Biomedical Research Institute, National Institute of Advanced Industrial Science and Technology (AIST), Tsukuba, Japan.
Structural Biology Research Center, Institute of Materials Structure Science, High Energy Accelerator Research Organization (KEK), Tsukuba, Japan.
FEBS J. 2023 Jan;290(2):412-427. doi: 10.1111/febs.16599. Epub 2022 Sep 5.
Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) spike protein (S protein) is highly N-glycosylated, and a "glycan shield" is formed to limit the access of other molecules; however, a small open area coincides with the interface to the host's receptor and also neutralising antibodies. Most of the variants of concern have mutations in this area, which could reduce the efficacy of existing antibodies. In contrast, N-glycosylation sites are relatively invariant, and some are essential for infection. Here, we observed that the S proteins of the ancestral (Wuhan) and Omicron strains bind with Pholiota squarrosa lectin (PhoSL), a 40-amino-acid chemically synthesised peptide specific to core-fucosylated N-glycans. The affinities were at a low nanomolar level, which were ~ 1000-fold stronger than those between PhoSL and the core-fucosylated N-glycans at the micromolar level. We demonstrated that PhoSL inhibited infection by both strains at similar submicromolar levels, suggesting its broad-spectrum effect on SARS-CoV-2 variants. Cryogenic electron microscopy revealed that PhoSL caused an aggregation of the S protein, which was likely due to the multivalence of both the trimeric PhoSL and S protein. This characteristic is likely relevant to the inhibitory mechanism. Structural modelling of the PhoSL-S protein complex indicated that PhoSL was in contact with the amino acids of the S protein, which explains the enhanced affinity with S protein and also indicates the significant potential for developing specific binders by the engineering of PhoSL.
严重急性呼吸综合征冠状病毒 2(SARS-CoV-2)的刺突蛋白(S 蛋白)高度糖基化,形成“聚糖盾牌”以限制其他分子的进入;然而,一个小的开放区域与宿主受体的结合界面以及中和抗体相吻合。大多数关注的变体在该区域都有突变,这可能会降低现有抗体的疗效。相比之下,N-糖基化位点相对不变,其中一些对感染至关重要。在这里,我们观察到,祖先(武汉)株和奥密克戎株的 S 蛋白与 Pholiota squarrosa 凝集素(PhoSL)结合,PhoSL 是一种 40 个氨基酸的化学合成肽,特异性识别核心岩藻糖基化 N-聚糖。亲和力处于纳摩尔水平,比微摩尔水平的核心岩藻糖基化 N-聚糖与 PhoSL 的亲和力强约 1000 倍。我们证明 PhoSL 以类似的亚微摩尔水平抑制了两种毒株的感染,表明其对 SARS-CoV-2 变体具有广谱作用。低温电子显微镜显示 PhoSL 导致 S 蛋白聚集,这可能是由于三聚体 PhoSL 和 S 蛋白的多价性所致。这种特性可能与抑制机制有关。PhoSL-S 蛋白复合物的结构建模表明 PhoSL 与 S 蛋白的氨基酸相互作用,这解释了与 S 蛋白增强的亲和力,也表明通过 PhoSL 的工程化开发特异性结合物具有重要的潜力。