Nuclear matrix, nuclear envelope and premature aging syndromes in a translational research perspective

Cau, Pierre; Navarro, Claire; Harhouri, Karim; Roll, Patrice; Sigaudy, Sabine; Kaspi, Elise; Perrin, Sophie; Sandre-Giovannoli, Annachiara De; Lévy, Nicolas

doi:10.1016/j.semcdb.2014.03.021

Cited by 64 publications

(72 citation statements)

References 471 publications

(509 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…To this aim, we initially focused on HGPS, caused by the accumulation of a truncated isoform of prelamin A called progerin that is also accumulated during normal ageing 17,18,23,41 . To study the effect of NF-κB blockade on HGPS cell reprogramming, we tested both genetic and pharmacological inhibitory approaches.…”

Section: Nf-κb Blocks Somatic Cell Reprogramming In Hgps and Chronolomentioning

confidence: 99%

NF-κB activation impairs somatic cell reprogramming in ageing

et al. 2015

View full text Add to dashboard Cite

Ageing constitutes a critical impediment to somatic cell reprogramming. We have explored the regulatory mechanisms that constitute age-associated barriers, through derivation of induced pluripotent stem cells (iPSCs) from individuals with premature or physiological ageing. We demonstrate that NF-κB activation blocks the generation of iPSCs in ageing. We also show that NF-κB repression occurs during cell reprogramming towards a pluripotent state. Conversely, ageing-associated NF-κB hyperactivation impairs the generation of iPSCs by eliciting the reprogramming repressor DOT1L, which reinforces senescence signals and downregulates pluripotency genes. Genetic and pharmacological NF-κB inhibitory strategies significantly increase the reprogramming efficiency of fibroblasts from Néstor-Guillermo progeria syndrome and Hutchinson-Gilford progeria syndrome patients, as well as from normal aged donors. Finally, we demonstrate that DOT1L inhibition in vivo extends lifespan and ameliorates the accelerated ageing phenotype of progeroid mice, supporting the interest of studying age-associated molecular impairments to identify targets of rejuvenation strategies.

show abstract

Section: Nf-κb Blocks Somatic Cell Reprogramming In Hgps and Chronolomentioning

confidence: 99%

NF-κB activation impairs somatic cell reprogramming in ageing

et al. 2015

View full text Add to dashboard Cite

show abstract

“…The NL is mainly composed of A-type and B-type lamins and remains located at the nucleoplasmic face of the inner nuclear membrane through its tight interactions with a wide range of transmembrane proteins (Cau et al, 2014). In mammals, there are three major A-type lamins, A, C and a male meiosis-specific isoform C2 and three major B-type lamins, B1, B2 and a spermatid-specific isoform B3.…”

Section: Introductionmentioning

confidence: 99%

Nuclear envelope remodelling during human spermiogenesis involves somatic B-type lamins and a spermatid-specific B3 lamin isoform

Elkhatib

Longepied

Paci

et al. 2014

MHR: Basic Science of Reproductive Medicine

View full text Add to dashboard Cite

The nuclear lamina (NL) is a filamentous protein meshwork, composed essentially of lamins, situated between the inner nuclear membrane and the chromatin. There is mounting evidence that the NL plays a role in spermatid differentiation during spermiogenesis. The mouse spermatid NL is composed of the ubiquitous lamin B1 and the spermatid-specific lamin B3, an N-terminally truncated isoform of lamin B2. However, nothing is known about the NL in human spermatids. We therefore investigated the expression pattern and localization of A-type lamins (A, C and C2) and B-type lamins (B1, B2 and B3) during human spermiogenesis. Here, we show that a lamin B3 transcript is present in human spermatids and that B-type lamins are the only lamins detectable in human spermatids. We determine that, as shown for their mouse counterparts, human lamin B3, but not lamin B2, induces strong nuclear deformation, when ectopically expressed in HeLa cells. Coimmunofluorescence revealed that, in human spermatids, B-type lamins are present at the nuclear periphery, except in the region covered by the acrosome, and that as the spermatid matures the B-type lamins recede towards the posterior pole. Only lamin B1 remains detectable on 33 -47% of ejaculated spermatozoa. On spermatozoa selected for normal head density, however, this fell to ,6%, suggesting that loss of the NL signal may be linked to complete sperm nucleus compaction. The similarities revealed between lamin expression during human and rodent spermiogenesis, strengthen evidence that the NL and lamin B3 have conserved functions during the intense remodelling of the mammalian spermatid nucleus.

show abstract

“…Secondly, the AAX sequence is cleaved by FACE1/ZMPSTE24 or by FACE2/Rce1. Thirdly, the cysteine residue on which the farnesyl group was previously fixed is carboxymethylated by a isoprenylcysteine carboxyl methyltransferase (Cau et al., 2014). After this step, B‐type lamins are mature and remain farnesylated.…”

Section: Lamins and Laminopathiesmentioning

confidence: 99%

“…They bear an NLS leading to their importation into the nucleoplasm. In the nucleus, lamins A and C are constituents of the nuclear matrix: (i) the lamina where they interact with B‐type lamins, with several nuclear envelope transmembrane partner proteins (NETs) of the INM and with the NPC, and (ii) the internal nuclear meshwork forming a component of the nucleoskeleton (Cau et al., 2014; Gruenbaum & Foisner, 2015; Turgay et al., 2017). This lamin meshwork plays a major role in cell structure by conferring the architecture of the nucleoplasm and maintaining the nuclear shape (Ungricht & Kutay, 2017).…”

Section: Lamins and Laminopathiesmentioning

confidence: 99%

MicroRNAs in hereditary and sporadic premature aging syndromes and other laminopathies

et al. 2018

Self Cite

View full text Add to dashboard Cite

SummaryHereditary and sporadic laminopathies are caused by mutations in genes encoding lamins, their partners, or the metalloprotease ZMPSTE24/FACE1. Depending on the clinical phenotype, they are classified as tissue‐specific or systemic diseases. The latter mostly manifest with several accelerated aging features, as in Hutchinson–Gilford progeria syndrome (HGPS) and other progeroid syndromes. MicroRNAs are small noncoding RNAs described as powerful regulators of gene expression, mainly by degrading target mRNAs or by inhibiting their translation. In recent years, the role of these small RNAs has become an object of study in laminopathies using in vitro or in vivo murine models as well as cells/tissues of patients. To date, few miRNAs have been reported to exert protective effects in laminopathies, including miR‐9, which prevents progerin accumulation in HGPS neurons. The recent literature has described the potential implication of several other miRNAs in the pathophysiology of laminopathies, mostly by exerting deleterious effects. This review provides an overview of the current knowledge of the functional relevance and molecular insights of miRNAs in laminopathies. Furthermore, we discuss how these discoveries could help to better understand these diseases at the molecular level and could pave the way toward identifying new potential therapeutic targets and strategies based on miRNA modulation.

show abstract

Nuclear matrix, nuclear envelope and premature aging syndromes in a translational research perspective

Cited by 64 publications

References 471 publications

NF-κB activation impairs somatic cell reprogramming in ageing

NF-κB activation impairs somatic cell reprogramming in ageing

Nuclear envelope remodelling during human spermiogenesis involves somatic B-type lamins and a spermatid-specific B3 lamin isoform

MicroRNAs in hereditary and sporadic premature aging syndromes and other laminopathies

Contact Info

Product

Resources

About