Author:
Paolacci Stefano,Li Yun,Agolini Emanuele,Bellacchio Emanuele,Arboleda-Bustos Carlos E,Carrero Dido,Bertola Debora,Al-Gazali Lihadh,Alders Mariel,Altmüller Janine,Arboleda Gonzalo,Beleggia Filippo,Bruselles Alessandro,Ciolfi Andrea,Gillessen-Kaesbach Gabriele,Krieg Thomas,Mohammed Shehla,Müller Christian,Novelli Antonio,Ortega Jenny,Sandoval Adrian,Velasco Gloria,Yigit Gökhan,Arboleda Humberto,Lopez-Otin Carlos,Wollnik Bernd,Tartaglia Marco,Hennekam Raoul C
Abstract
BackgroundWiedemann-Rautenstrauch syndrome (WRS) is a form of segmental progeria presenting neonatally, characterised by growth retardation, sparse scalp hair, generalised lipodystrophy with characteristic local fatty tissue accumulations and unusual face. We aimed to understand its molecular cause.MethodsWe performed exome sequencing in two families, targeted sequencing in 10 other families and performed in silico modelling studies and transcript processing analyses to explore the structural and functional consequences of the identified variants.ResultsBiallelic POLR3A variants were identified in eight affected individuals and monoallelic variants of the same gene in four other individuals. In the latter, lack of genetic material precluded further analyses. Multiple variants were found to affect POLR3A transcript processing and were mostly located in deep intronic regions, making clinical suspicion fundamental to detection. While biallelic POLR3A variants have been previously reported in 4H syndrome and adolescent-onset progressive spastic ataxia, recurrent haplotypes specifically occurring in individuals with WRS were detected. All WRS-associated POLR3A amino acid changes were predicted to perturb substantially POLR3A structure/function.ConclusionBiallelic mutations in POLR3A, which encodes for the largest subunit of the DNA-dependent RNA polymerase III, underlie WRS. No isolated functional sites in POLR3A explain the phenotype variability in POLR3A-related disorders. We suggest that specific combinations of compound heterozygous variants must be present to cause the WRS phenotype. Our findings expand the molecular mechanisms contributing to progeroid disorders.
Subject
Genetics (clinical),Genetics
Cited by
40 articles.
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