4.8 Article

Transplanted human cones incorporate into the retina and function in a murine cone degeneration model

Journal

JOURNAL OF CLINICAL INVESTIGATION
Volume 132, Issue 12, Pages -

Publisher

AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/JCI154619

Keywords

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Funding

  1. Bundesministerium for Bildung und Forschung (BMBF) ReSight [01EK1613A, 01EK1613E]
  2. Deutsche Forschungsgemeinschaft (DFG) [AD375/7-1]
  3. TU Dresden CRTD
  4. DFG [KA2794/5-1 SPP2127]
  5. State Ministry of Baden-Wuerttemberg for Economic Affairs, Labour and Tourism
  6. European Research Council [ERC-2020-PoC-966709 - iPhotoreceptors]
  7. Deutsche Forschungsgemeinschaft (Cluster of Excellence - ImmunoSensation2 at the University of Bonn) [SPP2127, EXC-2151-390873048]
  8. Volkswagen Foundation [A110720]
  9. European Regional Development Fund (EFRE)
  10. Funding Programs for DZNE Helmholtz [FZT 111, EXC68]
  11. [HGF ExNet-007]

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This study demonstrates the successful incorporation of induced pluripotent stem cell-derived human photoreceptors into mice with cone dysfunction, showing promising potential for the treatment of blinding diseases.
Once human photoreceptors die, they do not regenerate, thus, photoreceptor transplantation has emerged as a potential treatment approach for blinding diseases. Improvements in transplant organization, donor cell maturation, and synaptic connectivity to the host will be critical in advancing this technology for use in clinical practice. Unlike the unstructured grafts of prior cell-suspension transplantations into end-stage degeneration models, we describe the extensive incorporation of induced pluripotent stem cell (iPSC) retinal organoid???derived human photoreceptors into mice with cone dysfunction. This incorporative phenotype was validated in both cone-only as well as pan-photoreceptor transplantations. Rather than forming a glial barrier, M??ller cells extended throughout the graft, even forming a series of adherens junctions between mouse and human cells, reminiscent of an outer limiting membrane. Donor-host interaction appeared to promote polarization as well as the development of morphological features critical for light detection, namely the formation of inner and well-stacked outer segments oriented toward the retinal pigment epithelium. Putative synapse formation and graft function were evident at both structural and electrophysiological levels. Overall, these results show that human photoreceptors interacted readily with a partially degenerated retina. Moreover, incorporation into the host retina appeared to be beneficial to graft maturation, polarization, and function.

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