Delayed and Accelerated Aging Share Common Longevity Assurance Mechanisms

Schumacher, Björn; Pluijm, Ingrid van der; Moorhouse, Michael; Kosteas, Theodoros; Robinson, Andria Rasile; Suh, Yousin; Breit, Timo M.; Steeg, Harry van; Niedernhofer, Laura J.; IJcken, Wilfred F. J. van; Bartke, Andrzej; Spindler, Stephen R.; Hoeijmakers, Jan H.J.; Horst, Gijsbertus T. J. van der; Garinis, George A.

doi:10.1371/journal.pgen.1000161

Cited by 186 publications

(174 citation statements)

References 40 publications

(55 reference statements)

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“…Nonetheless, in select mouse models of severe NER progeria, effects on serum IGF-1 and glycemic index can be transient, occurring prior to weaning but normalizing in animals that survive this apparent developmental bottleneck (van de Ven et al 2006). Global profiling of gene expression in liver confirmed a significant overlap between NER progeria and long-lived dwarfism (Schumacher et al 2008) consistent with the physiologic data. Paradoxically, the core feature of IGF-1 signaling attenuation increases lifespan in several species (Rincon et al 2004;Longo and Finch 2003) but is associated with decreased longevity in NER progeria.…”

Section: Mouse Models Of Ner Progeriasupporting

confidence: 63%

Relationship Between DNA Damage and Energy Metabolism: Evidence from DNA Repair Deficiency Syndromes

Vose¹,

Mitchell²

2011

DNA Repair and Human Health

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Section: Mouse Models Of Ner Progeriasupporting

confidence: 63%

Relationship Between DNA Damage and Energy Metabolism: Evidence from DNA Repair Deficiency Syndromes

Vose¹,

Mitchell²

2011

DNA Repair and Human Health

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“…We carried out a series of in vivo chromatin immunoprecipitation (ChIP) assays to study occupancies of the Igf1, GhR, Dio1, and PrlR promoters. These genes are essential for postnatal animal growth (17). Unlike Ercc1 −/− livers, beginning on day 5, the wt livers demonstrated a robust increase in the mRNA levels of these genes ( Fig.…”

Section: Ercc1-xpf Is Recruited On the Promoters Of Genes Associated mentioning

confidence: 96%

Defective transcription initiation causes postnatal growth failure in a mouse model of nucleotide excision repair (NER) progeria

Kamileri

Karakasilioti

Sideri

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Nucleotide excision repair (NER) defects are associated with cancer, developmental disorders and neurodegeneration. However, with the exception of cancer, the links between defects in NER and developmental abnormalities are not well understood. Here, we show that the ERCC1-XPF NER endonuclease assembles on active promoters in vivo and facilitates chromatin modifications for transcription during mammalian development. We find that Ercc1 −/− mice demonstrate striking physiological, metabolic and gene expression parallels with Taf10 −/− animals carrying a liver-specific transcription factor II D (TFIID) defect in transcription initiation. Promoter occupancy studies combined with expression profiling in the liver and in vitro differentiation cell assays reveal that ERCC1-XPF interacts with TFIID and assembles with POL II and the basal transcription machinery on promoters in vivo. Whereas ERCC1-XPF is required for the initial activation of genes associated with growth, it is dispensable for ongoing transcription. Recruitment of ERCC1-XPF on promoters is accompanied by promoter-proximal DNA demethylation and histone marks associated with active hepatic transcription. Collectively, the data unveil a role of ERCC1/XPF endonuclease in transcription initiation establishing its causal contribution to NER developmental disorders.DNA damage | genetics | metabolism

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“…The expression of key genes known to be altered in old WT mice was also evaluated by qRT-PCR (47). The growth hormone/IGF-1 axis is downregulated in aged mice and progeroid ERCC1-deficient mice (45).…”

Section: K-nbd Alters Nf-κb Signaling In Vivomentioning

confidence: 99%

“…The syndrome is characterized by accelerated aging of virtually all organ systems, all driven by failure to repair stochastic endogenous DNA damage. A murine model of XFE progeroid syndrome, Ercc1 -/Δ mice, have about 10% of the normal amount of ERCC1 protein and spontaneously develop progressive, degenerative changes that correlate strongly with natural aging (43)(44)(45)(46)(47). Thus, Ercc1 -/-mice, which have a complete absence of ERCC1 protein, and Ercc1 -/Δ mice offer a unique opportunity to investigate the mechanism by which one type of cellular damage promotes aging and whether NF-κB plays a pivotal role.…”

Section: Introductionmentioning

confidence: 99%

NF-κB inhibition delays DNA damage–induced senescence and aging in mice

et al. 2012

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The accumulation of cellular damage, including DNA damage, is thought to contribute to aging-related degenerative changes, but how damage drives aging is unknown. XFE progeroid syndrome is a disease of accelerated aging caused by a defect in DNA repair. NF-κB, a transcription factor activated by cellular damage and stress, has increased activity with aging and aging-related chronic diseases. To determine whether NF-κB drives aging in response to the accumulation of spontaneous, endogenous DNA damage, we measured the activation of NF-κB in WT and progeroid model mice. As both WT and progeroid mice aged, NF-κB was activated stochastically in a variety of cell types. Genetic depletion of one allele of the p65 subunit of NF-κB or treatment with a pharmacological inhibitor of the NF-κB-activating kinase, IKK, delayed the age-related symptoms and pathologies of progeroid mice. Additionally, inhibition of NF-κB reduced oxidative DNA damage and stress and delayed cellular senescence. These results indicate that the mechanism by which DNA damage drives aging is due in part to NF-κB activation. IKK/NF-κB inhibitors are sufficient to attenuate this damage and could provide clinical benefit for degenerative changes associated with accelerated aging disorders and normal aging.

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Delayed and Accelerated Aging Share Common Longevity Assurance Mechanisms

Cited by 186 publications

References 40 publications

Relationship Between DNA Damage and Energy Metabolism: Evidence from DNA Repair Deficiency Syndromes

Relationship Between DNA Damage and Energy Metabolism: Evidence from DNA Repair Deficiency Syndromes

Defective transcription initiation causes postnatal growth failure in a mouse model of nucleotide excision repair (NER) progeria

NF-κB inhibition delays DNA damage–induced senescence and aging in mice

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