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Thermodynamic analysis of the binding of galactose and poly‐N‐acetyllactosamine derivatives to human galectin‐3

机译:半乳糖和聚-N-乙酰基乳糖胺衍生物与人半乳糖凝集素-3结合的热力学分析

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>Galectin-3, with a wide tissue distribution and marked developmental regulation, provides significant insights into the progression of various disease and developmental stages. Recognized by its specificity for galactose, a detailed characterization of its sugar binding ability has been investigated by isothermal titration calorimetry. The results presented here complement well with the earlier studies utilizing hapten inhibition assays. Among the various lactose derivatives studied, A-tetrasaccharide emerged with the highest affinity for binding to galectin-3 combining site. This blood group saccharide exhibited a binding affinity 37-fold higher and a 102 kJ/mol more favorable change in enthalpy over lactose at 280 K indicating the existence of additional subsites for both the α1-3-linked N-acetylgalactosamine at the non-reducing end and the α1-2-linked class="smallCaps">L-fucosyl residue. The thermodynamic parameters evaluated for other ligands substantiate further the carbohydrate recognition domain to be part of an extended binding site. Binding thermodynamics of galectin-3 with the galactose derivatives are essentially enthalpically driven and exhibit compensatory changes in ΔH° and TΔS owing to solvent reorganization.
机译:> Galectin-3具有广泛的组织分布和显着的发育调控,可为各种疾病和发育阶段的进展提供重要见识。通过其对半乳糖的特异性认识,已通过等温滴定量热法研究了其糖结合能力的详细特征。这里提出的结果与利用半抗原抑制测定的早期研究很好地互补。在研究的各种乳糖衍生物中,A-四糖以与半乳凝素3结合位点结合的最高亲和力出现。该血型糖在280 K时表现出比乳糖高37倍的结合亲和力和102焦耳/摩尔的焓更有利的变化,表明存在与α1-3连接的 N 额外的亚位点-乙酰半乳糖胺在非还原端和α1-2连接的 class =“ smallCaps”> L -岩藻糖基残基。对于其他配体评估的热力学参数进一步证实了碳水化合物识别结构域是扩展结合位点的一部分。 galectin-3与半乳糖衍生物的结合热力学本质上是受焓驱动的,并且由于溶剂而表现出Δ H °和 T Δ S 的补偿性变化。重组。

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