Optimized Design of Hyaluronic Acid-Lipid Conjugate Biomaterial for Augmenting CD44 Recognition of Surface-Engineered NK Cells
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초록

Triple-negative breast cancer (TNBC) presents treatment challenges due to a lack of detectable surface receptors. Natural killer (NK) cell-based adaptive immunotherapy is a promising treatment because of the characteristic anticancer effects of killing malignant cells directly by secreting cytokines and lytic granules. To maximize the cancer recognition ability of NK cells, biomaterial-mediated ex vivo cell surface engineering has been developed for sufficient cell membrane immobilization of tumor-targeting ligands via hydrophobic anchoring. In this study, we optimized amphiphilic balances of NK cell coating materials composed of CD44-targeting hyaluronic acid (HA)-poly(ethylene glycol) (PEG)-lipid to improve TNBC recognition and the anticancer effect. Changes in the modular design of our material by differentiating hydrophilic PEG length and incorporating lipid amount into HA backbones precisely regulated the amphiphilic nature of HA-PEG-lipid conjugates. The optimized biomaterial demonstrated improved anchoring into NK cell membranes and facilitating the surface presentation level of HA onto NK cell surfaces. This led to enhanced cancer targeting via increasing the formation of immune synapse, thereby augmenting the anticancer capability of NK cells specifically toward CD44-positive TNBC cells. Our approach addresses targeting ability of NK cell to solid tumors with a deficiency of surface tumor-specific antigens while offering a valuable material design strategy using amphiphilic balance in immune cell surface engineering techniques.

키워드

Gamma InterferonGranzyme BHyaluronic AcidLipidMacrogolPerforinBiocompatible MaterialsCd44 Protein, HumanHyaluronan ReceptorsHyaluronic AcidLipidsCell EngineeringCell ImmobilizationCell MembranesDiseasesOrganic AcidsPolyethylene GlycolsTumorsAmphiphilicsAnticancer EffectsCell Surface EngineeringCell-basedNatural Killer CellsOptimized DesignsPoly Ethylene GlycolsPoly(ethylene Glycol)Surface ReceptorsTriple-negative Breast CancersHyaluronic AcidBiomaterialCytokineFas LigandGamma InterferonGranzyme BHermes AntigenHyaluronic AcidLigandLipidLipopolysaccharideMacrogolMacrogol DerivativePerforinTumor AntigenTumor Necrosis FactorTumor Necrosis Factor Related Apoptosis Inducing LigandCd44 Protein, HumanHyaluronic Acid Binding ProteinAntineoplastic ActivityArticleCancer DiagnosisCancer ImmunotherapyCancer InhibitionCell CultureCell EngineeringCell MembraneCell SurfaceCoating (procedure)ConjugateConjugationControlled StudyCytokine ReleaseCytotoxicityDegree Of SubstitutionEnzyme Linked Immunosorbent AssayEvaluation StudyEx Vivo StudyFlow CytometryFluorescenceFluorescence IntensityHumanHuman CellHydrophobicityImmunocompetent CellImmunological SynapseMolecular InteractionMolecular WeightNatural Killer CellNuclear Magnetic ResonanceNuclear Magnetic Resonance SpectroscopyProton Nuclear Magnetic ResonanceRelease AssaySolid TumorSurface PropertySynthesisTriple Negative Breast CancerWst-1 AssayChemistryMetabolismTumor Cell LineBiocompatible MaterialsCell Line, TumorHumansHyaluronan ReceptorsHyaluronic AcidKiller Cells, NaturalLipidsTriple Negative Breast NeoplasmsMOLECULAR-WEIGHTCANCER-CELLSNANOPARTICLESGLYCOL)CHAIN
제목
Optimized Design of Hyaluronic Acid-Lipid Conjugate Biomaterial for Augmenting CD44 Recognition of Surface-Engineered NK Cells
저자
Park, Hee WonLee, WonjeongKim, SungjunJangid, Ashok KumarPark, JaewonLee, Chae EunKim, Kyobum
DOI
10.1021/acs.biomac.3c01373
발행일
2024-02
유형
Article
저널명
Biomacromolecules
25
3
페이지
1959 ~ 1971