Sage Journals: Discover world-class research

Abstract

Female sex hormones, the octamer-binding transcription factor 4 (OCT4), and human endogenous retroviruses (HERVs) are all involved in the development of breast cancer. However, whether there are cross talks between these factors to promote breast cancer is still unknown. Using the T47D human breast cancer cell line, we have found that estradiol and progesterone synergistically activate HERV-K through nuclear receptors. The progesterone receptor (isoform B) binds a progesterone-response element (PRE) in a long terminal repeat (LTR5HS) of HERV-K. There is another transcription factor-binding element in the LTR, the octamer motif, which is required for the hormones to activate gene transcription downstream of the LTR. Gel shift assays and co-immunoprecipitation indicate that the progesterone receptor (PR) and the OCT4 transcription factor interact on the protein level. Methylation of the PRE enhances binding of the PR. These findings help to elucidate the previously unknown cross talks among the sex hormones, OCT4, and HERVs in contributing to breast cancer proliferation and tumorigenesis, which may be useful in guiding further development of cancer therapies.

Get full access to this article

View all access options for this article.

References

Bernhardt

, Dasari

, Walsh

, Townsend

, Price

, Ingman

: Hormonal modulation of breast cancer gene expression: Implications for intrinsic subtyping in premenopausal women. Front Oncol, 2016; 6:241.

Giangrande

, McDonnell

: The A and B isoforms of the human progesterone receptor: Two functionally different transcription factors encoded by a single gene. Recent Prog Horm Res, 1999; 54:291–313.

Wei

, Miner

: Evidence for the existence of a third progesterone receptor protein in human breast cancer cell line T47D. Cancer Res, 1994; 54:340–343.

Lange

, Yee

: Progesterone and breast cancer. Womens Health (Lond), 2008; 4:151–162.

Faivre

, Daniel

, Hillard

, Lange

: Progesterone receptor rapid signaling mediates serine 345 phosphorylation and tethering to specificity protein 1 transcription factors. Mol Endocrinol, 2008; 22:823–837.

Migliaccio

, Piccolo

, Castoria

, et al.: Activation of the Src/p21ras/Erk pathway by progesterone receptor via cross-talk with estrogen receptor. EMBO J, 1998; 17:2008–2018.

Faivre

, Lange

: Progesterone receptors upregulate Wnt-1 to induce epidermal growth factor receptor transactivation and c-Src-dependent sustained activation of Erk1/2 mitogen-activated protein kinase in breast cancer cells. Mol Cell Biol, 2007; 27:466–480.

Zhou

, Li

, Wei

, et al.: Activation of HERV-K Env protein is essential for tumorigenesis and metastasis of breast cancer cells. Oncotarget, 2016; 7:84093–84117.

Lemaître

, Tsang

, Bireau

, Heidmann

, Dewannieux

: A human endogenous retrovirus-derived gene that can contribute to oncogenesis by activating the ERK pathway and inducing migration and invasion. PLoS Pathog, 2017; 13:e1006451.

10.

Ono

, Kawakami

, Ushikubo

: Stimulation of expression of the human endogenous retrovirus genome by female steroid hormones in human breast cancer cell line T47D. J Virol, 1987; 61:2059–2062.

11.

Golan

, Hizi

, Resau

, et al.: Human endogenous retrovirus (HERV-K) reverse transcriptase as a breast cancer prognostic marker. Neoplasia, 2008; 10:521–533.

12.

Patience

, Simpson

, Colletta

, Welch

, Weiss

, Boyd

: Human endogenous retrovirus expression and reverse transcriptase activity in the T47D mammary carcinoma cell line. J Virol, 1996; 70:2654–2657.

13.

Nusse

, Varmus

: Many tumors induced by the mouse mammary tumor virus contain a provirus integrated in the same region of the host genome. Cell, 1982; 31:99–109.

14.

Grow

, Flynn

, Chavez

, et al.: Intrinsic retroviral reactivation in human preimplantation embryos and pluripotent cells. Nature, 2015; 522:221–225.

15.

Gogvadze

, Stukacheva

, Buzdin

, Sverdlov

: Human-specific modulation of transcriptional activity provided by endogenous retroviral insertions. J Virol, 2009; 83:6098–6105.

16.

Kar

, Patra

: Overexpression of OCT4 induced by modulation of histone marks plays crucial role in breast cancer progression. Gene, 2018; 643:35–45.

17.

Liu

, Sun

, Zhao

, et al.: OCT4 expression and vasculogenic mimicry formation positively correlate with poor prognosis in human breast cancer. Int J Mol Sci, 2014; 15:19634–19649.

18.

Contreras-Galindo

, González

, Almodovar-Camacho

, González-Ramírez

, Lorenzo

, Yamamura

: A new real-time-RT-PCR for quantitation of human endogenous retroviruses type K (HERV-K) RNA load in plasma samples: Increased HERV-K RNA titers in HIV-1 patients with HAART non-suppressive regimens. J Virol Methods, 2006; 136:51–57.

19.

Wang-Johanning

, Frost

, Jian

, Epp

, Lu

, Johanning

: Quantitation of HERV-K env gene expression and splicing in human breast cancer. Oncogene, 2003; 22:1528–1535.

20.

Spinsanti

, Panti

, Bucalossi

, et al.: Selection of reliable reference genes for qRT-PCR studies on cetacean fibroblast cultures exposed to OCs, PBDEs, and 17beta-estradiol. Aquat Toxicol, 2008; 87:178–186.

21.

Toegel

, Huang

, Piana

, et al.: Selection of reliable reference genes for qPCR studies on chondroprotective action. BMC Mol Biol, 2007; 8:13.

22.

Mueller

, Moore

, Giovannucci

, et al.: Expression of human endogenous retroviruses in peripheral leukocytes during the menstrual cycle suggests coordinated hormonal regulation. AIDS Res Hum Retroviruses, 2018; 34:909–911.

23.

Lee

, Bieniasz

: Reconstitution of an infectious human endogenous retrovirus. PLoS Pathog, 2007; 3:e10.

24.

Manghera

, Douville

: Endogenous retrovirus-K promoter: A landing strip for inflammatory transcription factors?. Retrovirology, 2013; 10:16.

25.

Jackson

, Bartz

, Schelter

, et al.: Expression profiling reveals off-target gene regulation by RNAi. Nat Biotechnol, 2003; 21:635–637.

26.

Wang

Y-J

, Herlyn

: The emerging roles of Oct4 in tumor-initiating cells. Am J Physiol Cell Physiol, 2015; 309:C709–C718.

27.

María

, Paola

, Niki

, Mariacarmela

, Julià

, Rafael

: Human endogenous retroviruses and cancer. Cancer Biol Med, 2016; 13:483–488.

28.

Ohnuki

, Tanabe

, Sutou

, et al.: Dynamic regulation of human endogenous retroviruses mediates factor-induced reprogramming and differentiation potential. Proc Natl Acad Sci U S A, 2014; 111:12426–12431.

29.

Göke

, Lu

, Chan

, et al.: Dynamic transcription of distinct classes of endogenous retroviral elements marks specific populations of early human embryonic cells. Cell Stem Cell, 2015; 16:135–141.

30.

Gorbatenko

, Olesen

, Boedtkjer

, Pedersen

: Regulation and roles of bicarbonate transporters in cancer. Front Physiol, 2014; 5:130.

31.

Skildum

, Faivre

, Lange

: Progesterone receptors induce cell cycle progression via activation of mitogen-activated protein kinases. Mol Endocrinol, 2005; 19:327–339.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.03 MB

Female Sex Hormones Activate Human Endogenous Retrovirus Type K Through the OCT4 Transcription Factor in T47D Breast Cancer Cells

Abstract

Get full access to this article

References

Supplementary Material