Oriented immobilisation of histidine-tagged protein and its application in exploring interactions between ligands and proteins

A method based on reaction with a diazonium salt wasdevelopedtoimmobiliseorientedHis-taggedproteinonto silica gel. The binding efficiency of the phenylamine-group- coated gel was determined to be 65 %, providing a binding capacity of His-tagged protein up to the gram level. Using His-tagged β2-adrenoceptor (β2-AR) as a probe, we devel- oped a new mathematical model to elucidate the interactions between the receptor and five ligands (methoxyphenamine, terbutaline, salbutamol, tulobuterol and fenoterol). These drugs proved to only have one type of binding site on the immobilised β2-AR,yieldinghigherassociationconstantsand numbers of binding sites than random attachment assays. The association constants determined by the new model positively correlated to the values from a radioligand binding method, with a regression equation of y=1.75x−7.18 and a correlation coefficient of 0.9807. The oriented method resulted in a high binding capacity and quantitative immobilisation of the His-tagged protein. The proposed model can be used to deter- minethe interactionsbetweenthe ligandsandtheimmobilised protein with the advantages of drug and time saving.