Welcome to the new version of CaltechAUTHORS. Login is currently restricted to library staff. If you notice any issues, please email coda@library.caltech.edu
CaltechAUTHORS
Published February 2014 | Supplemental Material + Published + Accepted Version
Journal Article Open

Pol II Docking and Pausing at Growth and Stress Genes in C. elegans

Maxwell, Colin S.
Kruesi, William S.
Core, Leighton J.
Kurhanewicz, Nicole
Waters, Colin T.
Lewarch, Caitlin L.
Antoshechkin, Igor ORCID icon
Lis, John T.
Meyer, Barbara J.
Baugh, L. Ryan

Abstract

Fluctuations in nutrient availability profoundly impact gene expression. Previous work revealed postrecruitment regulation of RNA polymerase II (Pol II) during starvation and recovery in Caenorhabditis elegans, suggesting that promoter-proximal pausing promotes rapid response to feeding. To test this hypothesis, we measured Pol II elongation genome wide by two complementary approaches and analyzed elongation in conjunction with Pol II binding and expression. We confirmed bona fide pausing during starvation and also discovered Pol II docking. Pausing occurs at active stress-response genes that become downregulated in response to feeding. In contrast, "docked" Pol II accumulates without initiating upstream of inactive growth genes that become rapidly upregulated upon feeding. Beyond differences in function and expression, these two sets of genes have different core promoter motifs, suggesting alternative transcriptional machinery. Our work suggests that growth and stress genes are both regulated postrecruitment during starvation but at initiation and elongation, respectively, coordinating gene expression with nutrient availability.

Additional Information

© 2014 The Authors. Published by Elsevier Inc. Received: May 20, 2013. Revised: November 1, 2013. Accepted: January 6, 2014. Published: January 30, 2014. This is an open-access article distributed under the terms of the Creative Commons Attribution-NonCommercial-No Derivative Works License, which permits non-commercial use, distribution, and reproduction in any medium, provided the original author and source are credited. We thank Sergei Nechaev for providing protocols and advice for scRNA-seq. Some strains were provided by the CGC, which is funded by NIH Office of Research Infrastructure Programs (P40 OD010440). The Ellison Medical Foundation and the National Science Foundation (IOS-1120206) supported this work.

Attached Files

Published - 1-s2.0-S2211124714000096-main.pdf

Accepted Version - nihms579102.pdf

Supplemental Material - mmc1.pdf

Supplemental Material - mmc2.zip

Supplemental Material - mmc3.zip

Files

nihms579102.pdf
Files (14.0 MB)
Name Size Download all
md5:c3d5454bb812d5ab1aada8c8f9f3eaa7
2.1 MB Preview Download
md5:db39a0d3e01e1afdad6e0451c33cf452
408.1 kB Preview Download
md5:ed9921feec0cc4dcf163bd489e619742
2.7 MB Preview Download
md5:524f15e3c1f4d9ce451bc53ca8e37c89
2.1 kB Preview Download
md5:e2372446938333022c4d4a8c7eaabc50
8.9 MB Preview Download

Additional details

Identifiers Funding Dates
Created:
August 19, 2023
Modified:
October 25, 2023