ABSTRACT
Single-walled carbon nanotubes (SWCNTs) have potential for a wide range of applications in diverse fields, but the heterogeneous properties of the synthesized mixtures of SWCNT types hinder the realization of these aspirations. Recent developments in extractive purification methods of polychiral SWCNT mixtures have somewhat gradually alleviated this problem, but either the yield or purity of the obtained fractions remains unsatisfactory. In this work, we showed the possibility of simultaneously achieving both the aforementioned goals, commonly considered mutually exclusive, via the enhancement of the capabilities of the conjugated polymer extraction (CPE) technique. We found that combining small molecular species, which alone are unwanted in the system, with a selective poly(9,9'-dioctylfluorenyl-2,7-diyl-alt-6,6'-(2,2'-bipyridine)) polymer increased the concentration of the harvested SWCNTs by an order of magnitude while maintaining near-monochiral purity of the materials. The conducted modeling revealed that the presence of these additives facilitated the folding of conjugated polymers around (6,5) SWCNTs, leading to a substantial increase in the concentration and quality of the SWCNT suspension. The obtained results lay the foundation for the widescale implementation of the CPE of usually scarcely available chirality-defined SWCNTs owing to the molecular chaperones expediting the folding of the conjugated polymers.
ABSTRACT
V-shaped and star-shaped hydroxylamine-functionalized polymethacrylates designed as nanosized conjugates (<120 nm) with anticancer agent, namely, doxorubicin (DOX), were evaluated in vitro toward their potential usage as drug delivery systems in breast cancer (MCF-7) treatment. Statistical analysis of MTS assay results showed that the 4-arm conjugate (n(DOX) = 16) was the most effective polymeric system against MCF-7/W (wild type) and MCF-7/R (DOX resistant) cell lines. Apoptosis assay analysis showed that MCF-7/R cells cultured with nonlinear copolymers died due to necrosis and late apoptotis, whereas MCF-7/W cells were in early and late apoptosis. Among all tested conjugates, the most promising results with induction of apoptosis without inducing necrosis in both MCF-7 cell lines were obtained for conjugate based on 4-arm stars with low content of DOX. The cell cycle assay revealed that increase of MMA units in 4-arm copolymers induced MCF-7/R cell arrest in the SubG1 phase. In the same cell line, the corresponding conjugates triggered S and G2/M arrest. Gradual internalization of the chosen conjugate by MCF-7/R cells was monitored via fluorescence microscopy showing its main localization in the cytoplasm.
