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Binding of CML-Modified as Well as Heat-Glycated β-lactoglobulin to Receptors for AGEs Is Determined by Charge and Hydrophobicity

机译:通过电荷和疏水测定CML改性的CML改性以及热糖化的β-乳酰键对受体的结合

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Intake of dietary advanced glycation end products (AGEs) is associated with inflammation-related health problems. Nε-carboxymethyl lysine (CML) is one of the best characterised AGEs in processed food. AGEs have been described as ligands for receptors present on antigen presenting cells. However, changes in protein secondary and tertiary structure also induce binding to AGE receptors. We aimed to discriminate the role of different protein modifications in binding to AGE receptors. Therefore, β-lactoglobulin was chemically modified with glyoxylic acid to produce CML and compared to β-lactoglobulin glycated with lactose. Secondary structure was monitored with circular dichroism, while hydrophobicity and formation of β-sheet structures was measured with ANS-assay and ThT-assay, respectively. Aggregation was monitored using native-PAGE. Binding to sRAGE, CD36, and galectin-3 was measured using inhibition ELISA. Even though no changes in secondary structure were observed in all tested samples, binding to AGE receptors increased with CML concentration of CML-modified β-lactoglobulin. The negative charge of CML was a crucial determinant for the binding of protein bound CML, while binding of glycated BLG was determined by increasing hydrophobicity. This shows that sRAGE, galectin-3, and CD36 bind to protein bound CML and points out the role of negatively charged AGEs in binding to AGE receptors.
机译:摄入膳食晚期糖化末端产品(年龄)与炎症相关的健康问题有关。 Nε-羧甲基赖氨酸(CML)是加工食品中最佳特征的年龄之一。已经描述为抗原呈递细胞上存在的受体的配体。然而,蛋白质二级和三级结构的变化也诱导与年龄受体的结合。我们旨在区分不同蛋白质修饰在与年龄受体结合的作用。因此,用乙醛酸化学改性β-乳酰脱蛋白,并与乳糖糖化的β-乳酰蛋白酶进行比较。用圆形二色性监测二级结构,同时用ANS-测定和THT测定法测量β-片状结构的疏水性和形成。使用本机页面监视聚合。使用抑制ELISA测量与SRAGE,CD36和Galectin-3的结合。尽管在所有测试样品中观察到二级结构的变化,但是与年龄受体的结合随CML改性β-乳酰蛋白的CML浓度而增加。 CML的负电荷是蛋白质结合CML的结合的关键决定因素,而通过增加疏水性来确定糖化BLG的结合。这表明SRAGE,GALECTIN-3和CD36与蛋白质结合CML结合,并指出带负电荷年龄与年龄受体结合的作用。

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