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US20030223472A1 - Clinical tester wash and method - Google Patents

Clinical tester wash and method Download PDF

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Publication number
US20030223472A1
US20030223472A1 US10/158,495 US15849502A US2003223472A1 US 20030223472 A1 US20030223472 A1 US 20030223472A1 US 15849502 A US15849502 A US 15849502A US 2003223472 A1 US2003223472 A1 US 2003223472A1
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United States
Prior art keywords
probe
wash
sample
fluid
predetermined period
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Abandoned
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US10/158,495
Inventor
Patricia Ravalico
Charlie Wilson
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Abbott Laboratories
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Abbott Laboratories
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Publication date
Application filed by Abbott Laboratories filed Critical Abbott Laboratories
Priority to US10/158,495 priority Critical patent/US20030223472A1/en
Assigned to ABBOTT LABORATORIES reassignment ABBOTT LABORATORIES ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: RAVALICO, PATRICIA H., WILSON, III, CHARLIE W.
Priority to JP2004514403A priority patent/JP2005527839A/en
Priority to EP12150274.4A priority patent/EP2463663A3/en
Priority to CA2486264A priority patent/CA2486264C/en
Priority to PCT/US2003/016872 priority patent/WO2003102597A2/en
Priority to EP03756244A priority patent/EP1518125A2/en
Publication of US20030223472A1 publication Critical patent/US20030223472A1/en
Priority to US12/714,601 priority patent/US8759106B2/en
Priority to JP2010046040A priority patent/JP5437115B2/en
Priority to US14/306,961 priority patent/US9308560B2/en
Priority to US15/095,893 priority patent/US20160223575A1/en
Abandoned legal-status Critical Current

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    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1004Cleaning sample transfer devices
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B08CLEANING
    • B08BCLEANING IN GENERAL; PREVENTION OF FOULING IN GENERAL
    • B08B3/00Cleaning by methods involving the use or presence of liquid or steam
    • B08B3/04Cleaning involving contact with liquid
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1009Characterised by arrangements for controlling the aspiration or dispense of liquids
    • G01N35/1016Control of the volume dispensed or introduced
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B08CLEANING
    • B08BCLEANING IN GENERAL; PREVENTION OF FOULING IN GENERAL
    • B08B3/00Cleaning by methods involving the use or presence of liquid or steam
    • B08B3/02Cleaning by the force of jets or sprays
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N2035/00178Special arrangements of analysers
    • G01N2035/00277Special precautions to avoid contamination (e.g. enclosures, glove- boxes, sealed sample carriers, disposal of contaminated material)
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • G01N35/1004Cleaning sample transfer devices
    • G01N2035/1006Rinsing only the inside of the tip
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01NINVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
    • G01N35/00Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
    • G01N35/10Devices for transferring samples or any liquids to, in, or from, the analysis apparatus, e.g. suction devices, injection devices
    • YGENERAL 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
    • Y10TECHNICAL SUBJECTS COVERED BY FORMER USPC
    • Y10TTECHNICAL SUBJECTS COVERED BY FORMER US CLASSIFICATION
    • Y10T436/00Chemistry: analytical and immunological testing
    • Y10T436/11Automated chemical analysis
    • Y10T436/113332Automated chemical analysis with conveyance of sample along a test line in a container or rack
    • Y10T436/114998Automated chemical analysis with conveyance of sample along a test line in a container or rack with treatment or replacement of aspirator element [e.g., cleaning, etc.]
    • YGENERAL 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
    • Y10TECHNICAL SUBJECTS COVERED BY FORMER USPC
    • Y10TTECHNICAL SUBJECTS COVERED BY FORMER US CLASSIFICATION
    • Y10T436/00Chemistry: analytical and immunological testing
    • Y10T436/11Automated chemical analysis
    • Y10T436/115831Condition or time responsive
    • YGENERAL 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
    • Y10TECHNICAL SUBJECTS COVERED BY FORMER USPC
    • Y10TTECHNICAL SUBJECTS COVERED BY FORMER US CLASSIFICATION
    • Y10T436/00Chemistry: analytical and immunological testing
    • Y10T436/12Condition responsive control

Definitions

  • the present invention relates generally to clinical test equipment and in particular the present invention relates to reduction of sample carryover in clinical test equipment.
  • analysis of a test sample involves the reaction of test samples with one or more reagents with respect to one or more analytes wherein it is frequently desired that the analysis be performed on a selective basis with respect to each test sample.
  • Automated clinical analysis systems analyze a test sample for one or more characteristics. Automated clinical analyzers also provide results much more rapidly while frequently avoiding operator or technician error, thus placing emphasis on accuracy and repeatability of a variety of tests. Automated clinical analyzers presently available for routine laboratory tests include a transport or conveyor system designed to transport containers of sample liquids between various operating stations.
  • a robotic arm automatically processes the test samples with a probe and a carousel, or robotic track, that positions the samples for processing.
  • a typical tester has a sample probe arm to sample fluids and deposit the samples in a reaction vessel.
  • One or more reagents are added to the vessel using reagent probe arms.
  • the sample and reagent probe arms include a probe that can be moved between sample or reagent locations, the reagent vessel and wash stations.
  • Clinical chemistry and immunoassay testers have traditionally been standalone systems. These systems can be combined using a common transport system to provide a more efficient integrated system.
  • Previous standalone chemistry analyzers did not require sample-to-sample carryover performance requirements of an integrated clinical chemistry and immunoassay system. As laboratories integrate automated analytical systems, between-sample carryover becomes a critical goal. Many companies have elected to overcome this problem through use of disposable probe tips, but this approach is costly, wasteful and less reliable.
  • Another safeguard is to prioritize test sequencing such that immunoassay sampling is done prior to all chemistry tests. This approach impacts chemistry turnaround time and lowers total workflow throughput.
  • Yet another method to reduce sample carryover is to flush the system with large amounts of fluids (buffer, water, detergents).
  • a fluid tester comprises a probe having an interior region and an exterior surface. The probe is used to selectively aspirate a fluid into the interior region.
  • a first wash mechanism is coupled to the probe to dispense a wash fluid through the interior region of the probe for a first predetermined period.
  • a second wash mechanism is located to dispense the wash fluid on the exterior surface of the probe for a second predetermined period. The second predetermined period extends beyond the first predetermined period.
  • a method of cleaning a probe comprises flushing an interior region of the probe with a wash fluid for X seconds, and simultaneously flushing an exterior surface of the probe with the wash fluid for Y seconds, wherein Y is greater than X.
  • a method of sample carryover in an integrated chemistry and immunoassay analyzer comprises aspirating a first test sample from a first sample container using a probe, depositing the first test sample into a reaction vessel and performing a chemical analysis of the test sample.
  • the probe is washed by pumping a wash fluid through an interior region of the probe and pumping the wash fluid on the exterior of the probe. The pumping of the wash fluid is terminated from the interior region prior to terminating the pumping of the exterior.
  • a second test sample is then aspirated from a second sample container using the probe.
  • FIG. 1A is a perspective view of a clinical tester of an embodiment of the present invention.
  • FIG. 1B is a clinical chemistry analyzer of the tester of FIG. 1A;
  • FIG. 1C is an immunoassay analyzer of the tester of FIG. 1A;
  • FIG. 2 illustrates a probe arm of the clinical tester of FIG. 1
  • FIG. 3 is a simplified cross-section of a probe in a wash station.
  • test sample refers to a test material that can be used directly as obtained from a source or following a pretreatment to modify the character of the sample.
  • the test sample can be derived from any biological source, such as physiological fluid, including, whole blood, serum, plasma, saliva, ocular lens fluid, cerebral spinal fluid, sweat, urine, milk, ascites fluid, raucous, synovial fluid, peritoneal fluid, amniotic fluid or the like.
  • Carryover refers to cross-contamination or contact transfer between test samples. Carryover is a byproduct of using a common sample probe for multiple test samples.
  • HbsAg hepatitis surface-antigen
  • a probe wash protocol of an embodiment of the invention passes the between-sample carryover limit of 0.1 ppm without sample pre-aliquoting, use of additional consumables, test prioritization, or significant impact to system specimen throughput.
  • Critical variables include clinical chemistry sampling/aspiration volumes and external sample probe wash duration, sequencing relative to the internal sample probe wash. Other variables include positioning of the sample probe within the sample wash cup, sample wash cup design and external sample wash flow volumes/rates.
  • An embodiment of a wash protocol dictates the between sample wash mechanism based on clinical chemistry sampling volume.
  • the wash includes an external wash and an internal wash of the sample probe. All specimens with a maximum chemistry sampling volume below a predetermined threshold (such as 15 ⁇ L or less) are effectively washed using an extended single cycle wash mechanism. It is noted that a ‘dummy’ fluid volume may be aspirated in addition to the fluid sample volume. The dummy volume provides a buffer between the sample fluid and residual fluid in the probe. The dummy volume is not included in the sample volume levels described herein.
  • the extended single cycle wash mechanism utilizes a one second external probe wash that ends 100 ms after the internal probe wash. This timing relationship between the internal and external wash sequencing is particularly crucial for acceptable carryover performance.
  • Specimens that are processed with chemistry sampling volumes exceeding the threshold (15.1 ⁇ L or more) are washed using the same extended single cycle wash mechanism but also undergo an additional 3.2 seconds of supplemental external wash.
  • the wash protocol of the present invention is not limited to a specific timing duration or over-lap time between the termination of internal and external washes.
  • the magnitude of the failure was calculated by converting the reported concentration of the serum diluents into units of ppm from the reference dilution. Test conditions were created to represent worst-case performance and test result confidence.
  • the clinical chemistry sample volume was defined at 35 ⁇ L, a typical maximum sample volume for a chemistry application. HbsAg samples were processed in duplicate to ensure result integrity.
  • Results demonstrated a sample carryover performance trend associated with sample probe aspiration volume. As the clinical chemistry sample volume increases, between-sample carryover failures also increase. Most systems fail between-sample carryover with a frequency higher than 50% (without optimization critical parameters) at the maximum clinical chemistry sampling volume of 35 ⁇ L. The relationship between sample volume and sample-to-sample carryover performance is significant to understanding the mode of failure. This is because trending demonstrates that internal contamination of the sample probe has an impact on sample-to-sample carryover.
  • the sample probe aspirates a test sample from a sample tube and immediately dispenses the sample volume into a reaction vessel prior to entrance into a wash station.
  • a second variable to carryover performance is wash sequencing at the sample wash station. Further analysis of wash conditions at the sample wash station lead to a study evaluating external wash sequencing relative to the internal wash. Success of the probe wash was less dependent on the external wash duration than it was on the stop sequencing of the external wash relative to the internal wash. If the internal wash stops after the external wash, carryover performance is significantly worse than if the external wash if ends after the internal wash. This relationship supports a theory that internal contamination of the probe is a source for the external between-sample carryover.
  • One wash protocol utilizes a one second external probe wash that extends beyond the stop time of the internal wash to improve carryover performance at low sample volumes. A supplemental washing that would have required an additional instrument cycle is not required to meet carryover performance criteria.
  • FIG. 1A a perspective view of a simplified integrated clinical test system 100 of an embodiment of the present invention.
  • the test system includes a clinical chemistry tester 102 and an immunoassay tester 104 , see FIGS. 1B and 1C for more detail.
  • the two testers share a common sample transporter 106 that allows linear movement of test sample tubes 108 between the two testers.
  • Each tester has a sample probe arm 110 / 112 that includes a probe 114 (see FIG. 2).
  • the arms can move in both a horizontal arc and vertical directions.
  • the probe aspirates a test sample from tube 108 located on the transporter 106 .
  • the probe arm then moves to a sample vessel (not shown) and deposits the aspirated sample.
  • the arm moves to a wash station 120 where the probe is washed.
  • the sample vessel is moved to a location where a reagent is added to the sample by a reagent arm 122 .
  • the reagent arm is movable between a reagent location, the sample vessel and the wash station.
  • the sample vessel may receive additional reagents and is then subjected to chemistry testing, as know to those skilled in the art.
  • a second reagent arm 123 can be included to provide a second reagent to the sample vessel.
  • the sample tube 108 located on the transporter 106 is then moved to a location near the immunoassay tester 104 , FIG. 1C.
  • the immunoassay tester is similar in operation to the clinical chemistry tester in that a test sample from the sample tube is aspirated using sample probe 114 of sample probe arm 112 .
  • the sample arm then moves to a sample vessel (not shown) and deposits the aspirated sample. After the sample has been discharged from the probe, the arm moves to a wash station (not shown) where the probe is washed.
  • the sample vessel is moved to a location where a reagent is added to the sample by a reagent probe arm 115 .
  • the reagent arm is movable between a reagent location, the sample vessel and the wash station.
  • the sample vessel may receive additional reagents and is then subjected to testing, as know to those skilled in the art. It is clear that sample carryover, or contamination, can occur if the sample probes are not cleaned between aspirations of different
  • FIG. 2 illustrates an example probe arm 110 .
  • the arm includes a probe 114 that can be moved about a horizontal arc and in a vertical direction.
  • the probe has a hollow center that allows aspiration of a fluid and the subsequent introduction of a wash fluid.
  • the mechanics of the probe arm are not described in detail herein, but are generally know to those skilled in the art.
  • the arm is controllable to regulate the amount of sample aspirated and the amount and duration of wash fluid that flows through the probe.
  • the probe is substantially tube-shaped and includes an exterior surface 132 and an interior surface 130 .
  • An interior wash dispenser 136 is located to discharge a wash fluid into the interior region of the probe.
  • the wash cup includes one or more exterior wash dispensers 138 , or nozzles, positioned to spray a wash fluid toward a center region of the cup and onto the exterior of the probe.
  • the wash fluid pumped through the probe and on its exterior is the same fluid and depends upon the material that is to be removed from the probe.
  • the wash fluid can be located in a common reservoir 140 and pumped to the nozzles using separate pumps 142 and 144 . Alternately, a single pump and controllable valves can be used to pump the wash fluid to the nozzles.
  • the present invention is not limited to a specific pump design, provided the termination of the internal fluid and the external fluid can be separately controlled by pump(s) controller 150 .
  • the term ‘pump’ is intended to include any mechanism that allows for controlled movement of a liquid, such as the wash fluid.
  • the probe needs to be sufficiently cleaned between sample aspirations to reduce sample carryover.
  • the sample carryover can be a test sample or reagent depending upon the probe.
  • the internal wash is terminated prior to terminating the external wash. This termination overlap significantly reduces sample carryover and allows clinical chemistry testers to meet restrictive specifications of immunoassay testers.
  • One example wash for chemistry sampling volume below a predetermined threshold includes a one second external sample probe wash that ends 100 ms after the internal sample probe wash. The external wash can begin prior to the internal wash without departing from the present invention.
  • the present invention is not limited to an integrated clinical chemistry/immunoassay tester, and other analytical systems can utilize the relationship of between-sample carryover performance to improve sample wash parameters. This includes other clinical chemistry and immunoassay systems as well as hematology and other methodologies.
  • the wash method can also be used utilized for reagent carryover washing, sample pretreatment instrumentation, and with laboratory automation systems.
  • a clinical tester has been described that includes a probe to aspirate a fluid.
  • the probe is washed between aspirations to reduce carryover.
  • the wash operation includes both an internal and an external wash, where the internal wash operation is terminated prior to terminating the external wash.
  • the probe wash can be implemented on an integrated clinical chemistry/immunoassay tester.

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  • Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Chemical & Material Sciences (AREA)
  • Analytical Chemistry (AREA)
  • Biochemistry (AREA)
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Abstract

A clinical tester has been described that includes a probe to aspirate a fluid. The probe is washed between aspirations to reduce carryover. The wash operation includes both an internal and an external wash, where the internal wash operation is terminated prior to terminating the external wash. In one embodiment, the probe wash can be implemented on an integrated clinical chemistry/immunoassay tester.

Description

    FIELD OF THE INVENTION
  • The present invention relates generally to clinical test equipment and in particular the present invention relates to reduction of sample carryover in clinical test equipment. [0001]
  • BACKGROUND OF THE INVENTION
  • Although various known clinical analyzers for chemical, immunochemical and biological testing of samples are available, clinical technology is rapidly changing due to increasing demands in the clinical laboratory to provide new levels of service. These new levels of service must be more cost effective to decrease the operating expenditures such as labor cost and the like, and must provide shorter turnaround time of test results. Modernization of analytical apparatus and procedure demands consolidation of workstations to meet the growing challenge placed on clinical laboratories. [0002]
  • Generally, analysis of a test sample involves the reaction of test samples with one or more reagents with respect to one or more analytes wherein it is frequently desired that the analysis be performed on a selective basis with respect to each test sample. Automated clinical analysis systems analyze a test sample for one or more characteristics. Automated clinical analyzers also provide results much more rapidly while frequently avoiding operator or technician error, thus placing emphasis on accuracy and repeatability of a variety of tests. Automated clinical analyzers presently available for routine laboratory tests include a transport or conveyor system designed to transport containers of sample liquids between various operating stations. [0003]
  • Some of the presently available automated clinical analyzers, such as automated immunoassay analyzers, utilize procedures involving a variety of different assay steps. A robotic arm automatically processes the test samples with a probe and a carousel, or robotic track, that positions the samples for processing. A typical tester has a sample probe arm to sample fluids and deposit the samples in a reaction vessel. One or more reagents are added to the vessel using reagent probe arms. The sample and reagent probe arms include a probe that can be moved between sample or reagent locations, the reagent vessel and wash stations. [0004]
  • Clinical chemistry and immunoassay testers have traditionally been standalone systems. These systems can be combined using a common transport system to provide a more efficient integrated system. Previous standalone chemistry analyzers did not require sample-to-sample carryover performance requirements of an integrated clinical chemistry and immunoassay system. As laboratories integrate automated analytical systems, between-sample carryover becomes a critical goal. Many companies have elected to overcome this problem through use of disposable probe tips, but this approach is costly, wasteful and less reliable. Another safeguard is to prioritize test sequencing such that immunoassay sampling is done prior to all chemistry tests. This approach impacts chemistry turnaround time and lowers total workflow throughput. Yet another method to reduce sample carryover is to flush the system with large amounts of fluids (buffer, water, detergents). [0005]
  • For the reasons stated above, and for other reasons stated below which will become apparent to those skilled in the art upon reading and understanding the present specification, there is a need in the art for a reduction in sample carryover in clinical test equipment. [0006]
  • SUMMARY OF THE INVENTION
  • The above-mentioned problems with sample carryover and other problems are addressed by the present invention and will be understood by reading and studying the following specification. [0007]
  • In one embodiment, a fluid tester comprises a probe having an interior region and an exterior surface. The probe is used to selectively aspirate a fluid into the interior region. A first wash mechanism is coupled to the probe to dispense a wash fluid through the interior region of the probe for a first predetermined period. A second wash mechanism is located to dispense the wash fluid on the exterior surface of the probe for a second predetermined period. The second predetermined period extends beyond the first predetermined period. [0008]
  • In another embodiment, a method of cleaning a probe comprises flushing an interior region of the probe with a wash fluid for X seconds, and simultaneously flushing an exterior surface of the probe with the wash fluid for Y seconds, wherein Y is greater than X. [0009]
  • A method of sample carryover in an integrated chemistry and immunoassay analyzer comprises aspirating a first test sample from a first sample container using a probe, depositing the first test sample into a reaction vessel and performing a chemical analysis of the test sample. The probe is washed by pumping a wash fluid through an interior region of the probe and pumping the wash fluid on the exterior of the probe. The pumping of the wash fluid is terminated from the interior region prior to terminating the pumping of the exterior. A second test sample is then aspirated from a second sample container using the probe.[0010]
  • BRIEF DESCRIPTION OF THE DRAWINGS
  • FIG. 1A is a perspective view of a clinical tester of an embodiment of the present invention; [0011]
  • FIG. 1B is a clinical chemistry analyzer of the tester of FIG. 1A; [0012]
  • FIG. 1C is an immunoassay analyzer of the tester of FIG. 1A; [0013]
  • FIG. 2 illustrates a probe arm of the clinical tester of FIG. 1; and [0014]
  • FIG. 3 is a simplified cross-section of a probe in a wash station.[0015]
  • DETAILED DESCRIPTION OF THE DRAWINGS
  • In the following detailed description of the preferred embodiments, reference is made to the accompanying drawings, which form a part hereof, and in which is shown by way of illustration specific preferred embodiments in which the inventions may be practiced. These embodiments are described in sufficient detail to enable those skilled in the art to practice the invention, and it is to be understood that other embodiments may be utilized and that logical, mechanical and electrical changes may be made without departing from the spirit and scope of the present invention. The following detailed description is, therefore, not to be taken in a limiting sense, and the scope of the present invention is defined only by the claims. [0016]
  • The term “test sample”, as used herein, refers to a test material that can be used directly as obtained from a source or following a pretreatment to modify the character of the sample. The test sample can be derived from any biological source, such as physiological fluid, including, whole blood, serum, plasma, saliva, ocular lens fluid, cerebral spinal fluid, sweat, urine, milk, ascites fluid, raucous, synovial fluid, peritoneal fluid, amniotic fluid or the like. [0017]
  • The term “carryover” refers to cross-contamination or contact transfer between test samples. Carryover is a byproduct of using a common sample probe for multiple test samples. [0018]
  • Between-sample carryover is a critical factor to ensure result integrity on automated analytical systems. Immunoassay analyzers traditionally meet a sample-to-sample carryover goal of less than 0.1 ppm. Clinical chemistry systems utilize methodologies that are less sensitive and rarely characterized using carryover requirements to this level. As laboratories consolidate analytical systems, however, the between-sample carryover demands for immunoassay analyzers become applicable to clinical chemistry systems as well. Achieving a between-sample carryover goal of less than 0.1 ppm for an integrated immunoassay and clinical chemistry system can impact marketability of other variables including specimen throughput, system consumables, test prioritization, and sample pre-aliquoting. [0019]
  • Extensive research on an integrated system of an embodiment of the present invention identified critical variables associated with sample-to-sample carryover. High-speed video was used for qualitative characterization of the sample probe wash while concentrated samples of hepatitis surface-antigen (HbsAg) were used to quantitatively assess carryover performance. A probe wash protocol of an embodiment of the invention passes the between-sample carryover limit of 0.1 ppm without sample pre-aliquoting, use of additional consumables, test prioritization, or significant impact to system specimen throughput. Critical variables include clinical chemistry sampling/aspiration volumes and external sample probe wash duration, sequencing relative to the internal sample probe wash. Other variables include positioning of the sample probe within the sample wash cup, sample wash cup design and external sample wash flow volumes/rates. [0020]
  • An embodiment of a wash protocol dictates the between sample wash mechanism based on clinical chemistry sampling volume. The wash includes an external wash and an internal wash of the sample probe. All specimens with a maximum chemistry sampling volume below a predetermined threshold (such as 15 μL or less) are effectively washed using an extended single cycle wash mechanism. It is noted that a ‘dummy’ fluid volume may be aspirated in addition to the fluid sample volume. The dummy volume provides a buffer between the sample fluid and residual fluid in the probe. The dummy volume is not included in the sample volume levels described herein. The extended single cycle wash mechanism utilizes a one second external probe wash that ends 100 ms after the internal probe wash. This timing relationship between the internal and external wash sequencing is particularly crucial for acceptable carryover performance. Specimens that are processed with chemistry sampling volumes exceeding the threshold (15.1 μL or more) are washed using the same extended single cycle wash mechanism but also undergo an additional 3.2 seconds of supplemental external wash. The wash protocol of the present invention, as explained below, is not limited to a specific timing duration or over-lap time between the termination of internal and external washes. [0021]
  • Between-Sample Carryover was quantitatively evaluated using recombinant samples of concentrated hepatitis surface-antigen (HbsAg) in a pooled human serum matrix. Each concentrated HBsAg sample (with approximate immuno-reactivity of 4 mg/mL) was followed by pooled normal human serum (pre-screened non-reactive for HbsAg) and processed on a chemistry analyzer. The pooled human serum samples were evaluated on an immunoassay analyzer for HbsAg activity. Results were compared against serial dilutions of the concentrated stock. If the pooled human serum results exceeded that of the 0.1 ppm dilution of the concentrated stock, a test run was considered a failure. The magnitude of the failure was calculated by converting the reported concentration of the serum diluents into units of ppm from the reference dilution. Test conditions were created to represent worst-case performance and test result confidence. The clinical chemistry sample volume was defined at 35 μL, a typical maximum sample volume for a chemistry application. HbsAg samples were processed in duplicate to ensure result integrity. [0022]
  • Results demonstrated a sample carryover performance trend associated with sample probe aspiration volume. As the clinical chemistry sample volume increases, between-sample carryover failures also increase. Most systems fail between-sample carryover with a frequency higher than 50% (without optimization critical parameters) at the maximum clinical chemistry sampling volume of 35 μL. The relationship between sample volume and sample-to-sample carryover performance is significant to understanding the mode of failure. This is because trending demonstrates that internal contamination of the sample probe has an impact on sample-to-sample carryover. The sample probe aspirates a test sample from a sample tube and immediately dispenses the sample volume into a reaction vessel prior to entrance into a wash station. An over-aspiration or dummy volume is dispensed at the wash station but this volume is consistent and independent of chemistry sample volume (under the protocol test conditions). Since the frequency of the carryover increases with chemistry sample volume and since this sample volume is dispensed prior to external wash of the probe, it was theorized that the source of the carryover (leading to the between-sample failures) resulted from internal contamination of the sample probe. This theory was supported by a supplemental investigation that demonstrated that carryover failures were still prevalent without any dummy/over aspiration being dispensed at the sample wash station. Residual carryover remained on the external surface of the sample probe following sample probe washing, even when the probe did not dispense any concentrated sample at the wash station. The frequency of sample carryover failures can be reduced using supplemental probe washes. Unfortunately, supplemental washes require additional instrument cycles that can degrade system specimen throughput. [0023]
  • A second variable to carryover performance is wash sequencing at the sample wash station. Further analysis of wash conditions at the sample wash station lead to a study evaluating external wash sequencing relative to the internal wash. Success of the probe wash was less dependent on the external wash duration than it was on the stop sequencing of the external wash relative to the internal wash. If the internal wash stops after the external wash, carryover performance is significantly worse than if the external wash if ends after the internal wash. This relationship supports a theory that internal contamination of the probe is a source for the external between-sample carryover. One wash protocol utilizes a one second external probe wash that extends beyond the stop time of the internal wash to improve carryover performance at low sample volumes. A supplemental washing that would have required an additional instrument cycle is not required to meet carryover performance criteria. [0024]
  • Further studies demonstrated additional variables associated with between-sample carryover performance. These include wash cup design, hardware alignment at the sample wash station, and wash flow rates/volume. These variables are significant and require optimization for carryover performance. Failure to optimize these parameters can cause carryover failures. However, optimization, of these parameters will not create a passing condition without control of the critical variables of chemistry sampling volume and wash sequencing. [0025]
  • Referring to FIG. 1A, a perspective view of a simplified integrated [0026] clinical test system 100 of an embodiment of the present invention. The test system includes a clinical chemistry tester 102 and an immunoassay tester 104, see FIGS. 1B and 1C for more detail. The two testers share a common sample transporter 106 that allows linear movement of test sample tubes 108 between the two testers.
  • Each tester has a [0027] sample probe arm 110/112 that includes a probe 114 (see FIG. 2). The arms can move in both a horizontal arc and vertical directions. The probe aspirates a test sample from tube 108 located on the transporter 106. The probe arm then moves to a sample vessel (not shown) and deposits the aspirated sample. After the sample has been discharged from the probe, the arm moves to a wash station 120 where the probe is washed. The sample vessel is moved to a location where a reagent is added to the sample by a reagent arm 122. The reagent arm is movable between a reagent location, the sample vessel and the wash station. The sample vessel may receive additional reagents and is then subjected to chemistry testing, as know to those skilled in the art. A second reagent arm 123 can be included to provide a second reagent to the sample vessel.
  • The [0028] sample tube 108 located on the transporter 106 is then moved to a location near the immunoassay tester 104, FIG. 1C. The immunoassay tester is similar in operation to the clinical chemistry tester in that a test sample from the sample tube is aspirated using sample probe 114 of sample probe arm 112. The sample arm then moves to a sample vessel (not shown) and deposits the aspirated sample. After the sample has been discharged from the probe, the arm moves to a wash station (not shown) where the probe is washed. The sample vessel is moved to a location where a reagent is added to the sample by a reagent probe arm 115. The reagent arm is movable between a reagent location, the sample vessel and the wash station. The sample vessel may receive additional reagents and is then subjected to testing, as know to those skilled in the art. It is clear that sample carryover, or contamination, can occur if the sample probes are not cleaned between aspirations of different test samples.
  • FIG. 2 illustrates an [0029] example probe arm 110. The arm includes a probe 114 that can be moved about a horizontal arc and in a vertical direction. The probe has a hollow center that allows aspiration of a fluid and the subsequent introduction of a wash fluid. The mechanics of the probe arm are not described in detail herein, but are generally know to those skilled in the art. For purposes of understanding the invention, the arm is controllable to regulate the amount of sample aspirated and the amount and duration of wash fluid that flows through the probe.
  • Referring to FIG. 3, a cross-section view of a [0030] probe 114 and wash cup 126 are illustrated. The size and shape of the probe and wash cup are illustrative only and not intended to reflect actual designs or sizes. Those skilled in the art with the benefit of the present description will appreciate that the probe and wash cup design can vary without departing from the present invention. The probe is substantially tube-shaped and includes an exterior surface 132 and an interior surface 130. An interior wash dispenser 136, or nozzle, is located to discharge a wash fluid into the interior region of the probe. During a wash operation, the probe is vertically positioned in the wash cup. The wash cup includes one or more exterior wash dispensers 138, or nozzles, positioned to spray a wash fluid toward a center region of the cup and onto the exterior of the probe.
  • The wash fluid pumped through the probe and on its exterior is the same fluid and depends upon the material that is to be removed from the probe. The wash fluid can be located in a [0031] common reservoir 140 and pumped to the nozzles using separate pumps 142 and 144. Alternately, a single pump and controllable valves can be used to pump the wash fluid to the nozzles. The present invention is not limited to a specific pump design, provided the termination of the internal fluid and the external fluid can be separately controlled by pump(s) controller 150. The term ‘pump’ is intended to include any mechanism that allows for controlled movement of a liquid, such as the wash fluid.
  • As explained above, the probe needs to be sufficiently cleaned between sample aspirations to reduce sample carryover. The sample carryover can be a test sample or reagent depending upon the probe. The internal wash is terminated prior to terminating the external wash. This termination overlap significantly reduces sample carryover and allows clinical chemistry testers to meet restrictive specifications of immunoassay testers. One example wash for chemistry sampling volume below a predetermined threshold (such as 15 μL or less) includes a one second external sample probe wash that ends 100 ms after the internal sample probe wash. The external wash can begin prior to the internal wash without departing from the present invention. [0032]
  • The present invention is not limited to an integrated clinical chemistry/immunoassay tester, and other analytical systems can utilize the relationship of between-sample carryover performance to improve sample wash parameters. This includes other clinical chemistry and immunoassay systems as well as hematology and other methodologies. The wash method can also be used utilized for reagent carryover washing, sample pretreatment instrumentation, and with laboratory automation systems. [0033]
  • CONCLUSION
  • A clinical tester has been described that includes a probe to aspirate a fluid. The probe is washed between aspirations to reduce carryover. The wash operation includes both an internal and an external wash, where the internal wash operation is terminated prior to terminating the external wash. In one embodiment, the probe wash can be implemented on an integrated clinical chemistry/immunoassay tester. [0034]
  • Although specific embodiments have been illustrated and described herein, it will be appreciated by those of ordinary skill in the art that any arrangement, which is calculated to achieve the same purpose, may be substituted for the specific embodiment shown. This application is intended to cover any adaptations or variations of the present invention. Therefore, it is manifestly intended that this invention be limited only by the claims and the equivalents thereof. [0035]

Claims (25)

1. A fluid tester comprising:
a probe having an interior region and an exterior surface, wherein the sample probe is used to selectively aspirate a fluid into the interior region;
a first wash mechanism coupled to the probe to dispense a wash fluid through the interior region of the probe for a first predetermined period; and
a second wash mechanism located to dispense the wash fluid on the exterior surface of the probe for a second predetermined period, wherein the second predetermined period extends beyond the first predetermined period.
2. The fluid tester of claim 1 wherein the aspirated fluid is 15 μL or less in volume and the second predetermined period is about one second and the second predetermined period extends about 0.1 second beyond the first predetermined period.
3. The fluid tester of claim 1 wherein the second wash mechanism is a cup having at least one wash fluid nozzle directed toward a center area of the cup.
4. A clinical analyzer comprising:
a sample probe arm comprising a probe having an interior region and an exterior surface, wherein the probe is used to selectively aspirate a test sample into the interior region;
a sample wash mechanism coupled to the sample probe arm to dispense a sample wash fluid through the interior region of the probe for a first predetermined period; and
a sample wash station to receive the probe and dispense the sample wash fluid on the exterior surface of the probe for a second predetermined period, wherein the second predetermined period extends beyond the first predetermined period.
5. The clinical analyzer of claim 4 further comprising a reagent probe arm to aspirate a reagent.
6. The clinical analyzer of claim 5 further comprising:
a reagent wash mechanism coupled to the reagent probe arm to dispense a reagent wash fluid through an interior region of a reagent probe for a third predetermined period; and
a reagent wash station to receive the reagent probe and dispense the reagent wash fluid on the exterior surface of the reagent probe for a fourth predetermined period, wherein the fourth predetermined period extends beyond the third predetermined period.
7. The clinical analyzer of claim 4 wherein the second predetermined period is about one second and the second predetermined period extends about 0.1 second beyond the first predetermined period.
8. The clinical analyzer of claim 4 further comprising:
a sample transporter to transport a sample container containing a test fluid used to aspirate the test sample;
a chemistry analyzer coupled to sample the test fluid located on the sample transporter; and
an immunoassay analyzer coupled to sample the test fluid located on the sample transporter.
9. The clinical analyzer of claim 4 wherein the immunoassay analyzer comprises:
a second sample probe arm comprising a second probe having an interior region and an exterior surface, wherein the second probe is used to selectively aspirate a second test sample into the interior region of the second probe;
a second sample wash mechanism coupled to the second sample probe arm to dispense the sample wash fluid through the interior region of the second probe for a third predetermined period; and
a second sample wash station to receive the second probe and dispense the sample wash fluid on the exterior surface of the second sample probe for a fourth predetermined period, wherein the fourth predetermined period extends beyond the third predetermined period.
10. A probe cleaning system comprising:
a wash pump coupled to dispense a wash fluid through an interior region of the probe for a first predetermined time period; and
a second wash pump located to dispense the wash fluid on an exterior surface of the probe for a second predetermined period, wherein the second predetermined period extends beyond the first predetermined period.
11. The probe cleaning system of claim 10 wherein a difference between a termination time of the first predetermined period and a termination time of the second predetermined time period is about ten percent (10%) of the second predetermined period.
12. A method of cleaning a fluid probe comprising:
flushing an interior region of the fluid probe with a wash fluid for X seconds; and
simultaneously flushing an exterior surface of the fluid probe with the wash fluid for Y seconds, wherein Y is greater than X.
13. The method of claim 12 where a difference between a termination time of the interior region flush and a termination time of the exterior surface flush is about 0.1 Y.
14. The method of claim 13 where Y is approximately one second.
15. A method of reducing sample carryover in an integrated chemistry and immunoassay analyzer comprising:
aspirating a first test sample from a first sample container using a probe;
depositing the first test sample into a reaction vessel;
performing a clinical analysis of the test sample;
washing the probe by pumping a wash fluid through an interior region of the probe and pumping the wash fluid on an exterior of the probe, wherein the pumping of the wash fluid is terminated from the interior region prior to terminating the pumping of the exterior; and
aspirating a second test sample from a second sample container using the probe.
16. The method of claim 15 wherein the pumping of the wash fluid on the exterior starts prior to pumping the wash fluid through the interior region.
17. The method of claim 16 wherein the wash fluid is pumped on the exterior for about one second.
18. The method of claim 17 wherein the pumping of the wash fluid through the interior region is terminated about 0.1 seconds prior to terminating the pumping of the wash fluid on the exterior.
19. The method of claim 15 further comprising:
aspirating a second test sample from the first sample container using a second probe;
depositing the second test sample into a second reaction vessel; and
performing an immunoassay analysis of the second test sample.
20. The method of claim 19 wherein the clinical analysis is either a chemistry or immunoassay analysis.
21. A method of cleaning a probe comprising:
activating a first pump to pump a wash fluid through an interior region of the probe;
activating a second pump to pump the wash fluid onto an exterior region of the probe;
deactivating the first pump after a first predetermined time period; and
deactivating the second pump after a second predetermined time period, wherein the second predetermined time period is longer than the first predetermined time period.
22. A method of washing a probe comprising:
determining an amount of fluid to be aspirated inside the probe; and
selecting an external wash profile in response to the amount of fluid aspirated inside the probe.
23. The method of claim 22 wherein the wash profile comprises a first wash sequence having both an internal and external probe wash, and an extended external wash if the amount of fluid aspirated exceeds a predetermined threshold.
24. The method of claim 23 wherein the extended external wash is about three times as long as the first wash sequence.
25. A method of reducing carryover in a clinical tester as a result of external probe contamination comprising:
inserting the probe into a fluid;
determining an amount of fluid to be aspirated inside the probe;
dispensing the aspirated fluid;
washing the inside of the probe; and
selecting an external wash profile in response to the amount of fluid aspirated inside the fluid probe, wherein an extended external wash is provided if the amount of fluid aspirated exceeds a pre-determined amount.
US10/158,495 2002-05-29 2002-05-29 Clinical tester wash and method Abandoned US20030223472A1 (en)

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US10/158,495 US20030223472A1 (en) 2002-05-29 2002-05-29 Clinical tester wash and method
EP03756244A EP1518125A2 (en) 2002-05-29 2003-05-29 Probe washing method in a clinical tester
PCT/US2003/016872 WO2003102597A2 (en) 2002-05-29 2003-05-29 Probe washing method in a clinical tester
EP12150274.4A EP2463663A3 (en) 2002-05-29 2003-05-29 Clinical tester wash and method
CA2486264A CA2486264C (en) 2002-05-29 2003-05-29 Clinical tester wash and method
JP2004514403A JP2005527839A (en) 2002-05-29 2003-05-29 Probe cleaning method in clinical test equipment
US12/714,601 US8759106B2 (en) 2002-05-29 2010-03-01 Clinical analyzer wash and method
JP2010046040A JP5437115B2 (en) 2002-05-29 2010-03-03 Probe cleaning method in clinical test equipment
US14/306,961 US9308560B2 (en) 2002-05-29 2014-06-17 Clinical analyzer wash and method
US15/095,893 US20160223575A1 (en) 2002-05-29 2016-04-11 Clinical analyzer wash and method

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US14/306,961 Expired - Fee Related US9308560B2 (en) 2002-05-29 2014-06-17 Clinical analyzer wash and method
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US15/095,893 Abandoned US20160223575A1 (en) 2002-05-29 2016-04-11 Clinical analyzer wash and method

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CA2486264C (en) 2014-02-18
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US20160223575A1 (en) 2016-08-04
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US20140290706A1 (en) 2014-10-02

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