Heimler Syndrome Is Caused by Hypomorphic Mutations in the Peroxisome-Biogenesis Genes PEX1 and PEX6

Ilham Ratbi; Kim D. Falkenberg; Manou Sommen; Nada Al-Sheqaih; Soukaina Guaoua; Geert Vandeweyer; Jill Urquhart; Kate Chandler; Simon G. Williams; Neil Roberts; Mustapha El Alloussi; Graeme C. Black; Sacha Ferdinandusse; Hind Ramdi; Audrey Heimler; Alan Fryer; Sally Ann Lynch; Nicola Cooper; Kai Ren Ong; Claire E. L. Smith; C.F. Inglehearn; Alan J. Mighell; Claire Elcock; James A. Poulter; Marc Tischkowitz; Sally Davies; Abdelaziz Sefiani; Mironov Aa; William G. Newman; Hans R. Waterham; Guy Van Camp

doi:10.1016/j.ajhg.2015.08.011

Heimler Syndrome Is Caused by Hypomorphic Mutations in the Peroxisome-Biogenesis Genes PEX1 and PEX6

Ilham Ratbi(Mohammed V University), Kim D. Falkenberg(Amsterdam UMC Location University of Amsterdam), Manou Sommen(University of Antwerp), Nada Al-Sheqaih(Manchester Academic Health Science Centre), Soukaina Guaoua(Mohammed V University), Geert Vandeweyer(University of Antwerp), Jill Urquhart(Manchester Academic Health Science Centre), Kate Chandler(Manchester Academic Health Science Centre), Simon G. Williams(Manchester Academic Health Science Centre), Neil Roberts(Manchester Academic Health Science Centre), Mustapha El Alloussi(Mohammed V University), Graeme C. Black(Manchester Academic Health Science Centre), Sacha Ferdinandusse(Amsterdam UMC Location University of Amsterdam), Hind Ramdi(Mohammed V University), Audrey Heimler(Long Island Jewish Medical Center), Alan Fryer(University of Liverpool), Sally Ann Lynch(Children's Health Ireland at Crumlin), Nicola Cooper(Birmingham Women's Hospital), Kai Ren Ong(Birmingham Women's Hospital), Claire E. L. Smith(University of Leeds), C.F. Inglehearn(University of Leeds), Alan J. Mighell(University of Leeds), Claire Elcock(University of Sheffield), James A. Poulter(University of Leeds), Marc Tischkowitz(University of Cambridge), Sally Davies(University Hospital of Wales), Abdelaziz Sefiani(Mohammed V University), Mironov Aa(University of Manchester), William G. Newman(Manchester Academic Health Science Centre), Hans R. Waterham(Amsterdam UMC Location University of Amsterdam), Guy Van Camp(University of Antwerp)

The American Journal of Human Genetics

September 18, 2015

10.1016/j.ajhg.2015.08.011

Cited by 126Open Access

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Abstract

Heimler syndrome (HS) is a rare recessive disorder characterized by sensorineural hearing loss (SNHL), amelogenesis imperfecta, nail abnormalities, and occasional or late-onset retinal pigmentation. We ascertained eight families affected by HS and, by using a whole-exome sequencing approach, identified biallelic mutations in PEX1 or PEX6 in six of them. Loss-of-function mutations in both genes are known causes of a spectrum of autosomal-recessive peroxisome-biogenesis disorders (PBDs), including Zellweger syndrome. PBDs are characterized by leukodystrophy, hypotonia, SNHL, retinopathy, and skeletal, craniofacial, and liver abnormalities. We demonstrate that each HS-affected family has at least one hypomorphic allele that results in extremely mild peroxisomal dysfunction. Although individuals with HS share some subtle clinical features found in PBDs, the diagnosis was not suggested by routine blood and skin fibroblast analyses used to detect PBDs. In conclusion, our findings define HS as a mild PBD, expanding the pleiotropy of mutations in PEX1 and PEX6.

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