Mutation Analysis in Bardet-Biedl Syndrome by DNA Pooling and Massively Parallel Resequencing in 105 Individuals

Overview

Journal Hum Genet

Specialty Genetics

Date 2010 Nov 6

PMID 21052717

Citations 42

Authors

Sabine Janssen

Gokul Ramaswami

Erica E Davis

Toby Hurd

Rannar Airik

Jennifer M Kasanuki

Lauren Van Der Kraak

Susan J Allen

Philip L Beales

Nicholas Katsanis

Edgar A Otto

Friedhelm Hildebrandt

Affiliations

Soon will be listed here.

Abstract

Bardet-Biedl syndrome (BBS) is a rare, primarily autosomal-recessive ciliopathy. The phenotype of this pleiotropic disease includes retinitis pigmentosa, postaxial polydactyly, truncal obesity, learning disabilities, hypogonadism and renal anomalies, among others. To date, mutations in 15 genes (BBS1-BBS14, SDCCAG8) have been described to cause BBS. The broad genetic locus heterogeneity renders mutation screening time-consuming and expensive. We applied a strategy of DNA pooling and subsequent massively parallel resequencing (MPR) to screen individuals affected with BBS from 105 families for mutations in 12 known BBS genes. DNA was pooled in 5 pools of 21 individuals each. All 132 coding exons of BBS1-BBS12 were amplified by conventional PCR. Subsequent MPR was performed on an Illumina Genome Analyzer II™ platform. Following mutation identification, the mutation carrier was assigned by CEL I endonuclease heteroduplex screening and confirmed by Sanger sequencing. In 29 out of 105 individuals (28%), both mutated alleles were identified in 10 different BBS genes. A total of 35 different disease-causing mutations were confirmed, of which 18 mutations were novel. In 12 additional families, a total of 12 different single heterozygous changes of uncertain pathogenicity were found. Thus, DNA pooling combined with MPR offers a valuable strategy for mutation analysis of large patient cohorts, especially in genetically heterogeneous diseases such as BBS.

Citing Articles

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