Multiscale Approach to Investigate Self-Assembly ofTelodendrimer Based Nanocarriers for Anticancer Drug Delivery

摘要

Delivery of poorly soluble anticancer drugs can be achieved by employing polymeric drug delivery systems, capable of forming stable self-assembled nanocarriers with drug encapsulated within their hydrophobic cores. Computational investigations can aid the design of efficient drug-delivery platforms; however, simulations of nanocarrier self-assembly process are challenging due to high computational cost associated with the large system sizes (millions of atoms) and long time scales required for equilibration. In this work, we overcome this challenge by employing a multiscale computational approach in conjunction with experiments to analyze the role of the individual building blocks in the self-assembly of a highly tunable linear poly(ethylene glycol)-b-dendritic oligo(cholic acid) block copolymer called telodendrimer. The multiscale approach involved developing a coarse grained description of the telodendrimer, performing simulations over several microseconds to capture the self-assembly process, followed by reverse mapping of the coarse grained system to atomistic representation for structural analysis. Overcoming the computational bottleneck allowed us to runmultiple self-assembly simulations and determine average size, drug-telodendrimermicellar stoichiometry, optimal drug loading capacity, and atomisticdetails such hydrogen-bonding and solvent accessible area of the nanocarrier.Computed results are in agreement with the experimental data, highlightingthe success of the multiscale approach applied here.