Elsevier

Genetics in Medicine

Volume 13, Issue 11, November 2011, Pages 978-981
Genetics in Medicine

Brief Report
Novel recessive BFSP2 and PITX3 mutations: Insights into mutational mechanisms from consanguineous populations

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Abstract

Purpose

Designating mutations as recessive or dominant is a function of the effect of the mutant allele on the phenotype. Genes in which both classes of mutations are known to exist are particularly interesting to study because these mutations typically define distinct pathogenic mechanisms at the molecular level.

Methods

We studied two consanguineous families with different eye phenotypes and used a combination of candidate gene analysis and homozygosity mapping to identify the underlying genetic defects.

Results

In one family, a novel BFSP2 mutation causes autosomal recessive diffuse cortical cataract with scattered lens opacities, and in another, a novel PITX3 mutation causes an autosomal recessive severe form of anterior segment dysgenesis and microphthalmia.

Conclusion

We show that BFSP2 and PITX3, hitherto known to cause eye defects only in a dominant fashion, can also present recessively. The likely null nature of both mutations and lack of manifestation in heterozygotes strongly argues for a mechanism other than loss of function in the previously reported dominant mutations in these two genes. Thus, study of consanguineous populations has the additional advantage of not only identifying novel recessive genes but also defining the mutational mechanism of dominant disorders.

Keywords

sclerocornea
recessive mutations
homozygosity
intermediate fibers
BFSP2
PITX3
juvenile cataract

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Disclosure: The authors declare no conflict of interest.