Severe Phenotype of Cutis Laxa Type 1B with Antenatal Signs due to a Novel Homozygous Nonsense Mutation in EFEMP2

Létard, Pascaline; Schepers, Dorien; Albuisson, Juliette; Bruneval, Patrick; Spaggiari, Emmanuel; Beek, Gerarda van de; Khung‐Savatovsky, Suonavy; Belarbi, Nadia; Capri, Yline; Delezoide, Anne‐Lise; Loeys, Bart; Guimiot, Fabien

doi:10.1159/000489838

Cited by 6 publications

(6 citation statements)

References 17 publications

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“…First, both variants are located in the catalytic domain, absent in control databases and predicted deleterious by all in silico prediction algorithms including Polyphen2, SIFT, Provean and Mutation Taster. Second, Lysyl oxidase directly interacts with Fibulin‐4 ( FBLN4 ), the protein deficient in ARCL1B, with similar clinical effects on the vasculature, skin (cutis laxa), skeleton and respiratory system (including diaphragmatic abnormalities) 9,10,13,14 . Third, several LOX knockout mouse models ( Lox −/− ) have been generated that presented with a very similar clinical phenotype to that seen in our patients 5,6,15 .…”

Section: Discussionmentioning

confidence: 74%

“…Second, Lysyl oxidase directly interacts with Fibulin-4 (FBLN4), the protein deficient in ARCL1B, with similar clinical effects on the vasculature, skin (cutis laxa), skeleton and respiratory system (including diaphragmatic abnormalities). 9,10,13,14 Third, several LOX knockout mouse models (Lox À/À ) have been generated that presented with a very similar clinical phenotype to that seen in our patients. 5,6,15 Fourth, the ultrastructural findings can be mice was <20% in skin fibroblasts and aortic smooth muscle cells compared to Lox wt/wt mice.…”

Section: Postnatal Investigations Inmentioning

confidence: 66%

“…Table 1 compares the phenotypic features of the cases presented here and the three known subtypes of ARCL type 1. The associated vascular dilatation and tortuosity, along with bone fragility, resembles most closely the FBLN4 ‐associated subtype (ARCL1B, OMIM #614437), 1,3,9‐11 while the pulmonary hypoplasia resulting in early lethality indicates overlap with ARCL1A and ARCL1C due to FBLN5 (OMIM #604850) and LTBP4 (OMIM #604710) variants respectively. There was no obvious emphysema present in Patients 1 and 2, which is similar to ARCL1B (Unpublished data, B. Callewaert, MD, PhD & A. Beyens, MD, 2020), although X‐ray features of emphysema were present in Patient 3.…”

Section: Discussionmentioning

confidence: 95%

“…Table 1 compares the phenotypic features of the cases presented here and the three known subtypes of ARCL type 1. The associated vascular dilatation and tortuosity, along with bone fragility, resembles most closely the FBLN4-associated subtype (ARCL1B, OMIM #614437), 1,3,[9][10][11] while the pulmonary hypoplasia resulting in early lethality indicates overlap with ARCL1A and ARCL1C due to no relationship to the rate of fracture. 12 Several lines of evidence support the pathogenicity of the LOX variants in the patients' phenotype.…”

Section: Postnatal Investigations Inmentioning

confidence: 99%

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Severe congenital cutis laxa: Identification of novel homozygous LOX gene variants in two families

et al. 2021

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We report three babies from two families with a severe lethal form of congenital cutis laxa. All three had redundant and doughy‐textured skin and two siblings from one family had facial dysmorphism. Echocardiograms showed thickened and poorly contractile hearts, arterial dilatation and tortuosity. Post‐mortem examination in two of the babies further revealed widespread ectasia and tortuosity of medium and large sized arteries, myocardial hypertrophy, rib and skull fractures. The presence of fractures initially suggested a diagnosis of osteogenesis imperfecta. Under light microscopy bony matrices were abnormal and arterial wall architecture was grossly abnormal showing fragmented elastic fibres. Molecular analysis of known cutis laxa genes did not yield any pathogenic defects. Whole exome sequencing of DNA following informed consent identified two separate homozygous variants in the LOX (Lysyl Oxidase) gene. LOX belongs to the 5‐lysyl oxidase gene family involved in initiation of cross‐linking of elastin and collagen. A mouse model of a different variant in this gene recapitulates the phenotype seen in the three babies. Our findings suggest that the LOX gene is a novel cause of severe congenital cutis laxa with arterial tortuosity, bone fragility and respiratory failure.

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Section: Discussionmentioning

confidence: 74%

Section: Postnatal Investigations Inmentioning

confidence: 66%

Section: Discussionmentioning

confidence: 95%

“…Table 1 compares the phenotypic features of the cases presented here and the three known subtypes of ARCL type 1. The associated vascular dilatation and tortuosity, along with bone fragility, resembles most closely the FBLN4-associated subtype (ARCL1B, OMIM #614437), 1,3,[9][10][11] while the pulmonary hypoplasia resulting in early lethality indicates overlap with ARCL1A and ARCL1C due to no relationship to the rate of fracture. 12 Several lines of evidence support the pathogenicity of the LOX variants in the patients' phenotype.…”

Section: Postnatal Investigations Inmentioning

confidence: 99%

See 2 more Smart Citations

Severe congenital cutis laxa: Identification of novel homozygous LOX gene variants in two families

et al. 2021

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“…Given the phenotypic overlap among the different forms, proper differential diagnosis might be challenging as well as predicting the causative gene according to the clinical picture of patients, mainly due to the lack of detailed comparative phenotype data (Berk et al, 2012;Gardeitchik & Morava, 2013;. ARCL1 type 1 is subdivided in ARCL1A (MIM #219100), which is caused by pathogenic variants in the fibulin-5 gene (FBLN5, MIM *604,580) (Elahi et al, 2006;Hu et al, 2006;Loeys et al, 2002;Tekedereli et al, 2019), ARCL1B (MIM #614437) caused by mutations in the EGFcontaining fibulin-like extracellular matrix protein 2 gene or fibulin-4 gene (EFEMP2 or FBLN4; MIM *604,633) (Dasouki et al, 2007;Hucthagowder et al, 2006;Letard et al, 2018), and ARCL1C (MIM #613177), a.k.a. Urban-Rifkin-Davis syndrome, which is due to biallelic variants in the latent transforming growth factor-beta binding protein 4 gene (LTBP4, MIM *604,710) (Callewaert et al, 2013;Su et al, 2015;Urban et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

Clinical and molecular characterization of an 18‐month‐old infant with autosomal recessive cutis laxa type 1C due to a novel LTBP4 pathogenic variant, and literature review

Ritelli

Cammarata‐Scalisi

Cinquina

et al. 2019

Molec Gen & Gen Med

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Background Cutis laxa (CL) is a group of rare connective tissue disorders mainly characterized by wrinkled, redundant, inelastic, and sagging skin. Besides skin anomalies, in most CL forms multiple organs are involved, leading to severe multisystem disorders involving skeletal, cardiovascular, pulmonary, and central nervous systems. CL might be challenging to diagnose because of its different inheritance patterns, extensive phenotypic variability, and genetic heterogeneity. Herein, we report the clinical and molecular characterization of an 18‐month‐old infant with signs suggestive of recessive cutis laxa type 1C (ARCL1C), although with a relatively mild presentation. Methods To confirm the clinical suspicion, mutational screening of all the exons and intron‐flanking regions of the latent transforming growth factor‐beta binding protein 4 gene ( LTBP4 ) was performed by Sanger sequencing on an ABI3130XL Genetic Analyzer. Results Apart from the presence of the dermatological hallmark, the reported patient did not show pulmonary emphysema, which is the most common and discriminative finding of ARCL1C together with gastrointestinal and urinary involvement. Indeed, pulmonary involvement only included episodes of respiratory distress and diaphragmatic eventration; intestinal dilation and tortuosity and hydronephrosis were also present. Molecular analysis disclosed the novel homozygous c.1450del (p.Arg484Glyfs*290) pathogenic variant in exon 12 of LTBP4 , thus leading to the diagnosis of ARCL1C. Conclusion Our findings expand both the knowledge of the clinical phenotype and the allelic repertoire of ARCL1C. The comparison of the patient's features with those of the other patients reported up to now offers future perspectives for clinical research in this field.

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The Spectrum of Acquired Elastolytic Disorders

Gambichler

2021

New and Emerging Entities in Dermatology and Dermatopathology

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Severe Phenotype of Cutis Laxa Type 1B with Antenatal Signs due to a Novel Homozygous Nonsense Mutation in EFEMP2

Cited by 6 publications

References 17 publications

Severe congenital cutis laxa: Identification of novel homozygous LOX gene variants in two families

Severe congenital cutis laxa: Identification of novel homozygous LOX gene variants in two families

Clinical and molecular characterization of an 18‐month‐old infant with autosomal recessive cutis laxa type 1C due to a novel LTBP4 pathogenic variant, and literature review

The Spectrum of Acquired Elastolytic Disorders

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