Literature DB >> 18553163

Cell surface associated alpha-L-fucose moieties modulate human breast cancer neoplastic progression.

Kun Yuan1, Catherine M Listinsky, Raj K Singh, Jay J Listinsky, Gene P Siegal.   

Abstract

Glycosylation drives critical processes important for mammalian cell-cell and cell-matrix interactions. Alpha-L-fucose (alpha-L-f) is a key monosaccharide component of oligosaccharides that has been found to be overexpressed during tumor progression. Modification of cell surface fucosylation, we hypothesized, alters tumor cell phenotype and function at the end of the neoplastic progression cascade including tumor invasion. Alpha-L-fucosidase (alpha-L-fase) is a glycosidase that specifically removes (alpha-L-f) from oligosaccharide sites. We first verified the effectiveness of the alpha-L-fase to specifically decrease the level of alpha-L-f on the cell surface of several human breast cancer cell lines and also examined the recovery time for these cells to repopulate their surfaces. To investigate the potential effect of defucosylation on tumor functions, we studied the proliferation, and invasion in vitro of human breast cancer MDA-MB-231 cells as the representative cell model. We further examined several fucose-associated molecules previously shown to be involved in tumor progression, including CD44 and CD15 (Lewis X antigen). We found that alpha-L: -fase pretreatment significantly decreased the invasive capability of breast cancer cells. Deoxyfuconojirimycin (DFJ), a specific alpha-L: -fase inhibitor, reversed this effect. After fucosidase treatment, the level of both CD15 and CD44 were found to be reduced as measured by flow cytometry. alpha-L-fase treatment, further, did not affect tumor cell proliferation in vitro under identical experimental conditions. Gelatin zymography of conditioned media from tumor cells treated with alpha-L-fase demonstrated no change in MMP-2 activity while MMP-9 was significantly reduced. In summary, fucose containing glycans were found widely distributed on the cell surface of breast cancer cells and could be effectively removed by alpha-L-fase treatment. This decreased fucosylation, in turn, was seen to impair the interaction between tumor cells and extracellular matrices, and thus affected key cell functions modulating tumor invasion. Further elucidation of the molecular pathways involved in the inhibition of tumor cell invasion may suggest a rationale for the use of glycobiologic therapeutics to deter tumor progression.

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Year:  2008        PMID: 18553163     DOI: 10.1007/s12253-008-9036-x

Source DB:  PubMed          Journal:  Pathol Oncol Res        ISSN: 1219-4956            Impact factor:   3.201


  58 in total

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  15 in total

1.  The emerging importance of α-L-fucose in human breast cancer: a review.

Authors:  Jay J Listinsky; Gene P Siegal; Catherine M Listinsky
Journal:  Am J Transl Res       Date:  2011-07-20       Impact factor: 4.060

Review 2.  Tools for mammalian glycoscience research.

Authors:  Matthew E Griffin; Linda C Hsieh-Wilson
Journal:  Cell       Date:  2022-07-08       Impact factor: 66.850

3.  Alterations in human breast cancer adhesion-motility in response to changes in cell surface glycoproteins displaying alpha-L-fucose moieties.

Authors:  Kun Yuan; Dennis Kucik; Raj K Singh; Catherine M Listinsky; Jay J Listinsky; Gene P Siegal
Journal:  Int J Oncol       Date:  2008-04       Impact factor: 5.650

4.  Comparing the Immunoexpression of FUT3 and FUT6 between Prostatic Adenocarcinoma and Benign Prostatic Hyperplasia.

Authors:  Juliana Lúcia de Albuquerque Vasconcelos; Steffany de Almeida Ferreira; Amanda Lucena Rosendo de Lima; Moacyr Jesus Barreto de Melo Rêgo; Ana Rosa Galdino Bandeira; Carmelita de Lima Bezerra Cavalcanti; Mariana Montenegro de Melo Lira; Eduardo Isidoro Carneiro Beltrão
Journal:  Acta Histochem Cytochem       Date:  2013-06-20       Impact factor: 1.938

5.  Enhancive effects of Lewis y antigen on CD44-mediated adhesion and spreading of human ovarian cancer cell line RMG-I.

Authors:  Lili Gao; Limei Yan; Bei Lin; Jian Gao; Xiuyun Liang; Yanyan Wang; Juanjuan Liu; Shulan Zhang; Masao Iwamori
Journal:  J Exp Clin Cancer Res       Date:  2011-02-07

6.  Human GMDS gene fragment hypermethylation in chronic high level of arsenic exposure with and without arsenic induced cancer.

Authors:  Sarmishtha Chanda; Uma B Dasgupta; Debendranath Guha Mazumder; Jayita Saha; Bhaskar Gupta
Journal:  Springerplus       Date:  2013-10-24

7.  Down-regulation of α-L-fucosidase 1 expression confers inferior survival for triple-negative breast cancer patients by modulating the glycosylation status of the tumor cell surface.

Authors:  Tzu-Chun Cheng; Shih-Hsin Tu; Li-Ching Chen; Ming-Yao Chen; Wen-Ye Chen; Yen-Kuang Lin; Chi-Tang Ho; Shyr-Yi Lin; Chih-Hsiung Wu; Yuan-Soon Ho
Journal:  Oncotarget       Date:  2015-08-28

8.  Human a-L-fucosidase-1 attenuates the invasive properties of thyroid cancer.

Authors:  Giancarlo Vecchio; Alessia Parascandolo; Chiara Allocca; Clara Ugolini; Fulvio Basolo; Marco Moracci; Andrea Strazzulli; Beatrice Cobucci-Ponzano; Mikko O Laukkanen; Maria Domenica Castellone; Nobuo Tsuchida
Journal:  Oncotarget       Date:  2017-04-18

9.  Proteomic identification of fucosylated haptoglobin alpha isoforms in ascitic fluids and its localization in ovarian carcinoma tissues from Mexican patients.

Authors:  Olga Lilia Garibay-Cerdenares; Verónica Ivonne Hernández-Ramírez; Juan Carlos Osorio-Trujillo; Magdalena Hernández-Ortíz; Dolores Gallardo-Rincón; David Cantú de León; Sergio Encarnación-Guevara; Julio César Villegas-Pineda; Patricia Talamás-Rohana
Journal:  J Ovarian Res       Date:  2014-02-27       Impact factor: 4.234

10.  Proteomics analysis of bladder cancer invasion: Targeting EIF3D for therapeutic intervention.

Authors:  Agnieszka Latosinska; Marika Mokou; Manousos Makridakis; William Mullen; Jerome Zoidakis; Vasiliki Lygirou; Maria Frantzi; Ioannis Katafigiotis; Konstantinos Stravodimos; Marie C Hupe; Maciej Dobrzynski; Walter Kolch; Axel S Merseburger; Harald Mischak; Maria G Roubelakis; Antonia Vlahou
Journal:  Oncotarget       Date:  2017-04-20
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