Establishment of the expression system for studying the function of active caspase-3 in zebrafish |
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Authors: | Kim Ho-Young Kim Goo-Young Kim Sang-Soo Nam Min-Kyung Rhim Hyangshuk |
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Affiliation: | (1) Department of Biomedical Sciences, The Catholic University of Korea, Seoul, 137-701, Korea;(2) Research Institute of Molecular Genetics, College of Medicine, The Catholic University of Korea, Seoul, 137-701, Korea |
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Abstract: | Caspase-3, a key molecule in apoptosis, has been extensively studied in cell culture system; however, it has been less well characterized in vivo because certain mediators are required for the proteolytic activation of effector caspases, including caspase-3. In this study, various forms of caspase-3 with the C-terminal GFP tag were inserted into the pCS2+ plasmid, and the expression patterns of caspase-3 proteins were characterized in a zebrafish model system using microinjection of nucleic acids into zebrafish embryos. We have verified that active caspase-3 was generated by its autocatalytic activity under the condition of caspase-2 prodomain (C2P)-caspase-3-GFP overexpression, indicating that the C2P domain is crucial for the activation of caspase-3. We also confirmed that the C2P domain plays an important role in regulating the nuclear localization of the C2P-caspase-3 chimeric protein. We used this expression system to establish an animal model system suitable for the investigation of the functional characteristics of caspase-3 in vivo. Thus, our study provides a useful and specific tool for investigating the molecular mechanisms by which active caspase-3 regulates apoptosis during embryonic development. |
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Keywords: | Apoptosis Caspase-3 Microinjection Zebrafish |
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