Immunocytochemical characterization of cultured conjunctival explants; marker validation for the identification of squamous epithelial cells and goblet cells.

Front Med (Lausanne)

Laboratory of Cell Biology and Histology, Faculty of Pharmaceutical, Biomedical and Veterinary Sciences, University of Antwerp, Wilrijk, Belgium.

Published: February 2023

AI Article Synopsis

  • Tissue-engineered products offer innovative solutions for repairing severe conjunctival damage, where the body's natural healing processes often lead to scarring instead of full recovery.
  • There is currently a lack of consensus on how to accurately identify and characterize cultured conjunctival cells, particularly squamous epithelial and goblet cells, which are crucial for the efficacy of these engineered products.
  • The study highlights that while some markers, like K7, may not be effective, others (such as MUC1, MUC5AC, and K19) can reliably distinguish different types of conjunctival-derived cells, underlining the importance of proper cellular identification in clinical applications.

Article Abstract

Tissue-engineered products are at the cutting edge of innovation considering their potential to functionally and structurally repair various tissue defects when the body's own regenerative capacity is exhausted. At the ocular surface, the wound healing response to extensive conjunctival damage results in tissue repair with structural alterations or permanent scar formation rather than regeneration of the physiological conjunctiva. Conjunctival tissue engineering therefore represents a promising therapeutic option to reconstruct the ocular surface in severe cicatrizing pathologies. During the rapid race to be a pioneer, it seems that one of the fundamental steps of tissue engineering has been neglected; a proper cellular characterization of the tissue-engineered equivalents, both morphologically and functionally. Currently, no consensus has been reached on an identification strategy and/or markers for the characterization of cultured squamous epithelial and goblet cells. This study therefore evaluated the accuracy of promising markers to identify differentiated conjunctival-derived cells in human primary explant cultures through immunocytochemistry, including keratins (i.e., K7, K13, and K19) and mucins (i.e., MUC1, MUC5AC, and PAS-positivity). Comparison of the and cellular profiles revealed that the widely used goblet cell marker K7 does not function adequately in an setting. The other investigated markers offer a powerful tool to distinguish cultured squamous epithelial cells (i.e., MUC1 and K13), goblet cells (i.e., MUC5AC and PAS-staining), and conjunctival-derived cells in general (i.e., K19). In conclusion, this study emphasizes the power alongside potential pitfalls of conjunctival markers to assess the clinical safety and efficacy of conjunctival tissue-engineered products.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10008928PMC
http://dx.doi.org/10.3389/fmed.2023.1024926DOI Listing

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