Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects

To better understand telomere biology in budding yeast, we have performed systematic suppressor/enhancer analyses on yeast strains containing a point mutation in the essential telomere capping gene CDC13 (cdc13-1) or containing a null mutation in the DNA damage response and telomere capping gene YKU...

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Autores principales: Addinall, Stephen Gregory, Holstein, Eva-Maria, Lawless, Conor, Yu, Min, Chapman, Kaye, Banks, A. Peter, Ngo, Hien-Ping, Maringele, Laura, Taschuk, Morgan, Young, Alexander, Ciesiolka, Adam, Lister, Allyson Lurena, Wipat, Anil, Wilkinson, Darren James, Lydall, David
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3072368/
https://www.ncbi.nlm.nih.gov/pubmed/21490951
http://dx.doi.org/10.1371/journal.pgen.1001362
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author Addinall, Stephen Gregory
Holstein, Eva-Maria
Lawless, Conor
Yu, Min
Chapman, Kaye
Banks, A. Peter
Ngo, Hien-Ping
Maringele, Laura
Taschuk, Morgan
Young, Alexander
Ciesiolka, Adam
Lister, Allyson Lurena
Wipat, Anil
Wilkinson, Darren James
Lydall, David
author_facet Addinall, Stephen Gregory
Holstein, Eva-Maria
Lawless, Conor
Yu, Min
Chapman, Kaye
Banks, A. Peter
Ngo, Hien-Ping
Maringele, Laura
Taschuk, Morgan
Young, Alexander
Ciesiolka, Adam
Lister, Allyson Lurena
Wipat, Anil
Wilkinson, Darren James
Lydall, David
author_sort Addinall, Stephen Gregory
collection PubMed
description To better understand telomere biology in budding yeast, we have performed systematic suppressor/enhancer analyses on yeast strains containing a point mutation in the essential telomere capping gene CDC13 (cdc13-1) or containing a null mutation in the DNA damage response and telomere capping gene YKU70 (yku70Δ). We performed Quantitative Fitness Analysis (QFA) on thousands of yeast strains containing mutations affecting telomere-capping proteins in combination with a library of systematic gene deletion mutations. To perform QFA, we typically inoculate 384 separate cultures onto solid agar plates and monitor growth of each culture by photography over time. The data are fitted to a logistic population growth model; and growth parameters, such as maximum growth rate and maximum doubling potential, are deduced. QFA reveals that as many as 5% of systematic gene deletions, affecting numerous functional classes, strongly interact with telomere capping defects. We show that, while Cdc13 and Yku70 perform complementary roles in telomere capping, their genetic interaction profiles differ significantly. At least 19 different classes of functionally or physically related proteins can be identified as interacting with cdc13-1, yku70Δ, or both. Each specific genetic interaction informs the roles of individual gene products in telomere biology. One striking example is with genes of the nonsense-mediated RNA decay (NMD) pathway which, when disabled, suppress the conditional cdc13-1 mutation but enhance the null yku70Δ mutation. We show that the suppressing/enhancing role of the NMD pathway at uncapped telomeres is mediated through the levels of Stn1, an essential telomere capping protein, which interacts with Cdc13 and recruitment of telomerase to telomeres. We show that increased Stn1 levels affect growth of cells with telomere capping defects due to cdc13-1 and yku70Δ. QFA is a sensitive, high-throughput method that will also be useful to understand other aspects of microbial cell biology.
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spelling pubmed-30723682011-04-13 Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects Addinall, Stephen Gregory Holstein, Eva-Maria Lawless, Conor Yu, Min Chapman, Kaye Banks, A. Peter Ngo, Hien-Ping Maringele, Laura Taschuk, Morgan Young, Alexander Ciesiolka, Adam Lister, Allyson Lurena Wipat, Anil Wilkinson, Darren James Lydall, David PLoS Genet Research Article To better understand telomere biology in budding yeast, we have performed systematic suppressor/enhancer analyses on yeast strains containing a point mutation in the essential telomere capping gene CDC13 (cdc13-1) or containing a null mutation in the DNA damage response and telomere capping gene YKU70 (yku70Δ). We performed Quantitative Fitness Analysis (QFA) on thousands of yeast strains containing mutations affecting telomere-capping proteins in combination with a library of systematic gene deletion mutations. To perform QFA, we typically inoculate 384 separate cultures onto solid agar plates and monitor growth of each culture by photography over time. The data are fitted to a logistic population growth model; and growth parameters, such as maximum growth rate and maximum doubling potential, are deduced. QFA reveals that as many as 5% of systematic gene deletions, affecting numerous functional classes, strongly interact with telomere capping defects. We show that, while Cdc13 and Yku70 perform complementary roles in telomere capping, their genetic interaction profiles differ significantly. At least 19 different classes of functionally or physically related proteins can be identified as interacting with cdc13-1, yku70Δ, or both. Each specific genetic interaction informs the roles of individual gene products in telomere biology. One striking example is with genes of the nonsense-mediated RNA decay (NMD) pathway which, when disabled, suppress the conditional cdc13-1 mutation but enhance the null yku70Δ mutation. We show that the suppressing/enhancing role of the NMD pathway at uncapped telomeres is mediated through the levels of Stn1, an essential telomere capping protein, which interacts with Cdc13 and recruitment of telomerase to telomeres. We show that increased Stn1 levels affect growth of cells with telomere capping defects due to cdc13-1 and yku70Δ. QFA is a sensitive, high-throughput method that will also be useful to understand other aspects of microbial cell biology. Public Library of Science 2011-04-07 /pmc/articles/PMC3072368/ /pubmed/21490951 http://dx.doi.org/10.1371/journal.pgen.1001362 Text en Addinall et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Addinall, Stephen Gregory
Holstein, Eva-Maria
Lawless, Conor
Yu, Min
Chapman, Kaye
Banks, A. Peter
Ngo, Hien-Ping
Maringele, Laura
Taschuk, Morgan
Young, Alexander
Ciesiolka, Adam
Lister, Allyson Lurena
Wipat, Anil
Wilkinson, Darren James
Lydall, David
Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects
title Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects
title_full Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects
title_fullStr Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects
title_full_unstemmed Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects
title_short Quantitative Fitness Analysis Shows That NMD Proteins and Many Other Protein Complexes Suppress or Enhance Distinct Telomere Cap Defects
title_sort quantitative fitness analysis shows that nmd proteins and many other protein complexes suppress or enhance distinct telomere cap defects
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3072368/
https://www.ncbi.nlm.nih.gov/pubmed/21490951
http://dx.doi.org/10.1371/journal.pgen.1001362
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