Droplet emulsification in microfluidic devices involves the constant formation of fresh interfaces between two immiscible fluids. When the multiphase system contains surfactant, dynamic mass transfer of the surfactant onto the interface results in a dynamic interfacial tension different from the static interfacial tension measured in an equilibrium state. In this work, we have systematically investigated the effects of surfactant concentration and type on the dynamic interfacial tension of two different liquid-liquid two phase systems [N-hexane/water-sodium dodecyl sulfate (SDS) and N-hexane/water-cetyltrimethylammonium bromide (CTAB)] rapidly producing relatively small droplets in coaxial microfluidic devices. Dynamic interfacial tension experiments using the pendent drop method and a tensiometer were conducted, and a semiempirical equation was developed to put into context the effects of surfactants and the experimental conditions on droplet formation and dynamic interfacial tension in dynamic microchannel flows. The results presented in this work provide a more in-depth understanding of the dynamic effects of surfactants on droplet formation and the precise controllable preparation of monodispersed droplets in microfluidic devices.
This work describes a novel microfluidic method to prepare monodispersed chitosan microspheres by using the solvent extraction method. Our strategy is that a chitosan/acetic acid aqueous solution is emulsified in an organic phase containing the extractant by using the co-flowing shear method in a co-axial microfluidic device. The formed droplets are in situ solidified within a synthesizing channel by the extraction of acetic acid from the chitosan aqueous droplets to the organic solution. Based on this approach, the size of chitosan microspheres can be successfully controlled from 100 mum to 700 mum in diameter with a variation of less than 4%. Furthermore, high loading efficiency (>95%) of Bovine serum albumin (BSA) can be in situ encapsulated. The present method has the advantages of actively controlling the droplet diameter, narrow size distribution, good sphericity, and having a simple and low cost process, with a high throughput. This approach for the preparation of chitosan microspheres will provide many potential applications for pharmaceutical area.
In this study, we developed a new method for the direct measurement of differential pressures in a co-flow junction microfluidic device using a Capillary Laplace Gauge (CLG). The CLG - used inside the microchannel device--was designed using a tapered glass-capillary set up in co-flow junction architecture with a three-phase liquid-liquid-gas system with two flowing liquid phases and an entrained gas phase. By taking advantage of the Laplace equation, basic geometric relations and an integrated image analysis program, the movement of the entrained gas phase with the flow of the liquid-phases is tracked and monitored, allowing the gauge to function as an ultra-sensitive, integrated, differential pressure sensor measuring fluctuations in the liquid-dispersed phase channel pressure as small as tens of Pascals caused by droplet formation. The gauge was used to monitor the drop formation and breakup process in a co-flow junction microfluidic device under different flow conditions across a large range (1 × 10(-3) to 2.0 × 10(-1)) of capillary numbers. In addition to being able to monitor short and long term dispersed phase pressure fluctuation trends for both single drop and large droplet populations, the gauge was also used to clearly identify a transition between the dripping and jetting flow regimes. Overall, the combination of a unique, integrated image analysis program with this new type of sensor serves as a powerful tool with great potential for a variety of different research and industrial applications requiring sensitive microchannel pressure measurements.
This investigation of tuberculosis (TB) treatment regimens in 6 TB hospitals in China showed that only 18% of patients with new cases and 9% of patients with retreatment cases were prescribed standard TB treatment regimens. Adherence to treatment guidelines needs to be improved in TB hospitals to control multidrug-resistant TB in China.
In this work, a coflowing microfluidic device was used to determine the influence of different mixed sodium dodecyl sulfate (SDS)-poly(ethylene glycol) (PEG) compound systems on dynamic interfacial tension and, by extension, corresponding emulsion droplet sizes. The aqueous solutions were used as the continuous phase in the microfluidic device, while octane was used as the organic dispersed phase. Combined SDS-PEG systems lower the interfacial tension more than either component can alone up to the critical aggregation concentration (CAC) of SDS. Octane droplet sizes produced in the microfluidic device using combined SDS-PEG systems were smaller than those produced using SDS alone, and a reduction in dynamic interfacial tension as determined by drop size followed a pattern similar to that observed in the static case (PEG4000 > PEG600 > PEG400 > PEG200 > PEG8000) with the exception of PEG8000. Finally, a previously formulated model relating interfacial tension to droplet size was used to estimate the dynamic interfacial tensions in the microfluidic device.
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