GB2057142A - Nuclear magnetic resonance systems - Google Patents

Nuclear magnetic resonance systems Download PDF

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GB2057142A
GB2057142A GB8025616A GB8025616A GB2057142A GB 2057142 A GB2057142 A GB 2057142A GB 8025616 A GB8025616 A GB 8025616A GB 8025616 A GB8025616 A GB 8025616A GB 2057142 A GB2057142 A GB 2057142A
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gradient
region
slice
resonance
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    • GPHYSICS
    • G01MEASURING; TESTING
    • G01RMEASURING ELECTRIC VARIABLES; MEASURING MAGNETIC VARIABLES
    • G01R33/00Arrangements or instruments for measuring magnetic variables
    • G01R33/20Arrangements or instruments for measuring magnetic variables involving magnetic resonance
    • G01R33/44Arrangements or instruments for measuring magnetic variables involving magnetic resonance using nuclear magnetic resonance [NMR]
    • G01R33/48NMR imaging systems
    • G01R33/483NMR imaging systems with selection of signals or spectra from particular regions of the volume, e.g. in vivo spectroscopy
    • G01R33/485NMR imaging systems with selection of signals or spectra from particular regions of the volume, e.g. in vivo spectroscopy based on chemical shift information [CSI] or spectroscopic imaging, e.g. to acquire the spatial distributions of metabolites

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  • Physics & Mathematics (AREA)
  • Spectroscopy & Molecular Physics (AREA)
  • Optics & Photonics (AREA)
  • High Energy & Nuclear Physics (AREA)
  • Condensed Matter Physics & Semiconductors (AREA)
  • General Physics & Mathematics (AREA)
  • Magnetic Resonance Imaging Apparatus (AREA)

Abstract

The invention provides investigation of chemical shift for an element, e.g. phosphorus, in a region of a body. In one example resonance is excited in a line in a body slice. Frequency dispersion down the line is produced by pulsed field Gy having a switched gradient so that the frequency distribution is in steps to allow resolution of chemical shift in limited regions of the line, without overlap. Measured FID signals 1 are Fourier transformed to give spatial and chemical analysis of the line. Alternatively resonance is excited in a slice and lines are selected by a pulsed gradient to give chemical dispersion and spatial dispersion between the lines after Fourier Transformation. This is repeated for different directions of the pulsed gradient to allow analysis of a chemical line by convolution techniques and give a picture for the slice. <IMAGE>

Description

SPECIFICATION Nuclear magnetic resonance systems The present invention relates to systems for providing, by nuclear magnetic resonance (NMR), distributions of chemicals in a selected region of a body. In particular, but not exclusively, it relates to measuring distributions of phosphorus. The examination is particularly applicable also to use for medical investigation of patients.
Phosphorus (31p) exists in low concentrations in the human body. It has a small nuciear magnetic movement and has a gyromagnetic ratio of 17.43MH2 Tesla-' (compared with 426MHz r for the protons for which NMR studies are normally used).
Techniques have been described for obtaining proton images of bodies. However because of the low concentrations mentioned, times in the range 12-1200 minutes would be required to obtain such images for 3rep, for a pixel size 40 x 40 x 40 mm and a signal to noise ratio of 14. It is therefore perhaps not the preferred approach to attempt such images.
It is an object of this invention to provide an alternative method and apparatus for investigating phosphorus and other chemicals in the body by NMR.
According to the invention there is provided a method of determining the distribution, in a body, of chemicals including a chosen element, for example phosphorus, the method including the steps of: exciting resonance for said element preferentially in a region in said body; applying a magnetic field having a gradient in said region to introduce a frequency dispersion in said resonance, said gradient being switched to provide free induction decay signals, in the form of a line spectrum of a Fourier series; measuring the free induction decay signals; and Fourier transforming the free induction decay signals to provide the chemical shifts for said element for a plurality of individual parts of said region as dispersed spectra around the lines of said first mentioned spectrum.
According to another aspect of the invention there is provided a method of investigating the distribution of chemicals in a body the method including the steps of: applying magnetic fields to cause resonance preferentially in a region of said body at a frequency appropriate to a chosen element; applying a switched magnetic field having a gradient along said region to produce dispersion in said resonance, the timing of the field being such that the region is effectively divided into a plurality of smaller regions, the nuclei of the chosen element in each region resonating within a unique frequency band and dispersion in the band representing a chemical shift to be determined; sensing free induction decay and rephasing signals emitted by the nuclei as the field gradient is switched; sampling the free induction decay and rephasing signals and Fourier Transforming the samples so that the frequencies in the samples are dispersed, the dispersion being indicative of both spatial and chemical shift, the gradient being of sufficient amplitude that the frequency shift, is larger than the chemical shift by an amount sufficient to avoid ambiguity.
The invention embraces an apparatus for implementing the method of the two preceding paragraphs.
In order that the invention may be clearly understood and readily carried into effect it will now be described by way of example with reference to the accompanying drawings of which, Figure 1 shows a chemical shift between two resonance lines of the same element, Figure 2 shows two such lines in the presence of an excessively strong gradient, Figure 3 shows the same lines in the presence of a gradient of an intermediate strength allowing sufficient resolution, Figure 4a shows the form of the gradient field along a selected strip, Figure 4b shows the resulting FID and rephasing signals, Figure 5 shows an NMR imaging system which can be used for this invention, Figure 6 shows a distribution of field sensing probes for the apparatus of Figure 5, Figures 7a, 7b and 7c shows Bo and gradient field coils for this apparatus, Figure 8 shows RF coils for this apparatus, Figure 9 shows circuits, in block form for applying the examining fields to the coils, and Figure 10 shows a block diagrammatic circuit for processing the free induction decay and rephasing signals.
Biochemical studies (for example as described in the paper by Hollis et al.: J. Mag. Res. 29, 319 (1978)) have been performed on perfused animal hearts by monitoring the relative abundance of various chemicals containing 31p. The various chemicals are distinguished by the chemical shift of the 31P lines. These studies have shown strong correlation between the relative strengths of the different 31P lines and various heart conditions.
The chemical shifts are of the order of 10--20 ppm.
NMR imaging systems proposed can provide, in central regions generally at least as large as the heart, field uniformities around 1 ppm and it is proposed to use these systems to examine the human heart in vivo. This is equivalent to using the imaging system as a large scale spectrometer since what is to be measured is the spectrum given by the chemical shift of the 31P lines.
The chemical shift between resonance lines arises because atoms of the same element attached at various sites on the same molecule or to different molecules find themselves in different micro-fields, i.e. the fields due to neighbouring atoms of the same or other species. These fields are necessarily small and hence the shifts are also small, 10 ppm being a relatively large shift.
Figure 1 shows an example of two lines separated by a shift Ws. Each line has a line width W,. It should be noted that there is no reason for each line to have the same line width; independent lines have their own independent values of relaxation times T, and T2, reflecting their differing chemical environments.
If it is desired to perform imaging studies by any means, it is necessary to apply field gradients of some kind to introduce spatial encoding of the k'MR signal. Figure 2 shows the effect of too strong a gradient; it can be seen that each line is dispersed by the bandwidth of the gradient field and the two broadened lines overlap. The spectrum is degenerate; it is impossible uniquely to assign the origin of a given region of the spectrum. This is the normal situation in proton imaging in which chemical shifts of the proton lines are ignored.
Figure 3 shows that to avoid degeneracy the gradient field bandwidth must be restricted to less than the chemical shift of the two lines. The maximum number of pixels or strips that can be resolved is simply Ws WL The method which it is proposed to apply in one embodiment of the invention is in effect the same as that used for proton imaging in that it is proposed to isolate a cross-sectional slice of the body and then cause resonance, at a frequency appropriate to 31P (i.e. 1.743 My, for a 0.1field) preferentially in a line or strip of that slice.
The first requirement for this is to create a large uniform and steady magnetic field, which can be called Bo, to define the equilibrium spin polarization axis of the molecules in a direction which can be identified as z. This will probably be axial of the patient.
A linear magnetic field gradient Gz is applied, where Bz Gz= 3z Simultaneously there is applied an RF (G,) field.
The B1 field is tailored to saturate all of the spins except those in the selected slice, using a technique developed by Mansfield and described in U.S. Patent No. 4021726. Following this there is applied another gradient DBz Gx= ax where x is one of two orthogonal directions (x and y) in the slice. The effect of the Gx gradient is to provide a dispersion of Larmor frequencies in the x direction so that each of a plurality of adjacent strip perpendicular to the x-direction has Larmor frequencies within a respective small range about a mean for the strip. Selection of a strip is then by application of a 90 B, pulse as is well known in NRdR at the mean Larmor frequency for the chosen strip.This then excites all of the molecules in the strip preferentially over the other molecules in the slice. When the molecules have been excited a free induction decay (free induction decay) signal of known form results. It may be noted that the effect of saturating molecules outside the selected slice is that these molecules will not respond to the further fields; the line selection is then by that method which has been previously proposed for slice selection in NMR imaging. A gradient aBZ Gy(Gy ), ay where y is the direction along the line, can then be applied to disperse the frequencies along the line.
It is however also desired to accommodate the chemical shift which is to be measured. For that reason the Gy field gradient is switched as shown in Figure 4a. The result of this switching is that there is produced a spin echo signal each time the gradient is reversed, as shown in Figure 4b. The free induction decay signal, instead of being a continuous spectrum, is now a line spectrum of a Fourier series (because of the repetitive nature of the switching). In effect this means that instead of there being a continuous gradation of Larmor frequency down the strip, as is normally produced by a steady Gy gradient, the frequency dispersion is in steps. The strip is thus effectively divided into a plurality of small elements each at a respective Larmor frequency. However, adjacent elements are not at adjacent frequencies but are spaced.
The reason that this spacing is desired that the chemical shift to be measured (about 50-60 ppm for phosphorous) provides a further small frequency dispersion so that each small element has in fact a spectrum of frequencies and not a single value. The spacing (typically 100 ppm) produced by the stepped Gy gradient al!ows this chemical dispersion without causing frequency overlap between adjacent elements so that the chemical information is not lost. In practice quite a large spacing is required to accommodate the chemical shift and is not likely that more than six elements can be resolved in a line.
Turning to Figure 4a again it can be seen that the Gy gradient can be considered to be in small steps of duration and that each one of these gives an FID signal (1) or a rephasing signal (2) which is the mirror image of an FID.
For processing each rephasing signal is mirror imaged to take the same form as free induction decay.
The sampied data comprises information for both the spatial (y direction) dispersion and the chemical shift dispersion and can be Fourier transformed to give the chemical analysis for each element of the strip. The procedure is to be repeated with appropriately different fields to examine other strips. Reversal of the rephasing signals is a relatively straightforward operation since each free induction decay or rephasing signal is usually digitised and stored in digital form before Fourier transformation. It is merely necessary to withdraw the rephasing signal from storage in the reverse order to the free induction decay signals.
The procedure is repeated with different Gx gradients to select different strips so as to provide chemical information for a matrix of elements. It has previously been mentioned that in order to accommodate the chemical information it is, in practice, only possible to obtain low spatial resolution giving typically 6 x 6 or even 4 x 4 matrices. The chemical information may be displayed in different manners as desired. It is simple, for such a small matrix, to separate the lines for each element and to provide a different picture for each chemical line resolved.
Essentially the same procedure may be applied to other imaging techniques to allow chemical dispersion. That described hereinbefore involves strip excitation but another suitable method involves adapting the slice excitation methods such as described in our co-pending patent application No. 22291/78.
In that procedure the large uniform and steady Bo field is applied as before. Similarly the Gz field gradient is applied but the RF (B,) field applied with it is in this method a 900 pulse so that a substantially planar slice of the patient is excited.
Preferably this is followed by a further Gz gradient pulse to rephase the spins across the slice (as described in said application No. 22291/78).
Finally a GA gradient is applied where GA is a resultant of Gx and Gy gradients with the direction determined by the relative intensities of the components. This provides dispersion of the spins to give different resonance frequencies in a number of strips perpendicular to the direction of GA. According to this example of the present invention the procedure only differs from that described in the said co-pending application in that the GA gradient is switched to give a line spectrum free induction decay (FID) resonance signal. Thus the spacing of the strips in the slice is enough to accommodate the chemical shift spectrum. This FID signal is Fourier Transformed to obtain line integrals corresponding to a particular chemical shift for each of the strips.
This procedure is repeated for a plurality of different orientations of strips in the slice, by changing the direction of the GA gradient and the convolution techniques known for computed tomography x-ray procedures (as described in application No. 22291/78) are used to provide a picture for each chemical shift of interest. As in the previous embodiment this is only a low resolution matrix.
The method described hereinbefore may be performed on a suitable NMR examining apparatus of which one example is shown in simplified form in Figure 5. Illustrated schematically only are: coils 6, which provide the steady Bo field; 7, which provide the Gx field gradient; 8 which provide the Gy field gradient, 9; which provide the RF fields; and 10, which provide the Gz field gradient. The coils are driven by Bo, Gx, Gy, RF and Gz drive amplifiers 11, 12, 13, 14 and 1 5 respectively, controlled by Bo, Gxy, RF and Gz control circuits 16, 17, 1 8 and 1 9 respectively.
These circuits can take suitable forms which will be well known to those with experience of NMR equipment and other apparatus using coil induced magnetic fields. The circuits are controlled by a central processing and control unit 20 to achieve a desired pulse sequence such as that of this invention.
The FID signals sensed are received in this -example by the RF coils 9 and are amplified by an RF amplifier 21 before being applied to signal handling circuits 22. In certain circumstances it may be preferable to provide separate coils specifically designed for the purpose, to sense the signal. The circuits 22 are arranged to make any appropriate calibrations and corrections but essentially transmit the signals to the processing circuits to provide the required representation of the examined slice. These circuits can conveniently be combined with the circuits which control the pulse sequence and thus are included in the circuits indicated at 20. The information thus obtained can be displayed on a display 23, such as a television monitor, and this may include inputs and other peripherals 24 for the provision of commands and instructions to the machine, or other forms of output.
The apparatus also includes field measurement and error signal circuits 25 which receive signals via amplifiers 26 from field probes X1, X2, Yr, and Y2, shown. The positions of the probes, in relation to the examined slice of the body 27 of the patient, are further shown in Figure 6. X1,X2,Y1 and Y2 are in this example simply miniature cells of pure, or slightly doped water (such as a closed test tube) surrounded by a small coil. Preferably the water is doped to have a suitable value ofT1, relaxation time-constant. The probes give a reliable resonance of 4.26 kHz/Oe. Other types of probe may be used as desired.
Figures 7a and 7b show in end and side elevation respectively a practical coil arrangement to provide the Bo field. Figure 7a also shows the coils for production of the Gx and Gy field pulses and, to show approximate dimensions, the patient 27 in cross-section. The patient 27 is inserted in the tubular former of Gx and Gy coils 7,8 and is supported there by a suitable couch or other supporting means. Such supports may be readily provided in any suitable form.
The coils 7, 8 are two sets of coils axially displaced, each set comprising two pairs of saddle coils, the pair 7 being at 900 to the pair 8. These coils are themselves inserted into the central aperture in Bo coils 6 which are wound in four parts connected in series to provide an approximately circular configuration which is well known to be desirable for production of a uniform field.
Figure 7c is a partially cut-away perspective view which shows the coils 7, 8 in more detail.
Also visible in the cut-away are the two circular coils 10 which provide the Gz field component for the gradient superimposed on Bo.
The RF coils are shown in Figure 8 in perspective. They are two saddle shaped coils 9 which are driven in parallel to provide the rotating RF field and which are in this example, also used to detect the FID signals which are of approximately the same frequency.
Further details of the coil winding will not be given since suitable coils can readily be devised, by those with the appropriate skills, to provide the fields required.
Where x, y and z gradients and RF fields are required in this apparatus, their predetermined amplitudes and directions are prestored in profile stores 29 shown in Figure 10. The durations are in terms of a number of pulses of a system clock 28.
The operation of the four profile stores 29 is controlled by a sequence control store 30 which stores in similar manner a sequence of commands to operate the profile stores and the duration (number of clock pulses) of operation of each stage of the sequence, including gaps in the sequence. Stores 29 and 30 are conveniently programmable read only memories (PROM's).
When commanded by a central (operator) control (which is shown in Figure 9 but which may be associated with circuits 20) the sequence control store initiates the first pulse profiles. The appropriate stores 29 provide the amplitude and duration signals which are converted to analogue form in digital to analogue converters (DAC's) 31 and applied to respective coil drive circuits 12(x), 13(y), 1 4(RF) and 15(z). The respective drive circuits, which can take any form well known for driving field coils, provide the specified current to the appropriate coil for the specified duration.
The apparatus and circuits described so far may be adapted to provide different sequences of NMR examining pulses, by appropriately adjusting the stored sequence and profile data. Similarly other known NMR apparatus which are capable of applying a steady magnetic field, a pulsed RF field and Gx, Gy and Gz field gradients to a body, may be adapted in a manner straightforward to those skilled in the NMR art to apply the fields and pulse sequence described for this invention.
The basic features of the signal handling system are shown in Figure 10. The FID signals from the signal sensing coils, in this example the RF coils 9, are amplified in an RF amplifier 21 demodulated and filtered before sampling in a unit 36 and applied via an analogue to digital converter (ADC) 31 to a store 32, such as a random access memory (RAM).
System clock pulses from the clock 28 are also applied to the RAM 32 to indicate the timing of the switched Gy (or GR) pulse sequence causing the line spectrum FID's and hence the identities of the FID signals. The input and output from RAM store 32 is effected by a suitably preprogrammed address selector 33 using the system clock pulses for input timing.
The signals extracted from the RAM store 32 are processed by a Fourier Transform circuit 34 which operates in a well established manner. The processed data is held in another RAM store 35 in convenient form to be output for display.
Variations of the circuit given, for controlling the pulsed field gradients and for handling the FID signals, may readily be devised within the scope of this invention.
Furthermore it will be appreciated that there has been described one form of NMR imaging apparatus which may readily be used to examine chemical shifts as explained in this invention.
However other imaging systems have been proposed and they may be adapted to implement this invention.
As an alternative to the procedure first described of selecting the strip by first saturating outside a slice and then applying a gradient therein, it is possible to apply simultaneously two orthogonal AC gradients in z and x directions. This is however not a preferred alternative. It will also be understood that the procedures explained for obtaining measurements for chemical shifts for phosphorus may be adapted to measurements for other chemicals by appropriate changes of frequency.

Claims (14)

1. A method of determining the distribution, in a body, of chemicals including a chosen element, for example phosphorus, the method including the steps of: exciting resonance for said element preferentially in a region in said body; applying a magnetic field having a gradient in said region to introduce a frequency dispersion in said resonance, said gradient being switched to provide free induction decay signals, in the form of a line spectrum of a Fourier series; measuring the free induction decay signals; and Fourier transforming the free induction decay signals to provide the chemical shifts for said element for a plurality of individual parts of said region as dispersed spectra around the lines of said first mentioned spectrum.
2. A method according to claim 1 in which the region in which resonance is excited is a strip in said body and the switched gradient is a gradient along said strip.
3. A method according to claim 2 in which said steps are repeated to evaluate chemical shifts for a plurality of elements along each of the plurality of said strips.
4. A method according to claim 1 in which the region in which resonance is excited is a substantially planar slice of said body and the switched gradient is a gradient in a chosen direction in said slice to provide signals representing chemical shift for a plurality of parallel strips perpendicular to the direction thereof.
5. A method according to claim 4 in which the preceding steps are repeated for a plurality of directions of said gradient to provide signals representing chemical shifts for a plurality of sets of parallel strips at different orientation in said plane and the said signals are further processed to provide an image of said planar slice for one or more of said chemical shifts.
6. A method of investigating the distribution of chemicals in a body the method including the steps of: applying magnetic fields to cause resonance preferentially in a region of said body at a frequency appropriate to a chosen element; applying a switched magnetic field having a gradient along said region to produce dispersion in said resonance, the timing of the field being such that the region is effectively divided into a plurality of smaller regions, the nuclei of the chosen element in each region resonating within a unique frequency band and dispersion in that band representing a chemical shift to be determined; sensing free induction decay and rephasing signals emitted by the nuclei as the field gradient is switched: sampling the free induction decay and rephasing signals and Fourier Transforming the samples so that the frequencies in the samples are dispersed, the dispersion being indicative of both spatial and chemical shift, the gradient being of sufficient amplitude that the frequency shift, is larger than the chemical shift by an amount sufficient to avoid ambiguity.
7. A method of determining the distribution in a body of chemicals including a chosen element, the method including the steps of: applying a steady and substantially uniform magnetic field at least in a region of interest of said body; applying a magnetic field having a gradient in said region together with a pulse of RF energy tailored to saturate the spins of nuclei in the region with the exception of a substantially planar slice thereof perpendicular to the direction of the gradient; applying a magnetic field having a gradient in a direction in the slice together with a RF pulse sufficient to excite the nuclei in a strip therein; applying a magnetic field having a gradient in a direction orthogonal to the two previously mentioned gradients, said third mentioned gradient being switched to provide a line spectrum free induction decay signal, representing free induction decays for a plurality of elements along said line, such that the spacing of the lines of said spectrum is sufficient to accommodate the chemical shift spectrum of each element in the strip.
8. A method according to claim 7 including repeating said steps for a plurality of lines in said slice to provide chemical shifts for a matrix of said elements.
9. A method according to either of claim 7 or claim 8 in which said lines are excited by 7r/2 RF pulses as herein defined.
10. A method of determining the distribution in a body of chemicals including a chosen element, the method including the steps of: applying a steady and uniform magnetic field at least in a region of interest of said body; applying a magnetic field having a gradient in said region together with a pulse of RF energy to excite to resonance nuclei in a substantially planar slice of said region of interest; applying a further magnetic field having a gradient in a chosen direction in said slice, the further magnetic field being switched to provide a line spectrum free induction decay signal, representing a plurality of substantially parallel strips in said slice perpendicular to the chosen direction;Fourier Transforming the free induction decay signal to obtain line integrals of chemical shifts for each of said strips; repeating the preceding steps for a plurality of different directions, in the slice, of the gradient, of the further magnetic field, and processing the line integrals for all of said directions to provide said distribution.
11. A method of determining the distribution in a body of chemicals including a chosen element, the method being substantially as herein described with reference to the accompanying drawings.
12. An apparatus for determining the distribution in a part of a body of chemicals including a chosen element, the apparatus including: means for exciting resonance for said element preferentially in a region of said body; means for applying a magnetic field having a gradient in said region to introduce a frequency dispersion in said resonance, said gradient being switched to provide free induction decay signals as a line spectrum of a Fourier series; means for measuring the free induction decay signals to provide chemical shifts for said element for a plurality of individual parts of said region as dispersed spectra around the lines of said first mention spectrum.
13. An apparatus according to claim 12 in which the means for exciting is arranged to excite resonance in a strip in said body and the means for applying the field having a gradient is arranged to produce the gradient in the direction of the strip.
14. An apparatus according to claim 13 in which the means for exciting is arranged to excite a plurality of different strips.
1 5. An apparatus according to claim 12 in which the means for exciting is arranged to excite resonance in a substantially planar slice of said body; the means for applying a magnetic field is arranged to provide a gradient in said slice, for each of a plurality of directions thereof to provide signals representing chemical shifts for a plurality of parallel strips perpendicular to each of said directions; and means for processing the signals to provide an image of the planar slice for one or more of the chemical shifts.
1 6. An apparatus for determining the distribution of a body of chemicals including a chosen element, the apparatus being substantially as herein described with reference to the accompanying drawings.
GB8025616A 1979-08-10 1980-08-06 Nuclear magnetic resonance systems Expired GB2057142B (en)

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Cited By (14)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0071896A1 (en) * 1981-08-12 1983-02-16 Siemens Aktiengesellschaft High frequency coil system for a nuclear resonance imaging apparatus
EP0095124A1 (en) * 1982-05-26 1983-11-30 Bruker Medizintechnik GmbH Method for the non-invasive determination of measurement values inside a living body
EP0100183A2 (en) * 1982-07-28 1984-02-08 Picker International Limited Nuclear magnetic resonance method and apparatus
GB2123963A (en) * 1982-07-07 1984-02-08 Picker Int Ltd Nuclear magnetic resonance imaging for monitoring thermal treatment
GB2128339A (en) * 1982-10-06 1984-04-26 Peter Mansfield Nuclear magnetic resonance imaging
EP0109238A2 (en) * 1982-11-10 1984-05-23 Picker International Limited Nuclear magnetic resonance method and apparatus
GB2131957A (en) * 1982-12-17 1984-06-27 Picker Int Ltd Nuclear magnetic resonance imaging
US4471305A (en) * 1978-07-20 1984-09-11 The Regents Of The University Of Calif. Method and apparatus for rapid NMR imaging of nuclear parameters with an object
GB2160325A (en) * 1984-06-13 1985-12-18 Picker Int Ltd Nuclear magnetic resonance (nmr) imaging
DE3539256A1 (en) * 1984-11-21 1986-05-22 Instrumentarium Corp., Helsinki METHOD FOR RECORDING THE CORE MAGNETIC PROPERTIES OF AN OBJECT TO BE EXAMINED
US4599565A (en) * 1981-12-15 1986-07-08 The Regents Of The University Of Calif. Method and apparatus for rapid NMR imaging using multi-dimensional reconstruction techniques
EP0210038A2 (en) * 1985-07-15 1987-01-28 Siemens Aktiengesellschaft Chemical shift imaging with field inhomogeneity corrections
US4654595A (en) * 1983-06-23 1987-03-31 Instrumentarium Oy Method of analyzing properties of a matter or a magnetic field
USRE33259E (en) * 1978-07-20 1990-07-10 The Regents Of The University Of California Method and apparatus for rapid NMR imaging of nuclear parameters with an object

Cited By (21)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
USRE33259E (en) * 1978-07-20 1990-07-10 The Regents Of The University Of California Method and apparatus for rapid NMR imaging of nuclear parameters with an object
US4471305A (en) * 1978-07-20 1984-09-11 The Regents Of The University Of Calif. Method and apparatus for rapid NMR imaging of nuclear parameters with an object
EP0071896A1 (en) * 1981-08-12 1983-02-16 Siemens Aktiengesellschaft High frequency coil system for a nuclear resonance imaging apparatus
US4599565A (en) * 1981-12-15 1986-07-08 The Regents Of The University Of Calif. Method and apparatus for rapid NMR imaging using multi-dimensional reconstruction techniques
EP0095124A1 (en) * 1982-05-26 1983-11-30 Bruker Medizintechnik GmbH Method for the non-invasive determination of measurement values inside a living body
GB2123963A (en) * 1982-07-07 1984-02-08 Picker Int Ltd Nuclear magnetic resonance imaging for monitoring thermal treatment
EP0100183A2 (en) * 1982-07-28 1984-02-08 Picker International Limited Nuclear magnetic resonance method and apparatus
EP0100183A3 (en) * 1982-07-28 1985-01-09 Picker International Limited Nuclear magnetic resonance method and apparatus
GB2128339A (en) * 1982-10-06 1984-04-26 Peter Mansfield Nuclear magnetic resonance imaging
US4588948A (en) * 1982-10-06 1986-05-13 Peter Mansfield Nuclear magnetic resonance methods
EP0109238A3 (en) * 1982-11-10 1985-05-29 Picker International Limited Nuclear magnetic resonance method and apparatus
EP0109238A2 (en) * 1982-11-10 1984-05-23 Picker International Limited Nuclear magnetic resonance method and apparatus
GB2131957A (en) * 1982-12-17 1984-06-27 Picker Int Ltd Nuclear magnetic resonance imaging
US4654595A (en) * 1983-06-23 1987-03-31 Instrumentarium Oy Method of analyzing properties of a matter or a magnetic field
GB2160325A (en) * 1984-06-13 1985-12-18 Picker Int Ltd Nuclear magnetic resonance (nmr) imaging
US4646023A (en) * 1984-06-13 1987-02-24 Picker International Ltd. Nuclear magnetic resonance imaging
GB2160325B (en) * 1984-06-13 1989-05-04 Picker Int Ltd Nuclear magnetic resonance imaging
DE3539256A1 (en) * 1984-11-21 1986-05-22 Instrumentarium Corp., Helsinki METHOD FOR RECORDING THE CORE MAGNETIC PROPERTIES OF AN OBJECT TO BE EXAMINED
DE3539256C2 (en) * 1984-11-21 1999-08-12 Picker Nordstar Oy Method for displaying the nuclear magnetic properties of an object to be examined
EP0210038A2 (en) * 1985-07-15 1987-01-28 Siemens Aktiengesellschaft Chemical shift imaging with field inhomogeneity corrections
EP0210038A3 (en) * 1985-07-15 1988-02-24 Technicare Corporation Chemical shift imaging with field inhomogeneity corrections

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