TREA

Impedance measurement process

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Information

  • Patent Grant
  • 10070800
  • Patent Number
    10,070,800
  • Date Filed
    Tuesday, December 8, 2015
    8 years ago
  • Date Issued
    Tuesday, September 11, 2018
    6 years ago
Information
Abstract
A method for use in performing impedance measurements on a subject. The method includes, in a processing system, determining at least one first impedance value, measured at a site using a first electrode configuration, determining at least one second impedance value, measured at the site using a second electrode configuration, and determining the presence, absence or degree of an anomaly using the first and second impedance values.
Description
BACKGROUND OF THE INVENTION

The present invention relates to a method and apparatus for performing impedance measurements, and in particular to performing multiple impedance measurements at a given site to determine the presence, absence or degree of biological anomalies such as tissue lesions, and to allow impedance mapping to be performed accounting for any erroneous measurements.


DESCRIPTION OF THE PRIOR ART

The reference in this specification to any prior publication (or information derived from it), or to any matter which is known, is not, and should not be taken as an acknowledgment or admission or any form of suggestion that the prior publication (or information derived from it) or known matter forms part of the common general knowledge in the field of endeavour to which this specification relates.


One existing technique for determining biological parameters relating to a subject, such as fluid levels, involves the use of bioelectrical impedance. This involves measuring the electrical impedance of a subject's body using a series of electrodes placed on the skin surface. Changes in electrical impedance at the body's surface are used to determine parameters, such as changes in fluid levels, associated with the cardiac cycle or oedema, or other conditions which affect body habitus.


However, a number of factors, such as the connectively of the electrodes to the subject, can effect the accuracy of impedance measuring processes. An example of this is encountered with tetrapolar electrode configurations, which are routinely used for tissue characterisation. The tetrapolar configuration involves injecting a constant drive current between an adjacent pair of electrodes (drive electrodes), and measurement of the resulting potential between another pair of adjacent electrodes (measurement electrodes). This measured potential is dependent on the electrical characteristics of the volume of tissues being analysed. However, the tetrapolar configuration can produce erroneous results in the form of an increase in measured impedance when a low impedance lesion is located between a drive and measurement electrode.


As a result, when readings are obtained, it can be difficult to determine if the readings are accurate and if not, to determine the cause of the inaccuracy.


SUMMARY OF THE PRESENT INVENTION

The present invention seeks to substantially overcome, or at least ameliorate, one or more disadvantages of existing arrangements.


In a first broad form the present invention seeks to provide a method for use in performing impedance measurements on a subject, the method including, in a processing system:

    • a) determining at least one first impedance value, measured at a site using a first electrode configuration;
    • b) determining at least one second impedance value, measured at the site using a second electrode configuration; and,
    • c) determining the presence, absence or degree of an anomaly using the first and second impedance values.


Typically the method includes using a tetrapolar electrode arrangement, the first and second electrode configurations using a different configuration of drive and measurement electrodes.


Typically the method includes, in the processing system, determining an impedance value for each of four electrode configurations.


Typically the method uses apparatus including a signal generator, a sensor, a switching device and an electrode array having a number of electrodes, and wherein the method includes in the processing system, controlling the electrode configuration by:

    • a) selectively interconnecting the signal generator and electrodes using the switching device; and,
    • b) selectively interconnecting the sensor and electrodes using the switching device.


Typically the method includes, in the processing system:

    • a) causing at least one drive signals to be applied to the subject;
    • b) measuring at least one induced signal across the subject; and,
    • c) determining at least one impedance value using an indication of the excitation signal and the induced signal.


Typically the method includes, in the processing system:

    • a) determining impedance values at a number of different sites; and,
    • b) determining an impedance map using the impedance values at each site.


Typically the method includes, in the processing system:

    • a) determining the presence of an anomaly at any one of the sites; and,
    • b) determining the impedance map taking the anomaly into account.


Typically the method includes, in the processing system, for a site having an anomaly, at least one of:

    • a) excluding the site from the impedance map;
    • b) modifying the impedance value determined for the site.


Typically the method includes, in the processing system:

    • a) determining a difference between the first and second impedance values; and,
    • b) determining the presence, absence or degree of an anomaly using the determined difference.


Typically the method includes, in the processing system:

    • a) determining a difference between the first and second impedance values;
    • b) comparing the difference to a reference; and,
    • c) determining an anomaly depending on the result of the comparison.


Typically the method includes, in the processing system:

    • a) comparing first and second impedance values; and,
    • b) determining the presence, absence or degree of a biological anomaly using the results of the comparison.


Typically the reference in a previously measured difference value for the subject.


Typically the impedance values are at least one of:

    • a) measured impedance values; and,
    • b) impedance parameter values derived from measured impedance values.


Typically the impedance parameter values include at least one of:

    • a) an impedance at infinite applied frequency (R);
    • b) an impedance at zero applied frequency (R0); and,
    • c) an impedance at a characteristic frequency (Zc).


Typically the method includes, in the processing system, determining the impedance parameter values at least in part using the equation:






Z
=


R


+



R
0

-

R




1
+


(

j





ω





τ

)


(

1
-
α

)











    • where: R=impedance at infinite applied frequency;
      • R0=impedance at zero applied frequency;
      • ω=angular frequency;
      • τ is the time constant of a capacitive circuit modelling the subject response; and,
      • α has a value between 0 and 1.





Typically the method includes, in the processing system:

    • a) causing at least one first impedance value to be measured at a site using a first electrode configuration; and,
    • b) causing at least one second impedance value to be measured at the site using a second electrode configuration.


Typically the processing system forms part of a measuring device for performing impedance measurements.


Typically the anomaly includes any one or a combination of:

    • a) a tissue anomaly; and,
    • b) an erroneous measurement.


Typically the tissue anomaly is a tissue lesion.


Typically the impedance measurements are performed using apparatus including an electrode array having a number of electrodes provided thereon, and wherein the method includes, in the processing system, causing impedance measurements to be performed using different ones of the electrodes in the array.


Typically the method includes:

    • a) causing a first measurement to be performed at a site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes; and,
    • b) causing a second measurement to be performed at the site using first and third electrodes as drive electrodes and using second and fourth electrodes as measurement electrodes.


Typically the method includes:

    • a) causing a measurement to be performed at a site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes; and,
    • b) causing a measurement to be performed at a second site using at least two of the first, second, third and fourth electrodes.


Typically the method includes:

    • a) causing a first measurement to be performed at a first site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes;
    • b) causing a second measurement to be performed at the first site using first and third electrodes as drive electrodes and using second and fourth electrodes as measurement electrodes.
    • c) causing a first measurement to be performed at a second site using third and fifth electrodes as drive electrodes and using fourth and sixth electrodes as measurement electrodes; and,
    • d) causing a second measurement to be performed at the second site using third and fourth electrodes as drive electrodes and using fifth and sixth electrodes as measurement electrodes.


Typically the apparatus includes a signal generator for generating drive signals, a sensor for sensing measured signals, and a multiplexer, and wherein the method includes, in the processing system selectively interconnecting the signal generator and the sensor to electrodes in the array using the multiplexer.


In a second broad form the present invention seeks to provide apparatus for use in analysing impedance measurements performed on a subject, the apparatus including a processing system for:

    • a) determining at least one first impedance value, measured at a site using a first electrode configuration;
    • b) determining at least one second impedance value, measured at the site using a second electrode configuration; and,
    • c) determining the presence, absence or degree of an anomaly using the first and second impedance values.


Typically the apparatus includes:

    • a) a signal generator for applying drive signals to the subject using drive electrodes; and,
    • b) a sensor for determining measured signals using measurement electrodes.


Typically the processing system is for:

    • a) causing the signal generator to apply one or more drive signals to the subject; and,
    • b) determining an indication of the measured signals measured using the sensor.


Typically the processing system is for:

    • a) determining an indication of drive signals applied to the subject;
    • b) determining an indication of measured signals determined using the sensor; and,
    • c) using the indications to determine an impedance.


Typically the apparatus includes an electrode array having a number of electrodes provided thereon, and wherein in use, selected ones of the electrodes are used as drive and measurement electrodes.


Typically the processing system is for:

    • a) causing a first measurement to be performed at a site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes; and,
    • b) causing a second measurement to be performed at the site using first and third electrodes as drive electrodes and using second and fourth electrodes as measurement electrodes.


Typically the method includes:

    • a) causing a measurement to be performed at a site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes; and,
    • b) causing a measurement to be performed at a second site using at least two of the first, second, third and fourth electrodes.


Typically the method includes:

    • a) causing a first measurement to be performed at a first site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes;
    • b) causing a second measurement to be performed at the first site using first and third electrodes as drive electrodes and using second and fourth electrodes as measurement electrodes.
    • c) causing a first measurement to be performed at a second site using third and fifth electrodes as drive electrodes and using fourth and sixth electrodes as measurement electrodes; and,
    • d) causing a second measurement to be performed at the second site using third and fourth electrodes as drive electrodes and using fifth and sixth electrodes as measurement electrodes.


Typically the apparatus includes:

    • a) a signal generator for generating drive signals;
    • b) a sensor for sensing measured signals; and,
    • c) a multiplexer, and wherein the processing system is for selectively interconnecting the signal generator and the sensor to electrodes in the array using the multiplexer.


In a third broad form the present invention seeks to provide a method for use diagnosing the presence, absence or degree of a biological anomaly in a subject by using impedance measurements performed on the subject, the method including, in a processing system:

    • a) determining at least one first impedance value, measured at a site using a first electrode configuration;
    • b) determining at least one second impedance value, measured at the site using a second electrode configuration; and,
    • c) determining the presence, absence or degree of an anomaly using the first and second impedance values.


It will be appreciated that the broad forms of the invention may be used individually or in combination, and may be used for diagnosis of the presence, absence or degree of a range of conditions and illnesses, including, but not limited to the detection of lesions, tumours, or the like, as well as to allow impedance mapping to be performed more accurately by accounting for erroneous readings.





BRIEF DESCRIPTION OF THE DRAWINGS

An example of the present invention will now be described with reference to the accompanying drawings, in which:—



FIG. 1 is a schematic of an example of impedance measuring apparatus;



FIG. 2 is a flowchart of an example of a process for performing impedance measurements;



FIG. 3 is a flowchart of a second example of a process for performing impedance measurements;



FIG. 4 is a schematic of a specific example of impedance measuring apparatus;



FIGS. 5A and 5B are a flowchart of an example of a process for performing impedance measurements using the apparatus of FIG. 4;



FIGS. 6A to 6D are schematic diagrams of example tetrapolar electrode configurations;



FIGS. 6E to 6J are schematic diagrams of an example of a sequence of electrode configurations used for performing measurements at multiple sites;



FIG. 7 is a schematic diagram of an example of a region of red blood cells introduced to a plasma to show visible diffusion;



FIG. 8 is a schematic diagram of varying haematocrit value over an area of the electrode array of FIG. 4;



FIG. 9A is a schematic diagram of average R0 maps for haematocrit of 60% and for the tetrapolar electrode arrangements of FIGS. 6A to 6D;



FIG. 9B is a plot of an example of a mean value of R0 for each impedance map of FIG. 9A against haematocrit concentration;



FIG. 10 is a schematic diagram of example impedance maps for plasma with introduced red blood cells in the lower left corner for the tetrapolar electrode arrangements of FIGS. 6A to 6D;



FIG. 11 is a schematic diagram of an example impedance difference map for use in identifying a tissue anomaly;



FIG. 12A is a schematic diagram of example impedance maps for plasma with an introduced red blood cell clot covering a central electrode;



FIG. 12B is a schematic diagram of example impedance maps for plasma with an introduced red blood cell clot covering four electrodes associated with a respective measurement site; and,



FIG. 12C is a schematic diagram of example impedance maps for plasma with an introduced red blood cell clot covering two measurement sites.





DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

An example of apparatus suitable for performing an analysis of a subject's bioelectric impedance will now be described with reference to FIG. 1.


As shown the apparatus includes a measuring device 100 including a processing system 102 coupled to a signal generator 111 and a sensor 112. In use the signal generator 111 and the sensor 112 are coupled to first electrodes 113, 114, and second electrodes 115, 116, provided on a subject S, via respective first leads 123, 124, and second leads 125, 126.


The connection may be via a switching device 118, such as a multiplexer, allowing the leads 123, 124, 125, 126 to be selectively interconnected to signal generator 111 and the sensor 112, although this is not essential, and connections may be made directly between the signal generator 111, the sensor 112 and the electrodes 113, 114, 115, 116.


The processing system 102 typically includes a processor 105, a memory 106, an input/output device 107 such as a keyboard and display, and an external interface 108 coupled together via a bus 109, as shown. The external interface 108 can be used to allow the processing system 102 to be coupled to the signal generator 111 and the sensor 112, as well as to allow connection to one or more peripheral devices (not shown), such as an external database, or the like.


In use, the processing system 102 is adapted to generate control signals, which cause the signal generator 111 to generate one or more alternating drive signals, such as voltage or current signals, which can be applied to a subject S, via two of the electrodes 113, 114, 115, 116 (generally referred to as “drive” electrodes). The sensor 112 then determines measured signals representing the induced voltage across or current through the subject S, using the other two of the electrodes 113, 114, 115, 116 (generally referred to as “measurement” electrodes) and transfers appropriate signals to the processing system 102.


Accordingly, it will be appreciated that the processing system 102 may be any form of processing system which is suitable for generating appropriate control signals and interpreting an indication of the measured signals to thereby determine the subject's bioelectrical impedance, and optionally determine other information such as the presence, absence or degree of oedema, or the like.


The processing system 102 may therefore be a suitably programmed computer system, such as a laptop, desktop, PDA, smart phone or the like. Alternatively the processing system 102 may be formed from specialised hardware, such as an FPGA (field programmable gate array), or a combination of a programmed computer system and specialised hardware, or the like.


In use, the two electrodes 113, 114, 115, 116 that are to be used as drive electrodes are positioned on the subject to allow one or more signals to be injected into the subject S, with two other electrodes 113, 114, 115, 116 being positioned to act as measurement electrodes to allow signals induced within the subject, to be detected. The location of the electrodes will depend on the segment of the subject S under study.


Once the electrodes are positioned, one or more alternating signals are applied to the subject S, via the drive electrodes. The nature of the alternating signal will vary depending on the nature of the measuring device and the subsequent analysis being performed.


For example, the system can use Bioimpedance Analysis (BIA) in which a single low frequency current is injected into the subject S, with the measured impedance being used directly in the identification of anomalies (which can include tissue anomalies, erroneous measurements, or the like), or performing impedance mapping.


In contrast Bioimpedance Spectroscopy (BIS) devices apply signals at a number of frequencies either simultaneously or sequentially. BIS devices typically utilise frequencies ranging from low frequencies (4 kHz) to higher frequencies (1000 kHz), and can use 256 or more different frequencies within this range, to allow multiple impedance measurements to be made within this range.


Thus, the measuring device 100 may either apply an alternating signal at a single frequency, at a plurality of frequencies simultaneously, or may apply a number of alternating signals at different frequencies sequentially, depending on the preferred implementation. The frequency or frequency range of the applied signals may also depend on the analysis being performed.


In one example, the applied signal is a frequency rich current signal from a current source clamped, or otherwise limited, so it does not exceed a maximum allowable subject auxiliary current. However, alternatively, voltage signals may be applied, with a current induced in the subject being measured. The signal can either be constant current, impulse function or a constant voltage signal where the current is measured so it does not exceed the maximum allowable subject auxiliary current.


A potential difference and/or current are measured between the measurement electrodes. The acquired signal and the measured signal will be a superposition of potentials generated by the human body, such as the ECG, and potentials generated by the applied current.


To assist accurate measurement of the impedance, buffer circuits may be placed in connectors that are used to connect the electrodes 113, 114, 115, 116 to the leads 123, 124, 125, 126. This helps eliminate contributions to the measured voltage due to the response of the leads 123, 124, 125, 126, and reduce signal losses.


A further option is for the voltage to be measured differentially, meaning that the sensor used to measure the potential at each measurement electrode only needs to measure half of the potential as compared to a single ended system. In one example, current can also be driven or sourced through the subject S differentially, which again greatly reduced the parasitic capacitances by halving the common-mode current.


The acquired signal is demodulated to obtain the impedance of the system at the applied frequencies. One suitable method for demodulation of superposed frequencies is to use a Fast Fourier Transform (FFT) algorithm to transform the time domain data to the frequency domain. This is typically used when the applied current signal is a superposition of applied frequencies. Another technique not requiring windowing of the measured signal is a sliding window FFT.


In the event that the applied current signals are formed from a sweep of different frequencies, then it is more typical to use a processing technique such as multiplying the measured signal with a reference sine wave and cosine wave derived from the signal generator, or with measured sine and cosine waves, and integrating over a whole number of cycles. This process rejects any harmonic responses and significantly reduces random noise.


Other suitable digital and analog demodulation techniques will be known to persons skilled in the field.


In the case of BIS, impedance or admittance measurements can be determined from the signals at each frequency by comparing the recorded voltage and current signal. This allows demodulation to be used to produce an amplitude and phase signal at each frequency.


An example of the operation of the apparatus to detect anomalies when performing impedance mapping or other impedance measurements will now be described with reference to FIG. 2.


At step 200 a first impedance value is measured at a given site. The impedance value is typically measured using a first electrode configuration, and whilst any form of electrode configuration may be used, this is typically a tetrapolar electrode configuration utilised to allow impedance readings to be measured at the specific site.


At step 210 a second impedance value is measured at the (same) site. This is typically achieved utilising an alternative electrode configuration and in particular, a configuration which is a modified version of the first configuration.


In this regard, the configuration typically utilises the same electrode placements on the subject, but applies the signals to and measures signals from different ones of the electrodes. Thus, for example, in a tetrapolar electrode configuration, the first measurement may be made by applying a current across first electrodes and measuring a voltage across second electrodes, whereas the second measurement may be made by applying the current across the second electrodes and measuring the induced voltage across first electrodes.


At step 220 the first and second impedance values can be used to determine if the measurement made at the site is erroneous. In particular, such a reading will typically arise if a low impedance lesion or other biological anomaly is present between a drive and a measurement electrode pair.


The erroneous measurement (or reading) can then be taken into account when performing analysis of impedance measurements at step 230. For example, the erroneous reading may be used to identify and/or subsequently monitor the development of a low impedance lesion. Thus, this technique can be used to detect the presence, absence or degree of lesions or other biological anomalies. Additionally, and/or alternatively, knowledge of the anomaly can be taken into account when performing analysis of impedance measurements.


Thus, for example, impedance measurements can be performed over a region, such as an area of a subject's skin, to allow impedance mapping or other similar analysis to be performed. As the presence of erroneous readings can have a negative impact on any such impedance mapping process, identification of these erroneous readings allows readings at the corresponding site to be rejected or otherwise modified so that they do not adversely affect the impedance mapping process.


An example of the process for identifying anomalies, including but not limited to tissue anomalies, erroneous readings, or the like will now be described in more detail with respect to FIG. 3.


In particular, at step 300 the signal generator 111 is used to apply a first drive signal to the subject S using a first electrode configuration. Thus for example, the current source 111 may be connected to the leads 123, 124, via the switching device 118, so that the electrodes 113, 114 act as the drive electrodes.


At step 310 a first signal induced across the subject S is measured. This is typically achieved by utilising the switching device 118 to interconnect the remaining measurement electrodes, in this case the electrodes 115, 116, to the sensor 112, thereby allowing signals induced within the subject S to be detected.


At step 320 the processing system 102 utilises an indication of the applied and induced signals to determine a first impedance value. The first impedance value may be formed from one or more measured impedance values. Thus, for example, if a single frequency BIA device is used, a single measured impedance value may be determined, whereas if a BIS device is used, multiple measured values may be determined, with a single value being determined for each applied frequency.


In addition, or alternatively to the impedance values being actual measured values, the impedance values may be based on impedance parameter values derived from the actual measurements. This can include parameter values such as the impedance at zero, characteristic or infinite frequencies (R0, Zc, R), as will be described in more detail below.


At step 330 the processing system 102 controls the switching device 118 to switch to an alternative electrode configuration. In this instance, for example, the electrodes 113, 115 may be used as the drive electrodes with the electrodes 114, 116 being used as measurement electrodes. Any other alternative configuration may also be used, depending on the implementation.


At step 340, a second signal is applied to the subject S using the second electrode configuration, with the induced signal across subject S being measured at step 350. At step 360 the applied and induced signals are processed to determine a second impedance value, which again can be formed from one or more measured impedance values, or parameter values derived therefrom.


At step 370, the processing system 102 uses the first and second impedance values to determine if any tissue anomalies might exist. An erroneous measurement will typically be determined if the difference between the first and second impedance values is greater than a reference amount. The magnitude of this reference may vary depending upon a number of factors and the processing system 102 is therefore typically arranged to compare the difference between the first and second impedance values to a reference value, which can be stored in memory, or the like. The reference value could be previously determined for example based on sample data collected for a nominal reference population, or based on the difference determined for other sites, as will be described in more detail below.


Once detected, this information can be used in one of two ways. For example, the measured values can be used to derive information regarding any associated biological anomaly, such as the presence, absence or degree of any tissue lesion, tumour, or the like, at step 380. Alternatively, at step 390, the erroneous measurement can be taken into account when performing other impedance analysis. Thus, for example, if wound or other impedance mapping is being performed to monitor wound healing, or the like, any erroneous reading can be rejected to ensure that this does not overtly influence the outcome of the analysis. Examples of this will be described in more detail below.


An example of a specific apparatus arrangement for performing impedance measurements, and in particular, for performing impedance mapping, will now be described with reference to FIG. 4.


In particular in this instance an impedance measuring device 400 is connected to a multiplexer 410, which is controlled by a computer system 420, such as a personal computer or the like. In this instance the multiplexer 410 is coupled to an electrode array 430 having a number of electrodes 431 provided thereon.


In use the measuring device 400 generates signals to be applied to the subject via the electrode array with these signals being coupled to respective ones of the electrodes 431 utilising the multiplexer 410. Similarly, signals induced across the subject S can also be returned from electrodes 431 to the impedance measuring device 400 via the multiplexer 410. Overall operation of the multiplexer 410 can be controlled using the computer system 420, allowing this process to be substantially automated.


In one specific example, the measuring device 400 is in the form of an Impedimed Imp SFB7™. The drive and measurement electrodes from the SFB7 can be directed through a multiplexer 410, such as a 32 channel multiplexer (ADG732) from Analog Devices and switching of the multiplexer output channels can be controlled via custom software operating on a standard computer system 420.


In this example, the electrode array 430 includes twenty five, 1 mm diameter electrodes separated by 0.77 mm in a 5×5 square. This allows a total of 64 separate measurements to be taken at 16 different sites giving an impedance map of 49 mm2 on the surface of a subject, which may be an individual, a test medium, or the like. As a result of this, only 25 of the available 32 multiplexer channels are required for this arrangement.


An example of use of the system will now be described with reference to FIG. 5.


At step 500 the electrode array 430 is applied to the subject S, and connected to the multiplexer 410, as described above. At this stage, systems, such as the measuring device 400, the multiplexer 410 and the computer system 420 are activated and configured as required in order to allow the measurement procedure to be performed.


At step 510 the computer system 420 selects a next site for measurement. The electrodes 431 are typically selected so as to form a tetrapolar arrangement, with a group of four electrodes 431 in the array 430 defining the site being measured. An example of this is shown in FIGS. 6A to 6D, in which four electrodes 431A, 431B, 431C, 431D are selectively used as measurement and drive electrodes for a single site.


In this example, four measurements can be made at each site by using the drive and measurement electrode arrangements shown in FIGS. 6A to 6D. Thus, in FIG. 6A, the electrodes 431A, 431B act as the measurement electrodes M1, M2, whereas the electrodes 431C, 431D act as the drive electrodes D1, D2. Successive measurements at the site can be made using different electrode configurations in which the drive and measurement electrodes M1, M2, D1, D2 are used as shown so that the tetrapolar configuration is effectively rotated by 90° for each successive measurement.


To achieve this, at step 520 the measuring device 400 controls the multiplexer 410 to couple the measuring device to the electrodes in accordance with a next one of the electrode configurations for the currently selected tetrapolar array. Thus, for example, for the first measurement, the arrangement shown in FIG. 6A can be used so that the electrodes 431A, 431B act as the measurement electrodes M1, M2, whereas the electrodes 431C, 431D act as the drive electrodes D1, D2.


The measuring device 400 then applies a drive signal to the subject via the selected drive electrodes 431C, 431D, allowing the signal induced across the measurement electrodes 431A, 431B to be measured at step 530. An indication of this measured signal is returned to the measuring device 400, to allow the measuring device 400 to process the voltage and current signals and determine one or more an impedance values.


The impedance values determined will depend on the preferred implementation. For example, in the event that the measuring device 400 is performing BIA, then typically a single impedance value is calculated representing the measured impedance.


In contrast, if the measuring device performs a multiple frequency BIS analysis, as is the case with the SFB7™ device described above, then the impedance value can be based on impedance parameter values, such as values of the impedance at zero, characteristic or infinite frequencies (R0, Zc, R). These values can be derived by the measuring device 400 based on the impedance response of the subject, which at a first level can be modelled using equation (1), commonly referred to as the Cole model:









Z
=


R


+



R
0

-

R




1
+

(

j





ω





τ

)








(
1
)









    • where: R=impedance at infinite applied frequency,
      • R0=impedance at zero applied frequency,
      • ω=angular frequency,
      • τ is the time constant of a capacitive circuit modelling the subject response.





However, the above represents an idealised situation which does not take into account the fact that the cell membrane is an imperfect capacitor. Taking this into account leads to a modified model in which:









Z
=


R


+



R
0

-

R




1
+


(

j





ω





τ

)


(

1
-
α

)









(
2
)









    • where: α has a value between 0 and 1 and can be thought of as an indicator of the deviation of a real system from the ideal model.





The value of the impedance parameters R0 and R may be determined in any one of a number of manners such as by:

    • solving simultaneous equations based on the impedance values determined at different frequencies;
    • using iterative mathematical techniques;
    • extrapolation from a “Wessel plot”;
    • performing a function fitting technique, such as the use of a polynomial function.


It will be appreciated that as an alternative to the analysis being performed by the measuring device 400, the analysis can be performed in part, or in total, by the computer system 420, depending on the preferred implementation.


At step 550, the processing system 420 determines if all electrode configurations for the respective site are complete and if not returns to step 520. In this instance a next electrode configuration is selected, with steps 520 to 550 being repeated for this next electrode configuration. This process can then be repeated until each of the four electrode configurations shown in FIGS. 6A to 6D have been utilised for the current site.


Whilst it is possible to use all four of the indicated electrode configurations for the tetrapolar configuration, this is not essential, and in some circumstances, it is sufficient to use any two or more of the possible configurations. Thus, for example, the configurations used in FIGS. 6A and 6B can be used, in which the tetrapolar electrode configuration is effectively rotated by 90°. This is particularly useful as one drive and measurement electrode is effectively exchanged in the two different configurations, thereby maximising the chance of lesions located between the drive and measurement electrodes from being located, without requiring switching of each of the electrodes.


Furthermore, this arrangement can be used to provide a sequence of drive and measurement electrode configurations that can be used to perform multiple measurements at successive sites, with only a single drive and single measurement electrode being switched between successive measurements. An example of this is shown in FIGS. 6E to 6J.


Once all the electrode configurations are complete for a specific site, the measuring device 400 or the computer system 420 is used to analyse the impedance values and determine if the impedance measurements are indicative of a tissue anomaly. As mentioned above this may be achieved in any one of a number of ways but typically involves examining the difference between measured impedance values. The reason for this is that the impedance measured at a given site should be substantially invariant irrespective of the electrode configuration used. Consequently, any variation in measured impedance values for different electrode configurations indicates that the tissue is non-uniform and in particular that there is likely to be a low impedance lesion situated between the drive electrodes D1, D2 and the measurement electrodes M1, M2.


In this regard, when the electrodes are provided in the arrangement of FIGS. 6A to 6D, there are usually regions of positive sensitivity between the drive electrodes D1, D2 and between the measurement electrodes M1, M2. In addition to this, there are generally regions of negative sensitivity between each pair of drive and measurement electrodes D1, M2 and M1, D2. These size and magnitude of the areas of negative and positive sensitivity will vary depending on the exact electrode configuration.


For negative field region, a lower resistance than the surrounding tissue will result in an increase in measured impedance, whereas a lower resistance in the positive field region will result in a decrease in measured impedance. Example tissue electrical properties as given by Brown, B. H., Tidy, J. A., Boston, K., Blackett, A. D., Smallwood, R. H. and Sharp, F. (2000a). “Relation between tissue structure and imposed electrical current flow in cervical neoplasia,” The Lancet 355: 892-895, are shown in Table 1 below.













TABLE 1







Healthy Tissue Mean (SD)
Cancerous Tissue Mean (SD)



















RE = 19.0 (7.77)
m
RE = 3.85 (2.89)
m


RI = 2.31 (4.04)
m
RI = 6.10 (2.57)
m


C = 1.12 (1.96)
μF/m
C = 1.01 (1.93)
μF/m









Thus, as cancerous tissue generally has a lower resistance, a cancerous lesion between the drive electrodes D1, D2 or between the measurement electrodes M1, M2. will result in a decreased impedance measurement, whereas a lesion between the each pair of drive and measurement electrodes D1, M2 or M1, D2, will result in an increased impedance measurement.


It will therefore be appreciated that examining differences between impedance measurements with different electrode configurations can allow tissue anomalies such as lesions, to be detected.


In one example this is achieved by determining the difference between the impedance values determined using the different electrode configurations, at step 560. The maximum determined difference is then compared to a reference at step 570. The reference, which is typically previously determined and stored in memory of the measuring device 400 or the computer system 420, represents a threshold value so that if the difference between impedance values is greater than the reference, then this indicates that a tissue anomaly is present.


The reference can be determined in any one of a number of ways depending on the preferred implementation. For example, the reference may be determined by studying a number of healthy individuals (individuals without lesions or other biological anomalies) and/or unhealthy individuals (individuals with lesions or other anomalies) and calculating a range of variations between impedance values at a given site. This can be used to provide an indication of typical differences between impedance values for a healthy individual, thereby allowing a threshold to be established for tissue anomalies.


A further alternative is to derive the reference from previous measurements made for the respective individual. For example, if the individual undergoes a medical intervention, such as surgery, or the like, which may result in a lesion forming, then measurements can be made for the individual prior to the intervention, or following initial development of the lesion. This can be used to establish a baseline of differences in impedance values for the individual, either prior to the lesion forming, or following lesion formation. This baseline can then be used as a subject specific reference so that changes in the difference between the impedance values for the individual, can be used to monitor lesion development and/or effectiveness of treatment.


A further option is to determine the reference using a statistical analysis of measurements made for a number of different sites. This could be performed by examining the mean difference for a number of sites over a region, and then calculating the reference based on a value that is a number of standard deviations from the mean. Accordingly, in this instance, an anomaly is identified if the difference for a site is more than a set number of standard deviations from the mean difference value for a number of sites.


In any event, if the reference is exceeded and the result is determined to be indicative of a tissue anomaly at step 580, then the site is identified as a tissue anomaly at step 590. Once this is completed or otherwise, at step 600 the computer system 420 will determine if all sites are complete and if not will return to step 510 to select the next site in the electrode array 430. This will typically involve using the electrodes 631C, 631D and two electrodes in the next column in the array.


This process can be repeated for all of the sites defined by the electrode array 630, allowing an impedance map to be generated at 610. The impedance map can be used to indicate variations in tissue properties, or the like, which in turn can be used for a number of purposes, such as to monitor healing of wounds or the like.


As will be appreciated by persons skilled in the art, being able to identify, and subsequently discount or otherwise account for such tissue anomalies allows improved results to be obtained for impedance mapping processes.


Furthermore, this process can also be used to identify and monitor low impedance lesions, tumours or the like. For example, determining the magnitude of the difference between different impedance values obtained for a given site allows an indication of the severity of the lesion to be determined. By monitoring changes in the difference over time, this allows variations in lesion severity over time to be monitored.


Specific example trials of the process of performing impedance mapping will now be described.


The blood for each trial was collected from the same animal and treated with 70 mg/L of heparin to prevent coagulation. Blood for each measurement was prepared in the same manner by allowing it to cool to room temperature (22° C.) and the red blood cells separated via a centrifuge. The separated red blood cells and plasma could then be mixed in appropriate proportions to obtain the required haematocrit for testing. Samples were also collected and allowed to coagulate, these were used to represent a high impedance tissue medium at R0 due to the small extracellular space.


In a first example, impedance maps were initially established for homogenous haematocrit in an in-vitro environment. To achieve this, bovine blood was used as the conductive medium, with impedance maps being obtained using homogenous samples with a range of haematocrit values (0, 20, 40, 60, 80%).


The impedance maps of R0 measured for blood samples of various haematocrit are shown in FIG. 8. Each measurement location shown was measured using the tetrapolar electrode orientation arrangement described above, at each of the four possible electrode orientations. These four R0 values measured using different electrode orientation were then averaged to produce one R0 map as shown in FIG. 9A.


A plot of mean R0 for each impedance map against haematocrit is shown in FIG. 9B. This highlights that there is a large increase in impedance with haematocrit concentration. The plot follows an exponential trend as expected since the R0 value of a sample with haematocrit of 100% would approach infinity due to the very small extracellular space. The range of haematocrit values has also shown to have a significant and measurable change in R0. This is useful if impedance maps were to be determined with two or more volumes of blood with differing haematocrits.


In a second trial, the electrode array 430 was covered with plasma (haematocrit of 0%) and red blood cells (haematocrit of 100%) injected onto the corner of the electrode array, as shown for example in FIG. 7.


An example of the bioimpedance map of an average value of R0 obtained for each site is shown at 1000 in FIG. 10. The smaller four maps 1001, 1002, 1003, 1004, correspond to the impedance values for R0 measured using respective electrode configurations, as shown for example in FIGS. 6A to 6D.


It is evident from the above examples that bioimpedance maps for haematocrit 0 to 80% result in reasonably consistent values of R0 (standard deviation <3%). The uniform measurements also demonstrate that the remaining 21 electrodes have little effect on the measurements from the 4 electrodes actively involved. Hence these 21 electrodes do not shunt the current between the active drive electrodes.


The bioimpedance map of plasma with introduced cells clearly shows an increase in R0 at the site of the introduced cells, shown in FIG. 10. The R0 value in the lower left corner (95Ω) is much higher than that in the upper right corner (62Ω) which corresponds to that of the homogenous plasma sample. While the resistance in the lower left corner is higher than that of plasma it is less than that obtain for 80 and 60% haematocrit. The reason for this is due to the cells dispersing throughout the plasma (as shown in FIG. 7) effectively reducing the haematocrit of the introduced red blood cell sample.


As shown in this example, the values of R0 determined for the site 1005 differ significantly for the four different orientations, thereby indicating the presence of a biological anomaly at the site 1005.


In this example, the sensitivity region between the two electrodes 431B, 431D is positive for the maps 1002, 1004 resulting in an increased measured impedance if a higher impedance medium is present between the electrodes. This increase in impedance is clearly seen in the maps 1002, 1004. The maps 1001, 1003 on the left show a decrease in impedance because the region between the two electrodes 431B, 431D is of negative sensitivity in this configuration, thereby resulting in a decreased measured impedance when a higher impedance medium is located in the region.


When performing an impedance analysis, the can be taken into account by excluding this site from the larger impedance map, allowing an accurate average to be determined that excludes any anomaly. Alternatively different mechanisms may be used for taking this into account. For example, averaging of the four measured values of R0, at the given site, can reduce the impact of the tissue anomaly. In this regard, the averaged impedance map would be unaffected since the higher and lower measured impedance values effectively average to cancel each other out, so that the R0 value in this region of the larger map is not anomalous.


Alternatively, the impedance of adjacent sites can be used to determine a value for R0 which is unaffected by the tissue anomaly. Thus, for example, examination of the maps 1001, 1002, 1003, 1004 for each tetrapolar configuration highlights that the determined impedance values determined for the site 1005 in the maps 1001, 1003 are similar to those of adjacent sites, whereas the impedance values determined for the site 1005 in the maps 1002, 1004 are significantly different. This implies that the lesion or other tissue anomaly is located between the drive and measurement electrodes for the electrode configurations used in determining the maps 1002, 1004, meaning that these readings are erroneous. Consequently, the impedance value used for the overall impedance map could be based on the impedance values determined for the impedance maps 1001, 1003 as these readings are more likely to be accurate.


This can be performed for example to discount readings that are believed to be anomalous, for example due to errors in the measuring process, poor electrode contact, or the like.


However, more typically the results are used to detect tissue anomalies, such as lesions or the like. Thus, as measurements made using orthogonal electrode orientations at a region of non-homogeneity will produce different measured impedances, whereas a region of homogeneity will produce the same measurements. This allows tissue anomalies, such as lesions, to be identified, and furthermore allows lesion boundaries to be determined.


An example of this will now be described with reference to FIG. 11. For the purpose of this example, the impedance map of plasma with introduced red blood cells shown in FIG. 10 was used. In this example, the smaller maps 1001, 1003 are averaged, as are maps 1002, 1004, with the difference between these resulting maps being shown in the map 1100 of FIG. 11.


In this example, a region 1101 is highlighted which has low positive values of R0, where dispersed blood is present, and this is due to different haematocrits being located under each of these electrode sets. Within this region, the site 1102 has an R0 value of zero due to a high but homogeneous haematocrit sample being located under the electrode set.


In an upper right region 1103 of the impedance map, the average R0 values are close to zero due to the sample under the electrode sets being homogeneous plasma, the red blood cells having not dispersed into this region.


At the site 1105, a large negative value of R0 is present, implying the presence of a tissue anomaly or lesion. The site 1106 is also negative, but not to such a degree. This implies that a tissue anomaly is likely to be present at the site 1105 and that this may extend slightly into the site 1106. Accordingly, it will be appreciated that this not only allows tissue anomalies to be identified, but also allows the extent and/or boundaries of the tissue anomaly to be determined.


In a third example, a clot was introduced to the plasma in place of the red blood cells. FIGS. 12A, to 12C, display typical impedance maps 1200 with clots introduced in various regions on the electrode array. In the example of FIGS. 12A to 12C, the average value of R0 obtained for each site is shown at 1200, with the four smaller maps 1201, 1202, 1203, 1204, corresponding to the impedance values for R0 measured using respective electrode configurations, as shown for example in FIGS. 6A to 6D.


In FIG. 12A, the clot is introduced beneath a central electrode, the location of which is shown at 1210. In FIG. 12B, the clot is located at the site 1220, whilst in the example of FIG. 12C, the clot is provided in the region 1230, encompassing the sites 1231, 1232. These examples show clear impedance changes at the boundaries of the red blood cell clots due to minimal dispersion of red blood cells. This highlights how in practice the process can be used to identify the size of tissue anomalies, such as lesions and monitor their growth or change in shape over time.


It will therefore be appreciated that the above described methods provide techniques for identifying the presence, absence and even extent of tissue anomalies, such as lesions. These anomalies did not appear to alter the resultant impedance map once averaged, meaning that the averaging of results prevents the tissue anomalies being detected. However, this does mean that even in the event that anomalies exist, this avoids the need to remove and discard such measurements.


Thus, the above described techniques provide a non-subjective method for determining lesion size and hence possible biopsy margins.


By using an electrode array coupled to a suitable switching system, this allows measurements to be rapidly performed over an area of the subject. Furthermore, by using only two measurements at each site, this can reduce the number of measurements required at each region and minimise the time taken to acquire an impedance map.


Persons skilled in the art will appreciate that numerous variations and modifications will become apparent. All such variations and modifications which become apparent to persons skilled in the art, should be considered to fall within the spirit and scope that the invention broadly appearing before described.


Thus, for example, it will be appreciated that features from different examples above may be used interchangeably where appropriate. Furthermore, whilst the above examples have focussed on a subject such as a human, it will be appreciated that the measuring device and techniques described above can be used with any subject such as an animal, including but not limited to, primates, livestock, performance animals, such race horses, or the like, as well as to in-vitro samples, or the like.


The above described processes can be used for determining the health status of an individual, including determining the presence, absence or degree of a range of biological anomalies. It will be appreciated from this that whilst the above examples use the term lesion, this is for the purpose of example only and is not intended to be limiting.


Furthermore, whilst the above described examples have focussed on the application of a current signal to allow a voltage to be measured, this is not essential and the process can also be used when applying a voltage signal to allow a currant to be sensed.


The above described impedance maps are determined based on the value of the impedance parameter R0. However, it will be appreciated that impedance maps based on other impedance parameters, such as actual measured impedances, or values of R, Zc, or the like.

Claims
  • 1. Apparatus for use in performing impedance measurements on a subject, the apparatus comprising: a) an electrode array having a number of electrodes configured to form a rectangular array;b) a signal generator for generating signals to be applied to the subject using drive electrodes of the array;c) a sensor for determining measured signals induced across the subject using measurement electrodes of the array;d) a switching device coupled to the electrode array; and,e) a processing system that controls the switching device to selectively interconnect the signal generator and the sensor to the selected ones of the electrodes, which therefore function as drive and measurement electrodes, the processing system configured to control the switching device to: cause a first measurement to be performed at a first site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes;cause a second measurement to be performed at the first site using first and third electrodes as drive electrodes and using second and fourth electrodes as measurement electrodes;determine a presence, absence or degree of an anomaly at the first site using the first and second measurements;cause a third measurement to be performed at a second site using third and fifth electrodes as drive electrodes and using fourth and sixth electrodes as measurement electrodes;cause a fourth measurement to be performed at the second site using third and fourth electrodes as drive electrodes and using fifth and sixth electrodes as measurement electrodes; anddetermine a presence, absence or degree of an anomaly at the second site using the third and fourth measurements.
  • 2. The apparatus according to claim 1, wherein the switching device is a multiplexer.
  • 3. The apparatus according to claim 1, wherein the electrodes in the electrode array are configured to form a square grid.
  • 4. The apparatus according to claim 1, wherein the electrodes have a diameter of approximately 1 mm.
  • 5. The apparatus according to claim 1, wherein the electrode array is configured to form at least one of: a) a 2×2 array;b) a 2×4 array; and,c) a 5×5 array.
  • 6. The apparatus according to claim 1, wherein a spacing between adjacent electrodes is at least one of: a) less than the diameter of the electrodes;b) fixed; and,c) approximately 0.77 mm.
  • 7. The apparatus according to claim 1, wherein the processing system includes a processor, a memory, an input/output device and an external interface coupled together via a bus.
  • 8. The apparatus according to claim 1, wherein the processing system is an FPGA.
  • 9. The apparatus according to claim 1, wherein the processing system: a) determines a first impedance value, measured at a site using a first tetrapolar electrode configuration of drive and measurement electrodes selected from the array;b) causes at least one of the drive electrodes to become a measurement electrode and at least one of the measurement electrodes to become a drive electrode to thereby define a second tetrapolar electrode configuration by controlling the switching device;c) determines a second impedance value, measured at the site using the second electrode configurationd) determines a difference between the first and second impedance values; and,e) determines a presence, absence or degree of an anomaly using the determined difference.
  • 10. The apparatus according to claim 1, wherein the processing system: a) controls the signal generator to apply one or more drive signals to the subject; and,b) receives an indication of the measured signals measured using the sensor.
  • 11. The apparatus according to claim 1, wherein the processing system: a) receives an indication of drive signals applied to the subject;b) receives an indication of measured signals determined using the sensor; and,c) uses the indications to determine an impedance.
  • 12. The apparatus according to claim 1, wherein the processing system controls the switching device to: a) cause a first measurement to be performed at the site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes; and,b) cause a second measurement to be performed at the site using first and third electrodes as drive electrodes and using second and fourth electrodes as measurement electrodes.
  • 13. The apparatus according to claim 1, wherein the processing system controls the switching device to: a) cause a measurement to be performed at a site using first and second electrodes as drive electrodes and using third and fourth electrodes as measurement electrodes; and,b) cause a measurement to be performed at a second site using at least two of the first, second, third and fourth electrodes.
  • 14. The apparatus according to claim 1, wherein the processing system forms part of a measuring device for performing impedance measurements.
  • 15. The apparatus according to claim 9, wherein the processing system: a) determines impedance values at a number of different sites; and,b) determines an impedance map using the impedance values at each site.
  • 16. The apparatus according to claim 15, wherein the processing system selects a different site by controlling the switching device to interconnect the signal generator and sensor to a different combination of four electrodes than used to perform impedance measurements at a previous site.
  • 17. The apparatus according to claim 15, wherein the processing system: a) determines the presence of an anomaly at any one of the sites; and,b) determines the impedance map taking the anomaly into account.
  • 18. The apparatus according to claim 17, wherein the processing system, for any site having an anomaly, at least one of: a) excludes the site from the impedance map;b) modifies the impedance value determined for the site.
  • 19. The apparatus according to claim 18, wherein fluid levels in a region of the body are able to be determined from the impedance map taking into account any erroneous measurements caused by the anomaly.
  • 20. The apparatus according to claim 9, wherein the processing system: a) determines a difference between the first and second impedance values;b) compares the difference to a reference; and,c) determines an anomaly depending on the result of the comparison.
  • 21. The apparatus according to claim 20, wherein the reference is a previously measured difference value for the subject.
Priority Claims (1)
Number Date Country Kind
2007904287 Aug 2007 AU national
US Referenced Citations (204)
Number Name Date Kind
3851641 Toole Dec 1974 A
3866600 Rey Feb 1975 A
4082087 Howson Apr 1978 A
4169463 Piquard Oct 1979 A
4836214 Sramek Jun 1989 A
4890630 Kroll et al. Jan 1990 A
4924875 Chamoun May 1990 A
5020541 Marriott Jun 1991 A
5101828 Welkowitz et al. Apr 1992 A
5184624 Brown et al. Feb 1993 A
5233982 Kohl Aug 1993 A
5272624 Gisser et al. Dec 1993 A
5282840 Hudrlik Feb 1994 A
5284142 Goble et al. Feb 1994 A
5335667 Cha et al. Aug 1994 A
5351697 Cheney et al. Oct 1994 A
5353802 Ollmar Oct 1994 A
5381333 Isaacson et al. Jan 1995 A
5390110 Cheney et al. Feb 1995 A
5421345 Lekholm et al. Jun 1995 A
5423326 Wang et al. Jun 1995 A
5427113 Hiroshi Jun 1995 A
5454377 Dzwonczyk et al. Oct 1995 A
5469859 Tsoglin et al. Nov 1995 A
5526808 Kaminsky Jun 1996 A
5575929 Yu et al. Nov 1996 A
5611351 Sato et al. Mar 1997 A
5615689 Kotler Apr 1997 A
5626146 Barber et al. May 1997 A
5735284 Tsoglin et al. Apr 1998 A
5792073 Keefe Aug 1998 A
5876353 Riff Mar 1999 A
5947910 Zimmet Sep 1999 A
5957861 Combs et al. Sep 1999 A
5964703 Goodman et al. Oct 1999 A
6115626 Whayne et al. Sep 2000 A
6129666 DeLuca et al. Oct 2000 A
6167300 Cherepenin et al. Dec 2000 A
6253100 Zhdanov Jun 2001 B1
6280396 Clark Aug 2001 B1
6308097 Pearlman Oct 2001 B1
6376023 Mori Apr 2002 B1
6432045 Lemperle et al. Aug 2002 B2
6459930 Takehara et al. Oct 2002 B1
6469732 Chang et al. Oct 2002 B1
6472888 Oguma et al. Oct 2002 B2
6501984 Church et al. Dec 2002 B1
6511438 Bernstein et al. Jan 2003 B2
6512949 Combs et al. Jan 2003 B1
6516218 Cheng et al. Feb 2003 B1
6522910 Gregory Feb 2003 B1
6551252 Sackner et al. Apr 2003 B2
6556001 Wiegand Apr 2003 B1
6561986 Baura et al. May 2003 B2
6564079 Cory et al. May 2003 B1
6602201 Hepp et al. Aug 2003 B1
6615077 Zhu et al. Sep 2003 B1
6636754 Baura et al. Oct 2003 B1
6658296 Wong et al. Dec 2003 B1
6725089 Komatsu et al. Apr 2004 B2
6763263 Gregory et al. Jul 2004 B2
6788966 Kenan et al. Sep 2004 B2
6790178 Mault et al. Sep 2004 B1
6807443 Keren Oct 2004 B2
6829501 Nielsen et al. Dec 2004 B2
6829503 Alt Dec 2004 B2
6840907 Brydon Jan 2005 B1
6936012 Wells Aug 2005 B2
6940286 Wang et al. Sep 2005 B2
RE38879 Goodman et al. Nov 2005 E
6980852 Jersey-Willuhn et al. Dec 2005 B2
7065399 Nakada Jun 2006 B2
7079889 Nakada Jul 2006 B2
7096061 Arad Aug 2006 B2
7122012 Bouton et al. Oct 2006 B2
7149573 Wang Dec 2006 B2
7169107 Jersey-Willuhn Jan 2007 B2
7184820 Jersey-Willuhn et al. Feb 2007 B2
7184821 Belalcazar et al. Feb 2007 B2
7186220 Stahmann et al. Mar 2007 B2
7233823 Simond et al. Jun 2007 B2
7251524 Hepp et al. Jul 2007 B1
7288943 Matthiessen et al. Oct 2007 B2
7313435 Nakada et al. Dec 2007 B2
7317161 Fukuda Jan 2008 B2
7336992 Shiokawa Feb 2008 B2
7440796 Woo et al. Oct 2008 B2
7496450 Ortiz Aleman et al. Feb 2009 B2
7603158 Nachman Oct 2009 B2
7603171 Eror et al. Oct 2009 B2
7628761 Gozani et al. Dec 2009 B2
8068906 Chetham Nov 2011 B2
8744564 Ward Jun 2014 B2
20010051774 Littrup Dec 2001 A1
20020022773 Drinan Feb 2002 A1
20020106681 Wexler Aug 2002 A1
20020138019 Wexler Sep 2002 A1
20020183645 Nachaliel Dec 2002 A1
20030004403 Drinan Jan 2003 A1
20030009111 Cory Jan 2003 A1
20030105410 Pearlman Jun 2003 A1
20030120182 Wilkinson et al. Jun 2003 A1
20030173976 Wiegand Sep 2003 A1
20030176808 Masuo Sep 2003 A1
20030216664 Suarez Nov 2003 A1
20040073127 Istvan et al. Apr 2004 A1
20040073130 Bohm Apr 2004 A1
20040116819 Alt Jun 2004 A1
20040181163 Acumen Sep 2004 A1
20040210158 Organ Oct 2004 A1
20040220632 Burnes Nov 2004 A1
20040234113 Miga Nov 2004 A1
20040242989 Zhu Dec 2004 A1
20040243018 Organ Dec 2004 A1
20040260167 Leonhardt Dec 2004 A1
20040267333 Kronberg Dec 2004 A1
20050080460 Wang Apr 2005 A1
20050085743 Hacker et al. Apr 2005 A1
20050177061 Alanen et al. Aug 2005 A1
20050177062 Skrabal et al. Aug 2005 A1
20050201598 Harel Sep 2005 A1
20050215918 Frantz Sep 2005 A1
20050228309 Fisher Oct 2005 A1
20050251062 Choi Nov 2005 A1
20050270051 Yee et al. Dec 2005 A1
20050283091 Kink et al. Dec 2005 A1
20060025701 Kasahara Feb 2006 A1
20060041280 Stahmann et al. Feb 2006 A1
20060052678 Drinan Mar 2006 A1
20060064029 Arad Mar 2006 A1
20060135886 Lippert et al. Jun 2006 A1
20060184060 Belalcazar Aug 2006 A1
20060200033 Keren et al. Sep 2006 A1
20060241513 Hatlestad et al. Oct 2006 A1
20060241719 Foster Oct 2006 A1
20060247543 Cornish Nov 2006 A1
20060258952 Stahmann et al. Nov 2006 A1
20060264776 Stahmann et al. Nov 2006 A1
20060270942 Mcadams Nov 2006 A1
20070007975 Hawkins Jan 2007 A1
20070024310 Tokuno et al. Feb 2007 A1
20070049993 Hofmann et al. Mar 2007 A1
20070156061 Hess Jul 2007 A1
20070188219 Segarra Aug 2007 A1
20070208233 Kovacs Sep 2007 A1
20070246046 Teschner et al. Oct 2007 A1
20070270707 Belalcazar Nov 2007 A1
20080001608 Saulnier Jan 2008 A1
20080027350 Webler Jan 2008 A1
20080051643 Park et al. Feb 2008 A1
20080064981 Gregory Mar 2008 A1
20080139957 Hubbard et al. Jun 2008 A1
20080200802 Bhavaraju et al. Aug 2008 A1
20080221475 Gregory Sep 2008 A1
20080247502 Liao Oct 2008 A1
20080252304 Woo et al. Oct 2008 A1
20080287823 Chetham Nov 2008 A1
20080306400 Takehara Dec 2008 A1
20090018432 He Jan 2009 A1
20090043222 Chetham Feb 2009 A1
20090069708 Hatlestad et al. Mar 2009 A1
20090076410 Libbus et al. Mar 2009 A1
20090082679 Chetham Mar 2009 A1
20090084674 Holzhacker et al. Apr 2009 A1
20090093730 Grassl Apr 2009 A1
20090143663 Chetham Jun 2009 A1
20090209872 Pop Aug 2009 A1
20090216140 Skrabal Aug 2009 A1
20090216148 Freed Aug 2009 A1
20090234244 Tanaka Sep 2009 A1
20090240163 Webler Sep 2009 A1
20090264727 Markowitz Oct 2009 A1
20090264745 Markowitz Oct 2009 A1
20090264791 Gregory Oct 2009 A1
20090275854 Zielinski Nov 2009 A1
20090275855 Zielinski Nov 2009 A1
20090326408 Moon Dec 2009 A1
20100007357 Ammari et al. Jan 2010 A1
20100049077 Sadleir Feb 2010 A1
20100056881 Libbus et al. Mar 2010 A1
20100094160 Eror et al. Apr 2010 A1
20100100003 Chetham et al. Apr 2010 A1
20100106046 Shochat Apr 2010 A1
20100152605 Ward Jun 2010 A1
20100191141 Aberg Jul 2010 A1
20100228143 Teschner et al. Sep 2010 A1
20110034806 Hartov et al. Feb 2011 A1
20110046505 Cornish et al. Feb 2011 A1
20110054344 Slizynski Mar 2011 A1
20110060241 Martinsen et al. Mar 2011 A1
20110082383 Cory et al. Apr 2011 A1
20110208084 Seoane Martinez Aug 2011 A1
20110230784 Slizynski Sep 2011 A2
20110245712 Patterson Oct 2011 A1
20110274327 Wehnes et al. Nov 2011 A1
20110282180 Goldkuhl et al. Nov 2011 A1
20120071772 Chetham Mar 2012 A1
20120165884 Xi Jun 2012 A1
20120238896 Garber et al. Sep 2012 A1
20130102873 Hamaguchi Apr 2013 A1
20130165760 Erlinger et al. Jun 2013 A1
20130165761 De Limon et al. Jun 2013 A1
20140148721 Erlinger May 2014 A1
20140371566 Raymond et al. Dec 2014 A1
Foreign Referenced Citations (49)
Number Date Country
0 339 471 Nov 1989 EP
0 581 073 Feb 1994 EP
0 865 763 Sep 1998 EP
1 078 597 Feb 2001 EP
1 080 686 Mar 2001 EP
1 112 715 Jul 2001 EP
1 118 308 Jul 2001 EP
1 247 487 Oct 2002 EP
1 329 190 Jul 2003 EP
1 353 595 Aug 2008 EP
9119454 Dec 1991 WO
9318821 Sep 1993 WO
9410922 May 1994 WO
9601586 Jan 1996 WO
9711638 Apr 1997 WO
9724156 Jul 1997 WO
9806328 Feb 1998 WO
9833553 Aug 1998 WO
98151211 Nov 1998 WO
9942034 Aug 1999 WO
9948422 Sep 1999 WO
0019886 Apr 2000 WO
0078213 Dec 2000 WO
0127605 Apr 2001 WO
0152733 Jul 2001 WO
02053028 Jul 2002 WO
2004021880 Mar 2004 WO
2004030535 Apr 2004 WO
2004047638 Jun 2004 WO
2004084087 Sep 2004 WO
2004084723 Oct 2004 WO
2005051163 Jun 2005 WO
2005122881 Dec 2005 WO
2006045051 Apr 2006 WO
2006056074 Jun 2006 WO
2007070997 Jun 2007 WO
2007128952 Nov 2007 WO
2008011716 Jan 2008 WO
2009027812 Mar 2009 WO
2009068961 Jun 2009 WO
2009112965 Sep 2009 WO
2010003162 Jan 2010 WO
2010029465 Mar 2010 WO
2010069023 Jun 2010 WO
2010076719 Jul 2010 WO
2011018744 Feb 2011 WO
2011113169 Sep 2011 WO
2011136867 Nov 2011 WO
2014176420 Oct 2014 WO
Non-Patent Literature Citations (24)
Entry
English Translation of CN1180513A published May 6, 1998.
English Translation of CN12336597 published Dec. 1, 1999.
English Translation of CN1329875A published Jan. 9, 2002.
English Translation of JP2001037735 published Feb. 13, 2001.
English Translation of JP2001061804 published Mar. 13, 2001.
English Translation of JP2002502274 published Jan. 22, 2002.
English Translation of JP2003502092 published Jan. 21, 2003.
English Translation of JP2006501892 published Jan. 19, 2006.
English Translation of JP2008502382 published Jan. 31, 2008.
English Translation of JP2010526604 published Aug. 5, 2010.
English Abstract for WO9948422 published Sep. 30, 1999.
English Abstract for WO0152733 published Jul. 26, 2001.
Bernstein, “A new stroke volume equation for thoracic electrical bioimpedance: Theory and rationale,” Critical Care Medicine, 1986, pp. 904-909, vol. 14, No. 10.
Blad and Baldetorp, “Impedance spectra of tumour tissue in comparison with normal tissue; a possible clinical application for electrical impedance tomography,” Physiol. Meas., 1996, pp. A105-A115, vol. 17.
Lorenzo et al., “Determination of Intracelliar Water by Multifrequency Bioelectrical Impedance,” Ann. Nutr. Metab., 1995, pp. 177-184, vol. 39.
Edwards, “A Modified Pseudosection for Resistivity and IP,” Geophysics, Aug. 1977, pp. 1020-1036, vol. 42, No. 5.
Hansen, “On the influence of shape and variations in conductivity of the sample on four-point measurements,” Appl. Sci. Res., 1959, pp. 93-104, Section B, vol. 8.
Igel, “On the Small-Scale Variability of Electrical Soil Properties and its Influence on Geophysical Measurements,” Dissertation, University of Frankfurt, 2007, pp. 1-188.
Kyle et al., “Bioelectrical impedance analysis—part I: review of principals and methods,” Clinical Nutrition, 2004, pp. 1226-1243, vol. 23.
Loke and Barker, “Least-squares deconvolution of apparent resistivity pseudosections,” Geophysics, Nov. Dec. 1995, pp. 1682-1690, vol. 60, No. 6.
McAdams and Jossinet, “Tissue impedance: a historical overview,” Physiol. Meas., 1995, pp. A1-A13, vol. 16.
McEwan and Holder, “Battery powered and wireless Electrical Impedance Tomography Spectroscopy Imaging using Bluetooth,” IFMBE Proceedings, 2007, pp. 798-801, vol. 16.
Roy and Apparao, “Depth of investigation in direct current methods,” Geophysics, Oct. 1971, pp. 943-959, vol. 36, No. 5.
Wilson et al., “Feasibility studies of electrical impedance spectroscopy for monitoring tissue response to photodynamic therapy,” SPIE, May 1998, pp. 69-80, vol. 3247.
Related Publications (1)
Number Date Country
20160089051 A1 Mar 2016 US
Continuations (1)
Number Date Country
Parent 12672893 US
Child 14963018 US