Human CLK2 Links Cell Cycle Progression, Apoptosis, and Telomere Length Regulation

Jiang, Ning; Bénard, Claire; Kébir, Hania; Shoubridge, Eric A.; Hekimi, Siegfried

doi:10.1074/jbc.m300286200

Cited by 41 publications

(30 citation statements)

References 30 publications

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“…TTI1 is required to maintain the abundance of TEL2, as depletion of TTI1 results in a decrease in TEL2 protein levels, most likely by controlling its stability. TEL2 has been implicated in the DDR, in particular in response to agents that activate the ATR pathway (Jiang et al 2003;Collis et al 2007Collis et al , 2008. However, the DNA damage sensitivity phenotype observed with TTI1 depletion is not simply due to the decrease in TEL2 levels, since restoration of TEL2 expression cannot restore DNA damage resistance.…”

Section: Discussionmentioning

confidence: 93%

A genetic screen identifies the Triple T complex required for DNA damage signaling and ATM and ATR stability

Hurov

Cotta‐Ramusino²,

Elledge³

2010

Genes Dev.

201

247

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In response to DNA damage, cells activate a complex signal transduction network called the DNA damage response (DDR). To enhance our current understanding of the DDR network, we performed a genome-wide RNAi screen to identify genes required for resistance to ionizing radiation (IR). Along with a number of known DDR genes, we discovered a large set of novel genes whose depletion leads to cellular sensitivity to IR. Here we describe TTI1 (Tel two-interacting protein 1) and TTI2 as highly conserved regulators of the DDR in mammals. TTI1 and TTI2 protect cells from spontaneous DNA damage, and are required for the establishment of the intra-S and G2/M checkpoints. TTI1 and TTI2 exist in multiple complexes, including a 2-MDa complex with TEL2 (telomere maintenance 2), called the Triple T complex, and phosphoinositide-3-kinase-related protein kinases (PIKKs) such as ataxia telangiectasia-mutated (ATM). The components of the TTT complex are mutually dependent on each other, and act as critical regulators of PIKK abundance and checkpoint signaling. Organisms experience significant amounts of DNA damage, which threatens their survival on a daily basis. To address this damage and optimize survival, cells evolved the DNA damage response (DDR), a complex signal transduction network that activates transcription and DNA repair, and coordinates cell cycle transitions in order to maintain genomic stability. The central regulators of the DDR are ataxia telangiectasia-mutated (ATM) and ataxiatelangiectasia and Rad3-related (ATR), two members of the mammalian phosphoinositide-3-kinase-related protein kinase (PIKK) family. ATM is critical for the cellular response to DNA double-strand breaks (DSBs), and mutations in ATM lead to the neurodegenerative and cancer predisposition disease ataxia telangiectasia (Lavin 2008).

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Section: Discussionmentioning

confidence: 93%

A genetic screen identifies the Triple T complex required for DNA damage signaling and ATM and ATR stability

Hurov

Cotta‐Ramusino²,

Elledge³

2010

Genes Dev.

201

247

View full text Add to dashboard Cite

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“…Cell Lines and Cell Culture-Human dermal fibroblast (HDF) (ATCC PCS-201-010) and MCH58 (human skin fibroblast, obtained from E. Shoubridge, Montreal Neurological Institute and Hospital) were cultured in Dulbecco's minimum essential medium (DMEM) (HyClone) supplemented with 10% fetal bovine serum (FBS) (HyClone) and 1ϫ penicillin/streptomycin (MP Biomedicals) (36). For standard cultures (20% oxygen), cells were placed in an incubator (NuAire) with humidified ambient atmosphere containing 5% carbon dioxide at 37°C.…”

Section: Methodsmentioning

confidence: 99%

Membrane Oxidation Enables the Cytosolic Entry of Polyarginine Cell-penetrating Peptides

Wang

Sun

Muthukrishnan

et al. 2016

Journal of Biological Chemistry

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Arginine-rich peptides can penetrate cells and consequently be used as delivery agents in various cellular applications. The activity of these reagents is often context-dependent, and the parameters that impact cell entry are not fully understood, giving rise to variability and limiting progress toward their usage. Herein, we report that the cytosolic penetration of linear polyarginine peptides is dependent on the oxidation state of the cell. In particular, we find that hypoxia and cellular antioxidants inhibit cell penetration. In contrast, oxidants promote cytosolic cell entry with an efficiency proportional to the level of reactive oxygen species generated within membranes. Moreover, an antibody that binds to oxidized lipids inhibits cell penetration, whereas extracellularly administered pure oxidized lipids enhance peptide transport into cells. Overall, these data indicate that oxidized lipids are capable of mediating the transport of polyarginine peptides across membranes. These data may also explain variability in cell-penetrating peptide performance in different experimental conditions. These new findings therefore provide new opportunities for the rational design of future cell-permeable compounds and for the optimization of delivery protocols.

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“…Polyclonal rabbit anti-ATRIP 403 (rATRIP 403) (1:3,000) (34), anti-CINP (29), and anti-phospho-ATRIP S224 (1:3,000) (35) were previously described and provided by David Cortez (Vanderbilt University School of Medicine, Nashville, TN). Rabbit antiserum to HCLK2 was previously described and provided by Siegfried Hekimi (McGill University, Montreal, Quebec) (36).…”

Section: Methodsmentioning

confidence: 99%

Efficient Herpes Simplex Virus 1 Replication Requires Cellular ATR Pathway Proteins

Mohni

Dee

Smith

et al. 2013

J Virol

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aHerpes simplex virus 1 (HSV-1) is a double-stranded DNA virus that replicates in the nucleus of the host cell and is known to interact with several components of the cellular DNA-damage-signaling machinery. We have previously reported that the DNA damage response kinase, ATR, is specifically inactivated in HSV-1-infected cells. On the other hand, we have also shown that ATR and its scaffolding protein, ATRIP, are recruited to viral replication compartments, where they play beneficial roles during HSV-1 replication. In order to better understand this apparent discrepancy, we tested the hypothesis that some of the components of the ATR pathway may exert an antiviral effect on infection. In fact, we learned that all 10 of the canonical ATR pathway proteins are stable in HSV-infected cells and are recruited to viral replication compartments; furthermore, short hairpin RNA (shRNA) knockdown shows that several, including ATRIP, RPA70, TopBP1, Claspin, and CINP, are required for efficient HSV-1 replication. We also determined that activation of the ATR kinase prior to infection did not affect virus yield but did result in reduced levels of recombination between coinfecting viruses. Together, these data suggest that ATR pathway proteins are not antiviral per se but that activation of ATR signaling may have negative consequences during viral replication, such as inhibiting recombination.

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Human CLK2 Links Cell Cycle Progression, Apoptosis, and Telomere Length Regulation

Cited by 41 publications

References 30 publications

A genetic screen identifies the Triple T complex required for DNA damage signaling and ATM and ATR stability

A genetic screen identifies the Triple T complex required for DNA damage signaling and ATM and ATR stability

Membrane Oxidation Enables the Cytosolic Entry of Polyarginine Cell-penetrating Peptides

Efficient Herpes Simplex Virus 1 Replication Requires Cellular ATR Pathway Proteins

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