Vertebrate Animal Models of RP59: Current Status and Future Prospects |
| |
| Authors: | Steven J. Fliesler Sriganesh Ramachandra Rao Mai N. Nguyen Mahmoud Tawfik KhalafAllah Steven J. Pittler |
| |
| Affiliation: | 1.Departments of Ophthalmology and Biochemistry, Neuroscience Graduate Program, Jacobs School of Medicine, State University of New York—University at Buffalo, Buffalo, NY 14203, USA;2.Research Service, VA Western NY Healthcare System, Buffalo, NY 14215, USA;3.Department of Optometry and Vision Science, Vision Science Research Center, School of Optometry, University of Alabama at Birmingham, Birmingham, AL 35294, USA |
| |
| Abstract: | Retinitis pigmentosa-59 (RP59) is a rare, recessive form of RP, caused by mutations in the gene encoding DHDDS (dehydrodolichyl diphosphate synthase). DHDDS forms a heterotetrameric complex with Nogo-B receptor (NgBR; gene NUS1) to form a cis-prenyltransferase (CPT) enzyme complex, which is required for the synthesis of dolichol, which in turn is required for protein N-glycosylation as well as other glycosylation reactions in eukaryotic cells. Herein, we review the published phenotypic characteristics of RP59 models extant, with an emphasis on their ocular phenotypes, based primarily upon knock-in of known RP59-associated DHDDS mutations as well as cell type- and tissue-specific knockout of DHDDS alleles in mice. We also briefly review findings in RP59 patients with retinal disease and other patients with DHDDS mutations causing epilepsy and other neurologic disease. We discuss these findings in the context of addressing “knowledge gaps” in our current understanding of the underlying pathobiology mechanism of RP59, as well as their potential utility for developing therapeutic interventions to block the onset or to dampen the severity or progression of RP59. |
| |
| Keywords: | cis-prenyltransferase DHDDS dolichol nogo-B receptor retinal degeneration RP59 |
|
|
