Mutation Screening in Borjeson-Forssman-Lehmann Syndrome: Identification of a Novel De Novo PHF6 Mutation in a Female Patient

Overview

Journal J Med Genet

Specialty Genetics

Date 2005 Jul 5

PMID 15994862

Citations 23

Authors

J Crawford

K M Lower

R C M Hennekam

H Van Esch

A Megarbane

S A Lynch

G Turner

J Gecz

Affiliations

Soon will be listed here.

Abstract

Background: Börjeson-Forssman-Lehmann syndrome (BFLS; MIM 301900) is an infrequently described X linked disorder caused by mutations in PHF6, a novel zinc finger gene of unknown function.

Objective: To present the results of mutation screening in individuals referred for PHF6 testing and discuss the value of prior X-inactivation testing in the mothers of these individuals.

Results: 25 unrelated individuals were screened (24 male, one female). Five PHF6 mutations were detected, two of which (c.940A-->G and c.27_28insA) were novel. One of these new mutations, c.27_28insA, was identified in a female BFLS patient. This was shown to be a de novo mutation arising on the paternal chromosome. This is the first report of a clinically diagnosed BFLS female with a confirmed PHF6 mutation. In addition, the X-inactivation status of the mothers of 19 males with suggested clinical diagnosis of BFLS was determined. Skewed (> or =70%) X-inactivation was present in five mothers, three of whom had sons in whom a PHF6 mutation was detected. The mutation positive female also showed skewing.

Conclusions: The results indicate that the success of PHF6 screening in males suspected of having BFLS is markedly increased if there is a positive family history and/or skewed X-inactivation is found in the mother.

Citing Articles

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Hameed M, Siddiqui F, Sheikh F, Khan M, Admani B, Gangishetti P Brain Neurorehabil. 2023; 16(3):e32.

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