Silva Mariana, Fung Ronald Kam Fai, Donnelly Conor Brian, Videira Paula Alexandra, Sackstein Robert
Centro de Estudos de Doenças Crónicas, NOVA Medical School/Faculdade de Ciências Médicas, Universidade Nova de Lisboa, 1169-056 Lisbon, Portugal.
Department of Dermatology, Brigham and Women's Hospital, Boston, MA 02115.
J Immunol. 2017 May 1;198(9):3576-3587. doi: 10.4049/jimmunol.1601636. Epub 2017 Mar 22.
Both host defense and immunopathology are shaped by the ordered recruitment of circulating leukocytes to affected sites, a process initiated by binding of blood-borne cells to E-selectin displayed at target endothelial beds. Accordingly, knowledge of the expression and function of leukocyte E-selectin ligands is key to understanding the tempo and specificity of immunoreactivity. In this study, we performed E-selectin adherence assays under hemodynamic flow conditions coupled with flow cytometry and Western blot analysis to elucidate the function and structural biology of glycoprotein E-selectin ligands expressed on human PBMCs. Circulating monocytes uniformly express high levels of the canonical E-selectin binding determinant sialyl Lewis X (sLe) and display markedly greater adhesive interactions with E-selectin than do circulating lymphocytes, which exhibit variable E-selectin binding among CD4 and CD8 T cells but no binding by B cells. Monocytes prominently present sLe decorations on an array of protein scaffolds, including P-selectin glycoprotein ligand-1, CD43, and CD44 (rendering the E-selectin ligands cutaneous lymphocyte Ag, CD43E, and hematopoietic cell E-selectin/L-selectin ligand, respectively), and B cells altogether lack E-selectin ligands. Quantitative PCR gene expression studies of glycosyltransferases that regulate display of sLe reveal high transcript levels among circulating monocytes and low levels among circulating B cells, and, commensurately, cell surface α(1,3)-fucosylation reveals that acceptor sialyllactosaminyl glycans convertible into sLe are abundantly expressed on human monocytes yet are relatively deficient on B cells. Collectively, these findings unveil distinct cell-specific patterns of E-selectin ligand expression among human PBMCs, indicating that circulating monocytes are specialized to engage E-selectin and providing key insights into the molecular effectors mediating recruitment of these cells at inflammatory sites.
宿主防御和免疫病理学均由循环白细胞向受影响部位的有序募集所塑造,这一过程始于血源性细胞与靶内皮床处展示的E-选择素结合。因此,了解白细胞E-选择素配体的表达和功能是理解免疫反应的节奏和特异性的关键。在本研究中,我们在血流动力学条件下进行了E-选择素黏附试验,并结合流式细胞术和蛋白质印迹分析,以阐明人外周血单核细胞(PBMC)上表达的糖蛋白E-选择素配体的功能和结构生物学。循环单核细胞一致高水平表达经典的E-选择素结合决定簇唾液酸化路易斯X(sLe),并且与E-选择素的黏附相互作用明显强于循环淋巴细胞,循环淋巴细胞在CD4和CD8 T细胞中表现出可变的E-选择素结合,但B细胞不结合。单核细胞在一系列蛋白质支架上显著呈现sLe修饰,包括P-选择素糖蛋白配体-1、CD43和CD44(分别使E-选择素配体成为皮肤淋巴细胞抗原、CD43E和造血细胞E-选择素/L-选择素配体),而B细胞完全缺乏E-选择素配体。对调节sLe展示的糖基转移酶进行的定量PCR基因表达研究显示,循环单核细胞中的转录水平高,循环B细胞中的转录水平低,相应地,细胞表面α(1,3)-岩藻糖基化显示,可转化为sLe的受体唾液酸化乳糖胺聚糖在人单核细胞上大量表达,但在B细胞上相对缺乏。总的来说,这些发现揭示了人PBMC中E-选择素配体表达的独特细胞特异性模式,表明循环单核细胞专门用于与E-选择素结合,并为介导这些细胞在炎症部位募集的分子效应器提供了关键见解。
