4.8 Article

In Vivo Behavior of Ultrasmall Spherical Nucleic Acids

Journal

SMALL
Volume 19, Issue 24, Pages -

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/smll.202300097

Keywords

blood circulation; nanoparticle biodistribution; spherical nucleic acids; tumor accumulation; ultrasmall nanoparticles

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The biological properties of spherical nucleic acids (SNAs) are primarily determined by the oligonucleotide surface density, rather than the nanoparticle core identity. Furthermore, the payload-to-carrier mass ratio of SNAs is inversely proportional to the core size. Ultrasmall nanoparticle constructs (<10 nm diameter) exhibit unique properties, including increased payload-to-carrier ratios, reduced liver accumulation, renal clearance, and enhanced tumor infiltration.
The biological properties of spherical nucleic acids (SNAs) are largely independent of nanoparticle core identity but significantly affected by oligonucleotide surface density. Additionally, the payload-to-carrier (i.e., DNA-to-nanoparticle) mass ratio of SNAs is inversely proportional to core size. While SNAs with many core types and sizes have been developed, all in vivo analyses of SNA behavior have been limited to cores >10 nm in diameter. However, ultrasmall nanoparticle constructs (<10 nm diameter) can exhibit increased payload-to-carrier ratios, reduced liver accumulation, renal clearance, and enhanced tumor infiltration. Therefore, we hypothesized that SNAs with ultrasmall cores exhibit SNA-like properties, but with in vivo behavior akin to traditional ultrasmall nanoparticles. To investigate, we compared the behavior of SNAs with 1.4-nm Au-102 nanocluster cores (AuNC-SNAs) and SNAs with 10-nm gold nanoparticle cores (AuNP-SNAs). Significantly, AuNC-SNAs possess SNA-like properties (e.g., high cellular uptake, low cytotoxicity) but show distinct in vivo behavior. When intravenously injected in mice, AuNC-SNAs display prolonged blood circulation, lower liver accumulation, and higher tumor accumulation than AuNP-SNAs. Thus, SNA-like properties persist at the sub-10-nm length scale and oligonucleotide arrangement and surface density are responsible for the biological properties of SNAs. This work has implications for the design of new nanocarriers for therapeutic applications.

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