Department of Chemical and Biomolecular Engineering, Johns Hopkins University, 3400 N. Charles St., Baltimore, MD 21218, USA.
FASEB J. 2012 Mar;26(3):1349-59. doi: 10.1096/fj.11-195669. Epub 2011 Dec 9.
Selectins promote metastasis by mediating specific interactions between selectin ligands on tumor cells and selectin-expressing host cells in the microvasculature. Using affinity chromatography in conjunction with tandem mass spectrometry and bioinformatics tools, we identified mucin 16 (MUC16) as a novel selectin ligand expressed by metastatic pancreatic cancer cells. While up-regulated in many pancreatic cancers, the biological function of sialofucosylated MUC16 has yet to be fully elucidated. To address this, we employed blot rolling and cell-free flow-based adhesion assays using MUC16 immunopurified from pancreatic cancer cells and found that it efficiently binds E- and L- but not P-selectin. The selectin-binding determinants are sialofucosylated structures displayed on O- and N-linked glycans. Silencing MUC16 expression by RNAi markedly reduces pancreatic cancer cell binding to E- and L-selectin under flow. These findings provide a novel integrated perspective on the enhanced metastatic potential associated with MUC16 overexpression and the role of selectins in metastasis.
选择素通过介导肿瘤细胞上的选择素配体与微血管中表达选择素的宿主细胞之间的特异性相互作用,促进转移。我们使用亲和层析结合串联质谱和生物信息学工具,鉴定出黏蛋白 16(MUC16)是转移性胰腺癌细胞表达的一种新型选择素配体。虽然在许多胰腺癌中上调,但唾液酸化糖基化 MUC16 的生物学功能尚未完全阐明。为了解决这个问题,我们使用从胰腺癌细胞中免疫纯化的 MUC16 进行了印迹滚动和无细胞流动基础粘附测定,发现它可以有效地结合 E-和 L-选择素,但不能结合 P-选择素。选择素结合决定簇是在 O-和 N-连接糖上显示的唾液酸化糖基化结构。通过 RNAi 沉默 MUC16 的表达,显著减少了胰腺癌细胞在流动条件下与 E-和 L-选择素的结合。这些发现为 MUC16 过表达与选择素在转移中的作用相关的增强转移潜能提供了一个新的综合视角。
