Abstract

EXCEED THE SPACE PROVIDED. High resolution imaging is becoming an invaluable tool in biomedicalresearch much as it has to the clinician. In the clinic, imaging offers a precise, non-invasive means of diagnosis and directly influences both the therapeutic approach and prognosis. Unfortunately, the developmentof high-resolution imaging tools demandedby researchers has lagged behind that of the clinic; thus, characterization of the kinetics of in vivo pathology and the subsequent development of novel, effective therapeutics has been hampered. This is particularly true in the field of amyloid- related diseases which include Alzheimer's disease, type I1 diabetes and primary (AL) amyloidosis. It is impossible to fully appreciate and understand the complexityof these diseases, and the means by which they may be halted, without the ability to perform longitudinal studies in individual animals in vivo. To that end, the developmenthigh- resolution micro-imaging technologies capable of detecting and quantifying amyloid deposits in vivo is warranted and imperative. We intend to address these important issues through the design and application of a powerful new dual-modality imagingtechnology, microSPECT, combined with microCT, supported by state-of-the-art3-D image reconstruction and analysis software. This new technology will be employed to identify radiolabeled amyloid ldeposits in live animals and present the amyloiddistribution within the context of a high-resolution CT image of the 1visceral terrain. With this technology, the goal of quantifying organ-specific amyloid burden in vivo is attainable. IThe goals are thus to: (i) Complete the design and implementation of a high-resolution, small-animal speciJic dual lSPECT/CT imaging system. (ii). Develop a system of amyloid quantijkation in which microSPECT image data can be directly correlated to amyloid burden. (iii) Use these technologies to study the progression of systemic AA- amyloidosis in two murine models and the regression thereof in response to novel immunotherapies. This study will not only result in technological advancements in the field of small-animal imaging and amyloid-specific radio- tracers but will also provide a wealth of information on the natural progression of amyloidosis in vivo and establish a paradigm for the screening of therapeutic drugs in animal models of human disease. Furthermore, the translation of amyloid-specificimagingtechnologies will yield tangible clinicalbenefit. PERFORMANCESITE( ========================================Section End===========================================

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Biomedical Imaging and Bioengineering (NIBIB)
Type
Research Project (R01)
Project #
5R01EB000789-04
Application #
6937798
Study Section
Special Emphasis Panel (ZRG1-SRB (03))
Program Officer
Mclaughlin, Alan Charles
Project Start
2002-09-01
Project End
2007-08-31
Budget Start
2005-09-01
Budget End
2007-08-31
Support Year
4
Fiscal Year
2005
Total Cost
$945,071
Indirect Cost

  Institution

Name
University of Tennessee Knoxville
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
003387891
City
Knoxville
State
TN
Country
United States
Zip Code
37996

  Publications

Gregor, Jens; Benson, Thomas (2008) Computational analysis and improvement of SIRT. IEEE Trans Med Imaging 27:918-24
Wall, Jonathan S; Richey, Tina; Allen, Amy et al. (2008) Quantitative tomography of early-onset spontaneous AA amyloidosis in interleukin 6 transgenic mice. Comp Med 58:542-50
O'Nuallain, Brian; Allen, Amy; Ataman, Demet et al. (2007) Phage display and peptide mapping of an immunoglobulin light chain fibril-related conformational epitope. Biochemistry 46:13049-58
O'Nuallain, Brian; Allen, Amy; Kennel, Stephen J et al. (2007) Localization of a conformational epitope common to non-native and fibrillar immunoglobulin light chains. Biochemistry 46:1240-7
O'Nuallain, Brian; Hrncic, Rudi; Wall, Jonathan S et al. (2006) Diagnostic and therapeutic potential of amyloid-reactive IgG antibodies contained in human sera. J Immunol 176:7071-8
Price, Jeffrey R; Aykac, Deniz; Wall, Jonathan (2006) A 3D level sets method for segmenting the mouse spleen and follicles in volumetric microCT images. Conf Proc IEEE Eng Med Biol Soc 1:2332-6
Benson, T M; Gregor, J (2006) Three-dimensional focus of attention for iterative cone-beam micro-CT reconstruction. Phys Med Biol 51:4533-46
Wall, Jonathan S; Kennel, Stephen J; Paulus, Mike et al. (2006) Radioimaging of light chain amyloid with a fibril-reactive monoclonal antibody. J Nucl Med 47:2016-24
Wall, Jonathan S; Paulus, Michael J; Gleason, Shaun et al. (2006) Micro-imaging of amyloid in mice. Methods Enzymol 412:161-82
Wall, Jonathan S; Kennel, Stephen J; Paulus, Michael J et al. (2005) Quantitative high-resolution microradiographic imaging of amyloid deposits in a novel murine model of AA amyloidosis. Amyloid 12:149-56