Combinatorial Genetic Control of Rpd3S through histone H3K4 and H3K36 Methylation in Budding Yeast

Meneghini, Marc D.; Lee, Kwan Yin; Ranger, Mathieu

doi:10.1101/376046

“…Analysis of the 17 extragenic suppressors identified mutations in seven genes, all of which encode factors that regulate transcription elongation and chromatin ( Figure 2A). Four of these genes -SET2, RCO1, CHD1, and HTA1 -were previously identified as suppressors of either spt6 mutations or mutations that impair related elongation factors (Chu et al, 2006;Keogh et al, 2005;Lee et al, 2018;McCullough et al, 2015;Quan and Hartzog, 2010). As three of the genes, SET2, RCO1, and CHD1, are nonessential for viability, we tested complete deletions of each and found that they also suppressed spt6-YW, showing that suppression is conferred by loss of function (Table S2).…”

Section: Suppressors Of Spt6-yw Identify Important Transcription Elonmentioning

confidence: 93%

“…Spt16 and Pob3 are the two subunits of the histone chaperone FACT (Gurova et al, 2018), and Spt5 is a conserved elongation factor that interacts directly with RNAPII and has recently been implicated in controlling chromatin structure (Crickard et al, 2017;Ehara et al, 2019;Hartzog and Fu, 2013). The identification of spt6-YW suppressors in SPT16, POB3, and SPT5 was unexpected, as previously isolated mutations in these genes conferred similar, rather than opposite phenotypes as spt6 mutations (Cheung et al, 2008;Hainer et al, 2011;Hartzog et al, 1998;Jeronimo et al, 2019;Jeronimo et al, 2015;Kaplan et al, 2003;Lee et al, 2018;Malone et al, 1991;McCullough et al, 2015;Morillo-Huesca et al, 2010;Pathak et al, 2018;Swanson and Winston, 1992). The analysis of the FACT and Spt5 suppressors is the focus of the rest of these studies.…”

Section: Suppressors Of Spt6-yw Identify Important Transcription Elonmentioning

confidence: 99%

Essential histone chaperones collaborate to regulate transcription and chromatin integrity

Viktorovskaya

¹

,

Chuang

²

,

Jain

³

et al. 2020

Preprint

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Histone chaperones are critical for controlling chromatin integrity during transcription, DNA replication, and DNA repair. We have discovered that the physical interaction between two essential histone chaperones, Spt6 and Spn1/Iws1, is required for transcriptional accuracy and nucleosome organization. To understand this requirement, we have isolated suppressors of an spt6 mutation that disrupts the Spt6-Spn1 interaction. Several suppressors are in a third essential histone chaperone, FACT, while another suppressor is in the transcription elongation factor Spt5/DSIF. The FACT suppressors weaken FACT-nucleosome interactions and bypass the requirement for Spn1, possibly by restoring a necessary balance between Spt6 and FACT on chromatin. In contrast, the Spt5 suppressor modulates Spt6 function in a Spn1-dependent manner. Despite these distinct mechanisms, both suppressors alleviate the nucleosome organization defects caused by disruption of the Spt6-Spn1 interaction. Taken together, we have uncovered a network in which histone chaperones and other elongation factors coordinate transcriptional integrity and chromatin structure.

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“…2015) or that impair other chromatin-related factors, including FACT, Swi/Snf, Set2, and Rpd3S (Z hang et al . 2008; L ee et al . 2018b; V iktorovskaya et al .…”

Section: Introductionmentioning

confidence: 99%

Suppressor mutations that make the essential transcription factor Spn1/Iws1 dispensable in Saccharomyces cerevisiae

López-Rivera

¹

,

Chuang

²

,

Spatt

³

et al. 2022

Preprint

0

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Spn1/Iws1 is an essential eukaryotic transcription elongation factor that is conserved from yeast to humans as an integral member of the RNA polymerase II elongation complex. Several studies have shown that Spn1 functions as a histone chaperone to control transcription, RNA splicing, genome stability, and histone modifications. However, the precise role of Spn1 is not understood, and there is little understanding of why it is essential for viability. To address these issues, we have isolated eight suppressor mutations that bypass the essential requirement for Spn1 in Saccharomyces cerevisiae. Unexpectedly, the suppressors identify several functionally distinct complexes and activities, including the histone chaperone FACT, the histone methyltransferase Set2, the Rpd3S histone deacetylase complex, the histone acetyltransferase Rtt109, the nucleosome remodeler Chd1, and a member of the SAGA co-activator complex, Sgf73. The identification of these distinct groups suggests that there are multiple ways in which Spn1 bypass can occur, including changes in histone acetylation and alterations of other histone chaperones. Thus, Spn1 may function to overcome repressive chromatin by multiple mechanisms during transcription. Our results suggest that bypassing a subset of these functions allows viability in the absence of Spn1.

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“…Second, in vivo, a temperature-sensitive spn1 mutation, spn1-K192N (FISCHBECK et al 2002), causes changes in chromatin structure, resulting in altered spacing between nucleosomes and increased nucleosome fuzziness (VIKTOROVSKAYA et al 2021). Third, spn1-K192N is suppressed by mutations that alter histone H2A (MCCULLOUGH et al 2015) or that impair other chromatinrelated factors, including FACT, Swi/Snf, Set2, and Rpd3S (ZHANG et al 2008;LEE et al 2018b;VIKTOROVSKAYA et al 2021). Finally, spn1 mutations cause double mutant sickness or lethality when combined with mutations that impair other histone chaperones (LI et al 2018) or histone H3K4 methylation (LEE et al 2018a).…”

Section: Introductionmentioning

confidence: 99%

Suppressor mutations that make the essential transcription factor Spn1/Iws1 dispensable inSaccharomyces cerevisiae

López-Rivera

¹

,

Chuang

²

,

Spatt

³

et al. 2022

Genetics

4

0

View full text Add to dashboard Cite

Spn1/Iws1 is an essential eukaryotic transcription elongation factor that is conserved from yeast to humans as an integral member of the RNA polymerase II elongation complex. Several studies have shown that Spn1 functions as a histone chaperone to control transcription, RNA splicing, genome stability, and histone modifications. However, the precise role of Spn1 is not understood, and there is little understanding of why it is essential for viability. To address these issues, we have isolated eight suppressor mutations that bypass the essential requirement for Spn1 in Saccharomyces cerevisiae. Unexpectedly, the suppressors identify several functionally distinct complexes and activities, including the histone chaperone FACT, the histone methyltransferase Set2, the Rpd3S histone deacetylase complex, the histone acetyltransferase Rtt109, the nucleosome remodeler Chd1, and a member of the SAGA co-activator complex, Sgf73. The identification of these distinct groups suggests that there are multiple ways in which Spn1 bypass can occur, including changes in histone acetylation and alterations of other histone chaperones. Thus, Spn1 may function to overcome repressive chromatin by multiple mechanisms during transcription. Our results suggest that bypassing a subset of these functions allows viability in the absence of Spn1.

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Combinatorial Genetic Control of Rpd3S through histone H3K4 and H3K36 Methylation in Budding Yeast

Cited by 3 publications

References 41 publications

Essential histone chaperones collaborate to regulate transcription and chromatin integrity

Essential histone chaperones collaborate to regulate transcription and chromatin integrity

Suppressor mutations that make the essential transcription factor Spn1/Iws1 dispensable in Saccharomyces cerevisiae

Suppressor mutations that make the essential transcription factor Spn1/Iws1 dispensable inSaccharomyces cerevisiae

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