Mertk Drives Myosin II Redistribution during Retinal Pigment Epithelial Phagocytosis

doi:10.1167/iovs.08-3058

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Originally published In Press as doi:10.1167/iovs.08-3058 on December 30, 2008
(Investigative Ophthalmology and Visual Science. 2009;50:2427-2435.)
© 2009 by The Association for Research in Vision and Ophthalmology, Inc.
doi:10.1167/iovs.08-3058

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Mertk Drives Myosin II Redistribution during Retinal Pigment Epithelial Phagocytosis

David J. Strick,¹ Wei Feng,¹ and Douglas Vollrath¹^,2

^¹From the Departments of Genetics and ^²Ophthalmology, Stanford University, Stanford, California.

PURPOSE. Mertk is a key phagocytic receptor in the immune, malereproductive, and visual systems. In the retinal pigment epithelium,Mertk is required for the daily ingestion of photoreceptor outersegment (OS) tips. Loss of Mertk function causes retinal degenerationin rats, mice, and humans; however, little is known about themechanism by which Mertk regulates the ingestion phase of retinalpigment epithelial (RPE) phagocytosis. To address this, theauthors sought proteins that associated with Mertk during OSphagocytosis.

METHODS. Lysates of RPE-J cells challenged with OS for varioustimes were immunoprecipitated with Mertk antibody. Potentialinteracting proteins were identified by mass spectrometry andcharacterized with confocal microscopy, pharmacologic inhibition,and siRNA knockdown coupled with an in vitro phagocytic assayin primary RPE cells.

RESULTS. Myh9, the non–muscle myosin II-A heavy chain,was enriched in immunoprecipitates from OS-treated samples.Myosin II-A and II-B isoforms exhibited a striking redistributionin wild-type rat primary RPE cells challenged with OS, movingfrom the cell periphery to colocalize with ingested OS overtime. In contrast, myosin II-A redistribution in response toOS was blunted in primary RPE cells from RCS rats, which lackfunctional Mertk. Wild-type rat primary RPE cells treated withthe myosin II-specific inhibitor blebbistatin or myosin II siRNAsexhibited a significant phagocytic defect.

CONCLUSIONS. Mertk mobilizes myosin II from the RPE cell peripheryto sites of OS engulfment, where myosin II function is essentialfor the normal phagocytic ingestion of OS.

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