Publication:
The Major Pre- and Postmenopausal Estrogens Play Opposing Roles in Obesity-Driven Mammary Inflammation and Breast Cancer Development.

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Date

2020-05-11

Authors

Qureshi, Rehana
Picon-Ruiz, Manuel
Aurrekoetxea-Rodriguez, Iskander
Nunes de Paiva, Vanessa
D'Amico, Massimo
Yoon, Hyunho
Radhakrishnan, Ramya
Morata-Tarifa, Cynthia
Ince, Tan
Lippman, Marc E

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Cell Press
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Abstract

Many inflammation-associated diseases, including cancers, increase in women after menopause and with obesity. In contrast to anti-inflammatory actions of 17β-estradiol, we find estrone, which dominates after menopause, is pro-inflammatory. In human mammary adipocytes, cytokine expression increases with obesity, menopause, and cancer. Adipocyte:cancer cell interaction stimulates estrone- and NFκB-dependent pro-inflammatory cytokine upregulation. Estrone- and 17β-estradiol-driven transcriptomes differ. Estrone:ERα stimulates NFκB-mediated cytokine gene induction; 17β-estradiol opposes this. In obese mice, estrone increases and 17β-estradiol relieves inflammation. Estrone drives more rapid ER+ breast cancer growth in vivo. HSD17B14, which converts 17β-estradiol to estrone, associates with poor ER+ breast cancer outcome. Estrone and HSD17B14 upregulate inflammation, ALDH1 activity, and tumorspheres, while 17β-estradiol and HSD17B14 knockdown oppose these. Finally, a high intratumor estrone:17β-estradiol ratio increases tumor-initiating stem cells and ER+ cancer growth in vivo. These findings help explain why postmenopausal ER+ breast cancer increases with obesity, and offer new strategies for prevention and therapy.

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MeSH Terms

Animals
Breast Neoplasms
Cells, Cultured
Estrogens
Female
Humans
Inflammation
Mice
Mice, Congenic
Mice, Inbred C57BL
Mice, Transgenic
Obesity
Postmenopause
Premenopause

DeCS Terms

Células cultivadas
Estrógenos
Inflamación
Neoplasias de la mama
Obesidad
Posmenopausia
Premenopausia
Ratones congénicos
Ratones endogámicos C57BL
Ratones transgénicos

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Keywords

17β-estradiol, ER+ breast cancer, HSD17B14, NFκB, adipocytes, cancer stem cells, cytokines, estrone, inflammation, obesity

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