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Please use this identifier to cite or link to this item:
http://hdl.handle.net/10174/33739
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Title: | Development of a canine epidermis equivalent model for evaluation of sensitization |
Authors: | Marques, M Nunes, J Ustymenko, B Lagoa, Tânia Fialho, Luísa Martins, Luís Burke, Anthony Souza, E Filho, César Craveiro, Alexandre Costa, Ana Branco, Sandra Antunes, Célia |
Keywords: | Dog skin epidermis wound healing chitosan hydrogels |
Issue Date: | 2-Jul-2022 |
Publisher: | European Academy of Allergy and Clinical Immunology |
Citation: | Marques M, Nunes J, Ustymenko B, Lagoa, T, Fialho L, Martins L, Burke A, Souza EF, Filho CMC, Craveiro AC, Costa AR, Branco S, Antunes CM. Development of a canine epidermis equivalent model for evaluation of sensitization. P1693. ePoster Dermatology. EAACI Hybrid Congress 2022, 1-3 July 2022. |
Abstract: | Background
Canine atopic dermatitis (cAD) is a genetic-predisposed allergic and pruritic
inflammatory skin condition, associated with sensitization to environmental
allergens. Keratinocytes can produce several inflammatory mediators, in response
to several other host mediators, antigens, and pathogens by virtue of their wide
range of surface receptors, some of them dysregulated in cAD individuals.
A histotypical cell cultured-derived tissue may be used to replace animal testing
and are imperative to avoid armful, drawn-out tests to assess chemicals for their
capacity to disrupt skin or cause sensitization. The aim of our study was to
develop a histotypical canine epidermis equivalent, that could be used for the
assessment of skin irritation and sensitization, useful in studies of cAD pathogeny
and pharmacology.
Methods
Canine keratinocytes progenitor cells were seeded in air-lift culture, using an
adapted version of the CELLnTECTM protocol. Irritation and sensitization protocols
were adapted from human equivalent validated tests. For histological analysis,
samples fixed in neutral-buffered formalin and paraffin sections were routinely
processed for biopsies and stained with hematoxylin and eosin.
Results
A multilayer (3-4 cell-layer thick) of canine keratinocytes was developed in air-lift
culture, originating a stratified epidermal-like tissue, confirmed by histological
analysis. This epidermal-like tissue exhibited functional characteristics of the
normal epidermis, showing an adequate impermeabilization after 0.1% Triton X-100
exposure for 4h. Additionally, the epidermis model responded adequately to the
positive [5% SDS, 20% salicylic acid in AOO (acetone and olive oil 4:1)] and
negative (PBS and AOO) controls of the irritation and sensitization tests, assessed
by the quantification of cellular viability and of the secreted IL-18.
Conclusion
As predicted, a canine epidermis analog was developed. This is a promising canine
epidermis model that can be used for the study of skin-derived cAD triggering
factors, and in the development and evaluation of new drugs for topical
applications.
Acknowledgements: Project co-financed by the European Union Fund – Portugal
2020, Alentejo 2020 – Ref. 03/SI/2017 (ALT20-03-247-FEDER-033578). |
URI: | https://eaaci.org/events_congress/eaaci-hybrid-congress-2022/ http://hdl.handle.net/10174/33739 |
Type: | lecture |
Appears in Collections: | MED - Comunicações - Em Congressos Científicos Internacionais
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