylcholine into the lipid matrix. Enzyme activity in PC bilayers was stimulated by the presence of diacylglycerol, a lipid that has a conical dynamic molecular shape and disrupts bilayer stability. In PC/diacylglycerol mixtures the apparent Km for dolichyl-P was 30-fold lower than the apparent Km for the polyprenol acceptor in PC membranes. Enzyme activity was also stimulated when diacylglycerol was generated in situ by incubation of PC vesicles with phospholipase C. In contrast, the activity of enzyme reconstituted in PE dispersions, or in PE/PC bilayers, was markedly inhibited by the presence of lysophospholipids. Enzyme activity was also reduced by the in situ generation of lysophospholipids in PE/PC vesicles by incubation with phospholipase A2. Since lysophospholipids and diacylglycerols arise in vivo as products of phospholipid metabolism, modulation of enzyme activity by these compounds may represent a potential regulatory mechanism for the synthesis of oligosaccharide lipids.

摘要

当用在分离时倾向于非层状宏观结构的脂质(如磷脂酰乙醇胺(PE))重构大鼠肝脏多萜醇磷酸甘露糖合酶时,该酶具有最佳活性,但在通常形成稳定双层的脂质(如磷脂酰胆碱(PC))存在下,该酶的活性可忽略不计[Jensen, J.W., & Schutzbach, J.S. (1985) Eur. J. Biochem. 153, 41 - 48]。我们现在报道,通过将二酰基甘油和溶血磷脂酰胆碱掺入脂质基质中,可以调节合酶的活性。在PC双层中,二酰基甘油(一种具有锥形动态分子形状并破坏双层稳定性的脂质)的存在刺激了酶活性。在PC/二酰基甘油混合物中,多萜醇磷酸的表观Km比PC膜中聚异戊二烯受体的表观Km低30倍。当通过用磷脂酶C孵育PC囊泡原位产生二酰基甘油时,酶活性也受到刺激。相反,在PE分散体或PE/PC双层中重构的酶的活性在溶血磷脂存在下受到明显抑制。通过与磷脂酶A2孵育在PE/PC囊泡中原位产生溶血磷脂也会降低酶活性。由于溶血磷脂和二酰基甘油在体内作为磷脂代谢产物出现,这些化合物对酶活性的调节可能代表了寡糖脂合成的潜在调节机制。

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