Single riser/single capillary blood viscometer using mass detection or column height detection

Description

BACKGROUND OF THE INVENTION

A capillary viscometer is commonly used because of its inherent features such as simplicity, accuracy, similarity to process flows like extrusion dies, no free surface, etc. Viscous flow in capillary viscometry is firmly established both theoretically and experimentally. C. W. Macosko,

Rheology: Principles, Measurements, and Applications

(VCH, 1993). In fact, the capillary viscometer was the first viscometer and this device remains the most common for measuring viscosity for polymer solutions and other non-Newtonian fluids. However, most existing capillary viscometers produce viscosity measurement a shear rate at a time. In the case of Newtonian fluids the observation of the rate of flow at a single pressure drop is sufficient to define the flow behavior. However, in the case of non-Newtonian fluids, viscosity measurements need to be performed over a range of shear rates. In order to measure viscosity over a range of shear rates, it is necessary to repeat the measurement by varying either the driving pressure head or the capillary tube diameter, which leads to a time-consuming measurement requiring intensive labor. Hence, these methods are not suited for measuring the rheology of polymer fluids that may exhibit shear-dependent viscosities. Furthermore, application of such techniques often requires relatively large volumes of the test fluids. Therefore, there has been a need to develop a simple and labor-free viscometer which can measure the viscosity of fluids over shear rates at a time.

In U.S. Pat. No. 6,019,735 (Kensey et al.) and U.S. Pat. No. 6,077,234 (Kensey et al.), which are assigned to the same Assignee, namely Visco Technologies, Inc., of the present invention, there is disclosed a scanning-capillary-tube viscometer for measuring the viscosity of a fluid, e.g., circulating blood of a living being. Among other things, this scanning capillary tube viscometer discloses an apparatus that monitors the changing height of a column of fluid versus time in a riser that is in fluid communication with a living being's circulating blood. A further improvement of this type of scanning capillary tube viscometer is disclosed in application Ser. No. 09/439,735 entitled DUAL RISER/SINGLE CAPILLARY VISCOMETER, which is assigned to the same Assignee as the present invention, namely, Visco Technologies, Inc. and whose entire disclosure is incorporated by reference herein. In that application, a U-shaped tube structure is utilized that generates a falling and rising column of test fluid that is driven by a decreasing pressure differential for moving these columns of fluid through a plurality of shear rates, which is necessary for non-Newtonian fluid (e.g., blood) viscosity determinations. Such an apparatus can produce viscosity data in a low shear range (e.g., approximately 0.02 s

−1

).

However, there is a need for an alternative mechanism of monitoring the changing column of fluid over time, such as detecting the changing mass of the column of fluid, as set forth in the present application. The key principle of the mass-detection-capillary viscometer is that both flow rate and pressure drop at a capillary tube can be determined by a single measurement of collected fluid mass variation with time using a load cell. Thus, there also remains a need to develop a viscosity determination in a quasi-steady capillary flow and to measure the viscosity of non-Newtonian fluids (e.g., polymer solutions, circulating blood of a living being, etc.) over a range of shear rates.

SUMMARY OF THE INVENTION

An apparatus for determining the viscosity of the circulating blood of a living being over plural shear rates using a decreasing pressure differential. The apparatus comprises: a lumen (e.g., a riser tube) being positioned at an angle to a horizontal reference greater than zero degrees, wherein the lumen comprises a first end and a second end and wherein the first end is exposed to atmospheric pressure and wherein the lumen comprises a first known dimension (e.g., the diameter of the lumen); a flow restrictor (e.g., a capillary tube) having an inlet and an outlet wherein the outlet is arranged to deliver any blood that passes therethrough to a collector, and wherein the flow restrictor includes some known dimensions (e.g., the length and diameter of the flow restrictor); a valve coupled to the vascular system of the living being at a first port and wherein the valve comprises a second port coupled to the second end and a third port is coupled to the inlet; a sensor for detecting the movement of the blood over time (e.g., a mass detector, a column level detector, etc.) through the apparatus and wherein the sensor generates data relating to the movement of the blood over time; a processor, the valve to create a column of blood in the first lumen and the flow restrictor and to establish a pressure differential between the first end and the outlet, and wherein the column of blood moves through the lumen and the flow restrictor at a first shear rate caused by the pressure differential and wherein the movement of the column of blood causes the pressure differential to decrease from the first shear rate for generating the plural shear rates; and wherein the processor calculates the viscosity of the blood based on the data relating to the movement of the column of blood over time, the first known dimension of the lumen and the some known dimensions of the flow restrictor.

A method for determining the viscosity of the circulating blood of a living being over plural shear rates caused by a decreasing pressure differential. The method comprises the steps of: (a) providing a lumen having a first end and a second end and positioned at an angle to a horizontal reference greater than zero degrees, and wherein the lumen has a first known dimension (e.g., the diameter of the lumen) and wherein the first end is exposed to atmospheric pressure; (b) diverting a portion of the circulating blood into the lumen through the second end to form a column of blood therein; (c) coupling an inlet of a flow restrictor to the second end of the lumen to establish a pressure differential between the first end and the outlet and wherein the flow restrictor has an outlet that is arranged to deliver any blood that passes therethrough to a collector and wherein the flow restrictor has some known dimensions (e.g., the length and the diameter of the flow restrictor); (d) controlling the column of blood to form a continuous column of blood in the lumen and the flow restrictor, and wherein the column of blood moves through the lumen and the flow restrictor at a first shear rate caused by the pressure differential and wherein the movement of the column of blood causes the pressure differential to decrease from the first shear rate for generating the plural shear rates; (e) providing a sensor for detecting the movement of the column of blood over time (e.g., a mass detector, a column level detector, etc.) as the column of blood moves and passes from the outlet into the collector while maintaining the outlet submerged in blood that has collected in the collector, and wherein the sensor generates data regarding the movement; and (f) calculating the viscosity of the blood based on the generated data, the first known dimension and the some known dimensions.

An apparatus for determining the viscosity of the circulating blood of a living being over plural shear rates using a decreasing pressure differential. The apparatus comprises: a lumen (e.g., a riser tube) being positioned at an angle to a horizontal reference greater than zero degrees, and wherein the lumen comprises a first end and a second end and wherein the lumen also comprises a first known dimension (e.g., the diameter of the lumen); a flow restrictor (e.g, a capillary tube) having an inlet and an outlet wherein the outlet is arranged to deliver any blood that passes therethrough to a collector and wherein the inlet is coupled to the second end and wherein the flow restrictor includes some known dimensions (e.g., the length and diameter of the flow restrictor); a valve coupled to the vascular system of the living being at a first port and wherein the valve comprises a second port coupled to the first end; a sensor for detecting the movement of the blood over time (e.g., a mass detector, a column level detector, etc.) through the apparatus and wherein the sensor generates data relating to the movement of the blood over time; a processor, coupled to the valve and the sensor wherein the processor is arranged to operate the valve to create a column of blood in the first lumen and the flow restrictor and to establish a pressure differential between the first end and the outlet and wherein the column of blood moves through the lumen and the flow restrictor at a first shear rate caused by the pressure differential and wherein the movement of the column of blood causes the pressure differential to decrease from the first shear rate for generating the plural shear rates; and wherein the processor calculates the viscosity of the blood based on the data relating to the movement of the column of blood overtime, the first known dimension of the lumen and the some known dimensions of the flow restrictor.

A method for determining the viscosity of the circulating blood of a living being over plural shear rates caused by a decreasing pressure differential. The method comprises the steps of: (a) providing a lumen (e.g., a riser tube) having a first end and a second end and positioned at an angle to a horizontal reference greater than zero degrees and wherein the lumen has a first known dimension (e.g., the diameter of the lumen); (b) coupling an inlet of a flow restrictor (e.g., a capillary tube) to said second end and arranging an outlet of the flow restrictor to deliver any blood that passes therethrough to a collector and wherein the flow restrictor has some known dimensions (e.g., the length and diameter of the flow restrictor); (c) diverting a portion of the circulating blood into the lumen through the first end to form a column of blood in the lumen and the flow restrictor and to establish a pressure differential between the first end and the outlet; (c) exposing the first end to atmospheric pressure to cause the column of blood to move through the lumen and the flow restrictor, wherein the movement of the column of blood causes the pressure differential to decrease from the first shear rate for generating the plural shear rates; (d) providing a sensor for detecting the movement of the column of blood over time (e.g., a mass detector, a column level detector, etc.) as the column of blood moves and passes from the outlet into the collector while maintaining the outlet submerged in blood that has collected in the collector and wherein the sensor generates data regarding the movement; and (e) calculating the viscosity of the blood based on the generated data, the first known dimension and the some known dimensions.

An apparatus for determining the viscosity of the circulating blood of a living being over plural shear rates using a decreasing pressure differential. The apparatus comprises: a first lumen (a riser tube) being positioned at an angle to a horizontal reference greater than zero degrees and wherein the lumen comprises a first end and a second end and wherein the first end is exposed to atmospheric pressure and wherein the lumen comprises a first known dimension (e.g., the diameter of the first lumen); a flow restrictor (e.g., a capillary tube) having an inlet and an outlet wherein the inlet is coupled to the second end and wherein the flow restrictor includes some known dimensions (e.g., the length and diameter of the flow restrictor); a valve coupled to the vascular system of the living being at a first port wherein the valve comprises a second port coupled to the outlet and a third port coupled to an input of a second lumen (e.g., an adaptor, etc.) arranged to deliver any blood that passes therethrough to a collector through an output of the second lumen; a sensor for detecting the movement of the blood over time (e.g., a mass detector, a column level detector, etc.) through the apparatus and wherein the sensor generates data relating to the movement of the blood over time; a processor, coupled to the valve and the sensor and wherein the processor is arranged to operate the valve to create a column of blood in the first lumen and the flow restrictor and to establish a pressure differential between the first end and the output wherein the column of blood moves through the lumen and the flow restrictor at a first shear rate caused by the pressure differential and wherein the movement of the column of blood causes the pressure differential to decrease from the first shear rate for generating the plural shear rates; and wherein the processor calculates the viscosity of the blood based on the data relating to the movement of the column of blood over time, the first known dimension of the first lumen and the some known dimensions of the flow restrictor.

DESCRIPTION OF THE DRAWINGS

The invention of this present application will be readily appreciated as the same becomes better understood by reference to the following detailed description when considered in connection with the accompanying drawings wherein:

FIG. 1

is a block diagram of a single riser/single capillary (SRSC) blood viscometer using mass detection which is also referred to as a mass detection capillary blood viscometer (MDCBV);

FIG. 1A

is a height vs. time plot of the blood column in the riser tube of the MDCBV;

FIG. 1B

is a mass vs. time plot of the blood as it is collected in the collector of the MDCBV;

FIG. 2

is a front view of an embodiment of the MDCBV;

FIG. 3

is a side view of the MDCBV;

FIG. 4

is a functional diagram of the MDCBV;

FIG. 5A

is a functional diagram of the valve activated to create a column of blood;

FIG. 5B

is a functional diagram of the valve activated to permit the column of blood to fall and be collected in a collector;

FIG. 5C

is a functional diagram of the valve activated to halt all motion of the column of blood;

FIG. 5D

is a functional diagram of the valve activated to permit the column of blood to fall while data is taken as the collector receives the increasing amount of blood;

FIG. 6

is a functional diagram of a second embodiment of the MDCBV having an alternative position of the capillary tube;

FIG. 7

is a functional diagram of a third embodiment of the MDCBV having an alternative position of the valve mechanism;

FIG. 8A

is a functional diagram of the valve mechanism of

FIG. 7

activated to create a column of blood;

FIG. 8B

is a functional diagram of the valve mechanism of

FIG. 7

activated to permit the column of blood to move and be collected in a collector;

FIG. 9

depicts a fourth embodiment of the MDCBV wherein the changing mass of falling column of blood is detected;

FIG. 10

depicts the mass vs. time plot the falling column of blood for the fourth embodiment of

FIG. 9

;

FIG. 11

is a block diagram of a SRSC blood viscometer using a column height detector known as a column height detection capillary (CHDC) blood viscometer wherein the changing height of a falling column of blood is monitored;

FIG. 12

is a front view of an embodiment of the CHDC blood viscometer;

FIG. 13

is a functional diagram of the CHDC blood viscometer;

FIG. 14

is a functional diagram of a second embodiment of the CHDC blood viscometer having an alternative location of the flow restrictor; and

FIG. 15

is a functional diagram of a third embodiment of the CHDC blood viscometer having an alternative location of the valve mechanism.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

The present invention, generally referred to as a single riser/single capillary (SRSC) blood viscometer, uses a single riser tube and a single flow restrictor (e.g., a capillary tube) structure for determining the viscosity of the circulating blood of a living being.

Although the SRSC blood viscometer can be implemented in a number of ways, two exemplary apparatus/methods are set forth below. The first implementation uses the SRSC structure along with mass detection and hence is hereinafter referred to as a mass detection capillary blood viscometer (MDCBV)

20

. The second implementation uses the SRSC structure along with column height detection and hence is hereinafter referred to as a column height detection capillary (CHDC) blood viscometer

1020

.

Referring now in detail to the various figures of the drawing wherein like reference characters refer to like parts, there is shown at

920

a mass detecting capillary blood viscometer (MDCBV).

The MDCBV

920

basically comprises a blood receiver

922

and an analyzer/output portion

924

. The patient is coupled to the MDCBV

920

through a circulating blood conveyor

926

, e.g., a needle, an IV needle, an in-dwelling catheter, etc., or any equivalent structure that can convey circulating blood from a patient to the MDCBV

920

. As will be discussed in detail later, the analyzer/output portion

924

provides a display

28

for presenting the viscosity information, as well as other information to the operator. The analyzer/output portion

924

may also provide this information to other suitable output means

330

, such as a datalogger

332

, other computer(s)

334

, a printer

336

, a plotter

338

, remote computers/storage

340

, to the Internet

342

or to other on-line services

344

.

The blood receiver

922

basically comprises a valve mechanism

946

coupled to a riser tube R on one side and coupled to a flow restrictor

24

(e.g., a capillary tube) on the other side. The output of the flow restrictor

24

is directed into a fluid collector

26

via an adaptor

34

. When the blood conveyor

926

is coupled to the blood receiver

922

, the valve mechanism

946

controls the flow of blood into the blood receiver

922

, as will be discussed in detail later. The upper end of the riser tube R is exposed to atmospheric pressure. The riser tube R may be positioned at any non-zero angle to a horizontal reference position (e.g., the datum line as shown in FIG.

4

); one exemplary position is at a vertical orientation with respect to the datum line as shown in FIG.

4

.

It should be understood that the blood receiver

922

may be disposable or non-disposable. As will be discussed in detail later, where the blood receiver

922

is disposable, the components (valve mechanism

946

, riser tube R and flow restrictor

24

) are releasably secured in a blood receiver housing

962

that can be quickly and easily inserted, used during the viscosity test run and then quickly and easily removed for disposal; another disposable blood receiver

922

is then inserted in preparation for the next viscosity test run. On the other hand, where the blood receiver

922

is non-disposable, the components (valve mechanism

946

, riser tube R and flow restrictor

24

) can be thoroughly washed and cleaned in place in preparation for the next viscosity test run.

It should be understood that the flow restrictor

24

does not necessarily have to be an elongated tube but may comprise a variety of configurations such as a coiled capillary tube.

The analyzer/output portion

924

basically comprises a mass detector

28

, a level detector

400

, a processor

30

, the display

928

, a bar code reader

978

, an environmental control unit

980

, and overflow detector

981

, a first battery B

1

and a second back-up battery B

2

. The fluid collector

26

is positioned on top of the mass detector

28

which monitors the increasing mass of blood collecting in the fluid collector

26

. The overflow detector

981

ensures that when the column of blood is generated, no blood overflows the riser R. The processor

30

(e.g., a “386” microprocessor or greater, or any equivalent) is arranged to analyze the data from the mass detector

28

and to calculate the blood viscosity therefrom, as will also be discussed in detail later. Furthermore, the processor

30

also controls the display

928

for providing the viscosity information and the other information to the operator as well as to the other output means

330

. The processor

30

also controls the valve mechanism

946

based on the data from the mass detector

28

, as will be discussed later. Battery B

1

provides all of the requisite power to the analyzer/output portion

24

, with battery B

2

serving as a back-up power supply. The bar code reader

978

, the environmental control unit

980

and the level detector

400

will be described later.

In general, via the use of the valve mechanism

946

, a column of blood

38

is initially generated in the riser R and then that column of blood

38

is permitted to fall through the riser tube R, through the flow restrictor

24

and into the fluid collector

26

. This movement of blood can be represented by a height vs. time relationship (

FIG. 1A

) with regard to the column of blood in the riser R and by a mass vs. time relationship (

FIG. 1B

) with regard to the blood being received in the fluid collector

26

.

As shown more clearly in

FIGS. 2-3

, the preferred embodiment of the MDCBV

920

comprises the blood receiver

922

and the analyzer/output portion

924

contained in respective housings

960

and

962

, each of which can be releasably secured to a common frame, e.g., a conventional intravenous (IV) pole

48

. In this configuration, the analyzer/output portion

924

can be positioned in an inclined orientation (see

FIG. 3

) to facilitate user operation and viewing of the display

928

. However, it should be understood that the respective housing constructions are exemplary, and others can be incorporated without limiting the scope of this invention.

The display

928

may comprise any suitable conventional devices, e.g., an ELD (electroluminescent display) or LCD (liquid crystal display) that permits the visualization of both text and graphics. The resolution of this display

928

is preferably 800×600 VGA or above. Furthermore, while the preferred embodiment utilizes a touch screen display which incorporates, among other things:

graphical display

961

instruction, and/or data, display

965

(which also includes the command line display shown as “RUN TEST”; e.g., “TESTING”, “TEST IN PROGRESS,” etc.)

alphanumeric keypad

968

emergency stop button

970

battery status indicators,

972

A and

972

B

function buttons

974

,

it should be understood that any equivalent display device is within the broadest scope of the invention. Thus, any number of user interfaces and buttons may be available through the display

928

. Therefore the invention

920

is not limited to the embodiment that is shown in FIG.

2

. Moreover, the display

928

can be operated to minimize or maximize, or overlay any particular graphic or text screen, as is available in any conventional object-oriented operating system, such as Microsoft™ WINDOWS.

The lower housing

960

comprises the blood receiver

922

and the mass detector

28

. In the preferred embodiment, the mass detector

28

may comprise a precision balance, or load cell, such as The Adventurer™ by Ohaus Corporation of Florham Park, N.J. Thus, as the collector

26

collects more of the blood during the viscosity test run, the changing mass value is transmitted to the processor

30

from the mass detector

28

for viscosity determination; in particular, the mass detector

28

generates an electrical signal that corresponds to the mass variation in time. It should be understood that the term “mass” may be interchanged with the term “weight” for purposes of this invention. It should also be understood that the connection between the mass detector

28

and the processor

30

is bi-directional; this allows the processor

30

to reset the mass detector

28

in preparation for a new test run.

It should also be understood that although it is preferable to have the riser tube R in a vertical position, it is within the broadest scope of this invention to have the riser tube R oriented at any angle greater than zero degrees, with respect to a horizontal reference (e.g., datum line shown in FIG.

4

).

Where the blood receiver

922

is disposable, it is releasably secured in the housing

960

such that once a test run is completed and/or a new patient is to be tested, all of the lumens (e.g., the riser tube R, the capillary

24

, the adaptor

34

and the valve mechanism

946

) can be easily/quickly removed, disposed of and a new set inserted. For example, a bracket

147

(

FIG. 2

) may be used to releasably secure the upper portion of the riser tube R.

A door

976

(which can be vertically or horizontally hinged to the housing

960

) is provided to establish a temperature-controlled environment during the test run. In particular, the door

976

also supports an environmental control unit

980

(e.g., a heater, fan and/or thermostat) such that when it is closed in preparation for the test, the flow restrictor

24

is then heated (or cooled) and maintained throughout the test run at the same temperature and environment as the living being. Prior to the run, the living being's temperature is taken and the operator enters this temperature (via the touch screen display

928

). The environmental control unit

980

then operates to achieve and maintain this temperature. It should be noted that it is within the broadest scope of this invention to include a environmental control unit

980

that achieves and maintains the entire blood receiver

922

at the patient's temperature during the run. By properly maintaining the temperature throughout the test run, the effects of any temperature variation in the viscosity measurement is minimized.

The door

976

may also support the bar code reader

978

. The bar code reader

978

automatically reads a bar code (not shown) that is provided on the riser tube R. The bar code contains all of the predetermined data regarding the characteristics of the flow restrictor

24

(e.g., its length and diameter) and the characteristics of the riser tube R. This information is passed to the processor

30

which is then used to determine the viscosity.

The batteries B

1

/B

2

may each comprise a 12VDC, 4 amp-hour battery, or any equivalent power supply (e.g., batteries used in conventional lap-top computers such as lithium ion batteries). The display

928

provides the status indicators

972

A/

972

B for each battery in the MDCBV

920

. In particular, when the MDCBV

920

is operating off of battery B

1

, the two battery indicators

972

A/

972

B appear on the display

928

. However, once battery B

1

is depleted, the battery B

1

indicator

972

A disappears and the battery B

2

indicator

972

B blinks to warn the operator that the MDCBV

920

is now operating off of the back-up battery B

2

and re-charge of battery B

1

is necessary.

The preferred fluid collector

26

of the present invention is similar to that disclosed in application Ser. No. 09/789,350. In particular, the collector

26

comprises an inner circular wall

35

that divides the collector

26

into a central portion

31

and an annular portion

39

. The central portion

31

collects the blood as it enters the collector

26

. The column of blood

38

falls through the riser tube R, the flow restrictor

24

, the adaptor

34

and then into the central portion

31

. Any overflow spills into the annular portion

39

.

It should be understood that the phrase “column of blood 38” is meant to cover the continuous element of blood that occupies the riser tube R as well as the blood that occupies the flow restrictor

24

and the adaptor

34

.

To minimize any surface tension effects that would normally occur if an open end

36

of the adaptor was positioned above the level of collected blood

300

in the central portion

31

, it is necessary to begin collecting mass vs. time data only when the open end

36

of the adaptor

34

is submerged within the collected blood

300

. This is shown most clearly in FIG.

4

. In order to accomplish this, the open end

36

of the adaptor

34

is placed appropriately below the datum line (e.g., the top edge

37

of the inner wall

35

of the preferred collector

26

) and the level detector

400

is provided for detecting when the collected blood

300

has reached the datum level. The level detector

400

informs the processor

30

when this event has occurred. Thus, the processor

30

is able to determine those mass vs. time data points where surface tension effects are minimized. The level detector

400

can be implemented in various ways known to those skilled in art, e.g., float sensors, tuning fork sensors, ultrasonic sensors, optical sensors, proximity sensors, capacitance sensors, etc. and all of which generate an electrical signal when a particular fluid level has been reached. An exemplary sensor is the ColeParmer EW-20603-22 Capacitive Level Sensor.

It should be understood that the output side

3

of the flow restrictor

24

can be integrally formed with the input side

5

of the adaptor

34

.

The concept of the blood viscosity determination using the MDCBV

920

is that a portion of the circulating blood of the living being is diverted from the living being using the blood conveyor

926

into the blood receiver

922

to create a column of blood

38

(

FIG. 4

) in the riser tube R. Next, the column of blood

38

is allowed to fall and collect in the fluid collector

26

over time, whereby the changing mass of this collector

26

is monitored over time. From this mass vs. time data and based on the characteristics of the flow restrictor

24

and the riser tube R, the circulating blood viscosity can be determined. In addition, where the blood exhibits yield stress, τ

y

a residual amount of the column of blood

38

remains in the riser tube R after a long period of time at the end of the viscosity test run; furthermore, there are surface tension effects that also contribute to this residual amount of the column of blood

38

as a result of the gas-liquid interface

23

(FIG.

4

). The height of this residual column of fluid is known as Δh

∞

, where Δh=h(t)−datum level and where h(t) represents the height of the column of blood

38

in the riser tube R at any time; the term h

∞

(

FIG. 1A

) represents the final height of the column of blood

38

in the riser tube R at the end of the test run after a long period of time. As will also be discussed later, the viscosity determination of the blood can be determined using the MDCBV

920

without the need to determine h(t) or the initial position, h

i

, of the column of blood

38

in the riser tube R at which data is collected.

To obtain accurate data, it is important to “wet” all of the lumens, namely, the riser tube R, the valve mechanism

946

, the flow restrictor

24

and the adaptor

34

before data is taken. As a result, in order to generate the column of blood

38

and then allow it to fall, the valve mechanism

946

must be operated as follows: When the viscosity test run is initiated, the processor

30

activates the valve mechanism

946

by commanding a valve driver

986

(e.g., a 500 mA solenoid, or stepper motor, etc.) which rotates the valve into the position shown in FIG.

5

A. This allows the diverted portion of the circulating blood to flow up into the riser tube R to create the column of blood

38

. When the overflow detector

981

detects a predetermined height, h

0

, of the column of blood

38

, the overflow detector

981

informs the processor

30

which then commands the valve driver

986

to rotate the valve into the position shown in FIG.

5

B. As a result, the column of blood

38

begins to fall through the riser tube R, through the valve mechanism

946

, into the flow restrictor

24

, through the adaptor

34

and into the central portion

31

of the fluid collector

26

. As mentioned earlier, the processor

30

is informed by the level detector

400

when the open end

36

of the adaptor

34

is submerged under the level of the collected blood

300

in order to minimize any surface tension effects. Next, the valve driver

986

is commanded by the processor

30

into the position shown in

FIG. 5C

which halts all motion of the column of blood

38

. The initial position of the column of blood, h

i

, is thereby established for viscosity determination purposes, as will be discussed later. Finally, the processor

30

commands the valve driver

986

to rotate the valve into the position shown in FIG.

5

D and the column of blood

38

begins falling while data is collected.

The overflow detector

981

may comprise an optical source

981

A, e.g., a light emitting diode (LED) and a photodetector

981

B for detecting emitted light from the optical source

981

A; once the upper end of the column of blood

38

interrupts the emitted light, the photodetector

981

B informs the processor

30

which operates the valve mechanism

946

, as discussed previously. It should be understood that this implementation of the overflow detector

981

is exemplary only and that it is within the broadest scope of this invention to include all methods of level detection known to those skilled in the art of detecting the level of the column of blood

38

in the riser tube R.

FIG. 6

depicts a second embodiment of the MDCBV

920

wherein the flow restrictor

24

forms the lower end of the riser tube R, rather than being located on the other side of the valve mechanism

946

. As a result, the input side

5

of the adaptor

34

is coupled to the valve mechanism

946

. For proper operation, the datum line needs to be above the input side

7

of the flow restrictor

24

, as shown in FIG.

6

. Other than that, the operation of this variation is governed by the same equations for the first embodiment as will be discussed below.

FIG. 7

depicts a third embodiment of the MDCBV

920

wherein the valve mechanism

946

′ is positioned at the top of the riser tube R, rather than at the bottom. The advantage of this valve mechanism

946

′, position is that there is no need to first fill the riser tube R to a predetermined level before proceeding with the test run; instead, in accordance with the valve mechanism

946

′ operation as shown in

FIGS. 8A-8B

, the test run proceeds with the processor

30

commanding the valve driver

986

to rotate the valve to the position shown in FIG.

8

A and then the processor

30

stops any more input flow from the blood conveyor

926

as shown in FIG.

8

B. In particular, as used in this embodiment, the blood conveyor

926

is coupled to the valve mechanism

946

′ at a port

763

; the top end of the riser tube R is coupled to the valve mechanism

946

′ at a port

765

. The valve mechanism

946

′ also includes a vent coupler

762

that couples the top of the riser R to a third port

764

that is exposed to atmospheric pressure; thus when the valve is rotated into the position shown in

FIG. 8B

, the blood in the riser tube R will flow downwards. Again, it should be emphasized that to minimize any surface tension effects, the level detector

400

informs the processor

30

when the open end of the adaptor

34

is submerged in the collected blood

300

. Other than that, the operation of this variation is governed by the same equations mentioned previously.

MDCBV Theory of Operation

The concept of the blood viscosity determination using the MDCBV

920

is based on the discussion of determining the viscosity of non-Newtonian fluids, such as blood, as discussed in detail in application Ser. No. 09/789,350, whose entire disclosure is incorporated by reference herein. The MDCBV

920

basically comprises a cylinder (i.e., the riser tube R) having a diameter, φ

R

, into which a portion of the circulating blood of the living being is diverted for viscosity analysis. The bottom of the riser tube R is coupled to the flow restrictor

24

(e.g., a capillary tube), having a diameter φ

c

and a length L

c

. It is preferable that the diameter of the adaptor

34

be similar to the diameter of the riser tube R, φ

R

.

Using this configuration of riser tube R and flow restrictor

24

, once the column of blood

38

is generated (as shown in FIG.

4

), when the valve mechanism

946

is rotated to the position shown in

FIG. 5B

, the column of blood

38

is subjected to a decreasing pressure differential that moves the column

38

through a plurality of shear rates (i.e., from a high shear rate at the beginning of the test run to a low shear rate at the end of the test run, as can be clearly seen in the column height change—FIG.

1

A and the mass accumulating in the collector

26

′—FIG.

1

B), which is especially important in determining the viscosity of non-Newtonian fluids, such as blood. In particular, once the desired height, h

i

is achieved by the column of blood

38

and with the upper end of the riser tube R exposed to atmospheric pressure, a pressure differential is created between the column of fluid

38

and the outlet

36

of the adaptor

34

. As a result, the column of blood

38

flows down the riser tube R, through the flow restrictor

24

, through the adaptor

34

and into the collector

26

′. As the column of blood

38

flows through these components, the movement of column of blood

38

causes the pressure differential to decrease, thereby causing the movement of the column of blood

38

to slow down. This movement of the column of blood

38

, initially at a high shear rate and diminishing to a low shear rate, thus covers the plurality of shear rates. However, it should be understood that it is within the broadest scope of this invention to include any other configurations where the column of blood

38

can be subjected to a decreasing pressure differential in order to move the column of blood

38

through a plurality of shear rates.

The rate of flow through the flow restrictor

24

is equal to the rate of change of the mass of the blood

300

collected on the mass detector

28

. Hence, the corresponding flow rate in the flow restrictor

24

can be expressed as:

\begin{matrix} Q (t) = \frac{1}{ρ} \frac{ⅆ m}{ⅆ t} & (1) \end{matrix}

where ρ is the density of the blood.

In order to determine the viscosity of the blood, it is necessary to know the pressure drop across the flow restrictor

24

. What is measured using the MDCBV

20

is the total pressure drop between the riser tube R and the flow restrictor

24

including not only the pressure drop across the flow restrictor or capillary tube

24

(ΔP

c

) but also the pressure drop occurring at the inlet and outlet (ΔP

e

) of the capillary tube

24

. One of the accurate methods for determining (ΔP

e

) is to make a Bagley plot (see C. W. Macosko,

Rheology: Principles, Measurements, and Applications

(VCH, 1993)) with at least two short capillary tubes (not shown) of the same diameter. Hence, the pressure drop occurring at the inlet and at the outlet of the capillary tube

24

has to be subtracted from the total pressure difference (ΔP

t

). Considering these pressure drops, the pressure drop across the capillary tube

24

can be described as

ΔP

c

=ΔP

t

−ΔP

e

(2)

It should be noted that the contribution from the second term on the right hand side (ΔP

e

) in Eq. (2) is less than 0.5%; hence this term can be neglected for all practical purposes, and as a result, equation 2 reduces to:

Δ

P

c

=ΔP

t

(3)

An expression, therefore, for the total pressure as well as the pressure across the capillary tube

24

is:

ΔP

t

=ΔP

c

=ρg[h

i

−Δh

(

t

)−

h

∞

]=ρg[h

i

−h

∞

−Δh

(

t

)] (4),

where Δh(t) represents the changing height of the falling column of blood

38

and is given by the following equation:

\begin{matrix} Δ h (t) = \frac{4 m (t)}{{ρπθ}_{R}^{2}} & (5) \end{matrix}

and where:

h

i

is the initial height of the column of blood

38

;

h

∞

is the final height of the column of blood

38

after a long period of time; and

m(t) is the mass of the collector

26

over time.

In addition, the final mass after a long period of time, m

∞

, can be expressed in terms of the height of the column of blood

38

as follows:

\begin{matrix} m_{\infty} - m_{i} = ρ (\frac{{πθ}_{R}^{2}}{4}) (h_{i} - h_{\infty}); & (6) \end{matrix}

and solving equation 6 for (h

i

−h

∞

),

\begin{matrix} (h_{i} - h_{\infty}) = \frac{4 (m_{\infty} - m_{i})}{{ρπθ}_{R}^{2}} & (7) \end{matrix}

Thus, making the substitution of equations 5 and 7 into equation 4,

\begin{matrix} Δ P_{c} = ρ g [\frac{4 (m_{\infty} - m_{i})}{{ρπθ}_{R}^{2}} - \frac{4 m (t)}{{ρπθ}_{R}^{2}}] = \frac{4 g}{{πθ}_{R}^{2}} [m_{\infty} - m_{i} - m (t)] & (8) \end{matrix}

It is assumed that any surface tension effects are constant with time and throughout the test run, e.g., the surface tension experienced at h

i

is similar to the surface tension effect experienced at h

∞

.

The significance of equation 8 includes, among other things, that in order to determine the pressure across the capillary tube

24

, only the final mass, m

∞

, the diameter of the riser R and the mass data detected by the mass detector

28

, m(t), need be known; the initial height of the blood column

38

, h

i

, nor the final height, h

∞

, nor the initial mass, m

i

, need to be known. Furthermore, equation 8 also represents, in accordance with the assumption that the surface tension is constant, a surface tension-free capillary.

Non-Newtonian Fluids

The shear rate dependent viscosity for a non-Newtonian fluid, such as blood, flowing in the capillary tube

24

is obtained from experimental data with some mathematical treatment, and the necessary equations can be found in any standard handbook (e.g, C. W. Macosko). The shear rate at the capillary tube

24

wall is obtained form the classical Weissenberg-Rabinowitsch equation (see S. L. Kokal, B. Habibi, and B. B. Maini, Novel Capillary Pulse Viscometer for non-Newtonian Fluids, Review of Scientific Instrument, 67(9), pp. 3149-3157 (1996)):

{{\dot{γ}}_{w} (t) = - \frac{ⅆ V_{z}}{ⅆ r} &RightBracketingBar;}_{r = R}

\begin{matrix} = \frac{1}{4} {\dot{γ}}_{aw} [3 + \frac{ⅆ \ln Q}{ⅆ \ln τ_{w}}] & (9) \end{matrix}

where {dot over (γ)}

aw

is the apparent or Newtonian shear rate at the wall and where φ

c

is the diameter of the capillary tube

24

.

\begin{matrix} {\dot{γ}}_{aw} (t) = \frac{32 Q (t)}{{πφ}_{c}^{3}} & (10) \end{matrix}

and the shear stress at the wall is given by:

\begin{matrix} τ_{w} (t) = \frac{Δ P (t) φ_{c}}{4 L_{c}} & (11) \end{matrix}

Thus, the viscosity corresponding to the wall shear rate is calculated in the form of a generalized Newtonian viscosity:

\begin{matrix} η = \frac{τ_{w}}{{\dot{γ}}_{w}} = \frac{{πφ}_{c}^{4} Δ P}{32 {QL}_{c}} {(3 + \frac{ⅆ \ln Q}{ⅆ \ln τ_{w}})}^{- 1} = \frac{ρ g φ_{c}^{4}}{8 L_{c} φ_{R}^{2}} \frac{[m_{\infty} - m_{i} - m (t)]}{(\frac{ⅆ m}{ⅆ t}) (3 + \frac{1}{n^{'}})} & (12) \end{matrix}

where

\frac{1}{n^{'}} = \frac{ⅆ \ln Q}{ⅆ \ln τ_{w}} .

Thus, Equation 12 represents the viscosity of the blood in terms of the mass measured by the MDCBV

920

.

The viscosity versus shear rate information can be obtained from equations 9-12 by measuring the mass of the collected fluid with respect to the time from which the pressure drop and flow rate can be calculated. The values of R and L

c

must be obtained by calibration. Since equation (9) is non-linear, the procedure to calculate the shear rate and the corresponding viscosity is not straightforward. One of the approaches to obtain the viscosity from the general equations presented above is to adopt a finite difference technique for differentiation of equation (9). If there is enough data near the point of interest, it is possible to evaluate the derivative as:

\begin{matrix} \frac{1}{n^{'}} = \frac{ⅆ \ln Q}{ⅆ \ln τ_{w}} = \frac{1}{n} & (13) \end{matrix}

where n is simply the exponent of the power law constitutive equation. Even though the power-law exponent is used in the above equations, this does not limit the capability of the present measurement for power-law fluids. The rigorous approach can still be taken for obtaining a viscosity versus shear rate relationship for any fluid (see S. L. Kokal, B. Habibi, and B. B. Maini, “Novel Capillary Pulse Viscometer for non-Newtonian fluids, Review of Scientific Instrument, 67(9), 3149-3157 (1996)).

In application Ser. No. 09/789,350 there is a figure, namely,

FIG. 7

, which illustrates the viscosity results using a mass detector viscometer for blood and which shows an excellent agreement with those from a conventional rotating viscometer, e.g., the Physica UDS-200 over a range of shear rates.

As mentioned earlier

FIGS. 1A and 1B

provide a summary of the height vs. time characteristic, and the mass vs. time characteristic, of the falling column of blood

38

during the viscosity test run. As can be seen in

FIG. 8A

, the level of the column of blood

38

initially is at h

i

. During the test run, the column of blood

38

falls and arrives at a final column height of h

∞

after a long period of time (e.g., 2-5 minutes after the column of blood

38

begins to fall). As also mentioned earlier, this final height h

∞

can be attributed to both the surface tension effect of the gas-liquid interface

23

(

FIG. 4

) as well as any yield stress, τ

y

, exhibited by the blood. With regard to the change in mass, m(t), as shown in

FIG. 8B

, the mass climbs quickly and then slows down towards a final mass value, m

∞

after a long period of time. As mentioned earlier, what is important here is that the viscosity of the blood can be determined using the MDCBV

920

without the need to know h

i

and h

∞

.

FIG. 9

depicts a fourth embodiment of the MDCBV

920

wherein the changing mass of the riser R and flow restrictor

24

are detected, rather than detecting the change in mass of the collected blood

300

in the collector

26

. Thus, rather than obtaining an increasing mass with time, the mass detector

28

detects the decreasing mass of the riser R/flow restrictor

24

assembly with time, as shown in FIG.

10

. The empty weight of the riser R, flow restrictor

24

and a base

29

(upon which the flow restrictor

24

is disposed) are taken into account before the test run is conducted. As a result, the expression for the pressure drop across the capillary tube

24

is:

\begin{matrix} Δ P_{c} = \frac{4 g}{{πφ}_{R}^{2}} [(m_{i} - m_{\infty}) - m (t)] . & (14) \end{matrix}

Other than that, the theory of operation of this fourth embodiment of the MDCBV

920

is similar to that discussed above with regard to the other embodiments of the MDCBV

920

.

A column height detection capillary (CHDC) blood viscometer

1020

is discussed next.

The CHDC blood viscometer

1020

utilizes the same structure, for example, the riser tube R and the flow restrictor

24

, but with the mass detector

28

and the overflow detector

981

replaced by column level detector

1056

. As a result, the viscosity of the circulating blood of the living being can be determined using the CHDC viscometer

1020

. In particular, it can be shown that the viscosity of the circulating blood, η, is given by:

η = \frac{ρ g φ_{c}^{4}}{8 L_{c} φ_{R}^{2}} (\frac{h_{i} - h_{\infty} - Δ h (t)}{\frac{ⅆ h (t)}{ⅆ t} (3 + \frac{1}{n^{'}})})

The column level detector

1056

is similar to the one disclosed in application Ser. No. 09/573,267 whose entire disclosure is incorporated by reference herein. The column level detector

1056

detects the level of the column of blood in the riser tube R and may comprise and LED array

1064

and a CCD

1066

arrangement (FIG.

12

). To that end, the CHDC blood viscometer

1020

basically comprises the blood receiver

922

and an analyzer/output portion

1024

.

It should be emphasized that it is within the broadest scope of this invention to include all ways known in the art for detecting the level of the column of blood and the present invention is not limited, in any way, to the use of optical detection.

As with the MDCBV

920

, the output side

3

of the flow restrictor

24

can be integrally formed with the input side

5

of the adaptor

34

.

FIG. 12

depicts one embodiment of the CHDC blood viscometer

1020

which operates similarly to the MDCBV

920

except that the level of the column of blood

38

is monitored rather than the changing mass in the collector

26

. In addition, the function of the overflow detector

981

in the MDCBV

920

is accomplished by the column level detector

1056

, thereby informing the processor

30

when to operate the valve mechanism

960

to allow the column of blood

38

to fall. As a result, the CHDC blood viscometer

1020

utilizes height vs. time data, as shown in

FIG. 1A

, to determine the blood viscosity.

FIG. 13

is a functional diagram of the CHDC blood viscometer

1020

that depicts the operation of the CHDC blood viscometer

1020

, including the use of the submerged end

36

of the adaptor

34

and the level detector

400

.

FIG. 14

is a second embodiment of the CHDC blood viscometer

1020

wherein the flow restrictor

24

forms the lower end of the riser tube R, rather than being located on the other side of the valve mechanism

946

. As a result, the input side

5

of the adaptor

34

is coupled to the valve mechanism

946

. For proper operation, the datum line needs to be above the input side

7

of the flow restrictor

24

, as shown in FIG.

14

. Other than that, the operation of this variation is governed by the same equations for the first embodiment of the CHDC blood viscometer

1020

as will be discussed below.

FIG. 15

depicts a third embodiment of the CHDC blood viscometer

1020

wherein the valve mechanism

946

′ is positioned at the top of the riser tube R, rather than at the bottom. The same discussion that applies to the third embodiment of the MDCBV

920

that was discussed earlier, applies here for the CHDC blood viscometer

1020

.

Without further elaboration, the foregoing will so fully illustrate our invention and others may, by applying current or future knowledge, readily adapt the same for use under various conditions of service.

Claims

1. An apparatus for determining the viscosity of the circulating blood of a living being over plural shear rates using a decreasing pressure differential, said apparatus comprising:a lumen being positioned at an angle to a horizontal reference greater than zero degrees, said lumen comprising a first end and a second end, said first end being exposed to atmospheric pressure, said lumen comprising a first known dimension; a flow restrictor having an inlet and an outlet, said outlet being arranged to deliver any blood that passes therethrough to a collector, said flow restrictor including some known dimensions; a valve coupled to the vascular system of the living being at a first port, said valve comprising a second port coupled to said second end and a third port coupled to said inlet; a sensor for detecting the movement of the blood over time through said apparatus, said sensor generating data relating to the movement of the blood over time; a processor, coupled to said valve and said sensor, said processor arranged to operate said valve to create a column of blood in said first lumen and said flow restrictor and to establish a pressure differential between said first end and said outlet, said column of blood moving through said lumen and said flow restrictor at a first shear rate caused by said pressure differential, said movement of said column of blood causing said pressure differential to decrease from said first shear rate for generating said plural shear rates; and wherein said processor calculates the viscosity of the blood based on said data relating to the movement of the column of blood over time, said first known dimension of said lumen and said some known dimensions of said flow restrictor.
2. The apparatus of claim 1 wherein said outlet remains submerged in the blood that is being collected in said collector when said column of blood is moving.
3. The apparatus of claim 2 wherein said sensor detects the changing weight of said collector over time as the blood passes from said outlet into said collector.
4. The apparatus of claim 2 wherein said column of blood comprises a level that changes with time, said sensor detecting said changing level of fluid over time.
5. The apparatus of claim 3 wherein said flow restrictor is a capillary tube and wherein the pressure drop across said capillary tube, ΔPc, is given by: Δ⁢ ⁢Pc=4⁢gπφR2⁡[m∞-mi-m⁡(t)]⁢ where,g⁢ ⁢is⁢ ⁢gravitational⁢ ⁢acceleration;φR⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢lumen;m∞⁢ ⁢is⁢ ⁢the⁢ ⁢final⁢ ⁢weight⁢ ⁢of⁢ ⁢said⁢ ⁢collector⁢ ⁢after⁢ ⁢a⁢ ⁢long⁢ ⁢⁢ ⁢period⁢ ⁢of⁢ ⁢timemi⁢ ⁢is⁢ ⁢the⁢ ⁢initial⁢ ⁢weight⁢ ⁢of⁢ ⁢said⁢ ⁢collector⁢ ⁢before⁢ ⁢said⁢ ⁢column⁢ ⁢⁢ ⁢of⁢ ⁢blood⁢ ⁢starts⁢ ⁢moving;andm⁡(t)⁢ ⁢is⁢ ⁢the⁢ ⁢changing⁢ ⁢weight⁢ ⁢of⁢ ⁢the⁢ ⁢collector⁢ ⁢over⁢ ⁢time.
6. The apparatus of claim 5 wherein the viscosity, η, is given by: η=ρ⁢ ⁢g⁢ ⁢φc48⁢Lc⁢φR2⁢(m∞-mi-m⁡(t)(ⅆmⅆt)⁢(3+1n′))where,ρ⁢ ⁢is⁢ ⁢the⁢ ⁢density⁢ ⁢of⁢ ⁢the⁢ ⁢blood;φc⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢capillary⁢ ⁢tube;Lc⁢ ⁢is⁢ ⁢the⁢ ⁢length⁢ ⁢of⁢ ⁢said⁢ ⁢capillary⁢ ⁢tube;and1n′=ⅆln⁢ ⁢Qⅆln⁢ ⁢τw,whereQ is the volumetric flow rate through said capillary tube; and τw⁢ ⁢is⁢Δ⁢ ⁢Pc⁢φc4⁢Lc.
7. The apparatus of claim 6 wherein the quantity 1n′can be approximated by 1nwhere n is the exponent of a power law constitutive equation.
8. The apparatus of claim 3 wherein said sensor is a precision balance or load cell.
9. The apparatus of claim 3 wherein said collector comprises:a container having an inner compartment in which said outlet is disposed; and an annular compartment surrounding said inner compartment for forming an overflow chamber.
10. The apparatus of claim 4 wherein said flow restrictor is a capillary tube and wherein the pressure drop across said capillary tube, ΔPc, is given by:ΔPc=ρg[hi−h∞−Δh(t)]where:ρ is the density of the blood; g is gravitational acceleration; hi is the initial height of said column of blood; h∞ is the final height of said column of blood; and Δh(t) is the changing height of said column of blood over time.
11. The apparatus of claim 10 wherein the viscosity of the blood, η, is given by: η=ρ⁢ ⁢g⁢ ⁢φc48⁢Lc⁢φR2⁢(hi-h∞-Δ⁢ ⁢h⁡(t)ⅆh⁡(t)ⅆt⁢(3+1n′))where,φc⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢capillary⁢ ⁢tube;φR⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢lumen;Lc⁢ ⁢is⁢ ⁢the⁢ ⁢length⁢ ⁢of⁢ ⁢said⁢ ⁢capillary⁢ ⁢tube;and1n′=ⅆln⁢ ⁢Qⅆln⁢ ⁢τw,whereQ is the volumetric flow rate through said capillary tube; and τw⁢ ⁢is⁢ ⁢Δ⁢ ⁢Pc⁢φc4⁢Lc.
12. The apparatus of claim 11 wherein the quantity 1n′can be approximated by 1nwhere n is the exponent of a power law constitutive equation.
13. The apparatus of claim 4 wherein said sensor is a column level detector.
14. The apparatus of claim 4 wherein said collector comprises:a container having an inner compartment in which said outlet is disposed; and an annular compartment surrounding said inner compartment for forming an overflow chamber.
15. A method for determining the viscosity of the circulating blood of a living being over plural shear rates caused by a decreasing pressure differential, said method comprising the steps of:(a) providing a lumen having a first end and a second end and positioned at an angle to a horizontal reference greater than zero degrees, said lumen having a first known dimension, said first end being exposed to atmospheric pressure; (b) diverting a portion of the circulating blood into said lumen through said second end to form a column of blood therein; (c) coupling an inlet of a flow restrictor to said second end of said lumen to establish a pressure differential between said first end and said outlet, said flow restrictor having an outlet that is arranged to deliver any blood that passes therethrough to a collector, said flow restrictor having some known dimensions; (d) controlling said column of blood to form a continuous column of blood in said lumen and said flow restrictor, said column of blood moving through said lumen and said flow restrictor at a first shear rate caused by said pressure differential, said movement of said column of blood causing said pressure differential to decrease from said first shear rate for generating said plural shear rates; (e) providing a sensor for detecting the movement of the column of blood over time as the column of blood moves and passes from said outlet into said collector while maintaining said outlet submerged in blood that has collected in said collector, said sensor generating data regarding said movement; and (f) calculating the viscosity of the blood based on the generated data, said first known dimension and said some known dimensions.
16. The method of claim 15 wherein said step of providing a sensor comprises disposing said collector on a mass detector and obtaining an initial weight of said collector before said column of blood begins moving.
17. The method of claim 16 wherein said mass detector comprises a precision balance or a load cell.
18. The method of claim 15 wherein said step of providing a sensor comprises disposing a column level detector adjacent said lumen for detecting the changing position of a level of said column of blood.
19. The method of claim 16 wherein said flow restrictor is a capillary tube and wherein said step of calculating the viscosity comprises determining the pressure drop across said capillary tube, ΔPc, according to: Δ⁢ ⁢Pc=4⁢gπφR2⁡[m∞-mi-m⁢(t)]⁢ where,g⁢ ⁢is⁢ ⁢gravitational⁢ ⁢acceleration;φR⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢lumen;m∞⁢ ⁢is⁢ ⁢the⁢ ⁢final⁢ ⁢weight⁢ ⁢of⁢ ⁢said⁢ ⁢collector⁢ ⁢after⁢ ⁢a⁢ ⁢long⁢ ⁢period⁢ ⁢of⁢ ⁢timemi⁢ ⁢is⁢ ⁢the⁢ ⁢initial⁢ ⁢weight⁢ ⁢of⁢ ⁢said⁢ ⁢collector⁢ ⁢before⁢ ⁢said⁢ ⁢column⁢ ⁢of⁢ ⁢blood ⁢starts⁢ ⁢moving⁢ ;andm⁡(t)⁢ ⁢is⁢ ⁢the⁢ ⁢changing⁢ ⁢weight⁢ ⁢of⁢ ⁢the⁢ ⁢collector⁢ ⁢over⁢ ⁢time.
20. The method of claim 19 wherein said step of calculating the viscosity of the blood comprises determining the viscosity, η, of the blood according to: η=ρ⁢ ⁢g⁢ ⁢φc48⁢Lc⁢φR2⁢[m∞-mi-m⁢(t)](ⅆmⅆt)⁢(3+1n′)where,ρ is the density of the blood; φc is the diameter of said capillary tube; LC is the length of said capillary tube; and 1n′=ⅆln⁢ ⁢Qⅆln⁢ ⁢τw,whereQ is the volumetric flow rate through said capillary tube; and τw⁢ ⁢is⁢ ⁢Δ⁢ ⁢Pc⁢φc4⁢Lc.
21. The method of claim 20 wherein the quantity 1n′can be approximated by 1nwhere n is the exponent of a power law constitutive equation.
22. The method of claim 18 wherein said flow restrictor is a capillary tube and wherein said step of calculating the viscosity comprises determining the pressure drop across said capillary tube, ΔPc, according to:ΔPc=ρg(hi−h∞−Δh(t)) where,ρ is the density of the fluid; g is gravitational acceleration; h∞ is the final height of said column of blood after a long period of time; hi is the initial height of said column of blood before said column of blood starts moving; and h(t) is the changing weight of the collector over time.
23. The method of claim 22 wherein said step of calculating the viscosity of the blood comprises determining the viscosity, η, of the blood according to: η=ρ⁢ ⁢g⁢ ⁢φc48⁢Lc⁢φR2⁢(hi-h∞-Δ⁢ ⁢h⁡(t)ⅆh⁡(t)ⅆt⁢(3+1n′))where,φc⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢capillary⁢ ⁢tube;φR⁢ ⁢is⁢ ⁢the⁢ ⁢diameter⁢ ⁢of⁢ ⁢said⁢ ⁢lumen;Lc⁢ ⁢is⁢ ⁢the⁢ ⁢length⁢ ⁢of⁢ ⁢said⁢ ⁢capillary⁢ ⁢tube;and1n′=ⅆln⁢ ⁢Qⅆln⁢ ⁢τw,whereQ is the volumetric flow rate through said capillary tube; and τw⁢ ⁢is⁢ ⁢Δ⁢ ⁢Pc⁢φc4⁢Lc.
24. The method of claim 23 wherein the quantity 1n′can be approximated by 1nwhere n is the exponent of a power law constitutive equation.

RELATED APPLICATIONS

This application is a Divisional application of application Ser. No. 09/897,176, filed Jul. 2, 2001, Now U.S. Pat. No. 6,412,336 entitled SINGLE RISER/SINGLE CAPILLARY BLOOD VISCOMETER USING MASS DETECTION OR COLUMN HEIGHT DETECTION, which in turn is a Continuation-In-Part of application Ser. No. 09/789,350, filed Feb. 21, 2001, entitled Mass Detection Capillary Viscometer, now abandoned, which in turn is based on Provisional Application Serial No. 60/228,612 filed Aug. 29, 2000 entitled MASS DETECTION CAPILLARY VISCOMETER. This application is also a Continuation-in-Part of application Ser. No. 09/573,267 filed May 18, 2000, now U.S. Pat. No. 6,402,703 entitled DUAL RISER/SINGLE CAPILLARY VISCOMETER. The entire disclosures of all the above applications are incorporated by reference herein.

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Provisional Applications (1)

	Number	Date	Country
	60/228612	Aug 2000	US

Continuations (1)

	Number	Date	Country
Parent	09/573267	May 2000	US
Child	10/127091		US

Continuation in Parts (1)

	Number	Date	Country
Parent	09/789350	Feb 2001	US
Child	09/897176		US

Single riser/single capillary blood viscometer using mass detection or column height detection

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