Open AccessJournal Article
Tolerance and immunity to MUC1 in a human MUC1 transgenic murine model
Richard M. Tempero,Keita Morikane,Michelle L. VanLith,Sandra J. Gendler,Michael A. Hollingsworth +4 more
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TLDR
Data suggest that endogenous expression of MUC1 protein by M UC1 transgenic mice induces T-cell tolerance to stimulation by MUC2, and will facilitate the investigation of anti-MUC1 immunotherapy formulations.Abstract:
The human epithelial mucin, MUC1, is a large transmembrane glycoprotein that is expressed on most simple epithelia. It is overexpressed and aberrantly glycosylated on many human epithelial tumors, including more than 90% of human breast cancers. MUC1 is of interest as an immunotherapy target because patients with breast, ovarian, and pancreatic cancers have T lymphocytes in their tumor-draining lymph nodes that can be induced to recognize and lyse MUC1-expressing tumor cells. We have produced a transgenic mouse model that expresses the human MUC1 molecule on an inbred C57Bl/6 background to investigate the effect of endogenous expression of MUC1 on the ability of mice to generate antitumor immunity to MUC1-expressing tumors. Transgenic mice expressed the human transgene in a pattern and level consistent with that observed in humans. Transgenic mice were tolerant to stimulation by MUC1 as evidenced by the ability of MUC1-expressing tumor cells to grow in these mice, whereas MUC1-expressing cells were eliminated from wild-type mice. Moreover, transgenic mice immunized with MUC1 peptides failed to exhibit immunoglobulin class switching to the IgG subtypes. These data suggest that endogenous expression of MUC1 protein by MUC1 transgenic mice induces T-cell tolerance to stimulation by MUC1. The transgenic mice will provide a useful model to investigate the mechanisms that regulate immunological tolerance to tumor antigens and will facilitate the investigation of anti-MUC1 immunotherapy formulations.read more
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Journal ArticleDOI
MUC1, the renaissance molecule.
TL;DR: Recent discoveries that suggest that MUC1 may be a multifunctional protein, located on the surfaces of cells as a sensor of the environment, poised to signal to the interior when things go awry are highlighted.
Journal ArticleDOI
MUC1 and cancer
TL;DR: The MUC1 membrane mucin was first identified as the molecule recognised by mouse monoclonal antibodies directed to epithelial cells, and the cancers which develop from them, and its role in the immune response and in other interactions with the effector cells of the immune system is of particular interest.
Journal ArticleDOI
Immune recognition of tumor-associated mucin MUC1 is achieved by a fully synthetic aberrantly glycosylated MUC1 tripartite vaccine
Vani Lakshminarayanan,Pamela Thompson,Margreet A. Wolfert,Therese Buskas,Judy M. Bradley,Latha B. Pathangey,Cathy S. Madsen,Peter A. Cohen,Sandra J. Gendler,Geert-Jan Boons +9 more
TL;DR: The minimum requirements to consistently induce CTLs and ADCC-mediating antibodies specific for the tumor form of MUC1 are identified resulting in a therapeutic response in a mouse model of mammary cancer.
Journal ArticleDOI
Chemoenzymatically synthesized multimeric Tn/STn MUC1 glycopeptides elicit cancer-specific anti-MUC1 antibody responses and override tolerance.
Anne Louise Sørensen,Celso A. Reis,Celso A. Reis,Mads Agervig Tarp,Ulla Mandel,Kavitha Ramachandran,Vasanthi Sankaranarayanan,Tilo Schwientek,Ros Graham,Joyce Taylor-Papadimitriou,Michael A. Hollingsworth,Joy Burchell,Henrik Clausen +12 more
TL;DR: Chemoenzymatic synthesis of extended MUC1 TR glycopeptides with cancer-associated O-glycosylation using a panel of recombinant human glycosyltransferases is developed and a MAb with similar specificity as the elicited immune response was generated and shown to have the same remarkable cancer specificity.
Journal ArticleDOI
Reversal of tolerance to human MUC1 antigen in MUC1 transgenic mice immunized with fusions of dendritic and carcinoma cells
Jianlin Gong,Dongshu Chen,Masahiro Kashiwaba,Yongqing Li,Ling Chen,Hideya Takeuchi,Hui Qu,Gerald J. Rowse,Sandra J. Gendler,Donald Kufe +9 more
TL;DR: It is demonstrated that unresponsiveness to the M UC1 tumor-associated antigen is reversible by immunization with heterokaryons of dendritic cells and MUC1-positive carcinoma cells.
References
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Novel Mechanisms Underlying the Immediate and Transient Global Tolerization of Splenic Dendritic Cells after Vaccination with a Self-Antigen
Adam M. Farkas,Olivera J. Finn +1 more
TL;DR: TolerizedDCs were not refractory to maturation after stimulation with a TLR3 agonist, demonstrating that this tolerized state is not terminally differentiated and that tolerized DCs can recover their ability to induce immunity to foreign Ags.
Book ChapterDOI
Gene therapy for lung cancer.
TL;DR: Attempts to target molecular alterations in lung cancer using gene therapy techniques are reviewed, including introducing suicide genes into tumor cells, replacement of defective tumor suppressor genes, inactivating oncogenes, and immunotherapy-based approaches using gene Therapy technology.
MUC1 in the relationship between inflammation and cancer in IBD
TL;DR: It is postulate that induction of MUC1-specific immunity, including effector and regulatory T-cells, restores the balance between adaptive and innate immunity, which resolves chronic inflammation and stops progression of premalignant lesions to cancer.
Journal ArticleDOI
The National Cancer Institute's PREVENT Cancer Preclinical Drug Development Program: overview, current projects, animal models, agent development strategies, and molecular targets.
TL;DR: The PREVENT Cancer Preclinical Drug Development Program is a National Cancer Institute, Division of Cancer Prevention (NCI, DCP)-supported program whose primary goal is to bring new cancer preventive interventions through preclinical development towards clinical trials by creating partnerships between the public sector and industry.
Book ChapterDOI
Chapter 9 – tumor antigens as targets for anticancer drug development
TL;DR: The existence of tumor-specific or tumor-associated antigens, which are the molecular targets of an adaptive immune response, is now well established as mentioned in this paper, and there is substantial evidence that immune responses directed against tumor antigen can cause the regression of established tumors.