NHE8 Is Essential for RPE Cell Polarity and Photoreceptor Survival.
Document Type
Article
Publication Date
3-20-2015
JAX Source
Sci Rep 2015 Mar 20; 5:9358.
Volume
5
First Page
9358
Last Page
9358
ISSN
2045-2322
PMID
25791178
Abstract
A new N-ethyl-N-nitrosourea (ENU)-induced mouse recessive mutation, identified by fundus examination of the eye, develops depigmented patches, indicating retinal disorder. Histology data show aberrant retinal pigment epithelium (RPE) and late-onset photoreceptor cell loss in the mutant retina. Chromosomal mapping and DNA sequencing reveal a point mutation (T to A) of the Slc9a8 gene, resulting in mutant sodium/proton exchanger 8 (NHE8)-M120K protein. The lysine substitution decreases the probability of forming the 3(rd) transmembrane helix, which impairs the pore structure of the Na(+)/H(+) exchanger. Various RPE defects, including mislocalization of the apical marker ezrin, and disrupted apical microvilli and basal infoldings are observed in mutant mice. We have further generated NHE8 knockout mice and confirmed similar phenotypes, including abnormal RPE cells and late-onset photoreceptor cell loss. Both in vivo and in vitro data indicate that NHE8 co-localizes with ER, Golgi and intracellular vesicles in RPE cells. Thus, NHE8 function is necessary for the survival of photoreceptor cells and NHE8 is important for RPE cell polarity and function. Dysfunctional RPE may ultimately lead to photoreceptor cell death in the NHE8 mutants. Further studies will be needed to elucidate whether or not NHE8 regulates pH homeostasis in the protein secretory pathways of RPE. Sci Rep 2015 Mar 20; 5:9358.
Recommended Citation
Xia C,
Liu H,
Cheung D,
Tang F,
Chang B,
Li M,
Gong X.
NHE8 Is Essential for RPE Cell Polarity and Photoreceptor Survival. Sci Rep 2015 Mar 20; 5:9358.