Compromised telomere maintenance in hypomethylated Arabidopsis thaliana plants

Anna Ogrocká; Pavla Polanská; Eva Majerová; Zlatko Janeba; Jiří Fajkus; Miloslava Fojtová

doi:10.1093/nar/gkt1285

Compromised telomere maintenance in hypomethylated Arabidopsis thaliana plants

Nucleic Acids Research ◽

10.1093/nar/gkt1285 ◽

2013 ◽

Vol 42 (5) ◽

pp. 2919-2931 ◽

Cited By ~ 13

Author(s):

Anna Ogrocká ◽

Pavla Polanská ◽

Eva Majerová ◽

Zlatko Janeba ◽

Jiří Fajkus ◽

...

Keyword(s):

Arabidopsis Thaliana ◽

Dna Methyltransferase ◽

Cytosine Methylation ◽

Telomere Maintenance ◽

Model Systems ◽

Dna Repeats ◽

Telomeric Dna ◽

Telomere Shortening

Abstract Telomeres, nucleoprotein structures at the ends of linear eukaryotic chromosomes, are important for the maintenance of genomic stability. Telomeres were considered as typical heterochromatic regions, but in light of recent results, this view should be reconsidered. Asymmetrically located cytosines in plant telomeric DNA repeats may be substrates for a DNA methyltransferase enzyme and indeed, it was shown that these repeats are methylated. Here, we analyse the methylation of telomeric cytosines and the length of telomeres in Arabidopsis thaliana methylation mutants (met 1-3 and ddm 1-8), and in their wild-type siblings that were germinated in the presence of hypomethylation drugs. Our results show that cytosine methylation in telomeric repeats depends on the activity of MET1 and DDM1 enzymes. Significantly shortened telomeres occur in later generations of methylation mutants as well as in plants germinated in the presence of hypomethylation drugs, and this phenotype is stably transmitted to the next plant generation. A possible role of compromised in vivo telomerase action in the observed telomere shortening is hypothesized based on telomere analysis of hypomethylated telomerase knockout plants. Results are discussed in connection with previous data in this field obtained using different model systems.

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Essential roles for Pot1b in HSC self-renewal and survival

Blood ◽

10.1182/blood-2011-06-361527 ◽

2011 ◽

Vol 118 (23) ◽

pp. 6068-6077 ◽

Cited By ~ 22

Author(s):

Yang Wang ◽

Mei-Feng Shen ◽

Sandy Chang

Keyword(s):

Progenitor Cell ◽

Essential Role ◽

Dyskeratosis Congenita ◽

Telomere Maintenance ◽

Wild Type ◽

Telomere Shortening ◽

Damage Response ◽

First Time

Abstract Maintenance of mammalian telomeres requires both the enzyme telomerase and shelterin, which protect telomeres from inappropriately activating DNA damage response checkpoints. Dyskeratosis congenita is an inherited BM failure syndrome disorder because of defects in telomere maintenance. We have previously shown that deletion of the shelterin component Pot1b in the setting of telomerase haploinsufficiency results in rapid telomere shortening and fatal BM failure in mice, eliciting phenotypes that strongly resemble human syskeratosis congenita. However, it was unclear why BM failure occurred in the setting of Pot1b deletion. In this study, we show that Pot1b plays an essential role in HSC survival. Deletion of Pot1b results in increased apoptosis, leading to severe depletion of the HSC reserve. BM from Pot1bΔ/Δ mice cannot compete with BM from wild-type mice to provide multilineage reconstitution, indicating that there is an intrinsic requirement for Pot1b the maintenance of HSC function in vivo. Elimination of the p53-dependent apoptotic function increased HSC survival and significantly extended the lifespan of Pot1b-null mice deficient in telomerase function. Our results document for the first time the essential role of a component of the shelterin complex in the maintenance of HSC and progenitor cell survival.

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Genetic Control of Telomere Integrity in Schizosaccharomyces pombe: rad3+ and tel1+ Are Parts of Two Regulatory Networks Independent of the Downstream Protein Kinases chk1+ and cds1+

Genetics ◽

10.1093/genetics/152.4.1501 ◽

1999 ◽

Vol 152 (4) ◽

pp. 1501-1512 ◽

Cited By ~ 2

Author(s):

Akira Matsuura ◽

Taku Naito ◽

Fuyuki Ishikawa

Keyword(s):

Schizosaccharomyces Pombe ◽

Protein Kinases ◽

Regulatory Networks ◽

Telomere Maintenance ◽

Telomeric Dna ◽

Telomere Shortening ◽

Telomere Repeat ◽

Homologous Protein ◽

Drastic Effect

Abstract The Schizosaccharomyces pombe checkpoint gene named rad3+ encodes an ATM-homologous protein kinase that shares a highly conserved motif with proteins involved in DNA metabolism. Previous studies have shown that Rad3 fulfills its function via the regulation of the Chk1 and Cds1 protein kinases. Here we describe a novel role for Rad3 in the control of telomere integrity. Mutations in the rad3+ gene alleviated telomeric silencing and produced shortened lengths in the telomere repeat tracts. Genetic analysis revealed that the other checkpoint rad mutations rad1, rad17, and rad26 belong to the same phenotypic class with rad3 with regard to control of the telomere length. Of these mutations, rad3 and rad26 have a drastic effect on telomere shortening. tel1+, another ATM homologue in S. pombe, carries out its telomere maintenance function in parallel with the checkpoint rad genes. Furthermore, either a single or double disruption of cds1+ and chk1+ caused no obvious changes in the telomeric DNA structure. Our results demonstrate a novel role of the S. pombe ATM homologues that is independent of chk1+ and cds1+.

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AKT-dependent signaling of extracellular cues through telomeres impact on tumorigenesis

PLoS Genetics ◽

10.1371/journal.pgen.1009410 ◽

2021 ◽

Vol 17 (3) ◽

pp. e1009410

Author(s):

Raúl Sánchez-Vázquez ◽

Paula Martínez ◽

Maria A. Blasco

Keyword(s):

Telomere Maintenance ◽

Environmental Cues ◽

Phosphorylation Sites ◽

Telomeric Dna ◽

Telomere Shortening ◽

Akt Activation ◽

Extracellular Signals ◽

Telomere Protection ◽

Mutant Cells

The telomere-bound shelterin complex is essential for chromosome-end protection and genomic stability. Little is known on the regulation of shelterin components by extracellular signals including developmental and environmental cues. Here, we show that human TRF1 is subjected to AKT-dependent regulation. To study the importance of this modification in vivo, we generate knock-in human cell lines carrying non-phosphorylatable mutants of the AKT-dependent TRF1 phosphorylation sites by CRISPR-Cas9. We find that TRF1 mutant cells show decreased TRF1 binding to telomeres and increased global and telomeric DNA damage. Human cells carrying non-phosphorylatable mutant TRF1 alleles show accelerated telomere shortening, demonstrating that AKT-dependent TRF1 phosphorylation regulates telomere maintenance in vivo. TRF1 mutant cells show an impaired response to proliferative extracellular signals as well as a decreased tumorigenesis potential. These findings indicate that telomere protection and telomere length can be regulated by extracellular signals upstream of PI3K/AKT activation, such as growth factors, nutrients or immune regulators, and this has an impact on tumorigenesis potential.

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Swc4 positively regulates telomere length independently of its roles in NuA4 and SWR1 complexes

Nucleic Acids Research ◽

10.1093/nar/gkaa1150 ◽

2020 ◽

Vol 48 (22) ◽

pp. 12792-12803

Author(s):

Jia-Cheng Liu ◽

Qian-Jin Li ◽

Ming-Hong He ◽

Can Hu ◽

Pengfei Dai ◽

...

Keyword(s):

Telomere Length ◽

Essential Gene ◽

Telomerase Activity ◽

Telomere Maintenance ◽

Direct Role ◽

Telomere Shortening ◽

Length Regulation ◽

Telomere Length Regulation

Abstract Telomeres at the ends of eukaryotic chromosomes are essential for genome integrality and stability. In order to identify genes that sustain telomere maintenance independently of telomerase recruitment, we have exploited the phenotype of over-long telomeres in the cells that express Cdc13-Est2 fusion protein, and examined 195 strains, in which individual non-essential gene deletion causes telomere shortening. We have identified 24 genes whose deletion results in dramatic failure of Cdc13-Est2 function, including those encoding components of telomerase, Yku, KEOPS and NMD complexes, as well as quite a few whose functions are not obvious in telomerase activity regulation. We have characterized Swc4, a shared subunit of histone acetyltransferase NuA4 and chromatin remodeling SWR1 (SWR1-C) complexes, in telomere length regulation. Deletion of SWC4, but not other non-essential subunits of either NuA4 or SWR1-C, causes significant telomere shortening. Consistently, simultaneous disassembly of NuA4 and SWR1-C does not affect telomere length. Interestingly, inactivation of Swc4 in telomerase null cells accelerates both telomere shortening and senescence rates. Swc4 associates with telomeric DNA in vivo, suggesting a direct role of Swc4 at telomeres. Taken together, our work reveals a distinct role of Swc4 in telomere length regulation, separable from its canonical roles in both NuA4 and SWR1-C.

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Dynamics of Telomeric DNA Turnover in Yeast

Genetics ◽

10.1093/genetics/160.1.63 ◽

2002 ◽

Vol 160 (1) ◽

pp. 63-73

Author(s):

Michael J McEachern ◽

Dana Hager Underwood ◽

Elizabeth H Blackburn

Keyword(s):

Kluyveromyces Lactis ◽

Mutant Gene ◽

Dna Repeats ◽

Wild Type ◽

Telomeric Dna ◽

Cell Divisions ◽

Dna Turnover ◽

Length Regulation ◽

Turn Over

Abstract Telomerase adds telomeric DNA repeats to telomeric termini using a sequence within its RNA subunit as a template. We characterized two mutations in the Kluyveromyces lactis telomerase RNA gene (TER1) template. Each initially produced normally regulated telomeres. One mutation, ter1-AA, had a cryptic defect in length regulation that was apparent only if the mutant gene was transformed into a TER1 deletion strain to permit extensive replacement of basal wild-type repeats with mutant repeats. This mutant differs from previously studied delayed elongation mutants in a number of properties. The second mutation, TER1-Bcl, which generates a BclI restriction site in newly synthesized telomeric repeats, was indistinguishable from wild type in all phenotypes assayed: cell growth, telomere length, and in vivo telomerase fidelity. TER1-Bcl cells demonstrated that the outer halves of the telomeric repeat tracts turn over within a few hundred cell divisions, while the innermost few repeats typically resisted turnover for at least 3000 cell divisions. Similarly deep but incomplete turnover was also observed in two other TER1 template mutants with highly elongated telomeres. These results indicate that most DNA turnover in functionally normal telomeres is due to gradual replicative sequence loss and additions by telomerase but that there are other processes that also contribute to turnover.

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Functional analysis of the SUMOylation pathway in Drosophila

Biochemical Society Transactions ◽

10.1042/bst0360868 ◽

2008 ◽

Vol 36 (5) ◽

pp. 868-873 ◽

Cited By ~ 31

Author(s):

Ana Talamillo ◽

Jonatan Sánchez ◽

Rosa Barrio

Keyword(s):

Functional Analysis ◽

Fine Tuning ◽

Model Systems ◽

Post Translational Modification ◽

Reversible Process ◽

Cellular Processes ◽

Tuning Mechanism ◽

Sumo Conjugation

SUMOylation, a reversible process used as a ‘fine-tuning’ mechanism to regulate the role of multiple proteins, is conserved throughout evolution. This post-translational modification affects several cellular processes by the modulation of subcellular localization, activity or stability of a variety of substrates. A growing number of proteins have been identified as targets for SUMOylation, although, for many of them, the role of SUMO conjugation on their function is unknown. The use of model systems might facilitate the study of SUMOylation implications in vivo. In the present paper, we have compiled what is known about SUMOylation in Drosophila melanogaster, where the use of genetics provides new insights on SUMOylation's biological roles.

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SIRT1 contributes to telomere maintenance and augments global homologous recombination

The Journal of Cell Biology ◽

10.1083/jcb.201005160 ◽

2010 ◽

Vol 191 (7) ◽

pp. 1299-1313 ◽

Cited By ~ 156

Author(s):

Jose A. Palacios ◽

Daniel Herranz ◽

Maria Luigia De Bonis ◽

Susana Velasco ◽

Manuel Serrano ◽

...

Keyword(s):

Homologous Recombination ◽

Telomerase Activity ◽

Histone Deacetylation ◽

Telomere Maintenance ◽

Loss Of Function ◽

Entire Genome ◽

Telomere Shortening ◽

Telomere Biology ◽

Sir Complex

Yeast Sir2 deacetylase is a component of the silent information regulator (SIR) complex encompassing Sir2/Sir3/Sir4. Sir2 is recruited to telomeres through Rap1, and this complex spreads into subtelomeric DNA via histone deacetylation. However, potential functions at telomeres for SIRT1, the mammalian orthologue of yeast Sir2, are less clear. We studied both loss of function (SIRT1 deficient) and gain of function (SIRT1super) mouse models. Our results indicate that SIRT1 is a positive regulator of telomere length in vivo and attenuates telomere shortening associated with aging, an effect dependent on telomerase activity. Using chromatin immunoprecipitation assays, we find that SIRT1 interacts with telomeric repeats in vivo. In addition, SIRT1 overexpression increases homologous recombination throughout the entire genome, including telomeres, centromeres, and chromosome arms. These findings link SIRT1 to telomere biology and global DNA repair and provide new mechanistic explanations for the known functions of SIRT1 in protection from DNA damage and some age-associated pathologies.

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The conserved structure of plant telomerase RNA provides the missing link for an evolutionary pathway from ciliates to humans

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1915312116 ◽

2019 ◽

Vol 116 (49) ◽

pp. 24542-24550 ◽

Cited By ~ 8

Author(s):

Jiarui Song ◽

Dhenugen Logeswaran ◽

Claudia Castillo-González ◽

Yang Li ◽

Sreyashree Bose ◽

...

Keyword(s):

Telomerase Activity ◽

Telomere Maintenance ◽

Telomerase Rna ◽

Telomeric Dna ◽

Structural Element ◽

Stem Loop ◽

Evolutionary Pathway ◽

Pol Iii

Telomerase is essential for maintaining telomere integrity. Although telomerase function is widely conserved, the integral telomerase RNA (TR) that provides a template for telomeric DNA synthesis has diverged dramatically. Nevertheless, TR molecules retain 2 highly conserved structural domains critical for catalysis: a template-proximal pseudoknot (PK) structure and a downstream stem-loop structure. Here we introduce the authentic TR from the plant Arabidopsis thaliana, called AtTR, identified through next-generation sequencing of RNAs copurifying with Arabidopsis TERT. This RNA is distinct from the RNA previously described as the templating telomerase RNA, AtTER1. AtTR is a 268-nt Pol III transcript necessary for telomere maintenance in vivo and sufficient with TERT to reconstitute telomerase activity in vitro. Bioinformatics analysis identified 85 AtTR orthologs from 3 major clades of plants: angiosperms, gymnosperms, and lycophytes. Through phylogenetic comparisons, a secondary structure model conserved among plant TRs was inferred and verified using in vitro and in vivo chemical probing. The conserved plant TR structure contains a template-PK core domain enclosed by a P1 stem and a 3′ long-stem P4/5/6, both of which resemble a corresponding structural element in ciliate and vertebrate TRs. However, the plant TR contains additional stems and linkers within the template-PK core, allowing for expansion of PK structure from the simple PK in the smaller ciliate TR during evolution. Thus, the plant TR provides an evolutionary bridge that unites the disparate structures of previously characterized TRs from ciliates and vertebrates.

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Role for the Related Poly(ADP-Ribose) Polymerases Tankyrase 1 and 2 at Human Telomeres

Molecular and Cellular Biology ◽

10.1128/mcb.22.1.332-342.2002 ◽

2002 ◽

Vol 22 (1) ◽

pp. 332-342 ◽

Cited By ~ 197

Author(s):

Brandoch D. Cook ◽

Jasmin N. Dynek ◽

William Chang ◽

Grigoriy Shostak ◽

Susan Smith

Keyword(s):

Potential Role ◽

Telomere Maintenance ◽

Telomeric Dna ◽

Continuous Growth ◽

Telomere Elongation ◽

Bona Fide ◽

Tankyrase 1 ◽

Growth Of Tumor

ABSTRACT Telomere maintenance is essential for the continuous growth of tumor cells. In most human tumors telomeres are maintained by telomerase, a specialized reverse transcriptase. Tankyrase 1, a human telomeric poly(ADP-ribose) polymerase (PARP), positively regulates telomere length through its interaction with TRF1, a telomeric DNA-binding protein. Tankyrase 1 ADP-ribosylates TRF1, inhibiting its binding to telomeric DNA. Overexpression of tankyrase 1 in the nucleus promotes telomere elongation, suggesting that tankyrase 1 regulates access of telomerase to the telomeric complex. The recent identification of a closely related homolog of tankyrase 1, tankyrase 2, opens the possibility for a second PARP at telomeres. We therefore sought to establish the role of tankyrase 1 at telomeres and to determine if tankyrase 2 might have a telomeric function. We show that endogenous tankyrase 1 is a component of the human telomeric complex. We demonstrate that telomere elongation by tankyrase 1 requires the catalytic activity of the PARP domain and does not occur in telomerase-negative primary human cells. To investigate a potential role for tankyrase 2 at telomeres, recombinant tankyrase 2 was subjected to an in vitro PARP assay. Tankyrase 2 poly(ADP-ribosyl)ated itself and TRF1. Overexpression of tankyrase 2 in the nucleus released endogenous TRF1 from telomeres. These findings establish tankyrase 2 as a bona fide PARP, with itself and TRF1 as acceptors of ADP-ribosylation, and suggest the possibility of a role for tankyrase 2 at telomeres.

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G-Quadruplexes at Telomeres: Friend or Foe?

Molecules ◽

10.3390/molecules25163686 ◽

2020 ◽

Vol 25 (16) ◽

pp. 3686 ◽

Cited By ~ 3

Author(s):

Tracy M. Bryan

Keyword(s):

Tandem Repeats ◽

Genome Instability ◽

Protein Complexes ◽

Telomere Maintenance ◽

Telomeric Dna ◽

Positive Role ◽

Telomere Biology ◽

Linear Chromosomes

Telomeres are DNA-protein complexes that cap and protect the ends of linear chromosomes. In almost all species, telomeric DNA has a G/C strand bias, and the short tandem repeats of the G-rich strand have the capacity to form into secondary structures in vitro, such as four-stranded G-quadruplexes. This has long prompted speculation that G-quadruplexes play a positive role in telomere biology, resulting in selection for G-rich tandem telomere repeats during evolution. There is some evidence that G-quadruplexes at telomeres may play a protective capping role, at least in yeast, and that they may positively affect telomere maintenance by either the enzyme telomerase or by recombination-based mechanisms. On the other hand, G-quadruplex formation in telomeric DNA, as elsewhere in the genome, can form an impediment to DNA replication and a source of genome instability. This review summarizes recent evidence for the in vivo existence of G-quadruplexes at telomeres, with a focus on human telomeres, and highlights some of the many unanswered questions regarding the location, form, and functions of these structures.

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