Prostate Cancer Risk and DNA Methylation Signatures in Aging Rats following Developmental BPA Exposure: A Dose–Response Analysis

Prins, Gail S.; Ye, Shu Hua; Birch, Lynn; Zhang, Xiang; Cheong, Ana; Lin, Han; Calderon-Gierszal, Esther; Groen, Jacob; Hu, Wen‐Yang; Ho, Shuk Mei; Breemen, Richard B. van

doi:10.1289/ehp1050

Cited by 74 publications

(74 citation statements)

References 63 publications

(120 reference statements)

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“…Prostates were collected at one-year necropsy, coded and analysed for histopathology by Maarten Bosland, DVM, PhD who was blinded to treatments and controls. As previously reported by the Prins laboratory, 86,93 developmental or continuous exposure to BPA alone at any dose did not produce prostate pathology that differed from vehicle controls. However, in response to T+E, rats given developmental EE, 2.5, 250 or 25 000 μg BPA/kg BW/d showed significant increases in lateral prostate prostatic intraepithelial neoplasia (PIN) severity compared to vehicle controls at one year, shifting from low-grade PIN in controls to high-grade PIN in rats developmentally exposed to BPA with the highest PIN score observed at the 2.5 μg BPA/kg BW/d dose.…”

supporting

confidence: 83%

“…[83][84][85] In this context, previous work from the Prins, Ho and Walker laboratories determined that early-life, lowdose BPA exposure reprogrammed the rat prostate epigenome and increased its susceptibility to hormonal carcinogenesis with ageing, a finding that was subsequently confirmed in a humanized prostate model. [86][87][88][89][90][91][92][93] This is germane to human disease since elevated oestrogen levels rise in ageing men 94 and together with androgens, induce prostate cancer in the rat and human epithelium. 95,96 As part of the CLARITY-BPA consortium, the Prins laboratory had two main goals: (a) re-assess whether developmental BPA PRINS ET AL.…”

Section: Prostate End-pointsmentioning

confidence: 99%

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CLARITY‐BPA academic laboratory studies identify consistent low‐dose Bisphenol A effects on multiple organ systems

Prins

Patisaul

Belcher

et al. 2018

Basic Clin Pharma Tox

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Bisphenol A (BPA) is a high-production chemical used in a variety of applications worldwide. While BPA has been documented as an endocrine-disrupting chemical (EDC) having adverse health-related outcomes in multiple studies, risk assessment for BPA has lagged due to reliance on guideline toxicology studies over academic ones with end-points considered more sensitive and appropriate. To address current controversies on BPA safety, the United States National Institute of Environmental Health Sciences (NIEHS), the National Toxicology Program (NTP) and the Food and Drug Administration (FDA) established the Consortium Linking Academic and Regulatory Insights on BPA Toxicity (CLARITY-BPA) using the NCTR Sprague-Dawley rats. The goal of CLARITY-BPA is to perform a traditional regulatory toxicology study (Core study) in conjunction with multiple behavioural, molecular and cellular studies by academic laboratories focused on previously identified BPA-sensitive organ systems (Academic studies). Combined analysis of the data from both study types will be undertaken by the NTP with the aim of resolving uncertainties on BPA toxicity. To date, the Core study has been completed and a draft report released. Most of the academic studies have also been finalized and published in peer-reviewed journals. In light of this important milestone, the PPTOX-VI meeting held in the Faroe Islands, 27-30 May 2018 devoted a plenary session to CLARITY-BPA with presentations by multiple investigators with the purpose of highlighting key outcome. This MiniReview synthesizes the results of three academic studies presented at this plenary session, evaluates recently published findings by other CLARITY-BPA academic studies to provide an early combined overview of this emerging data and places this in the context of the Core study findings. This co-ordinated effort revealed a plethora of significant BPA effects across multiple organ systems and BPA doses with non-monotonic responses across the dose range utilized. Remarkably consistent across most studies, including the Core study, are low-dose effects (2.5, 25 and 250 μg BPA/kg body-weight). Collectively, the findings highlighted herein corroborate a significant body of evidence that documents adverse effects of BPA at doses relevant to human exposures and emphasizes the need for updated risk assessment analysis.

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supporting

confidence: 83%

Section: Prostate End-pointsmentioning

confidence: 99%

CLARITY‐BPA academic laboratory studies identify consistent low‐dose Bisphenol A effects on multiple organ systems

Prins

Patisaul

Belcher

et al. 2018

Basic Clin Pharma Tox

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“…Inappropriate hormone exposure can alter the gland's function, reprogram the gland, and may lead to prostate cancer. In the literature, there are many in vivo and in vitro studies about the effects of BPA on the prostate (Prins et al, ; Prins & Ho, ; Teng et al, ).…”

Section: Discussionmentioning

confidence: 99%

The effects of different bisphenol derivatives on oxidative stress, DNA damage and DNA repair in RWPE‐1 cells: A comparative study

Köse

Rachidi

Béal

et al. 2019

J of Applied Toxicology

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Bisphenol A (BPA) is a well-known endocrine disruptor and it is widely used mainly in the plastics industry. Due to recent reports on its possible impact on health (particularly on the male reproductive system), bisphenol F (BPF) and bisphenol S (BPS) are now being used as alternatives. In this study, RWPE-1 cells were used as a model to compare cytotoxicity, oxidative stress-causing potential and genotoxicity of these chemicals. In addition, the effects of the bisphenol derivatives were assessed on DNA repair proteins. RWPE-1 cells were incubated with BPA, BPF, and BPS at concentrations of 0-600 μM for 24 h. The inhibitory concentration 20 (IC 20 , concentration that causes 20% of cell viability loss) values for BPA, BPF, and BPS were 45, 65, and 108 μM, respectively. These results indicated that cytotoxicity potentials were ranked as BPA > BPF > BPS. We also found alterations in superoxide dismutase, glutathione peroxidase and glutathione reductase activities, and glutathione and total antioxidant capacity in all bisphenol-exposed groups. In the standard and modified Comet assay, BPS produced significantly higher levels of DNA damage vs the control. DNA repair proteins (OGG1, Ape-1, and MyH) involved in the base excision repair pathway, as well as p53 protein levels were down-regulated in all of the bisphenol-exposed groups. We found that the BPA alternatives were also cytotoxic and genotoxic, and changed the expressions of DNA repair enzymes. Therefore, further studies are needed to assess whether they can be used safely as alternatives to BPA or not.

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“…36 Bir diğer çalışmada, yenidoğan Sprague-Dawley erkek sıçanlar, doğum sonrası 1, 3 ve 5. günlerinde 0,1-5.000 μg/kg vücut ağırlığı BPA'ya kısa süre maruz bırakıldıktan sonra, en düşük BPA dozunun prostatın lateral bölgelerinde maksimal hormonal karsinogenezi başlattığı bulunmuştur. 37 Yapılan bir in vitro çalışmada, dört farklı prostat kanseri hücre hattında (LNCaP, C4-2, 22Rv1, PC-3) ve iki normal prostat epitel hücre hattında (NPrEC ve RWPE-1) düşük dozda (0,01-100 nM) BPA maruziyeti değerlendirilmiştir. Düşük dozlarda BPA, sentrozom amplifikasyonlu hücrelerin sayısını %2-8 oranında yükseltmiştir.…”

Section: Bisfenoller Ve Prostat Bezi üZerine Hücre Ve Hayvan çAlışmalarıunclassified

The Effects of Endocrine Disrupting Chemicals on Prostate Gland

Köse¹,

Erkekoğlu²,

Koçer-Gümüşel³

2020

J Lit Pharm Sci

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Prostate Cancer Risk and DNA Methylation Signatures in Aging Rats following Developmental BPA Exposure: A Dose–Response Analysis

Cited by 74 publications

References 63 publications

CLARITY‐BPA academic laboratory studies identify consistent low‐dose Bisphenol A effects on multiple organ systems

CLARITY‐BPA academic laboratory studies identify consistent low‐dose Bisphenol A effects on multiple organ systems

The effects of different bisphenol derivatives on oxidative stress, DNA damage and DNA repair in RWPE‐1 cells: A comparative study

The Effects of Endocrine Disrupting Chemicals on Prostate Gland

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