Annexin A8 identifies a subpopulation of transiently quiescent c-kit positive luminal progenitor cells of the ductal mammary epithelium.

Juan Manuel Iglesias,Howard Kendrick,Matthew J Smalley,Finian Martin,Kelly Soady,Karen Blyth,Roderick K Ferrier,Reginald O Morgan,Marie-Anne Pringle,Laura Mcdonald,Claire J Cairney,Torsten Stein,Tiffany Seagroves

doi:10.1371/journal.pone.0119718

Abstract

We have previously shown that Annexin A8 (ANXA8) is strongly associated with the basal-like subgroup of breast cancers, including BRCA1-associated breast cancers, and poor prognosis; while in the mouse mammary gland AnxA8 mRNA is expressed in low-proliferative isolated pubertal mouse mammary ductal epithelium and after enforced involution, but not in isolated highly proliferative terminal end buds (TEB) or during pregnancy. To better understand ANXA8’s association with this breast cancer subgroup we established ANXA8’s cellular distribution in the mammary gland and ANXA8’s effect on cell proliferation. We show that ANXA8 expression in the mouse mammary gland was strong during pre-puberty before the expansion of the rudimentary ductal network and was limited to a distinct subpopulation of ductal luminal epithelial cells but was not detected in TEB or in alveoli during pregnancy. Similarly, during late involution its expression was found in the surviving ductal epithelium, but not in the apoptotic alveoli. Double-immunofluorescence (IF) showed that ANXA8 positive (+ve) cells were ER-alpha negative (−ve) and mostly quiescent, as defined by lack of Ki67 expression during puberty and mid-pregnancy, but not terminally differentiated with ∼15% of ANXA8 +ve cells re-entering the cell cycle at the start of pregnancy (day 4.5). RT-PCR on RNA from FACS-sorted cells and double-IF showed that ANXA8+ve cells were a subpopulation of c-kit +ve luminal progenitor cells, which have recently been identified as the cells of origin of basal-like breast cancers. Over expression of ANXA8 in the mammary epithelial cell line Kim-2 led to a G0/G1 arrest and suppressed Ki67 expression, indicating cell cycle exit. Our data therefore identify ANXA8 as a potential mediator of quiescence in the normal mouse mammary ductal epithelium, while its expression in basal-like breast cancers may be linked to ANXA8’s association with their specific cells of origin.

Highlights

Annexins form a superfamily of calcium-dependent lipid-binding proteins broadly distributed throughout all eukaryotic phyla and even some bacteria and archea
We have previously shown that Anxa8 mRNA was up-regulated during mouse mammary gland involution [29], a multi-step process in which the alveolar epithelium regresses by programmed cell death to a near pre-pregnant morphology [27, 32]
Annexin A8 (ANXA8) is expressed in a distinct subpopulation of luminal ductal epithelial cells

Summary

Introduction

Annexins form a superfamily of calcium-dependent lipid-binding proteins broadly distributed throughout all eukaryotic phyla and even some bacteria and archea These proteins feature unique homologous repeats that contain the calcium and lipid binding sites. Annexins have been shown to act as extracellular anti-inflammatory and anti-coagulant factors as cell surface proteins, and some have even been proposed to have nuclear roles [2,3,4,5] They are further involved in phagocytosis as well as endo- and exocytosis (for reviews see [6,7,8,9]). Function-oriented studies have described annexins involved in cell growth and proliferation [10,11,12] and alterations of their expression have been associated with cancer subtypes and other diseases [13,14,15,16]

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