13C CP/MAS NMR experiments on polypeptides, poly(β-benzyl l-aspartate) (PBLA), poly(γ-benzyl l-glutamate) (PBLG) and PBLA/PBLG blend have been carried out, in order to elucidate the conformational stability of the polypeptides in the solid state over a wide range of temperatures and its blending effect. The PBLA/PBLG blend with a mixture ratio of 1/1 is prepared by adding trifluoroacetic acid (TFA) solution to alkaline water (TFA-alkaline treatment). From these experimental results, it is found that the conformation of PBLA in the PBLA/PBLG blend sample is changed from left-handed helix (αL-helix and/or ωL-helix) form to the αR-helix form, and then the origin of the formation of the αR-helix form in PBLA comes from the existence of PBLG. Further, from the variable-temperature 13C CP/MAS NMR experiments results, it is shown that the conformational behavior of PBLA in the PBLA/PBLG blend is similar to that of the TFA-alkaline treated PBLA, and also the conformational behavior of PBLG in the PBLA/PBLG blend is similar to that of the TFA-alkaline treated PBLG. 相似文献
Poly(amino acid)has been widely utilized in drug delivery,tissue engineering and biomedical materials.The biomaterials based on poly(glutamic acid)are usually modified via copolymerization with other monomers such as L-aspartic acid to improve the uncontrolled degradation rate.The ring-opening homo- and co-polymerization ofγ-benzyl-L-glutamate N-carboxyanhydride(BLG-NCA)andβ-benzyl-L-aspartate N-carboxyanhydride(BLA-NCA)were carried out in solution by using triethylamine(TEA)as initiator.The BLG-NCA homo... 相似文献
The ring opening polymerization of ε-caprolactone (CL) was initiated by glycol and yttrium tri(2,6-di-tert-butyl-4-methylphenolate)s (Y(OAr)3), preparing dihydroxy-capped poly (ε-caprolactone) (PCL) with controllable molecular weight. 1H NMR and SEC analyses indicate that two kinds of active species and corresponding PCL with different structures exist in
the system. Increasing the ratio of glycol to Y(OAr)3 benefits the formation of monofunctional active species. However, poly(ethylene glycol) (PEG)/Y(OAr)3 system only contains sole bifunctional active species to synthesize copolymer of CL with PEG (poly(CL-b-PEG-b-CL)). Dihydroxycapped PCL as macroinitiator can further initiate the polymerization of 2,2-dimethyltrimethylene carbonate
(DTC). Thus, triblock copolymer of CL with DTC (poly(DTC-b-CL-b-DTC)) has been prepared. 相似文献
Methods described in the literature are inadequate for the preparation of pure polyethylene glycol (PEG) tosylate. Therefore an improved method is presented. The hydroxyl groups on PEG can be quantitatively converted into the tosylate and isolated from the reaction medium free from impurities with no chain cleavage or reduction in molecular weight. 1,2-Di(N-phenyl 2-aminoethoxy) ethane, α,ω-di(N-phenyl 2-aminoethyl) poly(oxyethylene), and α,ω-di(N-phenyl, N-benzyl 2-aminoethyl) poly(oxyethylene) were prepared from the tosylates of tri- and poly(ethylene glycol)s and the corresponding primary and secondary aromatic amines. 相似文献
We combine nanotechnology and chemical synthesis to create a novel multifunctional platinum drug delivery vehicle based on magnetic carbon nanotubes (multiwall carbon nanotubes/Fe3O4@poly(citric acid)/cis‐[(Pt(1,7‐phenanthroline)(DMSO)Cl2)]‐b‐poly(ethylene glycol) (MCNTs/FO@PC/Pt(II)‐b‐PEG)) for targeted cancer therapy. MCNTs/FO@PC/Pt(II)‐b‐PEG was conveniently prepared by conjugating cis‐[Pt(1,7‐phenanthroline)(DMSO)Cl2] complex to MCNTs/FO@PC‐b‐PEG via strong hydrogen‐bonding interactions. In comparison with free cisplatin and Pt(II) complex, MCNTs/FO@PC/Pt(II)‐b‐PEG shows higher solubility in aqueous solution and higher cytotoxicity towards human cervical cancer HeLa cells and human breast cancer MDA‐MB‐231 cells. In vitro release experiments revealed that the platinum drug‐loaded delivery system is relatively stable under physiological conditions (pH = 7.4 and 37 °C) but susceptible to acidic environments (pH = 5.6 and 37 °C) which would trigger the release of loaded drugs. Fluorescence microscopy studies revealed that this magnetic nanohybrid system possesses marked cell‐specific targeting in vitro in the presence of an external magnetic field. The results indicated that the prepared superparamagnetic MCNTs/FO@PC/Pt(II)‐b‐PEG nanohybrid system is a promising candidate for inhibiting the proliferation of cancer cells. 相似文献
A biocompatible complex has been prepared as gene carrier via electrostatic interaction, which is composed of a polycation, that is, poly[(dimethylamino)ethyl methacrylate] end-capped with cholesterol moiety (Chol-PDMAEMA30), along with a polyanion named poly(aspartic acid)-grafted-poly(ethylene glycol) (PASP-g-PEG). The complexes have less cytotoxicity compared to the case of alone Chol-PDMAEMA30 or branched polyethylenimine (PEI) system. In the present study, biocompatible complexes have been prepared as gene carrier via electrostatic interaction, which is composed of a polycation, that is, poly[(dimethylamino)ethyl methacrylate] end-capped with cholesterol moiety (Chol-PDMAEMA30), along with a polyanion named poly(aspartic acid)-grafted-poly(ethylene glycol) (PASP-g-PEG). We first synthesized polysuccinimide (PSI) via condensation polymerization of aspartic acid, and then used PEG-NH2 to react with the partial pentacyclic rings of PSI to yield a kind of graft copolymer polysuccinimide-grafted-poly(ethylene glycol) (PSI-g-PEG). After hydrolysis of the residual succinimide units, a new biodegradable and biocompatible graft copolymer PASP-g-PEG was prepared successfully. Chol-PDMAEMA30 was synthesized via oxyanion-initiated polymerization, as reported in our previous literature. We investigated the interactions between every pair among calf thymus DNA, Chol-PDMAEMA30, and PASP-g-PEG by agarose gel retardation assay. The results indicate that the prepared complexes could completely bind DNA and may become more stable during systemic circulation. The complexes have less cytotoxicity compared to the case of alone Chol-PDMAEMA30 or branched polyethylenimine (PEI) system. Furthermore, the physicochemical properties of the complexes were also investigated by zeta potential, transmission electron microscopy (TEM) and dynamic light scattering (DLS) measurements. These biodegradable and biocompatible polymeric carriers have potential applications in gene delivery. 相似文献
The interaction of PEGylated poly(amino acid)s with their biological targets depends on their chemical nature and spatial arrangement of their building blocks. The synthesis, self‐assembly, and DNA complexation of ABC terblock copolymers consisting of poly(ethylene glycol), (PEG), poly(l ‐lysine), and poly(l ‐leucine), are reported. Block copolymers are produced by a metal‐free, living ring‐opening polymerization of respective amino acid N‐carboxyanhydrides using amino‐terminated PEG as macroinitiator: (PEG‐b‐p(l ‐Lys)x‐b‐p(l ‐Leu)y, PEG‐b‐p(l ‐Leu)x‐b‐p(l ‐Lys)y, and PEG‐b‐p((l ‐Lys)x‐co‐p(l ‐Leu)y). Sizes of self‐assembled nanoparticles depend on the formation method. The nanoprecipitation method proves useful for copolymers with the poly(l ‐lysine) block protected as trifluoroacetate, effective diameters range between 92 and 132 nm, while direct dissolution in distilled water is suitable for the deprotected copolymers, yielding effective diameters between 52 and 173 nm. Critical micelle concentration (CMC) analyses corroborate particle size analyses and show a distinct impact of the molecular architecture; the lowest CMC (8 µg mL−1) is observed when the poly(l ‐leucine) segment forms the C‐block and the hydrophilic, disassembly driving poly(l ‐lysine) segment is short. DNA complexation, evaluated by gel motility and RiboGreen analyses, depends strongly on the molecular architecture. A more efficient DNA complexation is observed when poly(l ‐lysine) and poly(l ‐leucine) form individual blocks as opposed to them forming a copolymer. 相似文献
The thermogravimetric analysis (TG) of two series
of tri-block copolymers based on poly(L,L-lactide) (PLLA) and poly(ethyleneglycol) (PEG)
segments, having molar mass of 4000 or 600 g mol–1,
respectively, is reported. The prepared block copolymers presented wide range
of molecular masses (800 to 47500 g mol–1)
and compositions (16 to 80 mass% PEG). The thermal stability increased with
the PLLA and/or PEG segment size and the tri-block copolymers prepared from
PEG 4000 started to decompose at higher temperatures compared to those copolymers
from PEG 600. The copolymers compositions were determined by thermogravimetric
analysis and the results were compared to other traditional quantitative spectroscopic
methods, hydrogen nuclear magnetic resonance spectrometry (1HNMR)
and Fourier transform infrared spectrometry (FTIR). The PEG 4000 copolymer
compositions calculated by TG and by 1HNMR, presented
differences of 1%, demonstrating feasibility of using thermogravimetric analysis
for quantitative purposes. 相似文献
A novel amphiphilic ABA‐type triblock copolymer poly(ethylene glycol)‐b‐poly(ethanedithiol‐alt‐nitrobenzyl)‐b‐poly(ethylene glycol) (PEG‐b‐PEDNB‐b‐PEG) is successfully prepared by sequential thiol‐acrylate Michael addition polymerization in one pot. PEG‐b‐PEDNB‐b‐PEG is designed to have light‐cleavable o‐nitrobenzyl linkages and acid‐labile β‐thiopropionate linkages positioned repeatedly in the main chain of the hydrophobic block. The light and pH dual degradation of PEG‐b‐PEDNB‐b‐PEG is traced by gel permeation chromatography (GPC). Such triblock copolymer can self‐assemble into micelles, which can be used to encapsulate anticancer drug doxorubicin (DOX). Because of the different degradation chemistry of o‐nitrobenzyl linkages and β‐thiopropionate linkages, DOX can be released from the micelles by two different manners, i.e., light‐induced rapid burst release and pH‐induced slow sustained release. Confocal laser scanning microscopy (CLSM) results indicated that DOX‐loaded micelles exhibited faster drug release in A549 cells after UV irradiation. Furthermore, 3‐(4,5‐dimethylthiazol‐2‐yl)‐2,5‐diphenyltetrazolium bromide (MTT) results show that the DOX‐loaded micelles under UV light degradation exhibit better anticancer activity against A549 cells than that of the nonirradiated ones.
This paper aims to report the fabrication of biodegradable thin films with micro‐domains of cylindrical nanochannels through the solvent‐induced microphase separation of poly(L ‐lactide)‐block‐poly(ethylene glycol)‐block‐poly(L ‐lactide) (PLA‐b‐PEG‐b‐PLA) triblock copolymers with different block ratios. In our experimental scope, an increase in each of the block lengths of the PLA and PEG blocks led to both a variation in the average number density (146 to 32 per 100 µm2) and the size of the micro‐domains (140 to 427 nm). Analyses by atomic force microscopy (AFM) and fluorescence microscopy indicated that the hydrophilic PEG nanochannels were dispersed in the PLA matrix of the PLA‐b‐PEG‐b‐PLA films. We demonstrated that the micro‐domain morphology could be controlled not only by the block length of PEG, but also by the solvent evaporation conditions.
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