Clinical and genetic heterogeneity in laminopathies

Bertrand, Anne T.; Chikhaoui, Khadija; Yaou, Rabah Ben; Bonne, Gisèle

doi:10.1042/bst20110670

Cited by 95 publications

(97 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Conflicting results have been reported regarding the cytoskeletal architecture in lamin-deficient cells, which has been found to be either almost unaffected (Lammerding et al, 2004;Lee et al, 2007;Hale et al, 2008) or disturbed (Khatau et al, 2009;Kim et al, 2012). Moreover, unlike the mouse and cellular models, which often require homozygous expression of the mutant lamin A/C (Worman and Bonne, 2007;Bertrand et al, 2011), human cells from LMNA-related muscular dystrophy carry only one mutated LMNA allele and therefore also express wild-type lamin.…”

Section: Introductionmentioning

confidence: 69%

“…This physical sensing mechanism involves a mechanical link between the extracellular matrix (ECM) and the nucleus through a complex network that involves cell adhesion sites, actinmyosin contractile apparatus and the nucleoskeleton (Geiger et al, 2009), of which lamins are the major component (Méjat and Misteli, 2010;Simon and Wilson, 2011). Mutations in the LMNA gene, which encodes for A-type lamins (lamin A/C), cause laminopathies, a highly heterogeneous group of disorders, including muscular dystrophies and cardiomyopathies (Worman and Bonne, 2007;Bertrand et al, 2011). The severity of the skeletal muscle myopathy is highly variable, the most severe being the LMNA-related congenital muscular dystrophy (L-CMD), that is characterized by an early onset of muscle hypotonia and weakness, joint contractures, spinal stiffness and respiratory involvement (Quijano-Roy et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Cellular micro-environments reveal defective mechanosensing responses and elevated YAP signaling in LMNA-mutated muscle precursors

Bertrand

Ziaei

Ehret

et al. 2014

Journal of Cell Science

Self Cite

101

111

View full text Add to dashboard Cite

The mechanisms underlying the cell response to mechanical forces are crucial for muscle development and functionality. We aim to determine whether mutations of the LMNA gene (which encodes lamin A/C) causing congenital muscular dystrophy impair the ability of muscle precursors to sense tissue stiffness and to respond to mechanical challenge. We found that LMNA-mutated myoblasts embedded in soft matrix did not align along the gel axis, whereas control myoblasts did. LMNA-mutated myoblasts were unable to tune their cytoskeletal tension to the tissue stiffness as attested by inappropriate cell-matrix adhesion sites and cytoskeletal tension in soft versus rigid substrates or after mechanical challenge. Importantly, in soft two-dimensional (2D) and/or static threedimensional (3D) conditions, LMNA-mutated myoblasts showed enhanced activation of the yes-associated protein (YAP) signaling pathway that was paradoxically reduced after cyclic stretch. siRNAmediated downregulation of YAP reduced adhesion and actin stress fibers in LMNA myoblasts. This is the first demonstration that human myoblasts with LMNA mutations have mechanosensing defects through a YAP-dependent pathway. In addition, our data emphasize the crucial role of biophysical attributes of cellular microenvironment to the response of mechanosensing pathways in LMNA-mutated myoblasts.

show abstract

Section: Introductionmentioning

confidence: 69%

Section: Introductionmentioning

confidence: 99%

Cellular micro-environments reveal defective mechanosensing responses and elevated YAP signaling in LMNA-mutated muscle precursors

Bertrand

Ziaei

Ehret

et al. 2014

Journal of Cell Science

Self Cite

101

111

View full text Add to dashboard Cite

show abstract

“…This gene is associated with about 15 different diseases including Emery-Dreifuss muscular dystrophy, limb-girdle muscular dystrophy type 1B and Huntchinson-Gilford progeria that mostly follow an autosomal-dominant mode of inheritance, and CharcotMarie-Tooth disease type 2B1 that is an autosomal recessive disorder. 7 In the field of epilepsy, such a situation has also been observed for several genes. Some variants in POLG are found in families with autosomal-dominant progressive external ophtalmoplegia, whereas other variants cause a range of autosomal-recessive conditions including Alpers syndrome, mitochondrial neurogastrointestinal encephalopathy, or sensory ataxic neuropathy, dysarthria, and ophtalmoparesis syndrome.…”

Section: Discussionmentioning

confidence: 97%

Novel homozygous missense variant of GRIN1 in two sibs with intellectual disability and autistic features without epilepsy

et al. 2017

View full text Add to dashboard Cite

We report on two consanguineous sibs affected with severe intellectual disability and autistic features due to a homozygous missense variant of GRIN1. Massive parallel sequencing was performed using a gene panel including 450 genes related to intellectual disability and autism spectrum disorders. We found a homozygous missense variation of GRIN1 (c.679G4C; p.(Asp227His)) in the two affected sibs, which was inherited from both unaffected heterozygous parents. Heterozygous variants of GRIN1, encoding the GluN1 subunit of the NMDA receptor, have been reported in patients with neurodevelopmental disorders including epileptic encephalopathy, severe intellectual disability, and movement disorders. The p.(Asp227His) variant is located in the same aminoterminal protein domain as the recently published p.(Arg217Trp), which was found at the homozygous state in two patients with a similar phenotype of severe intellectual disability and autistic features but without epilepsy. In silico predictions were consistent with a deleterious effect. The present findings further expand the clinical spectrum of GRIN1 variants and support the existence of hypomorphic variants causing severe neurodevelopmental impairment with autosomal recessive inheritance. European Journal of Human Genetics (2017) 25, 376-380; doi:10.1038/ejhg.2016.163; published online 4 January 2017 INTRODUCTION GRIN1 (MIM *138249) encodes the GluN1 subunit of N-methyl-Daspartate receptors, members of the glutamate receptor channel superfamily, which are heteromeric protein complexes with multiple subunits arranged to form a ligand-gated ion channel. These subunits have a key role in the plasticity of synapses, which underlies memory and learning. 1 De novo heterozygous variants of GRIN1 were first identified by targeted Sanger sequencing in two patients with intellectual disability (ID) with or without epilepsy (MIM #614254). 2 Recent advances in nextgeneration sequencing have shown that GRIN1 de novo heterozygous variants represent a recurrent cause of epileptic encephalopathy with early onset. 3,4 A recent paper provided a better delineation of the GRIN1 phenotypic spectrum that includes severe ID with absent speech, muscular hypotonia, hyperkinetic movements, oculogyric crises, hand stereotypies, cortical blindness, and epilepsy. 5 This article also reported for the first time two homozygous GRIN1 variants in families with severe neurodevelopmental phenotypes.In the present paper we report a second family including two affected sibs with a homozygous missense variant, thus expanding the phenotype-genotype correlations related to GRIN1 variants.

show abstract

“…Lamin A/C are ubiquitous proteins of the nuclear envelope. Mutations in lamin A/C give rise to a group of heterogeneous genetic disorders, collectively referred to as laminopathies, which display a large variety of complex clinical entities including skeletal and cardiac myopathies, lipodystrophy and metabolic abnormalities, neuropathy, leukodystrophy, and premature aging syndromes (4). The pathophysiologic mechanisms underlying the tissue-specific symptoms caused by mutant lamin A/C remain not fully understood.…”

mentioning

confidence: 99%

Deletion of MLIP (Muscle-enriched A-type Lamin-interacting Protein) Leads to Cardiac Hyperactivation of Akt/Mammalian Target of Rapamycin (mTOR) and Impaired Cardiac Adaptation

Cattin

Wang

Weldrick

et al. 2015

Journal of Biological Chemistry

View full text Add to dashboard Cite

show abstract

Clinical and genetic heterogeneity in laminopathies

Cited by 95 publications

References 50 publications

Cellular micro-environments reveal defective mechanosensing responses and elevated YAP signaling in LMNA-mutated muscle precursors

Cellular micro-environments reveal defective mechanosensing responses and elevated YAP signaling in LMNA-mutated muscle precursors

Novel homozygous missense variant of GRIN1 in two sibs with intellectual disability and autistic features without epilepsy

Deletion of MLIP (Muscle-enriched A-type Lamin-interacting Protein) Leads to Cardiac Hyperactivation of Akt/Mammalian Target of Rapamycin (mTOR) and Impaired Cardiac Adaptation

Contact Info

Product

Resources

About