Fatal neonatal nephrocutaneous syndrome in 18 Roma children with <i>EGFR</i> deficiency

Background: In this retrospective study, we analysed clinical, biochemical and molecular genetic data of 47 Czech patients with Single, Large-Scale Mitochondrial DNA Deletions (SLSMD). Methods: The diagnosis was based on the long-range PCR (LX-PCR) screening of mtDNA isolated from muscle biopsy in 15 patients, and from the buccal swab, urinary epithelial cells and blood in 32 patients. Results: A total of 57% patients manifested before the age of 16. We did not find any significant difference between paediatric and adult manifestation in either the proportion of patients that would develop extraocular symptoms, or the timespan of its progression. The survival rate in patients with Pearson Syndrome reached 60%. Altogether, five patients manifested with atypical phenotype not fulfilling the latest criteria for SLSMD. No correlation was found between the disease severity and all heteroplasmy levels, lengths of the deletion and respiratory chain activities in muscle. Conclusions: Paediatric manifestation of Progressive External Ophthalmoplegia (PEO) is not associated with a higher risk of multisystemic involvement. Contrary to PEO and Kearns-Sayre Syndrome Spectrum, Pearson Syndrome still contributes to a significant childhood mortality. SLSMD should be considered even in cases with atypical presentation. To successfully identify carriers of SLSMD, a repeated combined analysis of buccal swab and urinary epithelial cells is needed.

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“…Exons of the SSBP1 gene (NM_001256510) were analysed by Sanger sequencing, exome sequencing proceeded as described previously [ 15 ].…”

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confidence: 99%

The Phenotypic Spectrum of 47 Czech Patients with Single, Large-Scale Mitochondrial DNA Deletions

et al. 2020

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“…Dear Editor, We read with great interest the mutation report of fatal neonatal nephrocutaneous syndrome in 18 Roma children by Mazurova et al 1 Systemic inflammatory diseases caused by a germ line mutation in EGFR encoding epidermal growth factor receptor (EGFR) were first reported in 2014, as neonatal inflammatory skin and bowel disease (Online Mendelian Inheritance in Man #616069). 2 Later, Ganetzky et al 3 described a lethal syndrome of epithelial dysfunction with progeroid features caused by the identical EGFR mutation.…”

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confidence: 99%

“…2 Later, Ganetzky et al 3 described a lethal syndrome of epithelial dysfunction with progeroid features caused by the identical EGFR mutation. Mazurova et al 1 reported premature children with multisystem diseases, including one surviving 13-year-old boy with severe skin symptoms including ichthyosiform skin desquamation, as well as dentinogenesis imperfecta, Fanconi-like syndrome and secondary hyperaldosteronism. These findings extend the spectrum of EGFR mutations and provide further evidence for the genetic basis of disorders due to EGFR deficiency.…”

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confidence: 99%

“…These findings extend the spectrum of EGFR mutations and provide further evidence for the genetic basis of disorders due to EGFR deficiency. 1 Inspired by their report, we propose that systemic inflammatory diseases caused by germ line EGFR mutations be categorized as autoinflammatory keratinization diseases (AiKD). 4 Figure 1.…”

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confidence: 99%

“…The clinical features of patients associated with EGFR deficiency were as follows: intrauterine growth restriction, thin, translucent and fragile skin (14/15 cases); skin desquamation (10/17 cases); ichthyosis (9/17 cases); recurrent skin infections and sepsis (9/12 cases); nephromegaly (10/16 cases); and congenital heart defects (7/17 cases). 1 Other possible comorbidities are erythroderma, dentinogenesis imperfecta, tubulopathy, necrotizing enterocolitis/intestinal perforation, testicular retention and hyperimmunoglobulin E, although their frequencies have not been reported. All but one of the children died within 2.5 years after birth.…”

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confidence: 99%

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Systemic inflammatory diseases due to germ line EGFR mutations, with features suggestive of autoinflammatory keratinization diseases

Takeichi

Akiyama

2020

J. Dermatol.

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We read with great interest the mutation report of fatal neonatal nephrocutaneous syndrome in 18 Roma children by Mazurova et al. 1 Systemic inflammatory diseases caused by a germ line mutation in EGFR encoding epidermal growth factor receptor (EGFR) were first reported in 2014, as neonatal inflammatory skin and bowel disease (Online Mendelian Inheritance in Man #616069). 2 Later, Ganetzky et al. 3 described a lethal syndrome of epithelial dysfunction with progeroid features caused by the identical EGFR mutation. Mazurova et al. 1reported premature children with multisystem diseases, including one surviving 13-year-old boy with severe skin symptoms including ichthyosiform skin desquamation, as well as dentinogenesis imperfecta, Fanconi-like syndrome and secondary hyperaldosteronism. These findings extend the spectrum of EGFR mutations and provide further evidence for the genetic basis of disorders due to EGFR deficiency. 1 Inspired by their report, we propose that systemic inflammatory diseases caused by germ line EGFR mutations be categorized as autoinflammatory keratinization diseases (AiKD). 4 Figure 1. Suggested inflammatory pathways and processes induced by germ line EGFR mutations in the present autoinflammatory keratinization disease. CXCL1, C-X-C motif chemokine 1; EGFR, epidermal growth factor receptor; IL, interleukin; JNK1, c-Jun Nterminal kinase 1; NF-jB, nuclear factor-jB; PLA2, phospholipase A2.

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The genetics of monogenic intestinal epithelial disorders

2022

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Monogenic intestinal epithelial disorders, also known as congenital diarrheas and enteropathies (CoDEs), are a group of rare diseases that result from mutations in genes that primarily affect intestinal epithelial cell function. Patients with CoDE disorders generally present with infantile-onset diarrhea and poor growth, and often require intensive fluid and nutritional management. CoDE disorders can be classified into several categories that relate to broad areas of epithelial function, structure, and development. The advent of accessible and low-cost genetic sequencing has accelerated discovery in the field with over 45 different genes now associated with CoDE disorders. Despite this increasing knowledge in the causal genetics of disease, the underlying cellular pathophysiology remains incompletely understood for many disorders. Consequently, clinical management options for CoDE disorders are currently limited and there is an urgent need for new and disorder-specific therapies. In this review, we provide a general overview of CoDE disorders, including a historical perspective of the field and relationship to other monogenic disorders of the intestine. We describe the genetics, clinical presentation, and known pathophysiology for specific disorders. Lastly, we describe the major challenges relating to CoDE disorders, briefly outline key areas that need further study, and provide a perspective on the future genetic and therapeutic landscape.

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Fatal neonatal nephrocutaneous syndrome in 18 Roma children with EGFR deficiency

Cited by 6 publications

References 5 publications

The Phenotypic Spectrum of 47 Czech Patients with Single, Large-Scale Mitochondrial DNA Deletions

The Phenotypic Spectrum of 47 Czech Patients with Single, Large-Scale Mitochondrial DNA Deletions

Systemic inflammatory diseases due to germ line EGFR mutations, with features suggestive of autoinflammatory keratinization diseases

The genetics of monogenic intestinal epithelial disorders

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