Summary: Robust thermosensitive PAH‐g‐PNIPAAm/PSS particles were prepared by addition of a poly(allylamine)‐graft‐poly(N‐isopropylacrylamide) particle suspension into poly(styrene sulfonate) solution above the LCST of PAH‐g‐PNIPAAm. Scanning force microscopy revealed stable and well‐separated particles in water at room temperature. The zeta‐potential showed a negative surface charge of the particles. Their thermosensitive behavior was demonstrated by dynamic light scattering. The release of rhodamine 6G loaded particles could respond to the incubation temperature.
Fabrication of thermosensitive and robust particle by suspension of in situ formed PAH‐g‐PNIPAAm particle above the LCST in PSS solution. 相似文献
Self‐assembled poly(N‐methylaniline)–lignosulfonate (PNMA–LS) composite spheres with reactive silver‐ion adsorbability were prepared from N‐methylaniline by using lignosulfonate (LS) as a dispersant. The results show that the PNMA–LS composite consisted of spheres with good size distribution and an average diameter of 1.03–1.27 μm, and the spheres were assembled by their final nanofibers with an average diameter of 19–34 nm. The PNMA–LS composite spheres exhibit excellent silver‐ion adsorption; the maximum adsorption capacity of silver ions is up to 2.16 g g?1 at an adsorption temperature of 308 K. TEM and wide‐angle X‐ray results of the PNMA–LS composite spheres after absorption of silver ions show that silver ions are reduced to silver nanoparticles with a mean diameter of about 11.2 nm through a redox reaction between the PNMA–LS composite and the silver ions. The main adsorption mechanism between the PNMA–LS composite and the silver ions is chelation and redox adsorption. In particular, a ternary PNMA–LS–Ag composite achieved by using the reducing reaction between PNMA–LS composite spheres and silver ions can be used as an antibacterial material with high bactericidal rate of 99.95 and 99.99 % for Escherichia coli and Staphylococcus aureus cells, respectively. 相似文献
Electroconductive poly(N‐butylaniline)–lignosulfonate (PBA–LS) composite nanospheres were prepared in a facile way by in situ, unstirred polymerization of N‐butylaniline with lignosulfonate (LS) as a dispersant and dopant. The LS content was used to optimize the size, structure, electroconductivity, solubility, and silver ion adsorptive capacity of the PBA–LS nanospheres. Uniform PBA–LS10 nanospheres with a minimal mean diameter of 375 nm and high stability were obtained when the LS content was 10 wt %. The PBA–LS10 nanospheres possess an increased electroconductivity of 0.109 S cm?1 compared with that of poly(N‐butylaniline) (0.0751 S cm?1). Furthermore, the PBA–LS10 nanospheres have a maximal silver‐ion sorption capacity of 815.0 mg g?1 at an initial silver ion concentration of 50 mmol L ?1 (25 °C for 48 h), an enhancement of 70.4 % compared with PBA. Moreover, a sorption mechanism of silver ions on the PBA–LS10 nanospheres is proposed. TEM and wide‐angle X‐ray diffraction results showed that silver nanoparticles with a diameter size range of 6.8–55 nm was achieved after sorption, indicating that the PBA–LS10 nanospheres had high reductibility for silver ions. 相似文献
Despite the polymeric vascular disrupting agent (poly(L‐glutamic acid)‐graft‐methoxy poly(ethylene glycol)/combretastatin A4) nanoparticles can efficiently inhibit cancer growth, their further application is still a challenge owing to the tumor recurrence and metastasis after treatment. In this study, two poly(L‐glutamic acid)‐drug conjugates for chemo‐and photodynamic combination therapy are fabricated. PLG‐g‐mPEG‐CA4 nanoparticles are prepared by combretastatin A4 (CA4) and poly(L‐glutamic acid)‐graft‐methoxy poly(ethylene glycol) (PLG‐g‐mPEG) using the Yamaguchi esterification reaction. PLG‐g‐mPEG‐TPP (TPP: 5, 10, 15, 20‐tetraphenylporphyrin) nanoparticles are constructed using PLG‐g‐mPEG and amine porphyrin through condensation reaction between carboxyl group of PLG‐g‐mPEG and amino group of porphyrin. The results showed that PLG‐g‐mPEG‐CA4 nanoparticles have good antitumor ability. PLG‐g‐mPEG‐TPP nanoparticles can produce singlet oxygen under the laser irradiation. Moreover, the combined therapy of PLG‐g‐mPEG‐CA4 and PLG‐g‐mPEG‐TPP nanoparticles has higher antitumor effect than the single chemotherapy or the single photodynamic therapy in vitro. The combination of CA4 nondrug and photodynamic therapy provides a new insight for enhancing the tumor therapeutic effect with vascular disrupting agents and other therapy. 相似文献
Poly(4‐vinylpyridine) macromonomer (St‐P4VP) with a styryl end group was synthesized by atom transfer radical polymerization (ATRP) of 4‐vinylpyridine using p‐(chloromethyl)styrene (CMSt) as functional initiator, CuCl as catalyst and tris[2‐(dimethylamino)ethyl]amine (Me6TREN) as ligand in 2‐propanol. The structure of St‐P4VP macromonomer was identified by proton nuclear magnetic resonance (1H NMR). The result of gel permeation chromatography (GPC) illustrated that the number‐average molecular weight of St‐P4VP could be controlled by adjusting polymerization conditions. Poly(4‐vinylpyridine) grafted polystyrene microspheres (P4VP‐g‐PSt) were then prepared by dispersion copolymerization of styrene with St‐P4VP macromonomers. The effects of polymerization reaction parameters such as medium polarity, concentration of St‐P4VP macromonomer and polymerization temperature on the sizes and size distribution of P4VP‐g‐PSt microspheres were investigated. The results of transmission electron microscopy (TEM), scanning electron microscopy (SEM) and laser light scattering (LLS) indicated that mono‐dispersed P4VP‐g‐PSt microspheres with average diameters of 100–200 nm could be obtained when the molar ratio of St to St‐P4VP was 0.25:100 in ethanol/water mixed solvents (V/V=80:20) at 60°C. Such kind of graft copolymer microspheres was expected to be applied to many fields such as drug delivery system and protein adsorption/separation system due to their particular structure. 相似文献