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We report here a unique method of formulating camptothecin-polylactide (CPT-PLA) conjugate nanoparticles,
termed nanoconjugates (NCs), through CPT/(BDI)ZnN(TMS)2 [(BDI) ) 2-((2,6-diisopropylphenyl)amido)-4-
((2,6-bisalkyl)-imino)-2-pentene] mediated polymerization of lactide (LA) followed by nanoprecipitation. When
CPT was used as the initiator to polymerize LA in the presence of (BDI)ZnN(TMS)2, the polymerization was
completed within hours with nearly 100% CPT loading efficiency and 100% LA conversion. CPT loading as
high as 19.5% can be achieved for the CPT-polylactide (CPT-PLA) conjugate prepared at a LA/CPT ratio of 10.
The steric bulk of the chelating ligands and the type of metals used had a dramatic effect on the initiation of the
LA polymerization and the tendency of the ring-opening of the CPT lactone. The CPT/(BDI)ZnN(TMS)2-mediated
LA polymerization yielded CPT-PLA conjugates with well-controlled molecular weights and narrow molecular
weight distributions (1.02-1.18). The nanoprecipitation of CPT-PLA led to the formation of NCs around 100 nm
in size with narrow particle size distributions. Sustained release of CPT from CPT-PLA NCs was achieved without
burst release. CPT-PLA NCs were toxic to PC-3 cells with tunable IC50 possible by adjusting the drug loading
of the CPT-PLA NCs.

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