Tuning the Structure of Poly(aspartic acid)s' Self-Assemblies to Enhance Cellular Uptake.

Self-assembled nanoparticles formed with amphiphilic block or graft copolymers are being extensively studied for their use in a variety of biological and industrial applications, including targeted drug delivery. This study reports a novel strategy to tune the structure of self-assembled nanoparticles for enhancing the cellular uptake by varying the hydrophilic ratio of amphiphilic graft copolymers. We synthesized poly(aspartic acid) (PAsp) substituted with octadecyl chains (C18) at varying degrees of substitution (DS), ranging from 4.5 to 37.5 mol%, which could form self-assemblies in an aqueous solution. As the DS increased, a morphological transition was observed-from spherical assemblies (DS 4.5 and 9.1) to rod-like (DS 19.0), vesicular (DS 25.7), and lamellar-like structures (DS 37.6). Further, Trans-Activator of Transcription (TAT) as the cell penetrating peptide to the synthesized amphiphilic graft copolymers leads to an enhanced cellular uptake of the biomimetic self-assembly. In particular, the lamellar-like self-assemblies resulted in a 1.3-fold increase of cellular uptake, as compared to the spherical self-assemblies, and a 3.6-fold increase, as compared to the vesicles. Therefore, tuning the structure of poly(aspartic acid)s' self-assemblies was proven as an effective strategy to enhance the cellular uptake, while minimizing invasive cell damage. This new strategy to tune the morphologies of self-assemblies will serve to improve the cell penetrating activity for targeted drug delivery.