A circulating biomarker of facioscapulohumeral muscular dystrophy clinical severity, valid in skeletal muscle and blood

Banerji, Christopher R. S.; Grecco, Anna; Joosten, Leo A. B.; Engelen, B.G.M. van; Zammit, Peter S.

doi:10.1101/2022.08.31.506017

Cited by 2 publications

(4 citation statements)

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“…The comprehension of the mechanisms underlying the complex molecular background of FSHD is an area of active research. On this subject, recent studies described transcriptomic and proteomic markers associated with FSHD clinical severity and progression in muscle and blood (Banerji et al, 2019;Corasolla Carregari et al, 2020;Wong et al, 2020;Banerji et al, 2022). In addition, several studies highlighted DNA hypomethylation as a hallmark of disease (Hartwerk et al, 2013;Gaillard et al, 2014;Huichalaf et al, 2014;Calandra et al, 2016;Haynes et al, 2018;Lemmers et al, 2019;Roche et al, 2019;Gould et al, 2021;Banerji et al, 2022;Caputo et al, 2022b;Erdmann et al, 2022;Hiramuki et al, 2022).…”

Section: Discussionmentioning

confidence: 99%

“…On this subject, recent studies described transcriptomic and proteomic markers associated with FSHD clinical severity and progression in muscle and blood (Banerji et al, 2019;Corasolla Carregari et al, 2020;Wong et al, 2020;Banerji et al, 2022). In addition, several studies highlighted DNA hypomethylation as a hallmark of disease (Hartwerk et al, 2013;Gaillard et al, 2014;Huichalaf et al, 2014;Calandra et al, 2016;Haynes et al, 2018;Lemmers et al, 2019;Roche et al, 2019;Gould et al, 2021;Banerji et al, 2022;Caputo et al, 2022b;Erdmann et al, 2022;Hiramuki et al, 2022). In this scenario, the identification of SMCHD1, DNMT3B and LRIF1 as causative or modifier genes in FSHD1 and FSHD2 laid the foundations for considering FSHD as a complex disease, in which multiple genes are likely to contribute to the disease heterogeneity and variability (Caputo et al, 2022a) To this regard, NGS approaches are the ideal tool to allow the S3).…”

Section: Discussionmentioning

confidence: 99%

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Insights in Genetics of Common and Rare Diseases: 2022

2024

Frontiers Research Topics

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Frontiers is more than just an open access publisher of scholarly articles: it is a pioneering approach to the world of academia, radically improving the way scholarly research is managed. The grand vision of Frontiers is a world where all people have an equal opportunity to seek, share and generate knowledge. Frontiers provides immediate and permanent online open access to all its publications, but this alone is not enough to realize our grand goals. Frontiers journal seriesThe Frontiers journal series is a multi-tier and interdisciplinary set of openaccess, online journals, promising a paradigm shift from the current review, selection and dissemination processes in academic publishing. All Frontiers journals are driven by researchers for researchers; therefore, they constitute a service to the scholarly community. At the same time, the Frontiers journal series operates on a revolutionary invention, the tiered publishing system, initially addressing specific communities of scholars, and gradually climbing up to broader public understanding, thus serving the interests of the lay society, too. Dedication to qualityEach Frontiers article is a landmark of the highest quality, thanks to genuinely collaborative interactions between authors and review editors, who include some of the world's best academicians. Research must be certified by peers before entering a stream of knowledge that may eventually reach the public -and shape society; therefore, Frontiers only applies the most rigorous and unbiased reviews. Frontiers revolutionizes research publishing by freely delivering the most outstanding research, evaluated with no bias from both the academic and social point of view. By applying the most advanced information technologies, Frontiers is catapulting scholarly publishing into a new generation. What are Frontiers Research Topics?Frontiers Research Topics are very popular trademarks of the Frontiers journals series: they are collections of at least ten articles, all centered on a particular subject. With their unique mix of varied contributions from Original Research to Review Articles, Frontiers Research Topics unify the most influential researchers, the latest key findings and historical advances in a hot research area.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Insights in Genetics of Common and Rare Diseases: 2022

2024

Frontiers Research Topics

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show abstract

“…The comprehension of the mechanisms underlying the complex molecular background of FSHD is an area of active research. On this subject, recent studies described transcriptomic and proteomic markers associated with FSHD clinical severity and progression in muscle and blood ( Banerji et al, 2019 ; Corasolla Carregari et al, 2020 ; Wong et al, 2020 ; Banerji et al, 2022 ). In addition, several studies highlighted DNA hypomethylation as a hallmark of disease ( Hartwerk et al, 2013 ; Gaillard et al, 2014 ; Huichalaf et al, 2014 ; Calandra et al, 2016 ; Haynes et al, 2018 ; Lemmers et al, 2019 ; Roche et al, 2019 ; Gould et al, 2021 ; Banerji et al, 2022 ; Caputo et al, 2022b ; Erdmann et al, 2022 ; Hiramuki et al, 2022 ).…”

Section: Discussionmentioning

confidence: 99%

“…On this subject, recent studies described transcriptomic and proteomic markers associated with FSHD clinical severity and progression in muscle and blood ( Banerji et al, 2019 ; Corasolla Carregari et al, 2020 ; Wong et al, 2020 ; Banerji et al, 2022 ). In addition, several studies highlighted DNA hypomethylation as a hallmark of disease ( Hartwerk et al, 2013 ; Gaillard et al, 2014 ; Huichalaf et al, 2014 ; Calandra et al, 2016 ; Haynes et al, 2018 ; Lemmers et al, 2019 ; Roche et al, 2019 ; Gould et al, 2021 ; Banerji et al, 2022 ; Caputo et al, 2022b ; Erdmann et al, 2022 ; Hiramuki et al, 2022 ). In this scenario, the identification of SMCHD1 , DNMT3B and LRIF1 as causative or modifier genes in FSHD1 and FSHD2 laid the foundations for considering FSHD as a complex disease, in which multiple genes are likely to contribute to the disease heterogeneity and variability ( Caputo et al, 2022a ) To this regard, NGS approaches are the ideal tool to allow the simultaneous investigation of known FSHD causing ( SMCHD1 , DNMT3B and LRIF1 ) and other potential candidate gene modifiers.…”

Section: Discussionmentioning

confidence: 99%

Whole exome sequencing highlights rare variants in CTCF, DNMT1, DNMT3A, EZH2 and SUV39H1 as associated with FSHD

Strafella,

Caputo,

Bortolani

et al. 2023

Front. Genet.

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Introduction: Despite the progress made in the study of Facioscapulohumeral Dystrophy (FSHD), the wide heterogeneity of disease complicates its diagnosis and the genotype-phenotype correlation among patients and within families. In this context, the present work employed Whole Exome Sequencing (WES) to investigate known and unknown genetic contributors that may be involved in FSHD and may represent potential disease modifiers, even in presence of a D4Z4 Reduced Allele (DRA).Methods: A cohort of 126 patients with clinical signs of FSHD were included in the study, which were characterized by D4Z4 sizing, methylation analysis and WES. Specific protocols were employed for D4Z4 sizing and methylation analysis, whereas the Illumina® Next-Seq 550 system was utilized for WES. The study included both patients with a DRA compatible with FSHD diagnosis and patients with longer D4Z4 alleles. In case of patients harboring relevant variants from WES, the molecular analysis was extended to the family members.Results: The WES data analysis highlighted 20 relevant variants, among which 14 were located in known genetic modifiers (SMCHD1, DNMT3B and LRIF1) and 6 in candidate genes (CTCF, DNMT1, DNMT3A, EZH2 and SUV39H1). Most of them were found together with a permissive short (4–7 RU) or borderline/long DRA (8–20 RU), supporting the possibility that different genes can contribute to disease heterogeneity in presence of a FSHD permissive background. The segregation and methylation analysis among family members, together with clinical findings, provided a more comprehensive picture of patients.Discussion: Our results support FSHD pathomechanism being complex with a multigenic contribution by several known (SMCHD1, DNMT3B, LRIF1) and possibly other candidate genes (CTCF, DNMT1, DNMT3A, EZH2, SUV39H1) to disease penetrance and expressivity. Our results further emphasize the importance of extending the analysis of molecular findings within the proband’s family, with the purpose of providing a broader framework for understanding single cases and allowing finer genotype-phenotype correlations in FSHD-affected families.

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A circulating biomarker of facioscapulohumeral muscular dystrophy clinical severity, valid in skeletal muscle and blood

Cited by 2 publications

References 61 publications

Insights in Genetics of Common and Rare Diseases: 2022

Insights in Genetics of Common and Rare Diseases: 2022

Whole exome sequencing highlights rare variants in CTCF, DNMT1, DNMT3A, EZH2 and SUV39H1 as associated with FSHD

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