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抗体结合、血小板黏附以及蛋白质在各种聚合物表面的吸附。

Antibody binding, platelet adhesion, and protein adsorption on various polymer surfaces.

作者信息

Nowak Joanna, Watala Cezary, Boncler Magdalena

机构信息

Department of Haemostatic Disorders, Medical University of Lodz, Lodz, Poland.

出版信息

Blood Coagul Fibrinolysis. 2014 Jan;25(1):52-60. doi: 10.1097/MBC.0b013e328364a802.

Abstract

Commercially available polymer surfaces for in vitro applications are characterized to different extents in terms of hydrophobicity, binding preferences, and immunoglobulin capacity. We compared five, well or poorly defined polystyrene plates, used as standard hydrophobic surfaces for studying biological interactions. Antibody binding (ELISA) and platelet adhesion (release of alkaline phosphatase from adhered platelets) were contrasted with total protein adsorption (alkaline phosphatase assay and bicinchoninic acid assay). In the assays, we utilized four plasma proteins: human serum albumin (HSA), C-reactive protein (CRP), fibronectin, and fibrinogen. At 0.5 μg antigen/well, all antibodies bound to their antigens most effectively on Nunc (MaxiSorp and MediSorp, Waltham, Massachusetts, USA) microplates, as compared to Sarstedt (Nümbrecht, Germany) and Corning microplates (Tewksbury, Massachusetts, USA). The significant differences between Nunc and Corning were seen in the binding of anti-HSA (P ≤ 0.01) and anti-fibronectin (P ≤ 0.0002). Similar patterns were shown in experiments of ADP-induced platelet adhesion to fibrinogen immobilized at 200 μg/well. Platelet adhesion noted on Corning microplates was roughly three times lower compared to those observed on MaxiSorp (P < 0.01), MediSorp (P < 0.02), and Sarstedt (P < 0.05). In a parallel study, we have also shown the superiority of tissue culture-Sarstedt surface over micro test Sarstedt plate. Furthermore, the antibody binding, but not platelet adhesion, was positively correlated with total protein adsorption. Our findings indicate that of five polystyrene surfaces, Nunc microplates are optimal for studies of protein adsorption, as they had the highest binding capacity and relatively the least affected protein structure, pointing to the role of surface chemistry in protein adsorption and adsorption-induced conformational changes in a protein structure.

摘要

用于体外应用的市售聚合物表面在疏水性、结合偏好和免疫球蛋白容量方面具有不同程度的特征。我们比较了五种定义明确或不明确的聚苯乙烯板,它们用作研究生物相互作用的标准疏水表面。将抗体结合(酶联免疫吸附测定)和血小板黏附(黏附血小板释放碱性磷酸酶)与总蛋白吸附(碱性磷酸酶测定和二辛可宁酸测定)进行对比。在测定中,我们使用了四种血浆蛋白:人血清白蛋白(HSA)、C反应蛋白(CRP)、纤连蛋白和纤维蛋白原。与赛多利斯(德国努姆布雷希特)和康宁微孔板(美国马萨诸塞州蒂克斯伯里)相比,在每孔0.5μg抗原的情况下,所有抗体在Nunc(美国马萨诸塞州沃尔瑟姆的MaxiSorp和MediSorp)微孔板上与抗原的结合最为有效。在抗HSA(P≤0.01)和抗纤连蛋白(P≤0.0002)的结合中,Nunc和康宁之间存在显著差异。在将ADP诱导的血小板黏附于以每孔200μg固定的纤维蛋白原的实验中也显示出类似模式。与在MaxiSorp(P<0.01)、MediSorp(P<0.02)和赛多利斯(P<0.05)上观察到的情况相比,在康宁微孔板上观察到的血小板黏附大约低三倍。在一项平行研究中,我们还表明组织培养赛多利斯表面优于微量测试赛多利斯板。此外,抗体结合而非血小板黏附与总蛋白吸附呈正相关。我们的研究结果表明,在五种聚苯乙烯表面中,Nunc微孔板最适合蛋白质吸附研究,因为它们具有最高的结合能力且对蛋白质结构的影响相对最小,这表明表面化学在蛋白质吸附以及蛋白质结构中吸附诱导的构象变化中所起的作用。

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