Abstract
Droplet-based microfluidics offers unique advantages to create platforms that fabricate functionalized particles with increased accessibility, robustness, and simplicity. Herein we present a three-phase microfluidic device that can control the flow pattern to directly generate either core–shell or hole–shell microparticles. The major benefits of this device are the ease of controlling the morphology of the compound droplets by the flow rates and thus the microstructure of the synthesized microparticles. The transition between flow patterns enables the generation of either core–shell particles or Janus particles in a single device. We further show the versatility of the proposed device in fabrication of functionalized particles: the hole size of the hole–shell microparticle can be fine-tuned while its outer diameter is kept constant, and by adding Fe3O4 nanoparticles into the photocurable phase, the obtained magnetoresponsive microparticle can move rotationally or translationally under an external magnetic field. We anticipate that the present method could facilitate the fabrication of the functional microparticles for diverse applications.
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1 Introduction
Microparticles with tunable sizes, structures [1,2,3,4], and functions have important applications in the fields of drug delivery [5,6,7,8,9], controlled release [10,11,12,13,14], drug identification [15], biological diagnosis [3, 16], stabilizing liquid film [17], electrophoretic display [1, 18,19,20], and chemical microreaction [21]. In term of controlling drug release, functional behaviors of microparticles are strongly influenced by their sizes and structures. For instance, the drug release rate is proportional to the size of microparticles [22,23,24,25], a core–shell structure can protect the active substances in the core against undesired degradation [26], a hole–shell structure can control the release of the core contents through the hole [27], and a Janus structure can provide two compartments for encapsulating two different active materials and release them simultaneously [28]. Various conventional methods, such as inkjet printing [29], spray drying [30, 31], interfacial polymerization [32], membrane emulsification [33], were used to produce microparticles.
Recently, droplet-based microfluidics emerges as a powerful platform for generating highly monodisperse emulsion droplets in a controllable way [34,35,36,37,38]. Microdroplets are perfect templates for producing uniformly sized microparticles with different morphologies and functions. The size of synthesized microparticles can be precisely controlled by adjusting the flow rates [39, 40]. By photocuring the ultraviolet (UV)-curable phase of the core–shell droplets generated in axisymmetric capillary microfluidic devices, core–shell microparticles [26, 39, 41] can be synthesized. By changing the adhesion energy between the inner droplet and the outer phase, core–shell droplets can gradually evolve into Janus droplets for synthesizing hole–shell microparticles [42]. However, different fractions of ethoxylated trimethylolpropane triacrylate (ETPTA) monomer in the oil phase are needed to generate hole–shell microparticles with different shapes. Hole–shell microparticles can also be generated by gas–liquid Janus emulsions [9] or by solvent evaporation from core–shell microdroplets [43]. Still, these methods require the use of a gas or an easily vaporized substance as the inner phase, which brings in extra technical complication.
Microparticles can be functionalized for specific applications during synthesis [44]. Decorating chemical functional groups or molecules on the surface of microparticles can give them desired properties [45]. For instance, photo- and thermoresponsive microparticles synthesized by photochromic ploy (N-isopropylacrylamide-co-spironaphthoxazine methacryloyl) (PNIPA-SPO) copolymer will change their color when exposed to UV–Vis irradiation, and change their volume and color when exposed to temperature change [46]. Microparticles modified with MnO2 nanoparticles on the surface can be used as micromotors, which push themselves forward through bubbles generated by the decomposition of hydrogen peroxide catalyzed by MnO2, for wastewater treatment [47]. By adding quantum dots and Fe3O4 nanoparticles to distinct hemispherical compartments respectively, the Janus microparticles can realize fluorescent display under a magnetic field [48]. Magnetic micro-grippers synthesized by temperature-responsive hydrogel materials and Fe3O4 nanoparticles can achieve drug capture and loading and targeted release under the synergistic control of temperature and magnetic field [9].
Herein, we demonstrate a flow-pattern-altered synthesis of core–shell and hole–shell microparticles in a single axisymmetric microfluidic device, which is different from the existing works that can only synthesize one type of microparticle in the same device. Benefiting from the precise control of fluids in microfluidic capillaries, the morphology of the compound droplets can be easily tailored by tunning the flow rates. Compared with the existing methods, the present approach can continuously produce microparticles with desired structures in a relatively simple way. The resultant core–shell microparticles with adjustable hole size or magnetoresponsive microparticles doped with Fe3O4 nanoparticles could be ideal microcarriers for drug delivery.
2 Experimental section
2.1 Microfluidic device fabrication
The fabrication of the capillary microfluidic device follows the standard procedure [39, 49]. The borosilicate circular capillaries with an outer diameter of 0.96 mm and an inner diameter of 0.55 mm were pulled by a micropipette puller (P-97, Sutter Instrument Co., USA) to form capillaries with a tapered tip. The tips were scored and broken into a size of 20–200 µm with a clean 90° break technique [50] using a ceramic tile (Agilent Technologies, Inc., USA). Tips larger than 200 µm, which usually do not have a 90° break, require polishing on a sandpaper to form smooth cross-section at the final tips. The capillary microfluidic devices were fabricated by aligning two circular capillaries with different tip sizes inside a square tube with inner height of 1 mm. The circular capillary with a smaller tip size was used as the injection capillary, while another circular capillary with a larger tip size was used as the collection tube. Since the inner height of the square capillary is slightly larger than the outer diameters of the circular capillaries, it is easy to align the two circular capillaries in the square capillary. Note that the wetting condition of the capillaries plays an important role in stable and controllable generation of compound microdroplets. After being soaked in ethanol for 1 h, rinsed with deionized water, soaked again in 20% NaOH solution for 5 h, and rinsed thoroughly with deionized water, all the surfaces of the capillaries were assured to be hydrophilic. The assembling was accomplished at the stage of an inverted microscope (Nikon Eclipse Ti, Nikon Instruments, Inc., Japan). The capillaries were positioned on the glass slide using an epoxy glue (5-min Epoxy®, Devcon, Illinois Tool Works, Inc., USA). The openings of the injection capillary and the square tube were covered by syringe needles. These needles were connected to the syringe pumps (Pump 11 Elite, Harvard Apparatus, Inc., USA) through the polypropylene tubes.
2.2 Reagents
Inspired by the work of Nisisako and Hatsuzawa [51], three types of reagents were used in the present experiments—silicone oil (Sigma-Aldrich, density 0.93 g/cm3, kinematic viscosity 10 cSt, USA) as the inner phase, a photocurable solution, a monomer, 1,6-hexanediol diacrylate (HDDA, density 1.02 g/cm3, dynamic viscosity 6.27 mPa s, Ryoji, Korea), with 1.0 wt% photoinitiator 2-hydroxyl-2-methylpropiophenone (Darocur 1173, Nanjing SciChe New Materials Technology Co., Ltd., Nanjing, China) as the middle phase, and the deionized water dissolved with 1.0 wt% sodium dodecyl sulfate (SDS, Shanghai Ekear Biotechnology Co., Ltd., Shanghai, China) and 60% glycerol (Sinopharm Chemical Reagent Co., Ltd., Shanghai, China) as the outer aqueous phase. The interfacial tensions between any two phases were measured at room temperature by a tensiometer (Attension theta, Biolin Scientific Ltd., Finland). The interfacial tension σsw at the silicone oil/water interface is 13.15 mN/m, the interfacial tension σsm at the silicone oil/monomer interface is 1.89 mN/m, and the interfacial tension σmw at the monomer/water interface is 5.53 mN/m.
2.3 Generation of compound droplets and microparticles
The compound droplets were generated by delivering the three immiscible reagents through the microfluidic device using syringe pumps. As schematically illustrated in Fig. 1a, the circular capillary on the left (colored in blue) is used as the injection tube for silicone oil (inner phase, colored in yellow–orange and with volumetric flow rate of Q1). The circular capillary on the right (colored in yellow) is used as a collection tube to collect generated droplets. HDDA (middle phase, colored in red–purple and with volumetric flow rate of Q2) flows from left to right inside the gap between the outer surface of the injection capillary and the inner surface of the square tube. Aqueous phase (outer phase, colored in blue–green and with volumetric flow rate of Q3) flows from right to left inside the gap between the outer surface of the collection tube and the inner surface of the square capillary. These three phases meet at the junction between the tips of the injection and collection tubes to form a flow-focusing configuration. The generation of compound microdroplets was recorded using a high-speed charge coupled device (CCD) camera (Phantom V7.3, Vision Research, Inc., USA) and the Phantom Camera Control software (PCC 2.14, Vision Research, Inc., USA). The microdroplets were continuously photopolymerized in situ inside the collection tube by an UV light source (LC8, Hamamatsu Photonics, Shizuoka, Japan) to form microparticles. The microparticles were then collected and washed using ethanol to remove the non-curable reagents. The morphologies of the dried microparticles were examined with a scanning electron microscope (Quanta 250 FEG, FEI Company, USA). As shown in Fig. 1b, we found that the flow pattern can be changed to a way in which the two dispersed phases align parallelly at the channel junction to generate Janus microdroplets, which allows the generation of microdroplets with two totally different morphologies in a single device.
3 Results and discussion
3.1 Morphologies of compound microdroplets
The formation of the compound microdroplets is due to the instability of the fluid interfaces. Pinched or sheared by the continuous phase through the orifice of the collection tube, the dispersed phases break into microdroplets. Based on the breakup position, the formation process of the microdroplets can be classified as dripping and jetting modes. In the dripping mode, the small perturbations on the interfaces cause microdroplets to be pinched off at a fixed spatial position near the orifice of the collection tube. In the jetting mode, the perturbations are amplified along the interfaces of the jet, forming less uniform microdroplets. The transition between these two modes is strongly affected by the velocities of the three phases. Adjusting their flow rates results in three types of compound microdroplets, i.e., multiple-core, core–shell, and Janus morphologies as depicted in Fig. 2a. Compound microdroplets with multiple-core and core–shell structure, have been widely observed in the previous works [49, 52,53,54]. Their formation depends on the relationship between the breakup frequencies of the inner and middle phases [54]. When the breakup frequency of the inner phase is higher than that of the middle one, one droplet of the middle phase encapsulates several droplets of the inner phase, generating multiple-core droplets. Note that the multiple-core droplet is caused by the jetting model that is not used for particle fabrication here. Differently, the inner and middle phases break simultaneously or sequentially to form core–shell droplets. Compound microdroplets with Janus structure is due to the change in flow pattern and will be discussed in the next section. Figure 2b shows a regime diagram of three morphologies for a fixed Q3. In a wide range of Q1 (0.5–1.4 mL/h), the morphology of the compound droplets changes from Janus to core–shell and then to multiple-core as Q2 increases. When Q1 exceeds a critical value, the multiple-core morphology disappears as Q2 increases. Movies S1–S3 in the Supporting Information show the dynamic evolution of the three types of compound microdroplets.
The diameter of the compound droplet is determined by the flow rates of the three immiscible phases and the sizes of the capillary tips. We can readily adjust the flow rates or use a collection tube with a different tip to get larger or smaller compound droplets. Figure 3 displays the generation of the droplets with three morphologies in a device that has a smaller collection tip. Although the flow rate of the continuous phase is smaller than that used in Fig. 2, it can still generate smaller microdroplets. Without changing the flow rates of the inner phase and the continuous phase, the size of the compound droplets gradually decreases as the flow rate of the middle phase decreases (Fig. 3a). In fact, the size of the compound droplets also decreases if the flow rates of the inner phase or the continuous phase increase. A regime diagram of the morphologies of the compound microdroplets for a fixed Q3 can be obtained by gradually adjusting the flow rates of the inner and middle phases (Fig. 3b). The trend of the morphology evolution of the compound microdroplets is similar to that in Fig. 2b, demonstrating the robustness of the present microfluidic system.
3.2 Evolution of Janus mode
Direct generation of both core–shell and Janus microdroplets in the same microfluidic device, to the best of our knowledge, was observed in the present experiment for the first time. Besides, the transition of the compound droplet morphologies between core–shell and hole–shell can be realized by solely changing the flow pattern at the channel junction. Figure 4a shows again that, once the Janus microdroplet is generated, a large droplet of the inner phase always sticks at the upstream of the tip of the injection tube. This large droplet inclines to partially contact the outer wall of the injection tube and the inner wall of the square tube, therefore, the two dispersed phases form a side-by-side arrangement to create a triple-line at the junction of the three phases. The resulting compound droplets display the double-faced morphology, which is called the Janus mode.
To elucidate the occurrence of the Janus mode, we varied the flow rate of the inner phase to monitor how the core–shell mode transits to the Janus mode, as shown in Fig. 4b. The combination of the three flow rates is selected to be near the diagram boundary between the core–shell and Janus modes as provided in Fig. 2b. The dashed red line highlights the interfaces observed from the side view. The device initially generates core–shell droplets at t = 0 s. The flow rate of the inner phase then increases a bit to trigger the transition from the core–shell mode to the Janus one. At t = 3.0 s, the inner phase accumulates at the small orifice of the injection capillary, and the interface between the inner phase and the middle phase deforms rapidly under the action of the interfacial tension between the inner phase and middle phase. By contrast, the interface between the middle phase and the continuous phase deforms slowly because the square tube channel is much larger than the injection capillary orifice. The two interfaces approach each other but cannot directly touch each other. Since the interfacial tension between the inner phase and the middle phase is weaker than the interfacial tension between the middle phase and the continuous phase, the pressure of the inner phase cannot push the interface between the middle phase and the continuous phase to move downward. Therefore, the interface between the inner phase and the middle phase can only deforms backward. At t = 3.3 s and 3.9 s, the droplet of inner fluid continues to grow and finally occupies the cross-section of the square tube. The middle phase is solely stretched by the outer phase to form a momentary jetting mode. At t = 6.1 s, the droplet of inner fluid becomes large enough to move downwards and is stretched by the flow field. The interface between the innermost and middle phases contacts the interface between the middle and continuous phases to form a three-phase contact line. A side-by-side distribution of the inner and middle fluids thus generates compound droplets with side-by-side morphology, i.e., Janus droplets. Close observation shows that the inner and middle phases break in an alternate way. The shapes of the large droplet and the generated Janus droplets become steady at t = 12 s, suggesting the complete transition of the core–shell mode to the Janus mode.
3.3 Generation of core–shell and Janus droplets at the same flow rates
Thanks to the adhesive force experienced by the large droplet at the channel wall in the Janus mode, we can even produce compound droplets with different morphologies under the same combination of flow rates. Figure 5 shows the generation process of the compound droplets in dripping mode, under Q1 + Q2 = 0.9 mL/h and Q3 = 8 mL/h. Initially, the two interfaces do not contact with each other and the droplet of the inner phase is encapsulated inside the droplet of the middle phase. Therefore, the device generates core–shell microdroplets when Q1 = 0.1 mL/h (Q2 = 0.8 mL/h) at the beginning. As shown in the blue path, the core–shell microdroplets are generated until Q1 = 0.5 mL/h (Q2 = 0.4 mL/h), when the large droplet of the inner phase appears between the tip of the injection capillary and the inner wall of the square tube to change the flow pattern to the Janus mode. The inner phase is now connected with the inner wall of the square tube. As long as the large droplet of the inner phase keeps sticking on the capillary wall, compound microdroplets with different morphologies can be generated by decreasing Q1. With further decreasing of Q1 along the red path shown in Fig. 5, the large droplet does not disappear but its size decreases. All the droplets shown in Fig. 5 can be stably generated for a long time (at least 1 h). Note that, if the large droplet of the inner phase is flushed away by a sudden increase of Q2, the Janus mode will return to the core–shell mode again. In addition, the size of the compound microdroplets generated at such fixed combination of flow rates keeps almost the same, no matter how the ratio Q1/Q2 changes. The thickness of the shell can be precisely controlled by varying Q1/Q2. Consequently, if the total flow rate of the two dispersed phases and the flow rate of the continuous phase are fixed, we can obtain the compound microdroplets with uniform size and different morphology.
3.4 Fabrication of core–shell and hole–shell microparticles
Microparticles were fabricated by photopolymerizing the UV-curable phase in the compound droplets in situ inside the collection tube by UV irradiation, as shown schematically in Fig. 1. Briefly, the UV light causes the initiator molecules to homolytic cleavage forming benzoyl radicals, which then react with monomer molecules by taking a π electron from the C=C bond at the end of the monomer molecule to form a C–C bond [41]. The remaining unpaired π electron on the C atom of the monomer molecules makes the entire monomer molecule into another radical. The size and morphology of the resulting microparticles are controlled by the compound microdroplets, i.e., core–shell droplets for core–shell particles and Janus droplets for hole–shell particles. It should be noted that the hole–shell microparticles were fabricated by in situ curing the compound microdroplets that have not yet been able to evolve to the final equilibrium morphology, which is determined by the minimization of the interfacial free energies. The collected microparticles were washed with the absolute ethanol for several times to clean off the silicone oil and glycerin–water solution remaining on the particle surface (schematically shown in Fig. 6). Figure 6a shows the scanning electron microscope (SEM) image of the core–shell microparticles, one of which was stabbed to show the encapsulation of the silicone oil and the core–shell morphology. Figure 6b shows the SEM image of hole–shell microparticles fabricated from Janus microdroplets. These SEM images confirm that the sizes and shapes of the synthesized microparticles are highly uniform.
3.5 Controlling the hole size of microparticle
Janus microdroplets are spherical immediately after their formation since the balancing of the three interfaces at the triple-line cannot reach the steady state yet. Cured by UV light in situ, the generated hole–shell microparticles then have nearly spherical shape. The holes in the shell can facilitate mass transport through the shell for selectively capturing particles for classification and separation [42], confined synthesis of functional materials [42], and controlled release of molecules and nanoparticles [27]. The size of the hole also plays an important role in controlling the kinetics of drug release [25]. Here we further explored the possibility to tune the hole size. As demonstrated in the previous part, we can always change the shell thickness of the droplets while keep the size of droplets at the same time. Figure 7a, b shows the Janus droplets and the corresponding synthesized hole–shell microparticles generated under the same Q3, as well as the same sum of Q1 and Q2. When the ratio of Q1/Q2 is changed from 1:2 to 2:1, the hole size becomes larger. We measured the holes and diameters of these microparticles and found that the sizes of hole differ significantly (145 μm vs. 200 μm) while the diameters of particles are very close (210 μm vs. 225 μm).
We prepared a series of microparticles under Q1 + Q2 = 1 mL/h and Q3 = 9 mL/h. Figure 7c shows that the opening of microparticles increases with Q1 and the morphology of the microparticles gradually change from hole–shell to crescent-moon shape. The measurements in Fig. 7d confirm that the hole size increases monotonically while the shell diameter keeps about 225 ± 7 µm. To show the monodispersity of the generated microparticles, Fig. 7e gives the distribution of the shell diameters of the microparticles generated under Q1 = 0.3 mL/h and Q2 = 0.7 mL/h. The small coefficient of variation (CV) of 1.5% confirms that the present capillary microfluidic device can produce highly monodisperse microparticles.
3.6 Magnetic response of hole–shell microparticles
By adding magnetic Fe3O4 nanoparticles into the monomer solution, we synthesized magnetoresponsive hole–shell microparticles from Janus droplets. Figure 8 shows the orientations of two types of hole–shell microparticles without and with the external magnetic field in the ethanol solution, respectively. Figure 8a1 shows that, in the absence of a magnetic field, the holes of the hole–shell microparticles generated under Q1/Q2 = 1 face upward in the solution because of the uneven distribution of the magnetic nanoparticles in the asymmetrical structure. Here the hole of the microparticle acts as the head of a roly-poly toy. When subjected to a magnetic field, the holes of the microparticles rotate to the opposite direction of the magnetic field, as shown in Fig. 8a2. After removing the external magnetic field, these roly-poly toys put themselves right again. For microparticles with smaller holes in Fig. 8b, we also observed a swift response of hole–shell microparticles to the external magnetic field. An animation of the hole–shell particles rotating under a rotating magnetic field is provided in the Supporting Information (Movie S4). These microparticles can be loaded with drug molecules or small drug particles after being immersed in an aqueous solution of drug and treated by ultrasonic vibration [27, 42]. Guided by a magnetic field, the magnetoresponsive motion of these microparticle could be used for targeted drug delivery.
4 Conclusions
This work describes an axisymmetric flow-focusing capillary microfluidic device that can produce either core–shell microparticles or hole–shell ones by only tunning the flow rates. The versatility of the device allowed the easy adjustment of the morphologies of the compound droplets and thus the structures of the resultant microparticles. We characterized the physical mechanism triggering the transition from the core–shell model to the Janus model. Different from the well-studied core–shell microdroplets, Janus microdroplets were formed with the presence of a large droplet of the inner phase near the entrance of the collecting capillary, causing two dispersed phases to align parallelly at the entrance. The hole–shell microparticles with nearly constant shell diameter but varied hole sizes were readily generated by adjusting the flow rates. In addition, the introduction of magnetic nanoparticles endowed the resultant microparticles with ability to move rotationally or translationally under external magnetic fields. This robust method that only controls the flow rates in a single microfluidic device could facilitate the fabrication of microparticles as ideal microcarriers for controlled drug delivery.
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Acknowledgments
This work was supported by the National Natural Science Foundation of China (Grants 11832017, 11772343, and 12072350), the Chinese Academy of Sciences Key Research Program of Frontier Sciences (Grant QYZDB-SSW-JSC036), the Chinese Academy of Sciences Strategic Priority Research Program (Grant XDB22040403), and the Beijing Institute of Technology Research Fund Program for Young Scholars.
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Wang, D., Zheng, X., Chen, X. et al. Flow-pattern-altered syntheses of core–shell and hole–shell microparticles in an axisymmetric microfluidic device. Acta Mech. Sin. 37, 1378–1386 (2021). https://doi.org/10.1007/s10409-021-01096-w
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DOI: https://doi.org/10.1007/s10409-021-01096-w