Lamin A precursor induces barrier-to-autointegration factor nuclear localization

Capanni, Cristina; Cenni, Vittoria; Haraguchi, Tokuko; Squarzoni, Stefano; Schüchner, Stefan; Ogris, Egon; Novelli, Giuseppe; Maraldi, Nadir M.; Lattanzi, Giovanna

doi:10.4161/cc.9.13.12080

Cited by 38 publications

(53 citation statements)

References 39 publications

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“…Our data add to the evidence that prelamin A is accumulated in normal smooth muscle cells during ageing as an effect of FACE1 downregulation (Ragnauth et al, 2010) and to our previously published data showing a physiological role of prelamin A Capanni et al, 2010;Mattioli et al, 2011). We envisage that a non-modulated, thus inappropriate, response mechanism is activated in laminopathies as a result of molecular defects.…”

Section: Discussionmentioning

confidence: 52%

Centenarian lamins: rapamycin targets in longevity

Lattanzi

Ortolani

Columbaro

et al. 2013

Journal of Cell Science

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The dynamic organisation of the cell nucleus is profoundly modified during growth, development and senescence as a result of changes in chromatin arrangement and gene transcription. A plethora of data suggests that the nuclear lamina is a key player in chromatin dynamics and argues in favour of a major involvement of prelamin A in fundamental mechanisms regulating cellular senescence and organism ageing. As the best model to analyse the role of prelamin A in normal ageing, we used cells from centenarian subjects. We show that prelamin A is accumulated in fibroblasts from centenarians owing to downregulation of its specific endoprotease ZMPSTE24, whereas other nuclear envelope constituents are mostly unaffected and cells do not enter senescence. Accumulation of prelamin A in nuclei of cells from centenarians elicits loss of heterochromatin, as well as recruitment of the inactive form of 53BP1, associated with rapid response to oxidative stress. These effects, including the prelamin-A-mediated increase of nuclear 53BP1, can be reproduced by rapamycin treatment of cells from younger individuals. These data identify prelamin A and 53BP1 as new targets of rapamycin that are associated with human longevity. We propose that the reported mechanisms safeguard healthy ageing in humans through adaptation of the nuclear environment to stress stimuli.

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Section: Discussionmentioning

confidence: 52%

Centenarian lamins: rapamycin targets in longevity

Lattanzi

Ortolani

Columbaro

et al. 2013

Journal of Cell Science

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“…Early DNA methylation alterations at ankyrin 1 (ANK1), disco-interacting protein 2 (DIP2A), rhomboid family member 2 (RHBDF2), ribosomal protein L13 (RPL13), SERPINF1 and SERPINF2 are connected to a network of known AD susceptibility genes and may have a role in the onset of AD [116]. In another study, two genes, SORBS3, involved in cell adhesion, and S100A2, a calcium binding protein, have been found to become progressively more methylated with age and their methylation becomes accelerated in patients with AD [95]. However, not all genes implicated in AD pathogenesis are associated with age-related changes in DNA methylation.…”

Section: Epigenetic Changes In Age-related Diseasesmentioning

confidence: 99%

“…The consequences of such distortion are a loss of peripheral heterochromatin, rampant nuclear disorganization and nuclear lobulation or blebbing [89,94]. Of note, several proteins involved in maintaining nuclear architecture, such as barrier-to-autointegration factor (BAF) [95], inhibitor of growth protein 1 (ING1) [96] and D4Z4 [97], are also frequently lost in progeroid cells. In addition to aberrations in nuclear architecture, HGPS patients display a substantial down regulation of the histone variant γH2AX, an important marker of DNA repair.…”

Section: Epigenetic Changes In Age-related Diseasesmentioning

confidence: 99%

Epigenetic Changes in Aging and Age-related Disease

Rowbotham¹

2015

Aging Sci

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The epigenome refers to the complete set of heritable chemical modifications made to DNA and histone proteins. Certainly, the most well characterized epigenetic mark is the covalent addition of a methyl group to a CpG dinucleotide site in the genome. The DNA methylome-a collection of methyl marks established during embryogenesis-creates a complex regulatory network involved in cell type differentiation, homeostasis and regulating gene expression in response to environmental stimuli and stress throughout life. Collectively, an increasing body of research supports the notion that over time, diverging methylomes may account for substantial phenotypic discordance in monozygotic-twins and explain disparate susceptibilities to age-related disease. We review this evidence and discuss how a greater insight into the mechanisms of age-related epigenetic dysregulation may inform strategies for molecular diagnostics and therapeutic intervention.

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“…Notably, the 50-amino acids deletion that characterizes progerin does not interfere with progerin-BAF binding. Binding of BAF to progerin as well as to LA and prelamin A result in loss of BAF cytoplasmic pool, and in its partial dysfunction probably due to loss of BAF interactions with the chromatin-organizing protein RBBP4 (Capanni et al, 2010). Interestingly, a recessive mutation in BAF causes segmental premature-aging syndrome that resembles HGPS but lacks atherosclerosis (Puente et al, 2011).…”

Section: Barrier-to-autointegration Factor In Hgpsmentioning

confidence: 99%

Hutchinson–Gilford progeria syndrome through the lens of transcription

2013

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SummaryLamins are nuclear intermediate filaments. In addition to their structural roles, they are implicated in basic nuclear functions such as chromatin organization, DNA replication, transcription, DNA repair, and cell-cycle progression. Mutations in human LMNA gene cause several diseases termed laminopathies. One of the laminopathic diseases is Hutchinson-Gilford progeria syndrome (HGPS), which is caused by a spontaneous mutation and characterized by premature aging. HGPS phenotypes share certain similarities with several apparently comparable medical conditions, such as aging and atherosclerosis, with the conspicuous absence of neuronal degeneration and cancer rarity during the short lifespan of the patients. Cell lines from HGPS patients are characterized by multiple nuclear defects, which include abnormal morphology, altered histone modification patterns, and increased DNA damage. These cell lines provide insight into the molecular pathways including senescence that require lamins A and B1. Here, we review recent data on HGPS phenotypes through the lens of transcriptional deregulation caused by lack of functional lamin A, progerin accumulation, and lamin B1 silencing.

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Lamin A precursor induces barrier-to-autointegration factor nuclear localization

Cited by 38 publications

References 39 publications

Centenarian lamins: rapamycin targets in longevity

Centenarian lamins: rapamycin targets in longevity

Epigenetic Changes in Aging and Age-related Disease

Hutchinson–Gilford progeria syndrome through the lens of transcription

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