Transferring the C-terminus of the chemokine CCL21 to CCL19 confers enhanced heparin binding

将趋化因子 CCL21 的 C 端转移到 CCL19 可增强肝素结合

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作者:Austin J Barmore, Sally M Castex, Brittany A Gouletas, Alex J Griffith, Slater W Metz, Nicolas G Muelder, Michael J Populin, David M Sackett, Abigail M Schuster, Christopher T Veldkamp

Abstract

Chemokines direct the migration of cells during various immune processes and are involved in many disease states. For example, CCL19 and CCL21, through activation of the CCR7 receptor, recruit dendritic cells and naïve T-cells to the secondary lymphoid organs aiding in balancing immune response and tolerance. However, CCL19 and CCL21 can also direct the metastasis of CCR7 expressing cancers. Chemokine binding to glycosaminoglycans, such as heparin, is as important to chemokine function as receptor activation. CCL21 is unique in that it contains an extended C-terminus not found in other chemokines like CCL19. Deletion of this extended C-terminus reduces CCL21's affinity for heparin and transferring the CCL21 C-terminus to CCL19 enhances heparin binding mainly through non-specific, electrostatic interactions.

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