Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation

PURPOSE: Retinal detachment (RD) is one of the most frequently diagnosed ophthalmologic conditions requiring prompt surgical intervention. Combination of proper surgical technique and new diagnostic markers, both clinical and molecular, can help improve the diagnosis and prognosis of RD treatment. M...

Descripción completa

Detalles Bibliográficos
Autores principales: Josifovska, Natasha, Lumi, Xhevat, Szatmari-Tóth, Mária, Kristóf, Endre, Russell, Greg, Nagymihály, Richárd, Anisimova, Natalia, Malyugin, Boris, Kolko, Miriam, Ivastinović, Domagoj, Petrovski, Goran
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6559703/
https://www.ncbi.nlm.nih.gov/pubmed/31185026
http://dx.doi.org/10.1371/journal.pone.0217548
_version_ 1783425850039861248
author Josifovska, Natasha
Lumi, Xhevat
Szatmari-Tóth, Mária
Kristóf, Endre
Russell, Greg
Nagymihály, Richárd
Anisimova, Natalia
Malyugin, Boris
Kolko, Miriam
Ivastinović, Domagoj
Petrovski, Goran
author_facet Josifovska, Natasha
Lumi, Xhevat
Szatmari-Tóth, Mária
Kristóf, Endre
Russell, Greg
Nagymihály, Richárd
Anisimova, Natalia
Malyugin, Boris
Kolko, Miriam
Ivastinović, Domagoj
Petrovski, Goran
author_sort Josifovska, Natasha
collection PubMed
description PURPOSE: Retinal detachment (RD) is one of the most frequently diagnosed ophthalmologic conditions requiring prompt surgical intervention. Combination of proper surgical technique and new diagnostic markers, both clinical and molecular, can help improve the diagnosis and prognosis of RD treatment. METHODS: 12 patients with rhegmatogenous RD (rRD) were included into the study after obtaining patient consent and Regional Ethical Approval (average age: 58.1 ± 17.4 years). OCT was performed before and after 23G vitrectomy for RD. Pure subretinal fluid (SRF) was collected during surgery and analyzed by protein array profiling on a panel of 105 inflammatory cytokines (Human XL Cytokine Array), while the effect of SRF upon human macrophages-driven phagocytosis of apoptotic retinal pigment epithelial (RPE) cells ex vivo was quantified by flow cytometry. Immunohistochemistry (IHC) of retinectomized tissue due to PVR caused by RD was performed to determine presence of markers for microglial cells (CD34), macrophages and activated microglia (CD68), regulator of the immune response to infection (NFkB), progenitor and stem cell marker (Sox2), pluripotency marker (Oct4) and intermediate filament markers (GFAP and Nestin). RESULTS: OCT of fresh RD patients contained pre-operatively hyper reflective points (HRPs) at the detached neuroretina border and proximal to the RPE layer—their size and number decreased following successful reattachment surgery. IHC of the retinectomized tissue from detached retina due to severe PVR showed presence of cell conglomerates at the detached neuroretina border which were positive for CD68, NFkB, Sox2 and GFAP, less positive for CD47 and Nestin and negative for Oct4 and CD34. The SRF contained at least 37 cytokines with higher, and 4 cytokine with lower concentration compared to that in vitreous from non-RD pathology; when used as conditional medium to human macrophages ex vivo, the SRF doubled their capacity for engulfing dying RPEs. CONCLUSIONS: Fresh RD can be hallmarked by presence of HRPs at the detached neuroretina border on OCT; the HRPs decrease in size and number after successful reattachment surgery, and likely resemble the macrophage conglomerates seen by IHC. The neuroretina in RD contains progenitor/stem-like cells and signs of inflammatory reaction, while the SRF contains inflammatory cytokines and other factors which increase the ability of professional phagocytes to engulf dying RPE, or for that matter, other dying cells in the retina.
format Online
Article
Text
id pubmed-6559703
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-65597032019-06-17 Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation Josifovska, Natasha Lumi, Xhevat Szatmari-Tóth, Mária Kristóf, Endre Russell, Greg Nagymihály, Richárd Anisimova, Natalia Malyugin, Boris Kolko, Miriam Ivastinović, Domagoj Petrovski, Goran PLoS One Research Article PURPOSE: Retinal detachment (RD) is one of the most frequently diagnosed ophthalmologic conditions requiring prompt surgical intervention. Combination of proper surgical technique and new diagnostic markers, both clinical and molecular, can help improve the diagnosis and prognosis of RD treatment. METHODS: 12 patients with rhegmatogenous RD (rRD) were included into the study after obtaining patient consent and Regional Ethical Approval (average age: 58.1 ± 17.4 years). OCT was performed before and after 23G vitrectomy for RD. Pure subretinal fluid (SRF) was collected during surgery and analyzed by protein array profiling on a panel of 105 inflammatory cytokines (Human XL Cytokine Array), while the effect of SRF upon human macrophages-driven phagocytosis of apoptotic retinal pigment epithelial (RPE) cells ex vivo was quantified by flow cytometry. Immunohistochemistry (IHC) of retinectomized tissue due to PVR caused by RD was performed to determine presence of markers for microglial cells (CD34), macrophages and activated microglia (CD68), regulator of the immune response to infection (NFkB), progenitor and stem cell marker (Sox2), pluripotency marker (Oct4) and intermediate filament markers (GFAP and Nestin). RESULTS: OCT of fresh RD patients contained pre-operatively hyper reflective points (HRPs) at the detached neuroretina border and proximal to the RPE layer—their size and number decreased following successful reattachment surgery. IHC of the retinectomized tissue from detached retina due to severe PVR showed presence of cell conglomerates at the detached neuroretina border which were positive for CD68, NFkB, Sox2 and GFAP, less positive for CD47 and Nestin and negative for Oct4 and CD34. The SRF contained at least 37 cytokines with higher, and 4 cytokine with lower concentration compared to that in vitreous from non-RD pathology; when used as conditional medium to human macrophages ex vivo, the SRF doubled their capacity for engulfing dying RPEs. CONCLUSIONS: Fresh RD can be hallmarked by presence of HRPs at the detached neuroretina border on OCT; the HRPs decrease in size and number after successful reattachment surgery, and likely resemble the macrophage conglomerates seen by IHC. The neuroretina in RD contains progenitor/stem-like cells and signs of inflammatory reaction, while the SRF contains inflammatory cytokines and other factors which increase the ability of professional phagocytes to engulf dying RPE, or for that matter, other dying cells in the retina. Public Library of Science 2019-06-11 /pmc/articles/PMC6559703/ /pubmed/31185026 http://dx.doi.org/10.1371/journal.pone.0217548 Text en © 2019 Josifovska et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Josifovska, Natasha
Lumi, Xhevat
Szatmari-Tóth, Mária
Kristóf, Endre
Russell, Greg
Nagymihály, Richárd
Anisimova, Natalia
Malyugin, Boris
Kolko, Miriam
Ivastinović, Domagoj
Petrovski, Goran
Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation
title Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation
title_full Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation
title_fullStr Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation
title_full_unstemmed Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation
title_short Clinical and molecular markers in retinal detachment—From hyperreflective points to stem cells and inflammation
title_sort clinical and molecular markers in retinal detachment—from hyperreflective points to stem cells and inflammation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6559703/
https://www.ncbi.nlm.nih.gov/pubmed/31185026
http://dx.doi.org/10.1371/journal.pone.0217548
work_keys_str_mv AT josifovskanatasha clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT lumixhevat clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT szatmaritothmaria clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT kristofendre clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT russellgreg clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT nagymihalyrichard clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT anisimovanatalia clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT malyuginboris clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT kolkomiriam clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT ivastinovicdomagoj clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation
AT petrovskigoran clinicalandmolecularmarkersinretinaldetachmentfromhyperreflectivepointstostemcellsandinflammation

Ejemplares similares