Reduced expression of Sytl 1 and Ccdc21 and impaired induction of Mt I by oxidative stress in SII-K1 knockout mice

K. Tano; H. Hamamoto; T. Ito; E. Sumiya; R. Rakwal; J. Shibato; Y. Masuo; K. Ijiri; K. Sekimizu; N. Akimitsu

Reduced expression of Sytl 1 and Ccdc21 and impaired induction of Mt I by oxidative stress in SII-K1 knockout mice

K. Tano, H. Hamamoto, T. Ito, E. Sumiya, R. Rakwal, J. Shibato, Y. Masuo, K. Ijiri, K. Sekimizu, N. Akimitsu

Research output: Contribution to journal › Article › peer-review

Abstract

SII-K1 is a member of the transcription elongation factor S-II family. In the mouse, SII-K1 is expressed exclusively in the liver, kidney, heart, and skeletal muscle. Here, we report that deletion of the SII-K1 gene in mice resulted in the downregulation of the synaptotagmin-like 1 (Sytl 1) gene in liver and of the coiled-coil domain-containing 21 (Ccdc21) gene in liver and kidney. Moreover, the induction of the metallothionein I (Mt I) gene in SII-K1-deficient mice liver was impaired in diethyl maleate-induced oxidative stress conditions. Our results suggest that SII-K1 regulates these genes in vivo.

Original language	English
Pages (from-to)	368-372
Number of pages	5
Journal	Drug discoveries & therapeutics
Volume	4
Issue number	5
Publication status	Published - Oct 1 2010
Externally published	Yes

All Science Journal Classification (ASJC) codes

Medicine(all)

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title = "Reduced expression of Sytl 1 and Ccdc21 and impaired induction of Mt I by oxidative stress in SII-K1 knockout mice",

abstract = "SII-K1 is a member of the transcription elongation factor S-II family. In the mouse, SII-K1 is expressed exclusively in the liver, kidney, heart, and skeletal muscle. Here, we report that deletion of the SII-K1 gene in mice resulted in the downregulation of the synaptotagmin-like 1 (Sytl 1) gene in liver and of the coiled-coil domain-containing 21 (Ccdc21) gene in liver and kidney. Moreover, the induction of the metallothionein I (Mt I) gene in SII-K1-deficient mice liver was impaired in diethyl maleate-induced oxidative stress conditions. Our results suggest that SII-K1 regulates these genes in vivo.",

author = "K. Tano and H. Hamamoto and T. Ito and E. Sumiya and R. Rakwal and J. Shibato and Y. Masuo and K. Ijiri and K. Sekimizu and N. Akimitsu",

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T1 - Reduced expression of Sytl 1 and Ccdc21 and impaired induction of Mt I by oxidative stress in SII-K1 knockout mice

AU - Tano, K.

AU - Hamamoto, H.

AU - Ito, T.

AU - Sumiya, E.

AU - Rakwal, R.

AU - Shibato, J.

AU - Masuo, Y.

AU - Ijiri, K.

AU - Sekimizu, K.

AU - Akimitsu, N.

PY - 2010/10/1

Y1 - 2010/10/1

N2 - SII-K1 is a member of the transcription elongation factor S-II family. In the mouse, SII-K1 is expressed exclusively in the liver, kidney, heart, and skeletal muscle. Here, we report that deletion of the SII-K1 gene in mice resulted in the downregulation of the synaptotagmin-like 1 (Sytl 1) gene in liver and of the coiled-coil domain-containing 21 (Ccdc21) gene in liver and kidney. Moreover, the induction of the metallothionein I (Mt I) gene in SII-K1-deficient mice liver was impaired in diethyl maleate-induced oxidative stress conditions. Our results suggest that SII-K1 regulates these genes in vivo.

AB - SII-K1 is a member of the transcription elongation factor S-II family. In the mouse, SII-K1 is expressed exclusively in the liver, kidney, heart, and skeletal muscle. Here, we report that deletion of the SII-K1 gene in mice resulted in the downregulation of the synaptotagmin-like 1 (Sytl 1) gene in liver and of the coiled-coil domain-containing 21 (Ccdc21) gene in liver and kidney. Moreover, the induction of the metallothionein I (Mt I) gene in SII-K1-deficient mice liver was impaired in diethyl maleate-induced oxidative stress conditions. Our results suggest that SII-K1 regulates these genes in vivo.

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SN - 1881-7831

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ER -

Reduced expression of Sytl 1 and Ccdc21 and impaired induction of Mt I by oxidative stress in SII-K1 knockout mice

Abstract

All Science Journal Classification (ASJC) codes

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