US20030143726A1 - Biosensor involving the use of optically sensitive moieties - Google Patents
Biosensor involving the use of optically sensitive moietiesDownload PDFInfo
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- US20030143726A1 US20030143726A1US10/358,176US35817603AUS2003143726A1US 20030143726 A1US20030143726 A1US 20030143726A1US 35817603 AUS35817603 AUS 35817603AUS 2003143726 A1US2003143726 A1US 2003143726A1
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- C07K—PEPTIDES
- C07K14/00—Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof
- C07K14/195—Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof from bacteria
- C07K14/36—Peptides having more than 20 amino acids; Gastrins; Somatostatins; Melanotropins; Derivatives thereof from bacteria from Actinomyces; from Streptomyces (G)
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- G01N33/48—Biological material, e.g. blood, urine; Haemocytometers
- G01N33/50—Chemical analysis of biological material, e.g. blood, urine; Testing involving biospecific ligand binding methods; Immunological testing
- G01N33/53—Immunoassay; Biospecific binding assay; Materials therefor
- G01N33/543—Immunoassay; Biospecific binding assay; Materials therefor with an insoluble carrier for immobilising immunochemicals
- G01N33/54366—Apparatus specially adapted for solid-phase testing
- G01N33/54373—Apparatus specially adapted for solid-phase testing involving physiochemical end-point determination, e.g. wave-guides, FETS, gratings
- G01N33/5438—Electrodes
- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
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- Y10S436/00—Chemistry: analytical and immunological testing
- Y10S436/806—Electrical property or magnetic property
Definitions
- the present inventionrelates to biosensors which include or are fabricated using optically sensitive moieties.
- Biosensorshave been constructed comprising biomembranes which are a double layer of closely packed amphiphilic lipid molecules.
- the molecules of these bilayersexhibit the random motions characteristic of the liquid phase, in which the hydrogen tails of the lipid molecules have sufficient mobility to provide a soft, flexible, viscid surface.
- the moleculescan also diffuse sideways freely within their own monolayer so that two neighbouring lipids in the same monolayer exchange places with each other about once every microsecond, while the lipid molecules in opposite monolayers exchange places on the average of one a year.
- Ionophoresa class of molecules, called ionophores, which facilitate the transport of ions across these membranes.
- Ion channelsare a particular form of ionophore, which as the term implies, are channels through which ions may pass through membranes.
- a favoured ionophoreis gramicidin A which forms aqueous channels in the membrane. Examples of such biosensors are disclosed in the following International Patent Applications, the disclosures of which are incorporated herein by cross reference:
- PCT/AU92/00132PCT/AU93/00509, PCT/AU93/00620,
- PCT/AU94/00202PCT/AU95/00763, PCT/AU96/00304,
- the first of these referencesdiscloses receptor molecules conjugated with a support that is remote from the receptor site.
- the supportmay be a lipid head group, a hydrocarbon chain, a cross-linkable molecule or a membrane protein.
- the inner level of the membranemay be adjacent a solid surface with groups reactive with the solid surface, and spaced from the surface to provide a reservoir region as disclosed in U.S. Pat. No. 5,401,378.
- Biosensors based on ion channels or ionophores contained within lipid membranes tethered to or deposited onto metal electrodesare disclosed in Australian Patent 623,747 and U.S, Pat. No. 5,234,566. Those references disclose a membrane bilayer in which each layer has incorporated therein ionophores and in which the conductance of the membrane is dependent upon the presence or absence of an analyte.
- the disclosure of Australian Patent 623,747(incorporated herein by reference) describes various ionophore gating mechanisms termed local disruption gating. extended disruption gating, vertical disruption gating, and extended displacement gating mechanisms to modify the conductivity of the membrane in response to the presence of an analyte.
- an inner layer of the membrane(the layer closer to the solid electrode surface, if any) contains immobilized or tethered half membrane spanning ion channels which an outer layer contains more mobile half membrane spanning ion channels.
- One method for immobilising the ion channels of the inner layeris to employ a polymerisable lipid layer and then cross-link the molecules of the inner monolayer and the ionophore. The conductivity of the membrane is altered by the extent to which opposing half membrane spanning ion channels align to establish a membrane spanning channel for ion transmission across the membrane.
- local disruption gating receptor moleculesare linked to mobile ionophores in the outer layer that are aligned with tethered or immobilised ionophores in the inner layer.
- the introduction of an analyte particle that binds to two adjacent receptors in the outer layercauses the disruption of the orderly alignment of the membrane spanning ionophore.
- a loss of conductivityoccurs due to the deformation of the ionophores of the outer layer caused by the bonding of the analyte with the adjacent receptors.
- extended disruption gatingis similar, except that the displacement of the mobile ionophore is greater.
- extended disruption gatingthe binding of pairs of receptors to the same analyte particle cause the outer layer ionophores to move completely out of alignment with the inner layer ionophores.
- the mechanism of extended displacement gatingutilises two different receptors that bind to each other and are linked receptively to a half membrane ionophore and a membrane molecule.
- the binding of these two receptor molecules to each otherdisplaces the ionophore and disrupts conductivity.
- the analytecompetes with the second receptor for the binding site on the first receptor.
- the presence of the analytebreaks the bond between the two receptors and allows the half membrane ionophores to realign and provide an ion conductive path.
- Each of these mechanismshas in common that the binding of the analyte to the receptor molecule causes a change in the relationship between two half membrane spanning monomers such that the flow of ions across the membrane via the ionophores is allowed or prevented.
- biosensorsIn a number of sensing applications it is beneficial to incorporate within the one detection cell a positive or negative control to add to the utility of the biosensor. As will be recognised the fabrication of a biosensor having discrete areas of membrane which act as either a test area or control area can be very complex. The present inventors have developed methods by which such biosensors may be fabricated in a less complex manner using optically sensitive moieties.
- biosensorsIn a number of sensing applications it is beneficial to incorporate within the one detection cell a positive or negative control to add to the utility of the biosensor. As will be recognised the fabrication of a biosensor having discrete areas of membrane which act as either a test area or control area can be very complex. The present inventors have developed methods by which such biosensors may be fabricated in a less complex manner using optically sensitve moieties.
- the present inventionconsists in a method of fabricating a biosensor in which there is at least one discrete test and at least one discrete control zone, the method comprising the following steps:
- the methodfurther includes the following step:
- step (v)binding control ligands to the ion channels and membrane spanning lipid components after the ligands have been removed in step (iv).
- the membraneis rinsed between steps (iv) and (v).
- the present inventionconsists in a method of fabricating a biosensor in which there is at least one discrete test and at least one discrete control zone, the method comprising the following steps:
- the photocleavable linkersmay be any of a number of such molecules known in the art (eg see Pillai (1980)).
- the photoactivatable groupsmay be any number of such groups known in the art, such as, for example, photoactivatable biotins described by Pirrung (1996) or Cass (1996).
- the present inventionconsists in an improved biosensor, the biosensor comprising a membrane the conductance/impedance of which is altered by the presence or absence of an analyte and a conductive substrate, the membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers such that the membrane is tethered to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate, and ligands attached to the ion channels and membrane spanning lipids, the improvement comprising providing on at least one of the first and second half membrane spanning monomers or membrane spanning lipids a photoswitchable group derived from a compound in accordance with
- R 1represents 0 to about 3 groups where each is independently H or saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon;
- R 2represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon;
- Yrepresents H, saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or uinsubstituted C 1-4 hydrocarbon.
- R 6 , R 7 , R 8 , R 14 and R 15are each independently represent H, saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsatunted, substituted or unsubstituted CiA hydrocarbon or aryl;
- R 9is —C(O)X where X represents H, saturated or unsaturated, substituted or unsubstitited C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon, or OH, or OR 10 in which R 10 is alkyl, or NR 11 R 12 in which R 11 and R 12 are H, afkyl or taken together with N form a ring, or aryl or R 9 together with R 1 form a substituted or unsubstituted 5-6 member cyclic or heterocyclic ring;
- Zrepresents O or NR 13 R
- the compoundwill include a functional group at Y or R 9 such that the compound can be linked to at least one of the first and second half membrane spanning monomers or membrane spanning lipids.
- R 1represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon
- R 2represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon
- Xrepresents H, saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon, or aryl, or OH, or OR 10 in which R 10 is alkyl, or NR 11 R 12 in which R 11 and R 12 are H, alkyl or taken together with N form a ring
- Yrepresents H, or saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or
- R 13is H, saturated or unsaturated, substituted or unsubstituted C 1-10 hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C 1-4 hydrocarbon or aryl.
- FIG. 10Specific examples of suitable photoswitchable linkers that are suitable for use in the present invention are shown in FIG. 10.
- FIGS. 1 to 9are schematic representations of the biosensors of the presnt invention.
- FIG. 10shows the structure of some of the compounds of the present invention.
- FIG. 1An example of an improved biosensor in accordance with the invention is shown schematically in FIG. 1.
- the improved biosensorcan be advantageously used in the detection of an analyte.
- An exemplary protocol for use of this type of biosensoris as follows.
- the present inventionconsists in a method comprising the following steps:
- the photoswitchable binder to streptavidinis caged biotin, HABA or derivative thereof.
- the photoswitchable binderis caged biotin or a compound in accordance with Formula 1 above.
- the aim hereis to minimise the formation of any ga-SA-MSL linkages (i.e streptavidin gating).
- streptavidin gatingis reduced and thus the dynamic range is improved.
- step (v)the rinsing step can be avoided, meaning that additional SA in step (vi) need not be added.
- a tethered membrane assemblyis made with biotinylated MSL and gA bearing a photoswitchable group derived from a compound in accordance with Formula 1.
- a biotinylated antibody streptavidin complexis then introduced into the electrolyte solution.
- the light sourceis then switched on so that the antibody complex links to the biotinylated MSL but not to the photoswitchable group gA.
- the analyteis then added and continually stirred and allowed to incubate so that analyte liks to MSL via antibody streptavidin biotin complex. (Note at this point there is no crossluiking of MSL to gA or gA to gA because light is on).
- the solutionis then rinsed so that unlinked antibody is removed.
- An impedance measurementis then made which gives the channel on baseline. Impedance measurements continue and then the light is switched off.
- the time course of gatingis measured as gramicidin crosslinks to MSL via a photoswitchable group-streptavidin-biotin-antibody-analyte-antibody-biotin-streptavidin-photoswitchable group -MSL complex.
- the advantagesare improved dynamic range due to reduction of streptavidin gating and also an increase in sensitivity as the long incubation time required to crosslink the antibody to MSL no longer limits the rate of change of gating which is carried out rapidly after the crosslinking has occurred (this assumes that off times are significantly longer than on times). Further, analyte addition artifacts are avoided and thorough mixing can be carried out, and also this method is suitable for optically phase locked loop approaches.
- FIG. 4A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity is shown in FIG. 4.
- a tethered membrane assemblyis made with MSL and gA both bearing a photoswitchable group in accordance with the invention.
- a biotinylated antibody streptavidin complexis then introduced into the electrolyte solution.
- the light sourceis switched on so that the antibody complex is not bound to either MSL or gA.
- Analyteis added and continually stirred and allowed to incubate so that analyte crosslinks all antibody-streptavidin complexes. Impedance measurements then commence which gives the channel on baseline
- Impedance measurementscontinue and then the light is switched off whilst impedance measurements are made for a further period of time.
- the time course of gatingis measured as gramicidin crosslinks to MSL via a photoswitchable group -streptavidin-biotin-antibody-analyte-antibodv-biotin-streptavidin-biotin-MSL complex
- FIG. 5A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity is shown in FIG. 5.
- a method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity in a competition assay(such as depicted in FIG. 6) wherein non-specific effects are separated from the real gating response
- a tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a derivative of the required analyte and a photoswitchable group which binds to streptavidinis produced.
- a measurement of biosensor impedanceis made then the analyte is added.
- a second measurementis made then a light source is triggered on.
- a third measurement of the time course response to lightis made then the light source is triggered off.
- a fourth measurement of the time course response to the removal of lightis then made.
- the photoswitchable groupcould of course replace biotin.
- Such a groupmay be photoswitchable group or a derivative thereof.
- a method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity in a competition assay(such as depicted in FIG. 7) wherein any non-specific effects (caused during analyte addition) can be separated from the gating response.
- a tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a derivative of the required analyte and a photoswitchable group connected to a membrane spanning lipidis produced.
- a measurement of biosensor impedanceis then made prior to addition of analyte.
- Analyteis added and a second measurement is made.
- a light sourceis then triggered on and a third measurement of the time course response to light is made. The light source is then triggered off and a fourth measurement of the time course response to the removal is made.
- a tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a derivative of the required analyte and a photoswitchable tether to the bottom layer gramicidin (or other ion channel)is produced.
- a measurement of biosensor impedanceis made and the analyte is added.
- a second measurementis then made and a light source is triggered on.
- a third measurement of the time course response to lightis made then the light source is triggered off.
- a fourth measurement of the time course response to the removalis then made.
- a caged biotincould be used in place of a photoswitchable streptavidin ligand such as HABA (or a derivative) in the examples cited above, specifically those depicted in FIGS. 3,4, and 5 .
- a photoswitchable streptavidin ligandsuch as HABA (or a derivative)
- FIGS. 3,4, and 5Several caged biotin derivatives are known in the literature, such as those reported by Pirrung (1993, 1996). Such caged derivatives revert to biotin on irradiation with light and therefore cannot be switched between forms that bind streptavidin and forms that do not bind streptavidin.
- FIG. 9An additional example of the use of such caged biotin compounds is depicted in FIG. 9.
- streptavidinis added to the system, and attaches to biotin on the MSL4XB
- a biotinylated receptoris added to the system, and attaches to the SA on MSL4XB
- streptavidinis added to the system, and attaches to newly generated biotin (on the gramicidin)
- a biotinylated receptoris added to the system, and attaches to the SA on gramicidin
- the advantage of this manufacture processis that formation of gA-SA-MSL linkages (i.e. streptavidin gating) is minimised and thus the dynamic range is improved.
- a further advantageis that receptors can be selected to bind specifically at MSL4XB and the gramicidin derivative, which in turn may improve the response.
- the photoswitchable ligands of the general formulae 1 and 2are prepared by well known synthetic procedures. For example, the coupling of diazo aromatics with substituted phenols and their derivatives, has been well documented (Berwick 1972: Oku 1979; Weber 1994). It will be recognised that compounds derived from such a coupling reaction can be further functionalised. For example, a free hydroxyl group could be acylated or etherified using conventional synthetic methods. Representative examples of compounds prepared via these chemical synthetic pathways are depicted in FIG. 10.
- a photo-generatable derivative bf biotin(so called caged biotin) was prepared by a modification of the method of Pirrung et al ( Bioconj. Chem., 1996, 7, 317). This compound (9 mg) was dissolved in dichloromethane (5 ml) and treated with dicyclohexylcarbodiimide (DCC) (3 mg), N-hydroxy succinimide (NHS) (2 mg) and dimethylaminopyridine (0.2 mg).
- DCCdicyclohexylcarbodiimide
- NHSN-hydroxy succinimide
- dimethylaminopyridine0.2 mg
- the main fractionwas then purified by HPLC on a 40 mm ⁇ 200 mmn Waters Prep Nova-Pak® HR silica column (6 ⁇ m, 60 ⁇ ) eluting with dichloromethane-methanol-water (800:40:4) operating at a flow rate of 25 ml/min.
- the bond formationis very rapid and once formed, is unaffected by wide extremes of pH, temperature, organic solvents and other denaturing agents. Conditions which are usually sufficient for denaturing proteins fail to disassociate the avidin-biotin complex.
- a reporter moleculecould be bound to streptavidin covalently, or biotinylated and attached to streptavidin via the streptavidin-biotin interaction. Selective activation and functionalisation of this complex is targeted in this group of experiments.
- biotinthat is not active in the native state (i.e. will not bind to streptavidin) but can be activated by UV irradiation to bind streptavidin.
- This photoactivable form of biotinhas been conjugated with gramicidin and used as an essential component of the bilayer membrane for targeting chemistries using streptavidin-biotin complex.
- the gold electrodeswere built on commercially available glass microscope slides. The glass slides were cleaned for 2 hours in the glass cleaning solution “Extran 300”, rinsed several times with copious volumes of deionised water and dried in a stream of nitrogen in clean room conditions. The metal deposition was carried out using an Edwards evaporation unit. An adhesion layer of chromium ( ⁇ 20 nM) was deposited fouowed by a layer of gold (100 nM. One side of the glass slides was fully coated with metal. The metal treated glass slides were removed from the evaporator and quickly immersed in an ethanolic solution of monolayer components for an hour (AM300), rinsed profusely in ethanol and preserved in ethanol. These electrodes were stored at 4° C. for 24 hours before assembling the second layer of the membrane.
- AM300ethanolic solution of monolayer components
- the photoactivable biotic in its native formhas a molecular weight of 686 d and has a molecular weight of 2.809 kd in the form of gAxx[B].
- This compoundwas dissolved in ethanol to prepare a 2 mM solution (5.5 mg in 1.958 ml) and further diluted to a 10 uM solution.
- An aliquot of the gAxx[B] solutionwas activated by irradiating the solution at 350 nM for a period of 20 minutes.
- Second layer membrane solutionswere prepared with 3 mM lipids DPEPC (1,2-di(3RS, 7R, 11R-phytanyl)-glycero-3-phosphocholine) and GDPE (1,2-di(3RS, 7R, 11R-phytanyl)-glycerol) in 7:3 ratio and three types of gA5xB.
- the first solutionwas prepared with gA5xB (see FIG. 11), the second with the inactive form of photoactivatable gAxx[B] and the third solution with the activated form of photoactivatable gAxx[B].
- Streptavidinwas diluted in PBS to a concentration of 0.1 mg/ml.
- the matched pair of biotinylated Thyroid Stimulating Hormone (TSH) Fabs(E20650 M and E45650 M) was combined in equal molar ratio to give a 50 ug/ml solution in PBS.
- TSH analytewas diluted in chilled PBS to prepare a 2.5 nM solution.
- the monolayer AM300was deposited on metallised glass electrodes as per established protocol.
- the electrodeswere assembled into biosensor blocks.
- the second layer solutionwas added manually (15 ⁇ l per cell) and washed five times with PBS to assemble the bilayer membrane.
- the fully assembled blockshad the following second layers:
- Block 1Row A (cells 1-8) with a ratio of 40 k: 1 standard gA5xB Row B (cells 9-16) with a ratio of 40 k: 1 inactive for of gAxx[B]
- Block 3Row A(cells 1-8) with standard gA5xB as in blocks 1 and 2 Row B (cells 9-16) with the activated form of gAxx[B].
- a second group of 2 blockswere assembled with the inactive form of gAxx[B] and the cells were exposed to UV irradiation.
- the exposure time for pairs of cellswas varied to study the effects of time length of exposure and select the most effective time period for future experiments. Exposure times down to one minute were found to be effective.
- Cells 1-8used the standard composition of second layer as a positive control for comparison and these responded to streptavidin.
- Cells 9-16 using the inactive form of gAxx[B]showed no response when exposed to streptavidin.
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Abstract
Description
- The present invention relates to biosensors which include or are fabricated using optically sensitive moieties.[0001]
- Biosensors have been constructed comprising biomembranes which are a double layer of closely packed amphiphilic lipid molecules. The molecules of these bilayers exhibit the random motions characteristic of the liquid phase, in which the hydrogen tails of the lipid molecules have sufficient mobility to provide a soft, flexible, viscid surface. The molecules can also diffuse sideways freely within their own monolayer so that two neighbouring lipids in the same monolayer exchange places with each other about once every microsecond, while the lipid molecules in opposite monolayers exchange places on the average of one a year.[0002]
- These membranes may incorporate a class of molecules, called ionophores, which facilitate the transport of ions across these membranes. Ion channels are a particular form of ionophore, which as the term implies, are channels through which ions may pass through membranes. A favoured ionophore is gramicidin A which forms aqueous channels in the membrane. Examples of such biosensors are disclosed in the following International Patent Applications, the disclosures of which are incorporated herein by cross reference:[0003]
- PCT/AU88/00273, PCT/AU89/00352, PCT/AU90/00025,[0004]
- PCT/AU92/00132, PCT/AU93/00509, PCT/AU93/00620,[0005]
- PCT/AU94/00202, PCT/AU95/00763, PCT/AU96/00304,[0006]
- PCT/AU96/00368, PCT/AU96/00369 and PCT/AU96/00482.[0007]
- The first of these references discloses receptor molecules conjugated with a support that is remote from the receptor site. The support may be a lipid head group, a hydrocarbon chain, a cross-linkable molecule or a membrane protein.[0008]
- The inner level of the membrane may be adjacent a solid surface with groups reactive with the solid surface, and spaced from the surface to provide a reservoir region as disclosed in U.S. Pat. No. 5,401,378.[0009]
- Biosensors based on ion channels or ionophores contained within lipid membranes tethered to or deposited onto metal electrodes are disclosed in Australian Patent 623,747 and U.S, Pat. No. 5,234,566. Those references disclose a membrane bilayer in which each layer has incorporated therein ionophores and in which the conductance of the membrane is dependent upon the presence or absence of an analyte. The disclosure of Australian Patent 623,747 (incorporated herein by reference) describes various ionophore gating mechanisms termed local disruption gating. extended disruption gating, vertical disruption gating, and extended displacement gating mechanisms to modify the conductivity of the membrane in response to the presence of an analyte. In each of those gating mechanisms an inner layer of the membrane (the layer closer to the solid electrode surface, if any) contains immobilized or tethered half membrane spanning ion channels which an outer layer contains more mobile half membrane spanning ion channels. One method for immobilising the ion channels of the inner layer is to employ a polymerisable lipid layer and then cross-link the molecules of the inner monolayer and the ionophore. The conductivity of the membrane is altered by the extent to which opposing half membrane spanning ion channels align to establish a membrane spanning channel for ion transmission across the membrane.[0010]
- In local disruption gating receptor molecules are linked to mobile ionophores in the outer layer that are aligned with tethered or immobilised ionophores in the inner layer. The introduction of an analyte particle that binds to two adjacent receptors in the outer layer causes the disruption of the orderly alignment of the membrane spanning ionophore. In the case of local disruption gating a loss of conductivity occurs due to the deformation of the ionophores of the outer layer caused by the bonding of the analyte with the adjacent receptors.[0011]
- The mechanism of extended disruption gating is similar, except that the displacement of the mobile ionophore is greater. In extended disruption gating the binding of pairs of receptors to the same analyte particle cause the outer layer ionophores to move completely out of alignment with the inner layer ionophores.[0012]
- The mechanism of vertical disruption gating is also similar. In that case the presence of the analyte particle bound to two receptor molecules causes a separation of the two layers that disrupts the continuity of the ion channel across the membrane.[0013]
- The mechanism of extended displacement gating utilises two different receptors that bind to each other and are linked receptively to a half membrane ionophore and a membrane molecule. The binding of these two receptor molecules to each other displaces the ionophore and disrupts conductivity. The analyte competes with the second receptor for the binding site on the first receptor The presence of the analyte breaks the bond between the two receptors and allows the half membrane ionophores to realign and provide an ion conductive path. Each of these mechanisms has in common that the binding of the analyte to the receptor molecule causes a change in the relationship between two half membrane spanning monomers such that the flow of ions across the membrane via the ionophores is allowed or prevented.[0014]
- In a number of sensing applications it is beneficial to incorporate within the one detection cell a positive or negative control to add to the utility of the biosensor. As will be recognised the fabrication of a biosensor having discrete areas of membrane which act as either a test area or control area can be very complex. The present inventors have developed methods by which such biosensors may be fabricated in a less complex manner using optically sensitive moieties.[0015]
- In a number of sensing applications it is beneficial to incorporate within the one detection cell a positive or negative control to add to the utility of the biosensor. As will be recognised the fabrication of a biosensor having discrete areas of membrane which act as either a test area or control area can be very complex. The present inventors have developed methods by which such biosensors may be fabricated in a less complex manner using optically sensitve moieties.[0016]
- Accordingly in a first aspect the present invention consists in a method of fabricating a biosensor in which there is at least one discrete test and at least one discrete control zone, the method comprising the following steps:[0017]
- (i) providing a conductive substrate:[0018]
- (ii) forming a membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers such that the membrane is tethered to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate;[0019]
- (iii) linking a ligand reactive with an analyte of interest to the ion-channel and linking a ligand reactive with an analyte of interest to the membrane spanning lipid components of the tethered membrane via photocleavable linkers; and[0020]
- (iv) exposing the membrane to a focused light source to cleave the photocleavable linkers thereby releasing the ligands from the ion-channel and membrane spanning lipid components in discrete areas of the membrane.[0021]
- In a preferred embodiment the method further includes the following step:[0022]
- (v) binding control ligands to the ion channels and membrane spanning lipid components after the ligands have been removed in step (iv).[0023]
- In a further preferred embodiment the membrane is rinsed between steps (iv) and (v).[0024]
- In a second aspect the present invention consists in a method of fabricating a biosensor in which there is at least one discrete test and at least one discrete control zone, the method comprising the following steps:[0025]
- (i) providing a conductive substrate;[0026]
- (ii) forming a membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers such that the membrane is tethered to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate;[0027]
- (iii) providing on the ion channels and membrane spanning lipids a photoactivatable group which when illuminated will bind a receptor:[0028]
- (iv) illuminating discrete areas of the membrane and linking a ligand reactive with an analyte of interest to the ion-channel and membrane spanning lipid components of the tethered membrane via photoactivatable group to form test areas;[0029]
- (v) removing unbound ligand; and[0030]
- (vi) linking a control ligand to the remainder of the ion-channels and membrane spanning lipid components of the tethered membrane to form control areas.[0031]
- The photocleavable linkers may be any of a number of such molecules known in the art (eg see Pillai (1980)). The photoactivatable groups may be any number of such groups known in the art, such as, for example, photoactivatable biotins described by Pirrung (1996) or Cass (1996).[0032]
- In a fourth aspect the present invention consists in an improved biosensor, the biosensor comprising a membrane the conductance/impedance of which is altered by the presence or absence of an analyte and a conductive substrate, the membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers such that the membrane is tethered to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate, and ligands attached to the ion channels and membrane spanning lipids, the improvement comprising providing on at least one of the first and second half membrane spanning monomers or membrane spanning lipids a photoswitchable group derived from a compound in accordance with[0033]
- [0034]
Formula 1 - wherein R[0035]1represents 0 to about 3 groups where each is independently H or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; R2represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; Y represents H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or uinsubstituted C1-4hydrocarbon. COR6, CONR7R8, COOR14, S(O)nR15where n is 0, 1 or 2, R6, R7, R8, R14and R15are each independently represent H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsatunted, substituted or unsubstituted CiA hydrocarbon or aryl; R9is —C(O)X where X represents H, saturated or unsaturated, substituted or unsubstitited C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, or OH, or OR10in which R10is alkyl, or NR11R12in which R11and R12are H, afkyl or taken together with N form a ring, or aryl or R9together with R1form a substituted or unsubstituted 5-6 member cyclic or heterocyclic ring; Z represents O or NR13R13is H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl.
- The compound will include a functional group at Y or R[0036]9such that the compound can be linked to at least one of the first and second half membrane spanning monomers or membrane spanning lipids.
- wherein R[0038]1represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; R2represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; X represents H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, or aryl, or OH, or OR10in which R10is alkyl, or NR11R12in which R11and R12are H, alkyl or taken together with N form a ring, Y represents H, or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, COR6, CONR7R8, COOR14, S(O)nR15where n is 0, 1 or 2, R6, R7, R8, R14and R15are each independently represent H. saturated or unsaturated. substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl; Z represents O or NR13R13is H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl.
- Specific examples of suitable photoswitchable linkers that are suitable for use in the present invention are shown in FIG. 10.[0039]
- It will be appreciated that certain compounds of[0040]
Formula 1 are novel and the present invention therefore provides, in a fifth aspect, compounds in accordance withFormula 1. provided that when R9is —C(O)X and X is H, at least one of R1, R2, R3or Y is other than H. - Throughout this specification, unless the context requires otherwise, the word “comprise”, or variations such as “comprises” or “comprising”, will be understood to imply the inclusion of a stated element, integer or step, or group of elements, integers or steps, but not the exclusion of any other element, integer or step, or group of elements, integers or steps.[0041]
- In order that the nature of the present invention may be more clearly understood preferred forms thereof will now be described with reference to the following non-limiting examples and Figures in which:-[0042]
- FIGS.[0043]1 to9 are schematic representations of the biosensors of the presnt invention; and
- FIG. 10 shows the structure of some of the compounds of the present invention.[0044]
- An example of an improved biosensor in accordance with the invention is shown schematically in FIG. 1.[0045]
- The improved biosensor can be advantageously used in the detection of an analyte. An exemplary protocol for use of this type of biosensor is as follows.[0046]
- An initial measurement off biosensor impedance is made and the sample suspected to contain the analyte is then added. A second measurement is made and a light source is triggered on. A third measurement of the time course response to light is made. The light source is then triggered off and a fourth measurement of the time course response to the removal of light is made. These later steps may be repeated, switching the light on and off.[0047]
- Various combinations and subsets of the later measurement steps can be used depending on the type of photogroup and the level of sensitivity required. Such a construct would not allow a real gating response until illumination, and would therefore allow for non-specific effects (e.g. caused by seruin addition) to be separately deterrnined, and removed from the real gating response.[0048]
- The benefits of another fabrication protocol is shown in FIG. 2.[0049]
- Accordingly, in a fifth aspect the present invention consists in a method comprising the following steps:[0050]
- (i) providing a conductive substrate;[0051]
- (ii) forming a membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers, the membrane being attached to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate;[0052]
- (iii) providing on the half membrane spanning monomer remote from the conductive substrate a photoswitchable binder to streptavidin and providing biotin on the membrane spanning lipid;[0053]
- (iv) adding streptavidin;[0054]
- (v) triggering a light source and rinsing;[0055]
- (vi) triggering the light source off and adding streptavidin;[0056]
- (vii) optionally repeating steps (v) and (vi); and[0057]
- (viii) adding ligands specfic to an analyte to the ion channels and membrane spanning lipids.[0058]
- It is preferred that the photoswitchable binder to streptavidin is caged biotin, HABA or derivative thereof. Preferably the photoswitchable binder is caged biotin or a compound in accordance with[0059]
Formula 1 above. - The aim here is to minimise the formation of any ga-SA-MSL linkages (i.e streptavidin gating). The advantage of this process is that streptavidin gating is reduced and thus the dynamic range is improved. Note an alternative version is that in step (v) the rinsing step can be avoided, meaning that additional SA in step (vi) need not be added.[0060]
- A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity by separating any non-specific effect (caused during analyte addition) from the gating response (see FIG. 3).[0061]
- A tethered membrane assembly is made with biotinylated MSL and gA bearing a photoswitchable group derived from a compound in accordance with[0062]
Formula 1. A biotinylated antibody streptavidin complex is then introduced into the electrolyte solution. The light source is then switched on so that the antibody complex links to the biotinylated MSL but not to the photoswitchable group gA. The analyte is then added and continually stirred and allowed to incubate so that analyte liks to MSL via antibody streptavidin biotin complex. (Note at this point there is no crossluiking of MSL to gA or gA to gA because light is on). The solution is then rinsed so that unlinked antibody is removed. An impedance measurement is then made which gives the channel on baseline. Impedance measurements continue and then the light is switched off. The time course of gating is measured as gramicidin crosslinks to MSL via a photoswitchable group-streptavidin-biotin-antibody-analyte-antibody-biotin-streptavidin-photoswitchable group -MSL complex. - The advantages are improved dynamic range due to reduction of streptavidin gating and also an increase in sensitivity as the long incubation time required to crosslink the antibody to MSL no longer limits the rate of change of gating which is carried out rapidly after the crosslinking has occurred (this assumes that off times are significantly longer than on times). Further, analyte addition artifacts are avoided and thorough mixing can be carried out, and also this method is suitable for optically phase locked loop approaches.[0063]
- A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity is shown in FIG. 4.[0064]
- A tethered membrane assembly is made with MSL and gA both bearing a photoswitchable group in accordance with the invention. A biotinylated antibody streptavidin complex is then introduced into the electrolyte solution. The light source is switched on so that the antibody complex is not bound to either MSL or gA. Analyte is added and continually stirred and allowed to incubate so that analyte crosslinks all antibody-streptavidin complexes. Impedance measurements then commence which gives the channel on baseline[0065]
- Impedance measurements continue and then the light is switched off whilst impedance measurements are made for a further period of time. The time course of gating is measured as gramicidin crosslinks to MSL via a photoswitchable group -streptavidin-biotin-antibody-analyte-antibodv-biotin-streptavidin-biotin-MSL complex[0066]
- There are four principal advantages to this method; 1. An amplification in sensitivity is possible where the on rate of the optically switchable group is significantly greater than the on-rate of the antibody to the analyte, and the off times are greater than both, 2. The analyte binding is carried out in three dimensions rather than two, 3. Analyte addition artifacts are avoided and thorough mixing can be carried out, and 4. This method is suitable for optically phase locked loop approaches.[0067]
- A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity is shown in FIG. 5.[0068]
- These methods can be modified by using antibodies bearing a photoswitchable group instead of the gA of MSL. In this case the advantages are analyte addition artifacts are avoided and thorough mixing can be carried out, and this method is suitable for optically phase locked loop approaches.[0069]
- A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity in a competition assay (such as depicted in FIG. 6) wherein non-specific effects are separated from the real gating response[0070]
- A tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a derivative of the required analyte and a photoswitchable group which binds to streptavidin is produced. A measurement of biosensor impedance is made then the analyte is added. A second measurement is made then a light source is triggered on. A third measurement of the time course response to light is made then the light source is triggered off. A fourth measurement of the time course response to the removal of light is then made.[0071]
- The photoswitchable group could of course replace biotin. Such a group may be photoswitchable group or a derivative thereof.[0072]
- A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity in a competition assay (such as depicted in FIG. 7) wherein any non-specific effects (caused during analyte addition) can be separated from the gating response.[0073]
- A tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a derivative of the required analyte and a photoswitchable group connected to a membrane spanning lipid is produced. A measurement of biosensor impedance is then made prior to addition of analyte. Analyte is added and a second measurement is made. A light source is then triggered on and a third measurement of the time course response to light is made. The light source is then triggered off and a fourth measurement of the time course response to the removal is made.[0074]
- A method for using photoswitchable linkers during measurement of analyte responses to improve sensitivity in a lateral segregation assay wherein any non-specific effects (caused during analyte addition) can be separated from the gating response(such as depicted in FIG. 8).[0075]
- A tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a derivative of the required analyte and a photoswitchable tether to the bottom layer gramicidin (or other ion channel) is produced. A measurement of biosensor impedance is made and the analyte is added. A second measurement is then made and a light source is triggered on. A third measurement of the time course response to light is made then the light source is triggered off. A fourth measurement of the time course response to the removal is then made.[0076]
- It uill be recognised that a caged biotin could be used in place of a photoswitchable streptavidin ligand such as HABA (or a derivative) in the examples cited above, specifically those depicted in FIGS. 3,4, and[0077]5. Several caged biotin derivatives are known in the literature, such as those reported by Pirrung (1993, 1996). Such caged derivatives revert to biotin on irradiation with light and therefore cannot be switched between forms that bind streptavidin and forms that do not bind streptavidin.
- An additional example of the use of such caged biotin compounds is depicted in FIG. 9.[0078]
- i) manufacture (e.g. via evaporation) a gold coated substrate on a surface (such as glass or silicon)[0079]
- ii) manufacture a tethered bilayer employing a gramicidin (or other ion channel) derivative which bears a caged biotin[0080]
- iii) streptavidin is added to the system, and attaches to biotin on the MSL4XB[0081]
- iv) a biotinylated receptor is added to the system, and attaches to the SA on MSL4XB[0082]
- v) further biotin is added to block the remnaining binding sites on SA[0083]
- vi) a light source is triggered on[0084]
- vii) streptavidin is added to the system, and attaches to newly generated biotin (on the gramicidin)[0085]
- viii) a biotinylated receptor is added to the system, and attaches to the SA on gramicidin[0086]
- ix) analyte is added to the system[0087]
- x) an impedance measurement is made[0088]
- The advantage of this manufacture process is that formation of gA-SA-MSL linkages (i.e. streptavidin gating) is minimised and thus the dynamic range is improved. A further advantage is that receptors can be selected to bind specifically at MSL4XB and the gramicidin derivative, which in turn may improve the response.[0089]
- Materials and Methods[0090]
- The photoswitchable ligands of the[0091]
general formulae - A photo-generatable derivative bf biotin (so called caged biotin) was prepared by a modification of the method of Pirrung et al ([0093]Bioconj. Chem.,1996, 7, 317). This compound (9 mg) was dissolved in dichloromethane (5 ml) and treated with dicyclohexylcarbodiimide (DCC) (3 mg), N-hydroxy succinimide (NHS) (2 mg) and dimethylaminopyridine (0.2 mg). After stiing at room temperature for two hours a derivative of gramicidin bearing two aminocaproyl groups linked end-to-end and attached to the terminal hydroxyl of gramicidin (prepared by conventional peptide chemistry techniques) was added (30 mg, as a solution in methanol (1 ml) and triethylamine (0.1 ml)). The solution was stirred for 18 hours, evaporated to dryness and then passed through a Sephadex LH-20 column eluting with dichloromethane-methanol-water (800:50:4). The main fraction was then purified by HPLC on a 40 mm×200 mmn Waters Prep Nova-Pak® HR silica column (6 μm, 60 Å) eluting with dichloromethane-methanol-water (800:40:4) operating at a flow rate of 25 ml/min. The fraction, eluting at 24.5 minutes, possessed a 1H-nmr spectrum and mass spectrum in full agreement with the proposed structure.
- Investigation of specific photosensitive chemistry in Ion Channel Sensing System[0094]
- Avidin/Streptavidin-biotin chemistry is one of the most widely used reactions in immunochemistry and is the strongest known noncovalent, biological interaction between a protein and a ligand, with K[0095]A=1015M−1. The bond formation is very rapid and once formed, is unaffected by wide extremes of pH, temperature, organic solvents and other denaturing agents. Conditions which are usually sufficient for denaturing proteins fail to disassociate the avidin-biotin complex. A reporter molecule could be bound to streptavidin covalently, or biotinylated and attached to streptavidin via the streptavidin-biotin interaction. Selective activation and functionalisation of this complex is targeted in this group of experiments.
- There are at least two applications that can be identified with the use of photosensitive compounds. The first one is using this chemistry for maling the array and the other is for improving the signal by selectively filtering out the non-specific signals and other noise components. Both these applications can be used effectively either independently or together.[0096]
- The following experiment was conducted with a form of biotin that is not active in the native state (i.e. will not bind to streptavidin) but can be activated by UV irradiation to bind streptavidin. This photoactivable form of biotin has been conjugated with gramicidin and used as an essential component of the bilayer membrane for targeting chemistries using streptavidin-biotin complex.[0097]
- Materials and Methods[0098]
- Preparation of electrodes[0099]
- The gold electrodes were built on commercially available glass microscope slides. The glass slides were cleaned for 2 hours in the glass cleaning solution “Extran 300”, rinsed several times with copious volumes of deionised water and dried in a stream of nitrogen in clean room conditions. The metal deposition was carried out using an Edwards evaporation unit. An adhesion layer of chromium (−20 nM) was deposited fouowed by a layer of gold (100 nM. One side of the glass slides was fully coated with metal. The metal treated glass slides were removed from the evaporator and quickly immersed in an ethanolic solution of monolayer components for an hour (AM300), rinsed profusely in ethanol and preserved in ethanol. These electrodes were stored at 4° C. for 24 hours before assembling the second layer of the membrane.[0100]
- Preparation of Reagents and Biomolecules[0101]
- Preparation of Solutions of Test Compound and Control Compounds[0102]
- The photoactivable biotic in its native form has a molecular weight of 686 d and has a molecular weight of 2.809 kd in the form of gAxx[B]. This compound was dissolved in ethanol to prepare a 2 mM solution (5.5 mg in 1.958 ml) and further diluted to a 10 uM solution. An aliquot of the gAxx[B] solution was activated by irradiating the solution at 350 nM for a period of 20 minutes.[0103]
- Three types of second layer membrane solutions were prepared with 3 mM lipids DPEPC (1,2-di(3RS, 7R, 11R-phytanyl)-glycero-3-phosphocholine) and GDPE (1,2-di(3RS, 7R, 11R-phytanyl)-glycerol) in 7:3 ratio and three types of gA5xB. The first solution was prepared with gA5xB (see FIG. 11), the second with the inactive form of photoactivatable gAxx[B] and the third solution with the activated form of photoactivatable gAxx[B].[0104]
- Streptavidin was diluted in PBS to a concentration of 0.1 mg/ml. The matched pair of biotinylated Thyroid Stimulating Hormone (TSH) Fabs (E20650 M and E45650 M) was combined in equal molar ratio to give a 50 ug/ml solution in PBS. TSH analyte was diluted in chilled PBS to prepare a 2.5 nM solution.[0105]
- Assembling Biosensor Blocks[0106]
- The monolayer AM300 was deposited on metallised glass electrodes as per established protocol. The electrodes were assembled into biosensor blocks. The second layer solution was added manually (15 μl per cell) and washed five times with PBS to assemble the bilayer membrane. The fully assembled blocks had the following second layers:[0107]
- Block 1: Row A (cells 1-8) with a ratio of 40 k: 1 standard gA5xB Row B (cells 9-16) with a ratio of 40 k: 1 inactive for of gAxx[B][0108]
- Block 2: Same as above[0109]
- Block 3Row A (cells 1-8) with standard gA5xB as in[0110]
blocks - A second group of 2 blocks were assembled with the inactive form of gAxx[B] and the cells were exposed to UV irradiation. The exposure time for pairs of cells was varied to study the effects of time length of exposure and select the most effective time period for future experiments. Exposure times down to one minute were found to be effective.[0111]
- Observations[0112]
- The inactive form of gAxx[B] did not show a binding response when treated with 42 nM streptavidin. This was reproducible and the positive control used in cells could be continued further to complete the TSH assay, The activated form showed moderate response when exposed to streptavidin.[0113]
- Cells 1-8 used the standard composition of second layer as a positive control for comparison and these responded to streptavidin. Cells 9-16 using the inactive form of gAxx[B] showed no response when exposed to streptavidin.[0114]
- In the time course measurements the inactive gx[B] did not appear to facilitate a specific response as compared to the specific response elicited with standard gA5x[B].[0115]
- Determination of the impedance responses showed that the activated form of gAxx[B] (test cells 9-16) showed a positive response to the addition of streptavidin. The inactive from of gAxx[B] did not facilitate any specific response. It may be concluded from these experiments that photoactivable gAxx[B] can be effectively activated by ultra violet irradiation to actively bind to streptavidin and allow gating of the biosensor.[0116]
- It will be appreciated by persons skilled in the art that numerous variations and/or modifications may be made to the invention as shown in the specific embodiments without departing from the spirit or scope of the invention as broadly described. The present embodiments are, therefore, to be considered in all respects as illustrative and not restrictive.[0117]
- References[0118]
- 1. Pirrung et al,[0119]J. Am. Chem. Soc.,1993, 115, 12050; Pirrung et al,Bioconj. Chem.1996, 7, 137.
- 2. Berwick et al.,[0120]J. Org. Chem.,1972, 37, 2409.
- 3. Oku et al.,[0121]J. Org. Chem.,1979, 44, 3342.
- 4. Weber et al.[0122]J. Am. Chem. Soc.,1994, 116, 2717.
- 5. Pillai,[0123]Sythesis,1980, 1
Claims (13)
1. A method of fabricating a biosensor in which there is at least one discrete test and at least one discrete control zone, the method comprising the following steps:
(i) providing a conductive substrate;
(ii) forming a membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers, the membrane being attached to the conductive substrate in a manner such that a functioning reservoir exists between the membrane and the conductive substrate;
(iii) linking a ligand reactive with an analyte of interest to the ion-channel and linking a ligand reactive with an analyte of interest to the membrane spanning lipids via photocleavable linkers; and
(iv) exposing the membrane to a focused light source to cleave the photocleavable linkers thereby releasing the ligands from the ion-channel and membrane spanning lipid components in discrete areas of the membrane.
2. A method as claimed inclaim 1 in which the method further includes the following step:
(v) binding control ligands to the ion channels and membrane spanning lipid components after the ligands have been removed in step (iv).
3. A method as claimed inclaim 2 in which the membrane is rinsed between steps (iv) and (v).
4. A method of fabricating a biosensor in which there is at least one discrete test and at least one discrete control zone, the method comprising the following steps:
(i) providing a conductive substrate;
(ii) forming a membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers, the membrane being attached to the conductive substrate in amanner such that a functioning reservoir exists between the membrane and the conductive substrate;
(iii) providing on the ion channels and membrane spanning lipids a photoactivatable group which when illuminated will bind a receptor;
(iv) illuminating discrete areas of the membrane and linking a ligand reactive with an analyte of interest to the ion-channel and membrane spanning lipid components of the tethered membrane via photoactivated group to form test areas;
(v) removing unbound ligand; and
(vi) linking a control ligand to the remainder of the ion-channels and membrane spanning lipid components of the tethered membrane to form control areas.
5. A method as claimed inclaim 4 in which the photoactivatable group is caged biotin.
6. An improved biosensor, the biosensor comprising a membrane and an electrode having a conductive subsbate, the membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers, the membrane being attached to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate, ligands specific for an analyte attached the ion channels and membrane spanning lipids, the improvement comprising providing on at least one of the first and second half membrane spanning monomers a photocleavable/switchable group which inhibits dimer formation.
7. An improved biosensor, the biosensor comprising a membrane and an electrode having a conductive substrate, the membrane including membrane spanning lipids and ion channels comprsing first and second half membrane spanning monomers, the membrane being attached to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate, ligands specific for an analyte attached the ion channels and membrane spanning lipids, the improvement comprising the attachment of at least one of the ligands specific for an analyte attached the ion channels and membrane spanning lipids being attached by means of a photocleavable/switchable group.
8. A method of detecting the presence of an analyte in a sample, the method including the steps of:
(i) adding a sample suspected to contain the analyte to the biosensor as claimed inclaim 6 orclaim 7;
(ii) determining the conductance or impedance of the membrane;
(iii) exposing the biosensor to irradiation to which the photocleavable/switchable group is sensitive;
(iv) determining the conductance or impedance of the membrane following irradiation;
(v) comparing the conductance or impedance determination in step (ii) with the determination in step (iv); and
(vi) optionally repeating steps (ii) to (v).
9. A method of producing an improved biosensor, the method comprising the following steps:
(i) providing a conductive substrate;
(ii) forming a membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers, the membrane being attached to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate;
(iii) providing on the half membrane spanning monomer remote from the conductive substrate a photoswitchable binder to streptavidin and providing biotin on the membrane spanning lipid;
(iv) adding streptavidin;
(v) triggering a light source and rinsing;
(vi) triogering the light source off and adding streptavidin;
(vii) optionally repeating steps (v) and (vi); and
(viii) adding ligands specfic to an analyte to the ion channels and membrane spanning lipids.
10. A method as claimed inclaim 9 in which the photoswitchable binder to streptavidin is caged biotin, HABA or derivative thereof.
11. An improved biosensor, the biosensor comprising a membrane and an electrode having a conductive substrate, the membrane including membrane spanning lipids and ion channels comprising first and second half membrane spanning monomers, the membrane being attached to the conductive substrate such that a functioning reservoir exists between the membrane and the conductive substrate, and ligands specific for an analyte attached to the ion channels and membrane spanning lipids, the improvement comprising providing on at least one of the first and second half membrane spanning monomers or membrane spanning lipids a photoswitchable group derived from a compound in accordance with Formula 1:
wherein R1represents 0 to about 3 groups where each is independently H or saturated or unsaturated, substituted or unsubstituted C1-C10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; R2represents 0 to about 3 groups where each is independently hydrogen or satmuated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; Y represents H, saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, COR6, CONR7R8, COOR14, S(O)nR15where n is 0, 1 or 2, R6, R7, R8, R14and R15are each independently represent H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4, hydrocarbon or aryl; R9is —C(O)X where X represents H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, or OH, or OR10in which R10is alkyl, or NR11R12in which R11and R12are H, alkyl or taken together with N form a rincg, or arl or R9together with R1form a substituted or unsubstituted 5-6 member cyclic or heterocyclic ring; Z represents O or NR13R13is H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl, the compound including a functional group at Y or R9such that the compound can be linked to the the at least one of the first and second half membrane spanning monomers.
12. An improved biosensor as claimed inclaim 11 in which the photoswitchable linkers are derived are shown in Formula 2 below.
wherein R1represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or uinsubstituted C1-4hydrocarbon; R, represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; X represents H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, or aryl, or OH, or OR10in which R10is alkyl, or NR11R12in which R11and R12are H, alkyl or taken together with N form a ring,; Y represents H, or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, COR6, CONR7R8, COOR14, S(O)nR15where n is 0, 1 or 2, R6, R7, R8, R14and R15are each independently represent H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl; Z represents O or NR13R13is H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated. substituted or unsubstituted C1-4hydrocarbon or aryl.
13. A compound in accordance with Formula 1:
wherein R1represents 0 to about 3 groups where each is independently H or saturated or unsuaturated, substituted or usubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; R2represents 0 to about 3 groups where each is independently hydrogen or saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon; Y represents H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, COR6, CONR7R8, COOR14, S(O)nR15where n is 0, 1, or 2, R6, R7, R14and R15are each independently represent H, saturated or unsaturated, substituted or unsubstitusted C1-10hydrocarbon, preferably, saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl; R9is —C(O)X where X represents H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon, or OH, or OR10in which R10is alkyl, or NR11R12in which R11and R12are H, alkyl or taken together with N form a ring, or aryl or R9together with R1form a substituted or usubstituted 5-6 member cyclic or heterocyclic ring; Z represents O or NR13R13is H, saturated or unsaturated, substituted or unsubstituted C1-10hydrocarbon, preferably saturated or unsaturated, substituted or unsubstituted C1-4hydrocarbon or aryl, with the proviso that when R is —C(O)X and X is H, at least one of R1, R2, R3or Y is other than H.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US10/358,176US20030143726A1 (en) | 1997-06-04 | 2003-02-05 | Biosensor involving the use of optically sensitive moieties |
Applications Claiming Priority (6)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| AUPO7170 | 1997-06-04 | ||
| AUPO7170AAUPO717097A0 (en) | 1997-06-04 | 1997-06-04 | Improved biosensor involving the use of optically sensitive moieties |
| AUPP0449 | 1997-11-20 | ||
| AUPP0449AAUPP044997A0 (en) | 1997-11-20 | 1997-11-20 | Improved biosensor involving the use of optically sensitive moieties |
| US09/446,004US6537441B1 (en) | 1997-06-04 | 1998-06-04 | Biosensor involving the use of optically sensitive moieties |
| US10/358,176US20030143726A1 (en) | 1997-06-04 | 2003-02-05 | Biosensor involving the use of optically sensitive moieties |
Related Parent Applications (2)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| US09/446,004DivisionUS6537441B1 (en) | 1997-06-04 | 1998-06-04 | Biosensor involving the use of optically sensitive moieties |
| PCT/AU1998/000424DivisionWO1998055855A1 (en) | 1997-06-04 | 1998-06-04 | Improved biosensor involving the use of optically sensitive moieties |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| US20030143726A1true US20030143726A1 (en) | 2003-07-31 |
Family
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Family Applications (2)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| US09/446,004Expired - Fee RelatedUS6537441B1 (en) | 1997-06-04 | 1998-06-04 | Biosensor involving the use of optically sensitive moieties |
| US10/358,176AbandonedUS20030143726A1 (en) | 1997-06-04 | 2003-02-05 | Biosensor involving the use of optically sensitive moieties |
Family Applications Before (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| US09/446,004Expired - Fee RelatedUS6537441B1 (en) | 1997-06-04 | 1998-06-04 | Biosensor involving the use of optically sensitive moieties |
Country Status (4)
| Country | Link |
|---|---|
| US (2) | US6537441B1 (en) |
| EP (1) | EP0996855A4 (en) |
| CA (1) | CA2294080A1 (en) |
| WO (1) | WO1998055855A1 (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US20080012007A1 (en)* | 2004-04-01 | 2008-01-17 | Nanyang Technological University | Addressable Transistor Chip For Conducting Assays |
| EP2175022A1 (en) | 2003-02-21 | 2010-04-14 | Phylogica Limited | Methods of construction biodiverse gene fragment libraries |
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- 1998-06-04WOPCT/AU1998/000424patent/WO1998055855A1/ennot_activeApplication Discontinuation
- 1998-06-04EPEP98925325Apatent/EP0996855A4/ennot_activeWithdrawn
- 1998-06-04USUS09/446,004patent/US6537441B1/ennot_activeExpired - Fee Related
- 2003
- 2003-02-05USUS10/358,176patent/US20030143726A1/ennot_activeAbandoned
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| US4186243A (en)* | 1976-02-25 | 1980-01-29 | Ciba-Geigy Corporation | Image producing system |
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| US5234566A (en)* | 1988-08-18 | 1993-08-10 | Australian Membrane And Biotechnology Research Institute Ltd. | Sensitivity and selectivity of ion channel biosensor membranes |
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| US5096801A (en)* | 1989-04-03 | 1992-03-17 | Fuji Photo Film Co., Ltd. | Color image recording method |
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| US8138496B2 (en)* | 2004-04-01 | 2012-03-20 | Nanyang Technological University | Addressable transistor chip for conducting assays |
Also Published As
| Publication number | Publication date |
|---|---|
| US6537441B1 (en) | 2003-03-25 |
| EP0996855A1 (en) | 2000-05-03 |
| CA2294080A1 (en) | 1998-12-10 |
| EP0996855A4 (en) | 2001-08-01 |
| WO1998055855A1 (en) | 1998-12-10 |
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| Date | Code | Title | Description |
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| STCB | Information on status: application discontinuation | Free format text:ABANDONED -- FAILURE TO RESPOND TO AN OFFICE ACTION |