AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance

Telomeres are nucleoprotein complexes that protect the ends of linear chromosomes from incomplete replication, degradation and detection as DNA breaks. Mammalian telomeres are protected by shelterin, a multiprotein complex that binds the TTAGGG telomeric repeats and recruits a series of additional f...

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Autores principales: Burla, Romina, Carcuro, Mariateresa, Raffa, Grazia D., Galati, Alessandra, Raimondo, Domenico, Rizzo, Angela, La Torre, Mattia, Micheli, Emanuela, Ciapponi, Laura, Cenci, Giovanni, Cundari, Enrico, Musio, Antonio, Biroccio, Annamaria, Cacchione, Stefano, Gatti, Maurizio, Saggio, Isabella
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4481533/
https://www.ncbi.nlm.nih.gov/pubmed/26110528
http://dx.doi.org/10.1371/journal.pgen.1005167
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author Burla, Romina
Carcuro, Mariateresa
Raffa, Grazia D.
Galati, Alessandra
Raimondo, Domenico
Rizzo, Angela
La Torre, Mattia
Micheli, Emanuela
Ciapponi, Laura
Cenci, Giovanni
Cundari, Enrico
Musio, Antonio
Biroccio, Annamaria
Cacchione, Stefano
Gatti, Maurizio
Saggio, Isabella
author_facet Burla, Romina
Carcuro, Mariateresa
Raffa, Grazia D.
Galati, Alessandra
Raimondo, Domenico
Rizzo, Angela
La Torre, Mattia
Micheli, Emanuela
Ciapponi, Laura
Cenci, Giovanni
Cundari, Enrico
Musio, Antonio
Biroccio, Annamaria
Cacchione, Stefano
Gatti, Maurizio
Saggio, Isabella
author_sort Burla, Romina
collection PubMed
description Telomeres are nucleoprotein complexes that protect the ends of linear chromosomes from incomplete replication, degradation and detection as DNA breaks. Mammalian telomeres are protected by shelterin, a multiprotein complex that binds the TTAGGG telomeric repeats and recruits a series of additional factors that are essential for telomere function. Although many shelterin-associated proteins have been so far identified, the inventory of shelterin-interacting factors required for telomere maintenance is still largely incomplete. Here, we characterize AKTIP/Ft1 (human AKTIP and mouse Ft1 are orthologous), a novel mammalian shelterin-bound factor identified on the basis of its homology with the Drosophila telomere protein Pendolino. AKTIP/Ft1 shares homology with the E2 variant ubiquitin-conjugating (UEV) enzymes and has been previously implicated in the control of apoptosis and in vesicle trafficking. RNAi-mediated depletion of AKTIP results in formation of telomere dysfunction foci (TIFs). Consistent with these results, AKTIP interacts with telomeric DNA and binds the shelterin components TRF1 and TRF2 both in vivo and in vitro. Analysis of AKTIP- depleted human primary fibroblasts showed that they are defective in PCNA recruiting and arrest in the S phase due to the activation of the intra S checkpoint. Accordingly, AKTIP physically interacts with PCNA and the RPA70 DNA replication factor. Ft1-depleted p53(-/-) MEFs did not arrest in the S phase but displayed significant increases in multiple telomeric signals (MTS) and sister telomere associations (STAs), two hallmarks of defective telomere replication. In addition, we found an epistatic relation for MST formation between Ft1 and TRF1, which has been previously shown to be required for replication fork progression through telomeric DNA. Ch-IP experiments further suggested that in AKTIP-depleted cells undergoing the S phase, TRF1 is less tightly bound to telomeric DNA than in controls. Thus, our results collectively suggest that AKTIP/Ft1 works in concert with TRF1 to facilitate telomeric DNA replication.
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spelling pubmed-44815332015-07-01 AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance Burla, Romina Carcuro, Mariateresa Raffa, Grazia D. Galati, Alessandra Raimondo, Domenico Rizzo, Angela La Torre, Mattia Micheli, Emanuela Ciapponi, Laura Cenci, Giovanni Cundari, Enrico Musio, Antonio Biroccio, Annamaria Cacchione, Stefano Gatti, Maurizio Saggio, Isabella PLoS Genet Research Article Telomeres are nucleoprotein complexes that protect the ends of linear chromosomes from incomplete replication, degradation and detection as DNA breaks. Mammalian telomeres are protected by shelterin, a multiprotein complex that binds the TTAGGG telomeric repeats and recruits a series of additional factors that are essential for telomere function. Although many shelterin-associated proteins have been so far identified, the inventory of shelterin-interacting factors required for telomere maintenance is still largely incomplete. Here, we characterize AKTIP/Ft1 (human AKTIP and mouse Ft1 are orthologous), a novel mammalian shelterin-bound factor identified on the basis of its homology with the Drosophila telomere protein Pendolino. AKTIP/Ft1 shares homology with the E2 variant ubiquitin-conjugating (UEV) enzymes and has been previously implicated in the control of apoptosis and in vesicle trafficking. RNAi-mediated depletion of AKTIP results in formation of telomere dysfunction foci (TIFs). Consistent with these results, AKTIP interacts with telomeric DNA and binds the shelterin components TRF1 and TRF2 both in vivo and in vitro. Analysis of AKTIP- depleted human primary fibroblasts showed that they are defective in PCNA recruiting and arrest in the S phase due to the activation of the intra S checkpoint. Accordingly, AKTIP physically interacts with PCNA and the RPA70 DNA replication factor. Ft1-depleted p53(-/-) MEFs did not arrest in the S phase but displayed significant increases in multiple telomeric signals (MTS) and sister telomere associations (STAs), two hallmarks of defective telomere replication. In addition, we found an epistatic relation for MST formation between Ft1 and TRF1, which has been previously shown to be required for replication fork progression through telomeric DNA. Ch-IP experiments further suggested that in AKTIP-depleted cells undergoing the S phase, TRF1 is less tightly bound to telomeric DNA than in controls. Thus, our results collectively suggest that AKTIP/Ft1 works in concert with TRF1 to facilitate telomeric DNA replication. Public Library of Science 2015-06-25 /pmc/articles/PMC4481533/ /pubmed/26110528 http://dx.doi.org/10.1371/journal.pgen.1005167 Text en © 2015 Burla 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
Burla, Romina
Carcuro, Mariateresa
Raffa, Grazia D.
Galati, Alessandra
Raimondo, Domenico
Rizzo, Angela
La Torre, Mattia
Micheli, Emanuela
Ciapponi, Laura
Cenci, Giovanni
Cundari, Enrico
Musio, Antonio
Biroccio, Annamaria
Cacchione, Stefano
Gatti, Maurizio
Saggio, Isabella
AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance
title AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance
title_full AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance
title_fullStr AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance
title_full_unstemmed AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance
title_short AKTIP/Ft1, a New Shelterin-Interacting Factor Required for Telomere Maintenance
title_sort aktip/ft1, a new shelterin-interacting factor required for telomere maintenance
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4481533/
https://www.ncbi.nlm.nih.gov/pubmed/26110528
http://dx.doi.org/10.1371/journal.pgen.1005167
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