Table 2.
Preclinical strategy of nanoparticle-based NK cell therapy.
| Year | Cell Source | Nanoparticle | Tumor Type | Combination | Ref. |
|---|---|---|---|---|---|
| 2014 | Endogenous | Lipid-calcium-phosphate nanoparticle and liposome-protamine-hyaluronic acid nanoparticle | Melanoma | siTGF-β | [64] |
| 2012 | Endogenous | Liposomal polymeric gel | Metastatic melanoma | TGF-β inhibitor (SB505124) | [65] |
| 2020 | NK-92 | Nanoemulsion | Triple negative breast cancer | Selenocysteine, TGF-β inhibitor (SB505124) | [66] |
| 2017 | Endogenous | Chitosan nanoparticle | Colon cancer | NKG2D, IL-21 | [67] |
| 2018 | Endogenous | DOTAP:cholesterol nanovesicle | Lung cancer | TUSC2 gene, anti-PD-1 | [68] |
| 2019 | Endogenous | Lipid nanoparticle | Triple negative breast cancer | cdGMP, monophosphoryl lipid A | [69] |
| 2017 | Endogenous | PLGA microsphere | Hepatocellular carcinoma | IFN-γ, Transcatheter intra-arterial infusion | [70] |
| 2012 | NK-92MI | Magnetic nanoparticle | B cell lymphoma | External magnetic field | [71] |
| 2018 | Human primary NK cell | Magnetic nanoparticle | Non-small cell lung cancer | External magnetic field | [55] |
| 2015 | Mouse primary NK cell | TRAIL-coated liposome | Lymph node metastatic cancer | TRAIL, anti-NK1.1 | [72] |
| 2020 | NK-92MI | Cationic magnetic nanoparticle | Triple negative breast cancer | - | [73] |
| 2019 | Human primary NK cell | Immunomodulating nanoparticle | Triple negative breast cancer | phenylboronic acid, IgG | [74] |
| 2020 | Mouse primary NK cell | Trifunctional PLGA nanoparticle | EGFR positive solid tumor | Epirubicin | [75] |