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Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis

The expression pattern of the markers p19, Ki-67, MSX1, MSX2, PDL1, pRB, and CYCLINA2 was quantitatively and semiquantitatively analyzed in histologic sections of the developing and postnatal human eye at week 8, in retinoblastoma, and in various uveal melanomas post hoc studies by double immunofluo...

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Autores principales: Marin Lovrić, Josipa, Filipović, Natalija, Znaor, Ljubo, Rančić, Anita, Petričević, Joško, Kunac, Nenad, Šoljić, Violeta, Saraga-Babić, Mirna, Vukojević, Katarina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9409163/
https://www.ncbi.nlm.nih.gov/pubmed/36012688
http://dx.doi.org/10.3390/ijms23169421
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author Marin Lovrić, Josipa
Filipović, Natalija
Znaor, Ljubo
Rančić, Anita
Petričević, Joško
Kunac, Nenad
Šoljić, Violeta
Saraga-Babić, Mirna
Vukojević, Katarina
author_facet Marin Lovrić, Josipa
Filipović, Natalija
Znaor, Ljubo
Rančić, Anita
Petričević, Joško
Kunac, Nenad
Šoljić, Violeta
Saraga-Babić, Mirna
Vukojević, Katarina
author_sort Marin Lovrić, Josipa
collection PubMed
description The expression pattern of the markers p19, Ki-67, MSX1, MSX2, PDL1, pRB, and CYCLINA2 was quantitatively and semiquantitatively analyzed in histologic sections of the developing and postnatal human eye at week 8, in retinoblastoma, and in various uveal melanomas post hoc studies by double immunofluorescence. The p19 immunoreactivity characterized retinal and/or choroidal cells in healthy and tumor tissues: expression was lower in the postnatal retina than in the developing retina and retinoblastoma, whereas it was high in epithelioid melanomas. Ki67 expression was high in the developing eye, retinoblastoma, and choroidal melanomas. MSX1 and MSX2 expression was similar in the developing eye and retinoblastoma, whereas it was absent in the postnatal eye. Their different expression was evident between epithelioid and myxoid melanomas. Similarly, PDL1 was absent in epithelioid melanomas, whereas it was highly expressed in developing and tumor tissues. Expression of pRB and CYCA2 was characteristic of developing and tumorous eye samples but not of the healthy postnatal eye. The observed expression differences of the analyzed markers correlate with the origin and stage of cell differentiation of the tissue samples. The fine balance of expression could play a role in both human eye development and ocular tumorigenesis. Therefore, understanding their relationship and interplay could open new avenues for potential therapeutic interventions and a better understanding of the mechanisms underlying the developmental plasticity of the eye and the development of neoplasms.
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spelling pubmed-94091632022-08-26 Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis Marin Lovrić, Josipa Filipović, Natalija Znaor, Ljubo Rančić, Anita Petričević, Joško Kunac, Nenad Šoljić, Violeta Saraga-Babić, Mirna Vukojević, Katarina Int J Mol Sci Article The expression pattern of the markers p19, Ki-67, MSX1, MSX2, PDL1, pRB, and CYCLINA2 was quantitatively and semiquantitatively analyzed in histologic sections of the developing and postnatal human eye at week 8, in retinoblastoma, and in various uveal melanomas post hoc studies by double immunofluorescence. The p19 immunoreactivity characterized retinal and/or choroidal cells in healthy and tumor tissues: expression was lower in the postnatal retina than in the developing retina and retinoblastoma, whereas it was high in epithelioid melanomas. Ki67 expression was high in the developing eye, retinoblastoma, and choroidal melanomas. MSX1 and MSX2 expression was similar in the developing eye and retinoblastoma, whereas it was absent in the postnatal eye. Their different expression was evident between epithelioid and myxoid melanomas. Similarly, PDL1 was absent in epithelioid melanomas, whereas it was highly expressed in developing and tumor tissues. Expression of pRB and CYCA2 was characteristic of developing and tumorous eye samples but not of the healthy postnatal eye. The observed expression differences of the analyzed markers correlate with the origin and stage of cell differentiation of the tissue samples. The fine balance of expression could play a role in both human eye development and ocular tumorigenesis. Therefore, understanding their relationship and interplay could open new avenues for potential therapeutic interventions and a better understanding of the mechanisms underlying the developmental plasticity of the eye and the development of neoplasms. MDPI 2022-08-20 /pmc/articles/PMC9409163/ /pubmed/36012688 http://dx.doi.org/10.3390/ijms23169421 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Marin Lovrić, Josipa
Filipović, Natalija
Znaor, Ljubo
Rančić, Anita
Petričević, Joško
Kunac, Nenad
Šoljić, Violeta
Saraga-Babić, Mirna
Vukojević, Katarina
Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis
title Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis
title_full Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis
title_fullStr Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis
title_full_unstemmed Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis
title_short Expression of Cell Cycle Markers and Proliferation Factors during Human Eye Embryogenesis and Tumorigenesis
title_sort expression of cell cycle markers and proliferation factors during human eye embryogenesis and tumorigenesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9409163/
https://www.ncbi.nlm.nih.gov/pubmed/36012688
http://dx.doi.org/10.3390/ijms23169421
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