Summary: A series of thermally responsive dendritic core-shell polymers were prepared based upon dendritic polyamidoamine (PAMAM), modified with carboxyl end-capped linear poly(N-isopropylacrylamide) (PNIPAAm-COOH) in different ratios via an esterification process to obtain PNIPAAm-g-PAMAM. The graft ratio of PNIPAAm could be adjusted by changing the feed ratio of PAMAM-OH to PNIPAAm-COOH and was verified by 1H NMR and gel penetration chromatography (GPC). The lower critical solution temperature (LCST) of PNIPAAm-g-PAMAM evaluated by UV-vis spectrophotometer was about 32 °C. Indomethacin (IMC) as a model drug was loaded in the thermosensitive polymer-grafted dendrimer derivative and its release behavior was studied below and above its LCST (27 °C vs 37 °C). Results showed that the LCST of PNIPAAm-g-PAMAM was around 32 °C compared with that of the pure PNIPAAm. The release behavior of the indomethacin entrapped in the internal cavities of the PNIPAAm-g-PAMAM showed that almost 77% of the drug was cumulatively released at 27 °C after 10 hours, whereas only 20% was released at 37 °C. The release rate of IMC from the IMC/PNIPAAm-g-PAMAM complex at 37 °C is significantly slower than that at 27 °C, which indicates that the PNIPAAm chains grafted on the surface of PAMAM dendrimer could act as a channel switching on-off button through expending or contracting in response to the temperature variation and could control the drug release by varying the surrounding temperature. 相似文献
Summary: After synthesizing both hard poly(organophosphazenes), which acted as strong hydrogels at a temperature below 37 °C, and soft poly(organophosphazenes), which displayed the opposite properties, we blended the polymers. When these polymers were blended at an appropriate ratio, the blended aqueous solution changed into a transparent hydrogel with improved mechanical properties at a temperature of 37 °C. According to DSC and IR measurements, the two polymers blended homogeneously and exhibited a behavior characteristic of a completely different copolymer.
An aqueous poly(organophosphazene) solution at room temperature (left) is reversibly and rapidly transformed into a transparent hydrogel at body temperature (right) when a hard poly(organophosphazene) is blended with a soft one at an appropriate ratio. 相似文献
Thermosensitive poly[N-vinylacetamide-co-vinylacetate][P(NVA-co-VAc)] hydrogels were prepared via free radical copolymerization from hydrophilic NVA and hydrophobic VAc in the presence of butylenes-bis (N-vinylacetamide)(Bis-NVA) as crosslinker. Scanning electron microscopy(SEM) images reveal that the as-prepared hydrogels were of three-dimensional network with irregular cave structure. The prepared hydrogels with more NVA in the feed swelled faster and the swelling ratio of the hydrogels gradually decrease... 相似文献
AbstractThe antioxidant activity of pyridylselenium compounds has been evaluated by 1,1-diphenyl-2-picrylhydrazyl (DPPH) free radical and nitric oxide (NO) scavenging methods. Pyridylselenium compounds have shown far superior (100–1000 times) antioxidant property than ebselen. The control release of bis(2-pyridyl) diselenide from poly(acrylamide) hydrogels has been studied in order to evaluate its release mechanism and diffusion coefficient. The later study also demonstrates that the pyridylselenium loading into the polymer matrix increases the magnitude and the rate of the radical scavenging activity of the poly(acrylamide) hydrogels. 相似文献
Summary: In this work the releasing of Bovine Serum Albumin (BSA) from thermosensitive hydrogels of alginate-Ca2+/PNIPAAm was investigated. The hydrogels are constituted of PNPAAm network interpenetrated in alginate-Ca2+ network, so the hydrogels are IPN-typed. The PNIPAAm network was synthesized in the first step in which the sodium alginate remained soluble. The alginate-Ca2+ network was formed in the second step by immersion the membrane obtained on the first step in aqueous calcium chloride. It was changed the amount of NIPAAm in the feed solution of the first step. The fractions of BSA released as a function of time were treated according to the mathematical model recently published by our lab [J. Coll. Interf. Sci. 2007 , 310, 128] that allows predicting the whole profile of solute released from polymer networks. This mathematical model is based in the partition phenomena. The amount of BSA released from alginate-Ca2+/PNIPAAm hydrogels changes inversely to both amount of PNIPAAm and temperature. Thus, the IPN-typed matrixes of alginate-Ca2+/PNIPAAm may be considered as smart hydrogels for release the BSA because the amount and rate of released BSA can be tailored by the amount of PNIPAAm in the hydrogel and by the control of temperature. Finally, the whole profile of released BSA can be adequately fitted by the model based in the partition phenomenon. From that model the kinetic parameter t1/2 and rate constant of releasing, kR, were calculated for the different hydrogels investigated in this work. 相似文献
Biocompatible/biodegradable poly(D,L-lactic acid)/layered silicate nanocomposites were prepared by the solution-intercalation film casting technique. The obtained nanocomposites present a shift of glass transition temperature (Tg) to higher values. An increase in the onset temperature of thermal degradation (Tonset) was also observed by TGA. Hydrolytic degradation of PLA nanocomposites becomes apparent after the first 3 months of immersion of specimens into deionized water. Drug release studies from PLA/organoclay nanocomposite membranes showed slightly faster release behavior in comparison with unreinforced specimens containing 5 phr guaifenesin (GFN), whereas the different organic clay modifications studied in this work, did not seem to have any effect in the release profile of GFN. 相似文献
