Cerca i identificació del gen de retinitis pigmentària autosòmica recessiva del locus RP26
- Tuson Segarra, Miquel
- Gemma Marfany Nadal Director
- Roser Gonzàlez-Duarte Director
Universidade de defensa: Universitat de Barcelona
Fecha de defensa: 28 de xullo de 2005
- Ángel Carracedo Álvarez Presidente
- Daniel Grinberg Vaisman Secretario/a
- Mónica Bayés Colomer Vogal
- Julio Escribano Martínez Vogal
- Gemma Fabriàs Domingo Vogal
Tipo: Tese
Resumo
Retinitis Pigmentosa (RP), the main cause of adult blindness, is a genetically heterogeneous disorder characterized by progressive loss of photoreceptor cells through apoptosis. Up to now, 32 genes have been implicated in RP. The main goal of this PhD thesis has been the search of a novel autosomal recessive RP gene within the RP26 locus. This locus was identified by linkage analysis on 2q31.2-q32.3. As no obvious positional candidates were found among known genes, an expressed sequence tag (EST) database search was undertaken to identify sequences expressed in the retina. Following this approach, we characterized a novel gene within the RP26 locus, ORMDL1. This gene belonged to a eukaryotic gene family that encoded highly conserved endoplasmic reticulum transmembrane proteins. In the second part of the thesis, we refined the RP26 locus down to 2.5 Mb by homozygosity mapping. After unsuccessful mutational analysis of the nine genes initially reported in this region, a detailed gene search based on expressed-sequence-tag data was undertaken. We finally identified a novel gene encoding a ceramide kinase (CERKL), which encompassed 13 exons. All of the patients from the RP26 family bear a homozygous mutation in exon 5, which generates a premature termination codon. The same mutation was also characterized in another, unrelated, Spanish pedigree with arRP. Human CERKL is expressed in the retina, among other adult and fetal tissues. A more detailed analysis by in situ hybridization on adult murine retina sections shows expression of Cerkl in the ganglion cell layer. Ceramide kinases convert the sphingolipid metabolite ceramide into ceramide-1-phosphate, both key mediators of cellular apoptosis and survival. Ceramide metabolism plays an essential role in the viability of neuronal cells, the membranes of which are particularly rich in sphingolipids. Therefore, CERKL deficiency could shift the relative levels of the signaling sphingolipid metabolites and increase sensitivity of photoreceptor and other retinal cells to apoptotic stimuli. This is the first genetic report suggesting a direct link between retinal neurodegeneration in RP and sphingolipid-mediated apoptosis."