High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness

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High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness Publisher Pubmed

Mansoori M^{1, 2} ; Roudi R¹ ; Abbasi A³ ; Abolhasani M^{1, 4} ; Abdi Rad I⁵ ; Shariftabrizi A^{1, 6} ; Madjd Z^{1, 2}

Show Affiliations

1. Oncopathology Research Center, Iran University of Medical Sciences, Tehran, Iran
2. Department of Molecular Medicine, Faculty of Advanced Technologies in Medicine, Iran University of Medical Sciences, Tehran, Iran
3. Department of Pathology, Faculty of Medicine, Urmia University of Medical Sciences, Urmia, Iran
4. Hasheminejad Kidney Center, Iran University of Medical Sciences, Tehran, Iran
5. Cellular and Molecular Research Center, Urmia University of Medical Sciences, Urmia, Iran
6. Department of Nuclear Oncology, Memorial Sloan Kettering Cancer Center, New York, United States

Source: Experimental and Molecular Pathology Published:2019

Abstract

Introduction: Breast cancer is the most frequently diagnosed cancer among women. Cancer stem cells (CSCs)are suggested to be responsible for tumor initiation, progression, metastasis, recurrence and drug resistance. This study was conducted to evaluate the clinical significance of GD2, a newly suggested CSC marker and two other traditional CSC markers, CD44 and CD24 in breast cancer patients. Material and methods: A total of 168 primary breast cancer tissues were evaluated in terms of GD2, CD44 and CD24 expression using tissue microarray. Then, the correlation of expression levels of these markers with patients' clinicopathological characteristics was assessed. Results: Higher GD2 expression was mainly found in patients with advanced histological grade (p = 0.02), presence of lymph node invasion (p = 0.04), larger size of tumors (p = 0.04)and older age (p = 0.04). Breast cancer samples with advanced histological grade also showed higher CD44 (p = 0.03)and CD24 expression (p = 0.05). A significant positive association was found between increased CD24 expression and lymph node involvement (p = 0.01). Furthermore, GD2-high/CD44-high/CD24-low phenotype was frequently seen in breast cancer samples with positive lymph node involvement (p = 0.05). Conclusion: In summary, increased expression of GD2 may define more aggressive tumor behavior in breast cancer. GD2 can well be considered as a diagnostic and prognostic marker in breast cancer. © 2019 Elsevier Inc.

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Style	Citing Format
MLA	Mansoori M, et al.. "High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness." Experimental and Molecular Pathology, vol. 109, no. , 2019, pp. 25-35.
APA	Mansoori M, Roudi R, Abbasi A, Abolhasani M, Abdi Rad I, Shariftabrizi A, Madjd Z (2019). High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness. Experimental and Molecular Pathology, 109(), 25-35.
Chicago	Mansoori M, Roudi R, Abbasi A, Abolhasani M, Abdi Rad I, Shariftabrizi A, Madjd Z. "High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness." Experimental and Molecular Pathology 109, no. (2019): 25-35.
Harvard	Mansoori M et al. (2019) 'High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness', Experimental and Molecular Pathology, 109(), pp. 25-35.
Vancouver	Mansoori M, Roudi R, Abbasi A, Abolhasani M, Abdi Rad I, Shariftabrizi A, et al.. High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness. Experimental and Molecular Pathology. 2019;109():25-35.
BibTex	@article{ author = {Mansoori M and Roudi R and Abbasi A and Abolhasani M and Abdi Rad I and Shariftabrizi A and Madjd Z}, title = {High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness}, journal = {Experimental and Molecular Pathology}, volume = {109}, number = {}, pages = {25-35}, year = {2019} }
RIS	TY - JOUR AU - Mansoori M AU - Roudi R AU - Abbasi A AU - Abolhasani M AU - Abdi Rad I AU - Shariftabrizi A AU - Madjd Z TI - High Gd2 Expression Defines Breast Cancer Cells With Enhanced Invasiveness JO - Experimental and Molecular Pathology VL - 109 IS - SP - 25 EP - 35 PY - 2019 ER -

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