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Manipulating Nanoparticle Aggregates Regulates Receptor-Ligand Binding in Macrophages.

Yuri KimHee Joon JungYunjung LeeSagang KooRamar ThangamWoo Young JangSeong Yeol KimSangwoo ParkSungkyu LeeGunhyu BaeKapil Dev PatelQiang WeiKi-Bum LeeRamasamy PaulmuruganWoong Kyo JeongTaeghwan HyeonDokyoon KimHeemin Kang
Published in: Journal of the American Chemical Society (2022)
The receptor-ligand interactions in cells are dynamically regulated by modulation of the ligand accessibility. In this study, we utilize size-tunable magnetic nanoparticle aggregates ordered at both nanometer and atomic scales. We flexibly anchor magnetic nanoparticle aggregates of tunable sizes over the cell-adhesive RGD ligand (Arg-Gly-Asp)-active material surface while maintaining the density of dispersed ligands accessible to macrophages at constant. Lowering the accessible ligand dispersity by increasing the aggregate size at constant accessible ligand density facilitates the binding of integrin receptors to the accessible ligands, which promotes the adhesion of macrophages. In high ligand dispersity, distant magnetic manipulation to lift the aggregates (which increases ligand accessibility) stimulates the binding of integrin receptors to the accessible ligands available under the aggregates to augment macrophage adhesion-mediated pro-healing polarization both in vitro and in vivo. In low ligand dispersity, distant control to drop the aggregates (which decreases ligand accessibility) repels integrin receptors away from the aggregates, thereby suppressing integrin receptor-ligand binding and macrophage adhesion, which promotes inflammatory polarization. Here, we present "accessible ligand dispersity" as a novel fundamental parameter that regulates receptor-ligand binding, which can be reversibly manipulated by increasing and decreasing the ligand accessibility. Limitless tuning of nanoparticle aggregate dimensions and morphology can offer further insight into the regulation of receptor-ligand binding in host cells.
Keyphrases
  • lymph node
  • induced apoptosis
  • escherichia coli
  • stem cells
  • binding protein
  • staphylococcus aureus
  • cell proliferation
  • signaling pathway
  • transcription factor
  • pseudomonas aeruginosa
  • mass spectrometry
  • cell therapy