From a Single Whole Exome Read to Notions of Clinical Screening: Primary Ciliary Dyskinesia and RSPH9 P.Lys268del in the Arabian Peninsula

Overview

Journal Ann Hum Genet

Date 2012 Mar 6

PMID 22384920

Citations 16

Authors

Muslim M Alsaadi

Tom R Gaunt

Christopher R Boustred

Philip A I Guthrie

Xuan Liu

Luca Lenzi

Lucille Rainbow

Neil Hall

Khalid K Alharbi

Ian N M Day

Affiliations

Soon will be listed here.

Abstract

Primary ciliary dyskinesia (PCD) is a genetic disorder, usually autosomal recessive, causing early respiratory disease and later subfertility. Whole exome sequencing may enable efficient analysis for locus heterogeneous disorders such as PCD. We whole-exome-sequenced one consanguineous Saudi Arabian with clinically diagnosed PCD and normal laterality, to attempt ab initio molecular diagnosis. We reviewed 13 known PCD genes and potentially autozygous regions (extended homozygosity) for homozygous exon deletions, non-dbSNP codon, splice-site base variants or small indels. Homozygous non-dbSNP changes were also reviewed exome-wide. One single molecular read representing RSPH9 p.Lys268del was observed, with no wild-type reads, and a notable deficiency of mapped reads at this location. Among all observations, RSPH9 was the strongest candidate for causality. Searching unmapped reads revealed seven more mutant reads. Direct assay for p.Lys268del (MboII digest) confirmed homozygosity in the affected individual, then confirmed homozygosity in three siblings with bronchiectasis. Our finding in southwest Saudi Arabia indicates that p.Lys268del, previously observed in two Bedouin families (Israel, UAE), is geographically widespread in the Arabian Peninsula. Analogous with cystic fibrosis CFTR p.Phe508del, screening for RSPH9 p.Lys268del (which lacks sentinel dextrocardia) in those at risk would help in early diagnosis, tailored clinical management, genetic counselling and primary prevention.

Citing Articles

Mapping the Most Common Founder Variant in That Causes Primary Ciliary Dyskinesia in Multiple Consanguineous Families of Bedouin Arabs.

Al-Mutairi D, Alsabah B, Pennekamp P, Omran H J Clin Med. 2023; 12(20).

PMID: 37892643 PMC: 10607267. DOI: 10.3390/jcm12206505.

The Palestinian primary ciliary dyskinesia population: first results of the diagnostic and genetic spectrum.

Rumman N, Fassad M, Driessens C, Goggin P, Abdelrahman N, Adwan A ERJ Open Res. 2023; 9(2).

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A Study on the Genetics of Primary Ciliary Dyskinesia.

Alsamri M, Alabdouli A, Iram D, Alkalbani A, Almarzooqi A, Souid A J Clin Med. 2021; 10(21).

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