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水塑造了肿瘤相关碳水化合物 Tn 抗原的独特形状和动态:对其分子识别的影响。

Water Sculpts the Distinctive Shapes and Dynamics of the Tumor-Associated Carbohydrate Tn Antigens: Implications for Their Molecular Recognition.

机构信息

Departamento de Química, Centro de Investigación en Síntesis Química , Universidad de La Rioja , 26006 Logroño , Spain.

Departamento de Química Física, Facultad de Ciencia y Tecnología , Universidad del País Vasco (UPV-EHU), 48080 Bilbao , Spain.

出版信息

J Am Chem Soc. 2018 Aug 8;140(31):9952-9960. doi: 10.1021/jacs.8b04801. Epub 2018 Jul 30.

DOI:10.1021/jacs.8b04801
PMID:30004703
Abstract

The tumor-associated carbohydrate Tn antigens include two variants, αGalNAc- O-Thr and αGalNAc- O-Ser. In solution, they exhibit dissimilar shapes and dynamics and bind differently to the same protein receptor. Here, we demonstrate experimentally and theoretically that their conformational preferences in the gas phase are highly similar, revealing the essential role of water. We propose that water molecules prompt the rotation around the glycosidic linkage in the threonine derivative, shielding its hydrophobic methyl group and allowing an optimal solvation of the polar region of the antigen. The unusual arrangement of αGalNAc- O-Thr features a water molecule bound into a "pocket" between the sugar and the threonine. This mechanism is supported by trapping, for the first time, such localized water in the crystal structures of an antibody bound to two glycopeptides that comprise fluorinated Tn antigens in their structure. According to several reported X-ray structures, installing oxygenated amino acids in specific regions of the receptor capable of displacing the bridging water molecule to the bulk-solvent may facilitate the molecular recognition of the Tn antigen with threonine. Overall, our data also explain how water fine-tunes the 3D structure features of similar molecules, which in turn are behind their distinct biological activities.

摘要

肿瘤相关碳水化合物 Tn 抗原包括两种变体,αGalNAc-O-Thr 和 αGalNAc-O-Ser。在溶液中,它们呈现出不同的形状和动态,并且与相同的蛋白质受体结合方式不同。在这里,我们通过实验和理论证明了它们在气相中的构象偏好非常相似,揭示了水的重要作用。我们提出,水分子促使 threonine 衍生物中糖基连接的旋转,屏蔽其疏水性甲基,并允许抗原的极性区域得到最佳溶剂化。αGalNAc-O-Thr 的不寻常排列特征是一个水分子结合在糖和 threonine 之间的“口袋”中。这种机制得到了首次捕获的支持,即在与结构中包含氟化 Tn 抗原的两种糖肽结合的抗体的晶体结构中,捕获了这种局部水。根据几个报道的 X 射线结构,在受体的特定区域中安装含氧氨基酸,能够将桥接水分子置换到主体溶剂中,可能有助于 threonine 的 Tn 抗原的分子识别。总的来说,我们的数据还解释了水如何微调类似分子的 3D 结构特征,而这些特征又是它们不同生物活性的背后原因。

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