TAO kinases mediate activation of p38 in response to DNA damage

Raman, Malavika; Earnest, Svetlana; Zhang, Kai; Zhao, Yingming; Cobb, Melanie H.

doi:10.1038/sj.emboj.7601668

Cited by 172 publications

(141 citation statements)

References 27 publications

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“…The contribution of p38 to the DDR was attributed to the phosphorylation of cdc25B and cdc25C by MK2 (Manke et al, 2005). Moreover, rapid and transient activation of the p38/MK2 pathway was also reported after IR, or treatment with doxorubicin or alkylating agents such as methyl methanesulfonate (MMS) (Mikhailov et al, 2004;Raman et al, 2007;Lafarga et al, 2009;Phong et al, 2010). Activation of the p38/MK2 branch of the checkpoint has been reported to involve ATM/ATR-dependent activation of Thousand and one amino acid protein kinases (TAO) that belong to the MAPKKK family.…”

Section: Checkpoint Kinases-effectors Of the Checkpointmentioning

confidence: 98%

Checkpoint control and cancer

2011

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DNA-damaging therapies represent the most frequently used non-surgical anticancer strategies in the treatment of human tumors. These therapies can kill tumor cells, but at the same time they can be particularly damaging and mutagenic to healthy tissues. The efficacy of DNAdamaging treatments can be improved if tumor cell death is selectively enhanced, and the recent application of poly-(ADP-ribose) polymerase inhibitors in BRCA1/2-deficient tumors is a successful example of this. DNA damage is known to trigger cell-cycle arrest through activation of DNA-damage checkpoints. This arrest can be reversed once the damage has been repaired, but irreparable damage can promote apoptosis or senescence. Alternatively, cells can reenter the cell cycle before repair has been completed, giving rise to mutations. In this review we discuss the mechanisms involved in the activation and inactivation of DNA-damage checkpoints, and how the transition from arrest and cell-cycle re-entry is controlled. In addition, we discuss recent attempts to target the checkpoint in anticancer strategies.

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Section: Checkpoint Kinases-effectors Of the Checkpointmentioning

confidence: 98%

Checkpoint control and cancer

2011

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“…6; Hutchison et al, 1998;Chen et al, 2003;Raman et al, 2007). The cell cycle protein, Ataxia telangiectasia mutated (ATM), is activated in response to DNA damage, and directly phosphorylates TAOk.…”

Section: Tao Kinase (Taok1 Taok2 Taok3) (Omim#*610266)mentioning

confidence: 99%

“…The cell cycle protein, Ataxia telangiectasia mutated (ATM), is activated in response to DNA damage, and directly phosphorylates TAOk. Phosphorylated TAOk then causes activation of p38 MAPK leading cells to enter the G2/M damage checkpoint for DNA repair (Raman et al, 2007). To date, three of these MAP3Ks have been characterized: TAOk1, TAOk2, and TAOk3.…”

Section: Tao Kinase (Taok1 Taok2 Taok3) (Omim#*610266)mentioning

confidence: 99%

MAP3Ks as central regulators of cell fate during development

Craig

Stevens

Vaillancourt

et al. 2008

Developmental Dynamics

109

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“…Other functions of MARKK/TAO-1 involve mitosis progression and MAPK/p38 signaling upon stress induced activation. 94,95 By these mechanisms, apart from the toxic effects of S262/S356 phosphorylated tau, MARKK might contribute to neurodegeneration and cell death.…”

Section: Antiphosphorylation Strategiesmentioning

confidence: 99%

Tau-Based Treatment Strategies in Neurodegenerative Diseases

2008

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Summary:Neurofibrillary tangles are a characteristic hallmark of Alzheimer's and other neurodegenerative diseases, such as Pick's disease (PiD), progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and frontotemporal dementia and parkinsonism linked to chromosome 17 (FTDP-17). These diseases are summarized as tauopathies, because neurofibrillary tangles are composed of intracellular aggregates of the microtubule-associated protein tau. The molecular mechanisms of tau-mediated neurotoxicity are not well understood; however, pathologic hyperphosphorylation and aggregation of tau play a central role in neurodegeneration and neuronal dysfunction. The present review, therefore, focuses on therapeutic approaches that aim to inhibit tau phosphorylation and aggregation or to dissolve preexisting tau aggregates. Further experimental therapy strategies include the enhancement of tau clearance by activation of proteolytic, proteasomal, or autophagosomal degradation pathways or anti-tau directed immunotherapy. Hyperphosphorylated tau does not bind microtubules, leading to microtubule instability and transport impairment. Pharmacological stabilization of microtubule networks might counteract this effect. In several tauopathies there is a shift toward four-repeat tau isoforms, and interference with the splicing machinery to decrease four-repeat splicing might be another therapeutic option.

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TAO kinases mediate activation of p38 in response to DNA damage

Cited by 172 publications

References 27 publications

Checkpoint control and cancer

Checkpoint control and cancer

MAP3Ks as central regulators of cell fate during development

Tau-Based Treatment Strategies in Neurodegenerative Diseases

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