Revista Brasileira de Cirurgia Plástica (Oct 2024)

Elevated expression of galectin-3 in excessive scars: A pilot study

  • Victor Freire Salomão Ferreira,
  • Felipe Simões Lemos,
  • Roberto Stefan de Almeida Ribeiro,
  • Silvio Renan Pinheiro Victor de-Araújo,
  • Fabio Santiago Figueredo,
  • Maria Lidia de Abreu Silva,
  • Felipe Leite de-Oliveira,
  • Thaís Porto Amadeu

DOI
https://doi.org/10.5935/2177-1235.2024RBCP0936-EN
Journal volume & issue
Vol. 39, no. 3

Abstract

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Introduction: Hypertrophic scars and keloids are types of excessive scars from abnormal skin healing. Galectin-3 (gal-3) is a protein from the lectin family capable of identifying carbohydrates, which can combine and act on different molecules. In the literature, the action of gal-3 as the main regulatory agent of fibrogenesis has already been described and is currently used in anti-fibrotic therapy for various organs such as the lung and liver. The objective of this pilot study was to show preliminary results found in the expression of gal-3 in exacerbated scars. Method: Twenty biopsy samples from excessive scars (16 keloids and 4 hypertrophic scars) and 9 samples from normal scars were collected from 22 women and 7 men. These samples were processed for routine histopathological analysis by immunohistochemistry to detect gal-3. Gal-3 positive cells were quantified by the stereological method using a 36-point grid. Results: Immunohistochemistry showed high expression of gal-3 in endothelial and epithelial cells of all scar samples, as well as expression in cells distributed throughout the dermis. Higher gal-3 expression was found in keloid samples (28% positive cells) compared to normal (18%) and hypertrophic (22%) scars (p = 0.0075). The results were obtained from a small number of patients, as this was a pilot study. Conclusion: The data suggest that gal-3 participates in the healing process and, due to its greater presence in keloid samples, it may be a potential biomarker for keloid formation and a promising therapeutic target to be explored.

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