WO1999039120A1 - Commande de fluide par expansion thermique de dispositifs microfluidiques - Google Patents

Commande de fluide par expansion thermique de dispositifs microfluidiques Download PDF

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Publication number
WO1999039120A1
WO1999039120A1 PCT/US1999/001831 US9901831W WO9939120A1 WO 1999039120 A1 WO1999039120 A1 WO 1999039120A1 US 9901831 W US9901831 W US 9901831W WO 9939120 A1 WO9939120 A1 WO 9939120A1
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Prior art keywords
fluid
reservoir
flow
heating
sample
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PCT/US1999/001831
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English (en)
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WO1999039120B1 (fr
Inventor
James P. Landers
Andreas Huhmer
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University Of Pittsburgh
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Priority claimed from US09/015,278 external-priority patent/US6210882B1/en
Application filed by University Of Pittsburgh filed Critical University Of Pittsburgh
Priority to AU23477/99A priority Critical patent/AU2347799A/en
Publication of WO1999039120A1 publication Critical patent/WO1999039120A1/fr
Publication of WO1999039120B1 publication Critical patent/WO1999039120B1/fr

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    • FMECHANICAL ENGINEERING; LIGHTING; HEATING; WEAPONS; BLASTING
    • F16ENGINEERING ELEMENTS AND UNITS; GENERAL MEASURES FOR PRODUCING AND MAINTAINING EFFECTIVE FUNCTIONING OF MACHINES OR INSTALLATIONS; THERMAL INSULATION IN GENERAL
    • F16KVALVES; TAPS; COCKS; ACTUATING-FLOATS; DEVICES FOR VENTING OR AERATING
    • F16K13/00Other constructional types of cut-off apparatus; Arrangements for cutting-off
    • F16K13/08Arrangements for cutting-off not used
    • F16K13/10Arrangements for cutting-off not used by means of liquid or granular medium
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L3/00Containers or dishes for laboratory use, e.g. laboratory glassware; Droppers
    • B01L3/50Containers for the purpose of retaining a material to be analysed, e.g. test tubes
    • B01L3/502Containers for the purpose of retaining a material to be analysed, e.g. test tubes with fluid transport, e.g. in multi-compartment structures
    • B01L3/5027Containers for the purpose of retaining a material to be analysed, e.g. test tubes with fluid transport, e.g. in multi-compartment structures by integrated microfluidic structures, i.e. dimensions of channels and chambers are such that surface tension forces are important, e.g. lab-on-a-chip
    • B01L3/50273Containers for the purpose of retaining a material to be analysed, e.g. test tubes with fluid transport, e.g. in multi-compartment structures by integrated microfluidic structures, i.e. dimensions of channels and chambers are such that surface tension forces are important, e.g. lab-on-a-chip characterised by the means or forces applied to move the fluids
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L2300/00Additional constructional details
    • B01L2300/18Means for temperature control
    • B01L2300/1861Means for temperature control using radiation
    • B01L2300/1872Infrared light

Definitions

  • the present invention is an improvement of a commonly assigned patent application, Landers, J.P. Rapid Thermocycling For Sample Analysis. U.S. Serial No. 09/015,278, filed January 29, 1998, incorporated in its entirety by reference herein.
  • the present invention relates to methods and apparatus for performing precise manipulation of picoliter-nanoliter volumes in microfluidic chips.
  • This technique specifically relies on thermal induced hydrodynamic pressure, wherein the thermal expansion of fluids controls the flow and pressure of fluids in microfluidic chip devices.
  • thermal expansion-induced fluid pumping mechanism Several applications for fluid control and manipulation on microfluidic chips are proposed using the thermal expansion-induced fluid pumping mechanism.
  • microfabricated structures for total chemical analysis embodies a design wherein the total analysis of complex samples is carried out in a completely integrated "chip".
  • the ⁇ TAS or "Laboratory-on-a-Chip” concept involves miniaturization of benchtop analytical procedures into microfluidic chips roughly the size of a double-wide microscope slide ( ⁇ 100 mm. x 100 mm x 0.5 mm).
  • the improvement in functionality is driven by the basic concept that an overall reduction in the dimensions of fluid volume, handling and flow should result in the enhancement of analytical performance.
  • Harrison, D.J. Flurri, K.; Seiler, K.; Fan, Z.; Effenhauser, C.S.; Manz, A.
  • the chip architecture is composed of microfluidic channels and other three- dimensional structures on a suitable substrate (glass, plastics, etc.) with microchannel dimensions in the micrometer range and reservoir dimensions in the millimeter range.
  • the compact design and production of these devices allow for some standard liquid separation methods, like capillary electrophoresis, to be miniaturized into a format that is roughly 10-times smaller in size than conventional systems and allows for separations to be carried out roughly an order of magnitude faster.
  • U.S. Patent No. 5,770,029 discloses an electrophoretic microdevice for use in a variety of electrophoretic applications, including clinical assays. Despite the fact that rapid, microscalar analyses are possible with microfluidic chips, the potential of this platform lies in integrating other chemistries and sample manipulation processes into the very same chip used for electrophoretic analysis.
  • a prerequisite for the development of a functional microfluidic chip is the ability to precisely manipulate liquids and control their movement through the complex architecture of the microfluidic system.
  • electrokinetic phenomena e.g., electrophoretic and electroosmotic effects
  • hydrostatic pressure e.g., hydrostatic pressure
  • Electroosomotic flow relies on the surface charge of the channel, the ionic strength of the solution and the strength of an electric potential applied across the solution. For example, U.S.
  • Patent number 5,755,942 describes a system for processing a plurality of reactions comprising a sample channel for moving samples into a microlaboratory array wherein the control of samples having features that diffract light at various wavelengths are optically monitored by a device that can electrokinetically control the flow of the sample.
  • U. S. Patent No. 4,908,112 discloses a silicon semiconductor wafer for analyzing biological samples by directing the motion of liquids through the wafer by electroosmosis.
  • Elaborate electrokinetic injection schemes on microfluidic chips have been developed for either sample injection in a continuously proportional mode or injection with a fixed plug length using switching potentials between reservoirs. Seiler, K.;Fan, Z.H.; Flurri, K.; Harrison, D.J.
  • Electroosmotic Pumping and Valveless Control of Fluid Flow within a Manifold of Capillaries on a Glass Chip Anal. Chem. 1994, 66, 3485.
  • the combination of the compact, virtually dead volume- free design of the microchip devices and the electrokinetic control of picoliter volumes with high precision are the hallmark of the highly reproducible manipulation of fluids in microfluidic devices.
  • this technique is limited to solutions whose chemical composition allow for electroosmotic flow, e.g., low ionic strength solutions.
  • Many solutions, such as chaotropic agents or biological fluids where the ionic strength is high suppress the electroosmotic effect and, therefore, may not provide adequate electroosmotic flow and/or cannot be controlled precisely through voltage switching.
  • Fluid flow based on hydrostatic pressure is also utilized in capillary electrophoresis (CE) for sample injection and for rinsing the capillary between electrophoretic separations.
  • CE capillary electrophoresis
  • pressure driven pumping of fluids suitable for microfluidic devices is easily controlled by mechanical means, e.g., through valves.
  • hydrodynamic pressures 5-80 psi
  • Variations in the pressure of a central pressurized gas/air supply causes problems in miniaturized systems not encountered in the "macroworld" of capillary electrophoresis.
  • a reliable and practical interface for the plumbing from an external pressure source to the microfluidic chip constitutes a considerable challenge that is not easily solved. Therefore, there is a need for a hydrodynamically-driven fluid pumping technique for microfluidic devices.
  • U.S. Patent No. 5,375,979 discloses a method for creating hydrodynamic pressure on a microstructure, including a thermal micropump having a working chamber, intake valve and discharge valve.
  • the pump action of the micropump is achieved through a succession of overpressure and partial-vacuum cycles through a succession of heating and cooling steps of gas.
  • This micropump has a disadvantage of being quite complex, and presents valves tending to experience high leakage rates, and is of questionable functionality. Burns, M.A., Mastrangelo, C.H., Sammarco, T.S., Man, F.P., Webster, J.R. Johnson,
  • U.S. Patent No. 5,639,423 discloses the use of Lamb-wave pumps to effect fluid flow in a microfluidic device. Such pumps, however, are very difficult to control, given the transducers used are operational only at a narrow band of alternating voltage frequencies corresponding with the resonant frequency of the transducer. Furthermore, fluid control is not continuous over a wide range of flow rates. Lamb-wave pumps also are difficult to fabricate, occupy a relatively large amount of area on the chip, and require mechanical components, which are prone to wear/fatigue. Accordingly, an advance in the art would be achieved with a method and apparatus for the generation and precise control of hydrodynamic pressure for fluid manipulation in microfluidic devices without the use of an external pressure source or the need to rely on electroosmotic flow or Lamb-wave pumps.
  • the present invention meets the need for an effective hydrodynamic fluid flow based source that does not require an external pressure source or electroosmotic flow, providing methods and apparatus for accurate control of fluid flow in microfluidic devices.
  • the invention allows the provision of methods and apparatus comprising microfabricated structures for microscale total analysis systems.
  • This invention discloses a method for precisely manipulating liquids and controlling their movement through microfluidic systems in a manner that is not only noncontact, but also independent of solution ionic strength and surface charge. This method, referred to herein as thermal expansion-induced fluid pumping, precisely controls movement of small volumes
  • VIS/IR-induced fluid pumping means the pumping of fluids, in a microfluidic system, through use of a heat source not in contact with the system, which heat source, when directed toward the fluid of interest, causes that fluid to expand through thermal expansion, the heat source including light energy in the visible and infra-red range.
  • thermal expansion-induced fluid pumping includes VIS/IR-induced fluid pumping, and further includes other mechanisms for heating fluids on a microfluidic chip to achieve thermal expansion of the fluid, including other wavelengths of light, e.g., UV, and other heating methods such as providing thin heating films on the chip, and heating the fluid with heated forced air.
  • microfluidic chip is intended to include, but is not necessarily limited to, devices which have been microfabricated to contain one or more structural elements, such as channels, reaction chambers, etc., with minimal dimensions ranging from tens of microns (the dimensions of biological cells) to nanometers (the dimensions of some biological macromolecules), i.e., “mesoscale,” and even smaller.
  • the term “mesoscale” is used herein to define chambers and flow passages having a cross sectional dimension on the order of 0.1 ⁇ m to 500 ⁇ m.
  • microfluidic chip is further intended to include, but not necessarily be limited to, microfabricated devices which perform microscale and/or mesoscale chemical reactions including precise control of parameters of the reaction; the parameters controlled by such devices may include, e.g., temperature, pressure, concentration of reactants, the intensity or frequency of incident light, electromagnetic fields, ultrasonic pressure waves, etc.
  • the liquid expands and applies pressure to the walls of the reservoir and subsequently exits through its only outlet, a microchannel at the base of the reservoir, creating a constant flow of fluid through the channel.
  • the heat source be provided remotely, for example, by a halogen lamp that specifically heats the fluid through absorption of VIS/IR optical energy.
  • the rate and extent of fluid expansion is a function of the rate and the extent of temperature change, which is easily controlled by monitoring the temperature of the liquid.
  • a further object within the invention is to use an organic liquid with a high thermal expansion coefficient and that is immiscible with aqueous solutions.
  • toluene has a thermal expansion coefficient that is approximately 5 -times larger than an aqueous solution.
  • the internal pressure (at constant volume) generated due to the expansion of the heated organic liquid can be estimated from thermodynamics to be several atmospheres with several degrees change in temperature in the reservoir. This expansion can be effectively transferred to the aqueous solution in order to achieve higher flow rates of that aqueous solution that would be impossible by heating the aqueous solution alone.
  • this invention discloses a system that can precisely control the flow of small volumes in microfluidic devices using thermal expansion-induced fluid pumping.
  • the system of using thermal expansion-induced fluid pumping can be utilized in chemical reaction systems for synthesis or processing of organic, inorganic, or biochemical reactions and separations.
  • Figure 1 is an illustration of the microchannel configuration for a microchip designed to use thermal-induced fluid pumping according to one embodiment of the present invention.
  • Figure 2 is an illustration of a microfluidic pump designed to use thermal-induced fluid pumping according to one embodiment of the present invention.
  • Figure 3 is an illustration of a microfluidic valve designed to use thermal-induced fluid pumping according to one embodiment of the present invention.
  • Figure 4 is an illustration of a thermoreservoir connected to a plurality of liquid reservoirs designed to use thermal-induced fluid pumping according to one embodiment of the present invention.
  • Figure 5 is an example of how the thermoreservoir in concert with valves designed to use VIS/IR induced fluid pumping can continuously pump fluid in a microfluidic device.
  • Figure 6A illustrates temperature versus time in ten thermocycles achieved with heating according to the present invention.
  • FIG 6B illustrates temperature versus time as measured in the heating/cooling block of a conventional thermocycling instrument.
  • Electrophoretic "chips" consist of glass, plastic, silicon, or gallimarsenide substrates into which a pattern of microchannels, often simple but sometimes complicated, have been fabricated. Embodiments of such chips are shown in Figure 1.
  • the microchannels terminate at reservoirs which are often drilled holes in the structure itself and which hold volumes as low as a few microliters to as much as several hundred microliters. These reservoirs may also be prepared using known techniques, such as photolithography and etching.
  • Other microfabrication technologies include, but are not limited to sputtering, electrodeposition, and low-pressure vapor deposition.
  • crystalline materials such as silicon or gallium arsenide as substrates for microfabricated devices offer certain advantages over non- crystalline materials such as glass.
  • Crystalline semiconductor materials provide etched surfaces comprising crystal planes, the shapes and dimensions of which can be precisely controlled. Further, crystalline materials may be bonded by processes such as fusion at elevated temperatures, or with a field assisted method such as Mallory bonding. Semiconductors offer the further advantage of permitting electronic circuiting to be integrated with the microfabricated device using conventional IC fabrication techniques.
  • MicroChannel structures on electrophoretic chips are typically in the micrometer range, with depths ranging from 10-50 ⁇ m and widths from 30-100 ⁇ m.
  • a microchannel with the dimensions of 10 ⁇ m (deep) x 50 ⁇ m (wide) x 3 mm long has a total microchannel volume of 1.5 nanoliters (nL). Therefore, to flow the equivalent of 20 microchannel volumes of a given solution through this particular microchannel would require the pumping of 30 nL of solution.
  • the controlled flow of these ultralow volumes through the microchannels of microfabricated electrophoretic devices may be difficult to regulate with hydrostatic pressure.
  • the low volume pumping of solution on chips is more conducive to EOF which can be controlled quite accurately by the magnitude of the voltage applied.
  • a limitation associated with EO-driven flow is its dependence on two parameters: 1) the ionic strength of the constituents of the solution being pumped; and 2) the chemical composition of the microchannel wall.
  • a low, negligible EOF is likely to result when using solutions containing a large salt concentration, such as 100 mM NaCl or 2X Tris-borate- EDTA (TBE) solutions.
  • TBE Tris-borate- EDTA
  • the present invention overcomes these limitations in the art.
  • the ability to do accurate temperature cycling on localized volumes of solution ranging from as low as a few microliters to up to several hundred microliters, such as through the methods and apparatus taught herein, can be exploited for accurate pumping of small volumes (nL- ⁇ L) of solution through microchannel structures.
  • the basis for the pumping is thermal expansion of liquids. In a confined space, a change of 100°C can result, for example, in the generation of up to 10 psi within the chamber; if the only exit from the chamber is a microchannel, fluid can be forced from the chamber through the microchannel.
  • the flow rate can be controlled very accurately by changes in temperature as little as 1-2°C.
  • the relative accuracy of the pumping is a function of the accuracy of the temperature control, e.g., precisely raising the temperature of the fluid from a first temperature to a second temperature in a precisely controlled time-frame.
  • the absolute accuracy of the pumping operation e.g., how accurately the quantity of fluid being pumped is controlled is a function of the temperature control, channel geometry and liquid properties (e.g., homogeneous versus non-homogeneous).
  • the microdevice can be specifically designed to meet the desired pumping requirements.
  • the present invention is a microfluidic device that employs a thermal expansion- induced fluid pumping mechanism.
  • the system of employing thermal expansion-induced fluid pumping in microfluidic devices provides precise fluid control, that is more effective than the methods of controlling fluid flow in microfluidic devices as described in the prior art.
  • This system can be used in an array for a high-throughput microreaction unit.
  • Applications of the thermal expansion-induced microfluidic method are numerous and can generally encompass any analytical system that can be employed at a nano- to pico-liter scale.
  • reagents can be utilized in a reaction on such a device where they are contained in reservoirs that are interconnected to one another on the microfluidic device, and the addition of each reagent into a reaction chamber can be precisely controlled in order to successfully produce the desired product.
  • the microfluidic device can be used to chromatographically separate samples, spectrophotometrically detect the samples as well as collect the separated samples. This invention essentially discloses a concept applicable to developing microfabricated structures for total chemical analysis on a microscale.
  • Fluid flow according to the present invention is achieved by heating fluid contained in a sealed reservoir, causing the fluid to expand through one or more microchannels. This fluid flow can be reversed by cooling the fluid remaining in the reservoir, which causes the fluid to contract.
  • the heating and cooling of fluid contained in the fluid reservoir is accomplished remotely, i.e., using heating/cooling sources that do not directly contact the microfluidic chip or the reservoir.
  • the reservoir is remotely heated preferably using a radiation source, the wavelength of which matches the absorbance properties of the fluid in question, the intensity and focus of which can be precisely controlled to effect the desired amount of heating of the fluid in the reservoir.
  • select optical energy sources allows for heating primarily the fluid itself, rather than the container or microfluidic chip and other structural components.
  • IR-mediated heating is primarily achieved through the absorbance of radiation by molecules in the fluid sample, for example, water molecules in the sample being pumped.
  • other heating sources to induce thermal expansion and flow of the fluid of interest can also be used, and include, for example, heating coils, lasers, and heated forced air. See also U.S. Patent No. 5,589,136 (Northrup), which discloses the use of doped polysilicon for heating a reaction chamber and bulk silicon for convection cooling.
  • any heat or light source the energy from which can be manipulated by optical filters and/or lenses to effect absorbance of such energy by the fluid of interest in order to heat the fluid can be used.
  • a suitable reservoir according to the methods of the present invention is one in which extremely low volumes of sample can be effectively heated and cooled, including sample volumes in the nanoliter range.
  • the reservoir must be made of a material that allows the penetration of the desired wavelengths of light, such materials including by way of example but not limitation quartz glass, glass, silicon, transparent plastics, and the like.
  • the reservoir or container will have a high surface-to-volume ratio.
  • a high surface-to-volume ratio leads to a decrease in the thermal time constant, which can lead to an increase in the efficiency of heating and cooling cycles.
  • a high surface-to-volume ratio, while not as important for the heating step is related to the effectiveness of the cooling step.
  • suitable reservoirs include but are not limited to, microchambers, capillary tubes, and microchips.
  • a preferred example of a suitable reservoir is a microchamber made from thin- walled glass.
  • Another preferred embodiment is a glass capillary tube.
  • Such capillaries are typically used in capillary electrophoresis ("CE").
  • Suitable inner diameters of the capillaries having an outer diameter of about 370 ⁇ m typically vary between about 15 ⁇ m and 150 ⁇ m. Thermal gradients that lead to convection are substantially reduced in capillary tubes.
  • Glass capillary tubes are commercially available from Polymicron Technologies, Phoenix, AZ.
  • a suitable reservoir is the channel structure incorporated into a microfabricated device, such as the microfabricated substrate described by Wilding and co-workers in Nucleic Acids Res., 24:380-385 (1996).
  • a microfabricated device such as the microfabricated substrate described by Wilding and co-workers in Nucleic Acids Res., 24:380-385 (1996).
  • Any other reservoir can be used according to the methods of the present invention, provided that the vessel is made of a material which allows IR or other radiation to directly heat the sample. Further guidance in preparing such microfabricated devices is provided, for example, in U.S. Patent Nos. 5,250,263; 5,296,1 14; Harrison et al., Science 261 :895-897 (1993); and McCormick et al., Anal. Chem., 69:2626-2630 (1997), incorporated by reference herein.
  • Heating of the fluid is preferably accomplished through the use of optical energy from a noncontact heat source. While contact heating sources can also be used in accordance with the present invention, they are less preferred, as they are not as quickly or precisely able to effect fluid heating and allow for cooling as the non-contact sources.
  • the wavelength of the radiation source must match the absorbance properties of the fluid being heated in order to maximize heating effects on the fluid by the radiation. Wavelengths in the near infrared region are preferred, given that nearly everything shows absorbance in that region.
  • this optical energy is derived from an IR light source which emits light in the wavelengths known to heat water, which is typically in the wavelength range from about 0.775 ⁇ m to 7000 ⁇ m.
  • the infrared activity absorption bands of seawater are 1.6, 2.1, 3.0, 4.7 and 6. 9 ⁇ m with an absolute maximum for the absorption coefficient for water at around 3 ⁇ m.
  • the optical energy should be of a wavelength that matches the absorbance properties of the organic liquid.
  • the IR wavelengths are directed to the vessel containing the sample, and because the vessel is made of a clear or translucent material, the IR waves act directly upon the sample to cause heating of the sample. Although some heating of the sample might be the result of the reservoir itself absorbing the irradiation of the IR light, (particularly with silicon substrates) heating of the sample is primarily caused by the direct action of the IR wavelengths on the sample itself.
  • IR and near-IR wavelengths will be preferred for many applications, in certain instances visible and even UV wavelengths may be used, depending on the nature of the fluid and its absorbance characteristics.
  • Heating and fluid expansion and flow can be effected in either one step, or numerous steps, depending on the desired application. For example, a particular methodology might require that the sample be heated to a first temperature, allowing a first fluid expansion and flow to occur, maintained at that temperature for a given dwell time, then heated to a higher temperature, allowing a second fluid expansion and flow to occur, and so on. As many heating steps as necessary can be included. Similarly, continuous heating, whereby the temperature of the fluid is continuously and uniformly raised, may be used to provide continuous fluid flow over finite temperature ranges for limited heating cycle times.
  • cooling to a desired temperature can be effected in one step, or in stepwise reductions with a suitable dwell time at each temperature step, or over a continuous cooling step for limited times and temperature ranges.
  • Positive cooling is preferably effected by use of a non-contact air source that forces air at or across the reservoir.
  • this air source is a compressed air source, although other sources could also be used. It will be understood by those skilled in the art that positive cooling results in a more rapid cooling than simply allowing the vessel to cool to the desired temperature by heat dissipation. Cooling can be accelerated by contacting the reservoir with a heat sink comprising a larger surface than the reservoir itself; the heat sink is cooled through the non-contact cooling source.
  • the cooling effect can also be more rapid if the gas from the non-contact cooling source is at a lower temperature than ambient temperature. This can be accomplished in any number of ways, including using chilled air, nitrogen, etc., or forced air directed at the chip. Cooling can also be accomplished, of course, by removing the energy (heat) source or changing its wavelength to one of lower absorbance for the fluid being heated.
  • Figure 6A shows a plot of temperature versus time (seconds) in ten thermocycles run according to the present invention, in which two temperature stages are achieved.
  • the amount of time that elapses between the highest temperature is very small, with the temperature change being effected in less than 1 second.
  • the change from the lowest temperature back to the highest temperature takes generally less than one second, and can be done as quickly as 300 to 400 milliseconds. This rapid temperature change translates into fast response times for initiating and halting pumping and valving operations using the present-invention.
  • Figure 6B is representative of a typical temperature profile for one three-temperature thermocycle obtained from a commercially available thermocycling instrument.
  • the dotted line represents the temperature of the heating/cooling block of the apparatus, and the solid line the temperature of the sample. It can be seen that the time lags between the temperatures - the highest to lowest temperature about 30 seconds, the lowest to intermediate temperature about 15 seconds, and the intermediate to highest temperature about 25 seconds - is sufficiently longer than that achieved by the methods and apparatus of the present invention. Such long time lags would render the prior art device impractical for pumping or valving fluids in microfluidic chip applications. Desired temperature changes in the sample itself take even longer to achieve. The temperature transitions in the sample are not nearly as sharp as those obtained in the block, or those in the sample according to the present methods.
  • the temperature transition of the sample from the highest to lowest temperature takes about 100 seconds, and from the intermediate to highest temperature about 80 seconds.
  • This time lag becomes important in certain processes where rapid changes in fluid flow are desired, for example, when using the present invention as a chemical valve.
  • the lower temperature points may be viewed as an open valve scenario, which, according to the present invention, may be quickly closed by heating the valving fluid to the higher temperature.
  • the non-contact means for directly heating the sample can be any means known in the art for generating the desired range of wavelengths in the near IR wavelengths.
  • the heating means will be an IR source, such as an IR lamp, an IR diode laser or an IR laser.
  • An IR lamp is preferred, as it is inexpensive and easy to use.
  • Preferred IR lamps are halogen lamps and tungsten filament lamps. Halogen and tungsten filament lamps are powerful, and can heat several samples flowing in parallel.
  • a tungsten lamp has the advantages of being simple to use and inexpensive, and almost instantaneously (90% lumen efficiency in 100 msec) reach very high temperatures.
  • Such lamps are commercially available from General Electric, Cleveland, OH.
  • a particularly preferred lamp is the CXR, 8V, 50W tungsten lamp available from General Electric. This lamp is inexpensive and convenient to use, because it typically has all the optics necessary to focus the IR radiation onto the sample; no expensive lens system/optics will typically be required.
  • the IR source is positioned remotely (non-contact) from the sample, such that light emanating from the lamp impinges the sample.
  • the lamp is positioned remotely to the actual sample, and the radiation from the lamp is transferred via optically IR- transmissible fiberglass or through a combination of lenses and mirrors.
  • optical fibers the ends of the fibers are mounted in a platform such that they are close to, (e.g., a few millimeters or less) but do not touch, the chip.
  • the chip is slid into position on the platform, which maintains consistent orientation from chip to chip relative to the IR source.
  • Other embodiments in which the sample is placed in the path of the IR light source are equally within the scope of the present invention.
  • the heat source can be manipulated, such as through the use of lenses and filters mounted between the lamp and the reaction vessel. Such lenses and filters serve to focus the radiation as well as to eliminate wavelengths that could interfere with the fluid expansion taking place and/or the temperature sensing. Filtering and focusing of the IR light using, for example, IR transmissible lenses or filters is preferred, as this reduces the occurrence of temperature gradients in the sample or partial boiling of the sample.
  • the term "direct” or "directly” when used in reference to heating means that the sample itself is heated by the heating source, such as through absorption of IR radiation, as opposed to heating of the vessel containing the sample which in turn heats the sample. Direct heating of the sample is, therefore, achieved even when lenses, filters and the like are used.
  • non-contact with respect to an energy source, means that the energy source is directed at, or focused on, a region of the microfluidic chip desired to be heated, and may be quite close to that region, but does not physically touch it.
  • the term "remote" with respect to an energy source includes non- contact sources, but also includes truly remote sources of energy, which are not themselves near or focused at the microfluidic chip, but are brought to bear on the microfluidic chip by some intermediary, such as optical fibers, which transmit the energy from the remote heat source to the region of interest on the microfluidic chip.
  • the apparatus of the present invention uses finely tuned temperature ramping, which allows for rapid heating cycles of the sample.
  • heat transfer problems frequently encountered with solid block heaters are eliminated with the non-contact approach of the present invention.
  • the heater can be powered by any means, such as a low voltage power supply. Preferred is a 5 volt DC supply system, although it will be understood that any other suitable means can also be employed.
  • Cooling can be achieved by any non-contact means known in the art for positively cooling an object. Accordingly, the non-contact cooling source should also be positioned remotely to the sample or reaction vessel, while being close enough to effect the desired level of heat dissipation. Both the heating and cooling sources should be positioned so as to cover the largest possible surface area on the sample vessel.
  • the heating and cooling sources can be alternatively activated to control the temperature of the sample. It will be understood that more than one cooling source can be used.
  • the cooling means can be used alone or in conjunction with a heat sink.
  • a particularly preferred cooling source is a compressed air source. Compressed air is directed at the reservoir when cooling of the sample is desired through use, for example, of a solenoid valve which regulates the flow of compressed air at or across the sample.
  • the pressure of the air leaving the compressed air source can have a pressure of anywhere between 10 and 60 psi, for example. Higher or lower pressures could also be used.
  • the temperature of the air can be adjusted to achieve the optimum performance in the cooling process.
  • a means for monitoring the temperature of the sample, and a means for controlling the heating and cooling of the sample are preferably also provided.
  • monitoring and controlling is accomplished by use of a microprocessor or computer programmed to monitor temperature and regulate or change temperature.
  • An example of such a program is the Labview program, available from National Instruments, Austin, Texas. Feedback from a temperature sensing device, such as a thermocouple, is sent to the computer.
  • Other temperature sensing devices such as resistive heaters (RTD's or Resistive Temperature Devices), can also be used.
  • Such heaters may be bonded to the chip, and used to measure temperature by measuring electrical resistance through the heater. See generally Burns, et al., Microfabricated Structures for Integrated DNA Analysis, Proc. Nat. Acad. Sci., USA Vol. 93 pp. 5556-5561 (1996).
  • the temperature sensing device provides an electrical input signal to the computer or other controller, which signal corresponds to the temperature of the sample.
  • the rate of heating/cooling of the fluid in the reservoir can be used to determine the rate of fluid expansion/contraction and hence the flow rate of fluid from the reservoir into the microchannels.
  • the temperature sensor which can be coated or uncoated, can be placed in a temperature sensing reservoir placed adjacent to the fluid reservoir containing the sample to be pumped.
  • the temperature sensing reservoir should be of the same type as the sample fluid reservoir, only containing a blank, such as water or a buffer solution instead of sample.
  • the thermocouple can be placed directly into the sample fluid reservoir, provided that the thermocouple does not interfere with or affect the heating/cooling of the fluid, and provided that the thermocouple used does not act as a heat sink.
  • a suitable thermocouple for use with the present invention is constantan-copper thermocouple.
  • microfabrication sensors p/n-junctions
  • Other temperature sensing methods that comprise non-contact temperature sensing devices are: optical pyrometers, primary acoustic thermometers, or spectroscopic techniques for measuring temperature of liquids.
  • Signals from the computer control and regulate the heating and cooling means, such as through one or more switches and/or valves.
  • the desired temperature profile is programmed into the computer, which is operatively associated with heating and cooling means so as to control heating and cooling of the sample based upon feedback from the thermocouple and the predetermined temperature profile.
  • the optical energy is focused on the sample by means of IR transmissible lenses so that the sample is homogeneously irradiated.
  • This technique avoids "hotspots" that could otherwise result in the creation of undesirable temperature differences and/or gradients, or the partial boiling of the sample.
  • the homogeneous treatment ot the sample vessel with optical energy therefore contributes to a sharper temperature profile and more uniform and reproducible fluid expansion.
  • the homogenous sample irradiation can further be enhanced through the use of a mirror placed on the opposite site of the IR source, such that the reservoir is placed between the IR source and the mirror. This arrangement reflects the radiation back onto the sample and substantially reduces thermal gradients in the sample.
  • the radiation can be delivered by optical IR-transparent fiberglass, for example, optical fiberglass made from waterfree quartz glass (Fasertyp IR-QQ, Schott Glatechnike Weisbaden, Germany) that is positioned around the reservoir and that provides optimal irradiation of the sample.
  • optical IR-transparent fiberglass for example, optical fiberglass made from waterfree quartz glass (Fasertyp IR-QQ, Schott Glatechnike Weisbaden, Germany) that is positioned around the reservoir and that provides optimal irradiation of the sample.
  • FIG 1 there is illustrated an example of one possible embodiment of the invention, in this case a microfluidic device designed to perform microscale total chemical analysis on a microfluidic device. It will be appreciated that this is an illustrative example only of a preferred application of the invention, and a wide array of other uses of the invention is possible.
  • the sample to be analyzed is placed in a sample loading reservoir 4 in the microfluidic device.
  • the sample loading reservoir is preferably then sealed, with the exception of an opening leading to a microchannel 6. Sealing of the reservoir may be accomplished by filling the reservoir, then sealing it using known methods during production of the chip. Alternatively, the reservoir may be sealed with one or more valves, whereby the valve acts to seal the reservoir when the valve is closed, and upon being opened, acts to allow the reservoir to be refilled. Such valving can be accomplished using known methods, such as "virtual" valving, which relies on low Reynolds number flow of fluids through intersecting channels which are used to divert flow by controlling the pressure in the channels. See Brody, et. al, "Biotechnology at Low Reynolds Numbers," Biophysical Journal, Vol. 71, pp. 3430-3441 (1996).
  • valving techniques such as use of chemical valves of the present invention, discussed in greater detail hereinafter, may also be used.
  • the purification chamber 8 may be used, for example, in situations where the sample is a complex mixture of diverse macromolecules and the investigator needs to purify the molecule that he or she wants to study in order to successfully conduct the experiment of interest. From the purification chamber 8 the sample flows in to a second microchannel 10.
  • the second microchannel 10 is intersected at intersection 11 by a third microchannel 12 that is connected to a reaction reagent reservoir 14.
  • This intersection 11 may be used as a "virtual" valve, previously described, or as a chemical valve, as will subsequently be described. Also using VIS/IR induced pumping, reagent from the reaction reagent reservoir 14 can be pumped for mixing with the sample. Such mixing can occur in the microchannel 10, and/or in the reaction vessel 16, depending on the timing of pumping the reagent from the reagent vessel 14.
  • the sample flows into a sample injection microchannel 18.
  • the sample injection microchannel 18 is intersected at intersection 19 by a separation channel 22.
  • the flow of the sample into and through the separation channel 22 is controlled by reservoirs 20 which, in conjunction with the intersection 19, act as valves, and will be subsequently described.
  • the separation channel 22 From the separation channel 22, the sample flows into a detection device 24 where it is analyzed, for example, spectrophotometrically. From the detection device 24, the sample flows through a sample collection microchannel 26 and then to a sample collection reservoir 28.
  • each of the reservoirs 4, 14 and 20 can be heated and/or cooled according to the present invention in order to induce fluid flow from or to those reservoirs.
  • VIS/IR induced pumping can be used to effect fluid flow at every point of the process, it need not be used exclusively, rather, may be employed in conjunction with other fluid flow techniques such as those employed in the prior art.
  • FIG 2 illustrates one type of VIS/IR induced pumping according the present invention.
  • a sealed reservoir 34 contains an organic liquid 36 with high thermal expansion properties and an aqueous liquid 38.
  • the organic liquid 36 is immiscible with the aqueous liquid 38.
  • the sealed reservoir 34 is connected to a microchannel 40.
  • the sealed reservoir 34 is exposed to a heating / cooling source 30 whereby the flow 32 of heating irradiation or cooling air contacts the sealed reservoir 34 whereby, in the case of heating, the organic liquid 36 expands, forcing the aqueous liquid 38 to flow out of the sealed reservoir 34 into the microchannel 40.
  • the organic liquid 36 contracts, causing the aqueous liquid 38 to flow back into and/or in the direction of, the sealed reservoir 34.
  • FIG. 3A and 3B illustrate a VIS/IR induced chemical valve according to the teachings of the present invention.
  • An aqueous liquid-containing microchannel 44 intersects an organic liquid-containing microchannel 48 that is connected to an organic liquid- containing reservoir 47.
  • the flow of an aqueous liquid 42 flowing through the aqueous liquid microchannel 44 can be stopped by remotely heating the organic liquid 36 with the heating source 30, causing it to expand out of the organic liquid microchannel 48 into the aqueous liquid microchannel 44. Since the aqueous liquid 42 is immiscible with the organic liquid 36, the flow of the aqueous liquid 42 is stopped, as illustrated in FIG 3B.
  • the organic liquid 36 contracts, causing it to flow out of the aqueous liquid microchannel 44 and back into the organic liquid microchannel 48.
  • the walls of the aqueous liquid-containing microchannel 44 either comprise, or are coated with, a hydrophilic material
  • the walls of the organic liquid-containing microchannel 48 either comprise, or are coated with, a hydrophobic material, to further enhance the valving capabilities of the invention.
  • FIG 4 illustrates how the mixing of reagents on the microfluidic device can be achieved according to the teachings of the present invention.
  • a thermoreservoir 58 containing an aqueous liquid 38 is connected to several reagent reservoirs 52 by means of wide-bore microchannels 53. Reaction reagents, 46, 48 and 50, are contained in reagent reservoirs 52 in a lyophilized form.
  • the thermoreservoir 58 is heated by a heating/cooling source 30, the aqueous liquid 38 thermally expands into the reaction reagents reservoirs 52, whereby the lyophilized reagents, 46,48 and 50 are dissolved.
  • thermoreservoir When the thermoreservoir cools, the aqueous liquid 38 containing the dissolved reaction reagents, 46, 48 and 50 contracts back into the thermoreservoir 38 from the reagent reservoirs 52 whereby the reaction reagents, 46,48 and 50 are mixed. Further mixing can be accomplished by repeating the procedure any number of times.
  • the mixture can flow into the remaining microfluidic device architecture by means of a narrow-bore microchannel 54 that is connected to the thermoreservoir 58.
  • FIG 5 shows a thermal expansion driven micro-pump that can continuously achieve pumping action according to the teachings of the present invention.
  • a sealed thermoreservoir 63 is connected to a liquid reservoir 64, which need not be sealed, by means of a microchannel 54 that is intersected by a valve 66.
  • the thermoreservoir 63 is also connected to the remaining microfluidic device architecture by means of microchannel 67 that is also intersected by a valve 69.
  • the valves 66 and 69 may, but need not be, VIS/IR valves as previously discussed in reference to FIGS. 3A and 3B.
  • the valve 69 is open while the valve 66 is closed, causing the aqueous solution 38 to flow in the direction 72 from the thermoreservoir 63 through the microchannel 67 to the remaining microfluidic device architecture.
  • the valve 69 is closed, while valve 66 is open, causing the aqueous solution 38 in the liquid reservoir 64 to flow in the direction 74 into the thermoreservoir 63.
  • the reservoir 64 can be made larger relative to the thermoreservoir 63, allowing for a virtually limitless supply of fluid 38 over the duration of the microfluidic operation.

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Abstract

L'invention concerne un nouveau procédé de manipulation précise de volumes en picolitre-nanolitre dans des puces microfluidiques. La technique concerne l'expansion thermique d'un fluide, la pression et l'écoulement du fluide pouvant être facilement manipulées par régulation de la température du fluide. On peut appliquer efficacement de la chaleur de manière simple au moyen d'une source (30) lumineuse/infrarouge (par exemple une lampe halogène) qui chauffe sélectivement le fluide (36) dans la puce par absorption de l'énergie optique se trouvant dans la partie visible-infrarouge (VIS/IR) du spectre électromagnétique. On peut obtenir plusieurs applications de régulation et de manipulation de fluides sur des puces microfluidiques au moyen du mécanisme de pompe de fluide activé par VIS/IR, y compris une soupape.
PCT/US1999/001831 1998-01-29 1999-01-28 Commande de fluide par expansion thermique de dispositifs microfluidiques WO1999039120A1 (fr)

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AU23477/99A AU2347799A (en) 1998-01-29 1999-01-28 Thermal expansion-induced fluid control for microfluidic devices

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US09/015,278 1998-01-29
US09/015,278 US6210882B1 (en) 1998-01-29 1998-01-29 Rapid thermocycling for sample analysis
US16988698A 1998-10-12 1998-10-12
US09/169,886 1998-10-12

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Cited By (16)

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WO2001088204A1 (fr) * 2000-05-15 2001-11-22 Biomicro Systems, Inc. Regulation de l'ecoulement d'air dans des circuits microfluidiques destinee au reglage de la pression et a l'echange de gaz
DE10050943A1 (de) * 2000-10-10 2002-04-25 Epigenomics Ag Vorrichtung zur Hybridisierung von Proben an Arrays biologischer Stoffe
US6615856B2 (en) 2000-08-04 2003-09-09 Biomicro Systems, Inc. Remote valving for microfluidic flow control
FR2841158A1 (fr) * 2002-06-24 2003-12-26 Bio Merieux Dispositif fluidique permettant de maniere thermo-pneumatique l'isolement et eventuellement l'agitation du contenu d'une cavite operatoire
WO2005099901A1 (fr) * 2004-04-13 2005-10-27 Dtu Systeme de distribution d'echantillon microfluidique
US7118351B2 (en) 2002-05-16 2006-10-10 Roche Diagnostics Operations, Inc. Micropump with heating elements for a pulsed operation
US7192560B2 (en) 2001-12-20 2007-03-20 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using anion exchange
WO2007060635A2 (fr) * 2005-11-25 2007-05-31 Debiotech S.A. Système pour mesurer des paramètres rattachés à la coagulation du sang
US7347976B2 (en) 2001-12-20 2008-03-25 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using a hydrophilic solid support in a hydrophobic matrix
US7727710B2 (en) 2003-12-24 2010-06-01 3M Innovative Properties Company Materials, methods, and kits for reducing nonspecific binding of molecules to a surface
US7913928B2 (en) 2005-11-04 2011-03-29 Alliant Techsystems Inc. Adaptive structures, systems incorporating same and related methods
US7939249B2 (en) 2003-12-24 2011-05-10 3M Innovative Properties Company Methods for nucleic acid isolation and kits using a microfluidic device and concentration step
US7981600B2 (en) 2003-04-17 2011-07-19 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using an anion exchange material that includes a polyoxyalkylene
WO2020219304A1 (fr) * 2019-04-22 2020-10-29 Lam Research Corporation Porte-substrat électrostatique à couplage rf accordable spatialement sur une tranche
CN113357416A (zh) * 2021-06-29 2021-09-07 鞠长军 一种水封式回火防止机构
WO2022076132A1 (fr) * 2020-10-09 2022-04-14 Hewlett-Packard Development Company, L.P. Analyse de fluide avec système d'étanchéité fluidique

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EP0568024A2 (fr) * 1992-04-27 1993-11-03 Canon Kabushiki Kaisha Méthode pour le déplacement d'un liquide, dispositif de mesure et de déplacement d'un liquide utilisant celle-ci
WO1997002357A1 (fr) * 1995-06-29 1997-01-23 Affymetrix, Inc. Dispositif de diagnostic nucleotidique integre
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US5700695A (en) * 1994-06-30 1997-12-23 Zia Yassinzadeh Sample collection and manipulation method
WO1997002357A1 (fr) * 1995-06-29 1997-01-23 Affymetrix, Inc. Dispositif de diagnostic nucleotidique integre

Cited By (24)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6607907B2 (en) 2000-05-15 2003-08-19 Biomicro Systems, Inc. Air flow regulation in microfluidic circuits for pressure control and gaseous exchange
WO2001088204A1 (fr) * 2000-05-15 2001-11-22 Biomicro Systems, Inc. Regulation de l'ecoulement d'air dans des circuits microfluidiques destinee au reglage de la pression et a l'echange de gaz
US6615856B2 (en) 2000-08-04 2003-09-09 Biomicro Systems, Inc. Remote valving for microfluidic flow control
DE10050943B4 (de) * 2000-10-10 2005-08-25 Epigenomics Ag Vorrichtung zur Hybridisierung von Proben an Arrays biologischer Stoffe
DE10050943A1 (de) * 2000-10-10 2002-04-25 Epigenomics Ag Vorrichtung zur Hybridisierung von Proben an Arrays biologischer Stoffe
US7347976B2 (en) 2001-12-20 2008-03-25 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using a hydrophilic solid support in a hydrophobic matrix
US7192560B2 (en) 2001-12-20 2007-03-20 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using anion exchange
US7871827B2 (en) 2001-12-20 2011-01-18 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using anion exchange
US7118351B2 (en) 2002-05-16 2006-10-10 Roche Diagnostics Operations, Inc. Micropump with heating elements for a pulsed operation
CN100377770C (zh) * 2002-06-24 2008-04-02 比奥梅里欧公司 用于工作腔的内容物的热气压隔离和任选搅动的液压装置
WO2004000449A1 (fr) * 2002-06-24 2003-12-31 bioMérieux Dispositif fluidique permettant de maniere thermo-pneumatique l'isolement et eventuellement l'agitation du contenu d'une cavite operatoire
FR2841158A1 (fr) * 2002-06-24 2003-12-26 Bio Merieux Dispositif fluidique permettant de maniere thermo-pneumatique l'isolement et eventuellement l'agitation du contenu d'une cavite operatoire
US7981600B2 (en) 2003-04-17 2011-07-19 3M Innovative Properties Company Methods and devices for removal of organic molecules from biological mixtures using an anion exchange material that includes a polyoxyalkylene
US7727710B2 (en) 2003-12-24 2010-06-01 3M Innovative Properties Company Materials, methods, and kits for reducing nonspecific binding of molecules to a surface
US7939249B2 (en) 2003-12-24 2011-05-10 3M Innovative Properties Company Methods for nucleic acid isolation and kits using a microfluidic device and concentration step
WO2005099901A1 (fr) * 2004-04-13 2005-10-27 Dtu Systeme de distribution d'echantillon microfluidique
US7913928B2 (en) 2005-11-04 2011-03-29 Alliant Techsystems Inc. Adaptive structures, systems incorporating same and related methods
US8534570B2 (en) 2005-11-04 2013-09-17 Alliant Techsystems Inc. Adaptive structures, systems incorporating same and related methods
WO2007060635A3 (fr) * 2005-11-25 2007-10-11 Debiotech Sa Système pour mesurer des paramètres rattachés à la coagulation du sang
WO2007060635A2 (fr) * 2005-11-25 2007-05-31 Debiotech S.A. Système pour mesurer des paramètres rattachés à la coagulation du sang
WO2020219304A1 (fr) * 2019-04-22 2020-10-29 Lam Research Corporation Porte-substrat électrostatique à couplage rf accordable spatialement sur une tranche
WO2022076132A1 (fr) * 2020-10-09 2022-04-14 Hewlett-Packard Development Company, L.P. Analyse de fluide avec système d'étanchéité fluidique
CN113357416A (zh) * 2021-06-29 2021-09-07 鞠长军 一种水封式回火防止机构
CN113357416B (zh) * 2021-06-29 2022-12-13 湖南八达人防科技股份有限公司 一种水封式回火防止机构

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