Four linear and four star equimolar terpolymers based on non‐ionic hydrophilic methoxy hexa(ethylene glycol) methacrylate, ionizable hydrophilic 2‐(dimethylamino)ethyl methacrylate and neutral hydrophobic methyl methacrylate were synthesized using group transfer polymerization and investigated in aqueous dilute solutions. It was found that the (ABC)n multi‐arm star terpolymers formed unimolecular micelles comprising three centrosymmetric compartments. The position of each compartment could be determined by the block sequence (ABC, ACB or BAC) at will. On the other hand, the ABC linear counterparts formed loose associates with very low aggregation numbers. It was shown that the polymer architecture (linear versus star) greatly affected the micellization phenomena of the terpolymers in selective media.
Well‐defined ABC triblock copolymers based on two hydrophilic blocks, A and C, and a hydrophobic block B are synthesized and their self‐assembly behavior is investigated. Interestingly, at the same solvent, concentration, pH, and temperature, different shape micelles are observed, spherical and worm‐like micelles, depending on the preparation method. Specifically, spherical micelles are observed with bulk rehydration while both spherical and worm‐like micelles are observed with film rehydration.
Redox‐responsive micelles with cores crosslinked via click chemistry are developed to improve the stability of polymer micelles. Amphiphilic block copolymer mPEG‐b‐P(DTC‐ADTC) with pendant azido groups on the hydrophobic chains is synthesized by the ring‐opening polymerization of 2,2‐bis(azidomethyl)trimethylene carbonate (ADTC) and 2,2‐dimethyltrimethylene carbonate (DTC) with monomethoxy poly(ethylene glycol) (mPEG) as an initiator. mPEG‐b‐P(DTC‐ADTC) self‐assemble to form the micelles in aqueous solution and the cores of the micelles are crosslinked via click chemistry to afford redox‐responsive core‐crosslinked micelles. Core‐crosslinking enhances the stability of the micelles in aqueous solution and improve the drug‐loading property. The redox‐responsive core‐crosslinked micelles can be reduced by the addition of reducing agents such as dithiothreitol (DTT), and thus release the loaded drug quickly in the presence of DTT.
In this work, a novel type of block copolymer micelles with K+‐responsive characteristics for targeted intracellular drug delivery is developed. The proposed smart micelles are prepared by self‐assembly of poly(ethylene glycol)‐b‐poly(N‐isopropylacry‐lamide‐co‐benzo‐18‐crown‐6‐acrylamide) (PEG‐b‐P(NIPAM‐co‐B18C6Am)) block copolymers. Prednisolone acetate (PA) is successfully loaded into the micelles as the model drug, with loading content of 4.7 wt%. The PA‐loaded micelles display a significantly boosted drug release in simulated intracellular fluid with a high K+ concentration of 150 × 10−3m , as compared with that in simulated extracellular fluid. Moreover, the in vitro cell experiments indicate that the fluorescent molecules encapsulated in the micelles can be delivered and specifically released inside the HSC‐T6 and HepG2 cells responding to the increase of K+ concentration in intracellular compartments, which confirms the successful endocytosis and efficient K+‐induced intracellular release. Such K+‐responsive block copolymer micelles are highly potential as new‐generation of smart nanocarriers for targeted intracellular delivery of drugs. 相似文献
Summary: Diblock terpolymers that consist of homopolymer and statistical copolymer (polyampholyte) building blocks are synthesized by group transfer polymerization. Two types of block tepolymers are explored in aqueous media: the amphiphilic poly{[(diethylamino)ethyl methacrylate]‐co‐(methacrylic acid)}‐block‐poly(methyl methacrylate) and the double hydrophilic poly[oligo(ethylene glycol) methacrylate]‐block‐poly{[(diethylamino)ethyl methacrylate]‐co‐(methacrylic acid)}. The first terpolymer self‐assembles in aqueous media to form responsive micelles that change their corona charge sign upon switching pH. The second terpolymer exhibits a multi‐responsive behavior. It forms neutral, positive, or negative micelles depending on a combination of different environmental conditions such as temperature, pH, and ionic strength.
Redox‐responsive micelles are versatile nanoplatforms for on‐demand drug delivery, but the in situ evaluation of drug release is challenging. Fluorescence resonance energy transfer (FRET) technique shows potential for addressing this, while the aggregation‐caused quenching effect limits the assay sensitivity. The aim of the current work is to combine aggregation‐induced emission (AIE) probe with FRET to realize drug release assessment from micelles. Tetraphenylethene (TPE) is selected as AIE dye and curcumin (Cur) is chosen as the model drug as well as FRET receptor. The drug is covalently linked to a block copolymer via the disulfide bond linker and TPE is also chemically linked to the polymer via an amide bond; the obtained amphiphilic polymer conjugate self‐assembles into micelles with a hydrodynamic size of ≈125 nm. Upon the supplement of glutathione or tris(2‐carboxyethyl)phosphine) trigger (10 × 10−3m ), the drug release induces the fluorescence increase of both TPE and Cur. Accompanied with the FRET decay, absorption enhancement and particle size increase are observed. The same phenomenon is observed in MCF‐7 cells. The FRET–AIE approach can be a useful addition to the spectrum of available methods for monitoring drug release from stimuli‐responsive nanomedicine. 相似文献
A novel comb‐like derivative CPEG‐g‐DNQ was prepared by incorporating light responsive 2‐diazo‐1,2‐naphthoquinone (DNQ) groups into the structure of comb‐like poly(ethylene glycol) (CPEG). DLS and TEM results showed that CPEG‐g‐DNQ self‐assembled into spherical micelles with an average size of about 135 nm in water. Upon exposure to light, the micelles could be disrupted because of the conversion of hydrophobic DNQ to hydrophilic 3‐indenecarboylic acid. Additionally, hydrophobic coumarin 102 was successfully loaded into the micelles and photo‐induced ON‐OFF release was demonstrated by fluorescence spectroscopy. MTT assay revealed that the micelles are biocompatible. These photo‐responsive micelles might have great potential for controlled release of hydrophobic drugs.
Comprehensive three‐dimensional gas chromatography (GC3) is demonstrated using modified GC×GC apparatus. A new thermal modulation scheme employing a single moving heater to operate two thermal modulators is introduced. Considerations of the bandwidth/resolution tradeoff of GC3 show that high‐speed tertiary columns would make GC3 practical, with modest loss of underlying GC×GC peak capacity. 相似文献
We demonstrate the spontaneous and reversible transition between the two‐ and three‐dimensional self‐assembly of a supramolecular system at the solid–liquid interface under electrochemical conditions, using in situ scanning tunneling microscopy. By tuning the interfacial potential, we can selectively organize our target molecules in an open porous pattern, fill these pores to form an auto‐host–guest structure, or stack the building blocks in a stratified bilayer. Using a simple electrostatic model, we rationalize which charge density is required to enable bilayer formation, and conversely, which molecular size/charge ratio is necessary in the design of new building blocks. Our results may lead to a new class of electrochemically controlled dynamic host–guest systems, artificial receptors, and smart materials. 相似文献
New methodology for making novel materials is highly desirable. Here, an “ingredients” approach to functional self‐assembled hydrogels was developed. By designing a building block to contain the right ingredients, a multi‐responsive, self‐assembled hydrogel was obtained through a process of template‐induced self‐synthesis in a dynamic combinatorial library. The system can be switched between gel and solution by light, redox reactions, pH, temperature, mechanical energy and sequestration or addition of MgII salt. 相似文献
Two one‐dimensional compounds composed of a 1:1 ratio of MnIII salen‐type complex and NiII oximato moiety with different counter anions, PF6? and BPh4?, were synthesized: [Mn(3,5‐Cl2saltmen)Ni(pao)2(phen)]PF6 ( 1 ) and [Mn(5‐Clsaltmen)Ni(pao)2(phen)]BPh4 ( 2 ), where 3,5‐Cl2saltmen2?=N,N′‐(1,1,2,2‐tetramethylethylene)bis(3,5‐dichlorosalicylideneiminate); 5‐Clsaltmen2?=N,N′‐(1,1,2,2‐tetramethylethylene)bis(5‐chlorosalicylideneiminate); pao?=pyridine‐2‐aldoximate; and phen=1,10‐phenanthroline. Single‐crystal X‐ray diffraction study was carried out for both compounds. In 1 and 2 , the chain topology is very similar forming an alternating linear chain with a [‐MnIII‐ON‐NiII‐NO‐] repeating motif (where ‐ON‐ is the oximate bridge). The use of a bulky counteranion, such as BPh4?, located between the chains in 2 rather than PF6? in 1 , successfully led to the magnetic isolation of the chains in 2 . This minimization of the interchain interactions allows the study of the intrinsic magnetic properties of the chains present in 1 and 2 . While 1 and 2 possess, as expected, very similar paramagnetic properties above 15 K, their ground state is antiferromagnetic below 9.4 K and paramagnetic down to 1.8 K, respectively. Nevertheless, both compounds exhibit a magnet‐type behavior at temperatures below 6 K. While for 2 , the observed magnetism is well explained by a Single‐Chain Magnet (SCM) behavior, the magnet properties for 1 are induced by the presence in the material of SCM building units that order antiferromagnetically. By controlling both intra‐ and interchain magnetic interactions in this new [MnIIINiII] SCM system, a remarkable AF phase with a magnet‐type behavior has been stabilized in relation with the intrinsic SCM properties of the chains present in 1 . This result suggests that the simultaneous enhancement of both intrachain (J) and interchain (J′) magnetic interactions (with keeping J ? J′), independently of the presence of AF phase might be an efficient route to design high temperature SCM‐based magnets. 相似文献
Self‐stabilized nanoparticles with a temperature‐responsive poly[(N,N‐diethylacrylamide)‐co‐(N,N′‐methylenebisacrylamide)] microgel core and a covalently attached hairy shell were synthesized via a simple nitroxide‐mediated controlled free‐radical aqueous dispersion polymerization, using a poly(sodium acrylate) alkoxyamine macroinitiator. With this method, high solid content, surfactant‐free particle suspensions were prepared, with diameter ranging from 49 to 118 nm at high temperature, and able to reversibly swell with water at low temperature. The proposed method requires a limited number of reagents in a simple polymerization procedure and thus avoids many drawbacks generally encountered in the synthesis of thermally responsive microgel particles.
With a rational design of the supra‐amphiphiles, we have successfully demonstrated that not only the dimension of the self‐assembled nanostructures, but also the packing fashion of the functional naphthalene diimide (a typical n‐type chromophore), can be tuned in a noncovalent way in aqueous solution. Naphthalene diimide is incorporated into a bola‐amphiphile as the rigid core, whereas viologen derivatives are used as the hydrophilic head. The bola‐amphiphile self‐assembles into two‐dimensional nanosheets, in which naphthalene diimide adopts a “J‐type” aggregation. Water‐soluble supramolecular complexation between viologen derivatives and the 8‐hydroxypyrene‐1, 3, 6‐trisulfonic acid trisodium salt is used as a driving force for the formation of the supra‐amphiphiles. Upon formation of the supra‐amphiphiles, the nanosheets transform into ultralong nanofibers with a close packing of naphthalene diimide. Notably, just by mixing the two building blocks of the supra‐amphiphiles in aqueous solution, a dimension‐controlled evolution of the nanostructures is formed that leads to a different packing fashion of the n‐type functional chromophores, which is facile and environmental friendly. 相似文献
A poly(tert‐butyl acrylate) (P(tBA)) with a glycodendric endfunctionality with eight glucose moieties was synthesised in four steps via a combination of esterification, thiol‐alkyne conjugation and hetero‐Diels–Alder (HDA) cycloaddition. A linear glycopolymer of similar size and composition was also synthesised in order to compare the protein binding characteristics of the polymer with glycodendritic endfunctionality to the linear glycol blockcopolymer. The two amphiphilic polymers were self‐assembled in water into micelles. These particles were then tested for their ability to bind to Concanavalin A (Con A). In a turbidity assay, the polymer glycodendron exhibited a significantly faster clustering rate to the lectin as compared to the linear glycopolymer. In a precipitation assay, it is found that significantly less glucose residue is required for binding per Con A for the polymer with the glycodendritic endfunctionality.
下载免费PDF全文