Abstract

Simple SummaryEstrogens regulate key physiological functions in the human body, including the development of female reproductive organs. However, dysregulated estrogen signaling—mainly mediated by estrogen receptors (ER)—is associated with many developmental, mental, and other diseases, including cancer. An increasing number of studies have demonstrated that estrogen modulates inflammatory processes within many tissues. In addition to estrogens made within the body, humans are also constantly exposed to many outside estrogens, naturally occurring in plants and those artificially synthesized in industries. Here, we will also discuss the link between chronic exposure to environmental estrogens with tissue inflammation and breast cancer development.The oncogenic role of estrogen receptor (ER) signaling in breast cancer has long been established. Interaction of estrogen with estrogen receptor (ER) in the nucleus activates genomic pathways of estrogen signaling. In contrast, estrogen interaction with the cell membrane-bound G-protein-coupled estrogen receptor (GPER) activates the rapid receptor-mediated signaling transduction cascades. Aberrant estrogen signaling enhances mammary epithelial cell proliferation, survival, and angiogenesis, hence is an important step towards breast cancer initiation and progression. Meanwhile, a growing number of studies also provide evidence for estrogen’s pro- or anti-inflammatory roles. As other articles in this issue cover classic ER and GPER signaling mediated by estrogen, this review will discuss the crucial mechanisms by which estrogen signaling influences chronic inflammation and how that is involved in breast cancer. Xenoestrogens acquired from plant diet or exposure to industrial products constantly interact with and alter innate estrogen signaling at various levels. As such, they can modulate chronic inflammation and breast cancer development. Natural xenoestrogens generally have anti-inflammatory properties, which is consistent with their chemoprotective role in breast cancer. In contrast, synthetic xenoestrogens are proinflammatory and carcinogenic compounds that can increase the risk of breast cancer. This article also highlights important xenoestrogens with a particular focus on their role in inflammation and breast cancer. Improved understanding of the complex relationship between estrogens, inflammation, and breast cancer will guide clinical research on agents that could advance breast cancer prevention and therapy.

Highlights

  • Estrogen sex steroid hormones orchestrate a multitude of physiological functions ranging from development and regulation of the human reproductive system to modulation of neuroendocrine, skeletal, adipose, and cardiovascular systems [1,2]

  • While the expression and secretion of adiponectin are inhibited by TNFα and interleukin 6 (IL-6) as a counteraction from proinflammatory components [98], it is interesting to find that estradiol suppresses adiponectin but not leptin expression in 3T3-L1 adipocyte cell line [99] and that serum adiponectin level is negatively correlated with estradiol level in postmenopausal women, bringing up the hypothesis that estrogen may antagonize the anti-inflammatory effect of adiponectin [100]

  • The research articles reviewed here have delineated how natural and environmental estrogens participate in physiological processes as well as carcinogenesis

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Summary

Introduction

Estrogen sex steroid hormones orchestrate a multitude of physiological functions ranging from development and regulation of the human reproductive system to modulation of neuroendocrine, skeletal, adipose, and cardiovascular systems [1,2]. The anti-inflammatory roles of estrogen have been demonstrated in other models and human diseases [9]. It is well-appreciated that chronic tissue inflammation is an established risk factor for various events of cancer initiation and progression, including cellular transformation, survival, proliferation, invasion, angiogenesis, and metastasis [11,12,13]. In this current article, we review the implications of natural and synthetic estrogens in chronic inflammation and ensuing carcinogenesis

Estrogen Signaling
Canonical Estrogen Signaling within the Nucleus
Noncanonical Estrogen Signaling on the Surface
Mitochondrial ER Signaling
Differential ERα and ERβ Signaling
Estrogen Signaling in Breast Cancer
Estrogen and Inflammation—The Positive Feedback
IL-6 and Estrogen
PGE2 and Estrogen
Adipokines and Estrogen
Estrogen in Breast Cancer and the Involvement of Inflammation
Anti-Inflammatory Role of Estrogens
Endocrine Therapy for Breast Cancer and Inflammation
Xenoestrogens in Inflammation and Breast Cancer
Phytoestrogens and Cancer
Reduced Expression and Activity of NF-κB and AP-1 Signaling
Antioxidative Activity
Key Findings
Suppressed Proinflammatory Cytokines and Chemokine Production
Reduced Cyclooxygenase-2 Activity
Synthetic Xenoestrogens and Cancer
Specific Synthetic Xenoestrogens in Inflammation and Breast Cancer
Findings
Concluding Thoughts and Perspectives
Full Text
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