Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.

Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.

The main objective of this pilot study was to identify circulatory microRNAs in aqueous or plasma that were reflecting changes in vitreous of diabetic retinopathy patients. Aqueous, vitreous and plasma samples were collected from a total of 27 patients undergoing vitreoretinal surgery: 11 controls (...

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Main Authors: Zeljka Smit-McBride, Anthony T Nguyen, Alfred K Yu, Sara P Modjtahedi, Allan A Hunter, Saadia Rashid, Elad Moisseiev, Lawrence S Morse
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0235541
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spelling doaj-0f0ed9ad1116406c86e1f16d9cba92622021-03-03T21:55:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032020-01-01157e023554110.1371/journal.pone.0235541Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.Zeljka Smit-McBrideAnthony T NguyenAlfred K YuSara P ModjtahediAllan A HunterSaadia RashidElad MoisseievLawrence S MorseThe main objective of this pilot study was to identify circulatory microRNAs in aqueous or plasma that were reflecting changes in vitreous of diabetic retinopathy patients. Aqueous, vitreous and plasma samples were collected from a total of 27 patients undergoing vitreoretinal surgery: 11 controls (macular pucker or macular hole patients) and 16 with diabetes mellitus(DM): DM-Type I with proliferative diabetic retinopathy(PDR) (DMI-PDR), DM Type II with PDR(DMII-PDR) and DM Type II with nonproliferative DR(DMII-NPDR). MicroRNAs were isolated using Qiagen microRNeasy kit, quantified on BioAnalyzer, and profiled on Affymetrix GeneChip miRNA 3.0 microarrays. Data were analyzed using Expression Console, Transcriptome Analysis Console, and Ingenuity Pathway Analysis. The comparison analysis of circulatory microRNAs showed that out of a total of 847 human microRNA probes on the microarrays, common microRNAs present both in aqueous and vitreous were identified, and a large number of unique microRNA, dependent on the DM type and severity of retinopathy. Most of the dysregulated microRNAs in aqueous and vitreous of DM patients were upregulated, while in plasma, they were downregulated. Dysregulation of miRNAs in aqueous did not appear to be a good representative of the miRNA abundance in vitreous, or plasma, although a few potential candidates for common biomarkers stood out: let-7b, miR-320b, miR-762 and miR-4488. Additionally, each of the DR subtypes showed miRNAs that were uniquely dysregulated in each fluid (i.e. aqueous: for DMII-NPDR was miR-455-3p; for DMII-PDR was miR-296, and for DMI-PDR it was miR-3202). Pathway analysis identified TGF-beta and VEGF pathways affected. The comparative profiling of circulatory miRNAs showed that a small number of them displayed differential presence in diabetic retinopathy vs. controls. A pattern is emerging of unique molecular microRNA signatures in bodily fluids of DR subtypes, offering promise for the use of ocular fluids and plasma for diagnostic and therapeutic purposes.https://doi.org/10.1371/journal.pone.0235541
collection DOAJ
language English
format Article
sources DOAJ
author Zeljka Smit-McBride
Anthony T Nguyen
Alfred K Yu
Sara P Modjtahedi
Allan A Hunter
Saadia Rashid
Elad Moisseiev
Lawrence S Morse
spellingShingle Zeljka Smit-McBride
Anthony T Nguyen
Alfred K Yu
Sara P Modjtahedi
Allan A Hunter
Saadia Rashid
Elad Moisseiev
Lawrence S Morse
Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.
PLoS ONE
author_facet Zeljka Smit-McBride
Anthony T Nguyen
Alfred K Yu
Sara P Modjtahedi
Allan A Hunter
Saadia Rashid
Elad Moisseiev
Lawrence S Morse
author_sort Zeljka Smit-McBride
title Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.
title_short Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.
title_full Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.
title_fullStr Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.
title_full_unstemmed Unique molecular signatures of microRNAs in ocular fluids and plasma in diabetic retinopathy.
title_sort unique molecular signatures of micrornas in ocular fluids and plasma in diabetic retinopathy.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2020-01-01
description The main objective of this pilot study was to identify circulatory microRNAs in aqueous or plasma that were reflecting changes in vitreous of diabetic retinopathy patients. Aqueous, vitreous and plasma samples were collected from a total of 27 patients undergoing vitreoretinal surgery: 11 controls (macular pucker or macular hole patients) and 16 with diabetes mellitus(DM): DM-Type I with proliferative diabetic retinopathy(PDR) (DMI-PDR), DM Type II with PDR(DMII-PDR) and DM Type II with nonproliferative DR(DMII-NPDR). MicroRNAs were isolated using Qiagen microRNeasy kit, quantified on BioAnalyzer, and profiled on Affymetrix GeneChip miRNA 3.0 microarrays. Data were analyzed using Expression Console, Transcriptome Analysis Console, and Ingenuity Pathway Analysis. The comparison analysis of circulatory microRNAs showed that out of a total of 847 human microRNA probes on the microarrays, common microRNAs present both in aqueous and vitreous were identified, and a large number of unique microRNA, dependent on the DM type and severity of retinopathy. Most of the dysregulated microRNAs in aqueous and vitreous of DM patients were upregulated, while in plasma, they were downregulated. Dysregulation of miRNAs in aqueous did not appear to be a good representative of the miRNA abundance in vitreous, or plasma, although a few potential candidates for common biomarkers stood out: let-7b, miR-320b, miR-762 and miR-4488. Additionally, each of the DR subtypes showed miRNAs that were uniquely dysregulated in each fluid (i.e. aqueous: for DMII-NPDR was miR-455-3p; for DMII-PDR was miR-296, and for DMI-PDR it was miR-3202). Pathway analysis identified TGF-beta and VEGF pathways affected. The comparative profiling of circulatory miRNAs showed that a small number of them displayed differential presence in diabetic retinopathy vs. controls. A pattern is emerging of unique molecular microRNA signatures in bodily fluids of DR subtypes, offering promise for the use of ocular fluids and plasma for diagnostic and therapeutic purposes.
url https://doi.org/10.1371/journal.pone.0235541
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