Please use this identifier to cite or link to this item: 10.1155/2021/6265553
Title: Expression of Otx Genes in Müller Cells Using an In Vitro Experimental Model of Retinal Hypoxia
Authors: Azzolini, Claudio
Donati, Simone
Micheloni, Giovanni
Moretti, Vittoria
Valli, Roberto
Acquati, Francesco
Costantino, Lucy
Ferrara, Fulvio
Borroni, Davide
Premi, Elias
Testa, Francesco
Simonelli, Francesca
Porta, Giovanni
Department of Doctoral Studies
Keywords: 3.1 Basic medicine;3.2 Clinical medicine;1.1. Scientific article indexed in Web of Science and/or Scopus database;Ophthalmology
Issue Date: 2021
Citation: Azzolini , C , Donati , S , Micheloni , G , Moretti , V , Valli , R , Acquati , F , Costantino , L , Ferrara , F , Borroni , D , Premi , E , Testa , F , Simonelli , F & Porta , G 2021 , ' Expression of Otx Genes in Müller Cells Using an In Vitro Experimental Model of Retinal Hypoxia ' , Journal of Ophthalmology , vol. 2021 , 6265553 . https://doi.org/10.1155/2021/6265553
Abstract: Introduction. Müller glial cells typically activate to react to hypoxic tissue damage in several retinal diseases. We evaluated the in vitro response to a hypoxia-mimicking stimulus on the expression of a set of genes, known to contribute to eye morphogenesis and cell differentiation. Materials and Methods. A MIO-M1 Müller cell line was cultured in a hypoxia-mimicking environment by the addition of cobalt chloride to the culture medium, followed by a recovery time in which we mimic restoration from the hypoxic insult. The HIF-1α protein and VEGF-A gene expression were quantified to verify the induction of a hypoxia-like state. Results. Among the genes under study, we did not observe any difference in the expression levels of Otx1 and Otx2 during treatment; conversely, Otx1 was overexpressed during recovery steps. The VEGF-A gene was strongly upregulated at both the CoCl2 and recovery time points. The transactivated isoform (TA) of the TP73 gene showed an overexpression in long-term exposure to the hypoxic stimulus with a further increase after recovery. Discussion. Our molecular analysis is able to describe the activation of a set of genes, never before described, that can drive the response to a hypoxia-like status. The improved comprehension of these cellular events will be useful for designing new therapeutical approaches for retinal pathologies.
Description: Publisher Copyright: Copyright © 2021 Claudio Azzolini et al.
DOI: 10.1155/2021/6265553
ISSN: 2090-004X
Appears in Collections:Research outputs from Pure / Zinātniskās darbības rezultāti no ZDIS Pure

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