A large-scale CRISPR screen reveals context-specific genetic regulation of retinal ganglion cell regeneration

Author:

Emmerich Kevin1234,Hageter John5,Hoang Thanh1267,Lyu Pin12,Sharrock Abigail V.8,Ceisel Anneliese12,Thierer James12,Chunawala Zeeshaan12,Nimmagadda Saumya12,Palazzo Isabella9,Matthews Frazer12,Zhang Liyun12,White David T.12,Rodriguez Catalina12,Graziano Gianna12,Marcos Patrick12,May Adam12,Mulligan Tim12,Reibman Barak12,Saxena Meera T.12,Ackerley David F.8,Qian Jiang12,Blackshaw Seth123491011ORCID,Horstick Eric512,Mumm Jeff S.12341113ORCID

Affiliation:

1. Wilmer Eye Institute 1 and the Department of Ophthalmology , , Baltimore, MD 21287 , USA

2. Johns Hopkins University School of Medicine 1 and the Department of Ophthalmology , , Baltimore, MD 21287 , USA

3. McKusick-Nathans Institute 2 and the Department of Genetic Medicine , , Baltimore, MD 21287 , USA

4. Johns Hopkins University School of Medicine 2 and the Department of Genetic Medicine , , Baltimore, MD 21287 , USA

5. West Virginia University 3 Department of Biology , , Morgantown, WV 26505 , USA

6. University of Michigan School of Medicine 4 Department of Ophthalmology and Visual Sciences , , Ann Arbor, MI 48105 , USA

7. University of Michigan School of Medicine 5 Department of Cell and Developmental Biology , , Ann Arbor, MI 48105 , USA

8. School of Biological Sciences, Victoria University of Wellington 6 , Wellington 6012 , New Zealand

9. Institute for Cell Engineering, Johns Hopkins University School of Medicine 7 , Baltimore, MD 21287 , USA

10. Johns Hopkins University School of Medicine 8 Department of Neurology , , Baltimore, MD 21287 , USA

11. Johns Hopkins University School of Medicine 9 Department of Neuroscience , , Baltimore, MD 21287 , USA

12. West Virginia University 10 Department of Neuroscience , , Morgantown, WV 26506 , USA

13. Center for Nanomedicine, Johns Hopkins University School of Medicine 11 , Baltimore, MD 21287 , USA

Abstract

ABSTRACT Many genes are known to regulate retinal regeneration after widespread tissue damage. Conversely, genes controlling regeneration after limited cell loss, as per degenerative diseases, are undefined. As stem/progenitor cell responses scale to injury levels, understanding how the extent and specificity of cell loss impact regenerative processes is important. Here, transgenic zebrafish enabling selective retinal ganglion cell (RGC) ablation were used to identify genes that regulate RGC regeneration. A single cell multiomics-informed screen of 100 genes identified seven knockouts that inhibited and 11 that promoted RGC regeneration. Surprisingly, 35 out of 36 genes known and/or implicated as being required for regeneration after widespread retinal damage were not required for RGC regeneration. The loss of seven even enhanced regeneration kinetics, including the proneural factors neurog1, olig2 and ascl1a. Mechanistic analyses revealed that ascl1a disruption increased the propensity of progenitor cells to produce RGCs, i.e. increased ‘fate bias’. These data demonstrate plasticity in the mechanism through which Müller glia convert to a stem-like state and context specificity in how genes function during regeneration. Increased understanding of how the regeneration of disease-relevant cell types is specifically controlled will support the development of disease-tailored regenerative therapeutics.

Funder

National Institutes of Health

Brightfocus Foundation

National Science Foundation

Johns Hopkins University School of Medicine

Publisher

The Company of Biologists

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