The present disclosure relate to a microsampler for hermetically sealing a sample (e.g., chemical, biological, and explosive samples). Methods of making and using such microsamplers are also described herein.
During a chemical, biological, or explosive (CBE) event, the presence of detection systems will help mitigate infrastructure damage and/or limit loss of life. Post-event analysis and/or attempts at confirmatory analysis will be complicated by the presence of decontamination substances, the rapid decay of CBE substances in the environment, and the presence of general environmental pollutants. This post-event analysis is important because it enables the gathering of technical intelligence, such as the specific type of CBE agent, its origin, the origin of its precursors, and the CBE deployment method. Additionally, a captured CBE sample could be analyzed at foreign or third party laboratories for the purposes of establishing political consensus about suspected CBE events. There is a need for simplified methods and platforms to capture CBE samples and optionally archive such samples for later analysis.
Accordingly, certain aspects of the present disclosure relates to a phase-change microvalve technology in order to enable the development of safe, hermetic encapsulation of samples (e.g., aerosol samples, as well as chemical, biological, or explosive samples) for the purposes of archival sample storage. In the event that a portable (ground or UAV-mounted) or building-emplaced detection system positively detects a CBE event, this miniaturized archival storage system can be activated to entrain the CBE sample into an inert container and hermetically seal it within a miniaturized volume. This will allow subsequent confirmatory analyses to be performed on the sample at certified laboratory spaces for the purposes of agent attribution, technical intelligence gathering, and forensic documentation. Such analyses will provide policy makers, homeland security officials, and intelligence analysts with critical information about the event which could have important political and national security consequences.
In some non-limiting embodiments, the microsampler includes a normally-closed (NC) phase-change microvalve and a dual-layer stacked valve structure, thereby providing an archival storage system. In some embodiments, the NC valve operates in conjunction with a chamber maintained at vacuum pressure. When the phase-change material of the valve is thermally cycled and liquefied, the valve seal is ruptured, and the surrounding air rushes to fill the vacuum within the chamber. In other embodiments, the dual-layer stacked valve structure includes a normally-closed (NC) phase-change microvalve positioned at the entrance of the chamber, and a normally-opened (NO) phase-change micro-valve positioned immediately below it. In some embodiments, the microsampler is deployed in conjunction with a detector configured to detect one or more CBE agents. Thus, in further embodiments, cycling of the NC valve is timed so that air containing the CBE sample will be drawn into the chamber as it leaves the detector. Once the volume within the chamber equilibrates, the NO valve can be cycled, and the CBE sample is hermetically sealed within the container. Additional details are described herein.
As used herein, the term “about” means +/−10% of any recited value. As used herein, this term modifies any recited value, range of values, or endpoints of one or more ranges.
By “fluidic communication,” as used herein, refers to any duct, channel, tube, pipe, chamber, or pathway through which a substance, such as a liquid, gas, or solid may pass substantially unrestricted when the pathway is open. When the pathway is closed, the substance is substantially restricted from passing through. Typically, limited diffusion of a substance through the material of a plate, base, and/or a substrate, which may or may not occur depending on the compositions of the substance and materials, does not constitute fluidic communication.
By “microfluidic” or “micro” is meant having at least one dimension that is less than 1 mm. For instance, a microfluidic structure (e.g., any structure described herein) can have a length, width, height, cross-sectional dimension, circumference, radius (e.g., external or internal radius), or diameter that is less than 1 mm.
As used herein, the terms “top,” “bottom,” “upper,” “lower,” “above,” and “below” are used to provide a relative relationship between structures. The use of these terms does not indicate or require that a particular structure must be located at a particular location in the apparatus.
Other features and advantages of the application will be apparent from the following description and the claims.
Certain aspects of the present disclosure relates to a microsampler having a microvalve technology. In general, the microvalve technology includes a phase-change material (PCM) that responds to heat and a heating element disposed in proximity to the PCM. To form a normally-closed (NC) valve, the PCM is configured to substantially block a seat opening on a valve seat. When the NC valve is actuated, the PCM unblocks the seat opening, thereby opening the valve. To form a normally-opened (NO) valve, the PCM is configured to be disposed around a valve orifice (e.g., an opening is formed within a bulk PCM or an annular ring of PCM is formed around an opening). When the NO valve is actuated, the PCM blocks the valve orifice, thereby closing the valve. Such valves can be configured in any useful manner, e.g., a dual-layer stacked valve structure, in order to form an actuating microsampler.
The stacked valve structure includes a valve seat 130 disposed between the NC and NO valves 110, 120. As can be seen, the valve seat 130 includes a seat opening 135, and activating the NC valve 110 results in an opening that is formed in the opened NC valve 111 and aligned with the seat opening 135 and an opening in the heating element, according to at least one embodiment.
The NO valve 120 in turn includes a valve orifice 125, which is formed from an opening present in the PCM 105 and the heating element 106. The valve orifice 125 of the NO valve is aligned with inlet 102 of the chamber 101, which is optionally under vacuum, according to at least one embodiment. An exemplary NO valve is provided in
In order to capture a sample 10, both the NC and NO valves 110, 120 can be activated (e.g., by applying heat to the PCM). The valves can be activated in any order. In one instance, the NC valve 110 is opened, thereby providing a fluidic connection between the external environment and the internal chamber 101. As the chamber 101 is under vacuum, the pressure difference results in a capturing the sample 10 within the chamber 101. After sufficient time has elapsed to ensure capture of the desired sample, the NO valve 120 is closed, thereby providing a sealed sample 11. As can be seen, the sealed, activated microsampler 150 includes an opened NC valve 111 and a closed NO valve 121.
The microsampler can include any useful internal structures. For instance,
Furthermore, the microsampler can be integrated with any external component to form any useful system. For instance,
The microsampler can also include arrays of valves, where such arrayed microsamplers can include a plurality of chambers, and a valve system associated with each chamber. Exemplary arrays are shown in
The bottom layer 752 includes a plurality of chamber 701-704 configured to capture a sample or an analyte. In some embodiments, the top layer 751 includes a compartment 750, which is disposed above the chambers 701-704. Here, the compartment 750 is in fluidic communication with each of these chambers 701-704. This arrangement may be useful, for instance, when multiple aliquots of the same sample are desired and contamination is not a great concern.
Each chamber 701-704 is associated with a valve system. The valve system includes an NO valve 720 disposed in the bottom layer 752 and an NC valve 710 disposed in the top layer 751. Furthermore, each valve can be configured to be actuated individually. For instance, each valve can include an electrical connector 740 that is electrically connected to the heating element and an electrical contact 745. Each electrical contact 745 in turn can be readily accessible by a control unit to individually control each valve. As can be seen, electrical contacts can be arrayed on the edge(s) of the top and bottom layers 751, 752.
In an alternative configuration, the arrayed microsampler 800 can include a plurality of compartments 851-854 disposed above each internal chamber 801-804. In this architecture, contamination between each internal chamber is minimized because each chamber is only in fluidic communication with its own compartment. Again, the microsampler 800 can include a valve system 860 (e.g., an NC valve/NO valve combination) arranged between top and bottom layers, as well as electrical connectors 840 and electrical contacts 845 associated with each valve.
Electrical connections can be accomplished with any useful arrangement. For instance, as seen in
Methods of Fabrication
The microsamplers of the present disclosure can be fabricated in any useful manner. In one instance, the chamber can be formed by cutting the ends of tubing. Then, plates can be affixed to the cut ends of the tubing (e.g., by brazing), thereby serving as end caps. Inlet(s) to the chamber can be drilled into one or more of the plates. Next, one or more metallization steps can be conducted to install heating elements and/or electrical connectors (e.g., heating traces) to the plates. Finally, a pre-molded PCM can be placed on or in proximity to the heating elements, thereby forming a PCM-based microvalve.
In another instance, each of the structures for the microsampler can be pre-formed, and then these structures can be assembled to form the completed microsampler.
As can be seen, various inlets and orifices are aligned to ensure fluidic communication between the internal chamber 601 and the external environment when the NC valve 610 is actuated, in at least one embodiment. For instance, the orifice in the heaters 616, 626, the inlets or openings in the valve plates 631, 632, and the orifice in the PCM 625 for the NO valve are aligned and in fluidic communication with the chamber 601.
In another instance (as shown in
The method 1000 can include providing a body having a valve plate 1013 and a base plate 1010 that are affixed to the walls 1011 of the body using a filler or adhesive 1012. In the metallization step 1001, the method includes providing one or more electrical connectors and/or solder pads 1040 on the valve plate 1013 surface above the internal chamber 1015. In the next metallization step 1002, a heating element 1060 is patterned such that it is electrically connected to the electrical connectors and/or solder pads 1040. In the drilling step 1003, an orifice 1016 is placed in the valve plate 1013. Alternatively, the drilling step 1003 can be performed prior to the metallization steps 1001, 1002; or the drilling step 1003 can be performed after the PCM deposition step 1004. To complete the valved chamber 1105, a PCM 1050 (e.g., a preformed PCM) is patterned, deposited, or aligned with the orifice 1016.
The valved seat can be formed in any useful manner. In one embodiment, the method 1000 includes providing a valve plate 1017 affixed to a fitting 1018, where electrical connectors and/or solder pads 1041 are disposed on the valve plate 1017. In a metallization step 1005, a heating element 1061 is patterned such that it is electrically connected to the electrical connectors and/or solder pads 1041. In the drilling step 1006, an orifice 1019 is placed in the valve plate 1017. Alternatively, the drilling step 1006 can be performed prior to the metallization step 1005; or the drilling step 1006 can be performed after the PCM deposition step 1007. To complete the valved seat 1110, a PCM 1051 (e.g., a preformed PCM) is patterned, deposited, or aligned with the orifice 1019. Finally, in an alignment step 1008, the valved seat 1110 is aligned with and affixed to the valved chamber 1105 to provide the microsampler 1100. Other methods for fabricating and testing such microsamplers are described herein, as well as in Manginell R P et al., “A monolithically-integrated μGC chemical sensor system,” Sensors 2011; 11:6517-32; Manginell R P et al., “A materials investigation of a phase-change micro-valve for greenhouse gas collection and other potential applications,” Rev. Sci. Instrum. 2012; 83:031301 (11 pp.); and Galambos P et al., “Active MEMS valves for flow control in a high-pressure micro-gas-analyzer,” J. Microelectromech. Sys. 2011 October; 20(5):1150-62, each of which is incorporated herein by reference in its entirety.
Phase-Change Materials
As described herein, the microvalve includes use of one or more PCMs in conjunction with a heating element to melt the PCM. Any useful PCM can be employed, including those that have sufficient wettability that ensures adequate flow of the PCM to substantially block or unblock a valve orifice. Exemplary PCM include an organic material or an inorganic material. In particular embodiments, the PCM can be a eutectic, which is a composition of two or more components that melts or freezes nearly simultaneously. Eutectic metal alloys have a single melting point that is usually lower than the melting points of the corresponding two or more metals in the eutectic alloy. Exemplary eutectic metal alloys include a tin-lead alloy (e.g., a Sn—Pb alloy optionally including one or more other elements, such as Sn63Pb37, Sn10Pb90, Sn62Pb36Ag2, Sn62.5Pb36Ag2.5, Sn97.5Pb1Ag1.5, Pb90Sn5Ag5, Pb97.5Ag1.5Sn1, Sn51.2Pb30.6Cd18.2, Sn62Pb37Cu1, Sn70Pb18In12, and Sn63Pb37P0.0015-0.04); an indium-silver alloy (e.g., an In—Ag alloy optionally including one or more other elements, such as In97Ag3, In80Ag5Pb15); an indium-bismuth alloy (e.g., an In—Bi alloy optionally including one or more other elements, such as In66.3Bi33.7, In61.7Bi30.8Cd7.5, and In51.0Bi32.5Sn16.5 (Field's metal)); an indium-cadmium alloy (e.g., an In—Cd alloy optionally including one or more other elements, such as In74Cd26); an indium-lead alloy (e.g., an In—Pb alloy optionally including one or more other elements, such as In80Pb15Ag5); a tin-silver alloy (e.g., an Sn—Ag alloy optionally including one or more other elements, such as Sn96.5Ag3.5, Sn93.5Ag3.5Bi3.0, Sn96Ag2.5Bi1.0Cu0.5, Sn88Ag3.5Bi4.5In4.0, Sn95.5Ag4Cu0.5, Sn95.5Ag3.9Cu0.6, Sn95.6Ag3.5Cu0.9, Sn91.4Ag4.1Cu0.5In4.0, and Sn65Ag25Sb10); a bismuth-lead alloy (e.g., a Bi—Pb alloy optionally including one or more other elements, such as Bi52Pb32Sn16, Bi50Pb26.7Sn13.3Cd10, Bi49.5Pb27.3Sn13.1Cd10.1 (Lipowitz Metal), Bi50.0Pb25.0Sn12.5Cd12.5 (Wood's metal), Bi44.7Pb22.6In19.1Cd5.3Sn8.3, and Bi49Pb18Sn2In21); a gold alloy (e.g., an Au alloy optionally including one or more other elements, such as Sn90Au10, Au80Sn20, Au96.8Si3.2, Au87.5Ge12.5); a tin-copper alloy (e.g., a Sn—Cu alloy optionally including one or more other elements, such as Sn99.3Cu0.7 and Sn95Cu0.5Ga0.5In4); a tin alloy (e.g., a Sn alloy including one or more other elements, such as Sn99.3Cu0.7, Sn91Zn9, Bi58Sn42, In52Sn48, and In58Sn42); a zinc alloy (e.g., a Zn alloy including one or more elements, such as Zn95Al5, Cd82.5Zn17.5, and Zn95Sn5); and a lead alloy (e.g., a Pb alloy one or more elements, such as Pb97.5Ag2.5), where any of these alloys can optionally include a flux (e.g., an organic acid water-soluble flux, such as those including 2-propanol and glycerine (commercially available as Kester™ 2331-ZX soldering flux), or any including an acid and a solvent, such as those described in U.S. Pat. No. 8,444,774, which is incorporated herein by reference in its entirety) and any of these can be provided in any useful form (e.g., a paste, a wire, a mixture, etc.). Additional PCMs include solder-flux mixtures, such as those in U.S. Pat. Nos. 5,091,242, 5,411,602, 5,830,389, 7,017,795, 7,022,266, 7,059,512, 7,847,406, and RE32,309, as well as any in Shaikh K A et al., “Development of a latchable microvalve employing a low-melting-temperature metal alloy,” J. Microelectromech. Sys. 2008 October; 17(5):1195-203; and Yang B et al., “A latchable phase-change microvalve with integrated heaters,” J. Microelectromech. Sys. 2009 August; 18(4):860-7, each of which is incorporated herein by reference in its entirety.
In other embodiments, the PCM is robust against environmental exposure and thermo-mechanically stable against temperature cycling. In some instances, organic and inorganic phase-change materials can lack rigorous hermetic sealing capabilities and robustness to aggressive chemical decontamination.
The PCM can be employed in any useful form to fabricate the microsampler. In one instance, the PCM is machined or cast to include an entrance hole concentric with the microsampler opening. In another instance, the PCM is patterned onto the microsampler. In yet another instance, the PCM is formed to substantially surround and not block an opening or orifice (thereby forming an NO valve), then the valve is actuated to form an NC valve.
Materials
The microsampler herein can be formed with any useful material. For instance, the electrodes can be formed from a conductive material, and the body or valve plates from an insulative material or an inert material. Exemplary materials include an insulative material, e.g., ceramic, alumina, ceria, polytetrafluoroethylene, or dielectric; a conductive material, e.g., a metal, stainless steel, steel, titanium, aluminum, copper, nickel, chromium, tungsten, or alloys thereof, as well as any substrate or material described in U.S. Pat. No. 6,444,326, which is incorporated herein by reference in its entirety; or an inert material, e.g., stainless steel. In particular embodiment, the surface of the material is passivated. For instance, passivation for stainless steel can include an amorphous silicon coating or a Siltek® coating, such as that described in U.S. Pat. No. 6,444,326, which is incorporated herein by reference in its entirety. In another embodiment, the surface of the material is coated with a biocompatible material, e.g., a cell medium (e.g., an agar medium), polyethylene glycol, etc. In other embodiments, the surface of the material can include one or more preservation agents, such as proteolytic inhibitors, lipolytic inhibitors, sugars, salts, electrolytes, etc.
Additional Components
The microsampler can be integrated or interfaces with one or more other components. For instance, a system can include a microsampler, or an array thereof, for use with a cooler (e.g., an active or passive cooling apparatus, which enables rapid cooling via a thermo-electric cooler in order to actively condense sample aerosols and/or minimize agent breakdown, such as those described in U.S. Pat. No. 6,706,091, which is incorporated herein by reference in its entirety); a sealing mechanism that is robust enough to undergo decontamination procedures and survive transport to certified laboratory spaces for subsequent gold standard confirmatory analyses on the samples (e.g., a seal having a helium leak rate below 1×10−9 atm cm3/s); one or more media (e.g., collection medium); a filter; an aerosol concentrator or collector; and/or a portable power source (e.g., to control one or more microvalves, or any other component).
Uses and Analytes
The microsamplers and systems herein can be employed for any useful purpose. The microsampler can capture any useful sample (e.g., an aerosol, such as a chemical aerosol or a bioaerosol (e.g., an aerosol including one or more viruses, bacteria, fungi, and/or odors, as well as any analyte described herein); a gaseous sample, such as a plume; or a liquid sample, such as an aqueous sample). The microsampler can be employed for hermetic storage, preservation, and/or retrieval. In one instance, the miniaturized archival storage system can include a microsampler that is configured to entrain a positive sample eluting from any useful sensor system.
In another instance, the microsampler can be employed to capture one or more analytes in a sample (e.g., a GC sample). Exemplary analytes include one or more of the following: light gases (e.g., hydrogen (H2), methane (CH4), carbon dioxide (CO2), or carbon monoxide (CO), or any greenhouse gas (GHG)); volatile organic compounds (VOCs, e.g., from any source, such as microorganisms, pathogens, humans, toxic industrial chemicals (TICs), solvents, fixed/permanent gases, explosives, GHG, water contaminants, and/or chemical and biological warfare agents (CWAs and BWAs)), such as acids (e.g., isovaleric acid), aldehydes (e.g., acetaldehyde or 3-methylbutanal), ketones (e.g., acetoin or 2-nonanone), hydrocarbons (e.g., 2-butene or 1,10-undecadiene), alcohols (e.g., 2-methyl-1-propanol, 2-butanol), esters (e.g., ethyl formate or methyl 2-methylbutyrate), aromatics (e.g., benzene or toluene), including volatile nitrogen compounds (e.g., methylpyrrole), and volatile sulfur compounds (e.g., dimethylsulfide); semi-volatile organic compounds; human-specific volatile signals (e.g., hexenoic acid, such as 3-methyl-2-hexenoic acid or (E)-3-methyl-2-hexenoic acid; volatile signatures of pathogens (e.g., bacteria, fungi, food pathogens, or biological warfare agents, such as Salmonella, Staphylococcus (e.g., S. aureus), Bacillus (B. anthracis), Mycobacteria (e.g., M. bovis or M. tuberculosis), Pseudomonas (e.g., P. aeruginosa), Neisseria (e.g., N. meningitidis), Streptococcus (e.g., S. pneumoniae), Klebsiella (e.g., K. oxytoca), Salmonella, Acinetobacter (e.g., A. baumannii), Enterobacter (e.g., E. cloacae), Penicillium (e.g., P. brevicompactum), Proteus (e.g., P. vulgaris), Serratia (e.g., S. marcescens), Yersinia (e.g., Y. pestis), or Escherichia (e.g., E. coli)) and diseases in livestock and humans (e.g., acetaldehyde, acetic acid, acetone, acetonitrile, amine, 2-aminoacetophenone, butadiene, 1-butanol, 2-butanone, 1-decanol, dimethyl disulfide, dimethyl sulfide, ethanol, ethylene glycol, formaldehyde, hexanal, hydrogen sulfide, indole, isobutanol, isopentanol, 9-isopentanol, isopentyl acetate, isoprene, methanethiol, methanol, methyl p-anisate, 2-methyl-1-butanol, methyl nicotinate, 4-methylphenol, methyl phenylacetate, 2-nonanone, pentanol (including any isomer thereof), 2-pentanone, o-phenyl anisole, propanol, propene, pyrimidine, toluene, or trimethylamine); pesticides; water contaminants, e.g., trihalomethanes; explosives-related compounds (e.g., 2,3-butanediol, n-decane, dicyclohexylamine, 2,6-dimethylaniline, 2,6-dimethylphenol, 2,3-dimethyl-2,3-dinitrobutane (DMNB), 2-ethylhexanoic acid, methyl decanoate, methyl dodecanoate methyl undecanoate, nitrobenzene, 2-nitrotoluene, 3-nitrotoluene, nonanal, 1-octanol, triacetone triperoxide (TATP), or n-undecane); or chemical warfare agents (CWAs), e.g., dimethyl methylphosphonate (DMMP) in any sample (e.g., in soil, water, breath, saliva, food, liquid, milk, etc.), as well as gaseous or GC processed forms of any of these samples.
Other analytes and VOCs are described in Mainelis G et al., “Performance characteristics of the aerosol collectors of the Autonomous Pathogen Detection System (APDS),” Aerosol Sci. Technol. 2005; 39:461-71; Akutsu T et al., “Individual comparisons of the levels of (E)-3-methyl-2-hexenoic acid, an axillary odor-related compound, in Japanese,” Chem. Senses 2006 May; 31:557-63; McNerney R et al., “Production of volatile organic compounds by mycobacteria,” FEMS Microbiol. Lett. 2012; 328:150-6; Bostaris G et al., “Rapid detection methods for viable Mycobacterium avium subspecies paratuberculosis in milk and cheese,” Int. J. Food Microbiol. 2010; 141:S87-90; Biet F et al., “Zoonotic aspects of Mycobacterium bovis and Mycobacterium avium-intracellulare complex (MAC),” Vet. Res. 2005; 36:411-36; Syhre M et al. “The scent of Mycobacterium tuberculosis,” Tuberculosis 2008; 88:317-23; Syhre M et al., “The scent of Mycobacterium tuberculosis—Part II breath,” Tuberculosis 2009; 89:263-6; Straus E et al., “Radioimmunoassay of tuberculoprotein derived from Mycobacterium tuberculosis,” Proc. Nat'l Acad. Sci. USA 1980 July; 77:4301-4; Spooner A D et al., “Evaluation of a combination of SIFT-MS and multivariate data analysis for the diagnosis of Mycobacterium bovis in wild badgers,” Analyst 2009; 134:1922-7; Harris N B et al., “Recovery of Mycobacterium bovis from soft fresh cheese originating in Mexico,” Appl. Environ. Microbiol. 2007 February; 73:1025-8; Laurens J B et al., “Gas chromatographic analysis of trace gas impurities in tungsten hexafluoride,” J. Chromatogr. A 2001; 911:107-12; Roberge M T et al., “Evaluation of the pulsed discharge helium ionization detector for the analysis of hydrogen and methane in breath,” J. Chromatogr. A 2004; 1027:19-23; Forsyth D S et al., “Detection of organotin, organomercury, and organolead compounds with a pulsed discharge detector (PDD),” Anal. Bioanal. Chem. 2002; 374:344-7; Int. Pub. No. WO 2009/045116; Gibson T et al., “Not to be sniffed at,” Microbiol. Today 2000 February; 27:14-17; Adamovics J A et al., “Gas Chromatography,” Chapter 4 in Chromatographic analysis of pharmaceuticals, 2nd edition, Adamovics J A (ed.), 1997, Marcel Dekker, Inc., New York, N.Y., pp. 79-134; Ross B M et al., “Stability of methylnicotinate in aqueous solution as utilized in the ‘niacin patch test’,” BMC Res. Notes 2008 September; 1:89 (5 pp.); Achyuthan K E et al., “Design considerations for high-throughput screening and in vitro diagnostic assays,” Comb. Chem. High Throughput Screen. 2007 July; 10(6):399-412; Ringer M et al., “Ion mobility spectrometry for microbial volatile organic compounds: A new identification tool for human pathogenic bacteria,” Appl. Microbiol. Biotechnol. 2012 March; 93(6):2603-14; Dolch M E et al., “Volatile compound profiling for the identification of Gram-negative bacteria by ion-molecule reaction-mass spectrometry,” J. Appl. Microbiol. 2012; 113:1097-105; Filipiak W et al., “Molecular analysis of volatile metabolites released specifically by Staphylococcus aureus and Pseudomonas aeruginosa,” BMC Microbiol. 2012; 12:113 (16 pp.); Allardyce R A et al., “Detection of volatile metabolites produced by bacterial growth in blood culture media by selected ion flow tube mass spectrometry (SIFT-MS),” J. Microbiol. Meth. 2006; 65:361-5; Zhu J et al., “Fast detection of volatile organic compounds from bacterial cultures by secondary electrospray ionization-mass spectrometry,” J. Clin. Microbiol. 2010; 48:4426-31; Bunge M et al., “On-line monitoring of microbial volatile metabolites by proton transfer reaction-mass spectrometry,” Appl. Environ. Microbiol. 2008 April; 74(7):2179-86; Senecal A G et al., “Rapid detection of pathogenic bacteria by volatile organic compound (VOC) analysis,” Proc. SPIE 2002; 4575:121-31; Grob K, Jr. et al., “Comprehensive, standardized quality test for glass capillary columns,” J. Chromatogr. 1978; 156:1-20; Grob K et al., “Testing capillary gas chromatographic columns,” J. Chromatogr. 1981; 219:13-20; and Manginell R P et al., “Diagnostic potential of the pulsed discharged helium ionization detector (PDHID) for pathogenic Mycobacterial volatile biomarkers,” J. Breath Res. 2013; 7:037107 (9 pp.), each of which is incorporated herein by reference in its entirety.
An aspect of the present disclosure employs a microvalve technology. This microvalve includes a small opening (e.g., seat opening or valve orifice, such as about 250 μm in diameter), where the opening connects the interior chamber of the microsampler with the external environment.
Using our basic microvalve technology, two structures can be created: a normally-opened (NO) valve and a normally-closed (NC) valve. With these two valve structures as building blocks, we can create a large number of different sampling and capture schemes, as the subsequent size, shape, and material choice of the capture volume is largely independent of the valving mechanism. This technical attribute provides us with an immense flexibility in tailoring the microsampler to the desired sensing needs. The microvalve designs here are also appropriate for integration into liquid-based systems with active fluid control.
In one example, an annular resistive heating element 106 encircles the microsampler seat opening 135 or inlet 102, and over that a mass of phase-change material (PCM) 105 was deposited. Initially, we focused on Sn/Pb alloys as a candidate PCM. These alloys are not only inexpensive and common place but robust against environmental exposure and thermo-mechanically stable against temperature cycling. Some organic and inorganic phase-change materials may lack the rigorous hermetic sealing capabilities, as well as robustness to aggressive chemical decontamination.
The Sn—Pb PCM was machined or cast to include a valve orifice concentric with the microsampler seat opening or inlet. A few watts of current were applied to the resistive heating element for several seconds to melt the phase-change material. Reflow of this material wetted the valve seat and hermetically sealed the valve orifice.
The microsampler fabrication process is highly versatile and capable of producing a variety of geometries and internal volumes as necessary. An exemplary microsampler was constructed from alumina (99.9% pure, 0.80 mm thick), which is a beneficial material for its relative strength, weight, ease of commercial purchase in a variety of shapes and sizes, and compatibility with a variety of fabrication processes including brazing and laser machining. Microsamplers can also be fabricated from commercial alumina tubing of a 2.30 mm diameter diced to the desired length to provide ˜1 mL internal chamber (
End caps (or plates) made from laser-machined alumina plate were then brazed on with commercial brazing foils. After assembly, the brazing was performed at high temperature in a vacuum oven, which assured a strong, hermetic seal between alumina parts. After brazing, a metallized pad was electron beam deposited through a shadow mask to form the valve metallization, which included the heating element deposited on the valve seat and a heating trace. This pad was a stack of Ti (100 nm thick), Ni (1 μm thick), and Au (5 μm thick). This metal could also be deposited using screen printing techniques. In the geometric center of the pad, a 0.25 mm diameter hole was laser drilled through both the metal pad and alumina substrate to create the valve orifice.
Preforms of the phase-change material (PCM) were punched from Sn/Pb eutectic solder that was rolled to a 0.38-0.51 mm thickness. To create an entrance hole in the final microvalve, sections of 0.20 mm diameter tungsten wire are used to cast the microvalve orifice. The Sn/Pb eutectic does not chemically bond with the tungsten wire, which means the wire can be easily removed once the preform is thermally-cycled. The PCM preform was placed over the metallization, and the tungsten wire was strung through the center orifice. The microsampler was thermally cycled using an external hotplate or oven (allowing many to be processed in parallel on industrial equipment such as a belt-furnace), which reflowed the eutectic solder and wetted the material onto the metallization pad. After cooling, the tungsten wire was removed, and the microsampler surface was cleaned of flux residue. The fabrication process detailed above represents the microsampler as currently realized. These basic structures have been produced and tested to demonstrate their ability to hermetically seal a gas sample within their volume without outgassing contaminants.
For applications that require an active atmospheric collection, such as when an unmanned aerial vehicle (UAV) is deploying a microsampler toward an agent plume or when a microsampler is mounted at a building air intake, we can integrate a microsampler with a miniature pump. In one embodiment, as seen in
As shown in
To optimize the microsampler for bioaerosol collection, we propose a number of additions to the basic design herein. For instance, to promote the stability of the captured sample, we propose to deposit a bio-relevant coating within the chamber of the microsampler. An exemplary coating includes a thin layer of nutrient agar medium (such as Tryptic Soy Agar, TSA, for bacteria), as well as a cocktail of proteolytic and lipolytic inhibitors. The purpose of these last two components is to prevent sample degradation from environmental enzymes.
In addition, the microsampler can be configured to include a thermo-electric, or Peltier, cooling unit. A thermo-electric cooling unit will be integrated to reduce the temperature of the stored sample below ambient in order to promote bioaerosol condensation, minimize sample thermal degradation mechanisms, and encourage long-term sample preservation. A Peltier cooling unit is particularly beneficial due to its lack of moving parts, its high reliability, and its relatively small footprint and weight per unit of heat energy removed. Their primary drawback is the need for higher currents in order to maintain a large thermal gradient. It is our expectation that the relatively small thermal mass of the microsampler will allow for several hours of cooling at a modest cost in battery life. For situations where power is limited, lower-power thermo-electric cooling is critical. We estimate that two 1 mL microsamplers 501, 502 can be inserted into a machined aluminum holder 505 that is mounted to a thermo-electric cooler 506.
All publications, patents, and patent applications mentioned in this specification are incorporated herein by reference to the same extent as if each independent publication or patent application was specifically and individually indicated to be incorporated by reference.
While the invention has been described in connection with specific embodiments thereof, it will be understood that it is capable of further modifications and this application is intended to cover any variations, uses, or adaptations of the invention following, in general, the principles of the invention and including such departures from the present disclosure that come within known or customary practice within the art to which the invention pertains and may be applied to the essential features hereinbefore set forth, and follows in the scope of the claims.
Other embodiments are within the claims.
This application claims priority to U.S. Provisional Patent Application No. 62/082,495, filed on Nov. 20, 2014 under the title, “HERMETIC MICROSAMPLER FOR ARCHIVAL STORAGE,” the entirety of which is incorporated herein by reference.
This invention was made with Government support under contract no. DE-AC04-94AL85000 awarded by the U.S. Department of Energy to Sandia Corporation. The Government has certain rights in the invention.
Number | Name | Date | Kind |
---|---|---|---|
RE32309 | Hwang | Dec 1986 | E |
5091242 | Chung | Feb 1992 | A |
5411602 | Hayes | May 1995 | A |
5439639 | Vianco et al. | Aug 1995 | A |
5820922 | Ricco et al. | Oct 1998 | A |
5830389 | Capote et al. | Nov 1998 | A |
5834627 | Ricco et al. | Nov 1998 | A |
6096656 | Matzke et al. | Aug 2000 | A |
6171378 | Manginell et al. | Jan 2001 | B1 |
6224728 | Oborny et al. | May 2001 | B1 |
6444326 | Smith | Sep 2002 | B1 |
6527835 | Manginell et al. | Mar 2003 | B1 |
6666907 | Manginell et al. | Dec 2003 | B1 |
6699392 | Manginell et al. | Mar 2004 | B1 |
6706091 | Robinson et al. | Mar 2004 | B1 |
6772513 | Frye-Mason et al. | Aug 2004 | B1 |
6786716 | Gardner et al. | Sep 2004 | B1 |
6902701 | Hughes et al. | Jun 2005 | B1 |
6930051 | Manginell et al. | Aug 2005 | B1 |
7017795 | Liu et al. | Mar 2006 | B2 |
7022266 | Craig | Apr 2006 | B1 |
7059512 | Arita et al. | Jun 2006 | B2 |
7078237 | Mowry et al. | Jul 2006 | B1 |
7105098 | Shul et al. | Sep 2006 | B1 |
7118712 | Manginell et al. | Oct 2006 | B1 |
7168298 | Manginell et al. | Jan 2007 | B1 |
7399449 | Oborny et al. | Jul 2008 | B1 |
7422724 | Manginell et al. | Sep 2008 | B1 |
7597014 | Tans | Oct 2009 | B2 |
7708943 | Robinson et al. | May 2010 | B1 |
7727314 | Manginell et al. | Jun 2010 | B1 |
7799280 | Manginell et al. | Sep 2010 | B1 |
7847406 | Arita et al. | Dec 2010 | B2 |
7913534 | Robinson et al. | Mar 2011 | B1 |
8298488 | Lewis et al. | Oct 2012 | B1 |
8444774 | Duschesne et al. | May 2013 | B2 |
8736000 | Manginell et al. | May 2014 | B1 |
9472689 | Elizondo-Decanini et al. | Oct 2016 | B1 |
20020143437 | Handique | Oct 2002 | A1 |
20040007275 | Hui Liu | Jan 2004 | A1 |
20040219732 | Burns | Nov 2004 | A1 |
20090035847 | Cho | Feb 2009 | A1 |
20150116939 | Bernstein | Apr 2015 | A1 |
Number | Date | Country |
---|---|---|
WO 2009045116 | Apr 2009 | WO |
Entry |
---|
U.S. Appl. No. 14/332,831, filed Jul. 16, 2014, Moorman et al. |
U.S. Appl. No. 14/538,096, filed Nov. 11, 2014, Polsky et al. |
U.S. Appl. No. 14/992,871, filed Jan. 11, 2016, Moorman et al. |
U.S. Appl. No. 14/992,855, filed Jan. 11, 2016, Manginell et al. |
U.S. Appl. No. 15/466,608, filed Mar. 22, 2017, Vianco et al. |
U.S. Appl. No. 15/237,193, filed Aug. 15, 2016, Miller et al. |
Achyuthan KE et al., “Design considerations for high-throughput screening and in vitro diagnostic assays,” Comb. Chem. High Throughput Screen. Jul. 2007;10(6):399-412 (abstract, 1 p.). |
Adamovics JA et al., “Gas Chromatography,” Chapter 4 in Chromatographic analysis of pharmaceuticals, 2nd edition, Adamovics JA (ed.), 1997, Marcel Dekker, Inc., New York, NY, pp. 79-134. |
Akutsu T et al., “Individual comparisons of the levels of (E)-3-methyl-2-hexenoic acid, an axillary odor-related compound, in Japanese,” Chem. Senses May 2006;31:557-63. |
Allardyce RA et al., “Detection of volatile metabolites produced by bacterial growth in blood culture media by selected ion flow tube mass spectrometry (SIFT-MS),” J. Microbiol. Meth. 2006;65:361-5. |
Anderson G et al., “Determination of product shelf life and activation energy for five drugs of abuse,” Clin. Chem. 1991;37(3):398-402. |
Baker AK et al., “Analysis of non-methane hydrocarbons in air samples collected aboard the CARIBIC passenger aircraft,” Atmos. Meas. Tech. 2010;3:311-21. |
Bakwin PS et al., “Strategies for measurement of atmospheric column means of carbon dioxide from aircraft using discrete sampling,” J. Geophys. Res. Atmos. 2003;108(D16):4514 (7 pp.). |
Biet F et al., “Zoonotic aspects of Mycobacterium bovis and Mycobacterium avium-intracellulare complex (MAC),” Vet. Res. 2005;36:411-36. |
Bostaris G et al., “Rapid detection methods for viable Mycobacterium avium subspecies paratuberculosis in milk and cheese,” Int. J. Food Microbiol. 2010;141:S87-90. |
Bunge M et al., “On-line monitoring of microbial volatile metabolites by proton transfer reaction-mass spectrometry,” Appl. Environ. Microbiol. Apr. 2008;74(7):2179-86. |
Chen H et al., “High-accuracy continuous airborne measurements of greenhouse gases (CO2 and CH4) using the cavity ring-down spectroscopy (CRDS) technique,” Atmos. Meas. Tech. 2010;3:375-86. |
Chen Z et al., “Thermally-actuated, phase change flow control for microfluidic systems,” Lab Chip 2005;5:1277-85. |
Crevoisier C et al., “Region US carbon sinks from three-dimensional atmospheric CO2 sampling,” Proc. Nat'l Acad. Sci. USA 2010;107(43):18348-53. |
Daida JM et al., “A remote sensing unmanned aircraft vehicle system for flux measurements over forest canopies,” Proceedings of IEEE Topical Symposium on Combined Optical, Microwave, Earth and Atmosphere Sensing, held on Mar. 22-25, 1994 in Albuquerque, NM, pp. 126-129. |
Daida JM et al., “An unmanned aircraft vehicle system for boundary-layer flux measurements over forest canopies,” International Geoscience and Remote Sensing Symposium (IGARSS '94)—Surface and Atmospheric Remote Sensing: Technologies, Data Analysis and Interpretation, held on Aug. 8-12, 1994 in Pasadena, CA, pp. 1248-1250. |
De Maziere M et al., “Regional monitoring of tropospheric NO2 and CO using remote sensing from high altitude platforms—preliminary concepts,” Second International Workshop The Future of Remote Sensing, held on Oct. 17-18, 2006 in Antwerp, Belgium, 5 pp. |
Dolch ME et al., “Volatile compound profiling for the identification of Gram-negative bacteria by ion-molecule reaction-mass spectrometry,” J. Appl. Microbiol. 2012;113:1097-105. |
Dubourg V et al., “The STRATEOLE project status: 200 pressurized balloons for the polar vortex study,” AIAA International Balloon Technology Conference, held on Jun. 3-5, 19997 in San Francisco, CA, 7 pp. |
Favela KH et al., “Microcollection of gases in a capillary tube: preservation of spatial and temporal resolution,” Anal. Chem. 2012;84(19):8310-6. |
Filipiak W et al., “Molecular analysis of volatile metabolites released specifically by Staphylococcus aureus and Pseudomonas aeruginosa,” BMC Microbiol. 2012;12:113 (16 pp.). |
Forsyth DS et al., “Detection of organotin, organomercury, and organolead compounds with a pulsed discharge detector (PDD),” Anal. Bioanal. Chem. 2002;374:344-7. |
Galambos P et al., “Active MEMS valves for flow control in a high-pressure micro-gas-analyzer,” J. Microelectromech. Sys. Oct. 2011;20(5):1150-62. |
Gibson TD et al., “Not to be sniffed at,” Microbiol. Today Feb. 2000;27:14-17. |
Ginting D et al., “Construction and testing of a simple and economical soil greenhouse gas automatic sampler,” J. Plant Nutrition 2007;30(9):1441-54. |
Grob K et al., “Testing capillary gas chromatographic columns,” J. Chromatogr. 1981;219:13-20. |
Grob K, Jr. et al., “Comprehensive, standardized quality test for glass capillary columns,” J. Chromatogr. 1978;156:1-20. |
Harris NB et al., “Recovery of Mycobacterium bovis from soft fresh cheese originating in Mexico,” Appl. Environ. Microbiol. Feb. 2007;73:1025-8. |
Hesketh PJ et al., “Microvalve for fuel cells and miniature gas chromatographic system,” Sensors Update 2007;13(1):233-302. |
Jünger M et al., “Ion mobility spectrometry for microbial volatile organic compounds: A new identification tool for human pathogenic bacteria,” Appl. Microbiol. Biotechnol. Mar. 2012;93(6):2603-14. |
Karion A et al., “AirCore: an innovative atmospheric sampling system,” J. Atmos. Ocean Technol. 2010;27:1839-53. |
Kenisarin M et al., “Solar energy storage using phase change materials,” Renewable Sustainable Energy Rev. 2007;11(9):1913-65. |
Keppler F et al., “Methane emissions from terrestrial plants under aerobic conditions,” Nature 2006;439:187-91. |
Kukkonen CA et al., “Microsensors and microinstruments for space science and exploration,” Space Technol. 1997;17(3-4):195-203. |
Laurens JB et al., “Gas chromatographic analysis of trace gas impurities in tungsten hexafluoride,” J. Chromatogr. A 2001;911:107-12. |
Lewis PR et al., “Recent advancements in the gas-phase MicroChemLab,” IEEE Sensors J. 2006;6(3):784-95. |
MacDonald AE, “A global profiling system for improved weather and climate prediction,” Bull. Am. Meterol Soc. 2005; 86:1747-64. |
Machida T et al., “Worldwide measurements of atmospheric CO2 and other trace gas species using commercial airlines,” J. Atmos, Oceanic Technol. 2008;25:1744-54. |
Mainelis G et al., “Performance characteristics of the aerosol collectors of the autonomous pathogen detection system (APDS),” Aerosol Sci. Technol. 2005;39:461-71. |
Mäkiranta P et al., “Soil greenhouse gas emissions from afforested organic soil croplands and cutaway peatlands,” Boreal Env. Res. 2007;12(2):159-75. |
Manginell RP et al., “A materials investigation to enable miniaturized phase-change valving for greenhouse gas analysis with a micro analytical system,” Sandia Report No. SAND2010-6912, 2010, 27 pp. |
Manginell RP et al., “A monolithically-integrated μGC chemical sensor system,” Sensors 2011;11:6517-32. |
Manginell RP et al., “Diagnostic potential of the pulsed discharged helium ionization detector (PDHID) for pathogenic Mycobacterial volatile biomarkers,” J. Breath Res. 2013;7:037107 (9 pp.). |
Manginell RP et al., “Finite element modeling of a microhotplate for microfluidic applications,” Technical Proceedings of the 1999 International Conference on Modeling and Simulation of Microsystems, held on Apr. 19-21, 1999 in San Juan, Puerto Rico, pp. 663-666. |
Manginell RP et al., “Invited article: A materials investigation of a phase-change micro-valve for greenhouse gas collection and other potential applications,” Rev. Sci. Instrum. 2012;83:031301 (11 pp.). |
Manginell RP et al., “Mass-sensitive microfabricated chemical preconcentrator,” J. Microelectromech. Sys. 2008;17(6):1396-407. |
Marquis M et al., “Carbon crucible,” Science 2008;320(5875):460-1. |
McNerney R et al., “Production of volatile organic compounds by mycobacteria,” FEMS Microbiol. Lett. 2012;328:150-6. |
Moorman M et al., “Systems for plant volatile organic compound (VOC) analysis,” Sandia Report No. SAND2017-13451C, 2017, 1 p. |
Morimoto S et al., “A new compact cryogenic air sampler and its application in stratospheric greenhouse gas observation at Syowa Station, Antarctica,” J. Atmos. Ocean. Technol. 2009;26:2182-91. |
Nagel DJ, “Microsensor clusters,” Microelectron. J. 2002;33(1-2):107-19. |
Oh KW et al., “A review of microvalves,” J. Micromech. Microeng. 2006;16(5):R13-R39. |
Pal R et al., “Phase change microvalve for integrated devices,” Anal. Chem. 2004;76(13):3740-8. |
Pervov VS et al., “Supramolecular ensembles in eutectic alloys,” Russ. Chem. Rev. 2003;72(9):759-68. |
Pollmann J et al., “Evaluation of solid adsorbent materials for cryogen-free trapping—gas chromatographic analysis of atmospheric C2—C6 non-methane hydrocarbons,” J. Chromotogr. A 2006;1134(1-2):1-15. |
Pollmann J et al., “Sampling, storage, and analysis of C2—C7 non-methane hydrocarbons from the US National Oceanic and Atmospheric Administration Cooperative Air Sampling Network glass flasks,” J. Chromotogr. A 2008;1188(2):75-87. |
Roberge MT et al., “Evaluation of the pulsed discharge helium ionization detector for the analysis of hydrogen and methane in breath,” J. Chromatogr. A 2004;1027:19-23. |
Ross BM et al., “Stability of methylnicotinate in aqueous solution as utilized in the ‘niacin patch test’,” BMC Res. Notes Sep. 2008;1:89 (5 pp.). |
Schuck TJ et al., “Greenhouse gas analysis of air samples collected onboard the CARIBIC passenger aircraft,” Atmos. Meas. Tech. 2009;2:449-64. |
Schulz K et al., “Tedlar bag sampling technique for vertical profiling of carbon dioxide through the atmospheric boundary layer with high precision and accuracy,” Environ. Sci. Technol. 2004;38(13):3683-8. |
Senecal AG et al., “Rapid detection of pathogenic bacteria by volatile organic compound (VOC) analysis,” Proc. SPIE 2002;4575:121-31. |
Shaikh KA et al., “Development of a latchable microvalve employing a low-melting-temperature metal alloy,” J. Microelectromech. Sys. 2008;17(5):1195-203. |
Sharma A et al., “Review on thermal energy storage with phase change materials and applications,” Renewable Sustainable Energy Rev. 2009;13(2):318-45. |
Sim WY et al., “A phase-change type micropump with aluminum flap valves,” J. Micromech. Microeng. 2003;13:286-94. |
Sonnenfroh D et al., “LED-based CO2 sensor for balloon deployment,” CLEO:2011—Laser Applications to Photonic Applications, OSA Technical Digest (CD) (Optical Society of America, 2011), paper CThT5 (2 pp.). |
Spokas K et al., “Greenhouse gas production and emission from a forest nursery soil following fumigation with chloropicrin and methyl isothiocyanate,” Soil. Biol. Biochem. 2005;37(3):475-85. |
Spooner AD et al., “Evaluation of a combination of SIFT-MS and multivariate data analysis for the diagnosis of Mycobacterium bovis in wild badgers,” Analyst 2009;134:1922-7. |
Straus E et al., “Radioimmunoassay of tuberculoprotein derived from Mycobacterium tuberculosis,” Proc. Nat'l Acad. Sci. USA Jul. 1980;77:4301-4. |
Syhre M et al. “The scent of Mycobacterium tuberculosis,” Tuberculosis 2008;88:317-23. |
Syhre M et al., “The scent of Mycobacterium tuberculosis—Part II breath,” Tuberculosis 2009;89:263-6. |
Tans PP et al., “A feasible Global Carbon Cycle Observing System: a plan to decipher today's carbon cycle based on observations,” Global Change Biol. 1996;2(3):309-18. |
Tans PP et al., “Observational constraints on the global atmospheric CO2 budget,” Science 1990;247(4949):1431-8. |
Terry SC et al., “A gas chromatographic air analyzer fabricated on a silicon wafer,” IEEE Trans. Electron Devices 1979;26(12):1880-6. |
Ubachs RLJM et al., “Microstructure evolution of tin-lead solder,” IEEE Trans. Components Packaging Technols. 2004;27(4):635-42. |
Weiss RF et al., “Quantifying greenhouse-gas emissions from atmospheric measurements: a critical reality check for climate legislation,” Philos. Trans. R. Soc. A 2011;369:1925-42. |
Whiting JJ et al., “High-speed two-dimensional gas chromatography using microfabricated GC columns combined with nanoelectromechanical mass sensors,” International Solid-State Sensors, Actuators and Microsystems Conference (Transducers 2009), held on Jun. 21-25, 2009 in Denver, CO, pp. 1666-1669. |
Wilson ML, “General principles of specimen collection and transport,” Clin. Infect. Diseases 1996;22:766-77. |
Yang B et al., “A latchable microvalve using phase change of paraffin wax,” Sens. Actuat. A. Phys. 2007;134(1):194-200. |
Yang B et al., “A latchable phase-change microvalve with integrated heaters,” J. Microelectromech. Sys. 2009;18(4):860-7. |
Zhu J et al., “Fast detection of volatile organic compounds from bacterial cultures by secondary electrospray ionization-mass spectrometry,” J. Clin. Microbiol. 2010;48:4426-31. |
Number | Date | Country | |
---|---|---|---|
62082495 | Nov 2014 | US |