Open wound healing in vivo: Monitoring binding and presence of adhesion/growth- regulatory galectins in rat skin during the course of complete re-epithelialization

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Abstract

Galectins are a family of carbohydrate-binding proteins that modulate inflammation and immunity. This functional versatility prompted us to perform a histochemical study of their occurrence during wound healing using rat skin as an in vivo model. Wound healing is a dynamic process that exhibits three basic phases: inflammation, proliferation, and maturation. In this study antibodies against keratins-10 and -14, wide-spectrum cytokeratin, vimentin, and fibronectin, and non-cross-reactive antibodies to galectins-1, -2, and -3 were applied to frozen sections of skin specimens two days (inflammatory phase), seven days (proliferation phase), and twenty-one days (maturation phase) after wounding. The presence of binding sites for galectins-1, -2, -3, and -7 as a measure for assessing changes in reactivity was determined using labeled proteins as probes. Our study detected a series of alterations in galectin parameters during the different phases of wound healing. Presence of galectin-1, for example, increased during the early phase of healing, whereas galectin-3 rapidly decreased in newly formed granulation tissue. In addition, nuclear reactivity of epidermal cells for galectin- 2 occurred seven days post-trauma. The dynamic regulation of galectins during reepithelialization intimates a role of these proteins in skin wound healing, most notably for galectin-1 increasing during the early phases and galectin-3 then slightly increasing during later phases of healing. Such changes may identify a potential target for the development of novel drugs to aid in wound repair and patients' care. © 2011 The Japan Society of Histochemistry and Cytochemistry.

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Gál, P., Vasilenko, T., Kostelníková, M., Jakubco, J., Kováč, I., Sabol, F., … Smetana, K. (2011). Open wound healing in vivo: Monitoring binding and presence of adhesion/growth- regulatory galectins in rat skin during the course of complete re-epithelialization. Acta Histochemica et Cytochemica, 44(5), 191–199. https://doi.org/10.1267/ahc.11014

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