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球三糖神经酰胺脂肪酸α-羟基化对志贺毒素1和志贺毒素2结合的影响。

Effect of globotriaosyl ceramide fatty acid alpha-hydroxylation on the binding by verotoxin 1 and verotoxin 2.

作者信息

Binnington Beth, Lingwood Daniel, Nutikka Anita, Lingwood Clifford A

机构信息

Division of Infection, Immunity, Injury and Repair, Research Institute, Hospital for Sick Children, Toronto, Ontario, Canada.

出版信息

Neurochem Res. 2002 Aug;27(7-8):807-13. doi: 10.1023/a:1020261125008.

Abstract

Variation in the lipid moiety of the verotoxin (VT) receptor glycosphingolipid, globotriaosyl ceramide (Gb3) can modulate toxin binding. The binding of VT1 and VT2 to C18 and C22 alpha hydroxy and nonhydroxy fatty acid isoforms of Gb3 were compared using a receptor ELISA and a 125I-labeled toxin/glycolipid microtitre plate direct binding assay. Increased binding to the hydroxylated species, particularly C220H, was observed for both toxins. Increased RELISA binding at low glycolipid concentrations only, suggested the binding affinity is increased following Gb3 fatty acid hydroxylation. Nonlinear regression analysis of direct binding assay to these Gb3 isoforms confirmed the increased affinity of both toxins for the C22 hydroxylated Gb3. The capacity was also significantly increased. The increased binding of VTs for hydroxylated fatty acid Gb3 isoforms may be a factor in the selective renal pathology which can follow systemic verotoxemia, particularly in the mouse model. The more pronounced effect at lower glycolipid concentrations prompted investigation of VT1 binding affinity at different Gb3 concentrations. Unexpectedly, the VT1 Kd for Gb3 was found to decrease as an inverse function of the Gb3 concentration. This shows that glycolipids have "nonclassical" receptor properties.

摘要

志贺毒素(VT)受体糖鞘脂——球三糖基神经酰胺(Gb3)脂质部分的变异可调节毒素结合。使用受体酶联免疫吸附测定(ELISA)和125I标记毒素/糖脂微量滴定板直接结合测定法,比较了VT1和VT2与Gb3的C18和C22α-羟基及非羟基脂肪酸异构体的结合情况。两种毒素均观察到与羟基化形式,特别是C220H的结合增加。仅在低糖脂浓度下RELISA结合增加,表明Gb3脂肪酸羟基化后结合亲和力增加。对这些Gb3异构体的直接结合测定进行非线性回归分析,证实了两种毒素对C22羟基化Gb3的亲和力增加。结合容量也显著增加。VTs对羟基化脂肪酸Gb3异构体结合的增加可能是系统性志贺毒素血症后出现选择性肾脏病理改变的一个因素,特别是在小鼠模型中。在低糖脂浓度下更明显的效应促使研究不同Gb3浓度下VT1的结合亲和力。出乎意料的是,发现Gb3的VT1解离常数(Kd)作为Gb3浓度的反函数而降低。这表明糖脂具有“非经典”受体特性。

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