Microfluidic sorting using high gradient magnetic fields

US2019264166A1 · US · A1

Patent metadata
FieldValue
Publication numberUS-2019264166-A1
Application numberUS-201916256839-A
CountryUS
Kind codeA1
Filing dateJan 24, 2019
Priority dateOct 18, 2013
Publication dateAug 29, 2019
Grant date

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  1. Title

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  2. Abstract

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  5. First independent claim

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Abstract

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Microfluidic devices are described that include a microfluidic channel, a first array of one or more magnets above the microfluidic channel, each magnet in the first array having a magnetic pole orientation opposite to a magnetic pole orientation of an adjacent magnet in the first array, and a second array of one or more magnets beneath the microfluidic channel, each magnet in the second array having a magnetic pole orientation opposite to a magnetic pole orientation of an adjacent magnet in the second array. The first array is aligned with respect to the second array such that magnetic fields emitted by the first array and second array generate a magnetic flux gradient profile extending through the channel. An absolute value of the profile includes a first maximum and a second maximum that bound a local minimum. The local minimum is located within the microfluidic channel or less than 5 mm away from a wall of the microfluidic channel. Methods of using the new devices are also described.

First claim

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1 - 52 . (canceled) 53 . A microfluidic device comprising: a magnetophoresis region; an inertial focusing region upstream of the magnetophoresis region; and a microfluidic channel in the magnetophoresis region, wherein the magnetophoresis region comprises a first array of magnets arranged on top of the microfluidic channel, a second array of magnets arranged below the microfluidic channel, wherein each magnet in the first array has a magnetic pole orientation that is opposite to a magnetic pole orientation of an adjacent magnet in the first array, wherein each magnet in the second array has a magnetic pole orientation that is opposite to a magnetic pole orientation of an adjacent magnet in the second array, wherein an interface between two magnets in the first array is aligned with an interface between two magnets in the second array, wherein the first array and the second array produce a magnetic flux gradient profile that extends transverse to a central longitudinal axis of the microfluidic channel, wherein the magnetic flux gradient profile comprises a local minimum positioned within the channel and at least 50 microns away from walls of the microfluidic channel due to the alignment of the first and second magnet arrays with respect to one another, wherein the inertial focusing region is configured to localize fluid particles of a fluid sample along a common streamline, wherein the common streamline is positioned to be laterally offset from the local minimum of the magnetic flux gradient profile upon entering the magnetophoresis region. 54 . The microfluidic device of claim 53 , wherein an absolute value of the magnetic flux gradient profile comprises a first maximum and a second maximum that bound the local minimum in the magnetic flux gradient profile. 55 . The microfluidic device of claim 54 , wherein a distance between the first maximum and the second maximum is less than 5 mm. 56 . The microfluidic device of claim 54 , wherein each of the first maximum and the second maximum is at least 400 T/m. 57 . The microfluidic device of claim 54 , wherein both the first maximum and the second maximum occur within the microfluidic channel. 58 . The microfluidic device of claim 53 , further comprising a hydrodynamic particle sorting region upstream of the inertial focusing region, wherein the hydrodynamic particle sorting region is configured to sort particles based on particle size. 59 . The microfluidic device of claim 53 , comprising an additional inertial focusing region, wherein each inertial focusing region is configured to focus particles within a fluid sample to a corresponding streamline, and wherein the two inertial focusing regions are coupled to a common sample input port. 60 . The microfluidic device of claim 53 , wherein the local minimum is greater than or equal to a distance of 100 μm away from the walls of the microfluidic channel. 61 . The microfluidic device of claim 53 , wherein the local minimum is located substantially at a center of the microfluidic channel. 62 . A method of sorting analytes in a microfluidic device, wherein the microfluidic device comprises an inertial focusing region and a magnetophoresis region, the method comprising: flowing a fluid sample containing a mixture of a plurality of first analytes and a plurality of second analytes into a first microfluidic channel located within the inertial focusing region, wherein, upon entering the first microfluidic channel, the plurality of first analytes and the plurality of second analytes are inertially focused along a common streamline within the fluid sample, wherein the plurality of second analytes are bound to magnetic particles; and flowing the fluid sample comprising the plurality first analytes and the plurality of second analytes focused along the common streamline from the first microfluidic channel into a second microfluidic channel located within the magnetophoresis region, wherein the magnetophoresis region comprises a first array of magnets arranged above the second microfluidic channel and a second array of magnets arranged beneath the second microfluidic channel of the magnetophoresis region such that each magnet in the first array faces a corresponding magnet in the second array, wherein each magnet in the first array has a magnetic pole orientation that is opposite to a magnetic pole orientation of an adjacent magnet in the first array, wherein each magnet in the second array has a magnetic pole orientation that is opposite to a magnetic pole orientation of an adjacent magnet in the second array, wherein an interface between two magnets in the first array is aligned with an interface between two magnets in the second array, wherein the first array and the second array produce a magnetic flux gradient profile that extends transverse to a central longitudinal axis of the second microfluidic channel, wherein the magnetic flux gradient profile comprises a local minimum positioned within the second microfluidic channel and at least 50 microns away from each wall of the second microfluidic channel due to the alignment of the first and second magnet arrays with respect to one another, wherein the common streamline within the fluid sample, as the fluid sample enters the second microfluidic channel, is aligned so as to be laterally offset from the local minimum of the magnetic flux gradient profile, wherein the magnetic flux gradient profile within the magnetophoresis region deflects the plurality of second analytes from the one or more common streamlines in the fluid sample without deflecting the plurality of first analytes from the one or more common streamlines. 63 . The method of claim 62 , wherein an absolute value of the magnetic flux gradient profile comprises a first maximum and a second maximum that bound the local minimum in the magnetic flux gradient profile. 64 . The method of claim 63 , wherein a distance between the first maximum and the second maximum is less than 5 mm. 65 . The method of claim 63 , wherein each of the first maximum and the second maximum is at least 400 T/m. 66 . The method of claim 63 , wherein both the first maximum and the second maximum occur within the microfluidic channel. 67 . The method of claim 62 , further comprising, prior to flowing the fluid sample into the first microfluidic channel of the inertial focusing region, sorting particles within the fluid sample based on particle size in a hydrodynamic particle sorting region upstream of the inertial focusing region. 68 . The method of claim 62 , wherein the microfluidic device comprises an additional inertial focusing region, and wherein the method further comprises: flowing an additional fluid sample containing a mixture of a plurality of third analytes and a plurality of fourth analytes into the additional inertial focusing region, wherein, upon entering the additional inertial focusing region, the plurality of third analytes and the plurality of fourth analytes are inertially focused along a common streamline within the additional fluid sample, wherein the plurality of fourth analytes are bound to magnetic particles, and wherein the common streamline of the first fluid sample and the common streamline of the additional fluid sample are provided to the magnetophoresis region through a common sample input port. 69 . The method of claim 68 , wherein the magnetic flux gradient profile within the magnetophoresis region deflects the plurality of second analytes and the plurality of fourth analytes to a separate third fluid streamline. 70

Assignees

Inventors

Classifications

  • microstructural devices · CPC title

  • Containers or dishes for laboratory use, e.g. laboratory glassware; Droppers · CPC title

  • Magnetic means (C12M35/02 takes precedence) · CPC title

  • characterised by the magnetic field, e.g. its shape or generation · CPC title

  • Sampling; Preparing specimens for investigation · CPC title

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What does patent US2019264166A1 cover?
Microfluidic devices are described that include a microfluidic channel, a first array of one or more magnets above the microfluidic channel, each magnet in the first array having a magnetic pole orientation opposite to a magnetic pole orientation of an adjacent magnet in the first array, and a second array of one or more magnets beneath the microfluidic channel, each magnet in the second array …
Who is the assignee on this patent?
Massachusetts Gen Hospital
What technology area does this patent fall under?
Primary CPC classification G01N35/0098. Mapped technology areas include Physics.
When was this patent published?
Publication date Thu Aug 29 2019 00:00:00 GMT+0000 (Coordinated Universal Time) (A1). Legal status and post-grant events are not shown on this page.
What related patents are in patentsdb?
We list 8 related publications on this page (citations in our corpus or others sharing the same primary CPC).