Lamin A and ZMPSTE24 (FACE-1) defects cause nuclear disorganization and identify restrictive dermopathy as a lethal neonatal laminopathy

Navarro, Claire; Sandre-Giovannoli, Annachiara De; Bernard, R.; Boccaccio, Irène; Boyer, Anthony; Geneviève, David; Hadj‐Rabia, Smail; Gaudy‐Marqueste, C.; Smitt, Henk Sillevis; Vabres, P.; Faivre, Laurence; Verloes, Alain; Essen, Ton van; Flori, Elisabeth; Hennekam, Raoul C. M.; Beemer, Frits A.; Laurent, Nicole; Merrer, Martine Le; Cau, Pierre; Lévy, Nicolas

doi:10.1093/hmg/ddh265

Cited by 320 publications

(321 citation statements)

References 40 publications

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“…The aim of our study was to explore in detail the transcriptional prelamin A-/lamin C-expression patterns associated to the different mutations, in either lymphoblastoid or fibroblast cell lines of the patients. We report for the first time the frequent expression of a 270-nt-deleted prelamin A transcript ('dermopathin') that had only been evidenced before in patients affected with restrictive dermopathy, 15 and correlate our findings to the presence of a common LMNA polymorphism previously described to affect lamin A-/C-expression levels and to the severity of the patients' clinical phenotypes.…”

Section: Introductionsupporting

confidence: 62%

“…[8][9][10] Other LMNA-dominant mutations have been associated with the production of progerin or other deleted prelamin A isoforms (prelamin AΔ35 and prelamin AΔ90). [11][12][13][14][15][16] We enrolled eight patients, including two sibs and a parent of a family in which the disease segregated on an autosomal dominant basis, carrying four different LMNA mutations affecting prelamin A splicing. The aim of our study was to explore in detail the transcriptional prelamin A-/lamin C-expression patterns associated to the different mutations, in either lymphoblastoid or fibroblast cell lines of the patients.…”

Section: Introductionmentioning

confidence: 99%

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Truncated prelamin A expression in HGPS-like patients: a transcriptional study

et al. 2015

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Premature aging syndromes are rare genetic disorders mimicking clinical and molecular features of aging. A recently identified group of premature aging syndromes is linked to mutation of the LMNA gene encoding lamins A and C, and is associated with nuclear deformation and dysfunction. Hutchinson-Gilford progeria syndrome (HGPS) was the first premature aging syndrome linked to LMNA mutation and its molecular bases have been deeply investigated. It is due to a recurrent de novo mutation leading to aberrant splicing and the production of a truncated and toxic nuclear lamin A precursor (prelamin AΔ50), also called progerin. In this work and based on the literature data, we propose to distinguish two main groups of premature aging laminopathies: (1) HGPS and HGP-like syndromes, which share clinical features due to hampered processing and intranuclear toxic accumulation of prelamin A isoforms; and (2) APS (atypical progeria syndromes), due to dominant or recessive missense mutations affecting lamins A and C. Among HGPS-like patients, several deleted prelamin A transcripts (prelamin AΔ50, AΔ35 and AΔ90) have been described. The purpose of this work was to characterize those transcripts in eight patients affected with HGP-like rare syndromes. When fibroblasts were available, the relationships between the presence and ratios of these transcripts and other parameters were studied, aiming to increase our understanding of genotype-phenotype relationships in HGPS-like patients. Altogether our results evidence that progerin accumulation is the major pathogenetic mechanism responsible for HGP-like syndromes due to mutations near the donor splice site of exon 11.

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Section: Introductionsupporting

confidence: 62%

Section: Introductionmentioning

confidence: 99%

Truncated prelamin A expression in HGPS-like patients: a transcriptional study

et al. 2015

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“…This pathology is caused either by dominant de novo LMNA mutations or more frequently by recessive null (homozygous or compound heterozygous) ZMPSTE24 mutations. Depending on the implicated mutation, a farnesylated truncated or wild‐type full prelamin A accumulates in nuclei (Navarro et al., 2004). The Zmpste24 ‐deficient mouse model (Zmpste24 −/− ) presents severe growth retardation and premature death associated with cardiomyopathy, muscular dystrophy, and lipodystrophy (Pendás et al., 2002).…”

Section: Mirnas In Hereditary Laminopathiesmentioning

confidence: 99%

MicroRNAs in hereditary and sporadic premature aging syndromes and other laminopathies

et al. 2018

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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.

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“…The most severe laminopathy, restrictive dermopathy, results in neonatal death. This disease is due to a splicing mutation that skips 90 amino acids of exon 11 [19]. Interestingly, ZMPSTE24 mutations are also reported in MAD and restrictive dermopathy [15,19].…”

Section: Introductionmentioning

confidence: 99%

“…This disease is due to a splicing mutation that skips 90 amino acids of exon 11 [19]. Interestingly, ZMPSTE24 mutations are also reported in MAD and restrictive dermopathy [15,19]. The most striking cardiovascular manifestations of HGPS is a form of severe atherosclerosis.…”

Section: Introductionmentioning

confidence: 99%

Collagen expression in fibroblasts with a novel LMNA mutation

Nguyen

Leistritz

Turner

et al. 2007

Biochemical and Biophysical Research Communications

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Laminopathies are a group of genetic disorders caused by LMNA mutations; they include muscular dystrophies, lipodystrophies and progeroid syndromes. We identified a novel heterozygous LMNA mutation, L59R, in a patient with the general appearance of mandibuloacral dysplasia and progeroid features. Examination of the nuclei of dermal fibroblasts revealed the irregular morphology characteristic of LMNA mutant cells. The nuclear morphological abnormalities of LMNA mutant lymphoblastoid cell lines were less prominent compared to those of primary fibroblasts. Since it has been reported that progeroid features are associated with increased extracellular matrix in dermal tissues, we compared a subset of these components in fibroblast cultures from LMNA mutants with those of control fibroblasts. There was no evidence of intracellular accumulation or altered mobility of collagen chains, or altered conversion of procollagen to collagen, suggesting that skin fibroblastmediated matrix production may not play a significant role in the pathogenesis of this particular laminopathy.

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Lamin A and ZMPSTE24 (FACE-1) defects cause nuclear disorganization and identify restrictive dermopathy as a lethal neonatal laminopathy

Cited by 320 publications

References 40 publications

Truncated prelamin A expression in HGPS-like patients: a transcriptional study

Truncated prelamin A expression in HGPS-like patients: a transcriptional study

MicroRNAs in hereditary and sporadic premature aging syndromes and other laminopathies

Collagen expression in fibroblasts with a novel LMNA mutation

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