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霍乱毒素介导含神经节苷脂Gm1的磷脂囊泡与包被Gm1的聚苯乙烯微球的凝集反应。

Cholera toxin mediated agglutination of ganglioside Gm1 containing phospholipid vesicles and Gm1-coated polystyrene spheres.

作者信息

Dwyer J D, Bloomfield V A

出版信息

Biochemistry. 1982 Jun 22;21(13):3231-4. doi: 10.1021/bi00256a031.

Abstract

Quasi-elastic laser light scattering is used to examine the cholera toxin mediated agglutination of ganglioside GM1 containing phospholipid vesicles and Gm1-coated polystyrene spheres. We find that the ability of cholera toxin to agglutinate Gm1-containing phospholipid vesicles depends markedly on the lipid composition of the vesicle, with only those composed of short-chain lipids (C14, C16) being appreciably agglutinated. This is interpreted as due to poor mixing of these lipids with the longer chain gangliosides, resulting in lateral separation of the gangliosides in the membrane bilayer. A simple quantitative model, a modification of that developed by von Schulthess et al. [von Schulthess, G. K., Cohen, R. J., Sakato, N., & Benedek, G. B. (1976a) Immunochemistry 13, 955--962], is developed to describe these agglutination processes. Application of this model to the agglutination of Gm1-coated polystyrene spheres by cholera toxin allows an estimate of a minimum value of 4.5 x 10(4) M-1 for the association constant of cholera toxin for its initial Gm1 receptor.

摘要

准弹性激光光散射用于检测霍乱毒素介导的含神经节苷脂GM1的磷脂囊泡和GM1包被的聚苯乙烯球的凝集作用。我们发现,霍乱毒素凝集含GM1的磷脂囊泡的能力明显取决于囊泡的脂质组成,只有那些由短链脂质(C14、C16)组成的囊泡才会明显凝集。这被解释为是由于这些脂质与较长链神经节苷脂混合不良,导致神经节苷脂在膜双层中横向分离。我们开发了一个简单的定量模型,它是对冯·舒尔特斯等人[冯·舒尔特斯,G.K.,科恩,R.J.,坂东,N.,&贝内德克,G.B.(1976a)免疫化学13,955 - 962]所开发模型的改进,用于描述这些凝集过程。将该模型应用于霍乱毒素对GM1包被的聚苯乙烯球的凝集作用,可估算出霍乱毒素与其初始GM1受体的结合常数的最小值为4.5×10⁴ M⁻¹。

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