[No authors listed]
PURPOSE:Sigma receptors 1 (ÏR1) and 2 (ÏR2) are thought to be two distinct proteins which share the ability to bind multiple ligands, several of which are common to both receptors. Whether ÏR1 and ÏR2 share overlapping biological functions is unknown. Recently, progesterone receptor membrane component 1 (PGRMC1) was shown to contain the putative ÏR2 binding site. PGRMC1 has not been studied in retina. We hypothesize that biological interactions between ÏR1 and PGRMC1 will be evidenced by compensatory upregulation of PGRMC1 in ÏR1(-/-) mice. METHODS:Immunofluorescence, RT-PCR, and immunoblotting methods were used to analyze expression of PGRMC1 in wild-type mouse retina. Tissues from ÏR1(-/-) mice were used to investigate whether a biological interaction exists between ÏR1 and PGRMC1. RESULTS:In the eye, PGRMC1 is expressed in corneal epithelium, lens, ciliary body epithelium, and retina. In retina, PGRMC1 is present in Müller cells and retinal pigment epithelium. This expression pattern is similar, but not identical to ÏR1. PGRMC1 protein levels in neural retina and eye cup from ÏR1(-/-) mice did not differ from wild-type mice. Nonocular tissues, lung, heart, and kidney showed similar Pgrmc1 gene expression in wild-type and ÏR1(-/-) mice. In contrast, liver, brain, and intestine showed increased Pgrmc1 gene expression in ÏR1(-/-) mice. CONCLUSION:Despite potential biological overlap, deletion of ÏR1 did not result in a compensatory change in PGRMC1 protein levels in ÏR1(-/-) mouse retina. Increased Pgrmc1 gene expression in organs with high lipid content such as liver, brain, and intestine indicates a possible tissue-specific interaction between ÏR1 and PGRMC1. The current studies establish the presence of PGRMC1 in retina and lay the foundation for analysis of its biological function.
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