Difference between revisions of "DBP2:MIND:Roadmap"
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We will obtain gray matter, white matter, CSF, and lesion maps for each subject based on T1-weighted, T2-weighted, and FLAIR images. Ultimately, the NA-MIC Kit will provide a workflow for individual and group analysis of lesions. It will be implemented as a set of Slicer3 modules that can be used interactively within the Slicer3 application as well as in batch on a computing cluster using BatchMake. | We will obtain gray matter, white matter, CSF, and lesion maps for each subject based on T1-weighted, T2-weighted, and FLAIR images. Ultimately, the NA-MIC Kit will provide a workflow for individual and group analysis of lesions. It will be implemented as a set of Slicer3 modules that can be used interactively within the Slicer3 application as well as in batch on a computing cluster using BatchMake. | ||
− | + | The current status of the main modules to be used are: | |
=== Registration === | === Registration === | ||
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=== Lesion segmentation === | === Lesion segmentation === | ||
− | A number of algorithms for fully or semi-automated lesion analysis will be evaluated | + | A number of algorithms for fully or semi-automated lesion analysis will be evaluated. These include: |
− | :* UNC | + | :* Tools developed at UNC known as itkEMS Compare Lesion Analysis Tools (Marcel) |
− | :* EM-segment ( | + | :* EM-segment (Sandy Wells) |
:* MedX (commercial package) | :* MedX (commercial package) | ||
− | :* BRAINS2 ( | + | :* BRAINS2 (Magnotta) |
− | :* | + | :* Manual tracing by clinically trained rater |
=== Lesion Localization === | === Lesion Localization === | ||
Line 35: | Line 35: | ||
=== Performance characterization and validation === | === Performance characterization and validation === | ||
− | :* Data will be collected at both 1.5 and 3T. Data at 1.5T will be obtained with the protocol utilized for current project on lupus at UNM. | + | :* Data will be collected at both 1.5 and 3T. Data at 1.5T will be obtained with the protocol utilized for the current project on lupus at UNM. |
:* Data at 3T will be obtained with sequences optimized for segmentation by the group at Utah. | :* Data at 3T will be obtained with sequences optimized for segmentation by the group at Utah. | ||
:* Comparisons will be based on the approach developed by Martin-Fernandez et al. | :* Comparisons will be based on the approach developed by Martin-Fernandez et al. | ||
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* Sequence Optimization and Data Collection | * Sequence Optimization and Data Collection | ||
:* '''10/15/2007''' T1, T2, FLAIR optimized sequences for Siemens 3T Trio Tim scanner ('''Jeremy, Bruce, Chuck''') | :* '''10/15/2007''' T1, T2, FLAIR optimized sequences for Siemens 3T Trio Tim scanner ('''Jeremy, Bruce, Chuck''') | ||
− | :** | + | :** We will work with Bruce Fischl on using MEMPR, Mugler, and FLAIR sequences that have been optimized for maximum constrast and minimal geometric distortion across sequences |
:* '''11/15/2007''' collection of 5 lupus subjects on clinical sequence and optimized 3T sequence ('''Chuck''') | :* '''11/15/2007''' collection of 5 lupus subjects on clinical sequence and optimized 3T sequence ('''Chuck''') | ||
Revision as of 14:50, 27 September 2007
Home < DBP2:MIND:RoadmapBrain Lesion Analysis in Neuropsychiatric Systemic Lupus Erythematosus
Objective
We would like to create an end-to-end application within NA-MIC Kit allowing individual analysis of white matter lesions. Such a workflow applied to lupus patients is one of goals of the MIND DBP. This page describes the technology roadmap for lesion analysis in the NA-MIC Kit. The basic components necessary for this application are:
- Registration: co-registration of T1-weighted, T2-weighted, and FLAIR images
- Tissue segmentation: Should be multi-modality, correcting for intensity inhomogeneity and work on non-skull-stripped data.
- Lesion Localization: Each unique lesion should be detected and anatomical location summarized
- Lesion Load Measurement: Measure volume of each lesion, summarize lesion load by regions
- Tutorial: Documentation will be written for a tutorial and sample data sets will be provided
Roadmap
We will obtain gray matter, white matter, CSF, and lesion maps for each subject based on T1-weighted, T2-weighted, and FLAIR images. Ultimately, the NA-MIC Kit will provide a workflow for individual and group analysis of lesions. It will be implemented as a set of Slicer3 modules that can be used interactively within the Slicer3 application as well as in batch on a computing cluster using BatchMake.
The current status of the main modules to be used are:
Registration
- ITK has mutual information registration
- BRAINS2 has AIR package wrapped
Lesion segmentation
A number of algorithms for fully or semi-automated lesion analysis will be evaluated. These include:
- Tools developed at UNC known as itkEMS Compare Lesion Analysis Tools (Marcel)
- EM-segment (Sandy Wells)
- MedX (commercial package)
- BRAINS2 (Magnotta)
- Manual tracing by clinically trained rater
Lesion Localization
- Freesurfer has tools for labeling white matter lesions and summarizing their anatomical location
- BRAINS2 has tools for creating masks for white matter lesions and summarizing their anatomical location
Lesion Load Measurement
- Freesurfer has tools for measurement of labelled lesions
- BRAINS2 has tools for measurement of lesions and regional summaries
Performance characterization and validation
- Data will be collected at both 1.5 and 3T. Data at 1.5T will be obtained with the protocol utilized for the current project on lupus at UNM.
- Data at 3T will be obtained with sequences optimized for segmentation by the group at Utah.
- Comparisons will be based on the approach developed by Martin-Fernandez et al.
- The algorithm with the best performance will be incorporated into the NA-MIC kit.
Tutorial
- 5 Publically sharable T1,T2,Flair,Lesion Map data-sets (NIFTI format) will be made available
- A tutorial will be created that will guide end-users through each step needed to complete a lesion analysis in the NA-MIC kit
Schedule
- Sequence Optimization and Data Collection
- 10/15/2007 T1, T2, FLAIR optimized sequences for Siemens 3T Trio Tim scanner (Jeremy, Bruce, Chuck)
- We will work with Bruce Fischl on using MEMPR, Mugler, and FLAIR sequences that have been optimized for maximum constrast and minimal geometric distortion across sequences
- 11/15/2007 collection of 5 lupus subjects on clinical sequence and optimized 3T sequence (Chuck)
- 10/15/2007 T1, T2, FLAIR optimized sequences for Siemens 3T Trio Tim scanner (Jeremy, Bruce, Chuck)
- Registration
- 10/30/2007 optimized mutual information registration for clinical sequences and optimized 3T sequences (Jeremy)
- Lesion segmentation
- 11/30/2007 complete lesion segmentation methods for EM-segment, BRAINS2, manual, MedX, UNC packages (Jeremy, Chuck, Vince Magnotta, Kilian/Brad, Marcel)
- Lesion Localization
- 11/30/2007 complete lesion localizations and maps for EM-segment, BRAINS2, manual, MedX, UNC packages (Jeremy, Chuck, Vince Magnotta, Bruce, Steve)
- Lesion Measurement
- 11/30/2007 complete lesion measurements and regional lesion load summaries for EM-segment, BRAINS2, manual, MedX, UNC packages (Jeremy, Chuck, Vince Magnotta, Bruce, Steve)
- Performance characterization and validation
- 1/6/2008 report to 2008 NA-MIC AHM on performance and validation of lesion segmentation methods for EM-segment, BRAINS2, manual, MedX, UNC packages (Jeremy)
- 2/15/2008 submit manuscript on reliability and summary of novel NA-MIC kit lesion analysis method (Jeremy, Chuck, Mark Scully)
- 3/15/2008 analyze NIH study clinical sample using NA-MIC kit lesion analysis method (Jeremy, Chuck, Mark Scully)
- 4/15/2008 submit manuscript on clinical application of NA-MIC kit lesion analysis method (Jeremy, Chuck, Mark Scully, Carlos Roldan, Bill Sibbitt)
- Incorporation of approach into NA-MIC kit
- 11/1/2007 Slicer3 Lesion Analysis Module that handles co-registration of T1, T2, and Flair (Mark Scully, Steve)
- 12/1/2008 extend Slicer3 Lesion Analysis Module to handle lesion localization and measurement (Mark Scully, Steve)
- 1/6/2008 extend Slicer3 Lesion Analysis Module to implement the lesion analysis method (EM-segment, BRAINS2, MedX, UNC packages) with the best performance (Mark Scully, Steve)
- a demonstration will be given at the 2008 NA-MIC AHM--we would consider this version a prototype and would be testing, refining the module through the clinical application phase (Jeremy, Mark Scully)
- 4/1/2008 production version of lesion analysis Slicer3 Module complete (Mark Scully, Steve)
- Tutorial and Data-sharing
- 5/1/2008 make data sets and tutorial publically available (Jeremy, Sonja)
Team and Institute
- Co-PI: H Jeremy Bockholt (jbockholt at mrn.org)
- Co-PI: Charles Gasparovic (chuck at unm.edu)
- Software Engineer: Mark Scully (mscully at mrn .org)
- NA-MIC Engineering Contact: Steve Pieper, Isomics
- NA-MIC Algorithms Contact: Bruce Fischl, MGH
- Consultant: Vincent Magnotta, University of Iowa
- Host Institues: The MIND Institute and The University of New Mexico