Clinical Features of LMNA-Related Cardiomyopathy in 18 Patients and Characterization of Two Novel Variants

Ferradini, Valentina; Cosma, Joseph; Romeo, Fabiana; Masi, Claudia De; Murdocca, Michela; Spitalieri, Paola; Mannucci, Sara; Parlapiano, Giovanni; Lorenzo, Francesca Di; Martino, Annamaria; Fedele, Francesco; Calò, Leonardo; Novelli, Giuseppe; Sangiuolo, Federica; Mango, Ruggiero

doi:10.3390/jcm10215075

Cited by 7 publications

(9 citation statements)

References 60 publications

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“…Moreover, mutations in the LMNA gene result in severe nuclear abnormalities and a higher risk of thromboembolic complications ( 18 , 19 ). Patients carrying LMNA mutations present more aggressive laminopathies and have higher rates of life-threatening arrhythmias and end-stage heart failure ( 21 – 23 ).…”

Section: Discussionmentioning

confidence: 99%

Genomic analysis of a novel pathogenic variant in the gene LMNA associated with cardiac laminopathies found in Ecuadorian siblings: A case report

Guevara-Ramírez

Cadena-Ullauri²,

Ibarra-Castillo³

et al. 2023

Front. Cardiovasc. Med.

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IntroductionCardiac laminopathies are caused by mutations in the LMNA gene and include a wide range of clinical manifestations involving electrical and mechanical changes in cardiomyocytes. In Ecuador, cardiovascular diseases were the primary cause of death in 2019, accounting for 26.5% of total deaths. Cardiac laminopathy-associated mutations involve genes coding for structural proteins with functions related to heart development and physiology.Family descriptionTwo Ecuadorian siblings, self-identified as mestizos, were diagnosed with cardiac laminopathies and suffered embolic strokes. Moreover, by performing Next-Generation Sequencing, a pathogenic variant (NM_170707.3:c.1526del) was found in the gene LMNA.Discussion and conclusionCurrently, genetic tests are an essential step for disease genetic counseling, including cardiovascular disease diagnosis. Identification of a genetic cause that may explain the risk of cardiac laminopathies in a family can help the post-test counseling and recommendations from the cardiologist. In the present report, a pathogenic variant ((NM_170707.3:c.1526del) has been identified in two Ecuadorian siblings with cardiac laminopathies. The LMNA gene codes for A-type laminar proteins that are associated with gene transcription regulation. Mutations in the LMNA gene cause laminopathies, disorders with diverse phenotypic manifestations. Moreover, understanding the molecular biology of the disease-causing mutations is essential in deciding the correct type of treatment.

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Section: Discussionmentioning

confidence: 99%

Genomic analysis of a novel pathogenic variant in the gene LMNA associated with cardiac laminopathies found in Ecuadorian siblings: A case report

Guevara-Ramírez

Cadena-Ullauri²,

Ibarra-Castillo³

et al. 2023

Front. Cardiovasc. Med.

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“…Few studies have made quantitative measurements of nuclear morphology in DCM patients bearing LMNA mutations. Ferradini et al (2021) [ 11 ] reported increased area and elongation but decreased circularity in leukocyte nuclei from DCM patients bearing LMNA missense mutations (Arg189Gln and Glu317Lys). Consistently, our DCM patient with the Ser431* mutation also showed nuclei with decreased circularity and increased elongation; however, in contrast with the report in missense mutations, nuclear area measurements were higher than in wild-type nuclei ( p < 0.001).…”

Section: Discussionmentioning

confidence: 99%

“…The hallmark of laminopathies is the presence of nuclear abnormalities in different cell types, including blebs, herniations, and honeycomb-structures [ 9 ]. Leukocytes are one of several cell types that show nuclear morphology alterations in DCM patients with LMNA mutations [ 10 , 11 ]. However, the molecular mechanisms are not fully understood and are most likely explained by a combination of functional effects that are cell/tissue-specific [ 12 , 13 , 14 , 15 , 16 , 17 , 18 ].…”

Section: Introductionmentioning

confidence: 99%

Leukocyte Nuclear Morphology Alterations in Dilated Cardiomyopathy Caused by a Lamin AC Truncating Mutation (LMNA/Ser431*) Are Modified by the Presence of a LAP2 Missense Polymorphism (TMPO/Arg690Cys)

González-Garrido

Rosas-Madrigal

Rojo‐Domínguez

et al. 2022

IJMS

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The clinical phenotype of LMNA-associated dilated cardiomyopathy (DCM) varies even among individuals who share the same mutation. LMNA encodes lamin AC, which interacts with the lamin-associated protein 2 alpha (LAP2α) encoded by the TMPO gene. The LAP2α/Arg690Cys polymorphism is frequent in Latin America and was previously found to disrupt LAP2α-Lamin AC interactions in vitro. We identified a DCM patient heterozygous for both a lamin AC truncating mutation (Ser431*) and the LAP2α/Arg690Cys polymorphism. We performed protein modeling and docking experiments, and used confocal microscopy to compare leukocyte nuclear morphology among family members with different genotype combinations (wild type, LAP2α Arg690Cys heterozygous, lamin AC/Ser431* heterozygous, and LAP2α Arg690Cys/lamin AC Ser431* double heterozygous). Protein modeling predicted that 690Cys destabilizes the LAP2α homodimer and impairs lamin AC-LAP2α docking. Lamin AC-deficient nuclei (Ser431* heterozygous) showed characteristic blebs and invaginations, significantly decreased nuclear area, and increased elongation, while LAP2α/Arg690Cys heterozygous nuclei showed a lower perimeter and higher circularity than wild-type nuclei. LAP2α Arg690Cys apparently attenuated the effect of LMNA Ser431* on the nuclear area and fully compensated for its effect on nuclear circularity. Altogether, the data suggest that LAP2α/Arg690Cys may be one of the many factors contributing to phenotype variation of LMNA-associated DCM.

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“…We broaden the understanding of interdisease phenotypic variability here by characterizing the global proteomic changes from heterozygous overexpression (mutant and WT) of a nonaggregating (E317 K) 19,20 and two aggregating lamin A mutations (N195 K and Q353 K). 4,21,22 We discovered that there was very little overlap in differentially expressed proteins (DEPs) between any of the mutations; many of which play important roles in cardiac function.…”

Section: ■ Introductionmentioning

confidence: 99%

Global Proteomic Analysis Reveals Alterations in Differentially Expressed Proteins between Cardiopathic Lamin A/C Mutations

Anderson,

Brown,

North

et al. 2024

J. Proteome Res.

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Lamin A/C (LMNA) is an important component of nuclear lamina. Mutations cause arrhythmia, heart failure, and sudden cardiac death. While LMNA-associated cardiomyopathy typically has an aggressive course that responds poorly to conventional heart failure therapies, there is variability in severity and age of penetrance between and even within specific mutations, which is poorly understood at the cellular level. Further, this heterogeneity has not previously been captured to mimic the heterozygous state, nor have the hundreds of clinical LMNA mutations been represented. Herein, we have overexpressed cardiopathic LMNA variants in HEK cells and utilized state-ofthe-art quantitative proteomics to compare the global proteomic profiles of (1) aggregating Q353 K alone, (2) Q353 K coexpressed with WT, (3) aggregating N195 K coexpressed with WT, and (4) nonaggregating E317 K coexpressed with WT to help capture some of the heterogeneity between mutations. We analyzed each data set to obtain the differentially expressed proteins (DEPs) and applied gene ontology (GO) and KEGG pathway analyses. We found a range of 162 to 324 DEPs from over 6000 total protein IDs with differences in GO terms, KEGG pathways, and DEPs important in cardiac function, further highlighting the complexity of cardiac laminopathies. Pathways disrupted by LMNA mutations were validated with redox, autophagy, and apoptosis functional assays in both HEK 293 cells and in induced pluripotent stem cell derived cardiomyocytes (iPSC-CMs) for LMNA N195 K. These proteomic profiles expand our repertoire for mutation-specific downstream cellular effects that may become useful as druggable targets for personalized medicine approach for cardiac laminopathies.

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Clinical Features of LMNA-Related Cardiomyopathy in 18 Patients and Characterization of Two Novel Variants

Cited by 7 publications

References 60 publications

Genomic analysis of a novel pathogenic variant in the gene LMNA associated with cardiac laminopathies found in Ecuadorian siblings: A case report

Genomic analysis of a novel pathogenic variant in the gene LMNA associated with cardiac laminopathies found in Ecuadorian siblings: A case report

Leukocyte Nuclear Morphology Alterations in Dilated Cardiomyopathy Caused by a Lamin AC Truncating Mutation (LMNA/Ser431*) Are Modified by the Presence of a LAP2 Missense Polymorphism (TMPO/Arg690Cys)

Global Proteomic Analysis Reveals Alterations in Differentially Expressed Proteins between Cardiopathic Lamin A/C Mutations

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