WO2009155422A1 - Centrifuge loading process within an automated laboratory system - Google Patents

Centrifuge loading process within an automated laboratory system Download PDF

Info

Publication number
WO2009155422A1
WO2009155422A1 PCT/US2009/047803 US2009047803W WO2009155422A1 WO 2009155422 A1 WO2009155422 A1 WO 2009155422A1 US 2009047803 W US2009047803 W US 2009047803W WO 2009155422 A1 WO2009155422 A1 WO 2009155422A1
Authority
WO
WIPO (PCT)
Prior art keywords
centrifuge
loading
buckets
samples
centrifuges
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.)
Ceased
Application number
PCT/US2009/047803
Other languages
French (fr)
Inventor
Kerry Lynn Miller
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Siemens Healthcare Diagnostics Inc
Original Assignee
Siemens Healthcare Diagnostics Inc
Priority date (The priority date 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 date listed.)
Filing date
Publication date
Application filed by Siemens Healthcare Diagnostics Inc filed Critical Siemens Healthcare Diagnostics Inc
Priority to JP2011514808A priority Critical patent/JP5398827B2/en
Priority to EP09767731.4A priority patent/EP2296819B1/en
Publication of WO2009155422A1 publication Critical patent/WO2009155422A1/en
Anticipated expiration legal-status Critical
Ceased legal-status Critical Current

Links

Classifications

    • BPERFORMING OPERATIONS; TRANSPORTING
    • B04CENTRIFUGAL APPARATUS OR MACHINES FOR CARRYING-OUT PHYSICAL OR CHEMICAL PROCESSES
    • B04BCENTRIFUGES
    • B04B13/00Control arrangements specially designed for centrifuges; Program control of centrifuges
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B04CENTRIFUGAL APPARATUS OR MACHINES FOR CARRYING-OUT PHYSICAL OR CHEMICAL PROCESSES
    • B04BCENTRIFUGES
    • B04B5/00Other centrifuges
    • B04B5/10Centrifuges combined with other apparatus, e.g. electrostatic separators; Sets or systems of several centrifuges
    • 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
    • G01N35/00584Control arrangements for automatic analysers
    • G01N35/0092Scheduling
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B04CENTRIFUGAL APPARATUS OR MACHINES FOR CARRYING-OUT PHYSICAL OR CHEMICAL PROCESSES
    • B04BCENTRIFUGES
    • B04B11/00Feeding, charging, or discharging bowls
    • B04B11/04Periodical feeding or discharging; Control arrangements therefor
    • B04B2011/046Loading, unloading, manipulating sample containers
    • 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
    • G01N2035/00465Separating and mixing arrangements
    • G01N2035/00495Centrifuges
    • 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
    • G01N35/00584Control arrangements for automatic analysers
    • G01N35/0092Scheduling
    • G01N35/0095Scheduling introducing urgent samples with priority, e.g. Short Turn Around Time Samples [STATS]
    • 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
    • Y10T436/111666Utilizing a centrifuge or compartmented rotor

Definitions

  • the present invention relates to an automated clinical sample treatment and transportation system with one or more independent analytical stations having samples supplied thereto by a conveyor after being processed one of at least two centrifuges. More particularly, the present invention relates to a centrifuge loading process that enables high-priority samples to be centrifuged in a centrifuge that minimizing delays arising from other samples already loaded for centrifugation.
  • a wide variety of automated chemical analyzers are known in the art and are continually being improved to increase analytical menu and throughput, to reduce turnaround time, and to decrease requisite sample volumes.
  • These analyzers conduct assays using reagents to identify analytes in biological fluid samples such as urine, blood serum, plasma, cerebrospinal liquids and the like. For convenience and safety reasons, these fluid samples almost universally contained in capped sample tubes.
  • the assay reactions generate various signals that can be manipulated to determine the concentration of analyte in the sample. See for example, U. S. Pats. Nos. 7,101 ,715 and 5,985,672 and assigned to the assignee of the present application and incorporated herein by reference.
  • LAS Laboratory Automation Systems
  • U.S. Patents 6,984,527 and 6,442,440 both incorporated herein by reference.
  • These LAS handle a number of different patient specimens contained in standard, bar code- labeled, evacuated tubes.
  • the bar code label contains an accession number coupied to demographic information that is entered into a hospital's Laboratory Information System (US) along with test orders and other desired information.
  • US Laboratory Information System
  • An operator places the labeled tubes onto the LAS system which automatically sorts and routes samples to the requisite processing devices for pre-analyttcal operations like centrifugation, decapping, and aliquot preparation prior to the sample being subjected to analysis by one or more analytical stations also "linked" to the LAS.
  • plasma obtained from whole blood by centrifugation
  • an anticoagulant such as citrate or heparin is added to the blood specimen immediately after it is originally obtained or the anticoagulant is placed in an empty blood collection tube prior to the patient sample being obtained. The specimen may then be centrifuged at a later time to separate plasma from blood cells.
  • Plasma and blood serum can be used interchangeably. Serum resembles plasma in composition but lacks the coagulation factors as serum is obtained by allowing a blood specimen to clot prior to centrifugation.
  • a serum-separating tube may be used which contains an inert catalyst (glass beads or powder) to facilitate clotting as well as a portion of gel with a density designed to take up a location between the liquid and cellular layers in the tube after centrifugation, making separation more convenient.
  • an inert catalyst glass beads or powder
  • the anticoagulants in plasma can interfere with certain analytical results on serum.
  • a citrated evacuated blood collection tube is usually used, as the anticoagulant effects of citrate is dependent upon concentration and can be reversed for testing. Serum, therefore, is therefore inappropriate for coagulation tests.
  • centrifuge protocols For purposes of processing efficiency, when incoming samples are placed into an LAS 1 it is a general practice to set aside and “batch-together" those samples that have the same centrifuge protocol requirement. At a convenient time, an available centrifuge is adjusted to operate with the operating parameters to provide the required centrifuge protocol and the batch of samples are processed as a group.
  • centrifugation requires tens of minutes for cycling through a load of tubes by loading centrifuge baskets in a balanced pattern with blood samples taken from the LAS conveyor, spinning the loaded centrifuge baskets, unloading the processed tubes and returning them to the LAS conveyor, if all samples to be handled by an LAS are of routine priority, samples are processed in a first- in -first- out scheduling process.
  • STAT turn-around-time
  • STAT samples are identified during loading onto the LAS, are routed ahead of routine samples and are centrifuged per the requisite centrifuge protocol prior to being shuttled to an appropriate analyzer.
  • An undesirable and unavoidable delay arises when the LAS centrifuge is set up for one centrifuging protocol and the STAT sample has a different centrifuging requirement; this requires that centrifugation of samples in the centrifuge be completed and unloaded and that the established protocol be changed to match the STAT sample's requirements.
  • this delay can be partially ameliorated by providing more that one centrifuge set up with different operating protocols.
  • U.S. Pat. No. 6,060,022 discloses a LAS that is operated as generally described above.
  • the LAS has an input workstation, one or more analyzers, and an automated centrifuge for automatically processing multiple sample containers.
  • the workstation includes multiple input locations for inputting sample containers with at least one location selected for high-priority samples. Only one centrifuge is employed, thereby introducing processing inefficiencies because of the relatively long time required for centrifuging.
  • samples having similar centrifugation requirements are "staged together" and processed in serial batches until all are completed. STAT samples are placed at the front of the line of incoming samples but are not given any special priority as far as being centrifuge processing within a batch.
  • the present invention provides a scheduling process for loading samples into two or more centrifuges in a loading scheme that reduces the time required for high priority sample to be centrifuged. This is accomplished by initially loading a first centrifuge to less than full capacity and processing samples while the remaining second centrifuge is loaded to full capacity before being operated. Subsequently, both centrifuges are loaded to full capacity prior to being operated. As a result, there is a time-shift in the operational status of the two centrifuges so that a high-priority sample may advantageously be shuttled to whichever of the two centrifuges will be next-first- fully loaded and thus next-centrifuged.
  • the present invention is a method for operating a laboratory automation system having a conveyor for transporting individual sample tubes from a sample loading/unloading station to either of at least two centrifuges by initially loading one of the centrifuges to a centrifuging capacity that is less than or about half of full centrifuging capacity, and operating and refilling this centrifuge. Meanwhile, at the same time initially loading a second centrifuges to full capacity and operating and refilling this centrifuge so that STAT samples may be supplied to whichever of the centrifuges is most closely refilled to full capacity.
  • FiG. 1 is a simplified schematic plan view of a prior art automated sample handling system including a conveyor controlled in cooperation with several preanalysis sample treatment stations and analytical stations in which the present invention may be employed advantageously;
  • FIG. 2 is a simplified schematic plan view of two centrifuges in the automated sample handling system of FIG. 1 ;
  • FIGs. 3A-3D are a simplified schematic plan view of a prior art centrifuge loading scheme for the two centrifuges in the automated sample handling system of FIG. 1 ;
  • FIGs. 4A-4D are a simplified schematic plan view of the scheme of the present invention for loading samples into the two centrifuges in the automated sample handling system of FIG. 1 ;
  • FIG. 5 is a timing plot of the prior art loading scheme of FIGs. 3-3D.
  • FIG. 6 is a timing plot of the present invention loading scheme of FIGs.
  • FIG. 1 shows an automated clinical laboratory sample handling LAS 10 capable of automatically pre-processing multiple sample containers 20, typically sample test tubes 20, contained in multiple-tube sample racks 18 prior to analysis by an analyzer 32, 38 or 42.
  • specimens to be automatically processed are provided to laboratory automation system LAS 10 in capped containers 20.
  • Each of the sample containers 20 is provided with identification indicia, such as a bar code, machine readable by a sensor 19 and indicating a patient's identification as well as the assay procedures to be accomplished upon the sample therein.
  • the containers 20 are generally held in multiple-tube racks 18 that generally have additional identification indicia thereon.
  • LAS 10 comprises an operating base 12 upon which a belt-like conveyor track 14 transports individual sample tube containers 20 carried in sample container carriers 22 from a sample container loading/unloading station 16, having more than one multiple-tube rack 18, as well as a high-priority, STAT active input lane, to one of two automated centrifuges 24A and 24B. After being centrifuged, sample tube containers 20 are transported therefrom to an automated tube de-capper 30 for automatically removing caps from capped sample containers 20 and therefrom to one or more analyzers 32, 38, and 42 before returning the original sample tube containers 20 to the sample tube loading/unloading robotic station 16.
  • a remote analyzer 43 may be serviced by LAS 10 even though the remote analyzer 43 is not directly linked to LAS 10, for instance by an independent robotic system.
  • the sample handling LAS 10 has a number of sensors 19 for detecting the location of a sample tube container 20 by means of identifying indicia placed on or within each sample tube carrier 22. Conventional bar-code readers may be employed in such tracking operations.
  • Centrifuges 24A and 214B and each analyzer 38, 42 and 32 are generally equipped with various loading mechanisms 26A and 24B and 28, 40 and 44 or tracks 34 and 36, respectively, for removing a sample tube carrier 22 from track 14, moving the sample tube carrier 22 to and from centrifuges 24A and 24B, to and from or into and out from analyzers 38, 42 and 42, respectively.
  • sample tube containers 20 may be removed from a sample tube carrier 22 for such processing.
  • the loading/unloading station 16 includes at least two X-Y-Z robotic arms 21 conventionally equipped with robotic clamping hands.
  • Sample handling LAS 10 is controlled by a conventionally programmed computer 15, preferably a microprocessor based central processing unit CPU 15, housed as part of or separate from the system 10 to control movement of the sample tube carrier 22 throughout LAS 10 whereat various types of assay processing occurs, as described below.
  • CPU 15 controls sample handling system 10 according to software, firmware, or hardware commands or circuits like those used on the Dimension® clinical chemistry analyzer sold by Siemens Healthcare Diagnostics inc. of Deerfield, IL., and are typical of those skilled in the art of computer-based electromechanical control programming.
  • the present invention may be implemented using a computer interface module ClM that allows for a user to easily and quickly access a variety of control screens and status information display screens that fuily describe a plurality of interrelated automated devices used for sample preparation and clinical analysis of a patient's biological sample.
  • a CiM preferably employs a first display screen that is directly linked to a plurality of additional display screens containing on-line information about the operational status of plurality of interrelated automated devices as well as information describing the location of any specific sample and the status of clinical tests to be performed on the sample.
  • the CIM is thus adapted to facilitate interactions between an operator and automated clinical anaiytical system 10 wherein the module comprises a visual touch screen adapted to display a menu including icons, scroll bars, boxes and buttons through which the operator may interface with the clinical analytical system and wherein the menu comprises a number of function buttons programmed to display functional aspects of the cli ⁇ icai analytical system.
  • FIG. 2 illustrates a typical centrifuge loading station 46, like those disclosed in U. S. Pat. 6,060,022 and 6,589,789, adapted to remove a sample tube 20 carried by a sample tube carrier 22 from track 14 and to place individual sample tubes 20 in a weight-balanced pattern into open receptacles (not shown for purposes of clarity) in a centrifuge bucket 50 disposed temporarily on a first bucket weighing and loading platform 52.
  • Centrifuge loading station 46 is provided with a bucket transfer device 48 adapted to remove a weight-balanced centrifuge bucket 50 from first loading platform 52 and to place the weight-balanced centrifuge bucket 50 into centrifuge 24A for centrifuging.
  • centrifuge buckets 50 are loaded on the first loading platform 52 placed into centrifuge 24A so as to maintain an overall balanced load within centrifuge 24A.
  • centrifuge buckets 50 are placed into centrifuge 24A in opposing pairs, in addition, a bucket 50 may be artificially balanced by moving differently weighted sample tubes 20 into different open receptacles and/or by employing "dummy" tubes 20 having known weights therein.
  • centrifuge loading station 46 is even further provided with bucket transfer device 48 adapted to remove a centrifuge buckets 50 from centrifuge 24A one after another and to place each centrifuge bucket 50 onto a first bucket unloading platform 54.
  • bucket transfer device 48 is adapted to remove centrifuged sample tubes 20 from centrifuge bucket 50 disposed on first bucket unloading platform 54 and to replace the now-centrifuged sample tubes 20 into carriers 22 onto track 14 for subsequent pre- analytical processing and/or for analysis.
  • FIG. 2 basicaliy illustrates centrifuge loading station 46 with buckets 50 loaded with samples 20 removed from track 14 and awaiting centrifugation, buckets 50 loaded with samples 20 during centrifugation and buckets 50 loaded with samples 20 subsequent to centrifugation and ready to be replaced in sample tube carriers 22 on track 14.
  • This process is known to and practiced by those skilled in the art, particularly those bucket loading operations that involve and require weight balancing of buckets 50.
  • Terminology universally understood by those skilled in the art include phrases like "loaded”, “balanced”, “carrier”, “bucket”, “rotor”, “insert” and “rack” and are used herein without detailed explanation.
  • the present invention is advantageously practiced in an LAS 10 having at least two centrifuges 24A and 24B, the second centrifuge 24B provided with a second centrifuge loading station 56 for handling sample tubes 20 carried by a sample tube carriers 22 in a manner similar to that described for loading and unloading centrifuge 24A.
  • the second centrifuge loading station 56 is adapted to remove a sample tube 20 from a sample tube carrier 22 on track 14 and to place individual sample tubes 20 in a weight-balanced pattern within a centrifuge bucket 50 disposed temporarily onto a second bucket loading platform 58 and to place the weight-balanced centrifuge bucket 50 into centrifuge 24B for centrifuging.
  • centrifuge loading station 56 is even further adapted to remove a centrifuge bucket 50 from centrifuge 24B and to place the centrifuge bucket 50 onto a second bucket unloading platform 60.
  • centrifuge loading station 46 is adapted to remove a sample tube 20 from a centrifuge bucket 50 disposed on second bucket unloading platform 60 and to replace a now-centrifuged sample tubes 20 into a sample tube carrier 22 onto track 14 for subsequent processing.
  • sample tubes 20 are presented to centrifuges 24A and
  • Bucket loading procedures like this alternating "odd-even” scheme are employed in state of art laboratory automation because of an emphasis on increasing overall laboratory throughput.
  • "empty" centrifuge buckets 50 on bucket loading platform 52 continue to be loaded with "odd-numbered” sample tubes 20
  • "empty” centrifuge buckets 50 on bucket loading platform 58 on centrifuge 24B continue to be loaded with "even-numbered” sample tubes 20.
  • a hospital laboratory must also be prepared to handle high-priority STAT (short-turn-around-time) samples and this is usually done by having dedicated STAT processing lines. This is a costly but effective, approach particularly when the alternative of a delayed test result for a critically ill patient is considered.
  • the present invention embraces the needs of the laboratory and manages multiple priorities with minimal disruption to the processing of routine samples.
  • the present invention solves this dilemma and further reduces the time required to bring a high-priority, STAT sample tube 20 to either of centrifuge 24A or 24B by initially loading one of the two available centrifuges, 24A or 24B, with buckets 50 that have been loaded with less than the full capacity of each bucket 50. This is achieved using the previously described alternating "odd-even" sample tube 20 loading procedure.
  • FIG. 4B illustrates four of such sample tubes 20 loaded into opposed buckets 5OA and 50 C on bucket loading platform 52 and four of such sample tubes 20 loaded into bucket on bucket loading platform 58.
  • opposed buckets 5OA and 50 C may optionally be transferred to centrifuge 24A (FIG 4C) and the centrifuging process begun; alternately, the previously described alternating "odd-even" sample tube 20 loading procedure may be continued until all four buckets 50 A, 5OC, 5OD and 5OE are loaded to a less-than-ful! loading” condition prior to being transferred to centrifuge 24A as shown in FIG.
  • centrifuge 24A may be operated at this "iess-than-fully load” condition (Fig 4E).
  • Fig 4E the previously alternating "odd- even" sample tube 20 loading procedure of buckets 5OB, 50F, 5OG and 5OH on bucket loading platform 58 is continued as indicated in Fig. 4D.
  • the STAT sample may advantageously be shuttled to which ever of the two centrifuges 24A or 24B is in a most closely filled situation. Because the initial loading of the first centrifuge 24A was done in a manner that allowed centrifuging of the "less-than-full loaded" buckets 50A-C-D-E to begin after a loading-time less than the time required to normally fill buckets 50A-C-D-E to full capacity, one of the two centrifuges 24A or 24B will be "ahead" of the other in terms of being loaded for centrifuging.
  • This STAT processing advantage may also be illustrated by comparing the timing diagrams of centrifuge loading scheme of the prior art as depicted in Fig. 5 with the centrifuge loading scheme of the present invention as depicted in Fig. 6. in Fig. 5, buckets 50 A, 5OC, 5OD and 5OE on bucket loading platform 52 and buckets 5B, 50F, 5OG and 5OH on bucket loading platform 58 are filled to 100% of capacity in the alternating "odd-even" prior art loading scheme.
  • a STAT sample tube 20 appears at point "A", when minimal loading of any of buckets 50A-H has taken place, a relatively greater amount of time must lapse before the STAT tube can be placed in a bucket 50A-H to be spun by either centrifuge 24A or 24B. If a STAT sample tube 20 appears at point "B", when about 50% or half of any bucket 50A-H has taken place, an amount of time required for "half-loading" must lapse before bucket 50A-H can be placed in a centrifuge 24A or 24B for centrifuging.
  • Fig. 6 illustrates the reduction in time lapse before the STAT sample tube
  • centrifuge 24A begins processing sample tubes 20 a shorter amount of time before centrifuge 24B begins processing sample tubes 20.
  • at least the first two buckets 50A-C are less than or about half-loaded with sample tubes 20 and then placed onto centrifuge 24A for centrifuging.
  • the STAT sample tube 20 may be advantageously shuttled to which ever of the two centrifuges 24A or 24B is in a most closely filled situation and most immediately available for centrifuging. For example if a STAT sample tube 20 appears at point "A”, centrifuge 24A is much more closely ready for centrifuging than is centrifuge 24B and so the STAT sample tube 20 would be sent to centrifuge 24A. If a STAT sample tube 20 appears at point "B", centrifuge 24A is basically at the beginning of a loading process and so the STAT sample tube 20 would advantageously be sent to centrifuge 24B for centrifuging.
  • STAT sample tube 20 appears at point "C"
  • centrifuge 24B is nearly filled for centrifuging and so the STAT sample tube 20 would advantageously be sent to centrifuge 24B for centrifuging.
  • STAT sample tubes 20 will, on average, be presented for centrifuging with a processing delay that is about 50% less than STAT tubes 20 that are centrifuged using loading procedures that are currently practiced.

Landscapes

  • Physics & Mathematics (AREA)
  • Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Chemical & Material Sciences (AREA)
  • Analytical Chemistry (AREA)
  • Biochemistry (AREA)
  • General Health & Medical Sciences (AREA)
  • General Physics & Mathematics (AREA)
  • Immunology (AREA)
  • Pathology (AREA)
  • Automatic Analysis And Handling Materials Therefor (AREA)
  • Centrifugal Separators (AREA)

Abstract

A scheduling process for loading samples into two or more centrifuges in a loading scheme that reduces the time required for high priority sample to be centrifuged. One centrifuge is initially loaded to about one-half of capacity and samples processed while the remaining centrifuge is loaded to full capacity before being operated. This creates a time-shift in the operational status of the two centrifuges so that a high-priority sample may advantageously be shuttled to whichever of the two centrifuges will be first-fully loaded and thus next-operated.

Description

CENTRIFUGE LOADING PROCESS WITHIN AN AUTOMATED LABORATORY SYSTEM
FIELD OF THE INVENTION
[0001] The present invention relates to an automated clinical sample treatment and transportation system with one or more independent analytical stations having samples supplied thereto by a conveyor after being processed one of at least two centrifuges. More particularly, the present invention relates to a centrifuge loading process that enables high-priority samples to be centrifuged in a centrifuge that minimizing delays arising from other samples already loaded for centrifugation.
BACKGROUND OF THE INVENTION
[0002] A wide variety of automated chemical analyzers are known in the art and are continually being improved to increase analytical menu and throughput, to reduce turnaround time, and to decrease requisite sample volumes. These analyzers conduct assays using reagents to identify analytes in biological fluid samples such as urine, blood serum, plasma, cerebrospinal liquids and the like. For convenience and safety reasons, these fluid samples almost universally contained in capped sample tubes. The assay reactions generate various signals that can be manipulated to determine the concentration of analyte in the sample. See for example, U. S. Pats. Nos. 7,101 ,715 and 5,985,672 and assigned to the assignee of the present application and incorporated herein by reference. Improvements in analyzer technology, however, may be hampered if sufficient corresponding advances are not made in pre-analytical sample preparation and handling operations like sorting, batch preparation, centrifugation of sample tubes to separate sample constituents, cap removal to facilitate fluid access, and the like.
[0003] To address this need, commercial automated pre-analytical sample preparation systems, called Laboratory Automation Systems (LAS), have been developed to automatically transport sample in tubes to a number of pre-anaiytical sample processing stations that have been "linked together" like described in U.S. Patents 6,984,527 and 6,442,440, both incorporated herein by reference. These LAS handle a number of different patient specimens contained in standard, bar code- labeled, evacuated tubes. The bar code label contains an accession number coupied to demographic information that is entered into a hospital's Laboratory Information System (US) along with test orders and other desired information. An operator places the labeled tubes onto the LAS system which automatically sorts and routes samples to the requisite processing devices for pre-analyttcal operations like centrifugation, decapping, and aliquot preparation prior to the sample being subjected to analysis by one or more analytical stations also "linked" to the LAS.
[0004] For certain clinical assays, plasma, obtained from whole blood by centrifugation, is used in the analysis. To prevent dotting, an anticoagulant such as citrate or heparin is added to the blood specimen immediately after it is originally obtained or the anticoagulant is placed in an empty blood collection tube prior to the patient sample being obtained. The specimen may then be centrifuged at a later time to separate plasma from blood cells.
[0005] For some biochemical laboratory tests, plasma and blood serum can be used interchangeably. Serum resembles plasma in composition but lacks the coagulation factors as serum is obtained by allowing a blood specimen to clot prior to centrifugation. For this purpose, a serum-separating tube may be used which contains an inert catalyst (glass beads or powder) to facilitate clotting as well as a portion of gel with a density designed to take up a location between the liquid and cellular layers in the tube after centrifugation, making separation more convenient. However, the anticoagulants in plasma can interfere with certain analytical results on serum.
[0006] Coagulation tests diagnosis hemorrhagic conditions such as hemophilia, where one or more of the twelve blood clotting factors may be defective, require all clotting factors to be preserved. A citrated evacuated blood collection tube is usually used, as the anticoagulant effects of citrate is dependent upon concentration and can be reversed for testing. Serum, therefore, is therefore inappropriate for coagulation tests.
[0007] From the above, it can be seen that analytical tests may be performed on whole blood, plasma or serum, and that sometimes either plasma or serum may be used. Thus, different centrifugation processes may be required for different patient samples depending upon which clinical tests are to be performed by which analytical stations. Differential spin rates and lengths of time are examples of variables that make up what are hereinafter termed "centrifuge protocols" for different samples. For purposes of processing efficiency, when incoming samples are placed into an LAS1 it is a general practice to set aside and "batch-together" those samples that have the same centrifuge protocol requirement. At a convenient time, an available centrifuge is adjusted to operate with the operating parameters to provide the required centrifuge protocol and the batch of samples are processed as a group.
[0008] In general, centrifugation requires tens of minutes for cycling through a load of tubes by loading centrifuge baskets in a balanced pattern with blood samples taken from the LAS conveyor, spinning the loaded centrifuge baskets, unloading the processed tubes and returning them to the LAS conveyor, if all samples to be handled by an LAS are of routine priority, samples are processed in a first- in -first- out scheduling process. However, non-routine samples requiring a shortest possible turn-around-time (STAT) arise in emergency and surgical operations. STAT samples are consequently given the highest possible priority so as to require the shortest time between receipt and analytical result. STAT samples are identified during loading onto the LAS, are routed ahead of routine samples and are centrifuged per the requisite centrifuge protocol prior to being shuttled to an appropriate analyzer. An undesirable and unavoidable delay arises when the LAS centrifuge is set up for one centrifuging protocol and the STAT sample has a different centrifuging requirement; this requires that centrifugation of samples in the centrifuge be completed and unloaded and that the established protocol be changed to match the STAT sample's requirements. As disclosed in US Ser. No. 11/448,287 incorporated herein by reference, this delay can be partially ameliorated by providing more that one centrifuge set up with different operating protocols. While this provides flexibility if different centrifuges are operated with different operating protocols, throughput may be adversely affected unless the incoming operating load or demand is balanced to match centrifuging capacities. In addition, for simplicity in managing the incoming stream of samples to be centrifuges, incoming samples are processed in the order in which they are introduced to the LAS with different centrifuges being evenly "fed" with samples to be processed. STAT samples are simply placed at the front of the line of incoming samples. [0009] To resolve the difficulties associated with handling samples that require different centrifuge protocols and simultaneously providing accelerated pre-processing for high-priority STAT samples, an LAS having two centrifuges will batch together those samples having the same centrifuge requirements and send them alternately to the two centrifuges. When a STAT sample appears, it is transported to whichever of the two centrifuges can be unloaded must quickly and then the STAT sample is processed immediately if the centrifuge's operating conditions match the STAT sample's centrifuging protocol. If not, the centrifuge's operating conditions must be changed to match the STAT sample's centrifuging protocol and then the STAT sample may be properly centrifuged and conveyed to an appropriate analyzer.
[0010] U.S. Pat. No. 6,060,022 discloses a LAS that is operated as generally described above. The LAS has an input workstation, one or more analyzers, and an automated centrifuge for automatically processing multiple sample containers. The workstation includes multiple input locations for inputting sample containers with at least one location selected for high-priority samples. Only one centrifuge is employed, thereby introducing processing inefficiencies because of the relatively long time required for centrifuging. As discussed above, samples having similar centrifugation requirements are "staged together" and processed in serial batches until all are completed. STAT samples are placed at the front of the line of incoming samples but are not given any special priority as far as being centrifuge processing within a batch.
[0011] Although LAS have advanced the art of sample handling and processing, there remains the challenge of enabling STAT samples to be presented to a centrifuge processing station from the conveyor of an LAS in a scheduling order that minimizes delays from other samples scheduled to be processed by the same centrifuge. Because of the life-saving implications of even slightly reducing the time from receipt of an STAT sample until that STAT sample is made available to a clinical analyzer, such an improvement is highly desirable.
SUMMARY OF THE INVENTION
[0012] The present invention provides a scheduling process for loading samples into two or more centrifuges in a loading scheme that reduces the time required for high priority sample to be centrifuged. This is accomplished by initially loading a first centrifuge to less than full capacity and processing samples while the remaining second centrifuge is loaded to full capacity before being operated. Subsequently, both centrifuges are loaded to full capacity prior to being operated. As a result, there is a time-shift in the operational status of the two centrifuges so that a high-priority sample may advantageously be shuttled to whichever of the two centrifuges will be next-first- fully loaded and thus next-centrifuged. In particular, the present invention is a method for operating a laboratory automation system having a conveyor for transporting individual sample tubes from a sample loading/unloading station to either of at least two centrifuges by initially loading one of the centrifuges to a centrifuging capacity that is less than or about half of full centrifuging capacity, and operating and refilling this centrifuge. Meanwhile, at the same time initially loading a second centrifuges to full capacity and operating and refilling this centrifuge so that STAT samples may be supplied to whichever of the centrifuges is most closely refilled to full capacity.
BRIEF DESCRIPTION OF THE DRAWINGS
[0013] For a better understanding of the invention as well as other objects and further features thereof, reference is made to the following detailed description of various preferred embodiments thereof, taken in connection with the accompanying drawings wherein:
[0014] FiG. 1 is a simplified schematic plan view of a prior art automated sample handling system including a conveyor controlled in cooperation with several preanalysis sample treatment stations and analytical stations in which the present invention may be employed advantageously;
[0015] FIG. 2 is a simplified schematic plan view of two centrifuges in the automated sample handling system of FIG. 1 ;
[0016] FIGs. 3A-3D are a simplified schematic plan view of a prior art centrifuge loading scheme for the two centrifuges in the automated sample handling system of FIG. 1 ; [0017] FIGs. 4A-4D are a simplified schematic plan view of the scheme of the present invention for loading samples into the two centrifuges in the automated sample handling system of FIG. 1 ;
[0018] FIG. 5 is a timing plot of the prior art loading scheme of FIGs. 3-3D; and,
[0019] FIG. 6 is a timing plot of the present invention loading scheme of FIGs.
4A-4D.
DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS
[0020] FIG. 1 shows an automated clinical laboratory sample handling LAS 10 capable of automatically pre-processing multiple sample containers 20, typically sample test tubes 20, contained in multiple-tube sample racks 18 prior to analysis by an analyzer 32, 38 or 42. Typically, specimens to be automatically processed are provided to laboratory automation system LAS 10 in capped containers 20. Each of the sample containers 20 is provided with identification indicia, such as a bar code, machine readable by a sensor 19 and indicating a patient's identification as well as the assay procedures to be accomplished upon the sample therein. The containers 20 are generally held in multiple-tube racks 18 that generally have additional identification indicia thereon.
[0021] LAS 10 comprises an operating base 12 upon which a belt-like conveyor track 14 transports individual sample tube containers 20 carried in sample container carriers 22 from a sample container loading/unloading station 16, having more than one multiple-tube rack 18, as well as a high-priority, STAT active input lane, to one of two automated centrifuges 24A and 24B. After being centrifuged, sample tube containers 20 are transported therefrom to an automated tube de-capper 30 for automatically removing caps from capped sample containers 20 and therefrom to one or more analyzers 32, 38, and 42 before returning the original sample tube containers 20 to the sample tube loading/unloading robotic station 16. It should be understood that more than three analyzers 32, 38, and 42 may be linked by conveyor track 14; for purposes of simplicity, only three are shown. A remote analyzer 43 may be serviced by LAS 10 even though the remote analyzer 43 is not directly linked to LAS 10, for instance by an independent robotic system. The sample handling LAS 10 has a number of sensors 19 for detecting the location of a sample tube container 20 by means of identifying indicia placed on or within each sample tube carrier 22. Conventional bar-code readers may be employed in such tracking operations.
[0022] Centrifuges 24A and 214B and each analyzer 38, 42 and 32 are generally equipped with various loading mechanisms 26A and 24B and 28, 40 and 44 or tracks 34 and 36, respectively, for removing a sample tube carrier 22 from track 14, moving the sample tube carrier 22 to and from centrifuges 24A and 24B, to and from or into and out from analyzers 38, 42 and 42, respectively. Alternately, sample tube containers 20 may be removed from a sample tube carrier 22 for such processing. Typically, the loading/unloading station 16 includes at least two X-Y-Z robotic arms 21 conventionally equipped with robotic clamping hands.
[0023] Sample handling LAS 10 is controlled by a conventionally programmed computer 15, preferably a microprocessor based central processing unit CPU 15, housed as part of or separate from the system 10 to control movement of the sample tube carrier 22 throughout LAS 10 whereat various types of assay processing occurs, as described below. CPU 15 controls sample handling system 10 according to software, firmware, or hardware commands or circuits like those used on the Dimension® clinical chemistry analyzer sold by Siemens Healthcare Diagnostics inc. of Deerfield, IL., and are typical of those skilled in the art of computer-based electromechanical control programming.
[0024] The present invention may be implemented using a computer interface module ClM that allows for a user to easily and quickly access a variety of control screens and status information display screens that fuily describe a plurality of interrelated automated devices used for sample preparation and clinical analysis of a patient's biological sample. Such a CiM preferably employs a first display screen that is directly linked to a plurality of additional display screens containing on-line information about the operational status of plurality of interrelated automated devices as well as information describing the location of any specific sample and the status of clinical tests to be performed on the sample. The CIM is thus adapted to facilitate interactions between an operator and automated clinical anaiytical system 10 wherein the module comprises a visual touch screen adapted to display a menu including icons, scroll bars, boxes and buttons through which the operator may interface with the clinical analytical system and wherein the menu comprises a number of function buttons programmed to display functional aspects of the cliπicai analytical system.
[0025] Fig. 2 illustrates a typical centrifuge loading station 46, like those disclosed in U. S. Pat. 6,060,022 and 6,589,789, adapted to remove a sample tube 20 carried by a sample tube carrier 22 from track 14 and to place individual sample tubes 20 in a weight-balanced pattern into open receptacles (not shown for purposes of clarity) in a centrifuge bucket 50 disposed temporarily on a first bucket weighing and loading platform 52. Centrifuge loading station 46 is provided with a bucket transfer device 48 adapted to remove a weight-balanced centrifuge bucket 50 from first loading platform 52 and to place the weight-balanced centrifuge bucket 50 into centrifuge 24A for centrifuging. In order to avoid an unbalanced centrifuging condition, additional weight-balanced centrifuge buckets 50 are loaded on the first loading platform 52 placed into centrifuge 24A so as to maintain an overall balanced load within centrifuge 24A. Typically, centrifuge buckets 50 are placed into centrifuge 24A in opposing pairs, in addition, a bucket 50 may be artificially balanced by moving differently weighted sample tubes 20 into different open receptacles and/or by employing "dummy" tubes 20 having known weights therein.
[0026] After centrifuging is complete, centrifuge loading station 46 is even further provided with bucket transfer device 48 adapted to remove a centrifuge buckets 50 from centrifuge 24A one after another and to place each centrifuge bucket 50 onto a first bucket unloading platform 54. (For purposes of simplicity, only four sample tubes 20 are illustrated in each centrifuge bucket 50, while in practice a larger number on the order of ten-twenty sample tubes 20 are placed into each centrifuge bucket 50.) Finally, bucket transfer device 48 is adapted to remove centrifuged sample tubes 20 from centrifuge bucket 50 disposed on first bucket unloading platform 54 and to replace the now-centrifuged sample tubes 20 into carriers 22 onto track 14 for subsequent pre- analytical processing and/or for analysis. After all sample tubes 20 have been removed from a centrifuge bucket 50, the empty centrifuge bucket 50 is moved from unloading platform 54 onto loading platform 52 and the process is continued until all of the sample tubes 20 in sample carriers 22 in LAS 10 containing samples requiring some form of separation have been centrifuged and replaced onto conveyor track 14. FlG. 2 basicaliy illustrates centrifuge loading station 46 with buckets 50 loaded with samples 20 removed from track 14 and awaiting centrifugation, buckets 50 loaded with samples 20 during centrifugation and buckets 50 loaded with samples 20 subsequent to centrifugation and ready to be replaced in sample tube carriers 22 on track 14. This process is known to and practiced by those skilled in the art, particularly those bucket loading operations that involve and require weight balancing of buckets 50. Terminology universally understood by those skilled in the art include phrases like "loaded", "balanced", "carrier", "bucket", "rotor", "insert" and "rack" and are used herein without detailed explanation.
[0027] The present invention is advantageously practiced in an LAS 10 having at least two centrifuges 24A and 24B, the second centrifuge 24B provided with a second centrifuge loading station 56 for handling sample tubes 20 carried by a sample tube carriers 22 in a manner similar to that described for loading and unloading centrifuge 24A. In this instance, the second centrifuge loading station 56 is adapted to remove a sample tube 20 from a sample tube carrier 22 on track 14 and to place individual sample tubes 20 in a weight-balanced pattern within a centrifuge bucket 50 disposed temporarily onto a second bucket loading platform 58 and to place the weight-balanced centrifuge bucket 50 into centrifuge 24B for centrifuging. As before, after centrifuging is complete, centrifuge loading station 56 is even further adapted to remove a centrifuge bucket 50 from centrifuge 24B and to place the centrifuge bucket 50 onto a second bucket unloading platform 60. Finally, centrifuge loading station 46 is adapted to remove a sample tube 20 from a centrifuge bucket 50 disposed on second bucket unloading platform 60 and to replace a now-centrifuged sample tubes 20 into a sample tube carrier 22 onto track 14 for subsequent processing.
[0028] In the prior art, sample tubes 20 are presented to centrifuges 24A and
24B in an alternating pattern that begins when a "batch" of sample tubes 20 has been identified for processing within LAS 10. in such an alternating pattern, a first sample tube 20 is placed into a first bucket 5OA on bucket loading platform 52 on centrifuge 24A and then a second sample tube 20 is placed into a bucket 5OB on bucket loading platform 58 on centrifuge 24B. This process is continued, with "odd numbered" sample tubes 20 placed in a bucket 5OA on bucket loading platform 52 on centrifuge 24A while "even numbered" sample tubes 20 are placed in a bucket 50 on bucket loading platform 58 on centrifuge 24B, until both buckets 5OA and 5OB are fully loaded as illustrated in FiG. 3A. As described above and seen in Fig. 3B1 This loading process continues with a "odd-numbered" sample tubes 20 being placed in the remaining centrifuge buckets 50 on bucket loading platform 52 on centrifuge 24A and "even-numbered" sample tubes 20 being placed in the remaining centrifuge buckets 50 on bucket loading platform 58 on centrifuge 24B, as illustrated in FIG. 3B. Subsequently, loaded centrifuge buckets 50 are placed into centrifuges 24A and 24B, as seen in Fig. 3C and the centrifuges are operated using their respective operating protocols. After the centrifuging protocols are completed, the buckets 50 are removed from centrifuges 24A and 24B and placed on bucket unloading platforms 54 and 58, as illustrated in Fig. 3D. Bucket loading procedures like this alternating "odd-even" scheme are employed in state of art laboratory automation because of an emphasis on increasing overall laboratory throughput. Although not shown, during the bucket handling process of FIGs. 3A-D, "empty" centrifuge buckets 50 on bucket loading platform 52 continue to be loaded with "odd-numbered" sample tubes 20 and "empty" centrifuge buckets 50 on bucket loading platform 58 on centrifuge 24B continue to be loaded with "even-numbered" sample tubes 20. However, a hospital laboratory must also be prepared to handle high-priority STAT (short-turn-around-time) samples and this is usually done by having dedicated STAT processing lines. This is a costly but effective, approach particularly when the alternative of a delayed test result for a critically ill patient is considered. The present invention embraces the needs of the laboratory and manages multiple priorities with minimal disruption to the processing of routine samples.
[0029] This prior art procedure for loading in an LAS with at least two centrifuges in an alternating pattern to their full capacity is used because of the simplicity of programming the operation of LAS 10, centrifuge loading stations 46 and 56 and centrifuges 24A and 24B. This practice works well as long as no high-priority, STAT sample tubes 20 are presented to LAS 10, and maintains a constant stream of centrifuged sample tubes 20 to be supplied to subsequent analytical devices. In the event, however, that a high-priority, STAT sample tube 20 is presented to LAS 10 for processing, it is also a common practice to place the high-priority, STAT sample tubes 20 into a high-priority, STAT active input lane from which a high-priority, STAT sample tube 20 can be immediately placed in a sample tube carrier 22 on conveyor track 14. While this practice reduces the time required to bring such a high-priority, STAT sample tube 20 to either of centrifuge 24A or 24B, the previously described pattern for alternating placement into a bucket 50 on bucket loading platform 52 and then on bucket loading platform 58 introduces an adverse time delay because neither one of the buckets 50 on bucket loading platform 52 and on bucket loading platform 56 may be nearing a fully loaded condition.
[0030] The present invention solves this dilemma and further reduces the time required to bring a high-priority, STAT sample tube 20 to either of centrifuge 24A or 24B by initially loading one of the two available centrifuges, 24A or 24B, with buckets 50 that have been loaded with less than the full capacity of each bucket 50. This is achieved using the previously described alternating "odd-even" sample tube 20 loading procedure.
[0031] Subsequent to this "less-than-full initial loading" of, for example, centrifuge
24A, the previously described alternating placement of sample tubes 20 into bucket 5OC on bucket loading platform 52 and continuing into bucket 5OB on bucket loading platform 58, is resumed. Fig. 4B illustrates four of such sample tubes 20 loaded into opposed buckets 5OA and 50 C on bucket loading platform 52 and four of such sample tubes 20 loaded into bucket on bucket loading platform 58. At this stage, opposed buckets 5OA and 50 C may optionally be transferred to centrifuge 24A (FIG 4C) and the centrifuging process begun; alternately, the previously described alternating "odd-even" sample tube 20 loading procedure may be continued until all four buckets 50 A, 5OC, 5OD and 5OE are loaded to a less-than-ful! loading" condition prior to being transferred to centrifuge 24A as shown in FIG. 4D and after being transferred to centrifuge 24A, centrifuge 24A may be operated at this "iess-than-fully load" condition (Fig 4E). During the loading of buckets 50 on bucket loading platform 52, the previously alternating "odd- even" sample tube 20 loading procedure of buckets 5OB, 50F, 5OG and 5OH on bucket loading platform 58 is continued as indicated in Fig. 4D.
[0032] The important advantage of initially loading buckets 50A and 5OC of centrifuge 24A to this "less-than-full" condition as taught by the present invention can produce as much as a 50% reduction in STAT turn-around time in the instance that both centrifuges 24A and 24B are both fully loaded when a STAT sample is presented for processing. As explained below, this is achieved by loading a high-priority sample tube 20 into whichever centrifuge bucket 50 wil! be next placed into centrifuge 24A or 24B.
[0033] In the centrifuge loading scheme of the present invention like illustrated in
Figs. 4-4F, whenever a STAT sample appears, the STAT sample may advantageously be shuttled to which ever of the two centrifuges 24A or 24B is in a most closely filled situation. Because the initial loading of the first centrifuge 24A was done in a manner that allowed centrifuging of the "less-than-full loaded" buckets 50A-C-D-E to begin after a loading-time less than the time required to normally fill buckets 50A-C-D-E to full capacity, one of the two centrifuges 24A or 24B will be "ahead" of the other in terms of being loaded for centrifuging. As a result, there is a time-shift in the operational status of the two centrifuges 24A and 24B so that a high-priority STAT sample tube 20 may advantageously be shuttled to whichever of the two centrifuges 24A or 24B will be first- loaded and thus next-operated. This time differential thereby allows a STAT sample to begin and complete its centrifuging protocol, on average, in 50% less time than is required to fully load a bucket 50.
[0034] This STAT processing advantage may also be illustrated by comparing the timing diagrams of centrifuge loading scheme of the prior art as depicted in Fig. 5 with the centrifuge loading scheme of the present invention as depicted in Fig. 6. in Fig. 5, buckets 50 A, 5OC, 5OD and 5OE on bucket loading platform 52 and buckets 5B, 50F, 5OG and 5OH on bucket loading platform 58 are filled to 100% of capacity in the alternating "odd-even" prior art loading scheme. If a STAT sample tube 20 appears at point "A", when minimal loading of any of buckets 50A-H has taken place, a relatively greater amount of time must lapse before the STAT tube can be placed in a bucket 50A-H to be spun by either centrifuge 24A or 24B. If a STAT sample tube 20 appears at point "B", when about 50% or half of any bucket 50A-H has taken place, an amount of time required for "half-loading" must lapse before bucket 50A-H can be placed in a centrifuge 24A or 24B for centrifuging. if a STAT sample tube 20 appears at point "C", when a greater loading of any buckets 50A-H has taken place, a relatively smaller amount of time must lapse before the bucket 50 holding the STAT sample tube 20 can be placed in a centrifuge 24A or 24B for centrifuging. In general, then, when the experience of a large number of STAT sample tubes 20 is evaluated, point B will be the norm and a "naif-loaded" amount of time must lapse before the STAT tube 20 can be placed in any bucket 50A-H before being transferred to either centrifuge 24A or 24B for centrifuging. In this prior art loading scheme, regardless of whether a STAT sample tube 20 is placed in one of buckets 50A-C-D-E or buckets 50C-F-G-H1 a STAT sample tube 20 will experience the same time lapse before the STAT sample can be centrifuged.
[0035] Fig. 6 illustrates the reduction in time lapse before the STAT sample tube
20 can be placed in a centrifuge 24A or 24B for centrifuging achieved by the present invention. In accord with the present invention, with oniy less-than or half-loaded buckets 50 used in the initial loading of centrifuge 24A, centrifuge 24A begins processing sample tubes 20 a shorter amount of time before centrifuge 24B begins processing sample tubes 20. In particular, as previously described, at least the first two buckets 50A-C are less than or about half-loaded with sample tubes 20 and then placed onto centrifuge 24A for centrifuging. Consequently, there is a time-shift in the operational status of centrifuges 24A and 24B so that whenever a STAT sample tube 20 appears, the STAT sample tube 20 may be advantageously shuttled to which ever of the two centrifuges 24A or 24B is in a most closely filled situation and most immediately available for centrifuging. For example if a STAT sample tube 20 appears at point "A", centrifuge 24A is much more closely ready for centrifuging than is centrifuge 24B and so the STAT sample tube 20 would be sent to centrifuge 24A. If a STAT sample tube 20 appears at point "B", centrifuge 24A is basically at the beginning of a loading process and so the STAT sample tube 20 would advantageously be sent to centrifuge 24B for centrifuging. Finally, if a STAT sample tube 20 appears at point "C", centrifuge 24B is nearly filled for centrifuging and so the STAT sample tube 20 would advantageously be sent to centrifuge 24B for centrifuging. As a benefit of the present invention, STAT sample tubes 20 will, on average, be presented for centrifuging with a processing delay that is about 50% less than STAT tubes 20 that are centrifuged using loading procedures that are currently practiced.
[0036] It should be readily understood by those persons skilled in the art that the present invention is susceptible of a broad utility and application. Many embodiments and adaptations of the present invention other than those herein described, as well as many variations, modifications and equivalent arrangements will be apparent from or reasonably suggested by the present invention and the foregoing description thereof, without departing from the substance or scope of the present invention. For example, as described, either two buckets 5OA and 5OC or four buckets 50A-C-D-E may be initially less-than or about half-loaded to achieve the reduction in deiay of processing a STAT sample tube 20. Further, only two centrifuges have been used in this illustration even though the STAT processing time advantage may be increased by the inclusion of a third centrifuge. Furthermore, for purposes of simplicity in describing the present invention, two sample loading stations 46 and 56 have been employed even though a single sample loading station may be adapted to perform the tasks of both sample loading stations 46 and 56.
[0037] Accordingly, while the present invention has been described herein in detail in relation to specific embodiments, it is to be understood that this disclosure is only illustrative and exemplary of the present invention and is made merely for purposes of providing a full and enabling disclosure of the invention. The foregoing disclosure is not intended or to be construed to limit the present invention or otherwise to exclude any such other embodiments, adaptations, variations, modifications and equivalent arrangements, the present invention being limited only by the claims appended hereto and the equivalents thereof.

Claims

What is claimed is:
1. A method for operating a laboratory automation system having a conveyor for transporting individual sample tubes from a sample loading/unfoading station to either of at least two centrifuges, the centrifuges having known centrifuging capacities, the method comprising: initially loading a first one of said at least two centrifuges to a centrifuging capacity that is less than or about half of full centrifuging capacity; commencing an operation cycle of said first centrifuge and after the operation cycle of said first centrifuge is complete, refilling said first centrifuge to full capacity; initially loading a second one of said at least two centrifuges to a centrifuging capacity that is about full centrifuging capacity; commencing operation of said second centrifuge and after the operation cycle of said first centrifuge is complete, refilling said second centrifuge to full capacity; repeating the loading and operation of said at least two centrifuges; and, supplying high priority samples to whichever of said at least two centrifuges is most cϊosely filled to full capacity.
2. The procedure of claim 1 wherein loading said first centrifuge comprises placing samples in one or more pairs of buckets in a weight balanced pattern.
3. The procedure of claim 1 wherein loading said second centrifuge comprises placing samples in two or more pairs of buckets in a weight balanced pattern.
4. A laboratory automation system adapted for receiving samples to be analyzed and transporting the samples to pre-analytica! sample processing stations including first and second centrifuges, the laboratory automation system comprising: a computer programmed to control the operations of the laboratory automation system and the pre-analytical sample processing stations; a conveyor for transporting said samples to pre-analytical sample processing stations including a first and a second centrifuge; first and second centrifuge loading stations proximate said conveyor for loading samples into a plurality of buckets to be centrifuges by first and a second centrifuges, respectively; wherein the conveyor first and second centrifuge loading stations are controlled so as to alternately deposit samples into buckets at the first centrifuge loading station and into buckets at the second centrifuge loading station so that the buckets at the first centrifuge loading station are initially loaded to less than or about one-half of their full capacity and then placing the less than or about one-half loaded centrifuge buckets into the first centrifuge.
5. The laboratory automation system of claim 4 wherein the second loading station is controlled to load samples into buckets at the second centrifuge loading station until the buckets are loaded to about full capacity and then placing the fully loaded buckets into the second centrifuge.
6. The laboratory automation system of claim 4 wherein the first centrifuge is operated and thereafter the less than or about one-half loaded centrifuge buckets are removed and the first centrifuge loading station is controlled to load samples into buckets until the buckets are loaded to about full capacity and then placing the fully loaded buckets into the first centrifuge.
PCT/US2009/047803 2008-06-19 2009-06-18 Centrifuge loading process within an automated laboratory system Ceased WO2009155422A1 (en)

Priority Applications (2)

Application Number Priority Date Filing Date Title
JP2011514808A JP5398827B2 (en) 2008-06-19 2009-06-18 Centrifuge loading process in an automated laboratory system
EP09767731.4A EP2296819B1 (en) 2008-06-19 2009-06-18 Centrifuge loading process within an automated laboratory system

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US12/142,500 2008-06-19
US12/142,500 US7963900B2 (en) 2008-06-19 2008-06-19 Centrifuge loading process within an automated laboratory system

Publications (1)

Publication Number Publication Date
WO2009155422A1 true WO2009155422A1 (en) 2009-12-23

Family

ID=41431834

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/US2009/047803 Ceased WO2009155422A1 (en) 2008-06-19 2009-06-18 Centrifuge loading process within an automated laboratory system

Country Status (4)

Country Link
US (1) US7963900B2 (en)
EP (1) EP2296819B1 (en)
JP (1) JP5398827B2 (en)
WO (1) WO2009155422A1 (en)

Families Citing this family (29)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US7985375B2 (en) 2007-04-06 2011-07-26 Qiagen Gaithersburg, Inc. Sample preparation system and method for processing clinical specimens
US8703492B2 (en) 2007-04-06 2014-04-22 Qiagen Gaithersburg, Inc. Open platform hybrid manual-automated sample processing system
ITMI20080228A1 (en) * 2008-02-13 2009-08-14 Dachi S R L "CENTRIFUGAL SYSTEM OF URGENT CONTAINERS OF BIOLOGICAL MATERIAL"
US7963900B2 (en) * 2008-06-19 2011-06-21 Siemens Healthcare Diagnostics Inc. Centrifuge loading process within an automated laboratory system
DE102009027462A1 (en) * 2009-07-03 2011-01-05 Robert Bosch Gmbh Device for handling objects
US9953141B2 (en) 2009-11-18 2018-04-24 Becton, Dickinson And Company Laboratory central control unit method and system
EP2752668A3 (en) 2010-07-23 2014-10-15 Beckman Coulter, Inc. System Or Method Of Including Analytical Units
CN103299196B (en) * 2010-12-28 2015-06-24 株式会社日立高新技术 Centrifugal separation device, pretreatment system provided with centrifugal separation device, and control method for the system
KR20140091032A (en) 2011-11-07 2014-07-18 베크만 컬터, 인코포레이티드 Magnetic damping for specimen transport system
ES2778054T3 (en) 2011-11-07 2020-08-07 Beckman Coulter Inc System and method for transporting sample containers
US9446418B2 (en) 2011-11-07 2016-09-20 Beckman Coulter, Inc. Robotic arm
CN104040357B (en) 2011-11-07 2016-11-23 贝克曼考尔特公司 Halver system and workflow
KR20140091033A (en) 2011-11-07 2014-07-18 베크만 컬터, 인코포레이티드 Specimen container detection
WO2013070755A2 (en) * 2011-11-07 2013-05-16 Beckman Coulter, Inc. Centrifuge system and workflow
US9381524B2 (en) 2011-11-08 2016-07-05 Becton, Dickinson And Company System and method for automated sample preparation
WO2013151920A1 (en) * 2012-04-02 2013-10-10 Siemens Healthcare Diagnostics Inc. Virtual sample queues
EP2857822B1 (en) * 2012-05-28 2019-10-30 Hitachi High-Technologies Corporation Specimen processing system and processing method for a centrifuge system
JP6307446B2 (en) * 2013-01-30 2018-04-04 株式会社日立ハイテクノロジーズ Centrifuge system, specimen pretreatment system, and control method
US10058877B2 (en) * 2013-03-08 2018-08-28 Siemens Healthcare Diagnostics Inc. Centrifuge loading/unloading apparatus, systems, and methods
CA2904018C (en) * 2013-03-11 2020-10-27 Siemens Healthcare Diagnostics Inc. Centrifuge loading apparatus, systems, and methods
JP6560927B2 (en) * 2015-08-03 2019-08-14 株式会社日立製作所 Centrifugal processing equipment
US11625025B2 (en) * 2016-05-27 2023-04-11 BIOMéRIEUX, INC. System and method of load balancing specimen containers within detection instruments
JP6901209B2 (en) * 2016-07-21 2021-07-14 シーメンス・ヘルスケア・ダイアグノスティックス・インコーポレーテッドSiemens Healthcare Diagnostics Inc. Managing sample exposure to air on an automated system that performs laboratory in vitro diagnostics
US10427162B2 (en) 2016-12-21 2019-10-01 Quandx Inc. Systems and methods for molecular diagnostics
KR101929540B1 (en) * 2016-12-26 2018-12-14 (주)로봇앤드디자인 Robot and intellection type centrifuge system using the robot technic
EP3639025A1 (en) * 2017-06-16 2020-04-22 DRK Blutspendedienst Baden-Württemberg-Hessen gGmbH Method and apparatus for single tube blood donor screening
US11016070B2 (en) * 2017-07-06 2021-05-25 Live-Pure, Inc. System for assessing the quality of air and drinking water
CN110297100A (en) * 2019-07-04 2019-10-01 深圳市爱康生物科技有限公司 A kind of full-automatic sample processing device
CN115055289A (en) * 2022-07-13 2022-09-16 中元汇吉生物技术股份有限公司 Method, device, equipment and medium for centrifugal control of sample

Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6060022A (en) * 1996-07-05 2000-05-09 Beckman Coulter, Inc. Automated sample processing system including automatic centrifuge device
US20040184959A1 (en) * 2003-01-31 2004-09-23 Teruaki Itoh Specimen centrifuge apparatus
US20070020764A1 (en) * 2005-07-20 2007-01-25 Miller Kerry L Method for processing chemistry and coagulation test samples in a laboratory workcell

Family Cites Families (20)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3151073A (en) * 1960-10-07 1964-09-29 Res Specialties Co Centrifuging apparatus
FR2600166B1 (en) * 1986-06-17 1988-10-07 Rhone Poulenc Rech PROCESS AND DEVICE FOR AUTOMATICALLY SUPPORTING AND ANALYZING SAMPLES OF PRODUCTS RANDOMIZED
US5087423A (en) * 1988-10-20 1992-02-11 Olympus Optical Co., Ltd. Automatic analyzing apparatus comprising a plurality of analyzing modules
US5178834A (en) * 1989-07-19 1993-01-12 Tosoh Corporation Automatic immunoassay analyzer
US5209903A (en) * 1989-09-06 1993-05-11 Toa Medical Electronics, Co., Ltd. Synthetic apparatus for inspection of blood
US5623415A (en) * 1995-02-16 1997-04-22 Smithkline Beecham Corporation Automated sampling and testing of biological materials
JP3031237B2 (en) * 1996-04-10 2000-04-10 株式会社日立製作所 Method of transporting sample rack and automatic analyzer for transporting sample rack
JP3031242B2 (en) * 1996-05-20 2000-04-10 株式会社日立製作所 Multi-item analyzer
JP3336894B2 (en) * 1997-01-29 2002-10-21 株式会社日立製作所 Automatic analyzer
US5730697A (en) * 1997-03-25 1998-03-24 Automed Corporation Automatically loaded swing bucket centrifuge
JP3428426B2 (en) * 1997-03-26 2003-07-22 株式会社日立製作所 Sample analysis system
US6589789B1 (en) * 1997-07-21 2003-07-08 Quest Diagnostics Incorporated Automated centrifuge loading device
DK0902290T3 (en) * 1997-09-11 2009-02-09 Hitachi Ltd A sample handling system for automatic analysis devices
JP3484353B2 (en) * 1998-09-14 2004-01-06 アロカ株式会社 Centrifuge
US6581012B1 (en) * 1999-07-30 2003-06-17 Coulter International Corp. Automated laboratory software architecture
KR20040001439A (en) * 2002-06-28 2004-01-07 (주)바이오넥스 Automated centrifuge system
FR2842912B1 (en) * 2002-07-25 2004-09-10 Junior Instruments PROCESS AND DEVICE FOR THE PRETREATMENT BY CENTRIFUGAL OF SAMPLES.
JP3638931B2 (en) * 2002-10-31 2005-04-13 照明 伊藤 Sample centrifuge system
US7338803B2 (en) * 2003-07-18 2008-03-04 Dade Behring Inc. Method for increasing capacity in an automatic clinical analyzer by using modular reagent delivery means
US7963900B2 (en) * 2008-06-19 2011-06-21 Siemens Healthcare Diagnostics Inc. Centrifuge loading process within an automated laboratory system

Patent Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6060022A (en) * 1996-07-05 2000-05-09 Beckman Coulter, Inc. Automated sample processing system including automatic centrifuge device
US20040184959A1 (en) * 2003-01-31 2004-09-23 Teruaki Itoh Specimen centrifuge apparatus
US20070020764A1 (en) * 2005-07-20 2007-01-25 Miller Kerry L Method for processing chemistry and coagulation test samples in a laboratory workcell

Also Published As

Publication number Publication date
JP5398827B2 (en) 2014-01-29
US20090318276A1 (en) 2009-12-24
EP2296819A4 (en) 2017-05-10
JP2011525243A (en) 2011-09-15
US7963900B2 (en) 2011-06-21
EP2296819A1 (en) 2011-03-23
EP2296819B1 (en) 2018-08-01

Similar Documents

Publication Publication Date Title
US7963900B2 (en) Centrifuge loading process within an automated laboratory system
US6984527B2 (en) Automated quality control protocols in a multi-analyzer system
US9505012B2 (en) Automated sample workcell and method of operation
US20070020764A1 (en) Method for processing chemistry and coagulation test samples in a laboratory workcell
EP2804002B1 (en) Laboratory automated system with common sample buffer module
JP5654048B2 (en) Sample pretreatment system and centrifuge
JP5481122B2 (en) Centrifuge
JP5520385B2 (en) Sample test automation system and control method thereof
JP6307446B2 (en) Centrifuge system, specimen pretreatment system, and control method
EP1881329A2 (en) Method for scheduling samples in a combinational clinical analyzer
JP7181976B2 (en) automatic analyzer
WO2013180017A1 (en) Centrifugal separator, processing system provided with centrifugal separator, and method for controlling said system
JP6426569B2 (en) Sample inspection system
US20240183872A1 (en) Diagnostic instruments having sorting capability and sorting methods thereof
JP2019184604A (en) Laboratory analysis system in which sample pipetting is improved
JP2001004639A (en) Automatic analysis system
JPH03107766A (en) Clinical examination device
WO2025004481A1 (en) Specimen processing device and specimen processing method
CN119224348A (en) Sample analysis system, sample processing system and sample analysis method
JP2011027486A (en) Specimen treatment device
JPH0264462A (en) automatic analysis system

Legal Events

Date Code Title Description
121 Ep: the epo has been informed by wipo that ep was designated in this application

Ref document number: 09767731

Country of ref document: EP

Kind code of ref document: A1

WWE Wipo information: entry into national phase

Ref document number: 2009767731

Country of ref document: EP

ENP Entry into the national phase

Ref document number: 2011514808

Country of ref document: JP

Kind code of ref document: A

NENP Non-entry into the national phase

Ref country code: DE