Portable water quality instrument
Abstract
A hand-held microfluidic testing device is provided that includes a housing having a cartridge receiving port, a cartridge for input to the cartridge receiving port having a sample input and a channel, where the channel includes a mixture of Raman-scattering nanoparticles and a calibration solution, where the calibration solution includes chemical compounds capable of interacting with a sample under test input to the cartridge and the Raman-scattering nanoparticles, and an optical detection system in the housing, where the optical detection system is capable of providing an illuminated electric field, where the illuminating electric field is capable of being used for Raman spectroscopy with the Raman-scattering nanoparticles and the calibration solution to analyze the sample under test input to the cartridge.
Claims
exact text as granted — not AI-modifiedWe claim:
1 . A hand-held microfluidic testing device comprising:
a. a housing, wherein said housing comprises a cartridge receiving port; b. a cartridge for input to said cartridge receiving port, wherein said cartridge comprises a sample input and a channel, wherein said channel comprises a mixture of Raman-scattering nanoparticles and a calibration solution, wherein said calibration solution comprises chemical compounds capable of interacting with a sample under test input to said cartridge and said Raman-scattering nanoparticles; and c. an optical detection system in said housing, wherein said optical detection system is capable of providing an illuminated electric field, wherein said illuminating electric field is capable of being used for Raman spectroscopy with said Raman-scattering nanoparticles and said calibration solution to analyze said sample under test input to said cartridge.
2 . The hand-held microfluidic testing device of claim 1 , wherein said chemical compounds are selected from the group consisting of thiols, amines, silanes, polymeric particles, metallic particles, crown esters, cysteamine, cystamine, diethylaminethanethiol, mercaptopropionic acid, 1-propanethiol, octanethiol, octyldecanethiol, polystyrene, iron, and silica.
3 . The hand-held testing device in claim 1 wherein, said calibration solution comprises isotopes of said sample under test.
4 . The hand-held testing device in claim 1 wherein said calibration solution comprises a chemical composition in said sample under test.
5 . A hand-held microfluidic testing device comprising:
a. a housing, wherein said housing comprises at least one cartridge receiving port; b. at least one cartridge for input to said at least one cartridge receiving port, wherein said at least one cartridge comprises at least one separation channel; and c. an optical detection system in said housing, wherein said optical detection system is disposed to analyze at least one sample in said at least one cartridge.
6 . The hand-held microfluidic testing device of claim 5 , wherein said cartridge further comprises a detection window, a detection inlet, a detection outlet, a buffer inlet, a buffer outlet, a calibration inlet, a calibration outlet, a sample inlet, and a sample outlet.
7 . The hand-held microfluidic testing device of claim 5 , wherein said separation channel comprises:
a. at least one channel having a varying geometry along an x-axis, wherein said varying geometry is disposed to provide a distribution of velocities along a y-axis of said channel of a buffer solution moving in an x-direction; b. a first sample channel region and a second sample channel region, wherein a cross-section of said first sample channel region is smaller than a cross-section of said second sample channel region; c. a detection region comprising a first detection region and a second detection region, wherein a cross-section of said first detection region is larger than a cross-section of said second detection region and said second sample channel region is connected to said first detection region; and d. a marker input channel disposed to input markers into said second sample channel region, wherein said markers are larger than said cross-section of said first sample channel region and said cross-section of said second detection region, wherein said markers collect in said first detection region.
8 . The hand-held microfluidic testing device of claim 7 , wherein said markers have a size in a range of 10 nm to 10 μm.
9 . The hand-held microfluidic testing device of claim 7 , wherein said buffer solution moves when subject to forces selected from the group consisting of electroosmosis, electrophoresis, fluid pressure, moveable wall pressure, undulary electroosmosis, undulary electrophoresis, undulary fluid pressure and undulary moveable wall pressure, wherein said markers move according to movement of said buffer solution.
10 . The hand-held microfluidic testing device of claim 7 , wherein said markers are selected from the group consisting of gold particles, copper particles, silver particles, fluorescent particles, magnetic particles, particles having binding chemistry, latex particle, polystyrene particles and quantum dots.
11 . The hand-held microfluidic testing device of claim 7 , wherein said second detection region comprises a sieve structure having openings that are smaller than said markers.
12 . The hand-held microfluidic testing device of claim 7 , wherein said detection region comprises flexible material, wherein said flexible material is operably disposed to form said first sample channel region and said second detection channel region.
13 . The hand-held microfluidic testing device of claim 5 , wherein said optical detection system is selected from the group consisting of Raman spectroscopy, UV/visible spectroscopy, near infrared spectroscopy, and laser-induced fluorescence.
14 . A method of using electrokinetics for separating particles in a buffer solution comprising:
a. providing a chromatographic column, wherein said column has a non-uniform internal longitudinal cross-section; b. providing at least one main inlet and at least one main outlet, wherein said solution is input to said main inlet and output from said main outlet; c. providing at least one sample inlet and at least one sample outlet, wherein said particle is introduced to said column from said sample inlet and fractionated samples are eluted from said sample outlet, whereby quality control and further analysis are enabled; d. applying an electric field to said solution in said column to generate a charged double layer at a solid-liquid interface within said column, wherein said electric filed moves ions within said double layer, whereas a non-uniform velocity profile is induced to said buffer solution, whereby said moving ions carry said particles along said column and said particles are separated according to size or charge.
15 . The method of claim 14 , wherein said non-uniform internal longitudinal cross-section comprises a generally counter undulating-shape profile, whereby said counter undulation is between a first wall cross-section and a second wall cross-section.
16 . The method of claim 15 , wherein said undulation has a peak to peak distance, wherein said peak to peak distance is in a range from 1 μm to 500 μm.
17 . The method of claim 15 , wherein said undulation has an undulation linear density ranging from 0.05 peaks/μm to 1 peak/μm.
18 . The method of claim 15 , wherein said undulation first wall cross-section and said second wall cross-section have a ratio of a widest separation and a narrowest separation, wherein said ratio is greater than or equal to one.
19 . The method of claim 14 , wherein said column has a shape selected from a group consisting of linear, curved, circular, and spiral.
20 . The method of claim 14 , wherein said particles are selected from a group consisting of uncharged particles and charged particles.
21 . The method of claim 14 , wherein said solution is selected from a group consisting of water, phosphate buffered saline, TTE (0.5 M Tris, 0.5 M TAPS, 0.02 M EDTA) and any water-based solution.
22 . The method of claim 14 , wherein said particles have a particle size ranging from 1 nm to 500 m.Join the waitlist — get patent alerts
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