A theoretical study of the emulsion polymerization of styrene: The effect of the initial dispersion of the system on the molecular-mass distribution of polystyrene

On the basis of the mathematical model of emulsion polymerization, which takes into account the possibility of formation of polymer-monomer particles from monomer microdroplets, the molecular-mass distribution of the polymer formed in systems with different initial states of the original emulsion system (monodisperse or bidisperse system of microdroplets) is calculated. It is shown that the molecular-mass distribution of the polymer is governed by the state of the original emulsion system and the conversion of the monomer.     

A theoretical study of the emulsion polymerization of styrene: The effect of the initial dispersion of the system on the polymerization rate and size distribution of polymer-monomer particles

A mathematical model of emulsion polymerization that takes into account the possibility of formation of polymer-monomer particles from monomer microdroplets is proposed. It is shown that the theoretically calculated polymerization rate, the concentration of polymer-monomer particles, and their size distribution are governed by the initial state of the original emulsion system (monodisperse or bidisperse system of microdroplets).     

Microfluidic fabrication of water-in-water droplets encapsulated in hydrogel microfibers

By combining microfiber spinning techniques with aqueous two phase system (ATPS), a rapid and simple strategy to fabricate water-in-water (w/w) droplets encapsulated in microfibers was proposed for the first time. Hydrophilic environment in hydrogel and the fiber format facilitates higher biocompatibility, convenient manipulation of the droplets and recycling of the contents inside droplets, which would have promising development in biological, pharmacological and environmental fields.     

Miniaturizing chemistry and biology in microdroplets

By compartmentalizing reactions in aqueous microdroplets of water-in-oil emulsions, reaction volumes can be reduced by factors of up to 10(9) compared to conventional microtitre-plate based systems. This allows massively parallel processing of as many as 10(10) reactions in a total volume of only 1 ml of emulsion. This review describes the use of emulsions for directed evolution of proteins and RNAs, and for performing polymerase chain reactions (PCRs). To illustrate these applications we describe certain specific experiments, each of which exemplifies a different facet of the technique, in some detail. These examples include directed evolution of Diels-Alderase and RNA ligase ribozymes and several classes of protein enzymes, including DNA polymerases, phosphotriesterases, beta-galactosidases and thiolactonases. We also describe the application of emulsion PCR to screen for rare mutations and for new ultra-high throughput sequencing technologies. Finally, we discuss the recent development of microfluidic tools for making and manipulating microdroplets and their likely impact on the future development of the field.     

Microdroplet size prediction in microfluidic systems via artificial neural network modeling for water-in-oil emulsion formulation

In this paper, an experimental study and modeling by artificial neural networks were carried out to predict the generated microdroplet dimensionless size in a microfluidic system in order to formulate a water-in-oil emulsion. The various parameters that affect the size of microdroplets (flow rates, viscosities, surface tensions of both the two phases and the diameter of the microchannel) are studied and further grouped into dimensionless numbers; we used these numbers as input to the neural network and the dimensionless length as output. The better neural network architecture has 10 neurons in the hidden layer with a mean square error of 1.4 10^?6 and a determination’s coefficient near 1 value. The relative importance of inputs on the size of the microdroplets has been determined using the Garson algorithm and the results are in good agreement with other works.     

Artificial red cells with crosslinked hemoglobin membranes

Artificial cells containing concentrated hemoglobin (Hb) solution were prepared by interfacial polymerization of Hb with glutaraldehyde (GA) in liquid membrane capsules (LMC). A solution containing 30% of Hb was emulsified in mineral oil as red cell-size microdroplets, and this emulsion was dispersed in an aqueous phase containing glutaraldehyde to form LMC. The LMC were semipermeable templates that held the microdroplets of Hb in suspension while GA diffused through the oil to the microdroplet surfaces. The GA crosslinked Hb at the surface of each microdroplet to form an artificial red-cell membrane encapsulating Hb solution. A water-soluble surfactant was used to eject the cells from the LMC and suspend them in saline. Several surfactants were evaluated. Cell size was controlled by agitation speed during preparation of the original emulsion. Cells of 2.52 = ±1.69 μm were prepared. The encapsulated Hb retained capacity to bind and release O₂. The cells had aP ₅₀ of 8.9 torr (1200 Pa) and a capacity of 0.55 cc O₂/g of total Hb, indicating that the crosslinked portion of the Hb did not contribute to O₂ transport.     

Cross-linked starch nanoparticles stabilized Pickering emulsion polymerization of styrene in w/o/w system

Here, we present a method to synthesize expandable spherical polystyrene beads containing well-dispersed water microdroplets. The beads, 2–3 mm in diameter, were prepared through surfactant-free Pickering emulsion polymerization in water-in-oil-in-water (w/o/w) system using cross-linked starch nanoparticles (CSTN) as emulsifier. The CSTNs were in situ surface-modified by styrene maleic anhydride copolymer as confirmed by infrared spectroscopy and contact angle analysis. The entrapped water microdroplets with the average size of 3–4 μm were shown to be surrounded by a dense layer of the CSTN. The number droplet density as well as water encapsulation efficiency in the polystyrene beads increased with the CSTN concentration. Furthermore, regardless of CSTN content, all samples exhibited high encapsulation stability of over 68 % after 3 months. These characteristics along with good expansion behavior suggest the synthesized beads as expandable polystyrene containing water as a green blowing agent.     

Effects of structural transformations in magnetic emulsions

Structural transformations and relevant changes in the magnetic and optical properties of magnetosensitive emulsions based on magnetic fluids are experimentally studied. Peculiarities of the changes in the magnetic susceptibility of emulsions associated with the deformation of their microdroplets and the effect of phase inversion (the transformation of dispersions of magnetic droplets in nonmagnetic media into dispersions of nonmagnetic droplets in magnetic fluids) are established. Optical effects occurring in magnetic emulsions under the combined action of a shear flow and a magnetic field are studied. It is concluded that optically active composition media may be developed on the basis of magnetic fluids.     

Effect of surfactants on the porous structure of poly(<Emphasis Type="Italic">N</Emphasis>-isopropylacrylamide) hydrogels prepared by an emulsion templating method

Stimuli-sensitive porous hydrogels prepared with an emulsion templating method developed by the authors are potentially applicable in the medical and pharmaceutical fields; thermosensitive N-isopropylacrylamide (NIPA) hydrogels having randomly distributed sphere-like cavities have been prepared by the polymerization in an aqueous phase in an oil-in-water (O/W) emulsion, followed by the washing of oil (oleyl alcohol) microdroplets. The surfactant plays a dominant role in the preparation of porous hydrogels and the pore size. This study concerns with the surfactant effects on the stability of pre-gel O/W emulsions. The porous NIPA hydrogels were successfully prepared using the surfactants forming the stable emulsion and their internal structures and swelling properties were characterized. The O/W emulsions and the porous hydrogels prepared using various amounts of oil and surfactant were characterized. The information obtained serves for preparation of porous hydrogels having suitable porous structure for their applications.     

Preparation of poly(N-isopropylacrylamide) emulsion gels and their drug release behaviors

Stimuli-sensitive drug delivery systems (DDSs) have attracted considerable attention in medical and pharmaceutical fields; thermosensitive DDS dealing with poly(N-isopropylacrylamide) (poly(NIPA)) have been widely studied. Novel NIPA emulsion gels, i.e., NIPA hydrogels containing distributed oil (oleyl alcohol) microdroplets, were synthesized by means of an emulsion-gelation method in which the polymerization of hydrogels in an aqueous phase in an oil-in-water (O/W) emulsion and the loading of a lipophilic drug (indomethacin) dissolved in an oil phase were accomplished simultaneously. The pulsatile (on-off) drug release from the NIPA emulsion gel loading indomethacin to a phosphate buffered saline (PBS) solution was successfully controlled by a temperature swing between 25 degrees C (release off) and 40 degrees C (release on). The mechanism of the pulsatile drug release was discussed in relation to the diffusion rate, distribution ratio, solvent exchange of NIPA hydrogels, and drug release from an NIPA organogel. The mechanism was as follows: the solvent exchange occurred within the NIPA emulsion gel (the NIPA gel-network absorbed oleyl alcohol with indomethacin) at temperatures above the LCST, and the diffusion rate of indomethacin through the solvent-exchanged gel was higher at 40 degrees C than at 25 degrees C.     

Chemoselective N-Alkylation of Indoles in Aqueous Microdroplets

Many reactions show much faster kinetics in microdroplets than in the bulk phase. Most reported reactions in microdroplets mirror the products found in bulk reactions. However, the unique environment of microdroplets allows different chemistry to occur. In this work, we present the first chemoselective N-alkylation of indoles in aqueous microdroplets via a three-component Mannich-type reaction without using any catalyst. In sharp contrast, bulk reactions using the same reagents with a catalyst yield exclusively C-alkylation products. The N-alkylation yield is moderate in microdroplets, up to 53 %. We extended the scope of the microdroplet reaction and obtained a series of new functionalized indole aminals, which are likely to have biological activities. This work clearly indicates that microdroplet reactions can show reactivity quite different from that of bulk-phase reactions, which holds great potential for developing novel reactivities in microdroplets.     

Chemoselective N‐Alkylation of Indoles in Aqueous Microdroplets

Many reactions show much faster kinetics in microdroplets than in the bulk phase. Most reported reactions in microdroplets mirror the products found in bulk reactions. However, the unique environment of microdroplets allows different chemistry to occur. In this work, we present the first chemoselective N‐alkylation of indoles in aqueous microdroplets via a three‐component Mannich‐type reaction without using any catalyst. In sharp contrast, bulk reactions using the same reagents with a catalyst yield exclusively C‐alkylation products. The N‐alkylation yield is moderate in microdroplets, up to 53 %. We extended the scope of the microdroplet reaction and obtained a series of new functionalized indole aminals, which are likely to have biological activities. This work clearly indicates that microdroplet reactions can show reactivity quite different from that of bulk‐phase reactions, which holds great potential for developing novel reactivities in microdroplets.     

Microemulsion polymerization of styrene in the presence of a cationic emulsifier

The principal subject discussed in the current paper is the radical polymerization of styrene in the three- and four component microemulsions stabilized by a cationic emulsifier. Polymerization in the o/w microemulsion is a new polymerization technique which allows to prepare the polymer latexes with the very high particle interface area and narrow particle size distribution. Polymers formed are very large with a very broad molecular weight distribution. In emulsion and microemulsion polymerizations, the reaction takes place in a large number of isolated loci dispersed in the continuous aqueous phase. However, in spite of the similarities between emulsion and microemulsion polymerization, there are large differences caused by the much larger amount of emulsifier in the latter process. In the emulsion polymerization there are three rate intervals. In the microemulsion polymerization only two reaction rate intervals are commonly detected: first, the polymerization rate increases rapidly with the reaction time and then decreases steadily. Essential features of microemulsion polymerization are as follows: (1) polymerization proceeds under non-stationary state conditions; (2) size and particle concentration increases throughout the course of polymerization; (3) chain-transfer to monomer/exit of transferred monomeric radical/radical re-entry events are operative; and (4) molecular weight is independent of conversion and distribution of resulting polymer is very broad. The number of microdroplets or monomer-starved micelles at higher conversion is high and they persist throughout the reaction. The high emulsifier/water ratio ensures that the emulsifier is undissociated and can penetrate into the microdroplets. The presence of a large amount of emulsifier strongly influences the reaction kinetics and the particle nucleation. The mixed mode particle nucleation is assumed to govern the polymerization process. At low emulsifier concentration the micellar nucleation is dominant while at a high emulsifier concentration the interaction-like homogeneous nucleation is operative. Furthermore, the paper is focused on the initiation and nucleation mechanisms, location of initiation locus, and growth and deactivation of latex particles. Furthermore, the relationship between kinetic and molecular weight parameters of the microemulsion polymerization process and colloidal (water/particle interface) parameters is discussed. In particular, we follow the effect of initiator and emulsifier type and concentration on the polymerization process. Besides, the effects of monomer concentration and additives are also evaluated.     

The preparation of sterically stabilized polymer dispersions

The emulsion polymerizations of styrene (St) and butyl acrylate (BA) stabilized by nonionic polyoxyethylene type emulsifiers did not show the long stationary rate interval. This was discussed in terms of two opposing effects: 1) the decreased monomer concentration at the reaction loci due to the depletion of monomer droplets or depressed monomer droplet degradation and 2) the increased number of polymer particles with increasing conversion. The continuous particle nucleation is attributed to the continuous release of emulsifier from the emulsifier saturated monomer droplets and/or the presence of monomer swollen micelles (microdroplets). The limited particle flocculation operative at lower emulsifier concentrations increases the nonstationary-state polymerization. The particle agglomeration is accompanied by the increased reaction order x (N_p vs. [E]^x) above 0.6. The increased uniformity of monomer emulsion stabilized by Tween 20 by homogenization of monomer emulsion increased the final conversion and the polymerization rate as well. The polymerization rate vs. conversion curve of the homogenized emulsion characterized with broader stationary rate interval reminds the four rate intervals system typical for miniemulsion. The accumulation of polymer and nonionic emulsifier within the monomer phase preserves the monomer droplets up to high conversion. The decreased monomer droplet degradation rises the monomer-starved condition or the depressed transport of both monomer and emulsifier to the reaction loci.     

Droplet Precise Self-Splitting on Patterned Adhesive Surfaces for Simultaneous Multidetection

Precise separation and localization of microdroplets are fundamental for various fields, such as high-throughput screening, combinatorial chemistry, and the recognition of complex analytes. We have developed a droplet self-splitting strategy to divide an impacting droplet into predictable microdroplets and deposit them at preset spots for simultaneous multidetection. No matter exchange was observed between these microdroplets, so they could be manipulated independently. Droplet self-splitting was attributed to anisotropic liquid recoiling on the patterned adhesive surface, as influenced by the droplet Weber number and the width of the low-adhesive stripe. A quantitative criterion was also developed to judge the droplet self-splitting capability. The precise separation and distribution of microdroplets enabled simultaneous arrayed reactions and multiple analyte detection using one droplet of sample.     

Superparamagnetic Polymer Emulsion Particles from a Soap-Free Seeded Emulsion Polymerization and their Application for Lipase Immobilization

Using emulsion copolymer of styrene (St), glycidyl methacrylate (GMA) and 2-hydroxyethyl methacrylate (HEMA) as seed latexes, the superparamagnetic polymer emulsion particles were prepared by seeded emulsion copolymerization of butyl methacrylate (BMA), vinyl acetate (VAc) and ethylene glycol dimethacrylate in the presence of the seed latexes and superparamagnetic Fe₃O₄/SiOx nanoparticles (or Fe₃O₄-APTS nanoparticles) through a two-step process, without addition of any emulsifier. The magnetic emulsion particles named P(St-GMA-HEMA)/P(BMA-VAc) were characterized by transmission electron microscope and vibrating sample magnetometry. The results showed that the magnetic emulsion particles held a structure with a thinner shell (around 100 nm) and a bigger cavity (around 200 nm), and possessed a certain level of magnetic response. The resulting magnetic emulsion particles were employed in the immobilization of lipase by two strategies to immobilized lipase onto the resulting magnetic composites directly (S-1) or using glutaraldehyde as a coupling agent (S-2), thus, experimental data showed that the thermal stability and reusability of immobilized lipase based on S-2 were higher than that of S-1.     

Selective Transportation of Microdroplets Assisted by a Superhydrophobic Surface with pH‐Responsive Adhesion

We report a new strategy to realize the selective transportation of microdroplets assisted by a superhydrophobic surface with pH‐responsive adhesion. On the surface, only basic microdroplets can be pinned and acidic or neutral microdroplets can easily roll off. Therefore, by using the surface as a “mechanical hand”, microdroplets can be transported selectively according to one’s requirements by simply controlling the pH of the solution. The special ability of the surface to achieve selective transportation is ascribed to the following two reasons: 1) superhydrophobicity, which can avoid the wetting problem, and 2) pH‐responsive adhesion, which results from the combined effect of chemical variation of the carboxylic acid group and microstructures on the surface. Furthermore, we also demonstrated a process of selective transportation of microdroplets for applications in droplet‐based microreactors through our surface. The results reported herein advance a new method to realize the selective transportation of microdroplets and we believe that this method could potentially be used in a wide range of applications, such as biomolecular detection and transportation in biochips.     

Chaotic mixing in microdroplets

We describe a general methodology for introducing thorough chaotic mixing in microdroplets. The mixing properties of fluid flows in microdroplets are governed by their symmetries, which give rise to invariant surfaces serving as barriers to transport. Complete three-dimensional mixing by chaotic advection requires destruction of all flow invariants. To illustrate this idea, we demonstrate that complete mixing can be obtained in a time-dependent flow produced by moving a microdroplet along a two-dimensional path. The theoretical predictions are confirmed by experiments that use the thermocapillary effect to manipulate microdroplets.     

Electrical Properties of Chain Microstructure Magnetic Emulsions in Magnetic Field

The work deals with the experimental study of the emulsion whose dispersion medium is a magnetic fluid while the disperse phase is formed by a glycerin-water mixture. It is demonstrated that under effect of a magnetic field chain aggregates form from the disperse phase drops. Such emulsion microstructure change affects its macroscopic properties. The emulsion dielectric permeability and specific electrical conductivity have been measured. It is demonstrated that under the effect of relatively weak external magnetic fields (～1 kA/m) the emulsion electrical parameters may change several fold. The work theoretically analyzes the discovered regularities of the emulsion electrical properties.     

Discrete microfluidics with electrochemical detection

A droplet-based electrochemical digital magnetofluidics system has been developed. The system relies on the magnetic movement, in air, of different aqueous microdroplets containing magnetic microparticles--serving as the 'sample', 'blank', 'wash' and 'reagent' solutions--into and out of a three-electrode assembly. The movement of all droplets was controlled using the magnetic fields generated by three separate external magnets positioned below the superhydrophobic surface. Square-wave voltammetry was used for rapid measurements of dopamine in multiple successive microdrops with minimal cross talk. The ability of the droplet-based electrochemical microfluidic system to manipulate microliter solutions was also illustrated in bioassays of glucose, involving the merging of enzyme (GOx) and substrate droplets, followed by chronoamperometric measurements of the hydrogen peroxide product in the merged droplet. Variables of the new electrochemical digital magnetomicrofluidic technique were examined and optimized. The new droplet-based electrochemical microfluidic system offers a promising platform for automated clinical diagnostics and drug discovery.