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3 research outputs found

PHF3 regulates neuronal gene expression through the Pol II CTD reader domain SPOC

Author: Akalin Altuna
Appel Lisa-Marie
Beltzung Etienne
Bernecky Carrie A
Bruno Melania
Djinovic-Carugo Kristina
Ebenwaldner Carmen
Franke Vedran
Grishkovskaya Irina
Kasiliauskaite Aiste
Kaufmann Tanja
Kostrhon Sebastian
Leeb Martin
Lin Gen
Mechtler Karl
Pavri Rushad
Puchinger Martin G.
Schoeberl Ursula E.
Sebesta Marek
Slade Dea
Stark Alexander
Stefl Richard
Vlasova Anna
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2021
Field of study

The C-terminal domain (CTD) of the largest subunit of RNA polymerase II (Pol II) is a regulatory hub for transcription and RNA processing. Here, we identify PHD-finger protein 3 (PHF3) as a regulator of transcription and mRNA stability that docks onto Pol II CTD through its SPOC domain. We characterize SPOC as a CTD reader domain that preferentially binds two phosphorylated Serine-2 marks in adjacent CTD repeats. PHF3 drives liquid-liquid phase separation of phosphorylated Pol II, colocalizes with Pol II clusters and tracks with Pol II across the length of genes. PHF3 knock-out or SPOC deletion in human cells results in increased Pol II stalling, reduced elongation rate and an increase in mRNA stability, with marked derepression of neuronal genes. Key neuronal genes are aberrantly expressed in Phf3 knock-out mouse embryonic stem cells, resulting in impaired neuronal differentiation. Our data suggest that PHF3 acts as a prominent effector of neuronal gene regulation by bridging transcription with mRNA decay

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IST Austria: PubRep (Institute of Science and Technology)

Cooperation between intrinsically disordered and ordered regions of Spt6 regulates nucleosome and Pol II CTD binding, and nucleosome assembly

Author: Kasiliauskaite Aiste
Klumpler Tomas
Koutna Eliska
Kubicek Karel
Novacek Jiri
Stefl Richard
Zanova Martina
Zapletal David
Publication venue: Information Retrieval Ltd.
Publication date: 01/01/2022
Field of study

Transcription elongation factor Spt6 associates with RNA polymerase II (Pol II) and acts as a histone chaperone, which promotes the reassembly of nucleosomes following the passage of Pol II. The precise mechanism of nucleosome reassembly mediated by Spt6 remains unclear. In this study, we used a hybrid approach combining cryo-electron microscopy and small-angle X-ray scattering to visualize the architecture of Spt6 from Saccharomyces cerevisiae. The reconstructed overall architecture of Spt6 reveals not only the core of Spt6, but also its flexible N- and C-termini, which are critical for Spt6’s function. We found that the acidic N-terminal region of Spt6 prevents the binding of Spt6 not only to the Pol II CTD and Pol II CTD-linker, but also to pre-formed intact nucleosomes and nucleosomal DNA. The N-terminal region of Spt6 self-associates with the tSH2 domain and the core of Spt6 and thus controls binding to Pol II and nucleosomes. Furthermore, we found that Spt6 promotes the assembly of nucleosomes in vitro. These data indicate that the cooperation between the intrinsically disordered and structured regions of Spt6 regulates nucleosome and Pol II CTD binding, and also nucleosome assembly

PubMed Central

DESY

Yeast Spt6 Reads Multiple Phosphorylation Patterns of RNA Polymerase II C-Terminal Domain In Vitro

Crossref