Abstract

Breast cancer is the most prevalent cancer type (~1,383,500 new cases/year), the leading cause of cancer-associated death among woman worldwide (~458,400 death/year), and the 2nd most lethal cancer in the United States. One of the unforeseen consequences of mammography is the marked increase in detection of ductal carcinoma in situ (DCIS) and early-stage breast cancer, resulting in the overtreatment for such cancers. It is important for the accurate prediction and understanding the cause of relapse, which is vital for tailoring chemotherapy for early breast-cancer patients. Using a systems approach, we identified CD177 as an excellent predictor for breast-cancer relapse using a published meta-dataset including 3554 patient specimens. CD177 was initially studied in neutrophils and its function in cancer progression and relapse is unknown. Here we use various approaches to study the role of CD177 in breast-cancer development and metastasis, and try to understand the molecular mechanism of how CD177 regulates such process. We identified that CD177 sequesters beta-catenin to the plasma membrane of cells and prevents beta-catenin from activation. beta-catenin is a protein with several roles, the most important ones being a structural protein for adherens junctions and being an important signaling molecule to mediate WNT signaling pathway. The latter is known to be critically involved in different stages of breast-cancer development. Since CD177 is an extracellular protein and linked to plasma membrane via modification, we hypothesize that CD177 indirectly interacts with intracellular beta-catenin via transmembrane proteins. As such, we found a protein complex that mediates the sequestration of beta-catenin to the plasma membrane, a similar process as the recruitment and sequestration of beta-catenin to adherens junctions. We propose to examine the molecular mechanism how this sequestration happens in cells and during cancer development. Here are specific aims in this study:
Aim 1 : Examine the molecular mechanism how CD177-STX4-STXBP2 protein complex regulate ?-Catenin.
Aim 2 : Determine the role of CD177 in breast-cancer development. In addition to the proposed aims, we identified that the CD177-STX4-STXBP2 gene signature can predict metastasis-free survival, highlighting the potential to be developed as a prediction tool for breast cancer relapse and metastasis. Overall, we expect to understand how CD177 suppresses tumor growth and/or relapse/metastasis. The positive impact is the identification of a novel CD177-STXBP2-STX4 protein complex in controlling ?-Catenin-mediated biological functions and in breast-cancer biology. We add a novel arm of regulatory mechanism for WNT/?-Cat activation in the context of breast-cancer progression.

Public Health Relevance

The proposed research aims to establish CD177 as a novel breast-cancer suppressor. We identified CD177 as an excellent predictor for relapse free survival in patients and a suppressor for breast-cancer growth and metastasis. CD177 forms a functions complex with syntaxin 4 and its binding protein STXBP2, together to sequester beta-catenin to the plasma membrane and prevent its activation by WNT signaling.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA203834-02
Application #
9241393
Study Section
Tumor Progression and Metastasis Study Section (TPM)
Program Officer
Yassin, Rihab R
Project Start
2016-07-01
Project End
2021-06-30
Budget Start
2017-07-01
Budget End
2018-06-30
Support Year
2
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
University of Iowa
Department
Pathology
Type
Schools of Medicine
DUNS #
062761671
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Kolb, Ryan; Kluz, Paige; Tan, Zhen Wei et al. (2018) Obesity-associated inflammation promotes angiogenesis and breast cancer via angiopoietin-like 4. Oncogene :
Borcherding, Nicholas; Bormann, Nicholas L; Voigt, Andrew P et al. (2018) TRGAted: A web tool for survival analysis using protein data in the Cancer Genome Atlas. F1000Res 7:1235
Liu, Q; Kulak, M V; Borcherding, N et al. (2018) A novel HER2 gene body enhancer contributes to HER2 expression. Oncogene 37:687-694
Borcherding, Nicholas; Cole, Kimberly; Kluz, Paige et al. (2018) Re-Evaluating E-Cadherin and ?-Catenin: A Pan-Cancer Proteomic Approach with an Emphasis on Breast Cancer. Am J Pathol 188:1910-1920
Borcherding, Nicholas; Kolb, Ryan; Gullicksrud, Jodi et al. (2018) Keeping Tumors in Check: A Mechanistic Review of Clinical Response and Resistance to Immune Checkpoint Blockade in Cancer. J Mol Biol 430:2014-2029
Yang, Jiping; Li, Jingyi; Suzuki, Keiichiro et al. (2017) Genetic enhancement in cultured human adult stem cells conferred by a single nucleotide recoding. Cell Res 27:1178-1181
Shao, Peng; Liu, Qi; Maina, Peterson Kariuki et al. (2017) Histone demethylase PHF8 promotes epithelial to mesenchymal transition and breast tumorigenesis. Nucleic Acids Res 45:1687-1702
Ren, Ruotong; Deng, Liping; Xue, Yanhong et al. (2017) Visualization of aging-associated chromatin alterations with an engineered TALE system. Cell Res 27:483-504
Janowski, Ann M; Colegio, Oscar R; Hornick, Emma E et al. (2016) NLRC4 suppresses melanoma tumor progression independently of inflammasome activation. J Clin Invest 126:3917-3928
Yuan, Fang; Kolb, Ryan; Pandey, Gaurav et al. (2016) Involvement of the NLRC4-Inflammasome in Diabetic Nephropathy. PLoS One 11:e0164135

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