Multiple cancer pathways regulate telomere protection

Multiple cancer pathways regulate telomere protection

Abstract Telomeres are considered as universal anti‐cancer targets, as telomere maintenance is essential to sustain indefinite cancer growth. Mutations in telomerase, the enzyme that maintains telomeres, are among the most frequently found in cancer. In addition, mutations in components of the telom...

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Main Authors: Leire Bejarano, Giuseppe Bosso, Jessica Louzame, Rosa Serrano, Elena Gómez‐Casero, Jorge Martínez‐Torrecuadrada, Sonia Martínez, Carmen Blanco‐Aparicio, Joaquín Pastor, Maria A Blasco
Format: Article
Language:English
Published: Wiley 2019-07-01
Series:EMBO Molecular Medicine
Subjects:
drug resistance
ERK kinase
glioblastoma
telomeres
TRF1 inhibitors
Online Access:https://doi.org/10.15252/emmm.201910292
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spelling doaj-9779bb57d13c41769aa864bea9220f332021-08-02T20:06:55ZengWileyEMBO Molecular Medicine1757-46761757-46842019-07-01117n/an/a10.15252/emmm.201910292Multiple cancer pathways regulate telomere protectionLeire Bejarano0Giuseppe Bosso1Jessica Louzame2Rosa Serrano3Elena Gómez‐Casero4Jorge Martínez‐Torrecuadrada5Sonia Martínez6Carmen Blanco‐Aparicio7Joaquín Pastor8Maria A Blasco9Telomeres and Telomerase Group Molecular Oncology Program Spanish National Cancer Centre (CNIO) Madrid SpainTelomeres and Telomerase Group Molecular Oncology Program Spanish National Cancer Centre (CNIO) Madrid SpainTelomeres and Telomerase Group Molecular Oncology Program Spanish National Cancer Centre (CNIO) Madrid SpainTelomeres and Telomerase Group Molecular Oncology Program Spanish National Cancer Centre (CNIO) Madrid SpainExperimental Therapeutics Program Spanish National Cancer Centre (CNIO) Madrid SpainBiotechnology Program Spanish National Cancer Centre (CNIO) Madrid SpainExperimental Therapeutics Program Spanish National Cancer Centre (CNIO) Madrid SpainExperimental Therapeutics Program Spanish National Cancer Centre (CNIO) Madrid SpainExperimental Therapeutics Program Spanish National Cancer Centre (CNIO) Madrid SpainTelomeres and Telomerase Group Molecular Oncology Program Spanish National Cancer Centre (CNIO) Madrid SpainAbstract Telomeres are considered as universal anti‐cancer targets, as telomere maintenance is essential to sustain indefinite cancer growth. Mutations in telomerase, the enzyme that maintains telomeres, are among the most frequently found in cancer. In addition, mutations in components of the telomere protective complex, or shelterin, are also found in familial and sporadic cancers. Most efforts to target telomeres have focused in telomerase inhibition; however, recent studies suggest that direct targeting of the shelterin complex could represent a more effective strategy. In particular, we recently showed that genetic deletion of the TRF1 essential shelterin protein impairs tumor growth in aggressive lung cancer and glioblastoma (GBM) mouse models by direct induction of telomere damage independently of telomere length. Here, we screen for TRF1 inhibitory drugs using a collection of FDA‐approved drugs and drugs in clinical trials, which cover the majority of pathways included in the Reactome database. Among other targets, we find that inhibition of several kinases of the Ras pathway, including ERK and MEK, recapitulates the effects of Trf1 genetic deletion, including induction of telomeric DNA damage, telomere fragility, and inhibition of cancer stemness. We further show that both bRAF and ERK2 kinases phosphorylate TRF1 in vitro and that these modifications are essential for TRF1 location to telomeres in vivo. Finally, we use these new TRF1 regulatory pathways as the basis to discover novel drug combinations based on TRF1 inhibition, with the goal of effectively blocking potential resistance to individual drugs in patient‐derived glioblastoma xenograft models.https://doi.org/10.15252/emmm.201910292drug resistanceERK kinaseglioblastomatelomeresTRF1 inhibitors
collection DOAJ
language English
format Article
sources DOAJ
author Leire Bejarano
Giuseppe Bosso
Jessica Louzame
Rosa Serrano
Elena Gómez‐Casero
Jorge Martínez‐Torrecuadrada
Sonia Martínez
Carmen Blanco‐Aparicio
Joaquín Pastor
Maria A Blasco
spellingShingle Leire Bejarano
Giuseppe Bosso
Jessica Louzame
Rosa Serrano
Elena Gómez‐Casero
Jorge Martínez‐Torrecuadrada
Sonia Martínez
Carmen Blanco‐Aparicio
Joaquín Pastor
Maria A Blasco
Multiple cancer pathways regulate telomere protection
EMBO Molecular Medicine
drug resistance
ERK kinase
glioblastoma
telomeres
TRF1 inhibitors
author_facet Leire Bejarano
Giuseppe Bosso
Jessica Louzame
Rosa Serrano
Elena Gómez‐Casero
Jorge Martínez‐Torrecuadrada
Sonia Martínez
Carmen Blanco‐Aparicio
Joaquín Pastor
Maria A Blasco
author_sort Leire Bejarano
title Multiple cancer pathways regulate telomere protection
title_short Multiple cancer pathways regulate telomere protection
title_full Multiple cancer pathways regulate telomere protection
title_fullStr Multiple cancer pathways regulate telomere protection
title_full_unstemmed Multiple cancer pathways regulate telomere protection
title_sort multiple cancer pathways regulate telomere protection
publisher Wiley
series EMBO Molecular Medicine
issn 1757-4676
1757-4684
publishDate 2019-07-01
description Abstract Telomeres are considered as universal anti‐cancer targets, as telomere maintenance is essential to sustain indefinite cancer growth. Mutations in telomerase, the enzyme that maintains telomeres, are among the most frequently found in cancer. In addition, mutations in components of the telomere protective complex, or shelterin, are also found in familial and sporadic cancers. Most efforts to target telomeres have focused in telomerase inhibition; however, recent studies suggest that direct targeting of the shelterin complex could represent a more effective strategy. In particular, we recently showed that genetic deletion of the TRF1 essential shelterin protein impairs tumor growth in aggressive lung cancer and glioblastoma (GBM) mouse models by direct induction of telomere damage independently of telomere length. Here, we screen for TRF1 inhibitory drugs using a collection of FDA‐approved drugs and drugs in clinical trials, which cover the majority of pathways included in the Reactome database. Among other targets, we find that inhibition of several kinases of the Ras pathway, including ERK and MEK, recapitulates the effects of Trf1 genetic deletion, including induction of telomeric DNA damage, telomere fragility, and inhibition of cancer stemness. We further show that both bRAF and ERK2 kinases phosphorylate TRF1 in vitro and that these modifications are essential for TRF1 location to telomeres in vivo. Finally, we use these new TRF1 regulatory pathways as the basis to discover novel drug combinations based on TRF1 inhibition, with the goal of effectively blocking potential resistance to individual drugs in patient‐derived glioblastoma xenograft models.
topic drug resistance
ERK kinase
glioblastoma
telomeres
TRF1 inhibitors
url https://doi.org/10.15252/emmm.201910292
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AT giuseppebosso multiplecancerpathwaysregulatetelomereprotection
AT jessicalouzame multiplecancerpathwaysregulatetelomereprotection
AT rosaserrano multiplecancerpathwaysregulatetelomereprotection
AT elenagomezcasero multiplecancerpathwaysregulatetelomereprotection
AT jorgemartineztorrecuadrada multiplecancerpathwaysregulatetelomereprotection
AT soniamartinez multiplecancerpathwaysregulatetelomereprotection
AT carmenblancoaparicio multiplecancerpathwaysregulatetelomereprotection
AT joaquinpastor multiplecancerpathwaysregulatetelomereprotection
AT mariaablasco multiplecancerpathwaysregulatetelomereprotection
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