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Human conjunctiva organoids to study ocular surface homeostasis and disease. | LitMetric

Human conjunctiva organoids to study ocular surface homeostasis and disease.

Cell Stem Cell

Hubrecht Institute, Royal Netherlands Academy of Arts and Sciences (KNAW), University Medical Center, Utrecht, the Netherlands; Oncode Institute, Hubrecht Institute, Utrecht, the Netherlands. Electronic address:

Published: February 2024

AI Article Synopsis

  • The conjunctival epithelium has two key cell types: goblet cells that produce mucus and keratinocytes that secrete water, with keratinocytes presenting mucins on their surface.
  • Research involves long-term organoid cultures of human and mouse conjunctiva, revealing essential gene expression and identification of conjunctival stem cells.
  • The study also explores viral infections (HSV1, hAdV8, SARS-CoV-2) in conjunctival cultures, demonstrating treatment options for some infections and documenting gene expression changes induced by these viruses, highlighting the potential for organoid transplantation to study conjunctival health and disease.

Article Abstract

The conjunctival epithelium covering the eye contains two main cell types: mucus-producing goblet cells and water-secreting keratinocytes, which present mucins on their apical surface. Here, we describe long-term expanding organoids and air-liquid interface representing mouse and human conjunctiva. A single-cell RNA expression atlas of primary and cultured human conjunctiva reveals that keratinocytes express multiple antimicrobial peptides and identifies conjunctival tuft cells. IL-4/-13 exposure increases goblet and tuft cell differentiation and drastically modifies the conjunctiva secretome. Human NGFR+ basal cells are identified as bipotent conjunctiva stem cells. Conjunctival cultures can be infected by herpes simplex virus 1 (HSV1), human adenovirus 8 (hAdV8), and SARS-CoV-2. HSV1 infection was reversed by acyclovir addition, whereas hAdV8 infection, which lacks an approved drug therapy, was inhibited by cidofovir. We document transcriptional programs induced by HSV1 and hAdV8. Finally, conjunctival organoids can be transplanted. Together, human conjunctiva organoid cultures enable the study of conjunctival (patho)-physiology.

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Source
http://dx.doi.org/10.1016/j.stem.2023.12.008DOI Listing

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