Syndecan‐1 modulates β‐integrin‐dependent and interleukin‐6‐dependent functions in breast cancer cell adhesion, migration, and resistance to irradiation

Hassan, H. E.; Greve, Burkhard; Pavão, Mauro S. G.; Kiesel, L.; Ibrahim, Sherif; Götte, Martin

doi:10.1111/febs.12111

Cited by 98 publications

(125 citation statements)

References 69 publications

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“…Modulation of a 5 b 1 integrins by syndecan-1 was also reported during focal adhesion formation and migration [18][19][20]. Interestingly, the latter pathway can either enhance or suppress these processes [18][19][20]. Further, activation of focal adhesion kinase (FAK) and Rho GTPase has been implicated in syndecan-1-mediated effects on cell migration [16,21].…”

Section: Introductionmentioning

confidence: 93%

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A transmembrane C-terminal fragment of syndecan-1 is generated by the metalloproteinase ADAM17 and promotes lung epithelial tumor cell migration and lung metastasis formation

Pasqualon

Pruessmeyer

Weidenfeld

et al. 2015

Cell. Mol. Life Sci.

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Syndecan-1 is a heparan sulfate proteoglycan expressed by endothelial and epithelial cells and involved in wound healing and tumor growth. Surface-expressed syndecan-1 undergoes proteolytic shedding leading to the release of the soluble N-terminal ectodomain from a transmembrane C-terminal fragment (tCTF). We show that the disintegrin and metalloproteinase (ADAM) 17 generates a syndecan-1 tCTF, which can then undergo further intra-membrane proteolysis by γ-secretase. Scratch-induced wound closure of cultured lung epithelial A549 tumor cells associates with increased syndecan-1 cleavage as evidenced by the release of shed syndecan-1 ectodomain and enhanced generation of the tCTF. Both wound closure and the associated syndecan-1 shedding can be suppressed by inhibition of ADAM family proteases. Cell proliferation, migration and invasion into matrigel as well as several signaling pathways implicated in these responses are suppressed by silencing of syndecan-1. These defects of syndecan-1 deficient cells can be overcome by overexpression of syndecan-1 tCTF or a corresponding tCTF of syndecan-4 but not by overexpression of a tCTF lacking the transmembrane domain. Finally, lung metastasis formation of A549 cells in SCID mice was found to be dependent on syndecan-1, and the presence of syndecan-1 tCTF was sufficient for this activity. Thus, the syndecan-1 tCTF by itself is capable of mediating critical syndecan-1-dependent functions in cell proliferation, migration, invasion and metastasis formation and therefore can replace full length syndecan-1 in the situation of increased syndecan-1 shedding during cell migration and tumor formation.

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Section: Introductionmentioning

confidence: 93%

“…In addition, syndecan-1 can act as regulator of a v b 3 and a v b 5 integrin activation [15,17]. Modulation of a 5 b 1 integrins by syndecan-1 was also reported during focal adhesion formation and migration [18][19][20]. Interestingly, the latter pathway can either enhance or suppress these processes [18][19][20].…”

Section: Introductionmentioning

confidence: 96%

A transmembrane C-terminal fragment of syndecan-1 is generated by the metalloproteinase ADAM17 and promotes lung epithelial tumor cell migration and lung metastasis formation

Pasqualon

Pruessmeyer

Weidenfeld

et al. 2015

Cell. Mol. Life Sci.

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“…Recent studies showed that sdc1 knockdown in breast cancer cells increased their migration rate on FNcoated surfaces in a manner that was dependent on a 5 b 1 -or a v -containing integrins. 66 Whether similar results would be seen if cells were grown on LN332-coated surfaces is unknown.…”

mentioning

confidence: 91%

Syndecan-1 and Its Expanding List of Contacts

Stepp

Pal‐Ghosh

Tadvalkar

et al. 2015

Advances in Wound Care

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“…As highly glycosylated, sulfated molecules and, hence, negatively charged molecules, they have a large capacity to bind to other charged molecules such as cytokines and chemokines (2) and have been implicated in the presentation of cytokines to cells (3)(4)(5) and in the activation of integrin receptors (6)(7)(8). Syndecans are the best studied class of cell surface heparan sulfate proteoglycans (9); they exist in four different forms, syndecan 1-4, all of which consist of a core protein containing an ectodomain (extracellular domain), which carries the glycosylation sites, a transmembrane domain and a cytoplasmic domain.…”

mentioning

confidence: 99%

Syndecan-1, a Cell Surface Proteoglycan, Negatively Regulates Initial Leukocyte Recruitment to the Brain across the Choroid Plexus in Murine Experimental Autoimmune Encephalomyelitis

Zhang¹,

Wu²,

Song³

et al. 2013

The Journal of Immunology

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The cell surface heparan sulfate proteoglycan, syndecan-1, has been reported to be a negative regulator of various inflammatory processes, but its precise mode of action is poorly defined. In this study, we use the murine model of the 35–55 peptide of myelin oligodendrocyte glycoprotein–induced experimental autoimmune encephalomyelitis (EAE), a T lymphocyte–mediated inflammation where the steps in disease development and recovery are well characterized, to decipher how syndecan-1 impacts on the inflammatory reaction. Syndecan-1 knockout (Sdc-1−/−) mice show enhanced disease severity and impaired recovery. The use of bone marrow chimeric mice reveals that both an immune cell and a CNS-resident source of syndecan-1 contribute to this phenotype. Epithelial cells of the choroid plexus, where initial CCL20-induced leukocyte recruitment to the brain occurs, are identified as the predominant site of syndecan-1 expression. Syndecan-1 is lost from this site during the course of EAE by shedding into the cerebrospinal fluid, which correlates with loss of epithelial cell surface–bound CCL20 and is associated with the upregulation of IL-6 expression. In Sdc-1−/− mice, early leukocyte recruitment via the choroid plexus is enhanced, and IL-6 is elevated, which collectively results in higher numbers of the disease inducing Th17 cells in the CNS, thereby contributing to enhanced disease severity. Furthermore, Sdc-1−/− mice have intrinsically elevated plasma cell numbers and higher myelin oligodendrocyte glycoprotein–specific Ab levels during EAE, which we propose contributes to impaired recovery. Our data identify the choroid plexus epithelium as a novel source of IL-6 in EAE and demonstrate that its expression negatively correlates with syndecan-1 expression at this site.

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Syndecan‐1 modulates β‐integrin‐dependent and interleukin‐6‐dependent functions in breast cancer cell adhesion, migration, and resistance to irradiation

Cited by 98 publications

References 69 publications

A transmembrane C-terminal fragment of syndecan-1 is generated by the metalloproteinase ADAM17 and promotes lung epithelial tumor cell migration and lung metastasis formation

A transmembrane C-terminal fragment of syndecan-1 is generated by the metalloproteinase ADAM17 and promotes lung epithelial tumor cell migration and lung metastasis formation

Syndecan-1 and Its Expanding List of Contacts

Syndecan-1, a Cell Surface Proteoglycan, Negatively Regulates Initial Leukocyte Recruitment to the Brain across the Choroid Plexus in Murine Experimental Autoimmune Encephalomyelitis

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