Cross-linking of cationic block copolymer micelles by silica deposition

Diblock copolymer micelles comprising cationic poly(2-(dimethylamino)ethyl methacrylate) (PDMA) coronas and hydrophobic poly(2-(diisopropylamino)ethyl methacrylate) (PDPA) cores are used as nanosized templates for the deposition of silica from aqueous solution at pH 7.2 and 20 degrees C. Both noncross-linked and shell cross-linked (SCL) micelles can be coated with silica without loss of colloid stability. Under optimized conditions, the silica deposition is confined to the partially quaternized cationic PDMA chains, leading to hybrid copolymer-silica particles of around 35 nm diameter with well-defined core-shell morphologies. 1H NMR studies confirmed that the PDPA cores of these copolymer-silica particles became protonated at low pH and deprotonated at high pH, which suggests possible encapsulation and controlled release applications. Moreover, in situ silica deposition effectively stabilizes the PDPA-PDMA micelles, which remain intact on lowering the solution pH (whereas the original noncross-linked PDPA-PDMA micelles dissociate in acidic solution). This suggests a convenient route to silica-stabilized SCL micelles under mild conditions.     

基于介孔纳米粒子模板合成兼有荧光和近红外发光的稀土核-壳结构纳米材料

利用单分散性良好介孔SiO2纳米粒子为模板,选择Y2O3为基底,同时掺杂可见区红光中心Eu3+和近红外区Er3+(1.54 μm)发光中心,成功制备特殊结构的核壳多功能发光纳米材料. 光谱测试表明这种核壳材料同时具有可见区发光和近红外发光的双重性质. 表明Y2O3可作为红光Eu和近红外发光Er的良好基底材料. 该方法可以大大降低纳米发光材料中稀土元素的使用量,降低发光材料的成本,并且该核壳结构材料密度相对较低,易于分散在有机溶剂或者水中,在药物释放和多功能生物标记等方面有着潜在的应用价值.     

Preparation of asymmetrically nanoparticle-supported, monodisperse composite dumbbells by protruding a smooth polymer bulge from rugged spheres

A novel method is proposed to create asymmetrically nanoparticle-supported, monodisperse composite dumbbells. The method consists of the three steps of double soap-free emulsion polymerizations before and after a heterocoagulation. In the first step, soap-free emulsion polymerization was conducted to cover silica cores with cross-linked poly(methyl methacrylate) (PMMA) shells. Then, positively or negatively charged silica nanoparticles were heterocoagulated with the silica-PMMA core-shell particles. In the heterocoagulations, the nanoparticles surface-modified with a cationic silane coupling agent, 3-aminopropyltriethoxysilane, were used as the positively charged ones, and silica nanoparticles without any treatment were used as the negatively charged ones. In the third step, soap-free polymerizations at different pH values were performed to protrude a polystyrene (PSt) bulge from the core-shell particles supporting the charged silica nanoparticles. In the polymerization, the core-shell particles heterocoagulated with the positively charged silica nanoparticles were aggregated in an acidic condition whereas the silica nanoparticles supported on the core-shell particles were dissolved in a basic condition. For the negatively charged silica nanoparticle, a PSt bulge was successfully protruded from the core-shell particle in acidic and neutral conditions without aggregation of the core-shell particles. The protrusion of the PSt bulge became distinctive when the number of heterocoagulated silica nanoparticles per core-shell particle was increased. Additional heterocoagulation experiments, in which positively or negatively charged magnetite nanoparticles were mixed with the asymmetrically nanoparticle-supported composite dumbbells, confirmed direct exposure of silica nanoparticles to the outer solvent phase.     

无规-类接枝共聚物自组装制备交联纳米微球

无规-类接枝共聚物(SFG)由大分子单体-己内酯改性丙烯酸酯(FA)、亲油性单体苯乙烯和甲基丙烯酸缩水甘油酯(GMA)共聚所得，SFG与聚苯乙烯在甲醇溶液中进行自组装，形成核壳结构纳米胶束，进一步对PGMA壳进行化学交联。最终得到具有核壳结构的纳米微球。动态激光光散射和透射电子显微镜表征结果显示SFG自组装形成了窄分布的纳米微球，微球粒径在100～200nm之间。     

Facile synthesis of silver core - silica shell composite nanoparticles

Combining metal nanoparticles and dielectrics (e.g. silica) to produce composite materials with high dielectric constant is motivated by application in energy storage. Control over dielectric properties and their uniformity throughout the composite material is best accomplished if the composite is comprised of metal core - dielectric shell structured nanoparticles with tunable dimensions. We have synthesized silver nanoparticles in the range of 40-100nm average size using low concentration of saccharide simultaneously as the reducing agent and electrostatic stabilizer. Coating these silver particles with silica from tetraalkoxysilanes has different outcomes depending on the alcoholic solvent and the silver particle concentration. A common issue in solution-based synthesis of core-shell particles is heterogeneous nucleation whereupon two populations are formed: the desired core-shell particles and undesired coreless particles of the shell material. We report the formation of Ag@SiO(2) core-shell particles without coreless silica particles as the byproduct in 2-propanol. In ethanol, it depends on the silver surface area available whether homogeneous nucleation of silica on silver is achieved. In methanol and 1-butanol, core-shell particles did not form. This demonstrates the significance of controlling the tetraalkoxysilane hydrolysis rate when growing silica shells on silver nanoparticles.     

SiO2/聚合物核壳型杂化粒子及其空心结构的制备

SiO2/聚合物核壳型杂化粒子及其空心结构以其独特的形貌在药物控制释放、催化剂载体、生物医药等领域应用前景广阔,引起了人们的广泛关注。本文着重从乳液聚合法、仿生矿化法等制备方法角度阐述了SiO2/聚合物核壳型杂化粒子及其空心结构的研究进展。乳液聚合制备SiO2/聚合物核壳型杂化粒子简单易行,一般需要预先合成SiO2纳米粒子,其合成过程通常需要一些非理想的条件,如高温高压、极端pH、昂贵或有毒的有机试剂等,而且预先合成的SiO2粒子无法与聚合物实现100%匹配,即总有纯的聚合物粒子存在。相比之下,原位仿生矿化法制备SiO2杂化粒子不仅在环境条件下可进行,而且能够精确控制其纳米尺度的形态及分级有序结构。目前对材料科学家来讲,要使人工合成SiO2/聚合物杂化粒子实现像自然生物硅那样优异的性能,仍然是很大的挑战。     

Folic acid-conjugated nanostructured materials designed for cancer cell targeting

Shell cross-linked nanoparticles (SCKs) constitute a unique class of materials with amphiphilic core-shell morphology; SCKs are characterised by their structural integrity and available functionality to attach receptor-recognising or receptor-specific ligands on the shell surface and, therefore, hold great potential in drug delivery applications; in an attempt to develop novel, cancer cell specific delivery vehicles, folate receptor targeted SCKs have been prepared.     

Shell cross-linked stearic acid grafted chitosan oligosaccharide self-aggregated micelles for controlled release of paclitaxel

Stearic acid grafted chitosan oligosaccharide (CSO-SA) with different degree of amino substitution (SD) was synthesized by 1-ethyl-3-(3-dimethylaminopropyl) carbodiimide (EDC)-mediated coupling reaction. The critical micelle concentration (CMC) of CSO-SA with different SD was about 0.06, 0.04, 0.01 mg/ml, respectively. With the increase of micelle concentration, the micelle size decreased, and the zeta potential increased. On the other hand, with the increase of SD of CSO-SA, the micelle size and zeta potential decreased due to the increased hydrophobic interaction of SA and the reduced free amino groups. To increase the stability of the micelle in vivo and controll drug release, the shells of micelles were cross-linked by glutaraldehyde. By controlling the molar ratio of CSO-SA to glutaraldehyde, the cross-linking of intra-micelle could be reached, and the nanoparticle with smaller size than that of its initial micelle was obtained. Paclitaxel was then used as model drug to incorporate into the micelles, and the surfaces of the micelles were further cross-linked by glutaraldehyde to form drug loaded and shell cross-linked nanoparticles. The effects of drug loading, SD of CSO-SA and cross-link degree on the size, zeta potential, drug entrapment efficiency and in vitro drug release behavior of micelles and its cross-linked nanoparticles were investigated. The higher drug entrapment efficiencies (above 94%) were observed in all case. The charged amounts of drug did not affect the drug release behavior. The drug release rate decreased with the increase of SD of CSO-SA and cross-link degree.     

Synthesis of nano/microstructures at fluid interfaces

The generation of novel multifunctional materials with hierarchical ordering is a major focus of current materials science and engineering. For such endeavors, fluid interfaces, such as air-liquid and liquid-liquid interfaces, offer ideal platforms where nanoparticles or colloidal particles can accumulate and self-assemble. Different assembly processes and reactions have been performed at fluid interfaces to generate hierarchical structures, including two-dimensional crystalline films, colloidosomes, raspberry-like core-shell structures, and Janus particles, which lead to broad applications in drug delivery and controlled release, nanoelectronics, sensors, food supplements, and cosmetics.     

Synthesis and applications of shell cross-linked thermoresponsive hybrid micelles based on poly(N-isopropylacrylamide-co-3-(trimethoxysilyl)propyl methacrylate)-b-poly(methyl methacrylate)

Shell cross-linked (SCL) thermoresponsive hybrid micelles consisting of a cross-linked thermoresponsive hybrid hydrophilic shell and a hydrophobic core domain were synthesized from poly(N-isopropylacrylamide-co-3- (trimethoxysilyl)propyl methacrylate)-b-polymethyl methacrylate (P(NIPAAm-co-MPMA)-b-PMMA) amphiphilic block copolymers. Transmission electron microscopy (TEM) images showed that the SCL micelles formed regularly globular nanoparticles. The SCL micelles showed reversible dispersion/aggregation in response to temperature cycles through an outer polymer shell lower critical solution temperature (LCST) for PNIPAAm at around 33 degrees C, observed by turbidity measurements and dynamic light scattering (DLS). The drug loading and in vitro drug release properties of the SCL micelles bearing a silica-reinforced PNIPAAm shell were further studied, which showed that the SCL micelles exhibited a much improved entrapment efficiency (EE) as well as a slower release rate which allowed the entrapped molecules to be slowly released over a much longer period of time as compared with pure PNIPAAm-b-PMMA micelles.     

Stimuli-responsive hydrogel hollow capsules by material efficient and robust cross-linking-precipitation synthesis revisited

Monodisperse stimuli-responsive hydrogel capsules were synthesized in the 100-nm-diameter to 10-μm-diameter range from poly(4-vinylpyridine) (P4VP) and poly(ethyleneimine) (PEI) through a simple, efficient two-step cross-linking-precipitation template method under conditions of a good solvent. In this method, the core-shell particles were obtained by the deposition (heterocoagulation mechanism) of the cross-linked P4VP, PEI, or their mixtures on the surfaces of the template colloidal silica particles in nitromethane (for PEI) or a nitromethane-acetone mixture (for P4VP and P4VP-PEI mixtures) in the presence of cross-linker 1,4-diiodobutane. The cross-linked polymeric shell swollen in a good solvent stabilized the core-shell colloids. This mechanism provided the conditions for the synthesis of core-shell colloids in a submicrometer range of dimensions with an easily adjusted shell thickness (wall of the capsules) ranging from a few to hundreds of nanometers. The chemical composition of the shell was tuned by varying the ratio of co-cross-linked shell-forming polymers (P4VP and PEI). In the second step, the hollow capsules were obtained by etching the silica core in HF solutions. In this step, the colloidal stability of the hollow capsules was provided by ionized P4VP and PEI cross-linked shells. The hollow capsules demonstrate that the pH- and ionic-strength-triggered swelling and shrinking result in size-selective uptake and release properties. Cross-linked via quaternized functional groups, P4VP capsules undergo swelling and shrinking transitions at a physiologically relevant pH of around 6. The 200-nm-diameter hollow capsule with 25-nm-thick walls demonstrated a factor of 2 greater capacity to accommodate cargo molecules than the core-shell particles of the same dimensions because of an internal compartment and a combination of radial and a circumferential swelling modes in the capsules.     

核交联的含磺酸甜菜碱pH敏感胶束的制备与表征

制备了一种在疏水段带有侧基叠氮官能团的两亲性pH敏感的聚合物——聚己内酯-聚(甲基丙烯酸二乙氨基乙酯-磺酸甜菜碱)((PCL-ACL)-PDEAS);同时合成了两端带有炔基中间带有二硫键的交联剂,用红外、核磁表征了目标分子.通过两亲性高分子自组装形成胶束,并通过点击化学反应获得了核交联的胶束.通过动态光散射测定粒径,胶束酸碱滴定表征胶束的pH敏感性,还原条件下释放药物的速度,对比了非交联胶束和交联胶束的性质.结果表明,交联胶束在正常生理条件下的释放速度比未交联胶束更慢;而在有DTT的存在条件下,交联胶束由于二硫键断裂,释放速率明显加快.因此,核交联载药胶束有可能响应肿瘤的微环境实现靶向释放.     

Block ionomer complex micelles with cross-linked cores for drug delivery

Soft polymeric nanomaterials were synthesized by template-assisted method involving condensation of the poly(ethylene oxide)-b-polycarboxylate anions by metal ions into core-shell block ionomer complex micelles followed by chemical cross-linking of the polyion chains in the micelle cores. The resulting materials represent nanogels and are capable of swelling in a pH-dependent manner. The structural determinants that guide the self-assembly of the initial micelle templates and the swelling behavior of the cross-linked micelles include the block ionomer structure, the chemical nature of metal ions, the structure of the cross-links and the degree of cross-linking. The application of these materials for loading and release of a drug, cisplatin, is evaluated. These cross-linked block ionomer micelles have promise for delivery of pharmaceutical agents. The text was submitted by the authors in English. This work was supported by the grants from U.S.A. National Institute of Health CA116590 (T.B.), National Science Foundation DMR-0513699 (A.V.K. and T.B.) and Department of Defense USAMRMC 06108004 (A.V.K.).     

Fluorescent core-shell silica nanoparticles: towards "Lab on a Particle" architectures for nanobiotechnology

Novel nanoscale fluorescent materials are integral to the progress of emergent fields such as nanobiotechnology and facilitate new research in a variety of contexts. Sol-gel derived silica is an excellent host material for creating fluorescent nanoparticles by the inclusion of covalently-bound organic dyes. Significant enhancements in the brightness and stability of organic dye emission can be achieved for silica-based core-shell nanoparticle architectures at length scales down to tens of nanometers with narrow size distributions. This tutorial review will highlight these findings and describe the evolution of the fluorescent core-shell silica nanoparticle concept towards integration of multiple functionalities including mesoporosity, metal nanoshells and quantitative chemical sensing. These developments point towards the development of "lab on a particle" architectures with promising prospects for nanobiotechnology, drug development and beyond.     

Silica-metal core-shell nanostructures

Silica-metal nanostructures consisting of silica cores and metal nanoshells attract a lot of attention because of their unique properties and potential applications ranging from catalysis and biosensing to optical devices and medicine. The important feature of these nanostructures is the possibility of controlling their properties by the variation of their geometry, shell morphology and shell material. This review is devoted to silica-noble metal core-shell nanostructures; specifically, it outlines the main methods used for the preparation and surface modification of silica particles and presents the major strategies for the formation of metal nanoshells on the modified silica particles. A special emphasis is given to the St?ber method, which is relatively simple, effective and well verified for the synthesis of large and highly uniform silica particles (with diameters from 100 nm to a few microns). Next, the surface chemistry of these particles is discussed with a special focus on the attachment of specific organic groups such as aminopropyl or mercaptopropyl groups, which interact strongly with metal species. Finally, the synthesis, characterization and application of various silica-metal core-shell nanostructures are reviewed, especially in relation to the siliceous cores with gold or silver nanoshells. Nowadays, gold is most often used metal for the formation of nanoshells due to its beneficial properties for many applications. However, other metals such as silver, platinum, palladium, nickel and copper were also used for fabrication of core-shell nanostructures. Silica-metal nanostructures can be prepared using various methods, for instance, (i) growth of metal nanoshells on the siliceous cores with deposited metal nanoparticles, (ii) reduction of metal species accompanied by precipitation of metal nanoparticles on the modified silica cores, and (iii) formation of metal nanoshells under ultrasonic conditions. A special emphasis is given to the seed-mediated growth, where metal nanoshells are formed on the modified silica cores with deposited metal nanoparticles. This strategy assures a good control of the nanoshell thickness as well as its surface properties.     

Supramolecular core-shell nanosilica@liposome nanocapsules for drug delivery

The fabrication of core-shell structural nanosilica@liposome nanocapsules as a drug delivery vehicle is reported. SiO(2) nanoparticles are encapsulated within liposomes by a W/O/W emulsion approach to form supramolecular assemblies with a core of colloidal particles enveloped by a lipid bilayer shell. A nanosilica core provides charge compensation and architectural support for the lipid bilayer, which significantly improves their physical stability. A preliminary application of these core-shell nanocapsules for hemoglobin (Hb) delivery is described. Through the H-bonding interaction between the hydroxyl groups on nanosilicas and the amino nitrogens of Hb, Hb-SiO(2) nanocomplexes in which the saturated adsorption amount of Hb on SiO(2) is 0.47 g g(-1) are coated with lipids to generate core-shell Hb-SiO(2)@liposome nanocapsules with mean diameters of 60-500 nm and Hb encapsulation efficiency of 48.4-87.9%. Hb-SiO(2)@liposome supramolecular nanovehicles create a mode of delivery that stabilizes the encapsulated Hb and achieves long-lasting release, thereby improving the efficacy of the drug. Compared with liposome-encapsulated Hb and Hb-loaded SiO(2) particles, such core-shell nanovehicles show substantially enhanced release performance of Hb in vitro. This finding opens up a new window of liposome-based formulations as drug delivery nanovehicles for widespread pharmaceutical applications.     

Camptothecin-incorporating N-phthaloylchitosan-g-mPEG self-assembly micellar system: effect of degree of deacetylation

Amphiphilic grafted copolymers, N-phthaloylchitosan-grafted poly (ethylene glycol) methyl ether (PLC-g-mPEG), were synthesized from chitosan with different degree of deacetylation (DD=80%, 85%, 90% and 95%). Due to their amphiphilic characteristic, these copolymers could form micelle-like nanoparticles. The critical micelle concentration (CMC) of these nanoparticles with different DD in water was similar (28microg/ml). Under transmission electron microscope (TEM), the nanoparticles exhibited a regular spherical shape with core-shell structure. The particle sizes determined by dynamic light scattering were in the range of 100-250nm, and increased as the %DD of chitosan increased. The cytotoxicity of phthaloylchitosans (PLC) and PLC-g-mPEG in Hela cells line were evaluated. The results showed that cytotoxicity of PLC and PLC-g-mPEG increased with increasing %DD of chitosan. The cytotoxicity of PLC-g-mPEG was significantly lower than that of PLC. Camptothecin as a model drug was loaded into the inner core of the micelles by dialysis method. It was found that %DD of chitosan, corresponding to the N-phthaloyl groups in the inner core of the nanoparticle obtained, was a key factor in controlling %yield, stability of the drug-loaded micelles, and drug release behavior. As the %DD increased, the CPT-loaded micelles stability increased. Release of CPT from the micelles was dependent on the %DD and a sustained release was obtained in high %DD.     

Polymer micelle with cross-linked ionic core

This work reports the design of polymer micelles with cross-linked ionic cores that display high stability. Block ionomer complexes were utilized as a micellar template for the synthesis of the cross-linked micelles. Such micelles represent hydrophilic nanospheres of core-shell morphology. The core comprises a network of the cross-linked polyanions, which is surrounded by the shell of hydrophilic PEO chains.     

New advances in gated materials of mesoporous silica for drug controlled release

Drug delivery systems (DDS) are used to deliver therapeutic drugs to improve selectivity and reduce side effects. With the development of nanotechnology, many nanocarriers have been developed and applied to drug delivery, including mesoporous silica. Mesoporous silica nanoparticles (MSNs) have attracted a lot of attention for simple synthesis, biocompatibility, high surface area and pore volume. Based on the pore system and surface modification, gated mesoporous silica nanoparticles can be designed to realize on-command drug release, which provides a new approach for selective delivery of antitumor drugs. Herein, this review mainly focuses on the “gate keepers” of mesoporous silica for drug controlled release in nearly few years (2017–2020). We summarize the mechanism of drug controlled release in gated MSNs and different gated materials: inorganic gated materials, organic gated materials, self-gated drug molecules, and biological membranes. The facing challenges and future prospects of gated MSNs are discussed rationally in the end.     

具有肿瘤荧光成像性能的核壳纳米过氧化氢酶模拟物

运用微波法在硅核壳荧光材料的表面修饰了2-(二吡啶甲胺基)丙酸的锰配合物,获得具有荧光性能的锰-硅核壳纳米结构复合物,运用IR,UV,TEM等方法表征了纳米复合物的结构。H2O2岐化实验显示锰-硅核壳纳米复合物具有较好的过氧化氢酶模拟特性,是一种新的纳米过氧化氢酶模拟物。体外细胞荧光成像研究表明2-(二吡啶甲胺基)丙酸修饰的纳米球不能进入肿瘤细胞内,而锰-硅核壳纳米复合物能进入肿瘤细胞内,具备良好的肿瘤靶向性,显著提高肿瘤荧光成像效果,可作为新型的肿瘤成像剂。