Sample introduction device

Description

BACKGROUND OF THE INVENTION

1. Field of the Invention

This invention relates to sample handling devices, and more particularly to a device for introducing samples into sample chambers of a test instrument.

2. Background Information

Chemical analysis of liquids, including biological liquids such as blood, plasma or urine is often desirable or necessary. Sensors that utilize various analytical elements to facilitate liquid analysis are known. These elements have often included components which specifically react to a substance or characteristic under analysis, termed analyte herein. These components, upon contacting a liquid sample containing the analyte, effect formation of a colored or fluorescent material or another detectable response to the presence of the analyte.

In this regard, analytical elements such as disclosed in commonly assigned U.S. patent application Ser. No. 08/617,714 (hereinafter, the '714 Patent Application) have been provided. Analytical elements of this type are adapted for use within a sample chamber of an optical sensor assembly. In operation, a fluid sample of unknown analyte content (an “unknown sample”) is tested by introducing the sample into the sample chamber where it contacts the analytical element. Any change in the optical characteristics of the analytical element are observed to thus determine characteristics of the analyte of interest in the sample. An example of a sensor assembly of this type is disclosed in commonly assigned U.S. patent application Ser. No. 09/010,096, entitled “OPTICAL SENSOR AND METHOD OF OPERATION” filed on Jan. 21, 1998 (hereinafter referred to as the “OPTICAL SENSOR” patent application) which is hereby incorporated by reference in its entirety, herein. The sample chambers of this and similar types of sensor assemblies are generally incorporated into multiple use clinical instrumentation which utilize a sample introduction device, including an aspiration probe, to withdraw a sample, such as blood or other fluid, from a syringe or the like and transfer the sample into the sample chamber. An example of instrumentation that utilizes an aspiration probe to withdraw a sample is disclosed in commonly assigned U.S. patent application Ser. No. 60/006,741, entitled “MULTIFUNCTION VALVE” filed on Nov. 2, 1995.

In this type of instrumentation, once the tip of the aspiration probe is immersed within the syringe, a suction pump draws blood through the probe and into the instrument. As the blood sample flows from the syringe, its volume is replaced by air that passes through an opening in the coupling between the syringe and the instrument, and through an annular space between the probe and the opening of the syringe.

While multiple use instruments that draw blood in this manner may operate satisfactorily in many applications, they present some difficulties. In particular, the sample introduction device, including the inside of the aspiration probe, must be routinely cleaned between samples to prevent clogs and cross contamination of the samples. Although blood gas sample syringes are treated with an anti-coagulant, blood samples often contain micro-clots which can block the narrow flow passages of sample introduction devices of analytical instrumentation. In many current blood gas analyzers, such as the Rapidpoint 400 sold by Bayer Corporation of Medfield, Mass., problems associated with these clots are minimized by providing the inlet of the sample aspiration probe with the smallest diameter of the entire sample flow path through the sample introduction device. If a clog does occur, it is likely to be at the tip of the probe and can be cleared by wiping or flushing. However, the inclusion of probe washing facilities complicates the fluidics of a clinical analyzer. Moreover, the washing sequence is time consuming and disadvantageously reduces the availability of the instrument for sample analysis. Such delay may be particularly disadvantageous in some operating environments such as, for example, in critical care facilities.

Further, discarded wash fluid or reagent comprises a significant portion of the waste generated by such conventional analytical instrumentation. This waste is classified as biohazardous and thus disposal thereof is relatively expensive, both in economic and environmental terms. This waste also poses a potential health risk to health care workers and those who may otherwise come into contact with the waste during or after disposal.

Thus, a need exists for an improved sample introduction device that reduces the need for washing between samples to reduce the amount of reagent required therefor and that otherwise overcomes the drawbacks of the prior art.

SUMMARY OF THE INVENTION

According to an embodiment of the present invention, a sample introduction device is adapted for introducing a sample into a sample chamber of a sensor from a container maintained in fluid communicating relationship therewith. The sample introduction device comprises a probe of substantially tubular construction, having a first end adapted to extend into the container and a second end adapted for connection to a material volume supply. The probe is adapted to inject a predetermined volume of gas into the container to displace a predetermined volume of the sample from the container into the sample chamber.

In a variation of the first aspect of the present invention, a test apparatus is provided for determining analyte content of a sample. The test apparatus comprises the sample introduction device of the first aspect of the invention. In addition, the sensor has at least one sample chamber and the container is adapted for being maintained in fluid communicating relationship therewith.

In a second aspect of the present invention, a method is provided for introducing a sample into a sample chamber. This method comprises the steps of maintaining a sample container in fluid communicating relationship with the sample chamber; and injecting a predetermined volume of gas into the sample container, wherein a predetermined volume of a sample disposed within the sample container is displaced by the gas from the container into the sample chamber.

In a variation of this second aspect of the invention, a method of operating a sensor is provided. This method comprises the steps of introducing a sample into a single use sample chamber as set forth in the second aspect;

measuring predetermined parameters of the sample disposed in the single use sample chamber; and

discarding the sensor with sample fluid disposed within the sample chamber.

The above and other features and advantages of this invention will be more readily apparent from a reading of the following detailed description of various aspects of the invention taken in conjunction with the accompanying drawings.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1

is a perspective view, with portions thereof in phantom and portions thereof broken away, of a representative application utilizing an embodiment of the present invention;

FIG. 2

is a cross-sectional elevational view of an other similar representative application utilizing an embodiment of the present invention, during a step in the operation thereof;

FIG. 3

is a view similar to that of

FIG. 2

, during another step in the operation of the present invention;

FIG. 4

is a view similar to those of

FIGS. 2 and 3

, during a further step in the operation of the present invention;

FIG. 5

is a view similar to those of

FIGS. 2-4

, during a still further step in the operation of the present invention; and

FIG. 6

is a view similar to those of

FIGS. 2-5

, during a yet further step in the operation of the present invention.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

Referring to the figures set forth in the accompanying Drawings, illustrative embodiments of the present invention will be described in detail hereinbelow. For clarity of exposition, like features shown in the accompanying drawings shall be indicated with like reference numerals and similar features shown for example in alternate embodiments in the drawings, shall be indicated with similar reference numerals.

Briefly described, as shown in the Figs., the present invention includes a sample introduction device

10

(

FIG. 2

) adapted for introducing a liquid sample or test sample

12

(

FIG. 2

) from a container or syringe

14

to a sample chamber

116

of a sensor assembly

118

for analysis. Device

10

includes a Luer fitting or coupling

20

(

FIG. 2

) adapted to mate an outlet

22

of the container in a concentric orientation with an input aperture

24

of the sample chamber. A tubular probe

26

is adapted to extend in fluid tight engagement through backing web

38

of sensor assembly

18

in (

FIG. 1

) or sensor assembly

118

in (

FIG. 2

) , for concentric placement with both outlet

22

and inlet aperture

24

with a first end

28

thereof extending into the syringe. A distal end

29

is adapted for attachment to an air supply (not shown) as will be discussed hereinafter. Probe

26

has a predetermined diameter sufficient to provide an annular clearance or opening

30

(

FIGS. 1

,

3

and

6

) between the probe and each of outlet

22

and inlet aperture

24

. The probe is adapted to inject a predetermined volume of a material

32

, preferably a gas such as air (

FIGS. 4 and 5

) therein. The gas serves to displace a predetermined volume of sample

12

from container

14

through annular clearance

30

to enable the sample to pass therethrough into sample chamber

16

or

116

.

The combination of mating syringe

14

directly to sensor assembly

18

or

118

and injecting air into the syringe through probe

26

to displace the sample therefrom, rather than drawing the sample into the probe, serves to advantageously eliminate the need for washing the interior of the probe. Moreover, the use of the present invention in combination with the aforementioned multiple single use sensor assembly

18

or

118

advantageously provides “hands-off” sample introduction, substantially reduces the need for probe and sample chamber washing, to in turn, reduce use of wash reagents.

Sample introduction device

10

of the present invention is suitable for use in many types of analytical instrumentation. It is particularly useful in the critical care environment for the anaerobic withdrawal of small volumes of arterial blood from a sample collection syringe.

Throughout this disclosure, the term “analyte” shall refer to any substance, compound, or characteristic such as, for example, pH, oxygen, carbon dioxide and ions, among others, capable of detection and/or measurement relative to a liquid sample. Similarly, the term “concentration” shall refer to the level or degree to which an analyte is present in a sample. The term “tubular” shall refer to an elongated, hollow member of substantially any transverse cross-sectional geometry, including, but not limited to circular, square or other polygonal geometry.

Turning now to the drawings in detail, in

FIG. 1

portions of a sample introduction device

10

(

FIG. 2

) are shown in a representative application. Sensor assembly

18

includes a series of sample chambers

16

, each of which include an input aperture

24

and an output aperture

25

. Syringe

14

is disposed in operative engagement with an input aperture

24

of one of the sample chambers

16

. Probe

26

is shown in its fully inserted position concentrically disposed with both input aperture

24

and outlet

22

of syringe

14

, with first end

28

thereof extending into syringe

14

. Luer fitting

20

(FIG.

2

), including the fluid pathway between syringe

14

and input aperture

24

of the sample chamber have been omitted from

FIG. 1

for clarity.

As also shown, sensor assembly

18

comprises a multiple single use optical sensor of the type disclosed in the above-referenced “OPTICAL SENSOR” patent application. Alternatively, however, the present invention may be utilized in combination with substantially any type of sample chamber, including single and multiple use sample chambers, in addition to the multiple single use chambers shown. In this regard, the present invention may be effectively utilized in combination with sample chambers of various types of sensors in addition to the optical sensors shown, including, for example, chemical, electrical and/or electrochemical sensors.

Referring now to

FIG. 2

, a sample

12

, such as, for example, blood, urine or other fluid, is maintained within syringe

14

. Outlet

22

of the syringe is matingly engaged with a Luer fitting

20

of substantially conventional construction. Luer fitting

20

is sized and shaped to receive and maintain outlet

22

in fluid communicating relation with input aperture

24

of sample chamber

116

. In a preferred embodiment, as shown, the Luer fitting is adapted to provide a fluid tight seal with outlet

22

to prevent leakage of sample

12

during sample introduction as will be discussed hereinafter. As also shown, Luer fitting

20

is preferably disposed integrally with a sensor assembly

118

, in concentric alignment with an input aperture

24

. Thus, when fully engaged with fitting

20

, outlet

22

is preferably maintained in concentric orientation with the input aperture

24

.

Sensor assembly

118

is substantially similar to sensor assembly

18

shown in

FIG. 1

, with the exception that each sample chamber

116

thereof includes an integral waste receptacle

34

which will be discussed in greater detail hereinafter. A probe aperture

36

is disposed concentrically with input aperture

24

, on an opposite side of sensor assembly

118

therefrom. Thus, as shown, probe aperture

36

is disposed in substrate or backing web

38

of sensor assembly

118

. The probe aperture is sized and shaped to provide a substantially fluid tight seal with probe

26

when inserted therein, as will be discussed hereinafter. Thus, in a preferred embodiment, web

38

is fabricated as a flexible film as disclosed in the above referenced “OPTICAL SENSOR” patent application and probe aperture

36

is sized and shaped to be slightly smaller than, to provide an interference fit with, probe

26

to thus form the fluid tight seal therebetween.

As shown, probe

26

is maintained in a ready or retracted position relative sensor assembly

118

and syringe

14

by a fixture or support means (not shown) of a test apparatus (also not shown) within which the present invention is incorporated. The test apparatus also includes a series of emitter/receptor heads or optical reader heads

40

maintained in alignment with each of a series of sensor stripes

42

(

FIG. 1

) of the sensor assembly. Emitter/receptor heads

40

are thus adapted to measure response of sensor stripes

42

to the presence of analytes in sample

12

in a manner set forth in the above referenced “OPTICAL SENSOR” patent application, and as will be discussed in greater detail hereinafter with respect to the operation of the present invention. In this regard, moreover, the specific operations of sample introduction device

10

, including the operation of emitter/receptor heads

40

, operation of probe

26

and the supply of material

32

are preferably controlled by a logic device or control module (not shown) such as a computer incorporated into the test apparatus in a manner familiar to those skilled in the art.

The orientation of sample introduction device

10

, as shown, with outlet

22

matingly engaged with fitting

20

and probe

26

in its ready position, comprises an initial step in the operation of the present invention.

Referring now to

FIG. 3

, in a subsequent step in the operation of the present invention, probe

26

is inserted into probe aperture

36

, input aperture

24

and outlet

22

until first end

28

is disposed within sample

12

. As shown, probe

26

is preferably disposed concentrically with apertures

36

and

24

, as well as with outlet

22

. The volume of the probe inserted therein will displace a predetermined, relatively small volume of sample

12

into annular opening

30

within outlet

22

as shown.

Turning now to

FIG. 4

, the next step in the operation of the present invention is to supply a predetermined volume of material

32

to distal end

29

of probe

26

. Material

32

may be substantially any flowable substance, i.e. an immiscible liquid, a paste-like material such as silicone grease, solid beads or granules, or gas. The particular material selected is preferably inert. As used herein, the term ‘inert’ is defined as being substantially non-reactive with the sample. Similarly, the term ‘inert gas’ is defined as a gas that only changes the partial pressure through its fractional equivalence or when it is dissolved in the sample, as opposed to a chemically reactive gas such as a chloride which may rapidly react chemically with elements in the sample to form HCL.

Although a non-reactive material is preferred, one skilled in the art will recognize that non-reactivity with the sample is important only to the degree that sample remaining in the sample container is affected. The sample being analyzed is disposed within the sample chamber and is not in direct contact with the material

32

. Thus, if only one sample is to be taken from sample container, a reactive material may be utilized. In the case of a blood sample, the presence of any gas phase, for example, will affect the levels of some analytes (particularly dissolved oxygen). This is a potential problem with any sampling method which draws a sample from a fixed volume. From a practical viewpoint the degradation from an inert bubble such as air in a blood sample is relatively slow, and if the sample is to be used for multiple tests, the air bubbles are preferably expelled from the syringe immediately after sampling.

As discussed hereinabove, material

32

is preferably an inert gas. A particular gas is chosen based on convenience and availability. The gas may comprise any gas which does not adversely affect the sample, or a combination of such gases provided by any convenient gas supply, such as, for example, a commercially available compressed gas canister. In this regard, when the sample is whole blood, examples of suitable gases include air, nitrogen and propane. In a preferred embodiment, the gas comprises air and is provided by either a gas canister or by conventional pump or compressor means (not shown). As shown, once the supply of gas is initiated, a bubble of gas

32

is formed at first end

28

of probe

26

. Sample

12

is displaced thereby and as shown, begins to fill sample chamber

116

. Optical reader heads

40

, or alternatively, additional optical sensors (not shown), detect presence of sample

12

in the sample chamber and also determine the integrity (absence of bubbles) of the sample disposed within the sample chamber.

As shown in

FIG. 5

, once reader heads

40

(or the alternative optical sensors) detect sample chamber

116

is substantially filled by sample

12

, the supply of gas

32

is terminated. Alternatively, a predetermined fixed volume of gas is injected. Optical reader heads

40

are then operated in the manner set forth in the above-reference “OPTICAL SENSOR” patent application to test, or collect information, such as, for example, analyte concentration within sample

12

, from each portion of the sensor stripes

42

(

FIG. 1

) disposed within sample chamber

116

.

Turning now to

FIG. 6

, once testing of sample

12

is complete, probe

26

is withdrawn from syringe

14

. As the probe moves through probe aperture

36

, the aforementioned fluid tight engagement with probe

26

serves to effectively wipe any residual portion of sample

12

from the exterior of the probe. This wiping action advantageously cleans probe

26

without the need to flush the interior thereof with wash reagents, as would otherwise be necessary in the event samples were passed through the interior of the probe as in the aforementioned prior art devices.

In a preferred embodiment as shown, additional gas is supplied to the probe once the probe has been withdrawn from the sample fluid disposed within the syringe, and before first end

28

of the probe is withdrawn from probe aperture

36

. This additional gas serves to push sample

12

out of sample chamber

116

and into waste receptacle

34

. In this manner, sample

12

may simply remain in the sensor assembly to be discarded along with sensor assembly

118

once all of the sample chambers thereof have been utilized, as will be discussed hereinafter. Alternatively, in the aforementioned embodiment that utilizes a sample chamber

16

(

FIG. 1

) without a waste receptacle, probe withdrawal may be implemented without the additional supply of gas, to leave sample

12

in the sample chamber. Thus, in both these embodiments, the sample

12

may simply remain in the sensor assembly and be subsequently discarded along-with sensor assembly

18

or

118

once all of the sample chambers thereof have been utilized, as will be discussed hereinafter.

In a further alternative, rather than leave sample

12

within the sensor assembly, the aforementioned supply of additional gas may be utilized to push sample

12

out of output aperture

25

(FIG.

1

). The sample may then be collected by any suitable collection means (not shown) familiar to those skilled in the art.

The final step in the operation of the present invention is to completely withdraw probe

26

into its ready position as shown in

FIG. 2

, whereupon syringe

14

may be removed and a fresh sample chamber

16

or

116

indexed into sensing contact with emitter/receptor heads

40

for subsequent testing in the manner described hereinabove.

Thus, as shown and described hereinabove, the present invention serves to effectively reverse the flow path of prior art instrumentation which, as discussed hereinabove, use an aspiration probe to withdraw a blood sample from a syringe. In this manner, rather than removing a sample and letting air be drawn into the syringe to replace the volume of the withdrawn sample, the present invention pumps an air bubble from probe

26

into syringe

14

, displacing a volume of blood sample

12

, which flows through the syringe/probe annular opening

30

, into the instrument Luer coupling

20

and subsequently into sample chamber

16

or

116

. The benefit of this mode of operation is that blood does not enter the inside of probe

26

, and thus permits cleaning by wiping the exterior of the probe, rather than washing the interior thereof. Advantageously, this aspect serves to reduce time, safety and waste relative to the prior art.

It should be understood that although a gas bubble is used for the displacement volume in the prefered embodiment, any material (e.g. water, a liquid or a flowable paste-like substance such as silicone grease) which can be dispensed through the probe and will displace the sample material, may be used if contamination in re-sampling is not an issue.

Moreover, use of the present invention in combination with a single use sample chamber nominally eliminates the need for sample chamber washing and simplifies disposal since the sample can remain in the sample chamber after testing to be subsequently discarded therewith as a single unit. The present invention thus effectively provides a sample handling system that substantially reduces the need for wash reagent, waste containers to receive the used wash reagent and samples, and time consuming wash sequences.

The foregoing description is intended primarily for purposes of illustration. Although the invention has been shown and described with respect to an exemplary embodiment thereof, it should be understood by those skilled in the art that the foregoing and various other changes, omissions, and additions in the form and detail thereof may be made therein without departing from the spirit and scope of the invention.

Claims

1. A sample introduction device adapted for introducing a sample from a container into a sample chamber of a sensor, said sample introduction device comprising:a fitting adapted to mate an outlet of the container in fluid communicating relationship with an input aperture of the sample chamber; a probe of substantially tubular construction, having a first end and a second end, said probe adapted to extend in a fluid tight manner through a probe aperture disposed in a wall of the sample chamber, through the input aperture and through the outlet wherein said first end extends into the container, said second end being adapted for connection to a gas supply; said probe being sized and shaped to provide fluid communicating clearance between said probe and each of the input aperture and the outlet; and said probe adapted for communicating a predetermined volume of gas therethrough into the container; wherein said predetermined volume of gas serves to displace a predetermined volume of the sample from the container through the clearance into the sample chamber.
2. A sample introduction device adapted for introducing a sample into a sample chamber of a sensor assembly from a container maintained in fluid communicating relationship therewith, said sample introduction device comprising:a probe of substantially tubular construction, having a first end adapted to extend into the container and a second end adapted for connection to a material volume supply; an outlet of the container being disposable into fluid communicating relationship with an inlet aperture of the sample chamber; said probe being sized and shaped to extend through the inlet aperture and through the outlet into the container with sufficient clearance to enable the sample to be displaced between said probe and each of the inlet aperture and outlet, into the sample chamber; and said probe being adapted to inject a predetermined volume of material into the container to displace a predetermined volume of the sample from the container into the sample chamber.
3. The sample introduction device as set forth in claim 2, wherein said probe is substantially cylindrical and is adapted for disposition concentrically within the outlet and the inlet aperture, said clearance being substantially annular.
4. The sample introduction device as set forth in claim 2, wherein said probe is adapted to extend in fluid tight engagement through a probe aperture disposed in a wall of the sample chamber.
5. The sample introduction device as set forth in claim 4, wherein said probe is adapted for being withdrawn from said container, said fluid tight engagement between the probe aperture and said probe being adapted to wipe the sample from the exterior of said probe during said withdrawal.
6. The sample introduction device as set forth in claim 5, wherein said probe is substantially cylindrical and is adapted for simultaneous disposition within the probe aperture, the outlet and the inlet aperture.
7. The sample introduction device as set forth in claim 2, further comprising a fitting adapted to mate the outlet of the container in fluid communicating relationship with the input aperture of the sample chamber.
8. The sample introduction device as set forth in claim 7, wherein said fitting is adapted to maintain the outlet of the container in physical contact with the sample chamber.
9. The sample introduction device as set forth in claim 8, wherein said fitting is integrally fastened to the sample chamber.
10. The sample introduction device as set forth in claim 2, wherein said material is selected from the group consisting of a liquid, a paste, solid beads or granules, or gas.
11. The sample introduction device as set forth in claim 10, wherein said material is chemically inert.
12. The sample introduction device as set forth in claim 2, wherein said material comprises air.
13. A test apparatus for determining analyte content of a test sample, said test apparatus comprising:the sample introduction device as set forth in claim 2; the sensor assembly having at least one sample chamber; and the container adapted for being maintained in fluid communicating relationship with said at least one sample chamber.
14. A test apparatus for determining analyte content of a test sample, said test apparatus comprising:a sample introduction device adapted for introducing a sample into a sample chamber of a sensor assembly from a container maintained in fluid communicating relationship therewith, the sample introduction device including: a probe of substantially tubular construction, having a first end adapted to extend into the container and a second end adapted for connection to a material volume supply; wherein the probe is adapted to inject a predetermined volume of material into the container to displace a predetermined volume of the sample from the container into the sample chamber; the sensor assembly having at least one sample chamber; and the container adapted for being maintained in fluid communicating relationship with said at least one sample chamber; wherein said sensor assembly further comprises a multiple single use sensor assembly having a plurality of single use sample chambers disposed therein, said container and said sample introduction device adapted for being selectively engaged with each of said plurality of single use sample chambers for selectively introducing a sample therein.
15. A method of operating a sensor, comprising the steps of:(a) maintaining a sample container in fluid communicating relationship with the sample chamber; (b) injecting a predetermined volume of gas into the sample container, wherein a predetermined volume of a sample disposed within the sample container is displaced by the gas from the container into the sample chamber, by: extending the first end of the probe through an inlet aperture of the sample chamber and into the container through an outlet thereof, the probe being sized and shaped to provide clearance between the probe and each of the inlet aperture and outlet sufficient to enable the predetermined volume of the sample to be displaced from the container into the sample chamber therethrough; and supplying gas from a gas supply to a second end of the probe, wherein the gas is fed through the probe into the container.
16. The method as set forth in claim 15, wherein the probe is adapted to extend in fluid tight engagement through a probe aperture disposed in a wall of the sample chamber.
17. A method of operating a sensor, comprising:(a) maintaining a sample container in fluid communicating relationship with the sample chamber; and (b) injecting a predetermined volume of gas into the sample container, wherein a predetermined volume of a sample disposed within the sample container is displaced by the gas from the container into the sample chamber, by: (c) extending the first end of a probe of substantially tubular construction, into the container; and (d) supplying gas from a gas supply to a second end of the probe, wherein the gas is fed through the probe into the container; and (e) adapting the probe to extend in fluid tight engagement through a probe aperture disposed in a wall of the sample chamber, and withdrawing the probe, wherein the probe aperture serves to wipe sample fluid from the exterior of the probe.
18. The method as set forth in claim 17, wherein said withdrawing step (e) further comprises the step of withdrawing the probe from the probe aperture.
19. The method as set forth in claim 17, further comprising the steps of:(f) measuring predetermined parameters of the sample disposed in the single use sample chamber; and (g) discarding the sample chamber with sample fluid disposed therein.
20. The method as set forth in claim 17, wherein said withdrawing step (e) further comprises the steps of:withdrawing the probe from the sample fluid disposed in the container; and injecting a predetermined volume of gas into the probe, wherein the sample fluid disposed within the sample chamber is displaced therefrom.
21. The method as set forth in claim 20, wherein the sample fluid disposed within the sample chamber is displaced into a waste receptacle.
22. The method as set forth in claim 21, further comprising the step of discarding the waste receptacle with sample fluid disposed therein.

Parent Case Info

This application claims priority from Provisional application Ser. No. 60/085,278, filed May 13, 1998.

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Provisional Applications (1)

	Number	Date	Country
	60/085278	May 1998	US

Sample introduction device

Information

Patent Number

Date Filed

Date Issued

Inventors

Original Assignees

Examiners

Agents

CPC

US Classifications

Field of Search

US