Technology ID
TAB-4181

Denoising of Dynamic Magnetic Resonance Spectroscopic Imaging Using Low Rank Approximations in the Kinetic Domain

E-Numbers
E-063-2017-0
Lead Inventor
Brender, Jeffery (NCI)
Co-Inventors
Yamamoto, Kazutoshi (NCI)
Munasinghe, Jeeva (NCI)
Kishimoto, Shun (NCI)
Merkle, Hellmut (NINDS)
Cherukuri, Murali (NCI)
Mitchell, James (NCI)
Applications
Software / Apps
Therapeutic Areas
Oncology
Development Stages
Prototype
Lead IC
NCI
ICs
NINDS
NCI

Accurate measurement of low metabolite concentrations produced by medically important enzymes is commonly obscured by noise during magnetic resonance imaging (MRI). Measuring the turnover rate of low-level metabolites can directly quantify the activity of enzymes of interest, including possible drug targets in cancer and other diseases. Noise can cause the in vivo signal to fall below the limit of detection. A variety of denoising methods have been proposed to enhance spectroscopic peaks, but still fall short for the detection of low-intensity signals. Dynamic nuclear polarization (DNP) is one method that has been critical for boosting weak signals. DNP must be performed near zero absolute temperature, requiring high operating costs. Measurements are limited to imaging immediately after tracer injection, limiting the range of injectable tracers that can be used in vivo. 
To address these issues, scientists at the National Cancer Institute (NCI) and National Institute of Neurological Disorders and Stroke (NINDS) have invented a unique method for measuring low-abundance metabolites in vivo which does not rely on frequency or spatial domains – but instead works in the kinetic domain. Data processing structure is simpler. True weak spectroscopic peaks can be more easily distinguished from noise. This technology improves the signal-to-noise ratio by an order of magnitude or more and has already been tested in vivo. The denoising software enhances low-metabolic signal without the need for DNP, which was previously thought impossible. The method makes MRI more informative for determining the metabolic activity of key enzymes in serious pathologies, is more dynamic in the range of tracers that can be used, and is generally less expensive. This software is also highly adaptable as it can be added as a plug-in to already existing MRI processing software. 
The scientists seek co-development parties and/or licensees for their invention.

Competitive Advantages:

  • Unique method for measuring low-abundance metabolites in vivo which does not rely on frequency or spatial domains
  • Significant enhancement of raw signal and differentiation when detecting pyruvic acid metabolism to lactate

Commercial Applications:

  • Plug-in software adaptable for use with current MRI-processing software
  • MRIs for clinical or research purposes
  • Ancillary invention of X-nuclei leg coil which improves signal-to-noise ratio and is compatible with software

Request More Info

Licensing Contact:
Clouse, Thomas
thomas.clouse@nih.gov

Patents

  • US
    Provisional (PRV) 62/459,008
    Filed on 2017-02-14
  • Patent Cooperation Treaty
    (PCT) PCT/US2018/018217
    Filed on 2018-02-14
  • Japan
    National Stage 2019-543765
    Filed on 2018-02-14
  • Australia
    National Stage 2018221015
    Filed on 2019-08-13
  • Canada
    National Stage 3053157
    Filed on 2018-02-14
  • European Patent
    National Stage 18707581.7
    Filed on 2018-02-14
  • US
    National Stage 16/485,772
    Filed on 2019-08-13
  • US
    Continuation (CON) 17/576,283
    Filed on 2022-01-14
  • Germany
    European patent (EP) 18707581.7
    Filed on 2018-02-14
  • France
    European patent (EP) 18707581.7
    Filed on 2018-02-14
  • United Kingdom
    European patent (EP) 18707581.7
    Filed on 2018-02-14

Publications

Collaborations

  • Licensing
  • Collaboration
Date Published
Date Updated