ID | 116405 |
Author |
Morita, Akinori
Tokushima University
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Ochi, Shintaro
Tokushima University
Satoh, Hidetoshi
Tokyo University of Science
Ujita, Shohei
Tokushima University
Matsushita, Yosuke
Tokushima University|Nagasaki University
Tada, Kasumi
Tokushima University
Toyoda, Mihiro
Tokushima University
Mizuno, Kosuke
Tokyo University of Science
Deguchi, Yuichi
Nagasaki University
Suzuki, Keiji
Nagasaki University
Tanaka, Yoshimasa
Nagasaki University
Ueda, Hiroshi
Nagasaki University
Inaba, Toshiya
Hiroshima University
Hosoi, Yoshio
Tohoku University
Aoki, Shin
Tokyo University of Science
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Keywords | p53
RNA synthesis inhibitor
DNA intercalator
apoptosis
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Content Type |
Journal Article
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Description | RNA synthesis inhibitors and protein synthesis inhibitors are useful for investigating whether biological events with unknown mechanisms require transcription or translation; however, the dependence of RNA synthesis has been difficult to verify because many RNA synthesis inhibitors cause adverse events that trigger a p53 response. In this study, we screened a library containing 9600 core compounds and obtained STK160830 that shows anti-apoptotic effects in irradiated wild-type-p53-bearing human T-cell leukemia MOLT-4 cells and murine thymocytes. In many of the p53-impaired cells and p53-knockdown cells tested, STK160830 did not show a remarkable anti-apoptotic effect, suggesting that the anti-apoptotic activity is p53-dependent. In the expression analysis of p53, p53-target gene products, and reference proteins by immunoblotting, STK160830 down-regulated the expression of many of the proteins examined, and the downregulation correlated strongly with its inhibitory effect on cell death. mRNA expression analyses by qPCR and nascent RNA capture kit revealed that STK160830 showed a decreased mRNA expression, which was similar to that induced by the RNA synthesis inhibitor actinomycin D but differed to some extent. Furthermore, unlike other RNA synthesis inhibitors such as actinomycin D, p53 accumulation by STK160830 alone was negligible, and a DNA melting-curve analysis showed very weak DNA-intercalating activity, indicating that STK160830 is a useful inhibitor for RNA synthesis without triggering p53-mediated damage responses.
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Journal Title |
Life
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ISSN | 20751729
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Publisher | MDPI
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Volume | 11
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Issue | 10
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Start Page | 1087
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Published Date | 2021-10-15
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Rights | This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
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EDB ID | |
DOI (Published Version) | |
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language |
eng
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TextVersion |
Publisher
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departments |
Medical Sciences
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