Abstract
It is well established that the development and homeostasis of the mammary gland are highly dependent upon the actions of ovarian hormones progesterone and estrogen, as well as the availability of prolactin for the pregnant and lactating gland. More recently it has become apparent that immune system cells and cytokines play essential roles in both mammary gland development as well as breast cancer. Here, we review hormonal effects on mammary gland biology during puberty, menstrual cycling, pregnancy, lactation and involution, and dissect how hormonal control of the immune system may contribute to mammary development at each stage via cytokine secretion and recruitment of macrophages, eosinophils, mast cells and lymphocytes. Collectively, these alterations may create an immunotolerant or inflammatory immune environment at specific developmental stages or phases of the menstrual cycle. Of particular interest for further research is investigation of the combinatorial actions of progesterone and estrogen during the luteal phase of the menstrual cycle and key developmental points where the immune system may play an active role both in mammary development as well as in the creation of an immunotolerant environment, thereby affecting breast cancer risk.
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Introduction
It is increasingly recognized that the actions of hormones on mammary gland development and breast cancer are mediated by a number of paracrine interactions locally within the breast. Significantly, immune system cells are abundant in the stroma surrounding the mammary gland epithelium and provide essential support for hormone-driven mammary gland morphogenesis [1]. Estrogen, progesterone and prolactin each direct immune cell functions both alone and in combination, and the actions of these immune cells drive pubertal and adult mammary gland development [2, 3]. However, the specific functions of immune cells necessary for normal development may also be important in contributing to hormone-mediated increased breast cancer risk.
The immune system is a complex network of immune organs, cells, and soluble factors such as cytokines that act locally or systemically through a variety of mechanisms, such as an immediate inflammatory response through cytokines and phagocytes, a specific tailored immune response through adaptive immune cells, or a regulated immunotolerant response. The differing, and sometimes opposing, roles of the immune system are mediated by a complex interplay of intracellular and extracellular signaling pathways. Cells of the immune system participate in a diverse number of processes in the body which can be categorized into (1) protection of the host from invading pathogens, foreign antigens and incipient tumor cells, and (2) participation in development, maintenance of homeostasis, tissue repair and regeneration for processes such as wound healing.
In the highly cited review on the hallmarks of cancer by Hanahan et al. [4], ten key biological processes are identified as being required for cancer to establish itself and metastasize in the host. Two of these hallmarks involve the immune system with (1) the tumor avoiding immune detection and destruction, and (2) inflammation promoting tumor growth. Of particular interest is how incipient tumors avoid immune detection and destruction, where evidence suggests that the ovarian hormones estrogen and progesterone can promote immune suppression [5, 6]. In addition, estrogen, progesterone and prolactin can modulate inflammation both systemically and locally within the mammary gland. In the mammary gland the effects of estrogen, progesterone and prolactin on immune cells can be either direct, or indirect through hormonally-regulated mammary gland components of mammary epithelial cells and stroma. The direct effects of the hormones on immune cells are mediated when the immune cells express receptors for estrogen, progesterone and prolactin, which are engaged by their respective ligands. The indirect effects of estrogen, progesterone and prolactin on immune cells are mediated by paracrine signals from mammary epithelial cells and stroma. How estrogen and progesterone regulate the immune microenvironment in the mammary gland is less well studied than their roles in mammary epithelia (discussed below), but there is a growing body of evidence that demonstrates that the hormonally-regulated immune environment plays an essential role in mammary gland development.
The actions of estrogen and progesterone are inextricably involved in the development and homeostasis of the normal breast and in most breast cancers [reviewed in 1, 7]. Epidemiological evidence points to a number of breast cancer risk factors associated with menstrual cycling and hormone exposure. For every year earlier of menarche there is a 5 % increased lifetime risk of breast cancer, and a 3.5 % increased lifetime risk for every year later of menopause [8]. In addition to these reproductive factors, in one large scale trial including several periods of clinical follow up, an increased risk of developing and dying from breast cancer was found in individuals who have previously taken combined hormone replacement therapy, which consists of combined exogenous estrogen and the synthetic progestin medroxyprogesterone acetate when compared to patients who were administered placebo [9, 10]. In this same trial of 16,608 women, those women who had undergone hysterectomy were administered estrogen alone, and exhibited decreased breast cancer risk in comparison to those taking placebo [11]. Extrapolation of all of these risks to biological function infers that increased risk of breast cancer is related to the timing of puberty and the increased number of menstrual cycles, and thus exposure to repeated fluctuations in ovarian hormones. This risk was acknowledged by Pike et al. in 1993, who coined “the estrogen augmented by progestogen hypothesis”, which asserts that this increased breast cancer risk may be attributed to repeated cycles of progesterone-induced activity in combination with estrogen-induced activity [12].
However, although hormones act directly on the mammary gland epithelium to promote development, paracrine signals from the local immune population are essential in facilitating epithelial cell proliferation, differentiation and tissue remodeling [2, 3, 13, 14]. Together, the role of hormones in modulating breast cancer risk, combined with the role of the immune environment during dynamic structural remodeling and altered tissue composition of the normal breast may provide key mechanistic insights into factors that cause breast cancer. Hence, we outline here how estrogen, progesterone and prolactin impact on the immune microenvironment during different developmental stages of the mammary gland, and provide a summative model of how hormonally-regulated immune cells in the mammary gland impact on mammary gland development and the risk of breast cancer.
Immune System Cells and Cytokines in the Mammary Gland
Macrophages
Macrophages are derived from circulating blood monocytes that migrate into tissue and differentiate into tissue specific resident macrophages. They are highly plastic cells exquisitely sensitive to cytokine signals in the surrounding microenvironment and tailor their function accordingly [15]. Their functions are considerably varied compared to other immune cells and range from classically-activated cells that express MHC class II and participate in infection control, alternatively-activated cells for tissue remodeling that express mannose receptor, or cells involved in immune modulation. However, this historical categorization of macrophage phenotypes has long been recognized as being inadequate to convey the complexity of macrophage functional plasticity. A recent study using transcriptome analysis revealed that macrophages can be activated via numerous signals resulting in nine clusters of macrophage activation and function [16]. Such a broad scope of macrophage phenotype is yet to be determined in the macrophages resident in the mammary gland. Therefore, in this review mammary gland macrophages will be discussed from the broader categories of immunity and tissue development, while being mindful of the complexity of macrophage plasticity. The functions of macrophages, like other cells, are implemented by expression of receptors and secretion of specific molecules to direct cell response and tailor functions of adjacent cells. Macrophages are critically important immune cells in pubertal and adult mammary gland development and the function of macrophages at specific stages of development will be discussed in Hormones and the Immune Environment during Mammary Gland Development section.
T lymphocytes
T lymphocytes are immune cells that mediate the cellular, humoral and immunoregulatory branches of the immune system principally through local cytokine signals and specific cell-to-cell interactions through the T cell receptor that governs antigen-mediated immunity. A major class of T lymphocytes is the helper T cells (Th), which are categorized further into several subsets on the basis of cell surface markers and functional attributes. Th cells can be polarized to either Th1 or Th2 subsets that secrete different patterns of cytokines; Th1 cells secrete mostly pro-inflammatory cytokines such as interferon-gamma (IFNG) and tumor necrosis factor (TNF)-alpha (TNFA), and Th2 cells induce immunomodulating cytokines such as interleukin (IL)4 and IL10, which also are involved in tissue remodeling [17]. Regulatory T cells (Treg) regulate the balance between immunity and tolerance, to avoid excessive or insufficient immune function [18]. A population of intra-epithelial T cells has been identified in the normal human breast [19, 20], however studies into their function are limited. There is an absence of literature available regarding the influence of estrogen and progesterone on T lymphocytes in the mammary gland, therefore discussed below is the response of peripheral blood T lymphocytes to ovarian hormones.
Eosinophils and Mast Cells
Hormone-regulated immune cells that are necessary for mammary gland development and homeostasis also include eosinophils and mast cells. Eosinophils are large, phagocytic immune cells, which target helminthes and participate in allergic reactions [21]. Mast cells are tissue resident cells that participate in early inflammatory responses and in allergies [22].
Cytokines
In the mammary gland, cytokines are secreted by mammary epithelial cells, fibroblasts, adipocytes or immune cells. The profile of cytokines can be pro-inflammatory, anti-inflammatory, immunoregulatory or tissue growth promoting depending upon the predominant secretory profile. This cytokine microenvironment can directly affect the development and function of the mammary gland by ensuring the appropriate recruitment of immune cells such as macrophages and eosinophils at appropriate developmental phases through the secretion of factors such as colony-stimulating factor 1 (CSF1), interleukins (IL) 4 and10, and tumor necrosis factor alpha (TNFA) [2, 3, 14].
Hormones and the Immune Environment during Mammary Gland Development
Mammary Gland Development during Puberty
In mice immediately preceding puberty, the terminal end buds (TEB) form, which are the distal ends of the mammary ducts that swell as the cuboidal epithelial cells within the bud proliferate in response to rising pre-pubertal estrogen concentrations [23]. In comparison, in the human pre-pubertal mammary gland; the distal ends of the ductal structures lack these distinct spherical structures and instead form into clusters that are collectively called terminal duct lobular units (TDLU) [24]. However, both TEBs and TLDUs undergo estrogen driven bifurcation, ductal elongation and lateral ductal branching to produce the network of epithelial ducts observed in the adult mammary gland in mice, rats and humans. This process is dependent upon the presence of the transcriptional regulator of estrogen action, estrogen receptor alpha (ERα) [25]. Likewise, key ERα coregulators are also essential for the development of the mammary gland, such as SRC-3 and RIP140 [26, 27]. While activation of ERβ or androgen receptor (AR) is not essential at any stage of mammary development, these receptors have been described to contribute to mammary development by inhibition or enhancement of ductal growth during the pubertal stage [28–30].
The effects of ERα in the developing mammary gland are largely paracrine; only a subset of the mammary epithelium is required to express ERα for normal mammary gland development [25]. One of these ERα-regulated developmental paracrine signals is amphiregulin, which activates the epidermal growth receptor (ERBB1/EGFR) in the mammary stroma [31]. Indeed, mice with deficient ERBB1 stromal signaling have impaired alveolar development similar to that observed in ERα null mice, and amphiregulin-null mice fail to develop mature ductal trees due to defects in ductal outgrowth, which may in part be due to inhibited recruitment of macrophages and eosinophils to sites of tissue remodeling [2, 3, 25, 31–33].
Estrogen-regulated production of CSF1 in the murine mammary gland is essential for pubertal development, as CSF1-regulated macrophages associate with the expanding mammary epithelial ducts and buds [34, 35], and alter the structural alignment of collagen fibers around the expanding terminal end buds [36]. In a humanized mouse model, macrophages exposed to estrogen promote the growth of the pubertal mammary stroma through paracrine effects on mammary fibroblasts [37]. Macrophages are critical at the pubertal stage as their absence, in line with the effects of the absence of ERα as discussed above, delays mammary gland development in mice [35].
In the mammary gland of pubertal female mice, the rising estrogen concentration increases EGFR signaling via upregulation of amphiregulin, thus leading to increased recruitment of eosinophils, with modulation of eotaxin concentration identified as the primary paracrine mediator of eosinophil recruitment [3]. The association of eosinophils with mammary epithelia increases ductal branching and formation of TEBs in mice [35]. Interestingly, overabundance of eosinophils in the pubertal gland in mice actually retards mammary epithelial morphogenesis, implying that their optimal abundance controls the overall number of ductal structures in mammary gland development [38]. Mast cells are also necessary for development of the mammary gland during puberty. As with eosinophils, mast cells are important for mammary epithelial cell proliferation in mice, as their absence retards growth [39]. Thus, macrophages, eosinophils and mast cells are required for expansion of the mammary gland during puberty.
Menstrual Cycling Impact on the Mammary Gland Immune Environment
Steroid Receptors and Hormones
The menstrual cycle involves the cyclical production of estrogen and progesterone, governed by endocrine signals from the hypothalamus, pituitary, ovaries and adrenal glands. During the follicular phase, maturing ovarian follicles secrete increasing amounts of estrogen until a peak is reached which leads to ovulation. In contrast, the luteal phase is characterized by rising levels of progesterone produced by the remnant of the follicle, the corpus luteum. Importantly, this increase in progesterone concentration is accompanied by a concomitant second smaller peak of estrogen during the luteal phase (Fig. 1a). The follicular phase in humans and estrus phase in mice reflect similar profiles of circulating estrogen concentration, while in the metestrus and diestrus phases, circulating progesterone concentration increases and estrogen concentration is lower. It has been appreciated for four decades that the mammary gland undergoes dynamic morphological changes during the menstrual cycle in both humans and mice, and that these stages can be categorized histologically by examining the morphological structures within the gland [40, 41] (Fig. 1b). Detailed analyses of the changes in mammary epithelial cell proliferation and apoptosis over the human menstrual cycle have revealed that proliferation of the epithelial cells is highest during the luteal phase, and is positively associated with serum progesterone concentration, while apoptosis was relatively consistent between the follicular and luteal phases in some but not all studies [42–45]. However, from a human whole mammary gland perspective, the mammary epithelial ductal structures proliferate and undergo increased branching during the luteal phase and then regress during the follicular phase [46]. Thus, declining circulating progesterone towards the end of the luteal phase does not appear to be linked with apoptosis of human mammary epithelia [43, 45], unlike the observed positive correlation of progesterone withdrawal with mammary epithelial cell apoptosis in mice [47]. This conflict may be due to sampling difficulties and the histological techniques employed in human specimens. TUNEL staining and histological measures of apoptosis used in human studies detect late stage apoptosis, and these dying cells may be rapidly phagocytosed by adjacent macrophages before exhibiting these apoptotic markers [48].
Macrophages
Murine studies show macrophage abundance in the mammary gland fluctuates over the estrous cycle, peaking at metestrus and diestrus phases, when progesterone concentration is highest, and is lowest at proestrus and estrus, when progesterone concentration is reduced [2]. Macrophages have dual roles that are critical for progesterone-mediated epithelial cell growth and regression in the mammary gland; an absence of macrophages results in both reduced epithelial cell proliferation and impaired regression during estrogen and progesterone-mediated cyclical morphogenesis [2].
Progesterone alters the abundance of macrophages in the mammary gland expressing MHC class II, the scavenger receptor CD204 and DNA damage recognition receptor NKG2D during the estrous cycle, and in ovariectomised mice administered exogenous estrogen and progesterone [14]. The percentage of MHC class II-expressing macrophages is reduced by estrogen and progesterone administration, and elevated following administration of the progesterone receptor antagonist RU486. MHC class II is critical for macrophages to present antigens to T lymphocytes and activate them to elicit an immune response. Therefore, the progesterone-mediated reduction of MHC class II expression by macrophages is likely to limit their ability to initiate adaptive immune responses against pathogens. On the other hand, the percentage of NKG2D-expressing macrophages is elevated in response to estrogen and progesterone and declines upon administration of RU486 [14]. Surface expression of NKG2D on macrophages enables detection of DNA damaged cells, and stimulates secretion of inflammatory mediators to recruit other immune cells to the site [49].
Human macrophages are also stimulated by estrogen via ERα resulting in suppression of the nuclear factor-kappa B (NF-κB) signaling pathway [50], which is critical for phagocytosis and drives IL4-mediated alternative activation of murine macrophages, thus dampening the inflammatory response [51]. Indeed, rapid phagocytosis of apoptotic cells dampens inflammation through inhibition of the production of inflammatory cytokines IL1B, IL8, TNFA and CSF2 [52, 53], and increasing production of IL10 [52]. IL10, an anti-inflammatory cytokine, is necessary for mammary ductal branching, as observed in Il10 null mutant mice, suggesting that IL10 may skew macrophages towards a tissue remodeling role [54]. Thus, anti-inflammatory conditions via IL10 modulation and phagocytosis of apoptotic mammary epithelial cells during the regression of mammary epithelial cells in response to progesterone withdrawal in the context of rising estrogen may create an immunotolerant mammary environment for tumor initiation. This is supported by studies demonstrating increased murine mammary gland susceptibility to I-nitroso-I-methylurea(NMU)-induced carcinogenesis during the proestrus and estrus phases of the cycle, which exhibit declining serum progesterone concentrations and elevated estrogen, in comparison to the diestrus phase where the rat exhibits elevated serum progesterone and low estrogen [55, 56].
T lymphocytes
The immune environment of the mammary gland is dampened during different phases of the menstrual cycle in response to hormonal stimuli. During the luteal phase of the menstrual cycle, Th cells in the blood are biased towards the Th2 type, which secrete cytokines such as IL4 and IL10 [57]. Estrogen directly increases the abundance of Treg cells in blood and enhances their immunosuppressive functions [5, 58]. In the follicular phase the numbers of Treg cells increase and correlate positively with serum concentration of estrogen [59]. Progesterone, in combination with TGFB1, a growth factor that inhibits mammary epithelial cell proliferation, also induces high numbers of Treg cells in the blood, which are highly stable and more effective in their immunosuppressive function [6]. While further investigations into T cell function and abundance in the cycling mammary gland are required, the regulation of immunosuppressive Treg cells in the blood by estrogen and progesterone suggest that the abundance of Treg cells in the mammary gland may fluctuate over the menstrual cycle.
Cytokine Microenvironment
Estrogen and progesterone can have differing effects on the cytokine profile in mammary glands at the pubertal stage versus the adult stage. Mammary glands in pubertal female mice treated with only estrogen or progesterone induce expression of several pro-inflammatory genes for chemokines and cytokines including genes encoding IL17B and TNFA [3]. In contrast, in adult mice, recent findings demonstrate that the cytokine microenvironment of the murine mammary gland fluctuates over the estrous cycle, with the estrus phase skewed to a pro-inflammatory environment through increased protein secretion of CSF1, IFNG and TNFA [60]. However, the pro-inflammatory environment is dampened by the presence of progesterone, and the abundance of TNFA and IL6 in the mammary gland declines during the luteal phase [61, 62]. These results in dual hormone treated mammary glands of female mice contrast with the findings of Aupperlee et al., who report that steroid hormones invoke a response in inflammatory chemokines in the mammary gland upon sole estrogen or progesterone treatment [3].
Mammary Gland Development during Pregnancy and Lactation
During pregnancy, epithelial cells undergo dramatic proliferation followed by differentiation and enhanced survival. This dynamic remodeling is accompanied by stromal remodeling that encompasses enhanced angiogenesis, infiltration of macrophages and granulocytes, fibroblast reorganization and loss of adipocyte lipid droplets. The role of progesterone signaling in the non-neoplastic breast is most evident during pregnancy, where the PR-B isoform is required, but only in a subset of the lobuloalveolar epithelia, for the extensive proliferation of epithelial cells within the lobuloalveolar structures, thus supporting a paracrine role for PR-B in this process [63]. Another key hormone that is required for pregnancy-induced mammary development is prolactin, a peptide hormone produced by the pituitary in response to neuroendocrine signals from the hypothalamus [64]. At parturition, the fall in circulating progesterone, in the context of elevated prolactin, triggers the switch to secretory lactation, where tight junctions between epithelia close, and colostrum accumulate in the alveolar lumens for ejection from the breast.
Interestingly, the NF-κB signaling pathway, commonly known to mediate detection of invading pathogens, inflammation and cellular apoptosis, is identified as a critical mediator of lobuloalveolar development during pregnancy. Receptor activator of NF-κB ligand (RANKL), a member of the TNF cytokine family is a candidate paracrine signaling molecule in pregnancy-induced mammary gland morphogenesis. Signals from prolactin and progesterone both converge to activate the RANKL signaling and NF-κB pathways [65]. Mice with RANKL or RANK deficient lobuloalveolar buds fail to produce differentiated, milk producing alveoli but still form alveolar buds upon pregnancy, indicating that the preliminary progesterone-mediated proliferative effects in the lobuloalveolar epithelia upon pregnancy may be independent of RANK signaling, while the differentiation of the alveolar epithelial cells into mature milk secreting cells is RANK signaling dependent [66, 67]. The differentiation of alveolar epithelial cells is dependent upon NF-κB activation, as demonstrated by IKKα null mice, which is required for NK- κB activity. These IKKα null mice display mammary gland defects similar to RANKL deficient mice and do not express Cyclin D1, which has also been shown to be essential for lobuloalveolar differentiation during pregnancy, and is regulated by both progesterone and STAT5 [68, 69]. Thus, the network of PR, prolactin, NF-kB and STAT5 signaling are interlinked by mutual regulation of RANKL and its downstream effectors, resulting in differentiation or maturation of the lobuloalveolar epithelia into mature milk secreting glands.
While a role in pregnancy-induced mammary remodeling is yet to be described, cyclooxygenase 2 (COX2), an enzyme involved in the synthesis of pro-inflammatory prostanoids, has been shown to be hormonally regulated in murine mammary tissues in response to estrogen and progesterone, and is increased in expression in normal human mammary tissue during pregnancy [70]. However, there is also evidence progesterone suppresses systemic inflammatory responses; mononuclear immune cells from progesterone-treated blood, which is dominated by precursor macrophages, have decreased concentrations of NF-κB, TNFA and IL6 [71].
Macrophages
The epithelium within the ducts and alveoli of the lactating mammary gland express high concentrations of CSF1 receptor and CSF1 compared to non-pregnant, non-lactating mammary epithelium in mice [72]. During pregnancy, in the mammary gland macrophages regulate epithelial cell development, as absence of CSF1 leads to reduced ductal branching, excessive lobuloalveologenesis and precocious differentiation and milk production in mice [13]. Macrophages also play an essential role in mediating the switch from pregnancy to lactation, and mice deficient in these cells do not secrete milk. Although it is unknown how macrophages promote the switch to lactation, macrophages may regulate tight junction permeability. NF-κB activation is a key event in increasing membrane permeability during periods of inflammation in a number of tissues [73], and activation of NF-κB by the toll-like receptor 4 signaling pathway in a mouse model increases permeability of the milk-blood barrier [74]. Importantly, macrophage-mediated TLR4 activation regulates inflammation in the mammary gland [75] [76], and the decline in progesterone at parturition may affect the function of resident macrophages to promote tight junction closure.
T lymphocytes
Pregnancy places the mother in an immunotolerant, anti-inflammatory state for the survival of the allogeneic fetus [77]. Estrogen, at concentrations comparable to pregnancy, increases the proliferation and immunosuppressive ability of Treg cells in the blood [5] and also inhibits the inflammatory reaction via NF-κB in rat muscle cells [78]. As discussed above, NF-κB is upregulated during pregnancy by progesterone-driven upregulation of RANK, which also regulates Treg cells [79]. As in menstrual cycling, elevated progesterone in the mammary gland during pregnancy may increase immune tolerance while upregulating the factors which drive Treg cell function.
Limited evidence suggests a role for prolactin governing immune cell profiles during lactation in the mammary gland. A lactation deficient rat model with decreased serum prolactin does not have a skewed profile of B or T cell phenotypes, however they did observe reduced migration of T lymphocytes from the blood to the mammary gland, with reduced expression of chemokine receptors by those T lymphocytes [80]. Prolactin-induced differentiated luminal epithelial cells in mice upregulate expression of IL4 receptor and alter the immune microenvironment by altering their cytokine profile towards a Th2 bias [81]. Additionally, progesterone skews murine T lymphocytes towards the Th2 profile and inhibits the Th1 subtype while elevating secretion of IL10 by T lymphocytes [82]. Thus, both progesterone and prolactin in the pregnant/lactating mammary gland directly influence T lymphocytes through the mammary epithelial cells producing Th2-like cytokines such as IL4, IL5 and IL13.
The Involution Immune Environment
As involution commences, the extensive alveolar sacs and ductal branches undergo the dramatic process of remodeling that returns the mammary epithelia to the pre-pregnancy, basic ductal network. Initial changes can be observed within hours of the cessation of suckling, and involve a decline in the production and secretion of prolactin and oxytocin. Early cellular events within the epithelial cells in response to weaning in mice include activation of NF-κB, increased expression of proapoptotic proteins Bax and Bcl-x, a decrease in phosphorylated and cellular STAT5 and increases in STAT3 phosphorylation [83–85]. These changes are accompanied by an eight fold increase in recruitment of developmental, tissue remodeling phenotype macrophages to the mammary gland that allows remodeling of the mammary epithelial network to the earlier nulliparous state [86–88]. The immune microenvironment during the involution phase and the impact of this on breast cancer risk is reviewed elsewhere in this issue.
Estrogen-Mediated, Progesterone Fuelled Signaling and the Immune Environment in Breast Cancer Risk
Increasing evidence highlights progesterone-regulated immune system factors in breast cancer risk, with RANKL and NF-κB as key signaling mediators. Progestin increases RANKL expression in the murine mammary gland, which is required for DMBA-induced carcinogenesis [89, 90]. Progesterone also induces RANKL expression in human mammary glands [91]. Combination hormone replacement therapy (estrogen plus medroxyprogesterone acetate) in ovariectomised cynomolgus macaques induces a gene expression profile remarkably similar to that exhibited during the differentiation of the TDLU in late pregnancy or during the luteal phase of the menstrual cycle, where estrogen plus medroxyprogesterone acetate caused upregulation of PRL/STAT5, ERBB1 and RANKL pathways in conjunction with increased proliferation within the glands, an effect not observed in macaques treated with estrogen alone [92]. Likewise, an analysis of gene expression in cynomolgus macaques over several life stages revealed remarkable transcriptional similarities between the mammary glands of luteal phase and pregnant or lactating monkeys, including elevated expression of the RANKL-associated differentiation factor ELF5 [93]. Together, these results suggest that the actions of progestogens (synthetic progestins or naturally occurring progesterone) in the presence of estrogen activate NF-κB-mediated differentiation in estrogen-primed, progestogen-fuelled paracrine proliferation of mammary epithelial cells (Fig. 2).
RANKL signaling and NF-κB activation have profound effects on directing immune system responses that can promote carcinogenesis by subverting tumor immunity and driving persistent inflammation [94]. RANKL is expressed by Treg cells [95] and increases their local abundance [96]. Expression of RANKL by Treg cells is critical for Erbb2+ tumors to metastasize [95]. The RANKL-mediated tumor metastasis operates through Treg cells, though exogenous RANKL is equally effective. The elevated expression of RANKL in metastatic tumors is dependent on local populations of Treg cells in the adjacent stroma. Collectively these results suggest an underappreciated level of interplay between mammary epithelial cells and Treg cells governing cancer-associated inflammation.
The fluctuations of estrogen and progesterone during the menstrual cycle have direct and indirect effects on the local mammary gland immune system. The immune microenvironment during the luteal phase and pregnancy are characterized by high concentrations of serum estrogen and progesterone. The principal effects of estrogen and progesterone on the local immune system of the mammary gland are the recruitment of immune cells via CSF1, TGFB and IL10 which skew the cells towards a developmental role in mammary morphogenesis [6, 13, 52], thus reducing the active immune surveillance of the mammary epithelia. An additional effect of progesterone-driven mammary epithelia remodeling is the immune dampening by phagocytosis of apoptotic cells, which releases the immunomodulatory cytokines, IL4 and IL10. Estrogen and progesterone also have direct effects on the function of immune cells. Macrophages are directed into a tissue remodeling phenotype which downregulates expression of critical immune markers such as MHC class II and decreases the secretion of inflammatory cytokines. Collectively, these findings indicate that the combined effect of estrogen and progesterone in the mammary gland result in a net dampening of local immune surveillance, toward an environment exhibiting immune tolerance, which may lead to enhanced tumorigenesis due to decreased cancer cell detection and eradication.
Conclusion
The mammary gland undergoes hormonally mediated continual cycles of tissue remodeling, alongside cyclical modulation of the immune system between states of inflammation and immunotolerance. The cumulative effects of this process, which involves luteal phase-driven mammary epithelial cell proliferation and differentiation, may enhance tumor growth after the initial stage of genetic aberration in mammary epithelial cells that is necessary for tumorigenesis. If this stage occurs in a proliferating immunotolerant mammary gland that is ill-equipped to detect and eliminate aberrant cells, then breast cancer risk is likely to be exacerbated. In conclusion, immune system cells and cytokines have essential roles in hormonally-driven mammary gland development. Future studies investigating the precise relationship between estrogen, progesterone, mammary epithelial cell function and the immune environment are required in order to fully appreciate their combined influence on breast cancer risk.
Abbreviations
- AR:
-
Androgen receptor
- COX2:
-
Cyclooxygenase-2 enzyme
- CSF:
-
Colony-stimulating factor
- ERBB1/EGFR:
-
Epidermal growth factor receptor
- ERα:
-
Estrogen receptor alpha
- IFNG:
-
Interferon gamma
- IL:
-
Interleukin
- IκB:
-
Inhibitor of NF-κB
- LPS:
-
Lipopolysaccharide
- NF-κB:
-
Nuclear factor kappa B
- PR:
-
Progesterone receptor
- RANK:
-
Receptor activator of NF-κB
- RANKL:
-
Receptor activator of NF-κB ligand
- TDLU:
-
Terminal ductal lobular units
- TEB:
-
Terminal end buds
- Th:
-
Helper T lymphocytes
- TLR:
-
Toll-like receptor
- TNFA:
-
Tumor necrosis factor alpha
- Treg:
-
Regulatory T lymphocytes
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Funding Support
EFN is supported by The Hospital Research Foundation Early Career Research Fellowship. WVI is a THRF Associate Professor and National Breast Cancer Foundation Early Career Fellow. PD is supported by an Australian Breast Cancer Research Postdoctoral Fellowship. We thank Mr Peter Adams for his expert illustrative assistance with the figures.
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Need, E.F., Atashgaran, V., Ingman, W.V. et al. Hormonal Regulation of the Immune Microenvironment in the Mammary Gland. J Mammary Gland Biol Neoplasia 19, 229–239 (2014). https://doi.org/10.1007/s10911-014-9324-x
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DOI: https://doi.org/10.1007/s10911-014-9324-x