Autor: |
Zhang, Liang, Wang, Yuzhen, Homan, Kristoff T., Gaudette, Stephanie M., McCluskey, Andrew J., Chan, Ying, Murphy, Joanne, Abdalla, Mary, Nelson, Christine M., Sun, Victor Z., Erickson, Jamie E., Knight, Heather L., Clabbers, Anca, Sterman, Annette J. Schwartz, Mitra, Soumya |
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Zdroj: |
Molecular Imaging & Biology; Apr2023, Vol. 25 Issue 2, p314-323, 10p |
Abstrakt: |
Purpose: To image colon-expressed alternatively spliced D domain of tenascin C in preclinical colitis models using near infrared (NIR)-labeled targeted molecular imaging agents. Procedures. A human IgG1 with nanomolar binding affinity specific to the alternatively spliced D domain of tenascin C was generated. Immunohistochemistry identified disease-specific expression of this extracellular matrix protein in the colon of mice given dextran sulfate sodium in the drinking water. The antibody reagent was labeled with the NIR fluorophore IRDye 800CW via amine chemistry and intravenously dosed to evaluate in vivo targeting specificity. Increasing doses of imaging agent were given to estimate the saturating dose. Results: The NIR-labeled proteins successfully targeted colonic lesions in a murine model of colitis. Co-administration of a molar excess competing unlabeled dose reduced normalized uptake in diseased colon by > 70%. Near infrared ex vivo images of colon resected from diseased animals showed saturation at doses exceeding 1 nmol and was confirmed with additional quantitative ex vivo biodistribution. Cellular-level specificity and protein stability were assessed via microscopy. Conclusions: Our imaging data suggest the alternatively spliced D domain of tenascin C is a promising target for delivery-based applications in inflammatory bowel diseases. [ABSTRACT FROM AUTHOR] |
Databáze: |
Complementary Index |
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