Augmentation of CD47/SIRPα signaling protects cones in genetic models of retinal degeneration
Sean K. Wang, … , Yunlu Xue, Constance L. Cepko
Sean K. Wang, … , Yunlu Xue, Constance L. Cepko
Published July 1, 2021
Citation Information: JCI Insight. 2021;6(16):e150796. https://doi.org/10.1172/jci.insight.150796.
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Research Article Ophthalmology Therapeutics

Augmentation of CD47/SIRPα signaling protects cones in genetic models of retinal degeneration

Abstract

Inherited retinal diseases, such as retinitis pigmentosa (RP), can be caused by thousands of different mutations, a small number of which have been successfully treated with gene replacement. However, this approach has yet to scale and may not be feasible in many cases, highlighting the need for interventions that could benefit more patients. Here, we found that microglial phagocytosis is upregulated during cone degeneration in RP, suggesting that expression of “don’t-eat-me” signals such as CD47 might confer protection to cones. To test this, we delivered an adeno-associated viral (AAV) vector expressing CD47 on cones, which promoted cone survival in 3 mouse models of RP and preserved visual function. Cone rescue with CD47 required a known interacting protein, signal regulatory protein α (SIRPα), but not an alternative interacting protein, thrombospondin-1 (TSP1). Despite the correlation between increased microglial phagocytosis and cone death, microglia were dispensable for the prosurvival activity of CD47, suggesting that CD47 interacts with SIRPα on nonmicroglial cells to alleviate degeneration. These findings establish augmentation of CD47/SIRPα signaling as a potential treatment strategy for RP and possibly other forms of neurodegeneration.

Authors

Sean K. Wang, Yunlu Xue, Constance L. Cepko

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Figure 4

Effect of delayed CD47 expression on cone survival.

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Effect of delayed CD47 expression on cone survival. (A) Schematic of del...
(A) Schematic of delayed AAV expression experiments. P0–P1 rd1;CreERT2/+ mice were subretinally injected with FLEX vectors, which were subsequently activated by i.p. injections of tamoxifen from P19–P21. (B) Representative flat mounts of P30 rd1;CreERT2/+ retinas following infection with AAV8-RedO-FLEX-mCherry with or without i.p. injections of tamoxifen. Boundaries of each retina are depicted in yellow. Scale bars: 1 mm. (C) Representative images of central retinas from P50 rd1;CreERT2/+ mice following infection with AAV8-RedO-GFP plus AAV8-RedO-FLEX-CD47 with or without i.p. injections of tamoxifen. Scale bars: 500 μm. (D) Quantification of GFP-positive cones in central retinas of rd1;CreERT2/+ mice (n = 10–12) following infection with AAV8-RedO-GFP plus AAV8-RedO-FLEX-CD47 with or without i.p. injections of tamoxifen. Data are shown as mean ± SEM. ****P < 0.0001 by 2-tailed Student’s t test.