Patent Grant
11129557
This application claims the benefit of China Patent Application No. 201710400287.0, filed May 31, 2017, the content of which is herein incorporated by reference in its entirety.
Embodiments herein relate to implantable chemical sensors for detecting a physiological analyte and medical devices including the same.
Implantable medical devices (IMDs) are often used to provide treatment or therapy to patients. Certain physiological analytes impact many of the problems that IMDs are designed to treat. As one example, potassium ion concentrations can affect a patient's cardiac rhythm. Therefore, medical professionals frequently evaluate physiological potassium ion concentration when diagnosing a cardiac rhythm problem. However, measuring physiological concentrations of analytes, such as potassium, generally requires drawing blood from the patient. Blood draws are commonly done at a medical clinic or hospital and therefore generally require the patient to physically visit a medical facility. As a result, despite their significance, physiological analyte concentrations are frequently measured only sporadically.
Embodiments herein relate to chemical sensors for detecting a physiological analyte.
In a first aspect, an implantable medical device including a chemical sensor is provided. The chemical sensor can be configured to detect an ion concentration in a bodily fluid. The chemical sensor can include a sensing element. The sensing element can include an outer barrier layer forming a top, a bottom, and opposed sides of the sensing element. The top of the outer barrier layer can be created from a polymeric matrix permeable to physiological analytes. An active agent can be disposed within the top of the outer barrier layer, the active agent having anti-inflammatory effects. The chemical sensor can include an optical excitation assembly configured to illuminate the sensing element. The chemical sensor can also include an optical detection assembly configured to receive light from the sensing element.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a second aspect, the bottom and opposed sides of the outer barrier layer can include or be a polymeric matrix permeable to sodium ions, potassium ions, hydronium ions, urea and creatinine.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a third aspect, the bottom and opposed sides of the outer barrier layer can include or be a material that is impermeable to sodium ions, potassium ions, and hydronium ions.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a fourth aspect, the chemical sensor is coupled to the implantable housing and the implantable housing defines a recessed pan into which the sensing element fits.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a fifth aspect, the implantable housing defines an aperture occluded by a transparent member, the aperture disposed at the bottom of the recessed pan, the sensing element in optical communication with the excitation assembly and the detection assembly through the transparent member.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a sixth aspect, an aqueous solution is disposed within at least a portion of the sensing element, aqueous solution including potassium ions at a concentration from about 3.0 to about 6.0 mmol/L.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a seventh aspect, the outer barrier layer surrounds an interior volume and the chemical sensor further includes active-agent releasing particles disposed within the interior volume of the outer barrier layer.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in an eighth aspect, the outer barrier layer surrounds an interior volume and the active-agent releasing particles include a first particle type configured to release an anti-inflammatory agent during a first period of time and a second particle type configured to release an angiogenic agent after the passage of the first period of time.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a ninth aspect, the outer barrier layer surrounds an interior volume and the sensing element further includes a first indicator bead and a second indicator bead disposed within the interior volume.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a tenth aspect, the active agent is or includes a corticosteroid.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in an eleventh aspect, the polymeric matrix includes a polymer selected from the group consisting of hydroxyethylmethacrylate, cellulose, polyvinyl alcohol, dextran, polyurethanes, quaternized polystyrenes, sulfonated polystyrenes, polyacrylamides, polyhydroxyalkyl acrylates, polyvinyl pyrrolidones, polyamides, polyesters, and mixtures and copolymers thereof.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a twelfth aspect, the polymeric matrix is or includes poly hydroxyethylmethacrylate.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a thirteenth aspect, the device includes an opaque cover layer disposed on the top side of the sensing element, the opaque cover layer including an ion permeable polymeric matrix.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a fourteenth aspect, the chemical sensor is configured to detect an ion selected from the group consisting of potassium, sodium, chloride, calcium, magnesium, lithium and hydronium.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a fifteenth aspect, the excitation assembly includes a light source, the light source comprising a light emitting diode.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a sixteenth aspect, the detection assembly includes a component selected from the group consisting of a photodiode, a phototransistor, a charge-coupled device (CCD), a junction field effect transistor (JFET) optical sensor, a complementary metal-oxide semiconductor (CMOS) optical sensor, an integrated photo detector integrated circuit, and a light to voltage converter.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in a seventeenth aspect, an implantable medical device with a chemical sensor is included. The chemical sensor can be configured to detect an ion concentration in a bodily fluid. The chemical sensor can include a sensing element. The sensing element can include an outer barrier layer forming a top, a bottom, and opposed sides of the sensing element. The top of the outer barrier layer can be created from a polymeric matrix permeable to physiological analytes. The chemical sensor can include an optical excitation assembly configured to illuminate the sensing element. The chemical sensor can also include an optical detection assembly configured to receive light from the sensing element. The chemical sensor can also include a drug-eluting material with an active agent disposed therein positioned around the opposed sides of the sensing element. The active agent can include an active agent having anti-inflammatory effects.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in an eighteenth aspect, the drug-eluting material with an active agent disposed therein forms a ring around the sensing element.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in an nineteenth aspect, the drug-eluting material with an active agent disposed therein forms one or more discrete depots around the sensing element.
In addition to one or more of the preceding or following aspects, or in the alternative to some aspects, in an twentieth aspect, an active agent is disposed within a portion of the sensing element.
This summary is an overview of some of the teachings of the present application and is not intended to be an exclusive or exhaustive treatment of the present subject matter. Further details are found in the detailed description and appended claims. Other aspects will be apparent to persons skilled in the art upon reading and understanding the following detailed description and viewing the drawings that form a part thereof, each of which is not to be taken in a limiting sense. The scope herein is defined by the appended claims and their legal equivalents.
Aspects may be more completely understood in connection with the following drawings, in which:
While embodiments are susceptible to various modifications and alternative forms, specifics thereof have been shown by way of example and drawings, and will be described in detail. It should be understood, however, that the scope herein is not limited to the particular embodiments described. On the contrary, the intention is to cover modifications, equivalents, and alternatives falling within the spirit and scope herein.
Medical professionals frequently need to evaluate chemical analyte concentrations of a patient when assessing the patient's condition and/or diagnosing a problem. However, measuring physiological concentrations of analytes, such as potassium amongst others, generally requires drawing blood from the patient. Blood draws are commonly done at a medical clinic or hospital and therefore generally require the patient to physically visit a medical facility. As a result, despite their significance, physiological analyte concentrations are frequently measured only sporadically.
Implanted chemical sensors offer the promise of being able to gather data on analyte concentrations even while a patient is away from a medical treatment facility. For example, implanted chemical sensors can measure analyte concentrations continuously or semi-continuously providing a far richer data set for a medical professional to evaluate.
However, implanted chemical sensors can be hindered in their ability to function properly over a relatively long period of time. For example, a patient's foreign body response can result in the infiltration by fibroblasts which multiply and lay down collagen that begins to form an avascular connective tissue envelope or “pocket”. This process can continue for months and can result in the complete encasement of the chemical sensor and/or medical device in an avascular pocket with walls that are 50 μm to 200 μm thick. This avascular pocket can adversely affect the functioning of the medical device.
Embodiments herein, however, can include elute an active agent in order to attenuate the foreign body response and prevent or reduce the thickness of the avascular pocket. Improving the local communication between sensor and physiologic environment.
Referring now to
It will be appreciated that chemical sensor 106 can be positioned at any location along IMD 100, including along the implantable housing 102 and along the header 104. The IMD 100 can take on various dimensions. In a particular embodiment herein it can be approximately 2 to 3 inches in length, 0.4 to 0.6 inches wide, and 0.15 to 0.35 inches thick. However, in some embodiments, the IMD 100 can be about 0.25, 0.5, 1.0, 2.0, 3.0, 4.0, or 5.0 inches in length. In some embodiments the length can be in a range wherein any of the foregoing lengths can serve as the upper or lower bound of the range, provided that the upper bound is greater than the lower bound. In some embodiments, the IMD 100 can be about 0.25, 0.5, 0.75, 1.0, or 2.0 inches in width. In some embodiments the length can be in a range wherein any of the foregoing widths can serve as the upper or lower bound of the range, provided that the upper bound is greater than the lower bound. In some embodiments, the IMD 100 can be about 0.10, 0.25, 0.50, 0.75 or 1.0 inches thick. In some embodiments the thickness can be in a range wherein any of the foregoing thicknesses can serve as the upper or lower bound of the range, provided that the upper bound is greater than the lower bound.
Referring now to
Referring now to
The sensing element 202 can include an outer barrier layer 306 formed, in full or in part, from a permeable material, such as an ion permeable polymeric matrix material. Exemplary materials for the outer barrier layer 306 are described in greater detail below. Outer barrier layer 306 can form a top 308, a bottom 310, and opposed sides 312 and 314 to surround an interior volume 320 of sensing element 202. Bottom 310 and opposed sides 312 and 314 of outer barrier layer 306 will be discussed in more detail below in reference to
In will be appreciated, however, that bottom 310 may or may not be a discrete layer. For example, in some embodiments, bottom 310 and the transparent member 318 may be fused with different material or fused as one layer with same type of material.
The implantable housing 102 can include a recessed pan 316 into which the sensing element 202 fits. In some embodiments, the top of the recessed pan 316 can be substantially flush with the top of the sensing element 202.
In some embodiments, implantable housing 102 can define an aperture occluded by a transparent member 318. The transparent member 318 can be a glass (including but not limited to borosilicate glasses), a polymer or other transparent material. The aperture can be disposed at the bottom of the recessed pan 316. The aperture can provide an interface allowing for optical communication between sensing element 202 and the optical excitation 302 and optical detection 304 assemblies.
It will be appreciated that outer barrier layer, or portions thereof such as the bottom 310, can be made from a transparent polymer matrix material to allow for optical communication between the sensing element 202 and optical excitation 302 and optical detection 304 assemblies.
The optical excitation assembly 302 can be designed to illuminate the sensing element 202. Optical excitation assembly 302 can include a light source such as a light emitting diode (LED), vertical-cavity surface-emitting lasers (VCSELs), electroluminescent (EL) devices, and the like. Optical detection assembly 304 can include a component selected from the group consisting of a photodiode, a phototransistor, a charge-coupled device (CCD), a junction field effect transistor (JFET) optical sensor, a complementary metal-oxide semiconductor (CMOS) optical sensor, an integrated photo detector integrated circuit, a light to voltage converter, and the like. Optical excitation 302 and optical detection 304 assemblies are discussed in further detail below.
Referring now to
Referring now to
Referring now to
In particular,
The sensing element(s) 202 embodied herein can include an interior volume 320 and can also include various indicator beads for detecting an ion concentration of a bodily fluid when implanted in the body disposed within an interior volume 320. For example,
Beyond diffusion through the top, in some embodiments additional diffusion of physiological analytes is also possible through bottom 310 and opposing sides 312 and 314.
While
In some embodiments, the sensing element(s) 202 embodied herein can include an aqueous solution 706 disposed within the interior volume 320. In some embodiments, the aqueous solution 706 can include potassium ions at a concentration of about 3.0 to about 6.0 mmol/L. In some embodiments, the aqueous solution 706 can include potassium ions at a concentration of about 1.0, 2.0, 3.0, 4.0, 5.0, 6.0, 7.0, or 8.0 mmol/L. In some embodiments, the concentration of potassium ions in the aqueous solution 706 can be in a range between any of the foregoing multiples provided that the upper bound of the range is greater than the lower bound of the range.
It will be appreciated that some portions of the outer barrier layer can be formed of a different material, while in other embodiments the entire outer barrier layer is all formed of the same material.
As shown in
Referring now to
In some embodiments, it can be desirable to isolate the chemical sensor from ambient light that may otherwise enter the chemical sensor. Referring now to
In some embodiments, it may be desirably to ship the chemical sensor and/or medical device with the sensor pre-wetted (e.g., bathed in an aqueous solution). Referring now to
In some embodiments, the aqueous solution 1204 present in recessed pan 316 can also include potassium ions at a concentration of about 3.0 to about 6.0 mmol/L. In some embodiments, the aqueous solution 1204 can include potassium ions at a concentration of about 1.0, 2.0, 3.0, 4.0, 5.0, 6.0, 7.0, or 8.0 mmol/L. In some embodiments, the concentration of potassium ions in the aqueous solution 1204 can be in a range between any of the foregoing amounts provided that the upper bound of the range is greater than the lower bound of the range.
Seal 1202 can be removed from the chemical sensor 106 by a medical professional just prior to implantation. In some embodiments, seal 1202 can be non-porous to the passage of aqueous solutions. In some embodiments, seal 1202 can be made from a polymer such as polyethylene terephthalate (PET), polytetrafluoroethylene (PTFE), polyethylene, polystyrene, and the like. In some embodiments, the seal 1202 can be made from a foil, such as a metal foil. In some embodiments, the seal 1202 can be made from a radiopaque material.
Referring now to
Implantable housing 102 can define an interior volume 1304 that in some embodiments is hermetically sealed off from the area 1306 outside of IMD 100. The IMD 100 can include circuitry 1308. Circuitry 1308 can include various components, such as components 1310, 1312, 1314, 1316, 1318, and 1320. In some embodiments, these components can be integrated and in other embodiments these components can be separate. In some embodiments, the components can include one or more of a microprocessor, memory circuitry (such as random access memory (RAM) and/or read only memory (ROM)), recorder circuitry, telemetry circuitry, chemical sensor interface circuitry, power supply circuitry (which can include one or more batteries), normalization circuitry, chemical sensor control circuitry, and the like. In some embodiments recorder circuitry can record the data produced by the chemical sensor and record time stamps regarding the same. In some embodiments, the circuitry can be hardwired to execute various functions, while in other embodiments the circuitry can be implemented as instructions executing on a microprocessor or other computation device.
A telemetry interface 1322 can be provided for communicating with external devices such as a programmer, a home-based unit, and/or a mobile unit (e.g., a cellular phone, portable computer, etc.). In some embodiments telemetry interface 1322 can be provided for communicating with implanted devices such as a therapy delivery device (e.g. a pacemaker, cardiovertor-defibrillator) or monitoring-only device (e.g. an implantable loop recorder). In some embodiments, the circuitry can be implemented remotely, via either near-field, far-field, conducted, intra-body or extracorporeal communication, from instructions executing on any of the external or the implanted devices, etc. In some embodiments, the telemetry interface 1322 can be located within implantable housing 102. In some embodiments, the telemetry interface 1322 can be located in header 104.
The optical excitation 302 and optical detection 304 assemblies of the chemical sensor 106 can be in electrical communication with the circuitry 1308 within the interior volume 1304. In some embodiments, the control circuitry 1308 is configured to selectively activate the optical excitation 302 and optical detection 304 assemblies of the chemical sensor 106.
Referring now to
Ion-Permeable Polymeric Matrix Materials
As referenced above, the outer barrier layer of the sensing element can be formed of an ion-permeable polymeric matrix material in some embodiments. Suitable polymers for use as the ion-permeable polymeric matrix material can include, but are not limited to polymers forming a hydrogel. Hydrogels herein can include homopolymeric hydrogels, copolymeric hydrogels, and multipolymer interpenetrating polymeric hydrogels. Hydrogels herein can specifically include nonionic hydrogels. In some embodiments, hydrogels herein can be prepared from polymerization of various monomers or macromers including one or more of 2-hydroxyethyl methacrylate (HEMA), 2-hydroxypropyl methacrylate (HPMA), acrylamide, acrylic acid, N-isopropylacrylamide (NIPAm), methoxyl polyethylene glycol monoacrylate (PEGMA), and the like. In some embodiments, polymers can include, but are not limited to polyhydroxyethyl methacrylate (HEMA), cellulose, polyvinyl alcohol, dextran, polyacrylamides, polyhydroxyalkyl acrylates, polyvinyl pyrrolidones, and mixtures and copolymers thereof. In some embodiments, suitable polymers for use with the ion-permeable polymeric matrix described herein include those that are transparent.
Active Agents
The active agent can be any drug or bioactive agent which can serve as a useful therapeutic, prophylactic, or even diagnostic agent when released into the patient. Exemplary bioactive agents include, but are not limited to, the following: an anti-inflammatory; anti-proliferative; anti-arrhythmic; anti-migratory; anti-neoplastic; antibiotic; anti-restenotic; anti-coagulation; anti-infectives; anti-oxidants; anti-macrophagic agents (e.g., bisphosphonates); anti-clotting (e.g., heparin, coumadin, aspirin); anti-thrombogenic; immunosuppressive agents; an agent that promotes healing; steroids (e.g., a glucocorticosteroid)); and combinations thereof.
Suitable active agents for use with the embodiments herein can specifically include, but are not limited to anti-inflammatory agents. In some embodiments, suitable anti-inflammatory agents can include steroids generally and, in specific, corticosteroids. In some embodiments, the anti-inflammatory agent can include ketorolac, dexamethasone, hydrocortisone, prednisolone, methylprednisolone, indomethacin, diclofenac, ketoprofen, piroxicam, metamizol magnesium and the like. In some embodiments, anti-inflammatory agents can be configured to be eluted shortly after implantation of the device.
In some embodiments, suitable active agents can also include angiogenic agents, to promote the in-growth of capillaries. In some embodiments, angiogenic agents can be configured to be eluted at a later time (e.g., following elution of an anti-inflammatory at an earlier point in time) to promote the ingrowth of capillaries to the chemical sensor.
In some embodiments, suitable angiogenic agents can include growth factors such as vascular endothelial growth factor (VEGF), fibroblast growth factor (FGF), platelet-derived growth factor (PDGF), and the like. In some embodiments, the additional active agents can include immobilized heparin to prevent blot clot formation.
Active agents herein can be in various forms including in a solution, as a suspension, as a particulate, or the like.
Active Agent Eluting Materials
Various embodiments herein can include an active agent eluting material or matrix. The active agent eluting material can serve to provide a matrix into which the active agent can be disposed and from which the active agent can elute after the chemical sensor and/or medical device is implanted within the body of a patient. However, in other embodiments, the active agent can be disposed with or without an eluting material or matrix and in or on portions of the sensing element or other portions of the device including, but not limited to, the top, bottom, or opposed sides of the barrier layer, in depots adjacent to the sensing element, in a channel around the sensing element, above the sensing element, below the sensing element, to the sides of the sensing element, inside of the sensing element and the like.
The active agent eluting material can include, but is not limited to, one or more of the following polymers: SOLEF® (SOLEF® 21508 polymer); polyvinylidene-hexafluoropropylene or poly(VF2-co-HFP) from Solvay, Brussels, Belgium; acetoxy, cure, Room-Temperature-Vulcanizing (RTV) silicone elastomers; UV curable silicone; UV curable polymer; platinum catalyzed addition cure liquid silicone rubber; styrene isobutylene styrene (SIBS); peroxide cure silicone rubber; Nafion; silicone (including LSR), polymers based on the structural unit R2SiO, where R is an organic group; medical adhesives; cyanoacrylates; Rehau 1511; ethylene vinyl alcohol (E/VAL; a thermoplastic polymer); polyethylene glycol (PEG); polyvinyl alcohol; polyvinyl propylene; hyaluronic acid; polyacrylamides; polycaprolactone, polylactide (PLA); polyglycolide (PGA); poly(lactide-co-glycolide) (PLGA); polyurethane; polymethylmethacrylates; polyethylene; polyvinylpyrrolidone; polyacrylic acid; poly(2-hydroxyethyl methacrylate); pHEMA polyacrylamide; polyethylene-co-vinyl acetate; polyanhydrides; polyorthoesters; polyimides; polyamides; polyanhydrides; polyetherketones; polyaryletherketones; polysiloxane urethanes; polyisobutylene copolymers; and copolymers and combinations thereof.
The active agent eluting material can be in various forms including, but not limited to, depots, spots, discrete particles, layers, as a filling, as a particulate within other materials herein such as materials forming at least a portion of the barrier layer, and the like.
Optical Excitation and Detection Assemblies
In some embodiments, the optical excitation assembly 302 can include solid state light sources such as GaAs, GaAlAs, GaAlAsP, GaAlP, GaAsP, GaP, GaN, InGaAlP, InGaN, ZnSe, or SiC light emitting diodes or laser diodes that excite the sensing element(s) 202 at or near the wavelength of maximum absorption for a time sufficient to emit a return signal. However, it will be understood that in some embodiments the wavelength of maximum absorption/reflection varies as a function of concentration in the colorimetric sensor.
In some embodiments, the optical excitation assembly 302 can include other light emitting components including incandescent components. In some embodiments, the optical excitation assembly 302 can include a waveguide. The optical excitation assembly 302 can also include one or more bandpass filters, high pass filter, low pass filter, antireflection elements, and/or focusing optics.
In some embodiments, the optical excitation assembly 302 can include a plurality of LEDs with bandpass filters, each of the LED-filter combinations emitting at a different center frequency. According to various embodiments, the LEDs can operate at different center-frequencies, sequentially turning on and off during a measurement, illuminating the sensing element 202. As multiple different center-frequency measurements are made sequentially, a single unfiltered detector can be used in some embodiments. However, in some embodiments, a polychromatic source can be used with multiple detectors that are each bandpass filtered to a particular center frequency.
The sensing element 202 can include one or more types of indicator beads having embedded therein various types of ion selective sensors. Physiological analytes of interest can diffuse into and out of the sensing element 202 and bind with an ion selective sensor to result in a fluorimetric or colorimetric response. Reference analytes can similarly diffuse into and out of the sensing element 202 and serve as a control sample. Exemplary ion selective sensors are described more fully below.
The optical detection assembly 304 can be configured to receive light from the sensing element 202. In an embodiment, the optical detection assembly 304 can include a component to receive light. By way of example, in some embodiments, the optical detection assembly 304 can include a charge-coupled device (CCD). In other embodiments, the optical detection assembly 304 can include a photodiode, a junction field effect transistor (JFET) type optical sensor, or a complementary metal-oxide semiconductor (CMOS) type optical sensor. In some embodiments, the optical detection assembly 304 can include an array of optical sensing components. In some embodiments, the optical detection assembly 304 can include a waveguide. The optical detection assembly 304 can also include one or more bandpass filters and/or focusing optics. In some embodiments, the optical detection assembly 304 can include one or more photodiode detectors, each with an optical bandpass filter tuned to a specific wavelength range.
The optical excitation and detection assemblies, 302 and 304, respectively, can be integrated using bifurcated fiber-optics that direct excitation light from a light source to one or more sensing elements 202, or simultaneously to sensing element(s) 202 and a reference channel. Return fibers can direct emission signals from the sensing element(s) 202 and the reference channels to one or more optical detector assemblies 304 for analysis by a processor, such as a microprocessor. In some embodiments, the optical excitation and detection assemblies are integrated using a beam-splitter assembly and focusing optical lenses that direct excitation light from a light source to the sensing element and direct emitted or reflected light from the sensing element to an optical detector for analysis by a processor.
Ion Selective Sensors
In accordance with the embodiments herein, sensing elements 202 can include one or more ion selective sensors. Ion selective sensors may either rely on surface phenomena or on concentration changes inside the bulk of a phase. Ion selective sensors can include optical sensors, including both non-carrier optical sensors and carrier-based optical sensors, and ion-selective electrodes (ISEs). In some embodiments, the ion selective sensor is fluorimetric, and can include a complexing moiety and a fluorescing moiety. Fluorimetric ion selective sensors can exhibit differential fluorescent intensity based upon the complexing of an analyte to a complexing moiety. In some embodiments, the ion selective sensor can be colorimetric, and can include a complexing moiety and a colorimetric moiety. Colorimetric ion selective sensors can exhibit differential light absorbance based upon the complexing of an analyte to a complexing moiety.
In some embodiments, the ion selective sensor comprises a non-carrier or carrier-based fluorescent or colorimetric ionophoric composition that comprises a complexing moiety for reversibly binding an ion to be analyzed, and a fluorescing or colorimetric moiety that changes its optical properties as the complexing agent binds or releases the ion. The complexing agents of the invention can optionally be appended with one or more organic substituents chosen to confer desired properties useful in formulating the ion sensing composition. By way of example, the substituents can be selected to stabilize the complexing agent with respect to leaching into the solution to be sensed, for example, by incorporating a hydrophobic or polymeric tail or by providing a means for covalent attachment of the complexing agent to a polymer support within the ion selective sensor.
In some embodiments, the sensing element can include ion selective sensors such as an ionophore or a fluorionophore. Suitable ionophores for use with the embodiments herein can include, but not be limited to, sodium specific ionophores, potassium specific ionophores, calcium specific ionophores, magnesium specific ionophores, and lithium specific ionophores. Suitable fluorionophores for use with the embodiments herein can include, but not be limited to, lithium specific fluoroionophores, sodium specific fluoroionophores, and potassium specific fluoroionophores.
Exemplary ion selective sensors and methods for their use are disclosed in commonly assigned U.S. Pat. No. 7,809,441, the contents of which is herein incorporated by reference in its entirety.
The embodiments described herein are not intended to be exhaustive or to limit the invention to the precise forms disclosed in the following detailed description. Rather, the embodiments are chosen and described so that others skilled in the art can appreciate and understand the principles and practices. Aspects have been described with reference to various specific and preferred embodiments and techniques. However, it should be understood that many variations and modifications may be made while remaining within the spirit and scope herein.
It should be noted that, as used in this specification and the appended claims, the singular forms “a,” “an,” and “the” include plural referents unless the content clearly dictates otherwise. Thus, for example, reference to a composition containing “a compound” includes a mixture of two or more compounds. It should also be noted that the term “or” is generally employed in its sense including “and/or” unless the content clearly dictates otherwise.
It should also be noted that, as used in this specification and the appended claims, the phrase “configured” describes a system, apparatus, or other structure that is constructed or configured to perform a particular task or adopt a particular configuration to. The phrase “configured” can be used interchangeably with other similar phrases such as arranged and configured, constructed and arranged, constructed, manufactured and arranged, and the like.
All publications and patent applications in this specification are indicative of the level of ordinary skill in the art to which this invention pertains. All publications and patent applications are herein incorporated by reference to the same extent as if each individual publication or patent application was specifically and individually indicated by reference. Nothing herein is to be construed as an admission that the inventors are not entitled to antedate any publication and/or patent, including any publication and/or patent cited herein.
| Number | Date | Country | Kind |
|---|---|---|---|
| 201710400287.0 | May 2017 | CN | national |
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| Number | Date | Country | |
|---|---|---|---|
| 20180344218 A1 | Dec 2018 | US |
