Monodisperse polymer gel particles with micrometer‐scale dimensions serve for a variety of applications, including those as microcapsules for actives or as micrometer‐sized matrixes for mesoscopic additives. These particles can be produced with exquisite control through the use of droplet‐based microfluidic templating followed by subsequent droplet solidification. This can be achieved by two ways: One way is to use pre‐microgel solutions of low molecular weight monomers and to form microgels by polymerizing these monomers. Another way is to use pre‐polymerized, high molecular weight precursors and to gel them by polymer‐analogous crosslinking. Both approaches have their specific advantages, allowing microgels to be tailored and optimized for specific needs such as those as delivery systems or scaffolds for living cells. This article highlights some recent achievements in the development and use of these microfluidic techniques to fabricate functional microgel particles.
It still remains a big challenge to fabricate binary colloidal crystals (binary CCs) from hard colloidal spheres, although a lot of efforts have been made. Here, for the first time, binary CCs are assembled from soft hydrogel spheres, PNIPAM microgels, instead of hard spheres. Different from hard spheres, microgel binary CCs can be facilely fabricated by simply heating binary microgel dispersions to 37 °C and then allowing them to cool back to room temperature. The formation of highly ordered structure is indicated by the appearance of an iridescent color and a sharp Bragg diffraction peak. Compared with hard sphere binary CCs, the assembly of PNIPAM microgel binary CCs is much simpler, faster and with a higher “atom” economy. The easy formation of PNIPAM microgel binary CC is attributed to the thermosensitivity and soft nature of the PNIPAM microgel spheres. In addition, PNIPAM microgel binary CCs can respond to temperature change, and their stop band can be tuned by changing the concentration of the dispersion.
Polymer microgels with sizes of some tens to hundreds of micrometers can be formed with exquisite control by droplet‐based microfluidic templating. This study presents a systematic assessment of the effect of the premicrogel droplet size on the ability of production of such microgels. The focus is on two popular acrylamide‐derivatives at a fixed monomer concentration and external polymerization temperature. An exponential dependence of the success of droplet gelation on the droplet size is found, which can be rationalized in view of the balance between production and transfer of heat within and from the droplets on basis of a simple Arrhenius argument.
Summary: An in‐situ mineralization process in the presence of thermo‐responsive microgels leads to the formation of well‐defined hybrid materials. Experimental data suggest that control of the mineralization process in the presence of the microgels offers the possibility to obtain sub‐micrometer‐sized hybrid particles or macroscopic hybrid hydrogels. The rapid formation of CaCO3 crystals in the microgel structure favors the preparation of the hybrid particles wherein inorganic crystals cover the shell layer of the microgel. The slow formation of CaCO3 crystals leads to the simultaneous self‐assembly of the microgel particles on the bottom of the reaction vessel, and the formation of a physical network. It has been demonstrated that hybrid hydrogel materials with different calcium carbonate contents and temperature‐dependent swelling‐deswelling properties can be prepared.
Formation of a hybrid hydrogel by the vapor diffusion method. 相似文献
Colloidal supraparticles integrated with multicomponent primary particles come with emerging or synergetic functionalities. However, achieving the functional customization of supraparticles remains a great challenge because of the limited options of building blocks with tailorability and functional extensibility. Herein, we developed a universal approach to construct customizable supraparticles with desired properties from molecular building blocks obtained by the covalent conjugation of catechol groups with a series of orthogonal functional groups. These catechol-terminated molecular building blocks can assemble into primary particles driven by various intermolecular interactions (i.e. metal-organic coordination, host–guest, and hydrophobic interactions), and then further assemble into supraparticles governed by catechol-mediated interfacial interactions. Our strategy enables the formation of supraparticles with diverse functionalities, such as dual-pH responsiveness, light-controllable permeability, and non-invasive fluorescence labeling of living cells. The ease with which these supraparticles can be fabricated, and the ability to tailor their chemical and physical properties through the choice of metals and orthogonal functional groups used, should enable a variety of applications. 相似文献
Microgel capsules are micrometer‐sized particles that consist of a cross‐linked, solvent‐swollen polymer network complexed with additives. These particles have various applications, such as drug delivery, catalysis, and analytics. To optimize the performance of microgel capsules, it is crucial to control their size, shape, and content of encapsulated additives with high precision. There are two classes of microgel‐capsule structures. One class comprises bulk microcapsules that consist of a polymer network spanning the entire particle and entrapping the additive within its meshes. The other class comprises core–shell structures; in this case, the microgel polymer network just forms the shell of the particles, whereas their interior is hollow and hosts the encapsulated payload. Both types of structures can be produced with exquisite control by droplet‐based microfluidic templating followed by subsequent droplet gelation. This article highlights some early and recent achievements in the use of this technique to tailor soft microgel capsules; it also discusses applications of these particles. A special focus is on the encapsulation of living cells, which are very sensitive and complex but also very useful additives for immobilization within microgel particles. 相似文献
Cell‐free approaches to in situ tissue engineering require materials that are mechanically stable and are able to control cell‐adhesive behavior upon implantation. Here, the development of mechanically stable grafts with non‐cell adhesive properties via a mix‐and‐match approach using ureido‐pyrimidinone (UPy)‐modified supramolecular polymers is reported. Cell adhesion is prevented in vitro through mixing of end‐functionalized or chain‐extended UPy‐polycaprolactone (UPy‐PCL or CE‐UPy‐PCL, respectively) with end‐functionalized UPy‐poly(ethylene glycol) (UPy‐PEG) at a ratio of 90:10. Further characterization reveals intimate mixing behavior of UPy‐PCL with UPy‐PEG, but poor mechanical properties, whereas CE‐UPy‐PCL scaffolds are mechanically stable. As a proof‐of‐concept for the use of non‐cell adhesive supramolecular materials in vivo, electrospun vascular scaffolds are applied in an aortic interposition rat model, showing reduced cell infiltration in the presence of only 10% of UPy‐PEG. Together, these results provide the first steps toward advanced supramolecular biomaterials for in situ vascular tissue engineering with control over selective cell capturing.
Heteroporphyrins resulted from the replacement of one or two pyrrolic nitrogens with other hetero atoms such as O, S, Se and Te possess very interesting and distinct properties compared to tetrapyrrolic porphyrins. Specially, the singlet state energy levels can be fine tuned with suitable modification of porphyrin core by substituting pyrrolic “N” with other hetero atoms such as “O” and “S”. In this review, we describe our synthetic approaches for the synthesis of various mono‐functionalized heteroporphyrin building blocks and their use in the synthesis of several covalently and non‐covalently linked unsymmetrical porphyrin dyads containing two different porphyrin sub‐units. The photophysical studies are also described to show the possibility of singlet‐singlet energy transfer from one porphyrin sub‐unit to another in these unsymmetrical porphyrin dyads. 相似文献
The cyclo‐P4 complexes [CpRTa(CO)2(η4‐P4)] (CpR: Cp′′=1,3‐C5H3tBu2, Cp′′′=1,2,4‐C5H2tBu3) turned out to be predestined for the formation of hollow spherical supramolecules with non‐classical fullerene‐like topology. The resulting assemblies constructed with CuX (X=Cl, Br) showed a highly symmetric 32‐vertex core of solely four‐ and six‐membered rings. In some supramolecules, the inner cavity was occupied by an additional CuX unit. On the other hand, using CuI, two different supramolecules with either peanut‐ or pear‐like shapes and outer diameters in the range of 2–2.5 nm were isolated. Furthermore, the spherical supramolecules containing Cp′′′ ligands at tantalum are soluble in CH2Cl2. NMR spectroscopic investigations in solution revealed the formation of isomeric supramolecules owing to the steric hindrance caused by the third tBu group on the Cp′′′ ligand. In addition, a 2D coordination polymer was obtained and structurally characterized. 相似文献
We describe a facile approach for the synthesis of micrometer‐sized (∼3.5 μm), pH‐responsive microgel particles, which have functional carboxylic acid groups concentrated in the shell. The large size offers the possibility to directly study the interactions between individual, isolated microgel particles with active ingredients by optical microscopy. Our results show that the synthesized microgel particles can load and release active ingredients via changing pH values. The complexation of Ca2+ with the ‐COOH functional groups located at the microgel surfaces not only regulates the active ingredient's uptake efficiency, but also provides a novel way to reveal the spatial distribution of the functional groups inside the microgel particles. 相似文献
Well‐dispersed silver nanoparticles were successfully fabricated within poly[(N‐isopropylacrylamide)‐co‐(acrylic acid)] [P(NIPAM‐co‐AA)] microgel particles which were synthesized with different cross‐linking densities. Their structures were studied by field‐emission scanning electron microscopy, transmission electron microscopy, UV‐vis spectroscopy, X‐ray diffraction and FT‐IR spectroscopy. The interactions between the microgel particles and the incorporated silver nanoparticles were investigated by X‐ray photoelectron spectroscopy. The results revealed that there was charge transfer from the carbonyl groups of the microgel particles to the silver nanoparticles. Moreover, as the diameter of the AgNPs decreases, the charge‐transfer efficiency increases accordingly. The P(NIPAM‐co‐AA)/AgNPs hybrid microgel particles were thermoresponsive and their behavior completely reversible with several heating/cooling cycles.
We describe studies concerning the construction and characterization of insulin-impregnated poly(N-isopropylacrylamide-co-acrylic acid) microgel thin films prepared by Layer-by-Layer (LbL) polyelectrolyte assembly. These films can be built up in a highly uniform fashion and display linear buildup dependence even up to 30 layers. Thermoresponsivity of these drug loaded films can be utilized to obtain extended pulsatile release of insulin over many cycles. Continuous thermal pulsing allows solubilization of the embedded peptide and subsequent diffusion through the film layers. The magnitude of release can be tuned based on film thickness. This type of microgel thin film construct proves to be extremely robust and can potentially pulse out constant bursts of peptide for more than one month at a time. 相似文献
A supramolecular conjugate of myoglobin (Mb) and water‐soluble poly(acrylate), (PA5k and PA25k, where 5k and 25k represent the molecular weight of the polymers, respectively), is constructed on the basis of a noncovalent heme‐heme pocket interaction. The modified heme with an amino group linked to the terminus of one of the heme‐propionates is coupled to the side‐chain carboxyl groups of poly(acrylate) activated by N‐hydroxysuccinimide. The ratios of the heme‐modified monomer unit and the unmodified monomer unit (m:n) in the polymer chains of Heme‐PA5k and Heme‐PA25k were determined to be 4.5:95.5 and 3.1:96.9, respectively. Subsequent addition of apoMb to the conjugated polymers provides Mb‐connected fibrous nanostructures confirmed by atomic force microscopy. A mixture of the heme‐modified polymer and dimeric apomyoglobin as a cross‐linker forms a microgel in which the reconstituted myoglobin retains its native exogenous ligand binding activity. 相似文献
An antioxidant microgel with both glutathione peroxidase (GPx) and superoxide dismutase (SOD) activities is reported. Using computational design and genetic engineering methods, the main catalytic components of GPx are fabricated onto the surface of ferritin. The resulting seleno‐ferritin (Se‐Fn) monomers can self‐assemble into nanocomposites that exhibit remarkable GPx activity due to the well organized multi‐GPx catalytic centers. Subsequently, a porphyrin derivative is synthesized as an SOD mimic, and is employed to construct a synergistic dual enzyme system by crosslinking Se‐Fn nanocomposites into a microgel. Significantly, this dual enzyme microgel is demonstrated to display better antioxidant ability than single GPx or SOD mimics in protecting cells from oxidative damage.
A three‐dimensional DNA hydrogel was generated by self‐assembly of short linear double‐stranded DNA (dsDNA) building blocks equipped with sticky ends. The resulting DNA hydrogel is thermoresponsive and the length of the supramolecular dsDNA structures varies with temperature. The average diffusion coefficients of the supramolecular dsDNA structures formed by self‐assembly were determined by diffusion‐ordered NMR spectroscopy (DOSY NMR) for temperatures higher than 60 °C. Temperature‐dependent rheological measurements revealed a gel point of 42±1 °C. Below this temperature, the resulting material behaved as a true gel of high viscosity with values for the storage modulus G′ being significantly larger than that for the loss modulus G′′. Frequency‐dependent rheological measurements at 20 °C revealed a mesh size (ξ) of 15 nm. AFM analysis of the diluted hydrogel in the dry state showed densely packed structures of entangled chains, which are also expected to contain multiple interlocked rings and catenanes. 相似文献
Exclusive organic templating of macroporous oxide films is reported by using non‐close and lose packing of spherical copolymer aggregates, in combination with facile control of condensation degree/density of inorganic oxide frameworks. Unique macroporous oxide films, mainly titania showing highly porous, crystalline, and versatile properties, can be fabricated with continuous design from unusual 3‐D net‐shape to tunable spherical macrostructures, which expands the preparation of other inorganic oxide films (silica, alumina, and zirconia) and possibly adapts the use of other assembled organic polymers. The macroporous structures are helpful for effective accommodation of bulky biomoleculeshigh and diffusivity of organic molecules (useful for photocatalysts). Unusual structural variation, expansion of spherical voids, is also observed, being useful for fine tuning of optical property. 相似文献
The functionality of natural biopolymers has inspired significant effort to develop sequence‐defined synthetic polymers for applications including molecular recognition, self‐assembly, and catalysis. Conjugation of synthetic materials to biomacromolecules has played an increasingly important role in drug delivery and biomaterials. We developed a controlled synthesis of novel oligomers from hydroxyproline‐based building blocks and conjugated these materials to siRNA. Hydroxyproline‐based monomers enable the incorporation of broad structural diversity into defined polymer chains. Using a perfluorocarbon purification handle, we were able to purify diverse oligomers through a single solid‐phase extraction method. The efficiency of synthesis was demonstrated by building 14 unique trimers and 4 hexamers from 6 diverse building blocks. We then adapted this method to the parallel synthesis of hundreds of materials in 96‐well plates. This strategy provides a platform for the screening of libraries of modified biomolecules. 相似文献
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