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Modulation of Macrophages by In Situ Ligand Bridging
- Kim, Seong Yeol ;
- Thangam, Ramar ;
- Kang, Nayeon ;
- Hong, Hyunsik ;
- Kim, Chowon ;
- Lee, Sungkyu ;
- Son, Subin ;
- Lee, Hyun-Jeong ;
- Tag, Kyong-Ryol ;
- Min, Sunhong ;
- Jeong, Daun ;
- Hwang, Jangsun ;
- Kim, Kanghyeon ;
- Kim, Dahee ;
- Kim, Yuri ;
- Joo, Jinmyoung ;
- Kim, Bong Hoon ;
- Zhu, Yangzhi ;
- Park, Sung-Gyu ;
- Song, Hyun-Cheol ;
- Sun, Wujin ;
- Ahn, Jae-Pyoung ;
- Jang, Woo Young ;
- Paulmurugan, Ramasamy ;
- Kim, Hong-Kyu ;
- Kim, Jong Seung ;
- Kang, Heemin
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- Title
- Modulation of Macrophages by In Situ Ligand Bridging
- Issued Date
- 2023-04
- Citation
- Kim, Seong Yeol. (2023-04). Modulation of Macrophages by In Situ Ligand Bridging. Advanced Functional Materials, 33(16). doi: 10.1002/adfm.202215166
- Type
- Article
- Author Keywords
- in situ bridging ; ligand bridging ; macrophage adhesions ; macrophage polarization ; remote controls
- Keywords
- T-CELL-ACTIVATION ; DUAL ROLES ; ADHESION ; FIBRONECTIN ; POLARIZATION ; COLLAGEN ; BINDING ; INFLAMMATION ; RGD ; NEUTROPHILS
- ISSN
- 1616-301X
- Abstract
-
Extracellular matrix (ECM) proteins containing cell-attachable Arg-Gly-Asp (RGD) sequences exhibit variable bridging and non-bridging in fibronectin-collagen and laminin-collagen complexes that can regulate inflammation, tissue repair, and wound healing. In this study, linking molecule-mediated conjugation of 1D magnetic nanocylinders (MNCs) to material surfaces pre-decorated with gold nanospheres (GNSs) is performed, thereby yielding RGD-coated MNCs (RGD-MNCs) over RGD-coated GNSs (RGD-GNSs) in a non-bridging state. The RGD-MNCs are drawn closer to the RGD-GNSs via magnetic field-mediated compression of the linking molecules to establish the bridging between them. Relative proportion of the RGD-MNCs to the RGD-GNSs is optimized to yield effective remote stimulation of integrin binding to variably bridged RGDs similar to that of invariably bridged RGDs used as a control group. Remote manipulation of the RGD bridging facilitates the attachment structure assembly of macrophages that leads to pro-healing/anti-inflammatory phenotype acquisition. In contrast, the non-bridged RGDs inhibited macrophage attachment that acquired pro-inflammatory phenotypes. The use of various nanomaterials in constructing heterogeneous RGD-coated materials can further offer various modes in remote switching of RGD bridging and non-bridging to understand dynamic integrin-mediated modulation of macrophages that regulate immunomodulatory responses, such as foreign body responses, tissue repair, and wound healing. © 2023 Wiley-VCH GmbH.
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- Publisher
- John Wiley & Sons Ltd.
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