Source: https://patents.google.com/patent/CA2130013C/en
Timestamp: 2020-08-08 10:39:53
Document Index: 538617815

Matched Legal Cases: ['arts 92', 'art 2', 'art 2', 'art 2', 'art 92', 'art 9', 'art 92', 'art 9', 'art 9', 'art 9', 'arts 92', 'art 92', 'art 9', 'art 2']

CA2130013C - Apparatus for automatic performance of temperature cycles - Google Patents
Apparatus for automatic performance of temperature cycles
CA2130013C
CA2130013C CA 2130013 CA2130013A CA2130013C CA 2130013 C CA2130013 C CA 2130013C CA 2130013 CA2130013 CA 2130013 CA 2130013 A CA2130013 A CA 2130013A CA 2130013 C CA2130013 C CA 2130013C
CA 2130013
CA2130013A1 (en
1993-09-10 Priority to CH271793 priority Critical
1993-09-10 Priority to CH2717/93 priority
1994-08-12 Application filed by F Hoffmann La Roche AG filed Critical F Hoffmann La Roche AG
1995-03-11 Publication of CA2130013A1 publication Critical patent/CA2130013A1/en
1999-03-30 Publication of CA2130013C publication Critical patent/CA2130013C/en
239000011541 reaction mixture Substances 0.000 claims abstract description 23
230000004075 alteration Effects 0.000 claims abstract description 9
150000007523 nucleic acids Chemical class 0.000 claims description 8
238000005382 thermal cycling Methods 0.000 claims description 2
2 ~ Q :L 3 RAN 4090/239 The invention relates to a device for automatic performance of temperature cycles in a number of test tubes, each test tube being closed by a closure and containing a predetermined volume of a liquid reaction mixture, the device containing the following components:
(a) a holder formed with an arrangement of chambers for holding test tubes, each chamber being adapted to receive one test tube, and said holder being of a material which has a high thermal conductivity, and which has an upper surface, a bottom surface and a cylindrical o outer wall, each chamber having an opening located in the upper surface of said holder, (b) a computer-controlled automatic control system, and (c) means actuated by the automatic control system for cyclic alteration of the temperature of the holder.
The invention relates more particularly to a device of this kind, preferably suitable as an integrated component of an automatic analytical device for performing the polymerase chain reaction.
A device of the aforementioned kind is described in EP-A-0 236 069 A2. In this known device, the test tubes are disposed in a matrix, which makes it difficult to obtain a uniform temperature in all test tubes. The device constructed as per EP-A-0 236 069 A2 is relatively bulky and requires relatively high power in operation. It is therefore unsuitable for use as an integrated component of a modern automatic analytical device.
Devices of the initially-mentioned kind are called "thermal cyclers". This term is used in the description hereinafter.
The aim of the invention therefore is to provide a device of the initially-mentioned kind with minimum dimensions and requiring mlnimum power to operate.
Ve / 21.07.94 ~ - 2 - ~ 1 3 ~
According to the invention, this problem is solved by a device of the initially-mentioned kind, characterised in that the chambers in the holder are disposed in a ring and in that the closure of each test tube is piercable by a pipetting needle.
The main advantages of the device according to the invention are that it has relatively small dimensions and requires relatively little power in operation so that it is suitable for use as an integrated component of an automatic analytical device.
Summar,v of the Invention o In accordance with one aspect of the present invention there is provided an automatic analytical device, which comprises: (a) a plurality of test tubes, each for cont~ining a predetermined volume of a liquid reaction mixture, each of the plurality of test tubes being equipped with a pierceable closure; (b) a pipetting needle configured and dimensioned for piercing the pierceable closures and removing liquid reaction mixture from the text tubes; ~c) means for moving the pipetting needle from a position outside of each test tube, through the pierceable closure on the test tube, and into the test tube; (d) means for applying suction to the pipetting needle so as to enable the pipetting needle to withdraw liquid reaction mixture out of a given test tube when the pipetting needle is inside the given test tube and reaction mixture is present within the given test tube; and (e) a device for automatic performance of temperature cycles on the test tubes, which comprises: (1) a holder formed of a thermally conductive material and having an upper surface, a lower surface and acylindrical outer wall, the holder having an array of chambers for holding the test tubes equipped with pierceable closures, the chambers being disposed along an arc with each chamber having an opening located in the upper surface of the holder, each chamber being configured and dimensioned to receive one test tube equipped with a pierceable closure, the holder being configured and dimensioned so that when test tubes having pierceable closures are held in the array of chambers, the pierceable closures of the test tubes can be accessed by a pipetting needle; (2) a computer-regulated automatic control system; and (3) means actuated by the automatic control system for cyclic alteration of the temperature of the holder.
-~ ~ 3 ~ 3 In an embodiment of the present invention, a method for amplifying nucleic acid materials comprising the steps of a) inkoducing into a reaction vessel a sample suspected to contain a target nucleic acid material along with suitable reagents for amplification of said suspected target nucleic acid to form a reaction mixture; b) sealing the reaction mixture inside said reaction vessel by closing a tightly sealing lid of the reaction vessel; c) amplifying the target nucleic acid material within said reaction vessel by an amplification process including thermal cycling of the reaction mixture contained in the reaction vessel; said method being characterized by thefollowing steps:
i) providing said sealing lid with a part that is pierceable by a pipetting needle;
ii) removing a portion of the reaction mixture from said reaction vessel after said amplifying step and without removing the lid of the reaction vessel, wherein said removing is effected by piercing said lid with a pipetting needle and aspirating said portion of the reaction mixture into said pipetting needle; and iii) dispensing said removed portion of the reaction mixture into a distinct detection vessel.
-Description of an embodiment An embodiment of the invention will now be described with reference to the accompanying drawings, in which:
Fig. 2 is a section through line II-II in Fig. 1, the thermocycler 18 being closed;
Fig. 4 is a section on a larger scaIe than in Fig. 2, through the thermal cycler in the closed state;
Fig. 6 is a diagram of a "master-slave" control system for regula~ting and monitoring the operating parameters of a thermal cycler according to the invention;
213001~
Fig. 10 shows the individual parts 92 to 95 in Fig. 8, when B assembled and with the test tubes in the resulting arrangement 23 in the closed state;
Fig. 12 is a section through a test tube 21 in Fig. 9 with closed lid o 87, and Fig. 13 is a perspective overall view of an analytical device, one component of which is a thermal cycler part 2 according to the invention.
Thermal cycler lB In the following description, "thermal cycler" denotes a device for automatic performance of temperature cycles in at least one test tube 21 closed by a closure and holding a predetermined volume of a liquid reaction mixture.
The following is a description of a thermal cycler according to the invention, suitable preferably as a component of an automatic analytical device for performance of the polymerase chain reaction.
The analytical device is designed e.g. for immunoassays.
Fig. 1 shows a thermal cycler part 2 when dismantled from an analytical device 1 as per Fig. 13. The thermal cycler part 2 contains 2B e.g. two identical thermal cyclers 18, 19 and a standby station 22.
The following description of the thermal cycler 18 also applies to the thermal cycler 19.
a) a unit heater 33 which holds the test tubes and has an annular arrangement of recesses 27, each recess serving as a chamber for holding the lower part of a test tube 21, ~ 4 ~ 21~0~
b) a computer-controlled automatic control system shown in Fig.
6, and c) heating or cooling elements controlled by the automatic control system and used for cyclic alteration of the temperature of the 5 unit heater 33.
The unit heater is of a material which has a high thermal conductivity. The unit heater 33 is preferably an aluminium or silver body.
The unit heater 33 has an upper surface, a bottom surface and a 0 cylindrical outer wall, and each of the recesses 27 of the unit heater has an opening located in the upper surface of the unit heater.
The test tubes 21 are conical in their lower region and cylindrical in their upper region and closed in sealingtight manner by a lid 87.
As clearly shown in Figs. 1 and 3, a test tube arrangement 23 of this kind can be inserted into corresponding recesses 27 in the unit heater 33 of the thermal cycler 18.
Access to the contents of a test tube The thermal cycler 18 has a hinged lid 28 formed with an opening 29 for each recess 27 in the unit heater 33, enabling a pipetting needle to pierce the closure 87 of the test tube 21 inserted into the recess. As shown in Fig. 2, when the hinged lid 28 is in the closed position, each opening 29 is in line with the longitudinal axis 31 of the corresponding test tube 21.
Heat transfer between the unit heater and the test tube - S - '~130~3 As shown in Fig. 2, the recesses 27 in the unit heater 33 are adapted to the conical region of the test tubes 21, so that the peripheral wall of the test tubes 21 reliably abuts the inner wall of the recess 27, for optimum heat transfer. In order to increase the thermal reaction speed, precision and homogeneity, the unit heater 33 is substantially heatinsulated and secured in a casing 34 and has a small mass and good heat conductivity.
Heating element in the hinged lid of the thermal cycler The lid 28 preferably contains a heating element, e.g. an electric o resistance heat~r 52 for heating the sealed test tubes disposed in the unit heater 33.
The electric resistance heater 52 and the Peltier element~; S6 are 20 used in combination to obtain the required speed of the temperature changes in the unit heater 33 and the required precision and homogeneity of the temperature distribution. Another effect of the resistance heater 52 is to prevent any condensate forming in the lid region of the test tube 21.
26 Device for closing and pressing the hinged lid of the thermal cycler The hinged lid 28 preferably contains a closing and pressing device for securing the sealed test tubes 21 disposed in the unit heater 33. To this end the hinged lid 28 has a springheld pressure plate 46, which presses each test tube 21 with a defined force into the recesses 27 in the unit heater 33. Recesses 47 for holding the cap-shaped lids 87 of the test tubes 21 and openings 48 for piercing by the pipetting needles 32 are provided in the pressure plate 46 coaxially with the test tubes 21. The spring element can be a - 6 21~0013 corrugated washer 49. A safety ring S 1 prevents the pressure plate 46 falling out when the hinged lid 28 is opened.
A cooling or heating element in the form of a Peltier element As shown in Fig. 2, a thermal cycler 18 preferably contains at least one Peltier element 36 forming part of the means provided in the thermal cycler 18 for cyclic alteration of the temperature of the unit heater 33. One heat transfer surface 37 of the Peltier element 36 0 is in contact over a large area with the bottom surface of the unit heater 33 and the other heat transfer surface 38 is in contact over a large area with a cooling member 39 for heat dissipation. The cooling member 39 is preferably of aluminium or copper. A switchable fan 45 is provided for heat dissipation.
The Peltier element 36 diagr~mmatically shown in Fig. 2 is preferably an arrangement of such elements.
In the aforementioned first embodiment of the thermal cycler, the Peltier element 36 is used as a cooling or a heating element. This method of operating the Peltier element 36 and co-operation between 20 it and the electric resistance heater 52 enable the required temperature of the unit heater to be reached within a temperature profile.
To prolong its life, the Peltier element 36 is preferably protected from thermodynamic mechanical tension peaks by a central spring-25 biased securing means which presses the Peltier element and holds itagainst the unit heater 33. To this end the Peltier element is resiliently clamped between the heat transfer surfaces of the unit heater 33 and the cooling member 39. The contact surface of the cooling member 39 is pressed, e.g. by a pressure spring 41, against 30 the Peltier element 36. The spring tension can be adjusted via a screw 42, a spring washer 43 and a ball and socket joint 44, which further increases the degrees of freedom of the cooling member 39.
A cooling or heating element in the form of a Peltier element ~ 7 21~0013 In a modified version of the embodiment described above Peltier element 36 is used exclusively as a cold-producing element, i.e. only for cooling the heater unit 33. In this way a prolongation of the useful life of the Peltier element is obtained.
An additional heating element around the unit heater In a second embodiment of the thermal cycler, it preferably also contains an electric resistance heater 35 disposed around the heater unit 33 and along the periphery of the cylindrical outer wall of the unit heater 33. When the additional heating element is used in the thermal 0 cycler, the Peltier element 36 is used only for cooling. This has the advantage of relieving the Peltier element from mechanical thermal stress and thus contributes to increasing the service life of the Peltier element in the thermal cycler.
Means for recognising marking on the ring of test tubes The thermal cycler 18 also contains means for recognising marking on the arrangement of test tubes 23, e.g. marking in the form of a vertical lug 25. The lug co-operates with a detection device 26 inside the thermal cycler 18, to facilitate recognition of the presence of the ring of test tubes 23 in the thermal cycler 18. The detection device 26 20 is e.g. a light barrier. Also, the lug 25 permits the test tube arrangement 23 to be positioned only once in the unit heater 33. This single positioning can be combined with numbering on the seals of the test tubes, to obtain a one-toone correlation between samples and patients .
The test tube arrangement 23 also comprises a flap 24 serving e.g.
as a surface for carrying data on the contents of the samples in the arrangement 23, the data being present e.g. in the form of a bar code.
Lifting-out device As a result of the temperature changes and the action of spring 49, the conical regions of the reaction containers 21 adhere to the walls of the recesses 27 in the unit heater 33. The resulting non-positive connection makes it difficult to remove the reaction containers 21 from the thermal cycler 2. For this reason, in the embodiment in Figs. 3 to 5, - 8 - 2 1 3 0 1) 13 a lifting-out device 53 is proposed, and considerably facilitates removal of the reaction-container ring 23 out of the thermal block 33.
As shown in Figs. 3 to 5, the lifting-out device 53 contains a rocker 55 serving as an ejection lever. One end of the rocker SS is connected 5 to a hinge of the lid 28. The other end of the rock 55 is free. The lifting-out device 53 also contains an ejection disc 58, which is concentric with the axis of symmetry of the unit heater 33 on which the rocker 55 is disposed. On its periphery, the ejection disc 58 has an arrangement of recesses 61 for removing the reactioncontainer ring 23 0 from the recesses 27 in the unit heater 33.
As shown in Fig. 3, the rocker 55 is guided on the pivot 54 of the hinged lid 28. On the pivot side the rocker 55 has two lugs 56 with recesses 57 in which the pivot 54 engages. The ejection disc is screwed to the rocker 55. On its peripheral edge 59, the disc 58 has 5 semicircular recesses 61 which are exactly aligned with the projection of the recesses 27 in the unit heater 33 or the cylindrical regions of the reaction containers 21 inserted in the recesses 27 (Fig. 5). The peripheral edge 59 of the disc 58 thus extends under the inner flange-like region 62 of the reaction-container ring 23 or the flanges 2~ on the containers 21. Figs. 4 and 5 show the shape and function of the recess 57 in the lugs 56 of rocker 55 in conjunction with the pivot 54 of the lid 28 and a control pin 63 disposed at a distance e on the lid 28 and likewise engaging in the recess 57. When the lid 28 is closed, the lifting-out device 53 is inoperative. When the lid 28 is opened 25 beyond a certain angle, the pin 63 comes into contact with a control surface 64 on the recess 57 and pivots the rocker 55 around the point P, thus lifting the sample-containers 21. As a result of the tilting of the rocker 55 around the point P or the increasingly sloping position of the disc 58, the breakingloose forces associated with the individual 30 reaction containers 21 are offset in time, so that the containers 21 are progressively loosened from their recesses 27. The force applied and the stress on the material is thus kept at a low level and operation is more comfortable.
Automatic control of the thermal cycler - 9 - 2~ 13 Fig. 6 is a diagram of an automatic control system of a thermal cycler 18 according to the invention, via masterslave processors 72 and 73.
The temperature of the pressure plate 46 of the lid 28, and of the unit heater 33 and the environment is detected by sensors 65, 66, 67 and supplied via a temperature interface 68 to the slave processor 73.
The set temperatures, set times, number of temperature cycles and speed of the heating and cooling processes inter alia are input into the master processor 72 (the interface to the user).
0 Predetermined stored temperature/time profiles can be selected -and run. Input is via a keyboard 16 or another interface. These data are supplied to the slave processor 73, which via controllers 69 actuates a power output stage 71 which in turn controls the supply of energy to the heating elements 55, 52 and the Peltier element 36.
Feedback (actual values) are supplied via the slave processor 73 to the master processor 72, where they are processed or displayed to the user. In this manner the user is informed about the instantaneous temperature of the samples, the temperatures already reached, giving times, and the temperatures still to be reached, giving times.
ao The operating state of the system is permanently monitored and recorded. Faults which cannot be eliminated by the system, result in automatic switching-off or a fault alarm.
- 10 - 2~?001~
Fig. 8, by way of example, shows temperature curves in a cyclic o process. Curve A shows the temperature at the unit heater 33, and curve B shows the temperature of the liquid in the reaction container 21. The thermal cycler can be used for setting temperatures between 40 and 98 ~ C. Typically the lower temperatures are between 50 and 60 ~ C and the upper temperatures between 90 and 96 ~ C. When the average temperature is used, it is around 72 ~ C. The rate of heating and cooling by the thermal cycler is 1 ~ C per second. A typical cycle lasts 120 seconds. When the corresponding temperatures have to be held for longer than 10 seconds, the cycle is prolonged accordingly.
ao Test tubes As shown more particularly in Figs. 8 to 12, the test tubes 21 have a conical lower region 82 and a cylindrical upper region 81. The conical lower region 82 of the test tube 21 containing the sample for heat-treatment has a thinner wall, for better heat transfer, than the 25 upper cylindrical region 81. As Fig. 3 shows, the lower conical region 82 of the test tube 21 can be inserted with an exact fit into the correspondingly shaped recess 27 in the unit heater 33 of the thermal cycler 18, so that the conical inner wall of the recess 27 is fully in contact with the conical outer wall 85 of the bottom region 82 of the 30 test tube 21, thus ensuring optimum heat transfer.
The opening 86 of the test tube 21 can be closed in sealingtight manner by a lid 87. The lid 87 can be perforated by a pipetting needle 32 for drawing some sample material.
To reduce expense and facilitate handling the test tubes 21, a 35 number of test tubes (e.g. twelve) are combined in a unit, e.g. in a w - 11 - 21~ 0 ~ 13 circular arrangement to form a ring of test tubes, and the lid 87 is non-detachably secured by a film hinge 91.
Particularly advantageously, the arrangement 23 of test tubes is in two parts. One part 92 consists of test tubes 21 spaced at uniform 5 angular intervals and connected in a circle by thin webs 94 on flange-like larger-diameter portions 93 at the opening end. The webs 94 are V-shaped so that the ring 92 of test tubes has radially flexibility, which is advantageous when joining to the other part 9S. The part 92 is preferably made of polypropylene (PP).
0 The other part 9S of the test tube arrangement 23 comprises rings 97 disposed in a circle and interconnected by webs 96, the inner diameter of the rings being identical with the outer diameter of the cylindrical regions 81 of the test tubes 21, and the centres of the rings being in line with the longitudinal axes 98 of the test tubes 21. The webs 96 are V-shaped, to maintain radial elasticity. Radially outwardly extending film hinges 91 are integrally formed on the rings 97 and each end in a closure lid 87. Part 9S is preferably also made of polypropylene (PP).
Two radially outwardly extending, diametrically opposite extensions 99 and 101 are formed on the other part 9S and offset by half the spacing angle between the rings 97. One extension 99 has a horizontal surface 102 on which, for example, data on the samples in the test tubes 21 can be recorded in a bar code. The other extension 101, in the form of a vertical lug, co-operates with a detector 26, e.g. a light barrier, in the thermal cycler 18 (see Fig. 1). By this means, the test tube arrangement 23 is automatically inserted in a defined position into the thermal cycler 2.
When the two parts 92, 9S of the test tube arrangement 23 are brought together (Fig. 9), the flanges 93 on the test tubes 21 in one part 92 abut the top surfaces 104 of the rings 97 in the other part 9S.
As a result of the close fit between the cylindrical region 81 and the ring 97, the test tube arrangement 23 is relatively rigidly 35 preassembled and can be filled with the appropriate samples. The lid - 12- 212~3~13 87 is then folded over and the cylindrical extension l OS thereof is held in sealing-tight manner in the openings 86 of the test tubes 21 (Fig. 1 O).
The webs 94, 96 provided in the aforementioned test-tube 5 arrangement 23 give the arrangement sufficient flexibility for the test tubes 21 to be very easily insertable into the recesses 27 of the unit heater 33. If the arrangement 23 is rigid, such insertion can be difficult even if there are only small deviations from the dimensions of the unit heater or of the test tube arrangement.
lo As a result of the two-part construction of the test tube arrangement 23, extreme economies of material can be made and, if advantageous, materials (plastics) having different properties can be used, to give optimum results. This is important for throwaway articles (the test tube arrangement is thrown away after use).
Analytical device with a thermal cycler Fig. 13 shows an analytical device 1, designed e.g. for performance of immunoassays.
In order to increase the volume of substances under analysis, present in the samples, to above the detection limit in the subsequent ao process of analysis, the analytical device incorporates a thermal cycler part 2 containing previously-described thermal cyclers 18 and 19 according to the invention, for working a DNA amplification process using the polymerase chain reaction.
In order to increase the productivity of the analytical device, i.e.
25 process a maximum number of samples per unit time, the number of prepared samples has to be adapted to the subsequent process times, to avoid any idle times. This is achieved e.g. by two independently operating thermal cyclers 18 and 19, each capable of holding twelve reaction containers 21, and two standby stations 22, likewise each 30 capable of holding twelve reaction containers 21 taken from one of the thermal cyclers 18, 19 at the end of the process therein.
The analytical device 1 also contains all other equipment for the aforementioned immunoassays, e.g. two racks 3, 4 holding reagents on a vibrating table S, a rack 6 holding other reagents, three racks 7 w - 13 - 21~0~
containing throwaway reaction containers 8, a temperature-controlled incubator 9 into which the reaction containers 8 are inserted, a washing device 11 and a photometer device 12 for determining the result of the test.
Test head of the analytical device The samples, reagents, and reaction-holders are transferred by a head movable in an x-y co-ordinate system and containing a pipetting device 14 and a reaction-container gripper 15, both movable in the z direction .
0 After DNA amplification in the reaction containers 21 in the thermal cyclers 18 and 19, the pipetting device 14 takes volumes of sample from the reaction containers 21 and delivers them to reaction containers 8 disposed in the racks 7. The volumes of samples delivered to the reaction containers 8 are investigated in immunoassays made by the analytical device.
Control unit of the analytical device All required operations are controlled and co-ordinated by a central control unit (not shown) belonging to the analytical device. A
control panel 16 or keyboard for inputting process parameters, and a 20 display for displaying states of the process, are diagrammatically indicated. Data regarding the samples, recorded on the reaction containers e.g. in a bar code, can be read into a store via a manually guided wand or scanner 17. Interfaces for a printer etc (not shown) are provided.
(c) means for moving the pipetting needle from a position outside of each test tube, through the pierceable closure on the test tube, and into the test tube;
(d) means for applying suction to the pipetting needle so as to enable the pipetting needle to withdraw liquid reaction mixture out of a given test tube when the pipetting needle is inside the given test tube and reaction mixture is present within the given test tube; and (e) a device for automatic performance of temperature cycles on the test tubes, which comprises:
(1) a holder formed of a thermally conductive material and having an upper surface, a lower surface and a cylindrical outer wall, the holder having an array of chambers for holding the test tubes equipped with pierceable closures, the chambers being disposed along an arc with each chamber having an opening located in the upper surface of the holder, each chamber being configured and dimensioned to receive one test tube equipped with a pierceable closure, the holder being configured and dimensioned so that when test tubes having pierceable closures are held in the array of chambers, the pierceable closures of the test tubes can be accessed by a pipetting needle;
(2) a computer-regulated automatic control system; and (3) means actuated by the automatic control system for cyclic alteration of the temperature of the holder.
4 The device according to claim 2, wherein the at least one Peltier element has a central part and is pressed against the holder by spring-biased securing means positioned at the central part, which securing means comprises a spring pressed by a screw, the tension on the spring being adjustable by means of the screw.
6. The device according to claim 2 further comprising a hinged lid having a heating element for heating the test tubes having pierceable closures when such test tubes are held in the array of chambers, the lid having an opening for each chamber so that the pipetting needle can traverse each opening to access the pierceable closure of the test tube in the chamber.
7. The device of claim 6, wherein the hinged lid contains a closing and pressure means for securing the test tubes having pierceable closures when such test tubes are held in the array of chambers.
8. The device according to claim 2 further comprising a heating element disposed around the holder along the periphery of the cylindrical outer wall of the holder.
10. The device according to claim 6 further comprising a lifting-out device for facilitating removal of the test tubes from the chambers in the holder, the lifting-out device comprising an ejection lever having one end connected to the hinge of the bid and the other end free.
11. The device according to claim 10 further comprising an ejection disc which is secured to the lever and is concentric with the axis of symmetry of theholder, the disc having a peripheral arrangement of recesses for removing the test tubes from the chambers.
14. A method for amplifying nucleic acid materials comprising the steps of a) introducing into a reaction vessel a sample suspected to contain a target nucleic acid material along with suitable reagents for amplification of said suspected target nucleic acid to form a reaction mixture;
b) sealing the reaction mixture inside said reaction vessel by closing a tightly sealing lid of the reaction vessel;
c) amplifying the target nucleic acid material within said reaction vessel by an amplification process including thermal cycling of the reaction mixture contained in the reaction vessel;
said method being characterized by the following steps i) providing said sealing lid with a part that is pierceable by a pipetting needle;
15. A method according to claim 14 characterized in that the reaction vessel is placed in an automatic detection instrument which comprises an automatic pipetting instrument for performing said removing and said dispensing.
16. A method according to claim 15 wherein said removing and said dispensing are both performed by said automatic pipetting instrument.
CA 2130013 1993-09-10 1994-08-12 Apparatus for automatic performance of temperature cycles Expired - Fee Related CA2130013C (en)
CA2130013A1 CA2130013A1 (en) 1995-03-11
CA2130013C true CA2130013C (en) 1999-03-30
CA 2130013 Expired - Fee Related CA2130013C (en) 1993-09-10 1994-08-12 Apparatus for automatic performance of temperature cycles
EP (3) EP0807468B1 (en)
AT (3) AT199222T (en)
ES (3) ES2169294T3 (en)
GR (1) GR3035810T3 (en)
PT (1) PT642831E (en)
DE29505897U1 (en) * 1995-01-12 1995-08-24 Schulz Joachim Dipl Ing Thermal shaker
DE29519602U1 (en) * 1995-12-11 1996-04-18 Reimann Hans Juergen Prof Dr D Mobile incubation device
DE29706031U1 (en) * 1996-11-22 1997-08-21 Schulz Joachim Dipl Ing Device for tempering and shaking samples in sample vessels
AT251496T (en) * 1997-03-28 2003-10-15 Pe Corp Ny Device for thermocycling devices for pcr
CA2301023C (en) * 1997-08-20 2007-05-01 Biopore, Inc. Cassette device and system to facilitate cryopreservation
ES2224347T3 (en) * 1998-05-01 2005-03-01 F. Hoffmann-La Roche Ag Apparatus to simultaneously control the reactions that have placed a plurality of reaction containers.
DK0955097T3 (en) * 1998-05-04 2005-02-14 Hoffmann La Roche Thermal cycle apparatus which has an auto-positionable cover
CA2301153C (en) 1998-06-24 2008-08-26 Chen & Chen, Llc Fluid sample testing system
DE19859586C1 (en) * 1998-12-22 2000-07-13 Mwg Biotech Ag Thermal cycler device
DE50001774D1 (en) 1999-09-29 2003-05-22 Tecan Trading Ag Maennedorf Thermal cycler and lifting element for microtiter plate
DE10115848A1 (en) * 2001-03-30 2002-10-10 Biometra Biomedizinische Analy Device for thermally influencing, preferably liquid, sample material contained in a container
JPWO2003055973A1 (en) * 2001-12-26 2005-05-12 オリンパス株式会社 Reaction vessel and reaction vessel holding mechanism
DE10312197A1 (en) * 2003-03-19 2004-09-30 Roche Diagnostics Gmbh Sample treatment device, in particular automatic analysis device
US20050202484A1 (en) 2004-02-19 2005-09-15 The Governors Of The University Of Alberta Leptin promoter polymorphisms and uses thereof
DE102004024350A1 (en) * 2004-05-17 2005-12-15 H+P Labortechnik Ag Reaction vessel and its preparation and use
JP4187259B2 (en) * 2005-10-04 2008-11-26 キヤノン株式会社 Pressure support mechanism of structure
JP4307478B2 (en) * 2006-12-05 2009-08-05 キヤノン株式会社 Cartridge for biochemical reaction
EP2117713B1 (en) 2006-12-22 2019-08-07 DiaSorin S.p.A. Thermal transfer methods for microfluidic systems
EP2198968B1 (en) * 2008-12-16 2018-10-17 F. Hoffmann-La Roche AG Systems and methods for monitoring a thermoelectric heating and cooling device
KR101643196B1 (en) 2010-02-23 2016-07-27 루미넥스 코포레이션 Apparatus and methods for integrated sample preparation, reaction and detection
CN103589627B (en) 2010-07-23 2015-11-18 贝克曼考尔特公司 For carrying out heat circulator module and the system of PCR in real time in PCR reaction vessel
IT1403791B1 (en) * 2010-12-30 2013-10-31 St Microelectronics Srl Method for calibrating a temperature sensor of a chemical microreactor and analyzer for biochemical analysis
TWI427143B (en) * 2011-03-22 2014-02-21
TWI563080B (en) * 2011-03-24 2016-12-21 Genereach Biotechnology Corp Method for controlling thermosiphon circulation in biochemical reaction
ES2684525T3 (en) 2011-09-15 2018-10-03 David A. Shafer Probe compositions: antisonda for detection of DNA or RNA of high specificity
JP6062449B2 (en) 2011-11-07 2017-01-18 ベックマン コールター， インコーポレイテッド Specimen container detection
KR20140092375A (en) 2011-11-07 2014-07-23 베크만 컬터, 인코포레이티드 Centrifuge system and workflow
JP6082018B2 (en) 2011-11-07 2017-02-15 ベックマン コールター， インコーポレイテッド System and method for processing samples
EP2784150B1 (en) * 2011-11-22 2019-05-15 GeneReach Biotechnology Corp. Device for polymerase chain reaction via thermal convection
US9505004B2 (en) * 2012-03-09 2016-11-29 Genereach Biotechnology Corp. Device for controlling thermal convection velocity of biochemical reaction and method for the same
CN105263627B (en) 2013-01-18 2019-05-21 生米公司 Analytical equipment
WO2014149268A1 (en) 2013-03-19 2014-09-25 Life Technologies Corporation Thermal cycler cover
EP3017035A4 (en) * 2013-07-01 2018-09-05 Hakalehto, Eino Elias Device for microbial cultivation with options for field sterilization and gas generation
SE538287C2 (en) * 2013-09-30 2016-04-26 Symcel Sverige AB Sample holder adapted to isothermal calorimetry of parallel samples
JP6087264B2 (en) 2013-11-29 2017-03-01 株式会社日立ハイテクノロジーズ Component analyzer, medicinal effect analyzer, and analysis method
CN104130933B (en) * 2014-08-02 2016-01-13 张金木 A kind of fluorescence constant temperature PCR amplification instrument
EP3056277B1 (en) * 2015-02-12 2019-09-04 QIAGEN Lake Constance GmbH Tempering clamp
DE102015121362B4 (en) * 2015-12-08 2018-05-24 Analytik Jena Ag Temperature control device with a reaction vessel
US10029260B2 (en) 2016-05-24 2018-07-24 Taj King Centrifuge tube holding assembly
DE102017005835B4 (en) * 2017-06-20 2020-04-02 Diehl Metering Gmbh Device for the mobile determination of a property of a liquid, solid or gaseous sample
CN107539355A (en) * 2017-09-13 2018-01-05 重庆铜山天询科技有限公司 It is easy to carry the transportation equipment of experiment equipment
DE3769788D1 (en) * 1987-02-25 1991-06-06 Hewlett Packard Gmbh Apparatus for performing chemical reactions.
JPH0723847Y2 (en) * 1988-09-20 1995-05-31 三菱電機株式会社 Air bushing
AT397610B (en) * 1990-06-01 1994-05-25 Avl Verbrennungskraft Messtech Device for taking body liquids
DE69435255D1 (en) * 1993-10-22 2010-01-07 Abbott Lab Test vials and methods for minimizing contamination
1994-08-12 CA CA 2130013 patent/CA2130013C/en not_active Expired - Fee Related
1994-08-31 AT AT97112710T patent/AT211024T/en not_active IP Right Cessation
1994-08-31 EP EP97112710A patent/EP0807468B1/en not_active Expired - Lifetime
1994-08-31 EP EP19940113574 patent/EP0642831B1/en not_active Expired - Lifetime
1994-08-31 DK DK94113574T patent/DK0642831T3/en active
1994-08-31 ES ES97112702T patent/ES2169294T3/en not_active Expired - Lifetime
1994-08-31 DE DE1994510020 patent/DE59410020D1/en not_active Expired - Lifetime
1994-08-31 AT AT94113574T patent/AT199222T/en unknown
1994-08-31 DE DE1994509658 patent/DE59409658D1/en not_active Expired - Lifetime
1994-08-31 DE DE1994510021 patent/DE59410021D1/en not_active Expired - Lifetime
1994-08-31 ES ES97112710T patent/ES2169295T3/en not_active Expired - Lifetime
1994-08-31 ES ES94113574T patent/ES2155456T3/en not_active Expired - Lifetime
1994-08-31 PT PT94113574T patent/PT642831E/en unknown
1994-08-31 AT AT97112702T patent/AT211023T/en not_active IP Right Cessation
1994-08-31 EP EP97112702A patent/EP0807467B1/en not_active Expired - Lifetime
1994-09-07 US US08/301,932 patent/US5616301A/en not_active Expired - Lifetime
1994-09-09 JP JP21627294A patent/JPH07151764A/en active Granted
1996-10-23 US US08/735,943 patent/US5795547A/en not_active Expired - Lifetime
2001-04-27 GR GR20010400658T patent/GR3035810T3/en not_active IP Right Cessation
DK0642831T3 (en) 2001-05-21
DK642831T3 (en)
EP0807468B1 (en) 2001-12-19
DE59410021D1 (en) 2002-01-31
US5795547A (en) 1998-08-18
EP0807467A3 (en) 1998-06-03
CA2130013A1 (en) 1995-03-11
JPH07151764A (en) 1995-06-16
US5616301A (en) 1997-04-01
EP0807467A2 (en) 1997-11-19
EP0642831A1 (en) 1995-03-15
AT211023T (en) 2002-01-15
DE59409658D1 (en) 2001-03-29
EP0642831B1 (en) 2001-02-21
AT211024T (en) 2002-01-15
DE59410020D1 (en) 2002-01-31
EP0807468A2 (en) 1997-11-19
ES2169295T3 (en) 2002-07-01
EP0807468A3 (en) 1998-06-10
GR3035810T3 (en) 2001-07-31
ES2155456T3 (en) 2001-05-16
PT642831E (en) 2001-07-31
ES2169294T3 (en) 2002-07-01
AT199222T (en) 2001-03-15
EP0807467B1 (en) 2001-12-19
US7427510B2 (en) 2008-09-23 System for processing samples in a multichamber arrangement
US6662626B2 (en) 2003-12-16 Assembly for desorbing sampling tubes; adapter and sampling tubes for such an assembly; and kit of parts for forming such an assembly
DE60018386T2 (en) 2005-12-29 Station for nucleic acid reproduction for disposable supplements
1994-08-12 EEER Examination request