Siglecs are immunomodulatory receptors that regulate immune cell function. A fundamental challenge in studying Siglec-ligand interactions is the low affinity of Siglecs for their ligands. Inspired by how nature uses multivalency, we developed Siglec-liposomes as a highly multivalent and versatile platform for detecting Siglec glycan ligands in which recombinant Siglecs were conjugated to liposomes using the SpyCatcher-SpyTag system. Siglec-liposomes offer tunable multivalency and a modular assembly, enabling presentation of different Siglecs on the same liposome. Using Siglec-liposomes, we profiled Siglec ligands on human leukocytes, revealing new insights into Siglec ligands. Moreover, Siglec-liposomes are in vivo compatible, where we demonstrated that Siglec-7-liposomes bind to the brain vasculature in a mucin-dependent manner. Given the abundance of Siglec ligands on T cells, we investigated whether Siglec-liposomes modulate T cell function and find that Siglec-7-liposomes increase T cell proliferation in a ST3Gal1-dependent and CD43-independent manner. Taken together, Siglec-liposomes are a versatile and sensitive tool for detecting Siglec ligands and immunomodulation.
An ultrasensitive and modular platform to detect Siglec ligands and control immune cell function.
一种超灵敏且模块化的平台,用于检测 Siglec 配体并控制免疫细胞功能
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作者:Jame-Chenarboo Zeinab, Schmidt Edward N, Crichton Madeline, Takahashi-Yamashiro Kei, Lima Guilherme M, Luna-Dulcey Liany, Jung Jaesoo, Ivison Sabine, St Laurent Chris D, Enterina Jhon R, Lin Sung-Yao, Sarkar Susmita, John Reni, Nanjappa Som G, Malaker Stacy A, Levings Megan K, Marth Jamey D, Derda Ratmir, Macauley Matthew S
| 期刊: | bioRxiv | 影响因子: | 0.000 |
| 时间: | 2025 | 起止号: | 2025 Jun 12 |
| doi: | 10.1101/2025.06.10.658684 | 研究方向: | 细胞生物学 |
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