- Huh, Sung Jin;
- Clement, Kendell;
- Jee, David;
- Merlini, Alessandra;
- Choudhury, Sibgat;
- Maruyama, Reo;
- Yoo, Ronnie;
- Chytil, Anna;
- Boyle, Patrick;
- Ran, Fei Ann;
- Moses, Harold L;
- Barcellos-Hoff, Mary Helen;
- Jackson-Grusby, Laurie;
- Meissner, Alexander;
- Polyak, Kornelia
Postnatal mammary gland development and differentiation occur during puberty and pregnancy. To explore the role of DNA methylation in these processes, we determined the genome-wide DNA methylation and gene expression profiles of CD24(+)CD61(+)CD29(hi), CD24(+)CD61(+)CD29(lo), and CD24(+)CD61(-)CD29(lo) cell populations that were previously associated with distinct biological properties at different ages and reproductive stages. We found that pregnancy had the most significant effects on CD24(+)CD61(+)CD29(hi) and CD24(+)CD61(+)CD29(lo) cells, inducing distinct epigenetic states that were maintained through life. Integrated analysis of gene expression, DNA methylation, and histone modification profiles revealed cell-type- and reproductive-stage-specific changes. We identified p27 and TGFβ signaling as key regulators of CD24(+)CD61(+)CD29(lo) cell proliferation, based on their expression patterns and results from mammary gland explant cultures. Our results suggest that relatively minor changes in DNA methylation occur during luminal differentiation compared with the effects of pregnancy on CD24(+)CD61(+)CD29(hi) and CD24(+)CD61(+)CD29(lo) cells.