A Pliable Mediator Acts as a Functional Rather Than an Architectural Bridge between Promoters and Enhancers | Zendy

Laïla El Khattabi | Zendy; Haiyan Zhao | Zendy; Jens Kalchschmidt | Zendy; Natalie Young | Zendy; Seolkyoung Jung | Zendy; Peter Van Blerkom | Zendy; Philippe Kieffer-Kwon | Zendy; Kyong-Rim Kieffer-Kwon | Zendy; Solji Park | Zendy; Xiang Wang | Zendy; Jordan Krebs | Zendy; Subhash Tripathi | Zendy; Noboru J. Sakabe | Zendy; Débora R. Sobreira | Zendy; SuChen Huang | Zendy; Suhas S.P. Rao | Zendy; Nathanael Pruett | Zendy; Daniel Chauss | Zendy; Erica C. Sadler | Zendy; Á. López | Zendy; Marcelo A. Nóbrega | Zendy; E Aiden | Zendy; Francisco J. Asturias | Zendy; Rafael Casellas | Zendy

AI Assistant Blog Pricing

Home ZAIA Blog

Open Access

A Pliable Mediator Acts as a Functional Rather Than an Architectural Bridge between Promoters and Enhancers

Author(s) -

Laïla El Khattabi,

Haiyan Zhao,

Jens Kalchschmidt,

Natalie Young,

Seolkyoung Jung,

Peter Van Blerkom,

Philippe Kieffer-Kwon,

Kyong-Rim Kieffer-Kwon,

Solji Park,

Xiang Wang,

Jordan Krebs,

Subhash Tripathi,

Noboru J. Sakabe,

Débora R. Sobreira,

SuChen Huang,

Suhas S.P. Rao,

Nathanael Pruett,

Daniel Chauss,

Erica C. Sadler,

Á. López,

Marcelo A. Nóbrega,

E Aiden,

Francisco J. Asturias,

Rafael Casellas

Publication year - 2019

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2019.07.011

Subject(s) - biology , enhancer , mediator , promoter , microbiology and biotechnology , transcription factor , crispr , transcription (linguistics) , dna , degron , genetics , protein subunit , computational biology , gene , gene expression , ubiquitin ligase , linguistics , philosophy , ubiquitin

While Mediator plays a key role in eukaryotic transcription, little is known about its mechanism of action. This study combines CRISPR-Cas9 genetic screens, degron assays, Hi-C, and cryoelectron microscopy (cryo-EM) to dissect the function and structure of mammalian Mediator (mMED). Deletion analyses in B, T, and embryonic stem cells (ESC) identified a core of essential subunits required for Pol II recruitment genome-wide. Conversely, loss of non-essential subunits mostly affects promoters linked to multiple enhancers. Contrary to current models, however, mMED and Pol II are dispensable to physically tether regulatory DNA, a topological activity requiring architectural proteins. Cryo-EM analysis revealed a conserved core, with non-essential subunits increasing structural complexity of the tail module, a primary transcription factor target. Changes in tail structure markedly increase Pol II and kinase module interactions. We propose that Mediator's structural pliability enables it to integrate and transmit regulatory signals and act as a functional, rather than an architectural bridge, between promoters and enhancers.

The content you want is available to Zendy users.

Already have an account? Click here to sign in.

Having issues? You can contact us here

Accelerating Research