Krzeminski Mickaël, Singh Tanuja, André Sabine, Lensch Martin, Wu Albert M, Bonvin Alexandre M J J, Gabius Hans-Joachim
Bijvoet Center for Biomolecular Research, Faculty of Science, Utrecht University, Padualaan 8, 3584 CH Utrecht, The Netherlands.
Biochim Biophys Acta. 2011 Feb;1810(2):150-61. doi: 10.1016/j.bbagen.2010.11.001. Epub 2010 Nov 8.
Human galectin-3 (Mac-2 antigen) is a cell-type-specific multifunctional effector owing to selective binding of distinct cell-surface glycoconjugates harboring β-galactosides. The structural basis underlying the apparent preferences for distinct glycoproteins and for expression is so far unknown.
We strategically combined solid-phase assays on 43 natural glycoproteins with a new statistical approach to fully flexible computational docking and also processed the proximal promoter region in silico.
The degree of branching in N-glycans and clustering of core 1 O-glycans are positive modulators for avidity. Sialylation of N-glycans in α2-6 linkage and of core 1 O-glycans in α2-3 linkage along with core 2 branching was an unfavorable factor, despite the presence of suited glycans in the vicinity. The lectin-ligand contact profile was scrutinized for six natural di- and tetrasaccharides enabling a statistical grading by analyzing flexible docking trajectories. The computational analysis of the proximal promoter region delineated putative sites for Lmo2/c-Ets-1 binding and new sites with potential for RUNX binding.
These results identify new features of glycan selectivity and ligand contact by combining solid-phase assays with in silico work as well as of reactivity potential of the promoter.
人半乳糖凝集素-3(Mac-2抗原)是一种细胞类型特异性的多功能效应分子,因其能选择性结合含有β-半乳糖苷的不同细胞表面糖缀合物。目前尚不清楚其对不同糖蛋白明显偏好及表达的结构基础。
我们将对43种天然糖蛋白的固相分析与一种全新的统计方法策略性地结合起来,用于完全灵活的计算对接,并在计算机上处理近端启动子区域。
N-聚糖的分支程度和核心1 O-聚糖的聚类是亲和力的正调节剂。尽管附近存在合适的聚糖,但α2-6连接的N-聚糖和α2-3连接的核心1 O-聚糖的唾液酸化以及核心2分支是不利因素。对六种天然二糖和四糖的凝集素-配体接触情况进行了仔细研究,通过分析灵活的对接轨迹实现了统计分级。近端启动子区域的计算分析确定了Lmo2/c-Ets-1结合的假定位点以及具有RUNX结合潜力的新位点。
这些结果通过将固相分析与计算机模拟工作相结合,确定了聚糖选择性、配体接触的新特征以及启动子的反应潜力。
