EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines

Biomedical and Life Sciences

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https://doi.org/10.1080/17501911.2025.2453419
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EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines. / Latarani, Maryam; Pucci, Perla; Eccleston, Mark et al.
In: Epigenomics, Vol. 17, No. 3, 28.02.2025, p. 145-154.

Research output: Contribution to Journal/Magazine › Journal article › peer-review

Harvard

Latarani, M, Pucci, P, Eccleston, M, Manzo, M, Gangadharannambiar, P, Fischetti, I, Alborelli, I, Mongiardini, V, Mahmood, N, Colombo, MP, Grimaldi, B, Rigas, S, Akamatsu, S, Hawkes, C, Wang, Y, Jachetti, E & Crea, F 2025, 'EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines', Epigenomics, vol. 17, no. 3, pp. 145-154. https://doi.org/10.1080/17501911.2025.2453419

APA

Latarani, M., Pucci, P., Eccleston, M., Manzo, M., Gangadharannambiar, P., Fischetti, I., Alborelli, I., Mongiardini, V., Mahmood, N., Colombo, M. P., Grimaldi, B., Rigas, S., Akamatsu, S., Hawkes, C., Wang, Y., Jachetti, E., & Crea, F. (2025). EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines. Epigenomics, 17(3), 145-154. https://doi.org/10.1080/17501911.2025.2453419

Vancouver

Latarani M, Pucci P, Eccleston M, Manzo M, Gangadharannambiar P, Fischetti I et al. EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines. Epigenomics. 2025 Feb 28;17(3):145-154. Epub 2025 Jan 29. doi: 10.1080/17501911.2025.2453419

Author

Latarani, Maryam ; Pucci, Perla ; Eccleston, Mark et al. / EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines. In: Epigenomics. 2025 ; Vol. 17, No. 3. pp. 145-154.

Bibtex

@article{3c7b46cecc48437e8a0292eb612b07d2,

title = "EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines",

abstract = "BackgroundAggressive Variant Prostate Cancers (AVPCs) are incurable malignancies. Platinum-based chemotherapies are used for the palliative treatment of AVPC. The Polycomb Repressive Complex 2 (PRC2) promotes prostate cancer progression via histone H3 Lysine 27 tri-methylation (H3K27me3). EZH2 encodes the catalytic subunit of PRC2. A recently developed nucleosome capture technology (Nu.QⓇ).measures H3K27me3 levels in biological fluids. EZH2 inhibitors (EZH2i) are being tested in clinical trials. We hypothesize that epigenetic reprogramming via EZH2i improves the efficacy of Carboplatin in AVPC and that EZH2i activity can be measured via both cellular- and cell-free nucleosomal H3K27me3 (cf-H3K27me3) levels.MethodsWe studied the expression of PRC2 genes in clinical prostate cancer cohorts (bioinformatics). We determined the effect of EZH2i on cellular- and cf-H3K27me3 levels. We measured dose-dependent effects of Carboplatin with/without EZH2i on AVPC cell viability (IC50). We used RNA-Seq to study how EZH2i modulates gene expression in AVPC cells.ResultsPRC2 genes were significantly up-regulated in AVPC vs other prostate cancer types. EZH2i reduced both cellular and cf-H3K27me3 levels. EZH2i significantly reduced Carboplatin IC50. EZH2i reduced the expression of DNA repair genes and increased the expression of p53-dependent pro-apoptotic factors.ConclusionsEZH2i plus Carboplatin is a promising combination treatment for AVPC.",

author = "Maryam Latarani and Perla Pucci and Mark Eccleston and Massimiliano Manzo and Priyadarsini Gangadharannambiar and Irene Fischetti and Ilaria Alborelli and Vera Mongiardini and Namra Mahmood and Colombo, {Mario Paolo} and Benedetto Grimaldi and Sushila Rigas and Shusuke Akamatsu and Cheryl Hawkes and Yuzhuo Wang and Elena Jachetti and Francesco Crea",

year = "2025",

month = feb,

day = "28",

doi = "10.1080/17501911.2025.2453419",

language = "English",

volume = "17",

pages = "145--154",

journal = "Epigenomics",

issn = "1750-1911",

publisher = "Future Medicine Ltd.",

number = "3",

}

RIS

TY - JOUR

T1 - EZH2 inhibition enhances the activity of Carboplatin in aggressive-variant prostate cancer cell lines

AU - Latarani, Maryam

AU - Pucci, Perla

AU - Eccleston, Mark

AU - Manzo, Massimiliano

AU - Gangadharannambiar, Priyadarsini

AU - Fischetti, Irene

AU - Alborelli, Ilaria

AU - Mongiardini, Vera

AU - Mahmood, Namra

AU - Colombo, Mario Paolo

AU - Grimaldi, Benedetto

AU - Rigas, Sushila

AU - Akamatsu, Shusuke

AU - Hawkes, Cheryl

AU - Wang, Yuzhuo

AU - Jachetti, Elena

AU - Crea, Francesco

PY - 2025/2/28

Y1 - 2025/2/28

N2 - BackgroundAggressive Variant Prostate Cancers (AVPCs) are incurable malignancies. Platinum-based chemotherapies are used for the palliative treatment of AVPC. The Polycomb Repressive Complex 2 (PRC2) promotes prostate cancer progression via histone H3 Lysine 27 tri-methylation (H3K27me3). EZH2 encodes the catalytic subunit of PRC2. A recently developed nucleosome capture technology (Nu.QⓇ).measures H3K27me3 levels in biological fluids. EZH2 inhibitors (EZH2i) are being tested in clinical trials. We hypothesize that epigenetic reprogramming via EZH2i improves the efficacy of Carboplatin in AVPC and that EZH2i activity can be measured via both cellular- and cell-free nucleosomal H3K27me3 (cf-H3K27me3) levels.MethodsWe studied the expression of PRC2 genes in clinical prostate cancer cohorts (bioinformatics). We determined the effect of EZH2i on cellular- and cf-H3K27me3 levels. We measured dose-dependent effects of Carboplatin with/without EZH2i on AVPC cell viability (IC50). We used RNA-Seq to study how EZH2i modulates gene expression in AVPC cells.ResultsPRC2 genes were significantly up-regulated in AVPC vs other prostate cancer types. EZH2i reduced both cellular and cf-H3K27me3 levels. EZH2i significantly reduced Carboplatin IC50. EZH2i reduced the expression of DNA repair genes and increased the expression of p53-dependent pro-apoptotic factors.ConclusionsEZH2i plus Carboplatin is a promising combination treatment for AVPC.

AB - BackgroundAggressive Variant Prostate Cancers (AVPCs) are incurable malignancies. Platinum-based chemotherapies are used for the palliative treatment of AVPC. The Polycomb Repressive Complex 2 (PRC2) promotes prostate cancer progression via histone H3 Lysine 27 tri-methylation (H3K27me3). EZH2 encodes the catalytic subunit of PRC2. A recently developed nucleosome capture technology (Nu.QⓇ).measures H3K27me3 levels in biological fluids. EZH2 inhibitors (EZH2i) are being tested in clinical trials. We hypothesize that epigenetic reprogramming via EZH2i improves the efficacy of Carboplatin in AVPC and that EZH2i activity can be measured via both cellular- and cell-free nucleosomal H3K27me3 (cf-H3K27me3) levels.MethodsWe studied the expression of PRC2 genes in clinical prostate cancer cohorts (bioinformatics). We determined the effect of EZH2i on cellular- and cf-H3K27me3 levels. We measured dose-dependent effects of Carboplatin with/without EZH2i on AVPC cell viability (IC50). We used RNA-Seq to study how EZH2i modulates gene expression in AVPC cells.ResultsPRC2 genes were significantly up-regulated in AVPC vs other prostate cancer types. EZH2i reduced both cellular and cf-H3K27me3 levels. EZH2i significantly reduced Carboplatin IC50. EZH2i reduced the expression of DNA repair genes and increased the expression of p53-dependent pro-apoptotic factors.ConclusionsEZH2i plus Carboplatin is a promising combination treatment for AVPC.

U2 - 10.1080/17501911.2025.2453419

DO - 10.1080/17501911.2025.2453419

M3 - Journal article

C2 - 39878501

VL - 17

SP - 145

EP - 154

JO - Epigenomics

JF - Epigenomics

SN - 1750-1911

IS - 3

ER -

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