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通过表面等离子体共振测定霍乱毒素对神经节苷脂的结合亲和力和特异性。

Cholera toxin binding affinity and specificity for gangliosides determined by surface plasmon resonance.

作者信息

Kuziemko G M, Stroh M, Stevens R C

机构信息

Department of Chemistry, University of California-Berkeley 94720, USA.

出版信息

Biochemistry. 1996 May 21;35(20):6375-84. doi: 10.1021/bi952314i.

Abstract

The present study determines the affinity of cholera toxin for the ganglioside series GM1, GM2, GM3, GD1A, GD1B, GT1B, asialo GM1, globotriosyl ceramide, and lactosyl ceramide using real time biospecific interaction analysis (surface plasmon resonance, SPR). SPR shows that cholera toxin preferably binds to gangliosides in the following sequence: GM1 > GM2 > GD1A > GM3 > GT1B > GD1B > asialo-GM1. The measured binding affinity of cholera toxin for the ganglioside sequence ranges from 4.61 x 10-12 M for GM1 to 1.88 x 10-10 M for asialo GM1. The picomolar values obtained by surface plasmon resonance are similar to Kd values determined with whole-cell binding assays. Both whole-cell assays and SPR measurements on synthetic membranes are higher than free solution measurements by several orders of magnitude. This difference may be caused by the effects of avidity and charged lipid head-groups, which may play a major role in the binding between cholera toxin, the receptor, and the membrane surface. The primary difference between free solution binding studies and surface plasmon resonance studies is that the latter technique is performed on surfaces resembling the cell membrane. Surface plasmon resonance has the further advantage of measuring apparent kinetic association and dissociation rates in real time, providing direct information about binding events at the membrane surface.

摘要

本研究采用实时生物特异性相互作用分析(表面等离子体共振,SPR)来测定霍乱毒素对神经节苷脂系列GM1、GM2、GM3、GD1A、GD1B、GT1B、去唾液酸GM1、球三糖神经酰胺和乳糖神经酰胺的亲和力。SPR显示霍乱毒素优先按以下顺序与神经节苷脂结合:GM1 > GM2 > GD1A > GM3 > GT1B > GD1B > 去唾液酸GM1。霍乱毒素对该神经节苷脂序列的测量结合亲和力范围从GM1的4.61×10⁻¹² M到去唾液酸GM1的1.88×10⁻¹⁰ M。通过表面等离子体共振获得的皮摩尔值与全细胞结合试验测定的Kd值相似。全细胞试验和合成膜上的SPR测量值均比游离溶液测量值高几个数量级。这种差异可能是由亲和力和带电荷的脂质头部基团的影响引起的,它们可能在霍乱毒素、受体和膜表面之间的结合中起主要作用。游离溶液结合研究与表面等离子体共振研究之间的主要区别在于,后一种技术是在类似于细胞膜的表面上进行的。表面等离子体共振的进一步优势在于能够实时测量表观动力学缔合和解离速率,提供有关膜表面结合事件的直接信息。

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