THE ROLE OF THE PIGMENT EPITHELIUM IN THE ETIOLOGY OF INHERITED RETINAL DYSTROPHY IN THE RAT

doi:10.1083/jcb.49.3.664

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THE ROLE OF THE PIGMENT EPITHELIUM IN THE ETIOLOGY OF INHERITED RETINAL DYSTROPHY IN THE RAT

Dean Bok ¹ and Michael O. Hall ¹

¹ From the Department of Anatomy and the Jules Stein Eye Institute, University of California at Los Angeles School of Medicine, Los Angeles, California 90024

Visual cell outer segment renewal was studied in eyes of mutantRoyal College of Surgeons (RCS) and Sprague-Dawley (control)rats by a combination of microscopy and radioautography withthe light and electron microscopes. RCS and control rats wereinjected with amino acids-³H at 11 days of age. Radioactiverod outer segment discs were assembled at the outer segmentbase from radioactive proteins synthesized in the rod innersegments. In controls, all radioactive discs assembled at 11days of age were displaced the length of the outer segments,removed from outer segment tips, and phagocytized by the pigmentepithelium by 8 days after injection. In the RCS rats, discassembly and displacement resembled controls for the first 3days after injection. However, as disc assembly continued forsome time thereafter, a layer of labeled, disorganized, lamellardebris accumulated between the outer segment tips and the pigmentepithelium. The buildup of debris was accompanied by visualcell death. At no time during the study was there evidence forphagocytic activity by the pigment epithelium. 61 days afterinjection, the layer of debris was the only heavily radioactivecomponent in the retina. In the retina of RCS rats, the outersegment renewal mechanism malfunctions because the pigment epitheliumdoes not fulfill its normal phagocytic role. The end resultis visual cell death and blindness.

Submitted on August 19, 1970
Revised on November 20, 1970

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