Table 2.
Applications of NPs in osteoimunomodulation via modulating macrophage response.
| Strategies for Regulating Macrophage Polarization | Applications of NPs in Osteoimunomodulation | References |
|---|---|---|
| Intrinsic properties | Gold, TiO2, and cerium oxide (CeO2) NPs can enhance M2 polarization. | [116,117,118] |
| Nanopore structure and pore size | NPs with pores of larger size (100 and 200 nm) were highly anti-inflammatory and inhibited M1 polarization. | [119] |
| The nanoneedle structure induced M2 polarization. The micropattern sizes of 12 μm and 36 μm in the micro/nano hierarchy enhanced M2 polarization. |
[120] | |
| Surface roughness | Ti with smooth surface stimulated M1 activation. Ti with rough surface enhanced M2 polarization. |
[122] |
| Composition | Gold NPs fused hexapeptides Cys-Leu-Pro-Phe-Phe-Asp, peptide arginine-glycine-aspartic acid (RGD), and IL-4 could stimulate M2 polarization. | [112,126,127] |
| CeO2 NPs with hydroxyapatite could enhance M2 polarization. | [128] | |
| Strontium (Sr)- or copper (Cu)-doped bioactive glass particles promoted M2 polarization and enhanced osteogenesis. | [124,125] | |
| Drug delivery | Various nanocarriers have delivered IL-4 (anti-inflammatory cytokine) to induce M2 polarization. | [131,132,133] |
| NPs can deliver S1P synthetic analog to direct macrophage polarization toward M2. | [134] | |
| CD163 gene has been encapsulated into polyethyleneimine NPs decorated with a mannose ligand to induce CD163 expression and macrophage polarization toward M2. | [137] | |
| miR-223 5p mimic was delivered to induce macrophage polarization to M2. | [138] | |
| Resolvin D1-loaded gold nanocages (AuNC) were coated with M1-like macrophage membranes to enhance M2 polarization. | [139] | |
| A sequential release of therapeutics induces the M1-to-M2 phenotype switch during tissue regeneration. | Spillar et al. designed a scaffold that achieved a sequential release of first IFN-γ and then IL-4 to modulate macrophage polarization from early stage M1 to later-stage M2. | [142] |
| NPs carry both miRNA-155 and miRNA-21 to sequentially stimulate macrophage polarization first toward M1 and then the M2 phenotype. | [146] | |
| Microcrystalline bioactive glass scaffolds with different doses of ZnO orchestrate the sequential M1-to-M2 macrophage polarization. | [149] | |
| Sr-substituted nanohydroxyapatite (nano-SrHA) coatings and IFN-γ to the surface of native SIS membrane control a sequential M1-M2 macrophage transition. | [150] |