Epigenetic Control of Trefoil Factor Family (TFF) Peptide Expression in Human Retinoblastoma Cell Lines

Philippeit, Claudia; Busch, Maike; Dünker, Nicole

doi:10.1159/000366316

Cited by 20 publications

(14 citation statements)

References 58 publications

(78 reference statements)

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“…The loss of TFF1 in gastric cancer and its overexpression in ovarian cancer promote tumorigenesis involving the Wnt/ß‐catenin signaling pathway . Loss of TFF1 expression is epigenetically regulated by promotor methylation in gastric cancer and likewise in retinoblastoma cell lines as recently published by our group . The mechanisms by which TFF1 promotes apoptosis and changes proliferation behavior of tumor cells remain, however, largely unknown.…”

supporting

confidence: 51%

“…We performed TFF1 knockdown (KD) experiments in the RB cell line RBL30, exhibiting decently detectable endogenous TFF1 levels, to confirm TFF1 effects on growth and apoptosis. Testing different TFF1 ‐specific shRNA clones, we achieved a very efficient knockdown with an 80–95% reduction in TFF1 expression confirmed by quantitative Real‐time PCR (data not shown).…”

Section: Resultsmentioning

confidence: 99%

“…). Previous studies by our group revealed that only TFF3, but not TFF1 is expressed in the healthy human retina, whereby RB cell lines exhibit high levels of TFF1 …”

mentioning

confidence: 87%

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Reduction of the tumorigenic potential of human retinoblastoma cell lines byTFF1overexpression involves p53/caspase signaling and miR-18a regulation

et al. 2017

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Trefoil factor family (TFF) peptides have been shown to play a pivotal role in oncogenic transformation, tumorigenesis and metastasis by changing cell proliferation, apoptosis, migration and invasion behavior of various cancer cell lines. In the study presented, we investigated the effect of TFF1 overexpression on cell growth, viability, migration and tumorigenicity of different retinoblastoma (RB) cell lines. Transient TFF1 overexpression significantly increases RB cell apoptosis levels. Stable, lentiviral TFF1 overexpression likewise decreases RB cell viability, proliferation and growth and significantly increases apoptosis as revealed by WST-1 assays, BrdU and DAPI cell counts. TFF1-induced apoptosis is executed via cleaved caspase-3 activation as revealed by caspase blockage experiments and caspase-3 immunocytochemistry. Results from pG13-luciferase reporter assays and Western blot analyses indicate that TFF1-induced apoptosis is mediated through transcriptional activity of p53 with concurrently downregulated miR-18a expression. In ovo chicken chorioallantoic membrane (CAM) assays revealed that TFF1 overexpression significantly decreases the size of tumors forming from Y79 and RB355 cells and reduces the migration potential of RB355 cells. Differentially expressed genes and pathways involved in cancer progression were identified after TFF1 overexpression in Y79 cells by gene expression array analysis, underlining the effects on reduced tumorigenicity. TFF1 knockdown in RBL30 cells revealed caspase-3/7-independent apoptosis induction, but no changes on cell proliferation level. In summary, the in vitro and in vivo data demonstrate for the first time a tumor suppressor function of TFF1 in RB cells which is at least partly mediated by p53 activation and miR-18a downregulation.

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confidence: 51%

Section: Resultsmentioning

confidence: 99%

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Reduction of the tumorigenic potential of human retinoblastoma cell lines byTFF1overexpression involves p53/caspase signaling and miR-18a regulation

et al. 2017

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“…Our group was the first to investigate retinal expression of TFF peptides. Previous studies by our group revealed that only TFF3, but not TFF1 and TFF2 are expressed in the healthy human retina [ 11 ; 12 ], whereby retinoblastoma (RB) cell lines, established from malignant eye tumors of children, exhibit high levels of TFF1 [ 11 ; 12 ], but only trace amounts of TFF3 and no detectable TFF2 . Most recently, we demonstrated that the expression of TFF3 in retinoblastoma cell lines is regulated epigenetically [ 12 ].…”

Section: Introductionmentioning

confidence: 99%

Forced Trefoil Factor Family Peptide 3 (TFF3) Expression Reduces Growth, Viability, and Tumorigenicity of Human Retinoblastoma Cell Lines

et al. 2016

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Trefoil factor family (TFF) peptides have been shown to effect cell proliferation, apoptosis, migration and invasion of normal cells and various cancer cell lines. In the literature TFF peptides are controversially discussed as tumor suppressors and potential tumor progression factors. In the study presented, we investigated the effect of TFF3 overexpression on growth, viability, migration and tumorigenicity of the human retinoblastoma cell lines Y-79, WERI-Rb1, RBL-13 and RBL-15. As revealed by WST-1 and TUNEL assays as well as DAPI and BrdU cell counts, recombinant human TFF3 significantly lowers retinoblastoma cell viability and increases apoptosis levels. Transient TFF3 overexpression likewise significantly increases RB cell apoptosis. Stable, lentiviral TFF3 overexpression lowers retinoblastoma cell viability, proliferation and growth and significantly increases cell death in retinoblastoma cells. Blockage experiments using a broad-spectrum caspase inhibitor and capase-3 immunocytochemistry revealed the involvement of caspases in general and of caspase-3 in particular in TFF3 induced apoptosis in retinoblastoma cell lines. Soft agarose and in ovo chicken chorioallantoic membrane (CAM) assays revealed that TFF3 overexpression influences anchorage independent growth and significantly decreases the size of tumors forming from retinoblastoma cells. Our study demonstrates that forced TFF3 expression exerts a significant pro-apoptotic, anti-proliferative, and tumor suppressive effect in retinoblastoma cells, setting a starting point for new additive chemotherapeutic approaches in the treatment of retinoblastoma.

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“… 42 , 46 Interestingly, deletions of some of these tumor suppressor genes may drive RB. 46 Moreover, high-density methylation of numerous other genes, such as TFF3 , 47 the apoptotic effector CASP8, 48 , 49 the DNA repair gene MLH1 , 50 APC-2 , 31 and the RB2/p130 gene, is involved in RB 51 , 52 ( Table 1 ).…”

Section: Dna Methylation In Ocular Tumorsmentioning

confidence: 99%

Orchestrating epigenetic roles targeting ocular tumors

Wen¹,

Liu²,

Zhang³

et al. 2016

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Epigenetics is currently one of the most promising areas of study in the field of biomedical research. Scientists have dedicated their efforts to studying epigenetic mechanisms in cancer for centuries. Additionally, the field has expanded from simply studying DNA methylation to other areas, such as histone modification, non-coding RNA, histone variation, nucleosome location, and chromosome remodeling. In ocular tumors, a large amount of epigenetic exploration has expanded from single genes to the genome-wide level. Most importantly, because epigenetic changes are reversible, several epigenetic drugs have been developed for the treatment of cancer. Herein, we review the current understanding of epigenetic mechanisms in ocular tumors, including but not limited to retinoblastoma and uveal melanoma. Furthermore, the development of new pharmacological strategies is summarized.

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Epigenetic Control of Trefoil Factor Family (TFF) Peptide Expression in Human Retinoblastoma Cell Lines

Cited by 20 publications

References 58 publications

Reduction of the tumorigenic potential of human retinoblastoma cell lines byTFF1overexpression involves p53/caspase signaling and miR-18a regulation

Reduction of the tumorigenic potential of human retinoblastoma cell lines byTFF1overexpression involves p53/caspase signaling and miR-18a regulation

Forced Trefoil Factor Family Peptide 3 (TFF3) Expression Reduces Growth, Viability, and Tumorigenicity of Human Retinoblastoma Cell Lines

Orchestrating epigenetic roles targeting ocular tumors

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