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Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells

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Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells. / Werner, Stefan; Stamm, Hauke; Pandjaitan, Mutiha; Kemming, Dirk; Brors, Benedikt; Pantel, Klaus; Wikman, Harriet.

In: BMC CANCER, Vol. 15, No. 1, 2015, p. 896.

Research output: SCORING: Contribution to journalSCORING: Journal articleResearchpeer-review

Harvard

Werner, S, Stamm, H, Pandjaitan, M, Kemming, D, Brors, B, Pantel, K & Wikman, H 2015, 'Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells', BMC CANCER, vol. 15, no. 1, pp. 896. https://doi.org/10.1186/s12885-015-1907-4

APA

Werner, S., Stamm, H., Pandjaitan, M., Kemming, D., Brors, B., Pantel, K., & Wikman, H. (2015). Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells. BMC CANCER, 15(1), 896. https://doi.org/10.1186/s12885-015-1907-4

Vancouver

Werner S, Stamm H, Pandjaitan M, Kemming D, Brors B, Pantel K et al. Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells. BMC CANCER. 2015;15(1):896. https://doi.org/10.1186/s12885-015-1907-4

Bibtex

@article{85b4c4cfa8c34ba19637fb6cfb771906,
title = "Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells",
abstract = "BACKGROUND: Disseminated tumor cells (DTCs) can be detected using ultrasensitive immunocytochemical assays and their presence in the bone marrow can predict the subsequent occurrence of overt metastasis formation and metastatic relapse. Using expression profiling on early stage primary breast tumors, low IRX2 expression was previously shown to be associated with the presence of DTCs in the bone marrow, suggesting a possible role of IRX2 in the early steps of metastasis formation. The purpose of this study is to gain insights into the significance of IRX2 protein function in the progression of breast cancer.METHODS: To assess the physiological relevance of IRX2 in breast cancer, we evaluated IRX2 expression in a large breast cancer cohort (n = 1992). Additionally, constitutive IRX2 over expression was established in BT-549 and Hs578T breast cancer cell lines. Subsequently we analyzed whether IRX2 overexpression effects chemokine secretion and cellular motility of these cells.RESULTS: Low IRX2 mRNA expression was found to correlate with high tumor grade, positive lymph node status, negative hormone receptor status, and basal type of primary breast tumors. Also in cell lines low IRX2 expression was associated with mainly basal breast cancer cell lines. The functional studies show that overexpression of the IRX2 transcription factor in basal cell lines suppressed secretion of the pro-metastatic chemokines and inhibited cellular motility but did not influence cell proliferation.CONCLUSION: Our results imply that the IRX2 transcription factor might represent a novel metastasis associated protein that acts as a negative regulator of cellular motility and as a repressor of chemokine expression. Loss of IRX2 expression could therefore contribute to early hematogenous dissemination of breast cancer by sustaining chemokine secretion and enabling mobilization of tumor cells.",
author = "Stefan Werner and Hauke Stamm and Mutiha Pandjaitan and Dirk Kemming and Benedikt Brors and Klaus Pantel and Harriet Wikman",
year = "2015",
doi = "10.1186/s12885-015-1907-4",
language = "English",
volume = "15",
pages = "896",
journal = "BMC CANCER",
issn = "1471-2407",
publisher = "BioMed Central Ltd.",
number = "1",

}

RIS

TY - JOUR

T1 - Iroquois homeobox 2 suppresses cellular motility and chemokine expression in breast cancer cells

AU - Werner, Stefan

AU - Stamm, Hauke

AU - Pandjaitan, Mutiha

AU - Kemming, Dirk

AU - Brors, Benedikt

AU - Pantel, Klaus

AU - Wikman, Harriet

PY - 2015

Y1 - 2015

N2 - BACKGROUND: Disseminated tumor cells (DTCs) can be detected using ultrasensitive immunocytochemical assays and their presence in the bone marrow can predict the subsequent occurrence of overt metastasis formation and metastatic relapse. Using expression profiling on early stage primary breast tumors, low IRX2 expression was previously shown to be associated with the presence of DTCs in the bone marrow, suggesting a possible role of IRX2 in the early steps of metastasis formation. The purpose of this study is to gain insights into the significance of IRX2 protein function in the progression of breast cancer.METHODS: To assess the physiological relevance of IRX2 in breast cancer, we evaluated IRX2 expression in a large breast cancer cohort (n = 1992). Additionally, constitutive IRX2 over expression was established in BT-549 and Hs578T breast cancer cell lines. Subsequently we analyzed whether IRX2 overexpression effects chemokine secretion and cellular motility of these cells.RESULTS: Low IRX2 mRNA expression was found to correlate with high tumor grade, positive lymph node status, negative hormone receptor status, and basal type of primary breast tumors. Also in cell lines low IRX2 expression was associated with mainly basal breast cancer cell lines. The functional studies show that overexpression of the IRX2 transcription factor in basal cell lines suppressed secretion of the pro-metastatic chemokines and inhibited cellular motility but did not influence cell proliferation.CONCLUSION: Our results imply that the IRX2 transcription factor might represent a novel metastasis associated protein that acts as a negative regulator of cellular motility and as a repressor of chemokine expression. Loss of IRX2 expression could therefore contribute to early hematogenous dissemination of breast cancer by sustaining chemokine secretion and enabling mobilization of tumor cells.

AB - BACKGROUND: Disseminated tumor cells (DTCs) can be detected using ultrasensitive immunocytochemical assays and their presence in the bone marrow can predict the subsequent occurrence of overt metastasis formation and metastatic relapse. Using expression profiling on early stage primary breast tumors, low IRX2 expression was previously shown to be associated with the presence of DTCs in the bone marrow, suggesting a possible role of IRX2 in the early steps of metastasis formation. The purpose of this study is to gain insights into the significance of IRX2 protein function in the progression of breast cancer.METHODS: To assess the physiological relevance of IRX2 in breast cancer, we evaluated IRX2 expression in a large breast cancer cohort (n = 1992). Additionally, constitutive IRX2 over expression was established in BT-549 and Hs578T breast cancer cell lines. Subsequently we analyzed whether IRX2 overexpression effects chemokine secretion and cellular motility of these cells.RESULTS: Low IRX2 mRNA expression was found to correlate with high tumor grade, positive lymph node status, negative hormone receptor status, and basal type of primary breast tumors. Also in cell lines low IRX2 expression was associated with mainly basal breast cancer cell lines. The functional studies show that overexpression of the IRX2 transcription factor in basal cell lines suppressed secretion of the pro-metastatic chemokines and inhibited cellular motility but did not influence cell proliferation.CONCLUSION: Our results imply that the IRX2 transcription factor might represent a novel metastasis associated protein that acts as a negative regulator of cellular motility and as a repressor of chemokine expression. Loss of IRX2 expression could therefore contribute to early hematogenous dissemination of breast cancer by sustaining chemokine secretion and enabling mobilization of tumor cells.

U2 - 10.1186/s12885-015-1907-4

DO - 10.1186/s12885-015-1907-4

M3 - SCORING: Journal article

C2 - 26560478

VL - 15

SP - 896

JO - BMC CANCER

JF - BMC CANCER

SN - 1471-2407

IS - 1

ER -