Investigating Embryonic Expression Patterns and Evolution of <em>AHI1</em> and <em>CEP290</em> Genes, Implicated in Joubert Syndrome

Lindsay, S;, Cheng, YZ;, Sayer, JA;, Eley, L;, Overman, LM;, Simms, RJ;, Hynes, AM;, Barker, A;, Dawe, HR

doi:10.1371/journal.pone.0044975

Investigating Embryonic Expression Patterns and Evolution of AHI1 and CEP290 Genes, Implicated in Joubert Syndrome

Lookup NU author(s): Dr YuZhu Cheng, Dr Lorraine Eley, Dr Ann Marie Hynes, Lynne Overman, Dr Roslyn Simms, Emerita Professor Susan Lindsay, Professor John Sayer ORCiD

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Abstract

Joubert syndrome and related diseases (JSRD) are developmental cerebello-oculo-renal syndromes with phenotypes including cerebellar hypoplasia, retinal dystrophy and nephronophthisis (a cystic kidney disease). We have utilised the MRC-Wellcome Trust Human Developmental Biology Resource (HDBR), to perform in-situ hybridisation studies on embryonic tissues, revealing an early onset neuronal, retinal and renal expression pattern for AHI1. An almost identical pattern of expression is seen with CEP290 in human embryonic and fetal tissue. A novel finding is that both AHI1 and CEP290 demonstrate strong expression within the developing choroid plexus, a ciliated structure important for central nervous system development. To test if AHI1 and CEP290 may have co-evolved, we carried out a genomic survey of a large group of organisms across eukaryotic evolution. We found that, in animals, ahi1 and cep290 are almost always found together; however in other organisms either one may be found independent of the other. Finally, we tested in murine epithelial cells if Ahi1 was required for recruitment of Cep290 to the centrosome. We found no obvious differences in Cep290 localisation in the presence or absence of Ahi1, suggesting that, while Ahi1 and Cep290 may function together in the whole organism, they are not interdependent for localisation within a single cell. Taken together these data support a role for AHI1 and CEP290 in multiple organs throughout development and we suggest that this accounts for the wide phenotypic spectrum of AHI1 and CEP290 mutations in man.

Publication metadata

Author(s): Lindsay S; Cheng YZ; Sayer JA; Eley L; Overman LM; Simms RJ; Hynes AM; Barker A; Dawe HR

Publication type: Article

Publication status: Published

Journal: PloS One

Year: 2012

Volume: 7

Issue: 9

Print publication date: 24/09/2012

Date deposited: 20/02/2013

ISSN (electronic): 1932-6203

Publisher: Public Library of Science

URL: http://dx.doi.org/10.1371/journal.pone.0044975

DOI: 10.1371/journal.pone.0044975

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Funding

Funder reference	Funder name
	GlaxoSmithKline
	Kids Kidney Research Fund
	Medical Research Council
	Newcastle Healthcare Charity
	Kidney Research UK
	Northern Counties Kidney Research Fund
0688554/A/02/A	Wellcome Trust
G1001644	Medical Research Council
G9900837	Medical Research Council