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Park, Tae Joo
Morphogenesis Lab.
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Xenopus: An alternative model system for identifying muco-active agents.

Author(s)
Sim, Hyo JungKim, SMyung, KKwon, TLee, HPark, Tae Joo
Issued Date
2018-08-14
URI
https://scholarworks.unist.ac.kr/handle/201301/81057
Citation
17th International Xenopus conference
Abstract
The airway epithelium in human plays a central role as the first line of defense against environmental contaminants. Most respiratory diseases such as chronic obstructive pulmonary disease (COPD), asthma, and respiratory infections, disturb normal muco-ciliary functions by stimulating the hypersecretion of mucus. Several muco-active agents have been used to treat hypersecretion symptoms in patients. Current muco-active reagents control mucus secretion by modulating either airway inflammation, cholinergic parasympathetic nerve activities or by reducing the viscosity by cleaving crosslinking in mucin and digesting DNAs in mucus. However, none of the current medication regulates mucus secretion by directly targeting airway goblet cells. The major hurdle for screening potential muco-active agents that directly affect the goblet cells, is the unavailability of in vivo model systems suitable for high-throughput screening. In this study, we developed a high-throughput in vivo model system for identifying muco-active reagents using Xenopus laevis embryos. We tested mucus secretion under various conditions and developed a screening strategy to identify potential muco-regulators. Using this novel screening technique, we identified narasin as a potential muco-regulator. Narasin treatment of developing Xenopus embryos significantly reduced mucus secretion. Furthermore, the human lung epithelial cell line, Calu-3, responded similarly to narasin treatment, validating our technique for discovering muco-active reagents. In addition, we figured out diesel particulated matter hindered mucus secretion and α-tocopherol recovered this symptom.
Publisher
Genetics Society of America

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