Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells

Yingchen Zhuo; Xueqian Li; Qiaowei Zheng; Xingjun Fan; Wenbing Ma; Jingguo Chen; Xue Zhao; Peipei Zhao; Xuanlin Liu; Fengru Tang; Kai Cheng; Weiyi Feng

doi:10.3892/or.2018.6631

Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells

Yingchen Zhuo, Xueqian Li, Qiaowei Zheng, Xingjun Fan, Wenbing Ma, Jingguo Chen, Xue Zhao, Peipei Zhao, Xuanlin Liu, Fengru Tang, Kai Cheng, Weiyi Feng

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

Estradiol (E2) is a prime culprit for enhancing the progression of female hormone.related cancers. Bone marrow.derived cells (BMDCs) have been found to play a pivotal role in tumor growth. Estrogen receptors (ERs) are also found on certain subtypes of BMDCs, in addition to endothelial cells (ECs) and certain tumor cells. However, the role of BMDCs in E2-induced tumor biology is still unclear. Thus, the effects of E2 on ER-negative 4T1 breast cancer growth, the mobilization and recruitment of BMDCs, and interactions among BMDCs, ECs, and 4T1 cells were investigated. The results showed that E2 potentiated 4T1 tumor growth and angiogenesis in mice subjected to sham operation, ovariectomy (OVX), or OVX and E2 replacement treatment. E2 supplementation in mice with OVX upregulated the transcription of stromal cell.derived factor-1 (SDF-1) mRNA in tumor tissues and enhanced the recruitment of BMDCs into tumor tissues in vivo. E2 deficiency significantly decreased proangiogenic CXCR4⁺, β₃ ⁺, Sca-1⁺ and CXCR4⁺β₃ ⁺ BMDCs circulating in the peripheral blood. Cell-based system analyses showed that E2 augmented the transcription of β₃ mRNA in ECs, increased the adhesion of BMDCs to ECs. In addition, E2 enhanced the BMDC-induced EC proliferation and migration, the BMDC-induced 4T1 proliferation and the 4T1-stimulated EC proliferation in addition to enhancing the proliferation of tumor cells and the migration of ECs in vitro. Therefore, E2 enhanced the growth of breast tumors by stimulating tumor cells and ECs directly, as well as by increasing proangiogenic BMDC mobilization and recruitment leading to augmentation of the tumor and EC functions indirectly by cell proliferation assay. These findings reveal a separate mechanism via which E2 promotes the growth of female hormone-dependent tumors, which may be useful in explorations of new therapies for related cancers.

Original language	English (US)
Pages (from-to)	2147-2156
Number of pages	10
Journal	Oncology Reports
Volume	40
Issue number	4
DOIs	https://doi.org/10.3892/or.2018.6631
State	Published - Oct 2018
Externally published	Yes

Keywords

Angiogenesis
Bone marrow cells
Breast carcinoma
Carcinogenesis
Estradiol

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3892/or.2018.6631

Cite this

Zhuo, Y., Li, X., Zheng, Q., Fan, X., Ma, W., Chen, J., Zhao, X., Zhao, P., Liu, X., Tang, F., Cheng, K., & Feng, W. (2018). Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells. Oncology Reports, 40(4), 2147-2156. https://doi.org/10.3892/or.2018.6631

Zhuo, Y, Li, X, Zheng, Q, Fan, X, Ma, W, Chen, J, Zhao, X, Zhao, P, Liu, X, Tang, F, Cheng, K & Feng, W 2018, 'Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells', Oncology Reports, vol. 40, no. 4, pp. 2147-2156. https://doi.org/10.3892/or.2018.6631

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title = "Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells",

abstract = "Estradiol (E2) is a prime culprit for enhancing the progression of female hormone.related cancers. Bone marrow.derived cells (BMDCs) have been found to play a pivotal role in tumor growth. Estrogen receptors (ERs) are also found on certain subtypes of BMDCs, in addition to endothelial cells (ECs) and certain tumor cells. However, the role of BMDCs in E2-induced tumor biology is still unclear. Thus, the effects of E2 on ER-negative 4T1 breast cancer growth, the mobilization and recruitment of BMDCs, and interactions among BMDCs, ECs, and 4T1 cells were investigated. The results showed that E2 potentiated 4T1 tumor growth and angiogenesis in mice subjected to sham operation, ovariectomy (OVX), or OVX and E2 replacement treatment. E2 supplementation in mice with OVX upregulated the transcription of stromal cell.derived factor-1 (SDF-1) mRNA in tumor tissues and enhanced the recruitment of BMDCs into tumor tissues in vivo. E2 deficiency significantly decreased proangiogenic CXCR4+, β3 +, Sca-1+ and CXCR4+β3 + BMDCs circulating in the peripheral blood. Cell-based system analyses showed that E2 augmented the transcription of β3 mRNA in ECs, increased the adhesion of BMDCs to ECs. In addition, E2 enhanced the BMDC-induced EC proliferation and migration, the BMDC-induced 4T1 proliferation and the 4T1-stimulated EC proliferation in addition to enhancing the proliferation of tumor cells and the migration of ECs in vitro. Therefore, E2 enhanced the growth of breast tumors by stimulating tumor cells and ECs directly, as well as by increasing proangiogenic BMDC mobilization and recruitment leading to augmentation of the tumor and EC functions indirectly by cell proliferation assay. These findings reveal a separate mechanism via which E2 promotes the growth of female hormone-dependent tumors, which may be useful in explorations of new therapies for related cancers.",

keywords = "Angiogenesis, Bone marrow cells, Breast carcinoma, Carcinogenesis, Estradiol",

author = "Yingchen Zhuo and Xueqian Li and Qiaowei Zheng and Xingjun Fan and Wenbing Ma and Jingguo Chen and Xue Zhao and Peipei Zhao and Xuanlin Liu and Fengru Tang and Kai Cheng and Weiyi Feng",

note = "Funding Information: The present study was supported by the National Natural Science Foundation of China (no. 81071765 and 81372379), the Natural Science Foundation of Shaanxi Province (no. 2016JM8037), and the Research Foundation of The First Affiliated Hospital of Xi'an Jiaotong University (no. 2017MS-09).",

year = "2018",

month = oct,

doi = "10.3892/or.2018.6631",

language = "English (US)",

volume = "40",

pages = "2147--2156",

journal = "Oncology Reports",

issn = "1021-335X",

publisher = "Spandidos Publications",

number = "4",

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TY - JOUR

T1 - Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells

AU - Zhuo, Yingchen

AU - Li, Xueqian

AU - Zheng, Qiaowei

AU - Fan, Xingjun

AU - Ma, Wenbing

AU - Chen, Jingguo

AU - Zhao, Xue

AU - Zhao, Peipei

AU - Liu, Xuanlin

AU - Tang, Fengru

AU - Cheng, Kai

AU - Feng, Weiyi

N1 - Funding Information: The present study was supported by the National Natural Science Foundation of China (no. 81071765 and 81372379), the Natural Science Foundation of Shaanxi Province (no. 2016JM8037), and the Research Foundation of The First Affiliated Hospital of Xi'an Jiaotong University (no. 2017MS-09).

PY - 2018/10

Y1 - 2018/10

N2 - Estradiol (E2) is a prime culprit for enhancing the progression of female hormone.related cancers. Bone marrow.derived cells (BMDCs) have been found to play a pivotal role in tumor growth. Estrogen receptors (ERs) are also found on certain subtypes of BMDCs, in addition to endothelial cells (ECs) and certain tumor cells. However, the role of BMDCs in E2-induced tumor biology is still unclear. Thus, the effects of E2 on ER-negative 4T1 breast cancer growth, the mobilization and recruitment of BMDCs, and interactions among BMDCs, ECs, and 4T1 cells were investigated. The results showed that E2 potentiated 4T1 tumor growth and angiogenesis in mice subjected to sham operation, ovariectomy (OVX), or OVX and E2 replacement treatment. E2 supplementation in mice with OVX upregulated the transcription of stromal cell.derived factor-1 (SDF-1) mRNA in tumor tissues and enhanced the recruitment of BMDCs into tumor tissues in vivo. E2 deficiency significantly decreased proangiogenic CXCR4+, β3 +, Sca-1+ and CXCR4+β3 + BMDCs circulating in the peripheral blood. Cell-based system analyses showed that E2 augmented the transcription of β3 mRNA in ECs, increased the adhesion of BMDCs to ECs. In addition, E2 enhanced the BMDC-induced EC proliferation and migration, the BMDC-induced 4T1 proliferation and the 4T1-stimulated EC proliferation in addition to enhancing the proliferation of tumor cells and the migration of ECs in vitro. Therefore, E2 enhanced the growth of breast tumors by stimulating tumor cells and ECs directly, as well as by increasing proangiogenic BMDC mobilization and recruitment leading to augmentation of the tumor and EC functions indirectly by cell proliferation assay. These findings reveal a separate mechanism via which E2 promotes the growth of female hormone-dependent tumors, which may be useful in explorations of new therapies for related cancers.

AB - Estradiol (E2) is a prime culprit for enhancing the progression of female hormone.related cancers. Bone marrow.derived cells (BMDCs) have been found to play a pivotal role in tumor growth. Estrogen receptors (ERs) are also found on certain subtypes of BMDCs, in addition to endothelial cells (ECs) and certain tumor cells. However, the role of BMDCs in E2-induced tumor biology is still unclear. Thus, the effects of E2 on ER-negative 4T1 breast cancer growth, the mobilization and recruitment of BMDCs, and interactions among BMDCs, ECs, and 4T1 cells were investigated. The results showed that E2 potentiated 4T1 tumor growth and angiogenesis in mice subjected to sham operation, ovariectomy (OVX), or OVX and E2 replacement treatment. E2 supplementation in mice with OVX upregulated the transcription of stromal cell.derived factor-1 (SDF-1) mRNA in tumor tissues and enhanced the recruitment of BMDCs into tumor tissues in vivo. E2 deficiency significantly decreased proangiogenic CXCR4+, β3 +, Sca-1+ and CXCR4+β3 + BMDCs circulating in the peripheral blood. Cell-based system analyses showed that E2 augmented the transcription of β3 mRNA in ECs, increased the adhesion of BMDCs to ECs. In addition, E2 enhanced the BMDC-induced EC proliferation and migration, the BMDC-induced 4T1 proliferation and the 4T1-stimulated EC proliferation in addition to enhancing the proliferation of tumor cells and the migration of ECs in vitro. Therefore, E2 enhanced the growth of breast tumors by stimulating tumor cells and ECs directly, as well as by increasing proangiogenic BMDC mobilization and recruitment leading to augmentation of the tumor and EC functions indirectly by cell proliferation assay. These findings reveal a separate mechanism via which E2 promotes the growth of female hormone-dependent tumors, which may be useful in explorations of new therapies for related cancers.

KW - Angiogenesis

KW - Bone marrow cells

KW - Breast carcinoma

KW - Carcinogenesis

KW - Estradiol

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M3 - Article

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AN - SCOPUS:85051545290

SN - 1021-335X

VL - 40

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JO - Oncology Reports

JF - Oncology Reports

IS - 4

ER -

Estrogen enhances tumor growth and angiogenesis indirectly via mediation of bone marrow-derived cells as well as directly through stimulation of tumor and endothelial cells

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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