Structural distortion of β-cyclodextrin plays a key role for the pH-dependent host-guest chemistry with doxorubicin, evident by electrochemical and molecular dynamics approach

β-cyclodextrin (β-CD) is the potential drug carrier to deliver antitumor drugs like doxorubicin (DOX). However, the mechanism for the inclusion complex formation is still unclear and needs to be explored. This study investigated the effect of pH on the inclusion of DOX into thiolated β-CD (β-CD-SH) by electrochemical and molecular dynamics (MD) simulation. The electrochemical study shows a clear difference at different pH. The redox peak due to the DOX is strongly influenced by pH. At neutral pH, the peak intensity decreases with time, while slight variation is observed at acidic and basic pH. Depicting the association of DOX to the β-CD-SH cavity at neutral pH. Also, due to the association, the charge transfer resistance variation increased with time at neutral pH, decreased at basic and acidic pH. The electrochemical study was further supported by MD simulation, suggesting that the cyclodextrins ring gets slightly elongated due to the flipping of glucose units, specifically at neutral pH leads to a strong association. Also, another significant result observed that the DOX forms an inclusion complex with β-CD-SH in quinol conformation, not in quinone. Briefly, the study provides the necessary molecular binding information for designing an effective β-CD based targeted drug delivery system.