Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment

Mammary epithelial progenitors are the normal cell-of-origin of breast cancer. We previously defined a population of p27(+) quiescent hormone-responsive progenitor cells in the normal human breast whose frequency associates with breast cancer risk. Here, we describe that deletion of the Cdkn1b gene...

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Autores principales: Ding, Lina, Shunkwiler, Lauren B., Harper, Nicholas W., Zhao, Yang, Hinohara, Kunihiko, Huh, Sung Jin, Ekram, Muhammad B., Guz, Jan, Kern, Michael J., Awgulewitsch, Alexander, Shull, James D., Smits, Bart M. G., Polyak, Kornelia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6443185/
https://www.ncbi.nlm.nih.gov/pubmed/30893315
http://dx.doi.org/10.1371/journal.pgen.1008002
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author Ding, Lina
Shunkwiler, Lauren B.
Harper, Nicholas W.
Zhao, Yang
Hinohara, Kunihiko
Huh, Sung Jin
Ekram, Muhammad B.
Guz, Jan
Kern, Michael J.
Awgulewitsch, Alexander
Shull, James D.
Smits, Bart M. G.
Polyak, Kornelia
author_facet Ding, Lina
Shunkwiler, Lauren B.
Harper, Nicholas W.
Zhao, Yang
Hinohara, Kunihiko
Huh, Sung Jin
Ekram, Muhammad B.
Guz, Jan
Kern, Michael J.
Awgulewitsch, Alexander
Shull, James D.
Smits, Bart M. G.
Polyak, Kornelia
author_sort Ding, Lina
collection PubMed
description Mammary epithelial progenitors are the normal cell-of-origin of breast cancer. We previously defined a population of p27(+) quiescent hormone-responsive progenitor cells in the normal human breast whose frequency associates with breast cancer risk. Here, we describe that deletion of the Cdkn1b gene encoding the p27 cyclin-dependent kinase inhibitor in the estrogen-induced mammary tumor-susceptible ACI rat strain leads to a decrease in the relative frequencies of Cd49b(+) mammary luminal epithelial progenitors and pregnancy-related differentiation. We show by comprehensive gene expression profiling of purified progenitor and differentiated mammary epithelial cell populations that p27 deletion has the most pronounced effects on luminal progenitors. Cdkn1b(-/-) females have decreased fertility, but rats that are able to get pregnant had normal litter size and were able to nurse their pups implying that loss of p27 in ACI rats does not completely abrogate ovarian function and lactation. Reciprocal mammary gland transplantation experiments indicate that the p27-loss-induced changes in mammary epithelial cells are not only caused by alterations in their intrinsic properties, but are likely due to altered hormonal signaling triggered by the perturbed systemic endocrine environment observed in Cdkn1b(-/-) females. We also observed a decrease in the frequency of mammary epithelial cells positive for progesterone receptor (Pr) and FoxA1, known direct transcriptional targets of the estrogen receptor (Erα), and an increase in phospho-Stat5 positive cells commonly induced by prolactin (Prl). Characterization of genome-wide Pr chromatin binding revealed distinct binding patterns in mammary epithelial cells of Cdkn1b(+/+) and Cdkn1b(-/-) females and enrichment in genes with known roles in Notch, ErbB, leptin, and Erα signaling and regulation of G1-S transition. Our data support a role for p27 in regulating the pool size of hormone-responsive luminal progenitors that could impact breast cancer risk.
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spelling pubmed-64431852019-04-17 Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment Ding, Lina Shunkwiler, Lauren B. Harper, Nicholas W. Zhao, Yang Hinohara, Kunihiko Huh, Sung Jin Ekram, Muhammad B. Guz, Jan Kern, Michael J. Awgulewitsch, Alexander Shull, James D. Smits, Bart M. G. Polyak, Kornelia PLoS Genet Research Article Mammary epithelial progenitors are the normal cell-of-origin of breast cancer. We previously defined a population of p27(+) quiescent hormone-responsive progenitor cells in the normal human breast whose frequency associates with breast cancer risk. Here, we describe that deletion of the Cdkn1b gene encoding the p27 cyclin-dependent kinase inhibitor in the estrogen-induced mammary tumor-susceptible ACI rat strain leads to a decrease in the relative frequencies of Cd49b(+) mammary luminal epithelial progenitors and pregnancy-related differentiation. We show by comprehensive gene expression profiling of purified progenitor and differentiated mammary epithelial cell populations that p27 deletion has the most pronounced effects on luminal progenitors. Cdkn1b(-/-) females have decreased fertility, but rats that are able to get pregnant had normal litter size and were able to nurse their pups implying that loss of p27 in ACI rats does not completely abrogate ovarian function and lactation. Reciprocal mammary gland transplantation experiments indicate that the p27-loss-induced changes in mammary epithelial cells are not only caused by alterations in their intrinsic properties, but are likely due to altered hormonal signaling triggered by the perturbed systemic endocrine environment observed in Cdkn1b(-/-) females. We also observed a decrease in the frequency of mammary epithelial cells positive for progesterone receptor (Pr) and FoxA1, known direct transcriptional targets of the estrogen receptor (Erα), and an increase in phospho-Stat5 positive cells commonly induced by prolactin (Prl). Characterization of genome-wide Pr chromatin binding revealed distinct binding patterns in mammary epithelial cells of Cdkn1b(+/+) and Cdkn1b(-/-) females and enrichment in genes with known roles in Notch, ErbB, leptin, and Erα signaling and regulation of G1-S transition. Our data support a role for p27 in regulating the pool size of hormone-responsive luminal progenitors that could impact breast cancer risk. Public Library of Science 2019-03-20 /pmc/articles/PMC6443185/ /pubmed/30893315 http://dx.doi.org/10.1371/journal.pgen.1008002 Text en © 2019 Ding et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ding, Lina
Shunkwiler, Lauren B.
Harper, Nicholas W.
Zhao, Yang
Hinohara, Kunihiko
Huh, Sung Jin
Ekram, Muhammad B.
Guz, Jan
Kern, Michael J.
Awgulewitsch, Alexander
Shull, James D.
Smits, Bart M. G.
Polyak, Kornelia
Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
title Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
title_full Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
title_fullStr Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
title_full_unstemmed Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
title_short Deletion of Cdkn1b in ACI rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
title_sort deletion of cdkn1b in aci rats leads to increased proliferation and pregnancy-associated changes in the mammary gland due to perturbed systemic endocrine environment
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6443185/
https://www.ncbi.nlm.nih.gov/pubmed/30893315
http://dx.doi.org/10.1371/journal.pgen.1008002
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