Case report: Biochemical and clinical phenotypes caused by cysteine substitutions in the epidermal growth factor-like domains of fibrillin-1

Liu, Xin; Liu, Kaiqing; Nie, Danyao; Zhang, Jing; Zhang, Liyun; Liu, Xinhua; Wang, Jiantao

doi:10.3389/fgene.2022.928683

Cited by 3 publications

(1 citation statement)

References 36 publications

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“…Вопрос формирования дисульфидных связей имеет важное фундаментальное значение, поскольку раскрывает молекулярные механизмы развития заболеваний, связанных с неправильным сворачиванием (мисфолдингом) белков, окислительным и восстановительным стрессом [11,12]. Неспособность мутантных форм фибриллина-1 формировать дисульфидные связи в EGFподобном домене приводит к развитию синдрома Марфана [13]. Мутантные формы интегринов αIIbβ3 и αvβ3 с неправильным паттерном дисульфидных связей EGF-подобного домена имеют низкий уровень экспрессии на поверхности клетки [14].…”

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The role of disulfide bonds in the formation of the spatial structure of the human epidermal growth factor

Akunevich,

Khrustalev,

Khrustaleva

et al. 2023

Vescì Akademìì navuk Belarusì. Seryâ biâlagičnyh navuk

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The epidermal growth factor (EGF) is a peptide of the EGF-like growth factor family with a common conserved EGF-like domain formed by three intramolecular disulfide bonds. This article describes changes in the spatial structure of EGF and its mutant form with the D46G substitution in its C-terminal fragment observed upon disulfide bonds reduction in the corresponding synthetic peptides in a 0.01 M phosphate buffer (pH = 7.4). The structure was analyzed using circular dichroism spectroscopy, spectrofluorimetry, native polyacrylamide gel electrophoresis, and centrifugal ultrafiltration. It was shown that disulfide bonds reduction changes the geometry of the EGF-like domain towards an increase in the content of the beta-structure, while these peptides remain in dimeric form. According to the molecular modeling results, this can lead to the elongation of the main beta-hairpin of the EGF-like domain, to the elongation of the intermolecular beta-structure, or to the formation of a new beta-structure between the N- and C-terminal fragments of each molecule, which will change the intermolecular interface in dimeric form. Disulfide bonds reduction prevents EGF dimer dissociation to monomers. Under physiological conditions, this can lead to the inability of EGF to form binding sites for EGFR (epidermal growth factor receptor) and to cause its activation.

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The role of disulfide bonds in the formation of the spatial structure of the human epidermal growth factor

Akunevich,

Khrustalev,

Khrustaleva

et al. 2023

Vescì Akademìì navuk Belarusì. Seryâ biâlagičnyh navuk

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The population frequency of Marfan syndrome and the associated cardiac risks in a normal population

Choi,

Huang,

Savige

2024

Preprint

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Marfan syndrome is an autosomal dominantly (AD)-inherited disease that results from pathogenic variants in the Fibrillin 1 (FBN1) gene, and is characterised by tall stature, elongated limbs and digits, lens abnormalities and aortic root dilatation, aneurysms and dissection but milder forms also occur. Radiological imaging suggests that Marfan syndrome affects between one in 3000 and 5000 of the population. The aim of this study was to determine the population frequency of Marfan syndrome from the number of pathogenic FBN1 variants found in a normal variant database. FBN1 variants were downloaded from gnomAD v2.1.1 and annotated with ANNOVAR. The population frequency was determined from the number of pathogenic null and structural variants, and the number of predicted pathogenic missense changes classified by rarity and computational scores. This population frequency was then compared with the frequencies in the control subset, and from gnomAD variants assessed as Pathogenic or Likely pathogenic in the ClinVar or LOVD databases. Our strategy identified predicted pathogenic FBN1 variants in one in 416 individuals, which was confirmed in the control subset (one in 356, p NS). Predicted pathogenic variants were most common in East Asian people (one in 243, p < 0.0001) and least common in Ashkenazim (one in 5,185, p = 0.0082). The population frequencies based on pathogenic variants in the ClinVar or LOVD databases were one in 718 and one in 1014 respectively. Null variants which are associated with aortic aneurysms affected only one in 8624. Thus, Marfan syndrome is more common than previously recognised. Emergency departments and cardiac clinics in particular should be aware of undiagnosed Marfan syndrome and its cardiac risks, but many individuals may have a milder phenotype.

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A New Case Report of Traboulsi Syndrome: A Literature Review and Insights Into Genotype–Phenotype Correlations

Ibarra-Ramírez,

Campos-Acevedo,

Valenzuela-Lopez

et al. 2024

Genes

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Traboulsi syndrome is a rare genetic disorder characterized by facial dysmorphism, lens subluxation, anterior segment anomalies, and spontaneous filtering blebs. The syndrome is due to mutations in the ASPH gene, which plays a crucial role in the development and maintenance of the lens. This case report describes the clinical and genetic findings in a Mexican male with Traboulsi syndrome, highlighting the identification of a novel ASPH variant. A 21-year-old male presented with trauma to the right eye while playing soccer. He had a history of lens subluxation and dysmorphic facial features. Ophthalmic examination revealed right eye lens subluxation into the anterior chamber (with signs of a previous episode of acute angle closure) and left eye posterior and inferior lens subluxation with sectorial iris atrophy. Genetic analysis identified a pathogenic ASPH variant (NM_004318.3:c.1892G>A, p.Trp631*) and a novel likely pathogenic variant (deletion of exons 20–21), confirming Traboulsi syndrome. This is the first instance of Traboulsi syndrome in the Mexican population. The absence of spontaneous filtering blebs in this patient supports previous reports of the wide phenotypic variability that could be related to the type of mutation. This novel ASPH variant expands the known genetic heterogeneity of Traboulsi syndrome.

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Case report: Biochemical and clinical phenotypes caused by cysteine substitutions in the epidermal growth factor-like domains of fibrillin-1

Cited by 3 publications

References 36 publications

The role of disulfide bonds in the formation of the spatial structure of the human epidermal growth factor

The role of disulfide bonds in the formation of the spatial structure of the human epidermal growth factor

The population frequency of Marfan syndrome and the associated cardiac risks in a normal population

A New Case Report of Traboulsi Syndrome: A Literature Review and Insights Into Genotype–Phenotype Correlations

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