The protein and gold nanoparticle (AuNP) interfacial interaction has broad implications for biological and biomedical applications of AuNPs. In situ characterization of the morphology and structural evolution of protein on AuNPs is difficult. We have found that the protein coating layer formed by bovine serum albumin (BSA) on AuNP is highly permeable to further organothiol adsorption. Using mercaptobenzimidazole (MBI) as a molecular probe, it is found that BSA interaction with AuNP is an exceedingly lengthy process. Structural modification of BSA coating layer on AuNP continues even after 2 days’ aging of the (AuNP/BSA) mixture. While BSA is in a near full monolayer packing on the AuNPs, it passivates only up to 30% of the AuNP surfaces against MBI adsorption. Aging reduces the kinetics of the MBI adsorption. However, even in the most aged BSA-coated AuNP (3 days), 80% of the MBI adsorption occurs within the first 5 min of the MBI addition to the (AuNP/BSA) mixture. The possibility of MBI displacing the adsorbed BSA was excluded with quantitative BSA adsorption studies. Besides MBI, other organothiols including endogenous amino acid thiols (cysteine, homocysteine, and glutathione) were also shown to penetrate through the protein coating layer and be adsorbed onto AuNPs. In addition to providing critical new understanding of the morphology and structural evolution of protein on AuNPs, this work also provides a new venue for preparation of multicomponent composite nanoparticle with applications in drug delivery, cancer imaging and therapy, and material sciences.
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