| Literature DB >> 11462235 |
M G Miano1, F Testa, F Filippini, M Trujillo, I Conte, C Lanzara, J M Millán, C De Bernardo, B Grammatico, M Mangino, I Torrente, R Carrozzo, F Simonelli, E Rinaldi, V Ventruto, M D'Urso, C Ayuso, A Ciccodicola.
Abstract
X-linked Retinitis Pigmentosa (XLRP) shows a huge genetic heterogeneity with almost five distinct loci on the X chromosome. So far, only two XLRP genes have been identified, RPGR (or RP3) and RP2, being mutated in approximately 70% and 10% of the XLRP patients. Clinically there is no clearly significative difference between RP3 and RP2 phenotypes. In the attempt to assess the degree of involvement of the RP2 gene, we performed a complete mutation analysis in a cohort of patients and we identified five novel mutations in five different XLRP families. These mutations include three missense mutations, a splice site mutation, and a single base insertion, which, because of frameshift, anticipates a stop codon. Four mutations fall in RP2 exon 2 and one in exon 3. Evidence that such mutations are different from the 21 RP2 mutations described thus far suggests that a high mutation rate occurs at the RP2 locus, and that most mutations arise independently, without a founder effect. Our mutation analysis confirms the percentage of RP2 mutations detected so far in populations of different ethnic origin. In addition to novel mutations, we report here that a deeper sequence analysis of the RP2 product predicts, in addition to cofactor C homology domain, further putative functional domains, and that some novel mutations identify RP2 amino acid residues which are evolutionary conserved, hence possibly crucial to the RP2 function. Copyright 2001 Wiley-Liss, Inc.Entities:
Mesh:
Year: 2001 PMID: 11462235 DOI: 10.1002/humu.1160
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878