Synthesis,thermo-responsive micellization and caffeine drug release of novel PBMA-<Emphasis Type="Italic">b</Emphasis>-PNIPAAm block polymer brushes

Brush-like block copolymers with poly(t-butyl methacrylate) (PBMA) and poly(N-isopropylacrylamide) (PNIPAAm) as side arms, PBMA-b-PNIPAAm, were designed and synthesized via a simple free radical polymerization route. The chemical structure and molecular weight of these polymer brushes were characterized and determined by nuclear magnetic resonance (¹H NMR), Fourier transform infrared spectrometry (FTIR) and gel permeation chromatography (GPC). The micellar formation by these polymer brushes in aqueous solutions were detected by a surface tension technique, and the critical micelle concentration (CMC) ranged from 1.53 to 8.06 mg L⁻¹. The morphology and geometry of polymer micelles were investigated by transmission electron microscope (TEM) and dynamic light scattering (DLS). The polymer micelles assume the regularly-spherical core-shell structure with well-dispersed individual nanoparticles, and the particle size was in the range from 36 to 93 nm. The PNIPAAm segments exhibited a thermoreversible phase transition, so the resulting block polymer brushes were temperature-sensitive and the low critical solution temperature (LCST) was determined by UV-vis spectrometer at about 28.82–29.40°C. The characteristic parameters of the polymer micelles such as CMC, micellar size and LCST values were affected by their compositional ratios and the length of hydrophilic or hydrophobic chains. The evaluation for caffeine drug release behavior of the block polymer micelles demonstrated that the self-assembled micelles exhibited thermal-triggered properties in controlled drug release.     

ABA triblock copolymer containing two crystallizable components

A triblock copolymer of the ABA type in which both components were crystallizable was synthesized. The A block was poly(ethylene oxide), PEO, and the B block, poly(dimethyl siloxane), PDMS. Upon cooling from the melt to liquid nitrogen temperature, the PEO block crystallized at around 40°C. When the copolymer was heated from ?170°C after quenching, glass transition, crystallization and melting of the PDMS middle block were identified in the thermogram at ?117°C, ?74°C and ?42°C, respectively. The degree of crystallinity of the PDMS block was estimated from the heat of fusion to be about 27%. The growth rates of the PEO spherulites were reduced by the presence of the middle block.     

Novel active ester‐bridged copolynorbornene materials containing terminal functional hydroxyl,amino, methacryloyl,or ammonium groups via ring‐opening metathesis polymerization

Several random and block copolynorbornenes with side chains containing terminal hydroxyl, amino, methacryloyl or ammonium groups were derived from the functional alkyl ester‐containing norbornenes by ring‐opening metathesis polymerization (ROMP). The main chain of ROMP‐type polynorbornene had a more important role for glass‐transition temperature in comparison with vinyl addition polymerization. There is little effect on glass‐transition temperature (about ?39 °C) of polynorbornenes with different length of alkyl side chain. The organosoluble copolynorbornenes with active crosslinkable methylacryloyl side chains derived from functional hydroxyl group were prepared to improve the thermal stability of poly(methyl methacrylate) [decomposition temperature (T_d)^10% = 325 °C in nitrogen] by forming networked AB crosslinked polymer (T = 367 °C in nitrogen). The sizes of nanometer‐scale polymeric micelles of block copolymers having hydrophobic alkyl ester and hydrophilic ammonium groups were measured in the range of 11–25 nm by scanning electron microscopy. These polymeric materials with various functional groups or amphiphilic architectures are accessible by ROMP, whose topology makes them particularly attractive for application potential such as biomedical and photoelectric materials. © 2005 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 43: 4233–4247, 2005     

Crystallization of segmented trans-1,4-polyisoprene/epoxidized trans-1,4-polyisoprene block copolymers from solution

The crystallization of segmented block copolymers of trans-1,4-polyisoprene (TPI)/expoxidized TPI from solution was investigated. One preparation with an average TPI block length of 14.5 and an average epoxidized TPI block length of 10 was crystallized from 2-pentanol at 20°C, 2-octanol at 20°C, and 2-pentanone at 0°C. A second preparation with an average TPI block length of 18 and the same average epoxidized TPI block length was crystallized from 2-octanol at 20°C and 2-pentanone at 0°C. The crystallization products were expoxidized in suspension a second time and then characterized by carbon-13 solution NMR to determine the average noncrystalline traverse length and the average crystalline stem length. The crystallized products were also studied by scanning electron microscopy, Fourier transform infrared spectroscopy, and differential scanning calorimetry to determine the morphology, the crystal form and crystallinity, and the melting point, respectively. The average noncrystalline traverse length was found to be highly dependent on the crystallization conditions and the crystalline stem length of the parent TPI lamellas; the composition of these traverses is discussed.     

Tuning of the Temperature Window for Unit‐Cell and Pore‐Size Enlargement in Face‐Centered‐Cubic Large‐Mesopore Silicas Templated by Swollen Block Copolymer Micelles

The unit‐cell size and pore diameter as functions of temperature are investigated in the syntheses of FDU‐12 silicas with face‐centered cubic structure templated by Pluronic (PEO‐PPO‐PEO) block copolymer micelles swollen by toluene. The temperature range in which the unit‐cell size and pore size strongly increase as temperature decreases is correlated with the critical micelle temperature (CMT) of the surfactant. While Pluronic F127 affords a wide range of unit‐cell parameters (28–51 nm) and pore diameters (16–32 nm), it renders moderately enlarged pore sizes at 25 °C. The use of Pluronic F108 with higher CMT affords FDU‐12 with very large unit‐cell size (～49 nm) and large pore diameter (27 nm) at 23 °C. Large unit‐cell size (40–41 nm) and pore size (22 nm) were obtained even at 25 °C. The application of Pluronics F87 and F88 with much smaller molecular weights and higher CMTs also allows one to synthesize FDU‐12 with quite large unit‐cell parameters and pore sizes at room temperature. The present work demonstrates that one can judiciously select Pluronic surfactants with appropriate CMT to shift the temperature range in which the pore diameter is readily tunable.     

聚乙二醇-b-聚(D,L-丙交酯-co-碳酸丙二酯)的胶束化及其药物控释研究

通过开环共聚合成了由D,L-丙交酯、碳酸丙二酯和聚乙二醇构成的两亲性嵌段共聚物(PETLA),研究了PETLA胶束化及药物控释行为.嵌段共聚物和胶束通过核磁共振(1H-NMR)、荧光分光光度计、凝胶渗透色谱(GPC)、动态光散射(DLS)、透射电镜(TEM)和紫外光谱(UV)表征.实验结果发现临界胶束浓度随共聚物疏水链段长度增加而减小,胶束直径随疏水链段长度增加而增大.透射电镜照片表明载药胶束MT1直径为30~40nm,呈规则球形.体外释药表明9-NC以可控方式释放,突释后药物释放速率接近零级恒速.     

Synthesis and characterization of core–shell‐type polymeric micelles from diblock copolymers via reversible addition–fragmentation chain transfer

A method was developed to enable the formation of nanoparticles by reversible addition–fragmentation chain transfer polymerization. The thermoresponsive behavior of polymeric micelles was modified by means of micellar inner cores and an outer shell. Polymeric micelles comprising AB block copolymers of poly(N‐isopropylacrylamide) (PIPAAm) and poly(2‐hydroxyethylacrylate) (PHEA) or polystyrene (PSt) were prepared. PIPAAm‐b‐PHEA and PIPAAm‐b‐PSt block copolymers formed a core–shell micellar structure after the dialysis of the block copolymer solutions in organic solvents against water at 20 °C. Upon heating above the lower critical solution temperature (LCST), PIPAAm‐b‐PHEA micelles exhibited an abrupt increase in polarity and an abrupt decrease in rigidity sensed by pyrene. In contrast, PIPAAm‐b‐PSt micelles maintained constant values with lower polarity and higher rigidity than those of PIPAAm‐b‐PHEA micelles over the temperature range of 20–40 °C. Structural deformations produced by the change in the outer polymer shell with temperature cycles through the LCST were proposed for the PHEA core, which possessed a lower glass‐transition temperature (ca. 20 °C) than the LCST of the PIPAAm outer shell (ca. 32.5 °C), whereas the PSt core with a much higher glass‐transition temperature (ca. 100 °C) retained its structure. The nature of the hydrophobic segments composing the micelle inner core offered an important control point for thermoresponsive drug release and the drug activity of the thermoresponsive polymeric micelles. © 2006 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 44: 3312–3320, 2006     

Amphiphilic silica/fluoropolymer nanoparticles: Synthesis,tem‐responsive and surface properties as protein‐resistance coatings

A series of amphiphilic silica/fluoropolymer nanoparticles of SiO₂‐g‐P(PEGMA)‐b‐P(12FMA) were prepared by silica surface‐initiating atom transfer radical polymerization (SI‐ATRP) of poly(ethylene glycol) methyl ether methacrylate (PEGMA) and poly dodecafluoroheptyl methacrylate (P12FMA). Their amphiphilic behavior, lower critical solution temperature (LCST), and surface properties as protein‐resistance coatings were characterized. The introduction of hydrophobic P(12FMA) block leads SiO₂‐g‐P(PEGMA)‐b‐P(12FMA) to form individual spherical nanoparticles (～150 nm in water and ～170 nm in THF solution) as P(PEGMA)‐b‐P(12FMA) shell grafted on SiO₂ core (～130 nm), to gain obvious lower LCST at 36–52 °C and higher thermostability at 290–320 °C than SiO₂‐g‐P(PEGMA) (LCST = 78–90 °C, T_d = 220 °C). The water‐casted SiO₂‐g‐P(PEGMA)‐b‐P(12FMA) films obtain much rougher surface (125.3–178.4 nm) than THF‐casted films (11.5–16.9 nm) and all SiO₂‐g‐P(PEGMA) films (26.8–31.3 nm). Therefore, the water‐casted surfaces exhibit obvious higher water adsorption amount (Δf = ?494 ～ ?426 Hz) and harder adsorbed layer (viscoelasticity of ΔD/Δf = ?0.28 ～ ?0.36 × 10^?6/Hz) than SiO₂‐g‐P(PEGMA) films, but present loser adsorbed layer than THF‐casted films (ΔD/Δf = ?0.29 ～ ?0.63 × 10^?6/Hz). While, the introduction of P(12FMA) segments does not show obviously reduce in the protein‐repelling adsorption of SiO₂‐g‐P(PEGMA)‐b‐P(12FMA) films (△f = ?15.7 ～ ?22.3 Hz) compared with SiO₂‐g‐P(PEGMA) films (△f = ?8.3 ～ ?11.3 Hz) and no obvious influence on water adsorption of ancient stone. Therefore, SiO₂‐g‐P(PEGMA)‐b‐P(12FMA) is suggested to be used as protein‐resistance coatings. © 2015 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2016 , 54, 381–393     

Fabrication of polymeric micelles with core–shell–corona structure for applications in controlled drug release

Thermo-responsive polymeric micelles of poly (ethylene glycol)-b-poly(2-hydroxyethyl methacrylate-g-lactide)-b-poly(N-isopropylacrylamide) (PEG-P(HEMA-PLA)-PNIPAM) with core–shell–corona structure were fabricated for applications in controlled drug release. The graft copolymer of PEG-P(HEMA-PLA)-PNIPAM was self-assembled into core–shell micelles with a densely PLA core and mixed PEG/PNIPAM shells at 25 °C in aqueous media. By increasing the temperature above the lower critical solution temperature of PNIPAM, these core–shell micelles could be converted into core–shell–corona micelles because of the collapse of PNIPAM block on the PLA core as the inner shell and the soluble PEG block stretching outside as the outer corona. Anticancer drug doxorubicin (DOX) was loaded in the polymeric micelles as a model drug. Compared with polymeric micelles formed by liner PEG-b-PLA-b-PNIPAM triblock copolymer, these polymeric micelles exhibited higher loading capacity, and release of DOX from the polymeric micelles with core–shell–corona structure was well-controlled.     

Aggregation,gelation instability,and morphologies of diblock copolymers consisting of poly(p‐benzamide) and poly(m‐benzamide)

The solution, gelation, and morphological properties of monodisperse aromatic polyamide diblock copolymers consisting of poly(p‐benzamide) (PpBA), poly(m‐benzamide) (PmBA), and poly(N‐octyl m‐benzamide) (POmBA) were investigated. The block copolymers of these polymers, PpBA‐block‐POmBA and PmBA‐block‐POmBA, formed spherical micelles or amorphous aggregates in many solvents in addition to physical gels at concentrations higher than 5 wt %. A temperature‐induced sol‐gel transition was also exhibited for PpBA‐block‐POmBA in solvents with high boiling points such as N,N‐dimethylacetamide and N‐methylpyrrolidone (NMP), although the transition was not entirely thermoreversible; the transition temperature decreased by annealing at ～80 °C. Dynamic light scattering measurements of the PpBA‐block‐POmBA/NMP solutions revealed that metastable micelles in the sol state reorganized into smaller micelles upon annealing at 90 °C. The block copolymer, which forms strong associations, exhibited some transient structure as indicated by the need to sufficiently anneal the solution to reach equilibrium. Network‐like patterns with characteristic length of ～10 μm appeared on the gel surfaces upon evaporation of volatile solvents such as dichloromethane and chloroform, in which the copolymers were observed to aggregate. The unique properties of the copolymers originate from interactions between the highly polar N? H aromatic polyamide blocks. © 2010 Wiley Periodicals, Inc. J Polym Sci Part B: Polym Phys 48: 1732–1739, 2010     

Amphiphilic diblock copolymers based on poly(2‐ethyl‐2‐oxazoline) and poly(4‐substituted‐ε‐caprolactone): Synthesis,characterization, and cellular uptake

Amphiphilic diblock copolymers with various block compositions were synthesized on poly(2‐ethyl‐2‐oxazoline) (PEtOz) as a hydrophilic block and poly(4‐methyl‐ε‐caprolactone) (PMCL) or poly(4‐phenyl‐ε‐caprolactone) (PBCL) as a hydrophobic block. These PEtOz‐b‐PMCL and PEtOz‐b‐PBCL copolymers consisting of soft domains of amorphous PEtOz and PM(B)CL had no melting endothermal peaks but displayed T_g. The lower critical solution temperature (LCST) values for the PEtOz‐b‐PMCL, and the PEtOz‐b‐PBCL aqueous solution were observed to shift to lower temperature than PEtOz homopolymers. Their aqueous solutions were characterized using fluorescence techniques and dynamic light scattering (DLS). The block copolymers formed micelles with critical micelle concentrations (CMCs) in the range 0.6–11.1 mg L^?1 in an aqueous phase. As the length of the hydrophobic PMCL or PBCL blocks elongated, lower CMC values were generated. The mean diameters of the micelles were between 127 and 318 nm, with PDI in the range of 0.06–0.21, suggesting nearly monodisperse size distributions. The drug entrapment efficiency and drug‐loading content of micelles depend on block polymer compositions. In vitro cell viability assay showed that PEtOz‐b‐PMCL has low cytotoxicity. Doxorubicin hydrochloride (DOX)‐loaded micelles facilitated human cervical cancer (HeLa) cell uptake of DOX; uptake was completed within 2 h, and DOX was able to reach intracellular compartments and enter the nuclei by endocytosis. © 2013 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2013, 51, 2769–2781     

Synthesis and self‐association behavior of poly[bis(2‐(2‐methoxyethoxy)ethoxy)phosphazene]‐b‐poly(propyleneglycol) triblock copolymers

Amphilic triblock copolymers with varying ratios of hydrophilic poly[bis (methoxyethoxyethoxy)phosphazene] (MEEP) and relatively hydrophobic poly(propylene glycol) (PPG) blocks were synthesized via the controlled cationic‐induced living polymerization of a phosphoranimine (Cl₃P?NSiMe₃) at ambient temperature. A PPG block can function as either a classical hydrophobic block or a less hydrophobic component by varying the nature of a phosphazene block. The aqueous phase behavior of MEEP‐PPG‐MEEP block copolymers was investigated using fluorescence techniques, TEM, and dynamic light scattering (DLS). The critical micelle concentrations (cmcs) of MEEP‐PPG‐MEEP block copolymers were determined to be in the range of 3.7–16.8 mg/L. The mean diameters of MEEP‐PPG‐MEEP polymeric micelles, measured by DLS, were between 31 and 44 nm. The equilibrium constants of pyrene in these micelles ranged from 4.7 × 10⁴ to 9.6 × 10⁴. © 2008 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 47: 692–699, 2009     

Dual-response nanocarrier based on graft copolymers with hydrazone bond linkages for improved drug delivery

Core–shell micelles with biodegradability, thermo- and pH-response were successfully demonstrated by poly(2-oxepane-1,5-dione-co-ɛ-caprolactone) (P(OPD-co-CL)) grafted with hydrophilic segments of amine-terminated poly(N-isopropylacrylamide) (At-PNIPAM). To compare with the graft copolymer, P(OPD-co-CL) block PNIPAM polymer was also prepared. The micelles with core–shell structure were formed with both graft and block copolymers by self-assembly in aqueous solutions, of which PNIPAM shell is thermo-response. Furthermore, P(OPD-co-CL)-g-PNIPAM also showed pH-sensitivity, which was attributed to the acid-cleavable property of the hydrazone bond. The low critical micelle concentrations (CMCs) of graft polymers and block polymers were 6.7 mg/L and 14.3 mg/L, respectively, which indicated the formation of stable micelles. Both drug-free and drug-loaded micelles were in uniformly spherical shape observed by transmission electron microscopy (TEM). The sizes of the drug-free and drug-loaded micelles prepared from graft polymer were 123.5 nm and 146.5 nm, respectively, and the sizes of those prepared from block polymer were 197.5 nm and 211.5 nm, respectively. The lower critical solution temperature (LCST) for the graft polymer was 34.3 °C, while that for the block polymer was 28.1 °C, demonstrating a thermo-response. The graft polymeric micelles exhibited thermo-triggered decelerated release at pH 7.4, and pH-triggered accelerated release at 25 °C in vitro release test, indicating that the graft polymeric micelles could be a promising site-specific drug delivery system for enhancing the bioavailability of the drug in targeted pathological areas.     

Study of hierarchical microstructures self-assembled by π-shaped ABC block copolymers in dilute solution using self-consistent field theory

Microstructures self-assembled by amphiphilic ABC π-shaped block copolymers in dilute solution have been investigated by self-consistent field theory. The effects of architectural parameters and the interaction strength among the three blocks have been studied systematically. Our calculation results show that the distance of the two graft blocks has stronger effect than the length of graft blocks and the position of the first graft point on the phase behavior. The interaction strength among the three blocks is another important factor in controlling the resulting microstructures. Compound-core, multicompartment, and multicore micelles are observed in the case of π-shaped ABC block copolymers with hydrophilic backbone block A and hydrophobic graft blocks B and C. Core-shell-corona, incomplete skin-layered and hamburger micelles are formed when graft block C is hydrophilic and blocks A and B are hydrophobic. The wormlike multicore micelles have drawn our attention. We find that the morphology of wormlike multicore micelle can be controlled by changing the distance of the two graft blocks of the π-shaped block copolymers. In all of the wormlike multicore micelles, the streamline wormlike micelle is more stable than other wormlike micelles from the free energy analysis.     

Clonazepam release from core-shell type nanoparticles composed of poly(γ-benzyl L-glutamate) as the hydrophobic part and poly(ethylene oxide) as the hydrophilic part

Block copolymers consisting of poly(γ-benzyl L -glutamate) (PBLG) as the hydrophobic part and poly(ethylene oxide) (PEO) as the hydrophilic part were synthesized and characterized. Core shell type nanoparticles of the block copolymers (abbreviated GEG) were prepared by the dialysis method. Under fluorescence spectroscopy measurement, the GEG block copolymers were associated in water to form core shell type nanoparticles as polymeric micelles and the critical micelle concentrations (CMC) values of the block copolymers decreased with increasing PBLG chain length in the block copolymers. Transmission electron microscopy (TEM) observations revealed nanoparticles of spherical shapes. From dynamic light scattering (DLS) study, sizes of nanoparticles of GEG-1 and GEG-2 copolymer were 64.3 ± 28.7 nm and 28.9 ± 7.0 nm. The drug-loading contents of GEG-1 and GEG-2 nanoparticles were 15.2 and 8.3 wt %, respectively. These results indicated that the drug-loading contents were dependent on PBLG chain length in the copolymer. Then, the longer the PBLG chain length, the more the drug-loading contents. Release of clonazepam (CNZ) from the nanoparticles was slower in higher loading contents of CNZ than lower loading contents due to the hydrophobic interaction between PBLG core and CNZ. © 1998 John Wiley & Sons, Inc. J Polym Sci B: Polym Phys 36: 415–423, 1998     

Formation of Polymeric Nanocubes by Self‐Assembly and Crystallization of Dithiolane‐Containing Triblock Copolymers

Template‐free fabrication of non‐spherical polymeric nanoparticles is desirable for various applications, but has had limited success owing to thermodynamic favorability of sphere formation. Herein we present a simple way to prepare cubic nanoparticles of block copolymers by self‐assembly from aqueous solutions at room temperature. Nanocubes with edges of 40–200 nm are formed spontaneously on different surfaces upon water evaporation from micellar solutions of triblock copolymers containing a central poly(ethylene oxide) block and terminal trimethylene carbonate/dithiolane blocks. These polymers self‐assemble into 28±5 nm micelles in water. Upon drying, micelle aggregation and a kinetically controlled crystallization of central blocks evidently induce solid cubic particle formation. An approach for preserving the structures of these cubes in water by thiol‐ or photo‐induced crosslinking was developed. The ability to solubilize a model hydrophobic drug, curcumin, was also explored.     

From toroidal to rod‐like nanostructure,a mechanism study for the reversible morphological control on amphiphilic triblock copolymer micelles

Mechanism of the morphological changes between toroidal and rod‐like nanostructures of P4VP‐b‐PS‐b‐P4VP amphiphilic triblock copolymer micelles has been investigated in aqueous solution. This transition is proved to be highly reversible and tunable upon changing temperature. The toroidal structure, evolving from fibers at 20 °C, can transform to rod‐like morphology as the temperature either gradually or directly increases to 80 °C, and vice versa. However, the transition mechanisms are quite different in different temperature‐changing processes. The structure and thickness of the micelles are dependent on the specific temperature, whereas the transition mechanism is related to the method of the temperature change. These morphological changes are considered as a result from the interaction parameter between the solvent and the copolymer blocks, especially the hydrophobic block. Our research complements the external control over the reversible morphological transition of block copolymer micelles without changing the composition of the system or introducing additional influencing factors. © 2016 Wiley Periodicals, Inc. J. Polym. Sci., Part B: Polym. Phys. 2016 , 54, 1450–1457     

NIPAAm-containing amphiphilic block copolymers with tailored LCST: Aggregation behavior,cytotoxicity and evaluation as carriers of indomethacin,tetracycline and doxorubicin

Nanocarriers based on amphiphilic block copolymers, with tailored temperature and pH responsiveness, were prepared. The hydrophilic blocks consist of temperature-sensitive [N-isopropylacrylamide (NIPAAm)] or NIPAAm plus pH-sensitive units [5-methacryloyloxy pentatonic acid (5MPA) or 4-methacryloyloxy benzoic acid (4MBA)], while the hydrophobic block is composed of n-hexyl acrylate (HA) or styrene (ST). Particle sizes were within the suitable range for the desired application (30–182?nm). Drug loading was achieved via an organic solvent-free method and a THF-buffer method leading to drug loadings of indomethacin, tetracycline and doxorubicin of up to 11, 11 and 60?wt%, respectively. In vitro release kinetics were performed under simulated physiological conditions (pH 7.4 and 37?°C; pH 6.0 and 40?°C) and show differences depending on the copolymer composition. The average kinetic data were well fitted to the mathematical model of Peppas. NIPAAm-containing copolymers were slight or non-cytotoxic for rat primary hepatocytes at concentrations less than 200?µg mL^?1. Some of the polymeric aggregates prepared may find application as pharmaceutical carriers.     

Palladium-catalyzed Mizoroki-Heck reactions in water using thermoresponsive polymer micelles

Palladium-catalyzed Mizoroki-Heck reactions were carried out in water using thermoresponsive polymer micelles. The micelles were generated from thermoresponsive block copolymers consisting of a poly(N-isopropylacrylamide) (PNIPAAm) segment and a hydrophilic segment such as nonionic poly(ethylene glycol) (PEG) (2) and anionic poly(sodium p-styrenesulfonate) (PSSNa) (9). These copolymers exhibited lower critical solution temperature (LCST) behavior at ca. 40–50?°C and showed thermal stimuli-induced formation and dissociation of micelles. The copolymers formed micelles in aqueous solution at higher temperature, where catalytic reactions proceeded. At lower temperature, the micelles dissociated to form a clear solution, enabling efficient extraction of the products from aqueous reaction mixture. In the presence of these copolymers, palladium complexes catalyzed the coupling reactions between aryl iodides and alkene compounds inside the hydrophobic micelle cores in water under relatively milder conditions. Extraction of the products from the aqueous solution of 2 or 9 was found to be efficient enough in comparison with conventional surfactants.     

pH敏感型mPEG-Hz-PLA聚合物纳米载药胶束的制备

以合成的含有腙键的聚乙二醇大分子(mPEG-Hz-OH)为引发剂,以丙交酯为单体引发开环聚合反应,并通过调整投料比,制备出3种不同分子量的含腙键的生物可降解嵌段聚合物(mPEG-Hz-PLA).将腙键引入到聚合物的骨架中,以此构建聚合物胶束并作为pH敏感型纳米药物载体.制备的pH敏感型胶束的CMC值等于或低于5.46×10-4 mg/m L,DLS和TEM显示粒径均小于100 nm,且粒径分布均匀.非pH敏感型胶束在不同pH下的粒径变化不明显,而pH敏感型胶束在酸性环境下(pH=4.0和pH=5.0)胶束粒径出现了明显变化.以阿霉素为模型药物制备了pH敏感型载药胶束,其粒径比空白胶束大(100~200 nm),且粒径分布均匀.药物释放实验表明pH敏感型载药胶束随着释放介质pH降低累积释药量增高.MTT实验表明空白胶束对HeLa细胞和RAW264.7细胞几乎没有抑制作用,而载阿霉素的胶束对2种细胞的抑制作用都随着剂量的增大和时间的延长而增强.