The self-assembly of inorganic nanoparticles (NPs) has garnered considerable attention due to the potential for fabricating functional structures with unique collective properties. In recent years, polymers have emerged as valuable candidates in assisting the organization of NPs into complex architectures with multiple capabilities. Researchers have shown that polymer-grafted nanoparticles (PGNPs) facilitate the use of advanced nanostructures with tailored properties in biomedical applications. Although, continued exploration of the rational design and tailoring of PGNP assemblies is needed to expand our understanding before we can fully realize the potential of these structures in desired applications. My dissertation aims to investigate the fundamental aspects and elucidate the underlying mechanisms in the self-assembly of PGNPs for modern biomedical applications.

A facile and versatile solution-based strategy was utilized to explore the individual self-assembly of PGNPs with anisotropic NPs and the co-assembly of binary PGNPs with distinct sizes. We focused on designing, characterizing, and exploring the optical properties of hierarchical assembly structures produced from inorganic NPs tethered with amphiphilic block copolymers (BCPs). Individual PNGPs with anisotropic NPs and binary mixtures of small and large PGNPs produce vesicle structures with well-defined packing arrangements. My work shows how key parameters, including polymer chain length, nanoparticle size, and concentration, influence the self-assembly behavior and the formation of vesicles in each system. Through a combination of experimental observations and theoretical considerations, I highlight the significance of polymer shell shape in dictating the self-assembly behavior of individual anisotropic PGNPs. Moreover, I demonstrate that elevated temperatures impacted the stability and optical responses of the vesicle structures. In co-assembly studies, my work describes the macroscopic segregation of PGNPs with different sizes in the vesicular membrane, which is attributed to the conformation entropy gain of the grafted copolymer ligands. This research will provide valuable insights into the self-assembly behavior and fundamental design of PGNP structures relevant to biomedical applications.