4.7 Article

Effect of Protein Corona on Mitochondrial Targeting Ability and Cytotoxicity of Triphenylphosphonium Conjugated with Polyglycerol-Functionalized Nanodiamond

Journal

MOLECULAR PHARMACEUTICS
Volume 18, Issue 7, Pages 2823-2832

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.molpharmaceut.1c00188

Keywords

nanoparticles; triphenylphosphonium; protein corona; mitochondrial targeting; cytotoxicity; polyglycerol

Funding

  1. JSPS KAKENHI [20H02584]
  2. Grants-in-Aid for Scientific Research [20H02584] Funding Source: KAKEN

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Functionalization of nanoparticles with triphenylphosphonium (TPP) targeting moiety was explored in this study, revealing the influence of protein corona from fetal bovine serum and human plasma on targeting ability and cytotoxicity. The findings demonstrated that the protein corona could mitigate cytotoxicity of nanoparticle functionalization, but high protein density might reduce the targeting specificity at the subcellular level.
Functionalization of nanoparticles (NPs) with targeting moieties has a high potential to advance precision nanomedicine. However, the targeting moieties on a NP surface are known to be masked by a protein corona in biofluids, lowering the targeting efficiency. Although it has been demonstrated at the cellular level, little is known about the influence of the protein corona on the subcellular targeting. Herein, we adopted triphenylphosphonium (TPP) as a mitochondrial targeting moiety and investigated the effects of protein coronas from fetal bovine serum and human plasma on its targeting ability and cytotoxicity. Specifically, we introduced TPP in low (l) and high (h) densities on the surface of nanodiamond (ND) functionalized with polyglycerol (PG). Despite the corona-free PG interface, we found that the TPP moiety attracted proteins to form a corona layer with clear linearity between the TPP density and the protein amount. By performing investigations on human cervix epithelium (HeLa) and human lung epithelial carcinoma (A549) cells, we further demonstrated that (1) the protein corona alleviated the cytotoxicity of both ND-PG-TPP-l and -h, (2) a smaller amount of proteins on the surface of ND-PG-TPP-l did not affect its mitochondrial targeting ability, and (3) a larger amount of proteins on the surface of ND-PG-TPP-h diminished its targeting specificity by restricting the NDs inside the endosome and lysosome compartments. Our findings will provide in-depth insights into the design of NPs with active targeting moiety for more precise and safer delivery at the subcellular level.

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