"We synthesized TiO₂-HoMSs through sequential template approach, and introduced antibacterial agent Methylisothiazolinone (MIT) as model molecules into HoMSs," said Prof. WANG. 

By analyzing the behavior of HoMSs during drug release, the researchers discovered that the release of the molecules from HoMSs went through sequential release stages, namely burst release, sustained release, and stimulus responsive release. 

In detail, by simply adjusting the amount of MIT-HoMSs introduced into the environment, the desired concentration can be quickly reached in the burst release stage due to the MIT molecules absorbed on the outer surface of HoMSs. 

The sustained release of MIT molecules in π-π stacked state in the cavity of HoMSs could maintain the required concentration for a long period and inhibit the growth of bacteria. 

The triple-shelled HoMS could provide a long sterility period in a bacteria-rich environment that is nearly 8 times longer than that of the pure antimicrobial agent under the same conditions. 

Owing to different adsorption characteristics in HoMSs and physical barriers from the multishells, drug molecules in different locations of HoMSs have different release times. 

All these advantages could be attributed to chemical diffusion- and physical barrier-driven sequential drug release, providing a route for the design of intelligent nanomaterials.