Difference between revisions of "Projects:ShapeAnalysisFrameworkUsingSPHARMPDM"

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''In Print''
 
''In Print''
* [http://www.na-mic.org/pages/Special:Publications?text=Projects%3AShapeAnalysisFrameworkUsingSPHARMPDM&submit=Search&words=all&title=checked&keywords=checked&authors=checked&abstract=checked&sponsors=checked&searchbytag=checked| NA-MIC Publications Database]
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* [http://www.na-mic.org/pages/Special:Publications?text=SPHARMPDM&submit=Search&words=all&title=checked&keywords=checked&authors=checked&abstract=checked&sponsors=checked&searchbytag=checked| NA-MIC Publications Database]
  
 
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Revision as of 14:29, 25 April 2008

Home < Projects:ShapeAnalysisFrameworkUsingSPHARMPDM
Back to NA-MIC Collaborations, UNC Algorithms, Utah Algorithms

Shape Analysis Framework using SPHARM-PDM

UNCShape OverviewAnalysis MICCAI06.gif

The UNC shape analysis is based on an analysis framework of objects with spherical topology, described by sampled spherical harmonics SPHARM-PDM. In summary, the input of the proposed shape analysis is a set of binary segmentation of a single brain structure, such as the hippocampus or caudate. These segmentations are first processed to fill any interior holes and a minimal smoothing operation. The processed binary segmentations are converted to surface meshes, and a spherical parametrization is computed for the surface meshes using a area-preserving, distortion minimizing spherical mapping. The SPHARM description is computed from the mesh and its spherical parametrization. Using the first order ellipsoid from the spherical harmonic coefficients, the spherical parametrizations are aligned to establish correspondence across all surfaces. The SPHARM description is then sampled into a triangulated surfaces (SPHARM-PDM) via icosahedron subdivision of the spherical parametrization. These SPHARM-PDM surfaces are all spatially aligned using rigid Procrustes alignment. Group differences between groups of surfaces are computed using the standard robust Hotelling T 2 two sample metric (see below). Statistical p-values, both raw and corrected for multiple comparisons, result in significance maps. Additional visualization of the group tests are provided via mean difference magnitude and vector maps, as well as maps of the group covariance information.

The implementation has reached a stable framework and has been disseminated to several collaborating labs within NAMIC (BWH, GeorgiaTech, Utah). The current development focuses on integrating the current command line tools into the Slicer (v3) via the Slicer execution model.

Description

A considerable amount of work was spent on the development aspect of our shape analysis tools. The main visualization tool, KWMeshVisu, can be called directly from Slicer 3 for the overlay of scalar, vector and ellipsoid data onto surfaces (so-called attribution) and the application of a set of versatile colormaps. The display of a saved "attributed" surfaces is then again possible within Slicer 3 to close the loop. This lean visualization tool fills a niche and is also used in our cortical thickness analysis tool.

The individual shape analysis components have also been integrated into Slicer 3 modules. While it is entirely possible to run all steps of our shape analysis pipeline by calling the individual modules, this is highly inefficient. As a result we are developing, and a first prototype is ready, a separate shape pipeline tool to called from within Slicer3. This tool creates pipeline scripts for Batchmake, another NAMIC supported project at Kitware, to run the shape analysis pipeline as a distributed, background process. The whole shape analysis pipeline thus becomes entirely encapsulated and accessible to the trained clinical collaborator.

The current toolset distribution (via NeuroLib) now also contains open data for other researchers to evaluate novel shape analysis enhancements.

Key Investigators

  • UNC Algorithms: Martin Styner, Ipek Oguz, Christine Xu
  • Utah Algorithms: Guido Gerig

Publications

In Print

Links

Project Week Results: Jun 2005-1, Jun 2005-2, Jun 2005-3, Jan 2006-1, Jan 2006-2, Jun 2006, Jan 2007-1, Jan 2007-2