Smith L Courtney
Department of Biological Sciences and the Institute of Biomedical Sciences, George Washington University, 2023 George Washington Street, DC 20052, USA.
Dev Comp Immunol. 2002 Sep;26(7):603-14. doi: 10.1016/s0145-305x(02)00017-4.
The amino acid sequence of the thioester site in the alpha chain of SpC3, the sea urchin homologue of C3, is conserved. This implies a conserved function of covalent bond formation with amine or hydroxyl groups on target molecules. When coelomic fluid (CF) was incubated with 14C-methylamine, a classic assay for thioester binding function, the alpha chain became labeled. When CF was treated to induce autolysis, peptide bond cleavage occurred at the thioester site. Autolysis could be blocked or reduced by pre-treating CF with either methylamine or yeast, both of which are known to bind to thioester sites C3 proteins from other organisms. The data suggest that SpC3 can bind to target cell surfaces, constituting indirect evidence that it can covalently bind to pathogen surfaces and function as an opsonin in vivo. This activity may be an important aspect of host defense in the sea urchin.
海胆C3的同源物SpC3α链中硫酯位点的氨基酸序列是保守的。这意味着它与靶分子上的胺基或羟基形成共价键的功能是保守的。当体腔液(CF)与14C-甲胺一起孵育时(这是硫酯结合功能的经典检测方法),α链会被标记。当CF经处理诱导自溶时,硫酯位点会发生肽键断裂。用甲胺或酵母预处理CF可阻断或减少自溶,已知这两者都能与其他生物的C3蛋白的硫酯位点结合。数据表明SpC3可以结合到靶细胞表面,这构成了间接证据,证明它可以在体内与病原体表面共价结合并作为调理素发挥作用。这种活性可能是海胆宿主防御的一个重要方面。
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