Direct Regulation of tRNA and 5S rRNA Gene Transcription by Polo-like Kinase 1

J.A. Fairley; L.E. Mitchell; T. Berg; N.S. Kenneth; C. von Schubert; E.A. Nigg; H.H.W. Silljé; R.H. Medema; R.J. White

doi:10.1016/j.molcel.2011.11.030

Direct Regulation of tRNA and 5S rRNA Gene Transcription by Polo-like Kinase 1

J.A. Fairley, L.E. Mitchell, T. Berg, N.S. Kenneth, C. von Schubert, E.A. Nigg, H.H.W. Silljé, R.H. Medema, R.J. White

Biology

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

Abstract

Polo-like kinase Plk1 controls numerous aspects of cell-cycle progression. We show that it associates with tRNA and 5S rRNA genes and regulates their transcription by RNA polymerase III (pol III) through direct binding and phosphorylation of transcription factor Brf1. During interphase, Plk1 promotes tRNA and 5S rRNA expression by phosphorylating Brf1 directly on serine 450. However, this stimulatory modification is overridden at mitosis, when elevated Plk1 activity causes Brf1 phosphorylation on threonine 270 (T270), which prevents pol III recruitment. Thus, although Plk1 enhances net tRNA and 5S rRNA production, consistent with its proliferation-stimulating function, it also suppresses untimely transcription when cells divide. Genomic instability is apparent in cells with Brf1 T270 mutated to alanine to resist Plk1-directed inactivation, suggesting that chromosome segregation is vulnerable to inappropriate pol III activity.

Original language	English
Pages (from-to)	541-552
Number of pages	12
Journal	Molecular Cell
Volume	45
Issue number	4
DOIs	https://doi.org/10.1016/j.molcel.2011.11.030
Publication status	Published - 24 Feb 2012

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title = "Direct Regulation of tRNA and 5S rRNA Gene Transcription by Polo-like Kinase 1",

abstract = "Polo-like kinase Plk1 controls numerous aspects of cell-cycle progression. We show that it associates with tRNA and 5S rRNA genes and regulates their transcription by RNA polymerase III (pol III) through direct binding and phosphorylation of transcription factor Brf1. During interphase, Plk1 promotes tRNA and 5S rRNA expression by phosphorylating Brf1 directly on serine 450. However, this stimulatory modification is overridden at mitosis, when elevated Plk1 activity causes Brf1 phosphorylation on threonine 270 (T270), which prevents pol III recruitment. Thus, although Plk1 enhances net tRNA and 5S rRNA production, consistent with its proliferation-stimulating function, it also suppresses untimely transcription when cells divide. Genomic instability is apparent in cells with Brf1 T270 mutated to alanine to resist Plk1-directed inactivation, suggesting that chromosome segregation is vulnerable to inappropriate pol III activity.",

author = "J.A. Fairley and L.E. Mitchell and T. Berg and N.S. Kenneth and {von Schubert}, C. and E.A. Nigg and H.H.W. Sillj{\'e} and R.H. Medema and R.J. White",

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T1 - Direct Regulation of tRNA and 5S rRNA Gene Transcription by Polo-like Kinase 1

AU - Fairley, J.A.

AU - Mitchell, L.E.

AU - Berg, T.

AU - Kenneth, N.S.

AU - von Schubert, C.

AU - Nigg, E.A.

AU - Silljé, H.H.W.

AU - Medema, R.H.

AU - White, R.J.

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N2 - Polo-like kinase Plk1 controls numerous aspects of cell-cycle progression. We show that it associates with tRNA and 5S rRNA genes and regulates their transcription by RNA polymerase III (pol III) through direct binding and phosphorylation of transcription factor Brf1. During interphase, Plk1 promotes tRNA and 5S rRNA expression by phosphorylating Brf1 directly on serine 450. However, this stimulatory modification is overridden at mitosis, when elevated Plk1 activity causes Brf1 phosphorylation on threonine 270 (T270), which prevents pol III recruitment. Thus, although Plk1 enhances net tRNA and 5S rRNA production, consistent with its proliferation-stimulating function, it also suppresses untimely transcription when cells divide. Genomic instability is apparent in cells with Brf1 T270 mutated to alanine to resist Plk1-directed inactivation, suggesting that chromosome segregation is vulnerable to inappropriate pol III activity.

AB - Polo-like kinase Plk1 controls numerous aspects of cell-cycle progression. We show that it associates with tRNA and 5S rRNA genes and regulates their transcription by RNA polymerase III (pol III) through direct binding and phosphorylation of transcription factor Brf1. During interphase, Plk1 promotes tRNA and 5S rRNA expression by phosphorylating Brf1 directly on serine 450. However, this stimulatory modification is overridden at mitosis, when elevated Plk1 activity causes Brf1 phosphorylation on threonine 270 (T270), which prevents pol III recruitment. Thus, although Plk1 enhances net tRNA and 5S rRNA production, consistent with its proliferation-stimulating function, it also suppresses untimely transcription when cells divide. Genomic instability is apparent in cells with Brf1 T270 mutated to alanine to resist Plk1-directed inactivation, suggesting that chromosome segregation is vulnerable to inappropriate pol III activity.

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JO - Molecular Cell

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Direct Regulation of tRNA and 5S rRNA Gene Transcription by Polo-like Kinase 1

Abstract

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