![Author ORCID: We display the ORCID iD icon alongside authors names on our website to acknowledge that the ORCiD has been authenticated when entered by the user. To view the users ORCiD record click the icon. [opens in a new tab]](https://chemrxiv.org/engage/assets/public/chemrxiv/images/logos/orcid.png)
Abstract
Poly(lactic-co-glycolic acid) (PLGA) is a widely utilized polymer for biomedical applications due to its biocompatibility and degradability in vivo. Traditional methods of fabrication of drug-loaded nanoparticles (NPs) employ the random sequence form of linear PLGA to yield non-crosslinked polymeric NPs that form when the polymer nanoprecipitates out of solution. Given the large-scale use of PLGA-based polymeric drug delivery systems to date, it is crucial to be able to control the ratio and sequence of lactic and glycolic components in the overall drug delivery system, which in turn can impact factors such as stability, drug loading, drug release and degradability. In this work, we present a novel PLGA-inspired NP polymerization technique, which allows the formation of NPs via the cross-linking of precisely sequenced short oligolactoglycolic acid dimethacrylates (OLGADMAs). Following the synthesis of a range of OLGADMAs we successfully generated a library of NPs via this rapid and surfactant-free nanopolymerization method, which permits the simultaneous NP formation and encapsulation of drugs such as dexamethasone. Our results indicate that NPs produced through this nanopolymerization technique with precisely controlled sequences exhibit heightened stability compared to conventionally sequenced and non-sequence controlled PLGA, as evidenced by minimal pH changes over a five-week span. This improved stability is attributed to simultaneous crosslinking and co-polymerization of the OLGADMAs. Moreover, the long-acting NPs demonstrated minimal cytotoxicity and uniform cellular uptake in vitro. We conclude that the ability to precisely regulate the sequence of short PLGA-inspired monomers and employ a unique in situ nanopolymerizing reaction results in exceptionally stable NPs for sustained drug delivery and opens exciting possibilities for the development of a range of long-lasting drug delivery systems with programmable structure and function.
Supplementary materials
Title
Supplementary Information
Description
Table of Contents
S1. General procedures and instrumentation 2
S2. Synthesis of acids 1 3
S3. General synthetic procedures 11
S4. Characterization of compounds 14
S5. 1H and 13C NMR spectra of OLGADMs 49
S6. Typical composition of nanoprecipitation polymerization reactions 57
S7. Optimization of dexamethasone encapsulation 58
S8. ATR-FTIR spectra of NPs 59
S9. 1H NMR and DLS study of the nanoprecipitation polymerization reaction 61
S10. Stability of dexamethasone under typical reaction conditions 62
S11. 1H NMR analysis of released dexamethasone 63
S12. Size-tunability of dexamethasone-loaded OLGADM-based NPs 64
S13. Synthesis of PLGA alt 64
S14. Dynamic Light Scattering (DLS) and Electrophoretic Light Scattering (ELS) 66
S15. Intensity-weighted nanoparticle size distributions and correlation functions 67
S16. Quantitation of dexamethasone 73
S17. Transmission Electron Microscopy (TEM) 73
S18. ζ-potential Analysis During Storage at Room Temperature 73
S19. References 74
Actions
