Expression and Significance of CCR7 Protein and VEGF-D Protein in Progression of Breast Cancer_CHINESE JOURNAL OF BASES AND CLINICS IN GENERAL SURGERY

Authors：

 LIANGXiao-qin ^1,2 ,  SUQin-jun ¹

1. 1.Department of Pathology, Lanzhou General Hospital of Lanzhou Military Area Command, Lanzhou 730050, Gansu Province, China;
2. 2.Department of Pathology, Gansu Provincal Hospital, Lanzhou 730000, Gansu Province, China;

Corresponding author：

SUQin-jun, Email: 595437167@qq.com

Keywords：

Breast cancer; CCR chemokine receptor-7; Vascular endothelial growth factor-D; D2-40; Lymphatic microvessel density; Immunohistochemistry

DOI：

10.7507/1007-9424.20160190

Video：

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Objective To study the expression and significance of CCR chemokine receptor-7 (CCR7) protein and vascular endothelial growth factor-D (VEGF-D) protein in the progression of breast cancer, including normal breast tissue, slight and moderate atypical hyperplasia, severe atypical hyperplasia and intraductal carcinoma in situ, as well as invasive ductal carcinoma. Methods Immunohistochemistry was used to detect the expression of CCR7 and VEGF-D protein in the nomal breast tissue (n=20), slight and moderate ductal atypical hyperplasia tissue (n=20), severe atypical hyperplasia and intraductal carcinoma in situ tissue, as well as invasive ductal breast carcinoma tissue (n=73). In addition, the D2-40 staining was also used to determine lymphatic microvessel density (LMVD). Meanwhile, the relationship between the expression of the two kinds of protein and clinicopathological factors/LMVD was analyzed by statistical analysis in breast cancer, and the correlation between expression of CCR7 protein and expression of VEGF-D protein was analyzed too. Results ①The positive rates of CCR7 protein (χ ² =23.905，P<0.050) and VEGF-D protein (χ ² =22.349，P<0.050) were gradually increased in the normal breast tissue group 〔CCR7 protein: 0 (0/20), VEGF-D protein: 5.0% (1/20)〕, slight and moderate atypical hyperplasia group 〔CCR7 protein: 5.0% (1/20), VEGF-D protein: 20.0% (4/20)〕, severe atypical hyperplasia and intraductal carcinoma in situ group 〔CCR7 protein: 30.0% (6/20), VEGF-D protein: 40.0% (8/20)〕, and invasive ductal carcinoma group 〔CCR7 protein: 47.9% (35/73), VEGF-D protein: 57.5% (42/73)〕. ②The LMVD value gradually increased in normal breast tissue group (2.00±1.02), slight and moderate atypical hyperplasia group (6.70± 3.48), severe atypical hyperplasia and intraductal carcinoma in situ group (9.01±2.13), as well as invasive ductal carcinoma group (16.32±4.07), there was significant difference between any 2 groups (P<0.050). ③The expressions of CCR7 protein and VEGF-D protein were correlated with clinical staging, histological grading, lymph node metastasis, and expression of human epidermal growth factor receptor-2 (HER-2) protein in patients with breast cancer (P<0.050), the higher positive rates of CCR7 and VEGF-D protein occurred in patients with higher histological grading, later clinical staging of Ⅲ+Ⅳ (compared with staging of Ⅰ+Ⅱ), lymph node metastasis (compared with no lymph node metastasis), and positive expression of HER-2 protein (compared with negative expression of HER-2 protein). The result indicated that LMVD value was related with expression of VEGF-D protein (r=0.623, P<0.010) in patients with breast cancer, but there was no correlation with expression of CCR7 protein (r=-0.303, P>0.050). Furthermore, there was weak positive correlation between expression of CCR7 protein and expression of VEGF-D protein in breast cancer (r=0.112, P<0.050). Conclusion The results strongly suggest that the expression levels of the VEGF-D protein and CCR7 protein indicate the potential of translation some extent, and they play an important role in the progression of breast cancer.

Citation： LIANGXiao-qin, SUQin-jun. Expression and Significance of CCR7 Protein and VEGF-D Protein in Progression of Breast Cancer. CHINESE JOURNAL OF BASES AND CLINICS IN GENERAL SURGERY, 2016, 23(6): 715-721. doi: 10.7507/1007-9424.20160190 Copy

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3.	Keeley EC, Mehrad B, Strieter RM. Chemokines as mediators of neovascularization. Arterioscler Thromb Vasc Biol , 2008, 28(11): 1928-1936.
4.	Ben-Baruch A. Organ selectivity in metastasis: regulation by chemokines and their receptors. Clin Exp Metastasis , 2008, 25(4): 345-356.
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15.	Shimizu M, Saitoh Y, Itoh H. Immunohistochemical staining of Ha-ras oncogene product in normal, benign, and malignant human pancreatic tissues. Hum Pathol , 1990, 21(6): 607-612.
16.	Weidner N. Intratumor microvessel density as a prognostic factor in cancer. Am J Pathol , 1995, 147(1): 9-19.
17.	Raman D, Baugher PJ, Thu YM, et al . Role of chemokines in tumor growth. Cancer Lett , 2007, 256(2): 137-165.
18.	Zlotnik A. Chemokines and cancer. Int J Cancer , 2006, 11(9): 2026-2029.
19.	Malietzis G, Lee GH, Bernardo D, et al . The prognostic significance and relationship with body composition of CCR7-positive cells in colorectal cancer. J Surg Oncol , 2015, 112(1): 86-92.
20.	Takeuchi H, Fujimoto A, Tanaka M, et al . CCL21 chemokine regulates chemokine receptor CCR7 bearing malignant melanoma cells. Clin Cancer Res , 2004, 10(7): 2351-2358.
21.	孙仁虎, 王国斌, 李疆, 等. CCL21在人结肠癌SW480细胞侵袭过程中的作用. 癌症, 2009, 28(7): 708-713.
22.	朱旬, 甄林林, 郑伟, 等. 趋化因子受体CCR7在乳腺癌淋巴结转移中的作用. 第四军医大学学报, 2006, 27(13): 1205-1207.
23.	Majumder M, Tutunea-Fatan E, Xin X, et al . Co-expression of α9β1 integrin and VEGF-D confers lymphatic metastatic ability to a human breast cancer cell line MDA-MB-468LN. PLoS One , 2012, 7(4): e35094.
24.	Herrington CS, Worsham M, Southern SA, et al . Loss of sequences on the short arm of chromosome 17 is a late event in squamous carcinoma of the cervix. Mol Pathol , 2001, 54(3): 160-164.
25.	Thelen A, Scholz A, Benckert C, et al . VEGF-D promotes tumor growth and lymphatic spread in a mouse model of hepatocellular carcinoma. Int J Cancer , 2008, 122(11): 2471-2481.
26.	Onogawa S, Kitadai Y, Tanaka S, et al . Expression of VEGF-C and VEGF-D at the invasive edge correlates with lymph node metastasis and prognosis of patients with colorectal carcinoma. Cancer Sci , 2004, 95(1): 32-39.
27.	Stacker SA, Caesar C, Baldwin ME, et al . VEGF-D promotes the metastatic spread of tumor cells via the lymphatics. Nat Med , 2001, 7(2): 186-191.
28.	Roy H, Bhardwaj S, Yla-Herttuala S. Biology of vascular endothelial growth factors. FEBS Lett , 2006, 580(12): 2879-2887.
29.	Veikkola T, Jussila L, Makinen T, et al . Signalling via vascular endothelial growth factor receptor-3 is sufficient for lymphangiogenesis in transgenic mice. EMBO J , 2001, 20(6): 1223-1231.

1. Mantovani A, Bonecchi R, Locati M. Tuning inflammation and immunity by chemokine sequestration: decoys and more. Nat Rev Immunol , 2006, 6(12): 907-918.
2. Balkwill F. Cancer and the chemokine network. Nat Rev Cancer , 2004, 4(7): 540-550.
3. Keeley EC, Mehrad B, Strieter RM. Chemokines as mediators of neovascularization. Arterioscler Thromb Vasc Biol , 2008, 28(11): 1928-1936.
4. Ben-Baruch A. Organ selectivity in metastasis: regulation by chemokines and their receptors. Clin Exp Metastasis , 2008, 25(4): 345-356.
5. Garin A, Proudfoot AE. Chemokines as targets for therapy. Exp Cell Res , 2011, 317(5): 602-612.
6. Mishra P, Banerjee D, Ben-Baruch A. Chemokines at the crossroads of tumor-fibroblast interactions that promote malignancy. J Leukoc Biol , 2011, 89(1): 31-39.
7. Müller A, Homey B, Soto H, et al . Involvement of chemokine receptors in breast cancer metastasis. Nature , 2001, 410(6824): 50-56.
8. Niki T, Iba S, Tokunou M, et al . Expression of vascular endothelial growth factors A, B, C, and D and their relationships to lymph node status in lung adenocarcinoma. Clin Cancer Res , 2000, 6(6): 2431-2439.
9. Koch S, Claesson-Welsh L. Signal transduction by vascular endothelial growth factor receptors. Cold Spring Harb Perspect Med , 2012, 2(7): a006502.
10. Chung AS, Ferrara N. Developmental and pathological angiogenesis. Annu Rev Cell Dev Biol , 2011, 27: 563-584.
11. Lakhani SR, Ellis IO, Schnitt SJ, et al. WHO classification of tumours of the breast. World Health Organization classification of tumours. 4th ed. Lyon: L ARC Press, 2012: 29-31.
12. 赫尔曼尼克, 杨勇. 国际癌联盟(UICC)恶性肿瘤TNM分期图谱. 北京: 科学出版社, 1990: 201-212.
13. Liu Y, Ji R, Li J, et al . Correlation effect of EGFR and CXCR4 and CCR7 chemokine receptors in predicting breast cancer metastasis and prognosis. J Exp Clin Cancer Res , 2010, 29(1): 16-25.
14. Zhao YC, Ni XJ, Li Y, et al . Peritumoral lymphangiogenesis induced by vascular endothelial growth factor C and D promotes lymph node metastasis in breast cancer patients. World J Surg Oncol , 2012, 20(10): 165-174.
15. Shimizu M, Saitoh Y, Itoh H. Immunohistochemical staining of Ha-ras oncogene product in normal, benign, and malignant human pancreatic tissues. Hum Pathol , 1990, 21(6): 607-612.
16. Weidner N. Intratumor microvessel density as a prognostic factor in cancer. Am J Pathol , 1995, 147(1): 9-19.
17. Raman D, Baugher PJ, Thu YM, et al . Role of chemokines in tumor growth. Cancer Lett , 2007, 256(2): 137-165.
18. Zlotnik A. Chemokines and cancer. Int J Cancer , 2006, 11(9): 2026-2029.
19. Malietzis G, Lee GH, Bernardo D, et al . The prognostic significance and relationship with body composition of CCR7-positive cells in colorectal cancer. J Surg Oncol , 2015, 112(1): 86-92.
20. Takeuchi H, Fujimoto A, Tanaka M, et al . CCL21 chemokine regulates chemokine receptor CCR7 bearing malignant melanoma cells. Clin Cancer Res , 2004, 10(7): 2351-2358.
21. 孙仁虎, 王国斌, 李疆, 等. CCL21在人结肠癌SW480细胞侵袭过程中的作用. 癌症, 2009, 28(7): 708-713.
22. 朱旬, 甄林林, 郑伟, 等. 趋化因子受体CCR7在乳腺癌淋巴结转移中的作用. 第四军医大学学报, 2006, 27(13): 1205-1207.
23. Majumder M, Tutunea-Fatan E, Xin X, et al . Co-expression of α9β1 integrin and VEGF-D confers lymphatic metastatic ability to a human breast cancer cell line MDA-MB-468LN. PLoS One , 2012, 7(4): e35094.
24. Herrington CS, Worsham M, Southern SA, et al . Loss of sequences on the short arm of chromosome 17 is a late event in squamous carcinoma of the cervix. Mol Pathol , 2001, 54(3): 160-164.
25. Thelen A, Scholz A, Benckert C, et al . VEGF-D promotes tumor growth and lymphatic spread in a mouse model of hepatocellular carcinoma. Int J Cancer , 2008, 122(11): 2471-2481.
26. Onogawa S, Kitadai Y, Tanaka S, et al . Expression of VEGF-C and VEGF-D at the invasive edge correlates with lymph node metastasis and prognosis of patients with colorectal carcinoma. Cancer Sci , 2004, 95(1): 32-39.
27. Stacker SA, Caesar C, Baldwin ME, et al . VEGF-D promotes the metastatic spread of tumor cells via the lymphatics. Nat Med , 2001, 7(2): 186-191.
28. Roy H, Bhardwaj S, Yla-Herttuala S. Biology of vascular endothelial growth factors. FEBS Lett , 2006, 580(12): 2879-2887.
29. Veikkola T, Jussila L, Makinen T, et al . Signalling via vascular endothelial growth factor receptor-3 is sufficient for lymphangiogenesis in transgenic mice. EMBO J , 2001, 20(6): 1223-1231.

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Expression and Significance of CCR7 Protein and VEGF-D Protein in Progression of Breast Cancer

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