Abstract

IntroductionPuberty is a period of increased susceptibility to factors that cause increased breast cancer risk in adulthood. Mammary end buds (EBs) that develop during puberty are believed to be the targets of breast cancer initiation. Whereas the role of estrogen (E) has been extensively studied in pubertal mammary gland development, the role of progesterone (P) during puberty is less defined.MethodsPubertal and prepubertal ovariectomized mice were treated with vehicle control (C), E, P, or E+P. Mammary glands from these mice were analyzed for changes in morphology, proliferation, and expression of the downstream targets amphiregulin (AREG) and receptor activator of NF-κB ligand (RANKL).ResultsP, acting specifically through the progesterone receptor, induced increases in mammary gland proliferation and EB formation that were associated with increased AREG expression in ducts and EBs. E, acting specifically through the estrogen receptor, produced similar responses also mediated by AREG. Blocking AREG action by treatment with an EGFR inhibitor completely abrogated the effect of P on EB formation and proliferation and significantly reduced proliferation within ducts. P also increased expression of RANKL, primarily in ducts. Treatment with RANK-Fc, an inhibitor of RANKL, reduced P-dependent proliferation in ducts and to a lesser extent in EB, but did not cause EB regression.ConclusionsThese results demonstrate a novel P-specific effect through AREG to cause EB formation and proliferation in the developing mammary gland both before and during puberty. Thus, hormones and/or factors in addition to E that upregulate AREG can promote mammary gland development and have the potential to affect breast cancer risk associated with pubertal mammary gland development.

Highlights

  • Puberty is a period of increased susceptibility to factors that cause increased breast cancer risk in adulthood

  • We found that P acting through progesterone receptor (PR) caused pubertal end bud (EB) formation, which was dependent on an increase in amphiregulin (AREG) expression

  • Limited sidebranching was observed in response to P or E2+P in the pubertal mammary gland in contrast to the extensive sidebranching normally seen in the adult BALB/c mammary gland at the same hormone doses [24] (Figure 1C)

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Summary

Introduction

Puberty is a period of increased susceptibility to factors that cause increased breast cancer risk in adulthood. Mammary end buds (EBs) that develop during puberty are believed to be the targets of breast cancer initiation. Whereas the role of estrogen (E) has been extensively studied in pubertal mammary gland development, the role of progesterone (P) during puberty is less defined. The mouse mammary gland is used as a model for development of the human breast. Rapid changes in the hormonal milieu drive increased proliferation and expanded ductal development to fill the fat pad (reviewed in [1]). During this time, highly proliferative structures called end buds (EBs) are present at the leading growth front of ducts in the gland (reviewed in [2]). EBs progress into the mammary fat pad, and the ductal network is formed by bifurcation of the EBs and branching of ducts until the fat pad is filled with an extensive, branched ductal system.

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