Abstract

Sialomucin complex (SMC, rat Muc4) is a unique membrane mucin composed of a mucin subunit ASGP-1 and ASGP-1 and a trans-membrane subunit ASGP-2, derived from a single gene and originally isolated from a highly metastatic ascites rat mammary adenocarcinoma. Preliminary studies suggest that Muc4 over-expression correlates with tumor progression in human breast cancers. SMC is bifunctional as well as heterodimeric. The mucin has potent anti-recognition properties, blocking cell-cell and cell-matrix adhesions and protecting transfected tumor cells from immune cell lysis. ASGP-2 has two EGF-like domains and can act as a novel intramembrane ligand for the receptor tyrosine kinase ErbB2 to potentiate the phosphorylation of the heterodimeric receptor complex ErbB2/ErbB3. Our recent studies on the role of SMC in tumor progression have shown that it can act as an anti-apoptotic agent. Finally, ASGP-1 has the potential to act as a pro-adhesive component in tumor extravasation, as it can carry the ligand SLex for selectins implicated in metastasis. This proposal is directed primarily toward understanding the roles of SMC in tumor progression. Our recent studies indicate that SMC is tightly regulated in the mammary gland, specifically by TGF beta. Our working hypothesis for this proposal is that loss of SMC regulation leads to its over-expression and potentiates mammary tumor progression. We propose experiments to test the role of SMC in tumor progression and to examine the mechanism by which SMC expression is regulated by TGF beta.
Specific aim 1 will investigate the function(s) of SMCIMuc4 in ErbB2-induced mammary tumors in vivo using over-expression by transgenic technology.
Specific aim 2 will investigate the function(s) of SMCIMuc4 in normal mammary gland and its role in early tumor progression by blocking SMC expression by retroviral transfection of a ribozyme followed by mammary tissue transplantation.
Specific aim 3 will investigate a primary mechanism for regulating SMCIMuc4 expression in normal rat mammary gland, post-translational repression of SMC processing by TGFB. The hypothesis is that signaling through the SMAD pathway contributes to regulating a protease involved in post-translational processing of SMC precursor.
Specific aim 4 will investigate the role of SMC SLex in tumor metastasis. These studies are directed toward providing the evidence for SMC/MUC4 contributions to tumor progression as a prelude to developing methods for therapeutic targeting of this component.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA052498-13
Application #
6874361
Study Section
Special Emphasis Panel (ZRG1-SSS-2 (04))
Program Officer
Sussman, Daniel J
Project Start
1991-09-30
Project End
2006-03-31
Budget Start
2005-04-01
Budget End
2006-03-31
Support Year
13
Fiscal Year
2005
Total Cost
$272,700
Indirect Cost

  Institution

Name
University of Miami School of Medicine
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
052780918
City
Miami
State
FL
Country
United States
Zip Code
33146

  Publications

Kozloski, Goldi A; Carraway, Coralie A Carothers; Carraway, Kermit L (2010) Mechanistic and signaling analysis of Muc4-ErbB2 signaling module: new insights into the mechanism of ligand-independent ErbB2 activity. J Cell Physiol 224:649-57
Lomako, Joseph; Lomako, Wieslawa M; Carothers Carraway, Coralie A et al. (2010) Regulation of the membrane mucin Muc4 in corneal epithelial cells by proteosomal degradation and TGF-beta. J Cell Physiol 223:209-14
Lomako, Wieslawa M; Lomako, Joseph; Soto, Pedro et al. (2009) TGFbeta regulation of membrane mucin Muc4 via proteosome degradation. J Cell Biochem 107:797-802
Carraway, Kermit L; Theodoropoulos, George; Kozloski, Goldi A et al. (2009) Muc4/MUC4 functions and regulation in cancer. Future Oncol 5:1631-40
Theodoropoulos, George; Carraway, Coralie A Carothers; Carraway, Kermit L (2009) MUC4 involvement in ErbB2/ErbB3 phosphorylation and signaling in response to airway cell mechanical injury. J Cell Biochem 107:112-22
Workman, Heather C; Miller, Jamie K; Ingalla, Ellen Q et al. (2009) The membrane mucin MUC4 is elevated in breast tumor lymph node metastases relative to matched primary tumors and confers aggressive properties to breast cancer cells. Breast Cancer Res 11:R70
Carraway, Kermit L; Kozloski, Goldi A (2009) Conformational changes in receptor tyrosine kinase signaling: an ErbB garden of delights. F1000 Biol Rep 1:72
Theodoropoulos, George; Carraway, Kermit L (2007) Molecular signaling in the regulation of mucins. J Cell Biochem 102:1103-16
Jonckheere, Nicolas; Vincent, Audrey; Perrais, Michael et al. (2007) The human mucin MUC4 is transcriptionally regulated by caudal-related homeobox, hepatocyte nuclear factors, forkhead box A, and GATA endodermal transcription factors in epithelial cancer cells. J Biol Chem 282:22638-50
Pino, Vanessa; Ramsauer, Victoria P; Salas, Pedro et al. (2006) Membrane mucin Muc4 induces density-dependent changes in ERK activation in mammary epithelial and tumor cells: role in reversal of contact inhibition. J Biol Chem 281:29411-20

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