Incorporating microglia‐like cells in human induced pluripotent stem cell‐derived retinal organoids

Author:

Chichagova Valeria1ORCID,Georgiou Maria2,Carter Madeleine2,Dorgau Birthe12,Hilgen Gerrit23,Collin Joseph2,Queen Rachel2,Chung Git1,Ajeian Jila1,Moya‐Molina Marina12,Kustermann Stefan4,Pognan Francois5,Hewitt Philip6,Schmitt Michael6,Sernagor Evelyne2,Armstrong Lyle12,Lako Majlinda2

Affiliation:

1. Newcells Biotech Newcastle upon Tyne UK

2. Biosciences Institute Newcastle University Newcastle upon Tyne UK

3. Applied Sciences Northumbria University Newcastle upon Tyne UK

4. F. Hoffmann‐La Roche Ltd Basel Switzerland

5. Novartis Basel Switzerland

6. Merck Healthcare KGaA Darmstadt Germany

Abstract

AbstractMicroglia are the primary resident immune cells in the retina. They regulate neuronal survival and synaptic pruning making them essential for normal development. Following injury, they mediate adaptive responses and under pathological conditions they can trigger neurodegeneration exacerbating the effect of a disease. Retinal organoids derived from human induced pluripotent stem cells (hiPSCs) are increasingly being used for a range of applications, including disease modelling, development of new therapies and in the study of retinogenesis. Despite many similarities to the retinas developed in vivo, they lack some key physiological features, including immune cells. We engineered an hiPSC co‐culture system containing retinal organoids and microglia‐like (iMG) cells and tested their retinal invasion capacity and function. We incorporated iMG into retinal organoids at 13 weeks and tested their effect on function and development at 15 and 22 weeks of differentiation. Our key findings showed that iMG cells were able to respond to endotoxin challenge in monocultures and when co‐cultured with the organoids. We show that retinal organoids developed normally and retained their ability to generate spiking activity in response to light. Thus, this new co‐culture immunocompetent in vitro retinal model provides a platform with greater relevance to the in vivo human retina.

Funder

Biotechnology and Biological Sciences Research Council

Medical Research Council Canada

National Centre for the Replacement, Refinement and Reduction of Animals in Research

Publisher

Wiley

Subject

Cell Biology,Molecular Medicine

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