# A TGFB2/TNF-induced in vitro model of proliferative vitreoretinopathy (PVR) using ARPE-19 cells confirms nicotinamide as an inhibitor of EMT and VEGFA secretion

**Authors:** Yuqing Huang, Roland Meister, Migle Lindziute, Maximilian Binter, Jan Tode, Carsten Framme, Heiko Fuchs, Andre van Wijnen, Andre van Wijnen, Andre van Wijnen, Andre van Wijnen

PMC · DOI: 10.1371/journal.pone.0340614 · PLOS One · 2026-01-13

## TL;DR

A new lab model of eye disease shows that a form of vitamin B3 can reduce harmful cell changes and blood vessel growth linked to vision loss.

## Contribution

A novel in vitro model of PVR using ARPE-19 cells and confirmation of nicotinamide as an inhibitor of EMT and VEGFA secretion.

## Key findings

- TNT stimulation induces EMT-like features including cell elongation and ECM remodeling in ARPE-19 cells.
- Nicotinamide reduces ECM protein expression, cell migration, and VEGFA secretion in the PVR model.
- The model allows real-time tracking of cell migration and multicellular aggregation using live-cell imaging.

## Abstract

Proliferative vitreoretinopathy (PVR) is a vision-threatening fibrotic retinal disorder characterized by the epithelial-mesenchymal transition (EMT) of retinal pigment epithelial (RPE) cells. In this study, we established a pathophysiologically relevant in vitro model by co-stimulating ARPE-19 cells with transforming growth factor beta 2 (TGFB2) and tumor necrosis factor-alpha (TNF), referred to as ‘TNT’, and evaluated the anti-fibrotic and anti-angiogenic effects of Nicotinamide (NAM), a vitamin B3 derivative previously reported to counteract fibrosis in various disease models. Confluent ARPE-19 cells were treated with TGFB2, TNF, or TNT for up to six days. EMT progression was assessed via immunocytochemistry, Western blotting, and collagen gel contraction assays. Live-cell imaging (LCI) combined with Hoechst 33342 nuclear staining and automated tracking using Fiji/TrackMate enabled real-time analysis of cell migration and multicellular aggregation. VEGFA secretion was quantified by ELISA. TNT stimulation induced synergistic EMT-like features, including cell elongation, directional migration, extracellular matrix (ECM) remodeling, gel contraction, and formation of multicellular aggregates. TrackMate-based analysis revealed coordinated nuclear migration under TNT conditions. VEGFA secretion was significantly elevated at early time points. NAM co-treatment reduced ECM protein expression (FN1, COL1A1), attenuated migration and contraction, and significantly lowered VEGFA release. This TNT-based ARPE-19 model represents a robust, live-cell-compatible in vitro system that mimics both fibrotic and pro-angiogenic aspects of PVR. It allows real-time assessment of EMT progression and is suitable for screening anti-fibrotic compounds. Our findings suggest that Nicotinamide mitigates both fibrotic and angiogenic responses in this model and may hold therapeutic potential for fibrotic retinal diseases.

## Linked entities

- **Genes:** TGFB2 (transforming growth factor beta 2) [NCBI Gene 7042], TNF (tumor necrosis factor) [NCBI Gene 7124], FN1 (fibronectin 1) [NCBI Gene 2335], COL1A1 (collagen type I alpha 1 chain) [NCBI Gene 1277], VEGFA (vascular endothelial growth factor A) [NCBI Gene 7422]
- **Proteins:** VEGFA (vascular endothelial growth factor A)
- **Chemicals:** nicotinamide (PubChem CID 936), Hoechst 33342 (PubChem CID 1464)
- **Diseases:** proliferative vitreoretinopathy (MONDO:0100450)

## Full-text entities

- **Genes:** COL1A1 (collagen type I alpha 1 chain) [NCBI Gene 1277] {aka CAFYD, EDSARTH1, EDSC, OI1, OI2, OI3}, POTEF (POTE ankyrin domain family member F) [NCBI Gene 728378] {aka A26C1B, POTE2alpha, POTEACTIN}, CDH2 (cadherin 2) [NCBI Gene 1000] {aka ACOGS, ADHD8, ARVD14, CD325, CDHN, CDw325}, Fn1 (fibronectin 1) [NCBI Gene 14268] {aka E330027I09, Fn, Fn-1}, GAPDH (glyceraldehyde-3-phosphate dehydrogenase) [NCBI Gene 2597] {aka G3PD, GAPD, HEL-S-162eP}, Tjp1 (tight junction protein 1) [NCBI Gene 21872] {aka ZO1}, TNF (tumor necrosis factor) [NCBI Gene 7124] {aka DIF, IMD127, TNF-alpha, TNFA, TNFSF2, TNLG1F}, IL6 (interleukin 6) [NCBI Gene 3569] {aka BSF-2, BSF2, CDF, HGF, HSF, IFN-beta-2}, FGF2 (fibroblast growth factor 2) [NCBI Gene 2247] {aka BFGF, FGF-2, FGFB, HBGF-2}, CXCL8 (C-X-C motif chemokine ligand 8) [NCBI Gene 3576] {aka GCP-1, GCP1, IL8, LECT, LUCT, LYNAP}, MAPK14 (mitogen-activated protein kinase 14) [NCBI Gene 1432] {aka CSBP, CSBP1, CSBP2, CSPB1, EXIP, Mxi2}, C16orf82 (chromosome 16 open reading frame 82) [NCBI Gene 162083] {aka TNT}, LAP (Laryngeal adductor paralysis) [NCBI Gene 7939], F10 (coagulation factor X) [NCBI Gene 2159] {aka FX, FXA}, SMN1 (survival of motor neuron 1, telomeric) [NCBI Gene 6606] {aka BCD541, GEMIN1, SMA, SMA1, SMA2, SMA3}, ACTA1 (actin alpha 1, skeletal muscle) [NCBI Gene 58] {aka ACTA, ASMA, CFTD, CFTD1, CFTDM, CMYO2A}, PVR (PVR cell adhesion molecule) [NCBI Gene 5817] {aka CD155, HVED, NECL5, Necl-5, PVS, TAGE4}, OCLN (occludin) [NCBI Gene 100506658] {aka BLCPMG, PPP1R115, PTORCH1}, IFNG (interferon gamma) [NCBI Gene 3458] {aka IFG, IFI, IMD69}, TGFB2 (transforming growth factor beta 2) [NCBI Gene 7042] {aka CAEND2, G-TSF, LDS4, TGF-beta2}, CDH1 (cadherin 1) [NCBI Gene 999] {aka Arc-1, BCDS1, CD324, CDHE, ECAD, LCAM}, CCL2 (C-C motif chemokine ligand 2) [NCBI Gene 6347] {aka GDCF-2, HC11, HSMCR30, MCAF, MCP-1, MCP1}, SIRT1 (sirtuin 1) [NCBI Gene 23411] {aka SIR2, SIR2L1, SIR2alpha}, FN1 (fibronectin 1) [NCBI Gene 2335] {aka CIG, ED-B, FINC, FN, FNZ, GFND}, Col1a1 (collagen, type I, alpha 1) [NCBI Gene 12842] {aka Col1a-1, Cola-1, Cola1, Mov-13, Mov13}, SDCBP (syndecan binding protein) [NCBI Gene 6386] {aka MDA-9, MDA9, SDCBP1, ST1, SYCL, TACIP18}, TGFB1 (transforming growth factor beta 1) [NCBI Gene 7040] {aka CAEND1, CED, DPD1, IBDIMDE, LAP, TGF-beta1}, VIM (vimentin) [NCBI Gene 7431], VEGFA (vascular endothelial growth factor A) [NCBI Gene 7422] {aka L-VEGF, MVCD1, VEGF, VPF}, GREM1 (gremlin 1, DAN family BMP antagonist) [NCBI Gene 26585] {aka C15DUPq, CKTSF1B1, CRAC1, CRCS4, DAND2, DRM}, PGF (placental growth factor) [NCBI Gene 5228] {aka D12S1900, PGFL, PIGF, PLGF, PlGF-2, SHGC-10760}, NFKB1 (nuclear factor kappa B subunit 1) [NCBI Gene 4790] {aka CVID12, EBP-1, KBF1, NF-kB, NF-kB1, NF-kappa-B1}
- **Diseases:** fibrotic retinal diseases (MESH:D012164), Fibrosis (MESH:D005355), cancer (MESH:D009369), RRD (MESH:C563710), neurodegeneration (MESH:D019636), inflammation (MESH:D007249), phototoxicity (MESH:D017484), cytotoxicity (MESH:D064420), PVR (MESH:D018630), retinal disorder (MESH:D012173), retinal detachment (MESH:D012163), ocular trauma (MESH:D014947)
- **Chemicals:** CO2 (MESH:D002245), AlexaFluor 488 (MESH:C000711379), Tween 20 (MESH:D011136), NAD + (MESH:D009243), Penicillin (MESH:D010406), DMEM (-), Triton X-100 (MESH:D017830), PBS (MESH:D007854), paraformaldehyde (MESH:C003043), Phalloidin (MESH:D010590), 2-mercaptoethanol (MESH:D008623), Hoechst 33342 (MESH:C017807), melanin (MESH:D008543), PI (MESH:D011419), Streptomycin (MESH:D013307), ethanol (MESH:D000431), polyacrylamide (MESH:C016679), F12 (MESH:C007782), GlutaMAX (MESH:C054122), DAPI (MESH:C007293), PVDF (MESH:C024865), Rhodamine-phalloidin (MESH:C504731), NAM (MESH:D009536)
- **Species:** Homo sapiens (human, species) [taxon 9606]
- **Mutations:** T10K, M10
- **Cell lines:** ARPE-19 — Homo sapiens (Human), Spontaneously immortalized cell line (CVCL_0145), hRPE — Homo sapiens (Human), Spontaneously immortalized cell line (CVCL_VC45)

## Full text

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## Figures

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## References

35 references — full list in the complete paper: https://tomesphere.com/paper/PMC12798965/full.md

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Source: https://tomesphere.com/paper/PMC12798965