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WO2006001697A2 - Ultrasonic contrast agent detection and imaging by low frequency manipulation of high frequency scattering properties - Google Patents

Ultrasonic contrast agent detection and imaging by low frequency manipulation of high frequency scattering properties Download PDF

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Publication number
WO2006001697A2
WO2006001697A2 PCT/NO2004/000180 NO2004000180W WO2006001697A2 WO 2006001697 A2 WO2006001697 A2 WO 2006001697A2 NO 2004000180 W NO2004000180 W NO 2004000180W WO 2006001697 A2 WO2006001697 A2 WO 2006001697A2
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WO
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Prior art keywords
contrast agent
imaging
high frequency
pulses
ultrasound
Prior art date
Application number
PCT/NO2004/000180
Other languages
French (fr)
Inventor
Bjørn A.J. ANGELSEN
Rune Hansen
Original Assignee
Angelsen Bjoern A J
Rune Hansen
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Filing date
Publication date
Application filed by Angelsen Bjoern A J, Rune Hansen filed Critical Angelsen Bjoern A J
Priority to EP04748756A priority Critical patent/EP1774361A2/en
Priority to PCT/NO2004/000180 priority patent/WO2006001697A2/en
Publication of WO2006001697A2 publication Critical patent/WO2006001697A2/en

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Classifications

    • GPHYSICS
    • G01MEASURING; TESTING
    • G01SRADIO DIRECTION-FINDING; RADIO NAVIGATION; DETERMINING DISTANCE OR VELOCITY BY USE OF RADIO WAVES; LOCATING OR PRESENCE-DETECTING BY USE OF THE REFLECTION OR RERADIATION OF RADIO WAVES; ANALOGOUS ARRANGEMENTS USING OTHER WAVES
    • G01S7/00Details of systems according to groups G01S13/00, G01S15/00, G01S17/00
    • G01S7/52Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00
    • G01S7/52017Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00 particularly adapted to short-range imaging
    • G01S7/52019Details of transmitters
    • G01S7/5202Details of transmitters for pulse systems
    • G01S7/52022Details of transmitters for pulse systems using a sequence of pulses, at least one pulse manipulating the transmissivity or reflexivity of the medium
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01SRADIO DIRECTION-FINDING; RADIO NAVIGATION; DETERMINING DISTANCE OR VELOCITY BY USE OF RADIO WAVES; LOCATING OR PRESENCE-DETECTING BY USE OF THE REFLECTION OR RERADIATION OF RADIO WAVES; ANALOGOUS ARRANGEMENTS USING OTHER WAVES
    • G01S15/00Systems using the reflection or reradiation of acoustic waves, e.g. sonar systems
    • G01S15/88Sonar systems specially adapted for specific applications
    • G01S15/89Sonar systems specially adapted for specific applications for mapping or imaging
    • G01S15/8906Short-range imaging systems; Acoustic microscope systems using pulse-echo techniques
    • G01S15/895Short-range imaging systems; Acoustic microscope systems using pulse-echo techniques characterised by the transmitted frequency spectrum
    • G01S15/8952Short-range imaging systems; Acoustic microscope systems using pulse-echo techniques characterised by the transmitted frequency spectrum using discrete, multiple frequencies
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01SRADIO DIRECTION-FINDING; RADIO NAVIGATION; DETERMINING DISTANCE OR VELOCITY BY USE OF RADIO WAVES; LOCATING OR PRESENCE-DETECTING BY USE OF THE REFLECTION OR RERADIATION OF RADIO WAVES; ANALOGOUS ARRANGEMENTS USING OTHER WAVES
    • G01S7/00Details of systems according to groups G01S13/00, G01S15/00, G01S17/00
    • G01S7/52Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00
    • G01S7/52017Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00 particularly adapted to short-range imaging
    • G01S7/52077Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00 particularly adapted to short-range imaging with means for elimination of unwanted signals, e.g. noise or interference
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01SRADIO DIRECTION-FINDING; RADIO NAVIGATION; DETERMINING DISTANCE OR VELOCITY BY USE OF RADIO WAVES; LOCATING OR PRESENCE-DETECTING BY USE OF THE REFLECTION OR RERADIATION OF RADIO WAVES; ANALOGOUS ARRANGEMENTS USING OTHER WAVES
    • G01S7/00Details of systems according to groups G01S13/00, G01S15/00, G01S17/00
    • G01S7/52Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00
    • G01S7/52017Details of systems according to groups G01S13/00, G01S15/00, G01S17/00 of systems according to group G01S15/00 particularly adapted to short-range imaging
    • G01S7/52023Details of receivers
    • G01S7/52036Details of receivers using analysis of echo signal for target characterisation
    • G01S7/52038Details of receivers using analysis of echo signal for target characterisation involving non-linear properties of the propagation medium or of the reflective target

Definitions

  • This invention relates to methods and systems for ultrasonic detection and imaging of contrast agents located in soft tissue or tissue fluids.
  • Ultrasound contrast agents are typically made as solutions of micro gas bubbles or nano lipid particles.
  • the gas bubbles typically show strong and nonlinear scattering of the ultrasound, a phenomenon that is used to differentiate the contrast agent signal from the tissue signal.
  • the increased scattering from the contrast agent within the transmitted frequency band was used to enhance the scattering from blood.
  • second harmonic components in the nonlinearly scattered signal were used to further enhance the contrast agent signal above the tissue signal in methods generally referred to as nonlinear contrast harmonic imaging.
  • CTR Contrast signal to Tissue signal Ratio. This gives the ratio of the signal power scattered from the contrast agent in a region to the signal power scattered from the tissue in that region. This ratio is often referred to as specificity.
  • CNR Contrast signal to Noise Ratio. This gives the ratio of the signal power scattered from the contrast agent in a region to the noise power in that region. This ratio is often referred to as sensitivity.
  • the CNR determines the maximum depth for imaging the contrast agent while the CTR describes the enhancement of the contrast agent signal above the tissue signal in the image and thus the capability of differentiating contrast signal from tissue signal. High values of both these ratios are therefore necessary for good imaging of the contrast agent.
  • the nonlinear distortion of the signal scattered from the contrast agent is much stronger than for the tissue signal, a phenomenon that is extensively used to enhance the CTR.
  • received tissue signal components in the transmitted frequency band are reduced by- combining the received signal from two transmitted pulses with different amplitudes.
  • the second harmonic band of the nonlinearly scattered signal is obtained either by bandpass filtering or by combining the received signals from two or more transmitted pulses with different polarities.
  • the contrast agent will typically undergo strong nonlinear oscillations with significant amount of energy scattered at higher harmonic components only if driven into oscillations well below its resonance frequency and the harmonic component used for detection and imaging is often obtained in a bandpass filtering process.
  • the drive pulse typically has to be relatively narrowbanded. The consequence of a relatively narrowbanded and low frequency drive pulse is the low image resolution typically obtained with harmonic imaging.
  • the received nonlinear harmonic component from the contrast agent typically has low amplitude which reduces the CNR and may require so high transmitted amplitude that the contrast agent bubbles are destroyed. This can cause a problem when the inflow rate of contrast agent to the tissue region is low.
  • nonlinear contrast components scattered in the forward propagation direction will add in phase with the transmit field and hence accumulate.
  • these nonlinear contrast components may be linearly back-scattered from the tissue and falsely interpreted as contrast agent signal, hence reducing the CTR.
  • a limitation in all methods based on nonlinear harmonic detection is that nonlinear components in the tissue signal are preserved in the process, also limiting the CTR.
  • the new method described does not require nonlinear harmonic imaging and is therefore not constricted by the above mentioned limitations encountered in nonlinear contrast harmonic imaging techniques.
  • Ultrasound pulses containing both a low frequency band and a high frequency band overlapping in the time domain are transmitted towards the ultrasound contrast agent embedded in the tissue.
  • the low frequency components are used to manipulate the acoustic scattering properties of the contrast agent for frequency components in the transmitted high frequency band, and the scattered bubble signal from the high frequency transmitted components is used for image reconstruction.
  • the low frequency components in the received signals can for example be removed through bandpass filtering of the signals around the high frequency band.
  • the tissue signal is suppressed by transmitting at least two such dual-band pulses for each radial image line with different phases and/or amplitudes between the low and high frequency components, and performing a linear combination of the back-scattered signals from the different pulses.
  • the transmitted low frequency pulse will slightly influence the wave propagation of the transmitted high frequency pulse resulting in slightly different high frequency sound speeds when altering the phase and/or amplitude of the low frequency pulses.
  • the resulting echoes may then have to be digitally interpolated and adjusted relative to each other before combination to adequately suppress the high frequency tissue echoes.
  • non-moving, temporary stationary tissue With non-moving, temporary stationary tissue, one can for example transmit two pulses with different phase of the low frequency components and the same phase of the high frequency components, and perform a linear combination of the back- scattered signals from the two pulses.
  • the scattered high frequency components from the contrast bubble will be manipulated differently than from the tissue by the two low frequency pulses of different phases and/or amplitudes, and the bubble signal can be preserved while the tissue signal is heavily suppressed in the combination of the two echoes.
  • the back-scattered signals from these pulses are combined in a pulse to pulse high-pass filter as is commonly done in ultrasound imaging of blood velocities to suppress the tissue signal.
  • Typical filtering schemes that are used are FIR-type filters or orthogonal decomposition using for example Legendre polynomials, with filtering along the pulse number coordinate for each depth.
  • the present invention significantly increases the CNR relative to existing methods by using the total scattered high frequency signal, and in particular the strong linear components, from the contrast agent and not only nonlinear components of it.
  • the present invention can use a more broadbanded transmit pulse and will hence achieve a higher range image resolution.
  • a higher transmit frequency can be used resulting in a significant increase in both lateral and range resolution relative to nonlinear imaging methods.
  • the performance of the present invention is less sensitive to the amplitude of the imaging pulses compared to nonlinear imaging methods. Together with the indicated suppression of received tissue signal with resulting increase in CNR, this facilitates non-destructive detection and imaging of single contrast agent bubbles.
  • FIG.l displays the transfer functions from drive pressure to radial oscillation and to scattered pressure of a contrast bubble undergoing small amplitude oscillations.
  • FIG.2 illustrates transmit pulses containing both a low frequency pulse and a high frequency pulse where the high frequency pulse is placed in the peak positive or peak negative period of the low frequency pulse.
  • FIG.3 shows the radius responses from a bubble with resonance frequency around 4 MHz when driven by the pressure pulses in FIG.2.
  • FIG.4 shows the far-field scattered pressure pulses from a bubble with resonance frequency around 4 MHz when driven by the pressure pulses in FIG.2.
  • FIG.5 depicts the absolute value of the Fourier Transform of the pressure pulses in FIG.4.
  • FIG.6 displays the result obtained by subtracting the two scattered contrast pulses in FIG.4 so that the high frequency tissue components can be suppressed.
  • FIG.7 illustrates the method of digital sampling rate increase (interpolation) .
  • FIG.8 shows a realization of the interpolation process by the use of polyphase filters.
  • FIG.9 shows schematically the adjustment and combination of received echoes done in order to suppress the high frequency tissue components.
  • is the angular frequency and ⁇ 0 is the resonance frequency of the bubble while s is the stiffness of the gas and shell, m is the inertia of the surrounding liquid, and d is a damping factor of the resonant system.
  • H 1 (Q) The absolute value and phase angle of H 1 (Q) is shown in the upper and lower panel in FIG.Ia, respectively.
  • the displacement is ⁇ out of phase with the driving pressure.
  • the bubble responds differently and the displacement and drive pressure are now in phase so that the bubble is increased in size when the drive pressure is positive and vice versa.
  • the displacement is approximately ⁇ /2 out of phase with the drive pressure.
  • the absolute value of the amplitude of the transfer function is seen in the upper panel of FIG.Ia.
  • FIG.Ib displays the absolute value of H 2 (Cl) in the upper panel, while the phase angle of H 2 (Q) is shown in the lower panel.
  • the dashed lines are results obtained setting the parameter d equal to 0.1 while the solid lines are obtained for d equal to 0.5.
  • the amplitude of the scattered pressure as seen from the upper panel in FIG.Ib, significantly increases when going from drive frequencies below resonance towards resonance. For drive frequencies above resonance, the scattered amplitude approaches a constant level. In the lower panel of the figure, we see that for drive frequencies well below resonance, the scattered pressure is in phase with the driving pressure. This means that the bubble oscillation is dominated by s r the stiffness of the gas and shell.
  • the bubble responds differently and the oscillation is now dominated by m, the inertia of the co- oscillating fluid mass.
  • the scattered pressure and drive pressure are now ⁇ out of phase as seen in the lower panel of FIG.Ib.
  • the scattered pressure is approximately ⁇ /2 out of phase with the drive pressure.
  • the purpose of the present invention is to heavily suppress the high frequency tissue echoes in the image while maintaining the total high frequency contrast agent echoes, and the essence of the invention is now described by way of example through applying a simple two-pulse transmit scheme for each radial image line.
  • the high frequency component 202 is placed in the positive peak of the low frequency component 201 as shown in FIG.2a, whereas in the second transmitted pulse, the high frequency component 213 is placed in the negative peak of the low frequency component 212 as shown in FIG.2b.
  • FIG.2a and FIG.2b The difference between FIG.2a and FIG.2b is that the polarity of the transmitted low frequency components is inverted with respect to each other.
  • the phases between the two low frequency pulses may vary with a different value ( ⁇ .O), with possible variation in the amplitude of the low frequency pulses between the two low frequency pulses, even without variation of the phase.
  • FIG.3a shows the radius response from a contrast bubble with resonance frequency around 4 MHz when driven by the pulse in FIG.2a while the radius response from the same bubble when driven by the pulse in FIG.2b is seen in FIG.3b.
  • the high frequency components (202 and 213) in the transmitted pulses are here around 5 MHz and hence chosen to be in the same area as the equilibrium resonance frequency of the contrast bubble. This is, however, done only for purpose of illustration and not a limitation in the present invention. From the bubble radius oscillations, it is seen that the high frequency component in the first transmitted pulse occurs when the bubble is compressed (204) by the low frequency pulse, whereas the high frequency component in the second transmitted pulse occurs when the bubble is expanded (214) by the low frequency pulse. When compressed, the bubble will increase its resonance frequency, while when expanded, it will reduce its resonance frequency.
  • the resulting far-field scattered pressure from the contrast bubble when driven by the incident pressure pulse in FIG.2a is depicted in time domain in FIG.4a and in frequency domain in FIG.5a, while the scattered pressure obtained when driven by the incident pulse in FIG.2b is depicted in time domain in FIG.4b and in frequency domain in FIG.5b.
  • the scattered high frequency fundamental component (209) in FIG.5a is somewhat weaker than the scattered high frequency fundamental component (220) in FIG.5b.
  • Nonlinear scattered high frequency components (210 and 221) are also somewhat different.
  • Scattered low frequency components (207 and 218) have low amplitude and are not meant to be used for image reconstruction. The purpose of the low frequency components is only to manipulate the scattering properties of the contrast agent, i.e. to make the bubble oscillate with such a low frequency that high frequency components can be used to interrogate it while manipulated by the low frequency pulses.
  • the current method of enhancing the contrast agent signal while suppressing the tissue signal will however work in- such a situation also as the main essence is that the high frequency scattering properties of the bubbles are manipulated between transmitted pulses by the low frequency pulses, with limited change of the signal scattered from the tissue.
  • the tissue When the tissue is moving, it may be advantageously to transmit more than two pulses for each radial image line to adequately suppress the received high frequency tissue signal. For example, one can transmit a set of M pulses, all with the same phase and amplitude of the high frequency components, but with different phases and/or amplitiudes of the low frequency components for each pulse.
  • the back- scattered signals from these pulses are combined in a pulse to pulse high-pass filter as is commonly done in ultrasound imaging of blood velocities to suppress the tissue signal.
  • Typical filtering schemes that are used are FIR-type filters or orthogonal decomposition using for example Legendre polynomials, with filtering along the pulse number coordinate for each depth.
  • Ultrasound wave propagation in tissue is hence a weak nonlinear process for intensities commonly applied in medical imaging. Due to the nonlinear tissue elasticity, the high frequency components of the two dual-band pulses displayed in FIG.2 can have slightly different propagation velocities.
  • the high frequency component (202) in FIG.2a occurring during the positive pressure swing of the low frequency component, will travel with a slightly higher sound speed than the high frequency component (213) in FIG.2b, occurring during the negative pressure swing of the low frequency component.
  • C 0 equal to 1500 m/s
  • FIG.7 displays schematically an interpolation method of sampling rate increase by a factor of J.
  • the interpolation is here done by first introducing I - 1 zeros between each sample in the original sequence x(n) with a sampling rate of F x to obtain the desired sampling rate IF x .
  • the sequence v(m) is then passed through a lowpass filter h (m) to obtain the desired output y(m) and this lowpass filter is typically implemented as a linear phase FIR-type filter where the z-transform of the filter is defined as
  • This set of smaller filters are usually called polyphase filters and have unit sample responses
  • the polyphase filters perform the computations at the original low sampling rate F x and the rate conversion results from the fact that I output samples are generated, one from each of the filters, for each input sample. Interpolation by use of polyphase filters are shown schematically in FIG.8.
  • the polyphase filters are arranged as a parallel realization and the output of each filter is selected by a commutator rotating in the counterclockwise direction.
  • the decomposition of h(m) into the set of I subfilters with impulse responses g k ⁇ m) results in filtering of the input samples x(n) by a periodically time-varying linear filter g(m,k) .
  • FIG.9 shows schematically the adjustment and combination process done to suppress the received high frequency tissue signal components.
  • the received echoes are first temporally interpolated and given a variable time adjustment (901) before the pulse to pulse combination (902) to heavily suppress the high frequency tissue components.
  • the time delay effect of this variation in propagation velocity of the high frequency pulse is an integrating effect along the beam depth.
  • the phase between the high and the low frequency pulses may even vary in sign along the beam depth for the same transmit pulse, as described above.
  • the induced variation of the high frequency pulse propagation velocity by the low frequency pulse has less total effect on the delay of the high frequency pulses between different transmissions, compared to when the phase between the high and the low frequency components stays fairly constant along the beam.
  • the separated contrast agent image is typically shown as an overlay with different color or pattern of the standard tissue image as obtained with only one of the transmit pulses for each radial image line.
  • a weak tissue background in the ultrasound image can be obtained by using inaccurate or no time adjustments of the high frequency pulses with different phases of the low frequency pulses. Some of the tissue signal power can thus be brought to partly pass through the high pass filter for tissue signal cancellation.

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Description

Ultrasonic Contrast Agent Detection and Imaging by Low Frequency Manipulation of High Frequency Scattering Properties
Field of invention
This invention relates to methods and systems for ultrasonic detection and imaging of contrast agents located in soft tissue or tissue fluids.
Background
Ultrasound contrast agents are typically made as solutions of micro gas bubbles or nano lipid particles. The gas bubbles typically show strong and nonlinear scattering of the ultrasound, a phenomenon that is used to differentiate the contrast agent signal from the tissue signal. In the earliest applications (~1985) the increased scattering from the contrast agent within the transmitted frequency band was used to enhance the scattering from blood. Later, second harmonic components in the nonlinearly scattered signal were used to further enhance the contrast agent signal above the tissue signal in methods generally referred to as nonlinear contrast harmonic imaging.
The following two signal power ratios have vital importance for the quality of performance of a contrast imaging system:
CTR— Contrast signal to Tissue signal Ratio. This gives the ratio of the signal power scattered from the contrast agent in a region to the signal power scattered from the tissue in that region. This ratio is often referred to as specificity.
CNR— Contrast signal to Noise Ratio. This gives the ratio of the signal power scattered from the contrast agent in a region to the noise power in that region. This ratio is often referred to as sensitivity.
The CNR determines the maximum depth for imaging the contrast agent while the CTR describes the enhancement of the contrast agent signal above the tissue signal in the image and thus the capability of differentiating contrast signal from tissue signal. High values of both these ratios are therefore necessary for good imaging of the contrast agent.
The nonlinear distortion of the signal scattered from the contrast agent is much stronger than for the tissue signal, a phenomenon that is extensively used to enhance the CTR. In one method, received tissue signal components in the transmitted frequency band (linear components) are reduced by- combining the received signal from two transmitted pulses with different amplitudes. In other methods, the second harmonic band of the nonlinearly scattered signal is obtained either by bandpass filtering or by combining the received signals from two or more transmitted pulses with different polarities.
The contrast agent will typically undergo strong nonlinear oscillations with significant amount of energy scattered at higher harmonic components only if driven into oscillations well below its resonance frequency and the harmonic component used for detection and imaging is often obtained in a bandpass filtering process. To obtain distinct scattered harmonic components, the drive pulse typically has to be relatively narrowbanded. The consequence of a relatively narrowbanded and low frequency drive pulse is the low image resolution typically obtained with harmonic imaging.
Also, the received nonlinear harmonic component from the contrast agent typically has low amplitude which reduces the CNR and may require so high transmitted amplitude that the contrast agent bubbles are destroyed. This can cause a problem when the inflow rate of contrast agent to the tissue region is low.
In addition, nonlinear contrast components scattered in the forward propagation direction will add in phase with the transmit field and hence accumulate. In tissue regions beyond a contrast filled area, these nonlinear contrast components may be linearly back-scattered from the tissue and falsely interpreted as contrast agent signal, hence reducing the CTR. Finally, a limitation in all methods based on nonlinear harmonic detection is that nonlinear components in the tissue signal are preserved in the process, also limiting the CTR.
The new method described does not require nonlinear harmonic imaging and is therefore not constricted by the above mentioned limitations encountered in nonlinear contrast harmonic imaging techniques.
Summary of the Invention
Ultrasound pulses containing both a low frequency band and a high frequency band overlapping in the time domain, are transmitted towards the ultrasound contrast agent embedded in the tissue. The low frequency components are used to manipulate the acoustic scattering properties of the contrast agent for frequency components in the transmitted high frequency band, and the scattered bubble signal from the high frequency transmitted components is used for image reconstruction. The low frequency components in the received signals can for example be removed through bandpass filtering of the signals around the high frequency band.
The tissue signal is suppressed by transmitting at least two such dual-band pulses for each radial image line with different phases and/or amplitudes between the low and high frequency components, and performing a linear combination of the back-scattered signals from the different pulses.
Due to nonlinear tissue elasticity, the transmitted low frequency pulse will slightly influence the wave propagation of the transmitted high frequency pulse resulting in slightly different high frequency sound speeds when altering the phase and/or amplitude of the low frequency pulses. The resulting echoes may then have to be digitally interpolated and adjusted relative to each other before combination to adequately suppress the high frequency tissue echoes.
With non-moving, temporary stationary tissue, one can for example transmit two pulses with different phase of the low frequency components and the same phase of the high frequency components, and perform a linear combination of the back- scattered signals from the two pulses. The scattered high frequency components from the contrast bubble will be manipulated differently than from the tissue by the two low frequency pulses of different phases and/or amplitudes, and the bubble signal can be preserved while the tissue signal is heavily suppressed in the combination of the two echoes.
When the tissue is moving, one may have to transmit more than two pulses for each radial image line to adequately suppress the received tissue signal. For example, one can transmit a set of M pulses, all with the same phase of the high frequency components, but with different phases and/or amplitude of the low frequency components for each pulse. The back-scattered signals from these pulses are combined in a pulse to pulse high-pass filter as is commonly done in ultrasound imaging of blood velocities to suppress the tissue signal.
With electronic steering of the beam direction one would use the same beam direction and focus for all the pulses that are combined to suppress the tissue signal for each radial image line. Typical filtering schemes that are used are FIR-type filters or orthogonal decomposition using for example Legendre polynomials, with filtering along the pulse number coordinate for each depth.
With mechanical scanning of the beam direction, as with annular arrays, one would typically transmit pulses with variations in the phase and/or amplitude of the low frequency components as the beam direction is swept continuously, feeding the signal for each depth to a high pass filter along the pulse number coordinate. The outputs of the high pass filters are then sampled for each depth and radial image line to give the contrast agent signal, with suppresion of the tissue signal, to be used for image reconstruction.
The present invention significantly increases the CNR relative to existing methods by using the total scattered high frequency signal, and in particular the strong linear components, from the contrast agent and not only nonlinear components of it.
Relative to nonlinear harmonic imaging methods, the present invention can use a more broadbanded transmit pulse and will hence achieve a higher range image resolution. In addition, a higher transmit frequency can be used resulting in a significant increase in both lateral and range resolution relative to nonlinear imaging methods.
The performance of the present invention is less sensitive to the amplitude of the imaging pulses compared to nonlinear imaging methods. Together with the indicated suppression of received tissue signal with resulting increase in CNR, this facilitates non-destructive detection and imaging of single contrast agent bubbles. Brief Description of the Drawings
FIG.l displays the transfer functions from drive pressure to radial oscillation and to scattered pressure of a contrast bubble undergoing small amplitude oscillations. FIG.2 illustrates transmit pulses containing both a low frequency pulse and a high frequency pulse where the high frequency pulse is placed in the peak positive or peak negative period of the low frequency pulse. FIG.3 shows the radius responses from a bubble with resonance frequency around 4 MHz when driven by the pressure pulses in FIG.2. FIG.4 shows the far-field scattered pressure pulses from a bubble with resonance frequency around 4 MHz when driven by the pressure pulses in FIG.2. FIG.5 depicts the absolute value of the Fourier Transform of the pressure pulses in FIG.4. FIG.6 displays the result obtained by subtracting the two scattered contrast pulses in FIG.4 so that the high frequency tissue components can be suppressed. FIG.7 illustrates the method of digital sampling rate increase (interpolation) . FIG.8 shows a realization of the interpolation process by the use of polyphase filters. FIG.9 shows schematically the adjustment and combination of received echoes done in order to suppress the high frequency tissue components.
Description of Embodiments of the Invention
The invention will now be described in more detail with reference to the figures.
For small amplitude radius excursions, the mathematical equations governing contrast bubble oscillation can be linearized and we obtain the following transfer function from incident pressure on the bubble surface to radial bubble displacement
#,(Ω)= l Qr -1-iΩd
where (1)
Figure imgf000006_0001
Here, ω is the angular frequency and ω0 is the resonance frequency of the bubble while s is the stiffness of the gas and shell, m is the inertia of the surrounding liquid, and d is a damping factor of the resonant system.
The absolute value and phase angle of H1(Q) is shown in the upper and lower panel in FIG.Ia, respectively. In the lower panel, we see that for drive frequencies well below resonance the displacement is π out of phase with the driving pressure. For frequencies well above resonance the bubble responds differently and the displacement and drive pressure are now in phase so that the bubble is increased in size when the drive pressure is positive and vice versa. Around resonance the displacement is approximately π/2 out of phase with the drive pressure. The absolute value of the amplitude of the transfer function is seen in the upper panel of FIG.Ia. Going from frequencies below resonance towards resonance the amplitude increases gradually culminating with a prominent peak around resonance for the situation with low damping (dashed line, d = 0.1) and a considerable smaller peak for the situation with higher damping (solid line, d = 0.5) . In both cases, the amplitude decreases rapidly above resonance.
The transfer function from incident pressure on the bubble surface to scattered far-field pressure for this small amplitude linearized situation is
Ω2 H2(O)=
(2) FIG.Ib displays the absolute value of H2(Cl) in the upper panel, while the phase angle of H2(Q) is shown in the lower panel. As previously, the dashed lines are results obtained setting the parameter d equal to 0.1 while the solid lines are obtained for d equal to 0.5. The amplitude of the scattered pressure, as seen from the upper panel in FIG.Ib, significantly increases when going from drive frequencies below resonance towards resonance. For drive frequencies above resonance, the scattered amplitude approaches a constant level. In the lower panel of the figure, we see that for drive frequencies well below resonance, the scattered pressure is in phase with the driving pressure. This means that the bubble oscillation is dominated by sr the stiffness of the gas and shell. For frequencies well above resonance, the bubble responds differently and the oscillation is now dominated by m, the inertia of the co- oscillating fluid mass. The scattered pressure and drive pressure are now π out of phase as seen in the lower panel of FIG.Ib. Around resonance the scattered pressure is approximately π/2 out of phase with the drive pressure.
The purpose of the present invention is to heavily suppress the high frequency tissue echoes in the image while maintaining the total high frequency contrast agent echoes, and the essence of the invention is now described by way of example through applying a simple two-pulse transmit scheme for each radial image line.
In the first transmitted dual-band pulse, the high frequency component 202 is placed in the positive peak of the low frequency component 201 as shown in FIG.2a, whereas in the second transmitted pulse, the high frequency component 213 is placed in the negative peak of the low frequency component 212 as shown in FIG.2b. The difference between FIG.2a and FIG.2b is that the polarity of the transmitted low frequency components is inverted with respect to each other. In other example embodiments according to the invention, the phases between the two low frequency pulses may vary with a different value (≠.O), with possible variation in the amplitude of the low frequency pulses between the two low frequency pulses, even without variation of the phase.
FIG.3a shows the radius response from a contrast bubble with resonance frequency around 4 MHz when driven by the pulse in FIG.2a while the radius response from the same bubble when driven by the pulse in FIG.2b is seen in FIG.3b. The high frequency components (202 and 213) in the transmitted pulses are here around 5 MHz and hence chosen to be in the same area as the equilibrium resonance frequency of the contrast bubble. This is, however, done only for purpose of illustration and not a limitation in the present invention. From the bubble radius oscillations, it is seen that the high frequency component in the first transmitted pulse occurs when the bubble is compressed (204) by the low frequency pulse, whereas the high frequency component in the second transmitted pulse occurs when the bubble is expanded (214) by the low frequency pulse. When compressed, the bubble will increase its resonance frequency, while when expanded, it will reduce its resonance frequency.
From FIG.Ia we see that both the amplitude and phase angle of the radius oscillation will change for a given drive frequency when changing the resonance frequency of the bubble.
The resulting far-field scattered pressure from the contrast bubble when driven by the incident pressure pulse in FIG.2a is depicted in time domain in FIG.4a and in frequency domain in FIG.5a, while the scattered pressure obtained when driven by the incident pulse in FIG.2b is depicted in time domain in FIG.4b and in frequency domain in FIG.5b. The scattered high frequency fundamental component (209) in FIG.5a is somewhat weaker than the scattered high frequency fundamental component (220) in FIG.5b. Nonlinear scattered high frequency components (210 and 221) are also somewhat different. Scattered low frequency components (207 and 218) have low amplitude and are not meant to be used for image reconstruction. The purpose of the low frequency components is only to manipulate the scattering properties of the contrast agent, i.e. to make the bubble oscillate with such a low frequency that high frequency components can be used to interrogate it while manipulated by the low frequency pulses.
From FIG.Ib we notice that both the amplitude and phase angle of the scattered pressure will vary for a given drive frequency when varying the resonance frequency as done when manipulating the bubble by the low frequency pulses.
To suppress the tissue signal the two scattered pressure pulses in FIG.4 are then subtracted and the result is depicted in time domain in FIG.6a. In FIG.6b, we see the spectrum of the resulting pulse. We notice that even if the two high frequency drive pulses in FIG.2 occur at the exact same relative time from the pulse start, due to the manipulation by the low frequency pulses, the scattered high frequency energy from the bubble is not canceled or significantly reduced in the subtraction process of the two bubble echoes. We may thus utilize the total scattered high frequency energy from the bubble for image reconstruction and not only a nonlinear component of it as done in all non¬ destructive nonlinear contrast agent detection techniques.
It is also possible to use two transmit pulses where one of the transmit pulses only contains the high frequency imaging pulse whereas the other transmit pulse contains both the manipulating low frequency pulse and the high frequency imaging pulse overlapping in the time domain. This would then be a version of amplitude modulation for the low frequency transmit pulse, as described above. Other variations of the phase and/or the amplitude between the two low frequency pulses are also possible. Due to the large separation in frequency of the low and high frequency pulses, one might use separate transducer elements to transmit the two pulse components. If the low and high frequency transducer elements have different spatial positions, the phase between the high and low frequency pulses can vary with depth. The current method of enhancing the contrast agent signal while suppressing the tissue signal, will however work in- such a situation also as the main essence is that the high frequency scattering properties of the bubbles are manipulated between transmitted pulses by the low frequency pulses, with limited change of the signal scattered from the tissue.
When the tissue is moving, it may be advantageously to transmit more than two pulses for each radial image line to adequately suppress the received high frequency tissue signal. For example, one can transmit a set of M pulses, all with the same phase and amplitude of the high frequency components, but with different phases and/or amplitiudes of the low frequency components for each pulse. The back- scattered signals from these pulses are combined in a pulse to pulse high-pass filter as is commonly done in ultrasound imaging of blood velocities to suppress the tissue signal.
With electronic steering of the beam direction one would use the same beam direction and focus for all the pulses that are combined to suppress the tissue signal for each radial image line of the contrast agent image. Typical filtering schemes that are used are FIR-type filters or orthogonal decomposition using for example Legendre polynomials, with filtering along the pulse number coordinate for each depth.
With mechanical scanning of the beam direction, as with annular arrays, one would typically transmit pulses with variations in the phase and/or amplitude of the low frequency components as the beam direction is swept continuously, using the signal for each depth as inputs to high pass filters along the pulse number coordinate, as is commonly done in Doppler blood velocity imaging. The outputs of the high pass filters are then sampled for each depth and radial image line to give the contrast agent signal, with suppression of the tissue signal, to be used for image reconstruction of the contrast agent image.
Acoustic wave propagation is in the linear regime governed by the linear wave equation where the speed of sound is defined as
1 C0 = \pκ
where p is the density and K is the compressibility of the propagation medium. Due to nonlinear tissue elasticity we get, based on a plane wave approximation, a nonlinear propagation velocity that depends on the wave pressure as
Figure imgf000010_0001
where β is a non-linearity parameter accounting for nonlinear intermolecular forces in the propagation medium and p is the acoustic pressure. The last approximation is valid for the case when Kp «\ . In medical ultrasound imaging, Kp typically
lies in the range from 2-10" to 2-10~ whereas β is around 5.
Ultrasound wave propagation in tissue is hence a weak nonlinear process for intensities commonly applied in medical imaging. Due to the nonlinear tissue elasticity, the high frequency components of the two dual-band pulses displayed in FIG.2 can have slightly different propagation velocities. The high frequency component (202) in FIG.2a, occurring during the positive pressure swing of the low frequency component, will travel with a slightly higher sound speed than the high frequency component (213) in FIG.2b, occurring during the negative pressure swing of the low frequency component. Using Eq.12 with C0 equal to 1500 m/s, we get a typical sound speed of 1500.5 m/s for the transmitted high frequency component in FIG.2a and 1499.5 m/s for the high frequency component in FIG.2b.
The consequence of this difference in sound speed is that the two resulting high frequency echoes obtained from the indicated transmit pulses may have to be slightly time- shifted relative to each other before combined to adequately suppress the tissue echoes. These time-shifts are typically smaller than the sampling interval of the signal which requires interpolation for adequately accurate signal values. FIG.7 displays schematically an interpolation method of sampling rate increase by a factor of J. The interpolation is here done by first introducing I - 1 zeros between each sample in the original sequence x(n) with a sampling rate of Fx to obtain the desired sampling rate IFx .
Mathematically, the resulting sequence can be described as
oo v(m)= ∑x(m/ϊ) for m= 0,±I,+2I,... and m=-∞ v(m)=0 otherwise
The sequence v(m) is then passed through a lowpass filter h (m) to obtain the desired output y(m) and this lowpass filter is typically implemented as a linear phase FIR-type filter where the z-transform of the filter is defined as
M-I H(Z)= ∑h(k)z"k k=0
for a filter of length M.
The direct-form realization of the interpolation algorithm is computationally not very efficient due to all the zeros in the sequence v(m) . To increase the efficiency, the filter h (m) can be divided into a set of smaller filters of length K=MII, where M is selected to be a multiple of I. This set of smaller filters are usually called polyphase filters and have unit sample responses
gk(m)=h(k+ml) for k=0,1,...,/-1 and W=0,1,...,.K-I
Thus, the polyphase filters perform the computations at the original low sampling rate Fx and the rate conversion results from the fact that I output samples are generated, one from each of the filters, for each input sample. Interpolation by use of polyphase filters are shown schematically in FIG.8. Here, the polyphase filters are arranged as a parallel realization and the output of each filter is selected by a commutator rotating in the counterclockwise direction. The decomposition of h(m) into the set of I subfilters with impulse responses gk{m) results in filtering of the input samples x(n) by a periodically time-varying linear filter g(m,k) .
FIG.9 shows schematically the adjustment and combination process done to suppress the received high frequency tissue signal components. The received echoes are first temporally interpolated and given a variable time adjustment (901) before the pulse to pulse combination (902) to heavily suppress the high frequency tissue components.
One should note that the time delay effect of this variation in propagation velocity of the high frequency pulse is an integrating effect along the beam depth. With spatially offset between the transducer elements for the low and the high frequency pulses, the phase between the high and the low frequency pulses may even vary in sign along the beam depth for the same transmit pulse, as described above. In this case, the induced variation of the high frequency pulse propagation velocity by the low frequency pulse has less total effect on the delay of the high frequency pulses between different transmissions, compared to when the phase between the high and the low frequency components stays fairly constant along the beam. The separated contrast agent image is typically shown as an overlay with different color or pattern of the standard tissue image as obtained with only one of the transmit pulses for each radial image line.
A weak tissue background in the ultrasound image can be obtained by using inaccurate or no time adjustments of the high frequency pulses with different phases of the low frequency pulses. Some of the tissue signal power can thus be brought to partly pass through the high pass filter for tissue signal cancellation.

Claims

ClaimsWe claim:
1. A method for detection and imaging of ultrasound contrast agent in a region of soft tissue, where
at least one ultrasound pulse containing frequency components in separated low and high frequency bands, is transmitted toward said region,
- the time signals of said low and high frequency components are overlapping in time, so that said transmitted low frequency components are used to manipulate the acoustic scattering properties of the contrast agent for the incident frequency components in said high frequency band,
- where the scattered signal from said transmitted high frequency components is used for ultrasound contrast image reconstruction of said region.
2. A method for detection and imaging of ultrasound contrast agent according to Claim 1, where to reduce the low frequency components in the received signal before image reconstruction, the received signal is filtered in range to attenuate the low frequency components.
3. A method for detection and imaging of ultrasound contrast agent according to Claim 1, where,
at least two ultrasound pulses are transmitted consecutively toward said region with substantially same focus and direction of the ultrasound beam,
- the phase and/or the amplitude of said low frequency components in said pulses is changed for each transmitted pulse,
- the received signal from the consecutive pulses are for each depth combined to suppress tissue signal components, while the signal components from the contrast agent are to a large degree presereved for imaging of the contrast agent.
4. A method for detection and imaging of ultrasound contrast agent according to Claim 3, where,
- the ultrasound beam direction is scanned in steps, and for each radial image line a group of pulses is transmitted, each pulse with differences in the phase and/or amplitude of said low frequency components, - the back-scattered signal is sampled as a function of depth for each pulse and the samples for each depth are combined linearly along the pulse number coordinate,
- the linear combination for each depth being selected so that the received high frequency components from the tissue are heavily suppressed, while the received high frequency components from the contrast agent are not significantly suppressed by the linear combination,
- so that the output of the linear combination is used to form the image of the contrast agent for each depth along said radial image line.
5. A method for imaging and detection of ultrasound contrast agent according to Claim 1, where,
- multiple ultrasound pulses are transmitted consecutively while the ultrasound beam direction is swept continuously over the region to be imaged,
- the phase and/or amplitude of said low frequency components of the transmitted pulses being changed for each transmitted pulse,
- the received signal being sampled in depth along the beam direction, and the samples used as input to high-pass filters operating along the pulse number coordinate for each depth,
- the output of the high-pass filters for each depth being sampled at defined radial image lines to be used for construction of the contrast agent image as a function of depth along said radial image lines.
6. A method for imaging and detection of ultrasound contrast agent according to Claim 3 or 5, where the received signals from the consecutive pulses are digitally interpolated and temporally adjusted relative to each other before combination to adequately suppress the high frequency tissue components.
7. A method for imaging and detection of ultrasound contrast agent according to Claim 3 or 5, where in said transmitted pulses the amplitude of said high frequency bands may be separately adjusted.
8. A method for imaging and detection of ultrasound contrast agent according to Claim 3 or 5, where in said transmitted pulses the amplitude of said low frequency bands may be separately adjusted.
9. A method for imaging and detection of ultrasound contrast agent according to Claim 1, where the resulting contrast agent image is shown as an overlay on the resulting tissue image with a different intensity, color, or pattern.
10. A method for imaging and detection of ultrasound contrast agent according to Claim 6, where the temporal adjustment is done so that a part of the received high frequency tissue signal remains after the combination and is shown as a weak tissue image overlayed by the contrast agent image.
PCT/NO2004/000180 2004-06-18 2004-06-18 Ultrasonic contrast agent detection and imaging by low frequency manipulation of high frequency scattering properties WO2006001697A2 (en)

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WO2008016992A1 (en) 2006-08-01 2008-02-07 Scimed Life Systems, Inc. Pulse inversion sequences for nonlinear imaging

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EP0770352B1 (en) * 1995-10-10 2004-12-29 Advanced Technology Laboratories, Inc. Ultrasonic diagnostic imaging with contrast agents
GB9800813D0 (en) * 1998-01-16 1998-03-11 Andaris Ltd Improved ultrasound contrast imaging method and apparatus
US6440075B1 (en) * 2000-10-02 2002-08-27 Koninklijke Philips Electronics N.V. Ultrasonic diagnostic imaging of nonlinearly intermodulated and harmonic frequency components
US6953434B2 (en) * 2002-09-24 2005-10-11 Ge Medical Systems Global Technology Company, Llc Method and apparatus to enhance ultrasound contrast imaging using stepped-chirp waveforms

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