Magnetic resonance with time sequential spin excitation

Information

  • Patent Grant
  • 7852084
  • Patent Number
    7,852,084
  • Date Filed
    Tuesday, April 3, 2007
    17 years ago
  • Date Issued
    Tuesday, December 14, 2010
    13 years ago
Abstract
In a magnetic resonance scanner, a main magnet (20, 22) generates a static magnetic field at least in an examination region. A magnetic field gradient system (30, 54) selectively superimposes magnetic field gradients on the static magnetic field at least in the examination region. A magnetic resonance excitation system (36, 36′) includes at least one radio frequency coil (30, 301, 302, 303) arranged to inject radio frequency B1 fields into the examination region and at least two radio frequency amplifiers (38, 40, 40′) coupled with different input ports of the at least one radio frequency coil. A controller (66, 70) controls the magnetic resonance excitation system to produce a time varying spatial B1 field distribution in a subject (16) in the examination region that time integrates to define a spatial tip angle distribution in the subject having reduced spatial non uniformity.
Description

The present application relates to the magnetic resonance arts. It particularly relates to reducing spatial non-uniformity in magnetic resonance applications due to coil B1 non-uniformity at ultra high field due to dielectric and conductivity effects by a subject, and is described with particular reference thereto. The following relates more generally to reducing spatial non-uniformity in magnetic resonance applications generally, such as due to coil loading, equipment imperfections, static (B0) magnetic field non-uniformity, dielectric or eddy current effects, or so forth.


Radio frequency coils for use in magnetic resonance scanners are typically configured to produce a substantially uniform B1 field within an examination region in the unloaded condition. That is, the radio frequency coil produces a substantially uniform B1 field without a subject arranged in the examination region. Ideally, a subject placed in the examination region will therefore experience a substantially spatially uniform B1 field that defines a substantially spatially uniform tip angle distribution of the spins throughout the subject, which is conducive to accurate magnetic resonance imaging and/or spectroscopy.


However, the insertion of an object, such as a human imaging subject, into the examination region can distort the B1 field, especially at B0 fields of 3T or higher. Such distortions are typically due to dielectric and/or conductivity effects, and are related to the RF wavelength in the object becoming comparable to the size of the object. Subject-induced B1 field distortion and loading, becomes increasingly problematic as the asymmetry of the imaging subject increases (e.g., in the case of a “broad-shouldered” or otherwise asymmetric human imaging subject) and as the strength of the static (i.e., B0) magnetic field increases. Hence, coil loading has become increasingly problematic as commercial magnetic resonance scanners have progressed from low-field (e.g., 0.23 Tesla, 1.5 Tesla) to progressively higher static magnetic fields (e.g., 3 Tesla, 7 Tesla, or so forth).


Loading the coil can also be more problematic for large coils that couple to a large examination region, both because of the larger subject size and the larger area over which a substantially uniform B1 field is to be maintained. For large-volume imaging of human subjects, a quadrature body coil is sometimes used. Quadrature body coils provide efficient radio frequency coupling with a large region of interest such as a torso, legs, or other portion of a human imaging subject. A quadrature body coil is generally cylindrical in shape, and has radial symmetry. Examples include a quadrature birdcage body coil and a quadrature transverse-electromagnetic (TEM) body coil. The quadrature body coil includes I and Q channel input ports that are driven by radio frequency energy at a 90o phase difference to produce a rotating B1 field for exciting magnetic resonance.


B1 non-uniformity has been addressed in various ways.


In a post-acquisition processing approach, the acquired magnetic resonance data is corrected after acquisition to account for distortion of the B1 field. While a correction for the receive coil sensitivity pattern can be made the excitation still has a distribution of tip angles that affects the MR experiment. The range of excited tip angles can be reduced by using adiabatic RF pulses but this approach is time and RF exposure expensive as well a limiting RE sequences.


In another approach, multiple independent radio frequency amplifiers are used to generate a custom B1 field. For example, in the case of a quadrature body coil, each of the I and Q ports may be driven by a different amplifier. The amplitude and phase of each amplifier are selected to tailor the B1 field distribution. This approach works well, except that the extent of B1 field distribution tailoring is limited to four degrees of freedom, namely the amplitude and phase of each of the two amplifiers. To provide additional degrees of freedom, the radio frequency coil can be reconfigured to include additional ports that are connected with additional radio frequency amplifiers. For example, a TEM coil can be configured to have each rung, or each selected group of rungs, independently driven by a different radio frequency amplifier. For an eight element TEM coil, for example, up to eight amplifiers can be used providing sixteen degrees of freedom for tailoring the B1 field.


The substantial flexibility in tailoring the B1 field to compensate for coil loading using these approaches comes, however, at the cost of substantial increase in system complexity and cost. Radio frequency amplifiers are costly components. Each separately driven port requires its own waveform generation control, amplifier, and dedicated radio frequency cabling, trapping, and so forth. The additional radio frequency connections occupy valuable bore space and introduces opportunities for detrimental radio frequency cross-coupling.


In accordance with one aspect, a magnetic resonance scanner is disclosed. A main magnet generates a static magnetic field at least in an examination region. A magnetic resonance excitation system includes at least one radio frequency coil arranged to inject radio frequency energy into the examination region and at least two radio frequency amplifiers coupled with different input ports of the at least one radio frequency coil. A controller controls the magnetic resonance excitation system to produce a time-varying spatial B1 field distribution in a subject in the examination region that time-integrates to define a spatial tip angle distribution in the subject having reduced spatial non-uniformity.


In accordance with another aspect, a magnetic resonance excitation method is disclosed. A B1 non-uniformity imposed on at least one radio frequency coil by a subject coupled with the at least one radio frequency coil is determined. A time-varying spatial B1 field distribution is generated in the subject using the at least one radio frequency coil. The time-varying spatial B1 field distribution time-integrates to define a spatial tip angle distribution in the subject that is more spatially uniform than the time-varying spatial B1 field distribution.


In accordance with another aspect, a magnetic resonance excitation apparatus is disclosed. Means are provided for determining a B1 non-uniformity imposed on at least one radio frequency coil by a subject coupled with the at least one radio frequency coil. Means including the at least one radio frequency coil are provided for generating a time-varying spatial B1 field distribution in the subject. The time-varying spatial B1 field distribution time-integrates to define a spatial tip angle distribution in the subject having reduced spatial non-uniformity.


One advantage resides in providing flexible and effective compensation for B1 field non-uniformity.


Another advantage resides in providing compensation for different types of patterns of B1 non-uniformity without using different compensation coils or other loading-specific hardware.


Another advantage resides in acquisition of more accurate magnetic resonance data with reduced effects of B1 non-uniformity.


Another advantage resides in improved reconstructed image quality.


Another advantage resides in improved magnetic resonance spectra.


Still further advantages of the present invention will be appreciated to those of ordinary skill in the art upon reading and understand the following detailed description.





The invention may take form in various components and arrangements of components, and in various steps and arrangements of steps. The drawings are only for purposes of illustrating the preferred embodiments and are not to be construed as limiting the invention.



FIG. 1 diagrammatically shows a magnetic resonance scanner including a quadrature body coil, two independent radio frequency amplifiers separately driving the I and Q input ports of the quadrature body coil, and a two channel scanner controller with temporal sequencer for exciting a time-varying spatial B1 field distribution.



FIG. 2 diagrammatically shows the magnetic resonance excitation system of the magnetic resonance scanner of FIG. 1 in greater detail.



FIG. 3 show spatial B1 field distributions for modeling of an elliptical cardiac phantom placed in a quadrature body coil in a 3 Tesla magnetic field, for four different excitation conditions.



FIGS. 4 and 5 show spatial tip angle distributions produced by two different time-invariant B1 field distributions.



FIG. 6 shows a spatial tip angle distribution for a time-integrated combination of the time-invariant B1 field distributions of FIGS. 4 and 5.



FIG. 7 diagrammatically shows another magnetic resonance scanner employing a plurality of local coils in place of the quadrature body coil of FIG. 1.



FIG. 8 diagrammatically shows the magnetic resonance excitation system of the magnetic resonance scanner of FIG. 7 in greater detail.





With reference to FIG. 1, a magnetic resonance scanner 10 includes a scanner housing 12 in which a patient 16 or other subject is at least partially disposed. A protective insulating bore liner 18 of the scanner housing 12 optionally lines a generally cylindrical bore or opening of the scanner housing 12 inside of which the subject 16 is disposed. A main magnet 20 disposed in the scanner housing 12 is controlled by a main magnet controller 22 to generate a static (B0) magnetic field in at least a scanning region including at least a portion of the subject 16. Typically, the main magnet 20 is a persistent superconducting magnet surrounded by cryoshrouding 24. In some embodiments, the main magnet 20 generates a main magnetic field of at least about 0.2 Tesla, such as 0.23 Tesla, 1.5 Tesla, 3 Tesla, 7 Tesla, or so forth. Magnetic field gradient coils 28 are arranged in or on the housing 12 to superimpose selected magnetic field gradients on the main magnetic field in at least the scanning region. Typically, the magnetic field gradient coils include coils for producing three orthogonal magnetic field gradients, such as x-gradient, y-gradient, and z-gradient.


A generally cylindrical quadrature body coil 30 is mounted substantially coaxially with the bore of the magnetic resonance scanner 10. In some embodiments, the quadrature body coil 30 is a permanent fixture mounted inside the scanner housing 12. In some embodiments, the quadrature body coil 30 is mounted on a dielectric former or other holder that can be slidably inserted into and removed from the bore of the magnetic resonance scanner 10, or slidably inserted into and removed from an annular receptacle of the scanner housing 12. In other embodiments, the quadrature coil 30 can be a local quadrature coil, such as a head quadrature coil or a knee quadrature coil. In some embodiments the quadrature body coil 30 is a quadrature birdcage coil including a plurality of rungs arranged generally parallel with the axis of the bore and operatively interconnected by two or more endrings, endcaps, or other terminating structures disposed at or near the opposite ends of the rungs. In some embodiments the quadrature body coil 30 is a quadrature transverse-electromagnetic (TEM) coil including a plurality of rods arranged generally parallel with the axis of the bore and operatively interconnected by a generally annular radio frequency shield or screen substantially surrounding the rods. The quadrature body coil 30 optionally includes capacitances, inductances, resistances, chokes, transistors, relays, or other components for providing radio frequency tuning, decoupling, current blocking or trapping, or other functionality.


In some embodiments, the quadrature body coil 30 performs both transmit and receive functions. That is, the quadrature body coil 30 is externally energized to excite magnetic resonance in the subject 16, and is also used to receive magnetic resonance signals generated by the excitation. In some embodiments, the quadrature body coil 30 performs the transmit function, and a separate receive coil 34 receives magnetic resonance signals generated by the excitation. The optional separate receive coil 34 can be a surface coil as illustrated, or a surface coils array, or an arm coil, leg coil, or other local coil. In some embodiments, the scanner 10 is configurable so that in some imaging applications the quadrature body coil 30 performs both transmit and receive functions while in other imaging applications the quadrature body coil 30 performs the transmit function and a separate receive coil performs the receive function. The optional separate receive coil 34 typically includes detuning circuitry that detunes the receive coil during the transmit phase to avoid overloading the receive coil.


With continuing reference to FIG. 1 and with further reference to FIG. 2 which shows a magnetic resonance excitation system 36 of the magnetic resonance scanner of FIG. 1 in greater detail, an I-channel radio frequency amplifier 38 generates an I-channel radio frequency drive signal having an amplitude AI and a phase φI at the magnetic resonance frequency, while a Q-channel radio frequency amplifier 40 generates a Q-channel radio frequency drive signal having an amplitude AQ and a phase φQ at the same magnetic resonance frequency. The I-channel and Q-channel radio frequency drive signals are independent in that they may have different amplitudes AI, AQ (within the limits imposed by the dynamic ranges of the amplifiers 38, 40) and different relative phases φI, φQ. The I-channel drive signal output by the I-channel radio frequency amplifier 38 is fed into an I-channel input port 42 of the quadrature body coil 30. The Q-channel drive signal output by the Q-channel radio frequency amplifier 40 is fed into a Q-channel input port 44 of the quadrature body coil 30.


If the I-channel and Q-channel radio frequency drive signals are of equal amplitude (AI=AQ) with a 90° phase difference between the I- and Q-channel radio frequency drive signals (φQ−φI=90°), then the quadrature body coil 30 is operated in the usual quadrature mode that produces a B1 field vector that rotates at the magnetic resonance frequency. However, if two separate RF waveform generators and two independent amplifiers 38, 40 are provided, there is in general no restriction on the I- and Q-channel radio frequency drive signal amplitudes AI, AQ and the phase difference φQ−φI therebetween.


With reference to FIG. 1, optionally a magnetic field gradients controller 54 operates the magnetic field gradient coils 28 to spatially localize the magnetic resonance excitation to a slab or other localized region. Optionally, the magnetic field gradient controller 54 operates the magnetic field gradient coils 28 to apply one or more spatial encoding magnetic field gradient pulses.


In the embodiment of FIG. 1, a radio frequency receiver 56 is operatively connected with the illustrated local coil 34 to read magnetic resonance signals during a readout phase of the magnetic resonance sequence. Alternatively, in some embodiments the radio frequency receiver 56 is operatively coupled with the I and Q channel input ports 42, 44 of the quadrature body coil 30 during the readout phase, with suitably radio frequency circuitry being provided to switch between operative connection of the quadrature body coil 30 with the radio frequency amplifiers 38, 40 during the transmit phase and operative connection with the radio frequency receiver 56 during the readout phase. Optionally, the magnetic field gradient controller 54 operates the magnetic field gradient coils 28 during the readout phase to provide additional spatial encoding (i.e., readout encoding) of the magnetic resonance signals.


The magnetic resonance samples acquired during the readout are stored in a data buffer 58. A magnetic resonance data processor 60 performs processing of the acquired magnetic resonance data to extract useful information. In imaging applications, the data processor 60 suitably performs image reconstruction using a Fast Fourier transform or other image reconstruction algorithms comporting with the selected spatial encoding applied during generation of the magnetic resonance data. In spectroscopic applications, the processing performed by the data processor 60 may include, for example, performing spectral fast Fourier transform operations to recover chemical shift and J-coupling data. The resulting processed data (e.g., images, spectra, or so forth) are suitably stored in a data/images memory 62, displayed on a user interface 64, printed, communicated over the Internet or a local area network, stored on a non-volatile storage medium, or otherwise used. In the example configuration illustrated in FIG. 1, the user interface 64 also interfaces a radiologist or other operator with the scanner controller 66 to control the magnetic resonance scanner 10. In other embodiments, a separate scanner control interface may be provided.


With reference to FIGS. 1 and 2, the magnetic resonance excitation system 36 is configured to allow time-averaging of a B1( r) field so as to compensate for B1 spatial non-uniformity. In this notation, r denotes spatial position, so that B1( r) denotes the spatial B1 field distribution. Applying a time-invariant B1( r) field for a time τ produces a spatial tip angle distribution θ( r) given by:











θ


(

r
_

)


=



0
τ



γ





B
1
+



(

r
_

)











t




,




(
1
)








where γ is the gyromagnetic ratio and | B1+( r)| is the component of the B1( r) vector that contributes to magnetic resonance excitation. For the time-invariant B1( r) field the component | B1+( r)| is independent of time, and Equation (1) simplifies to:











θ


(

r
_

)


=

γ






B
1
+



(

r
_

)




·
τ



,




(
2
)








where τ is the duration of application of the constant |B1+| field.


The magnetic resonance scanner 10 includes the capability of generating a time-varying spatial B1( r) field distribution that varies in spatial shape, by independently controlling the I and Q channel radio frequency amplifiers 38, 40. Denoting the time-varying spatial B1( r) field distribution as B1( r,t) where t denotes time, Equation (1) becomes:










θ


(

r
_

)


=



0
τ



γ





B
1
+



(


r
_

,
t

)












t

.







(
3
)







If only a single radio frequency amplifier was used in conjunction with a hybrid circuit to produce the I and Q components, then the time-varying spatial B1( r,t) field distribution could only be varied in amplitude or phase—that is, the spatial shape of the spatial B1( r,t) field distribution could not be varied. This is the case with a typical MR system. In contrast, in the scanner 10 the time-varying spatial B1( r,t) field distribution can have varying shape.



FIG. 3 shows spatial B1( r,t) field distributions for modeling of an elliptical cardiac phantom (aspect ratio=19 cm/35 cm=0.54, length=34 cm, conductivity=0.5 S/m, and relative permittivity=78) placed in a quadrature body coil in a 3 Tesla static (B0) magnetic field. FIG. 3 shows the spatial B1( r,t) field distributions for four conditions: AI=1, AQ=0 (i.e., driving only the I channel using the I-channel amplifier 38); AI=0, AQ=1 (i.e., driving only the Q channel using the Q-channel amplifier 40); AI=1, AQ=1, φI=0°, φQ=90° (i.e., driving the quadrature body coil 30 in quadrature mode using both amplifiers 38, 40); and AI=1, AQ=1, φI=90°, φQ=0° (i.e., driving the quadrature body coil 30 in anti-quadrature mode using both amplifiers 38, 40). In the |B1+|-field maps of FIG. 3 (as well as those of FIGS. 4-6), regions of about average |B1+|-field intensity are shown with whiter grayscale values; whereas, regions of low or high |B1+|-field intensity are shown with darker grayscale values. That is, relatively uniform regions are whiter, while regions substantially contributing to non-uniformity are darker. Substantial spatial non-uniformities are seen for each of the coil operational modes, principally due to dielectric and eddy current effects in the cardiac phantom.


By suitably combining different spatial B1( r,t) field distributions in time, a time-varying spatial B1 field distribution can be produced in a subject that time-integrates to define a spatial tip angle distribution in the subject having reduced spatial non-uniformity. The combination can be continuous, e.g. by applying Equation (3), or can involve combining two or more time-invariant spatial B1 field distributions each held constant over selected time interval τ. For example, the amplifiers 38, 40 can be controlled by the controller 66 to produce a first time-invariant spatial B1 field distribution | B1+( r)|(1) over a time τ1 and a second time-invariant spatial B1 field distribution | B1+( r)|(2) over a time τ2, the first and second time-invariant spatial B1 field distributions being different due to different RF excitation conditions. The combined tip angle θ( r) is given by a linear combination of Equation (2):










θ


(

r
_

)


=


γ







B
1
+



(

r
_

)





(
1
)


·

τ
1



+

γ







B
1
+



(

r
_

)





(
2
)


·


τ
2

.








(
4
)







If a third time-invariant spatial B1 field distribution | B1+( r)|(3) is applied over a time τ3, where the first, second, and third time-invariant spatial B1 field distributions are different, then the resulting tip angle θ( r) is given by:










θ


(

r
_

)


=


γ







B
1
+



(

r
_

)





(
1
)


·

τ
1



+

γ







B
1
+



(

r
_

)





(
2
)


·

τ
2



+

γ







B
1
+



(

r
_

)





(
3
)


·


τ
3

.








(
5
)








More generally still, if N different time-invariant spatial B1 field distributions | B1+( r)|(n) are applied each for a selected time τn, where n=1 . . . N indexes the applied time-invariant spatial field distributions, then the resulting tip angle θ( r) is given by:










θ


(

r
_

)


=

γ





n
=
1

N








B
1
+



(

r
_

)





(
n
)


·


τ
n

.








(
6
)








FIGS. 4-6 show an application of Equation (4). FIG. 4 shows a spatial tip angle distribution θ1( r) produced by a time-invariant | B1+( r)|(1) field distribution in which AI=1, AQ=0.1, φI=0°, φQ=40° applied for a time interval τ1. FIG. 5 shows a spatial tip angle distribution θ2( r) produced by a time-invariant | B1+( r)|(2) field distribution in which AI=0.4, AQ=0.9, φI=120°, φQ=0° applied for a time interval τ2. In the spatial tip angle distribution θ1( r) of FIG. 4, the central region represents a large tip angle of about 90-120°, while in the spatial tip angle distribution θ2( r) of FIG. 5, the central region represents a small tip angle of about 0-40°.



FIG. 6 shows a spatial tip angle distribution θ( r) for the time-integrated combination of the time-invariant | B1+( r)|(1) and | B1+( r)|(2) field distributions of FIGS. 4 and 5 combined in accordance with Equation (4) with τ12. The field spatial tip angle distribution θ( r) of FIG. 6 has a tip angle of 90°±9.25°, with a 67% decrease in standard deviation versus operation of the coil 30 in quadrature. While FIG. 6 shows a combination of two different time-invariant B1 field distributions | B1+( r)|(1) and | B1+( r)|(2), it is anticipated that by selectively combining three different time-invariant B1 field distributions in accordance with Equation (5), or four or more different time-invariant B1 field distributions in accordance with Equation (6), can provide still further reduced spatial nonuniformity in the spatial tip angle distribution θ( r). In general, it can be expected that it will usually be possible to combine two selected different time-invariant B1 field distributions so as to produce a spatial tip angle distribution θ( r) that is more spatially uniform than either constituent time-invariant spatial B1 field distribution. Similarly, it can be expected that a time-varying spatial B1 field distribution can be chosen to produce a spatial tip angle distribution that is more spatially uniform than the time-varying spatial B1 field distribution.


With reference to FIGS. 1 and 2, the time-invariant spatial B1 field distribution used to create a more uniform spatial tip angle distribution can be either continuously varying (analyzed using Equation (3)) or discretely varying (analyzed using Equations (4)-(6)). In the continuously varying approach, the controller 66 controls the radio frequency amplifiers 38, 40 to generate output radio frequency signals with amplitudes AI(t), AQ(t) and phases φI(t), φQ(t) that are functions of time to produce a time-varying field distribution | B1+( r,t)| that time-integrates in accordance with Equation (3) to produce a spatial tip angle distribution θ( r) having reduced spatial non-uniformity. In the discretely varying approach, the controller 66 controls the radio frequency amplifiers 38, 40 to generate a temporal sequence of time-invariant output radio frequency signals each having amplitudes AI(n), AQ(n) and phases φI(n), φQ(n) that produce time-invariant field distributions | B1+( r)|(n) that sum in accordance with Equation (6) to produce a spatial tip angle distribution θ( r) having reduced spatial non-uniformity. A temporal sequencer 70 determines suitable continuous functions AI(t), AQ(t), φI(t), φQ(t) or discrete values AI(n), AQ(n), φI(n), φQ(n) that provide the spatial tip angle distribution θ( r) having reduced spatial non-uniformity based on a determination of the coil loading imposed on the radio frequency coil 30 by a subject in the examination region.


The determination of B1 non-uniformity can be done in various ways. In some embodiments, a pre-scan is performed and an image of the subject reconstructed, and the B1 non-uniformity estimated from the reconstructed image. In other embodiments, the B1 non-uniformity may be estimated based on measurements of the dimensions of the subject. For example, the shoulder width and chest diameter of a human subject may be measured to estimate the amount of B1 non-uniformity the human subject will impose upon the coil. In some embodiments, the temporal sequencer 70 includes a look-up table of continuous functions AI(t), AQ(t), φI(t), φQ(t) or discrete values AI(n), AQ(n), φI(n), φQ(n) that provide substantial uniformity for the spatial tip angle distribution θ( r). The look-up table values are suitably pre-determined by finite element analysis simulations, or by experimental measurements on phantoms or human objects with different aspect ratios, or so forth. In other embodiments, the temporal sequencer 70 may include a finite element analysis electromagnetic simulator or other calculator for estimating suitable values of the continuous functions AI(t), AQ(t), φ1(t), φQ(t) or discrete values AI(n), AQ(n), φI(n), φQ(n) that provide substantial uniformity for the spatial tip angle distribution θ( r). That is, in the discrete embodiment a composite B1 pulse or pulse packet is applied by the amplifiers 38, 40 which includes a series of two (Equation (4)), three (Equation (5)), or N (Equation (6)) sub-pulses which cumulatively produce the selected spatial tip angle distribution. Each sub-pulse has a selectable amplitude, phase, and/or duration to provide numerous degrees of freedom in tailoring the overall B1 pulse or pulse packet.


In some embodiments, a sensor, sensor array or analyzer detects or measures the B1 field distribution to provide feedback 72 of the actual applied B1 field at the region of interest. In these embodiments, a series of pilot B1 pulses are suitably applied and the detected or measured B1 field distribution is used by the temporal sequencer 70 to dynamically or iteratively adjust the B1 sub-pulses or B1 pulse shape to achieve the desired spatial tip angle distribution. For these embodiments, a dedicated sensor, sensor array or analyzer can be used, or the receive coil 34 can be used as the sensor, along with suitable processing performed by the data processor 60 or another processor, to produce the feedback 72 for dynamically or iteratively tailoring the B1 sub-pulses or B1 pulse shapes.


With reference to FIGS. 7 and 8, the technique of using a time-varying field distribution | B1+( r,t)| that time-integrates (for example, using a suitable one of Equations (3)-(6)) to define a spatial tip angle distribution in the subject that is more spatially uniform than the time-varying spatial B1 field distribution can be applied to other magnetic resonance excitation systems. A magnetic resonance scanner 10′ includes a different magnetic resonance excitation system 36′ in which the quadrature body coil 30 is replaced by an array of local coils 301, 302, 303. While three local surface coils 301, 302, 303 are shown, other types and/or numbers of local coils can be used. The I-channel and Q-channel radio frequency amplifiers 38, 40 are replaced by a set of three radio frequency amplifiers 40′ that are independently controlled by the scanner controller 66. More generally, each local coil 301, 302, 303 has an input port that is coupled to its own independent amplifier—accordingly, the local coil 301 can be operated at amplitude A1(t) and phase φ1(t), the local coil 302 can be operated at amplitude A2(t) and phase φ2(t), and the local coil 303 can be operated at amplitude A3(t) and phase φ3(t). In the embodiment of FIG. 7, the local coils 301, 302, 303 operate as transmit/receive (Tx/Rx) coils that are selectively coupled with either the radio frequency amplifiers 40′ or the radio frequency receiver 56 by a suitable switch 80. The time-varying B1 field distribution | B1+( r,t)| is generated by the combination of local coils 301, 302, 303 based on the time-varying amplitudes A1(t), A2(t), A3(t) and time-varying phases φI(t), φ2(t), φ3(t). As in the quadrature body coil embodiment, the time integration can be either continuous (where A1(t), A2(t), A3(t), φ1(t), φ2(t), φ3(t) are in general continuous functions of time) or discrete (where the amplitudes and phases are varied discretely, e.g. A1(n), A2(n), A3(n), φ1(n), φ2(n), φ3(n) where n=1 . . . N denotes the number of discrete time-invariant B1 field distributions | B1+( r)|(n) that are combined in accordance with Equation (6).


The example magnetic resonance excitation systems 36, 36′ are not exhaustive. As another example of a suitable magnetic resonance excitation system, a degenerate birdcage or TEM coil can be used, with individual rungs or rods driven by separate radio frequency amplifiers in accordance with the techniques disclosed herein.


It is to be appreciated that less than all of the coil parameters may be varied. For example, referencing back to the embodiment of FIGS. 1 and 2, in some instances it may be sufficient to keep AI and φI constant (that is, the output of amplifier 38 is held constant) and to vary AQ and φQ continuously or discretely to effectuate the time-varying B1 field distribution | B1+( r,t)|. Indeed, it may be sufficient to vary only AQ or only φQ continuously or discretely to effectuate the time-varying B1 field distribution | B1+( r,t)|.


The invention has been described with reference to the preferred embodiments. Modifications and alterations may occur to others upon reading and understanding the preceding detailed description. It is intended that the invention be constructed as including all such modifications and alterations insofar as they come within the scope of the appended claims or the equivalents thereof.

Claims
  • 1. A magnetic resonance scanner comprising: a main magnet for generating a static magnetic field at least in an examination region;a magnetic resonance excitation system including: a quadrature coil having I and Q input ports, the quadrature coil being arranged to inject radio frequency energy into the examination region;an I channel radio frequency amplifier coupled with the I input port; anda Q channel radio frequency amplifier coupled with the Q input port; anda controller that controls the magnetic resonance excitation system to produce a time-varying spatial B1 field distribution in a subject in the examination region that time integrates to define a spatial tip angle distribution in the subject having reduced spatial non uniformity.
  • 2. The magnetic resonance scanner as set forth in claim 1, wherein the quadrature coil is one of a quadrature body coil and a quadrature head quadrature coil.
  • 3. The magnetic resonance scanner as set forth in claim 1, wherein the magnetic resonance excitation system includes: a plurality of local coils each having an input port; anda radio frequency amplifier coupled with the input port of each local coil.
  • 4. The magnetic resonance scanner as set forth in claim 1, further including: a sensor, sensor array or analyzer which provides feedback on the B1 field distribution.
  • 5. The magnetic resonance scanner as set forth in claim 1, wherein the controller controls each of the I channel and the Q channel radio frequency amplifiers to produce at least a first time-invariant spatial B1 field distribution over a time τ1 and a second time-invariant spatial B1 field distribution over a time τ2, the first and second time-invariant spatial B1 field distributions being different.
  • 6. The magnetic resonance scanner as set forth in claim 5, wherein the controller controls each of the I channel and the Q channel radio frequency amplifiers to further produce a third time-invariant spatial B1 field distribution over a time τ3, the first, second, and third time-invariant spatial B1 field distributions being different.
  • 7. The magnetic resonance scanner as set forth in claim 1, wherein the controller controls each of the I channel and the Q channel radio frequency amplifiers to produce continuously time-varying spatial B1 field distributions over a time τ.
  • 8. The magnetic resonance scanner as set forth in claim 1, wherein the controller controls each of the I channel and the Q channel radio frequency amplifiers to produce time-varying radio frequency signals to cause the quadrature coil to produce the time-varying spatial B1 field distribution.
  • 9. The magnetic resonance scanner as set forth in claim 8, wherein the at least one time-varying radio frequency signals include a time-varying amplitude and a time-varying phase.
  • 10. The magnetic resonance scanner as set forth in claim 1, wherein the controller includes: a look up table specifying a plurality of different sets of radio frequency signals corresponding to different coil loadings of the quadrature coil, each set of radio frequency signals being configured to be applied by the I channel and Q channel radio frequency amplifiers to produce a time-varying spatial B1 field distribution that time integrates to define a spatial tip angle distribution having reduced spatial non uniformity for the corresponding coil loading.
  • 11. The magnetic resonance scanner as set forth in claim 1, wherein the controller controls each of the amplifiers to apply a composite pulse made up of a plurality of sub pulses, each sub pulse having a selectable amplitude, phase, and duration.
  • 12. A magnetic resonance excitation method comprising: determining B1 non-uniformity imposed on at least one radio frequency coil by a subject coupled with the at least one radio frequency coil; andgenerating a time-varying spatial B1 field distribution in the subject using the at least one radio frequency coil, the time-varying spatial B1 field distribution time integrating to define a spatial tip angle distribution in the subject that is more spatially uniform than the time-varying spatial B1 field distribution, including: generating a first composite pulse made up of at least three sub-pulses, each sub-pulse having a selectable amplitude, phase, and duration.
  • 13. The magnetic resonance excitation method as set forth in claim 12, wherein each of the sub-pulses is different with regard to at least one of the amplitude, phase, and duration.
  • 14. The magnetic resonance excitation method as set forth in claim 13, wherein the generating further includes: generating a second composite pulse made up of at least three sub-pulses, each sub-pulse having a selectable amplitude, phase, and duration.
  • 15. The magnetic resonance excitation method as set forth in claim 14, further including: applying the first composite pulse to an I input port of a quadrature coil and the second composite pulse to a Q input port of the quadrature coil.
  • 16. The magnetic resonance excitation method as set forth in claim 14, further including: selecting the amplitude, phase, and duration of each sub-pulse by inputting physical characteristics of the subject into a look-up table and retrieving the amplitude, the phase, and the duration for each sub-pulse from the look-up table.
  • 17. A magnetic resonance scanner with a controller programmed to operate the scanner according to the method of claim 12.
  • 18. The magnetic resonance excitation method as set forth in claim 12, further including: sensing a spatial tip angle distribution defined in the subject; and,adjusting at least one of the amplitude, the phase, and the duration of at least one of the first and second composite pulses.
  • 19. A magnetic resonance excitation apparatus comprising: a look-up table for determining a B1 non-uniformity imposed on at least one radio frequency coil by a subject coupled with the at least one radio frequency coil, the look-up table being preprogrammed to correlate an aspect ratio of the subject with a time-varying spatial B1 field distribution to be generated in the subject, the time-varying spatial B1 field distribution time integrating to define a spatial tip angle distribution in the subject having reduced spatial non uniformity;a controller which receives the time-varying spatial B1 field distribution from the look-up table and controls at least one radio frequency amplifier to produce the received time-varying spatial B1 field distribution in the subject.
  • 20. The magnetic resonance excitation apparatus as set forth in claim 19, wherein the at least one radio frequency coil is a quadrature coil, and the at least one radio frequency amplifier includes: two radio frequency amplifiers coupled with two quadrature ports of the quadrature coil, each of the two radio frequency amplifiers outputting at least one of a time-varying radio frequency amplitude and a time-varying radio frequency phase.
  • 21. The magnetic resonance excitation apparatus as set forth in claim 19, wherein the controller controls the at least one radio frequency amplifier to apply a composite pulse made up of at least three sub-pulses, each sub-pulse having a selectable amplitude, phase, and duration.
  • 22. The magnetic resonance excitation apparatus as set forth in claim 19, wherein the at least one radio frequency coil includes a plurality of local coils.
CROSS REFERENCE TO RELATED APPLICATIONS

This application claims the benefit of U.S. provisional application Ser. No. 60/745,290 filed Apr. 21, 2006, which is incorporated herein by reference.

PCT Information
Filing Document Filing Date Country Kind 371c Date
PCT/US2007/065841 4/3/2007 WO 00 10/20/2008
Publishing Document Publishing Date Country Kind
WO2007/124245 11/1/2007 WO A
US Referenced Citations (21)
Number Name Date Kind
4710718 Shaka Dec 1987 A
6608480 Weyers Aug 2003 B1
6946840 Zou et al. Sep 2005 B1
6975114 Ledden Dec 2005 B1
7075302 Zhu Jul 2006 B2
7078901 Feiweier et al. Jul 2006 B2
7166999 Duensing Jan 2007 B2
7498809 Takahashi et al. Mar 2009 B2
20010033166 Hoult et al. Oct 2001 A1
20040012391 Vaughan, Jr. et al. Jan 2004 A1
20040150401 Eberler et al. Aug 2004 A1
20050099178 King et al. May 2005 A1
20050110487 Zhu May 2005 A1
20050174116 Leussler et al. Aug 2005 A1
20050194975 Duensing Sep 2005 A1
20050231203 Feiweier et al. Oct 2005 A1
20080129298 Vaughan et al. Jun 2008 A1
20090021254 Gore et al. Jan 2009 A1
20090273345 Ruhm Nov 2009 A1
20100052679 Zelinski et al. Mar 2010 A1
20100066361 Setsompop et al. Mar 2010 A1
Foreign Referenced Citations (1)
Number Date Country
2006033047 Mar 2006 WO
Related Publications (1)
Number Date Country
20090102483 A1 Apr 2009 US
Provisional Applications (1)
Number Date Country
60745290 Apr 2006 US