Loss of α-Dystroglycan Laminin Binding in Epithelium-derived Cancers Is Caused by Silencing of LARGE

Bernabé, Daniel Beltrán-Valero de; Inamori, Kei-ichiro; Yoshida‐Moriguchi, Takako; Weydert, Christine J.; Harper, Hollie A.; Willer, Tobias; Henry, Michael D.; Campbell, Kevin P.

doi:10.1074/jbc.c900007200

Cited by 102 publications

(113 citation statements)

References 32 publications

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“…Hence, ␣-DG-dependent migration controlled by HNK-1ST might predominate in HNK-1-negative melanomas. The unique glycan structure expressed on ␣-DG has been shown to have a close relationship to tumor-related phenotypes such as invasiveness (32,33). Previous studies reported that the IIH6 mAb-reactive glycan of ␣-DG had a suppressive effect on tumor invasion in cases of breast, prostate, and lung carcinoma (32,33), although we obtained the opposite results using melanoma cells (Figs.…”

Section: Discussionmentioning

confidence: 52%

“…It has been demonstrated that ␣-DG, especially the glycan attached to it, is involved in tumor invasiveness in various cancer types such as breast, prostate, and lung carcinomas (32,33). Because HNK-1ST associates with the modification of glycans, up-regulation of HNK-1ST expression might affect the glycosylation in cells.…”

Section: Specific Induction Of Hnk-1st Expression and Alternatementioning

confidence: 99%

“…These observations indicate that O-mannosyl modification is essential for the functional glycosylation of ␣-DG. Furthermore, altered glycosylation of ␣-DG is also implicated in epithelium-derived cancer progression, demonstrating the involvement of ␣-DG in tumorigenic phenotypes (32,33).…”

mentioning

confidence: 99%

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Human Natural Killer-1 Sulfotransferase (HNK-1ST)-induced Sulfate Transfer Regulates Laminin-binding Glycans on α-Dystroglycan

Nakagawa¹,

Manya²,

Toda³

et al. 2012

Journal of Biological Chemistry

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Background: ␣-Dystroglycan undergoes extensive glycosylation required for the interaction between ␣-dystroglycan and its ligands such as laminin. Results: HNK-1ST suppressed the glycosylation and reduced the ligand binding activity of ␣-dystroglycan. Conclusion:The sulfotransferase activity of HNK-1ST is essential for the modulation of ␣-dystroglycan. Significance: This study identifies a novel role for HNK-1ST as a regulator of the functional glycans on ␣-dystroglycan other than HNK-1 biosynthesis.

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Section: Discussionmentioning

confidence: 52%

Section: Specific Induction Of Hnk-1st Expression and Alternatementioning

confidence: 99%

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Human Natural Killer-1 Sulfotransferase (HNK-1ST)-induced Sulfate Transfer Regulates Laminin-binding Glycans on α-Dystroglycan

Nakagawa¹,

Manya²,

Toda³

et al. 2012

Journal of Biological Chemistry

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“…This situation is exemplified in studies using cancer cells. It has been reported that several malignant cancer cell types lose the laminin-binding glycan of ␣-DG due to epigenetic down-regulation of LARGE or defects in the LARGE-binding protein ␤3GnT1, raising the possibility of defects in post-phosphoryl modification of ␣-DG in those cells (31,33).…”

Section: Discussionmentioning

confidence: 99%

Absence of Post-phosphoryl Modification in Dystroglycanopathy Mouse Models and Wild-type Tissues Expressing Non-laminin Binding Form of α-Dystroglycan

Kuga

Kanagawa

Sudo

et al. 2012

Journal of Biological Chemistry

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Background:The biosynthetic pathway for the ligand-binding moiety of ␣-dystroglycan, defects in which cause dystroglycanopathy, remains unclear. Results:The phosphodiester-linked moiety on O-mannose is absent in dystroglycanopathy models and in wild-type lung and testis. Conclusion: Post-phosphoryl modification is a key determinant of the functional expression of ␣-dystroglycan as a laminin receptor. Significance: This work expands our understanding of the molecular mechanism of a unique post-translational modification.

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“…These results demonstrated antimigratory activity of laminin-binding glycans attached to ␣-DG. While we were preparing our article, a report appeared showing that downregulation of LARGE resulted in higher migration of carcinoma cells (29).…”

Section: Expression Of ␤3gnt1 Directs the Synthesis Of Laminin-bindinmentioning

confidence: 99%

Tumor suppressor function of laminin-binding α-dystroglycan requires a distinct β3- N -acetylglucosaminyltransferase

Bao

Kobayashi

Hatakeyama

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

112

159

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␣-Dystroglycan (␣-DG) represents a highly glycosylated cell surface molecule that is expressed in the epithelial cell-basement membrane (BM) interface and plays an essential role in epithelium development and tissue organization. The ␣-DG-mediated epithelial cell-BM interaction is often impaired in invasive carcinomas, yet roles and underlying mechanisms of such an impaired interaction in tumor progression remain unclear. We report here a suppressor function of laminin-binding glycans on ␣-DG in tumor progression. In aggressive prostate and breast carcinoma cell lines, lamininbinding glycans are dramatically decreased, although the amount of ␣-DG and ␤-dystroglycan is maintained. The decrease of lamininbinding glycans and consequent increased cell migration were associated with the decreased expression of ␤3-N-acetylglucosaminyltransferase-1 (␤3GnT1). Forced expression of ␤3GnT1 in aggressive cancer cells restored the laminin-binding glycans and decreased tumor formation. ␤3GnT1 was found to be required for laminin-binding glycan synthesis through formation of a complex with LARGE, thus regulating the function of LARGE. Interaction of the laminin-binding glycans with laminin and other adhesive molecules in BM attenuates tumor cell migratory potential by antagonizing ERK/AKT phosphorylation induced by the components in the ECM. These results identify a previously undescribed role of carbohydrate-dependent cell-BM interaction in tumor suppression and its control by ␤3GnT1 and LARGE.glycosylation ͉ cell adhesion ͉ basement membrane ͉ carcinoma I nteraction of epithelial cells with basement membrane (BM) is mediated by cell adhesion molecules, which operate at the interface of epithelial cell-ECM and regulate cell growth, motility, and differentiation by integrating signals from ECM or soluble factors (1-3). One of the most important epithelial cell-BM interactions is mediated by ␣-dystroglycan (␣-DG) on epithelial cells (4).␣-DG is a cell surface receptor for several major BM proteins, including laminin, perlecan, and agrin. A laminin G-like domain in all these glycoproteins binds to a unique glycan structure attached to ␣-DG, and this interaction has been shown to be critical in assembling BM (5, 6). This unique glycan structure is referred to as laminin-binding glycans hereafter. ␣-DG is not attached directly to the plasma membrane but is bound to it through attachment to the transmembrane protein ␤-dystroglycan (␤-DG), which binds to the cytoplasmic protein dystrophin, which, in turn, binds to the actin cytoskeleton and many adaptor molecules involved in cellular signaling (4,5).␣-DG is highly glycosylated and contains both N-linked glycans and mucin type O-glycans. The mucin type O-glycans are clustered in a mucin-like domain at the N-terminal of mature ␣-DG, which includes unique O-mannosyl glycans and sialic acid ␣233Gal␤134GlcNAc␤132Man␣13Ser/Thr (7). Defects in glycosylation of the O-mannosyl glycans have been shown to cause muscular dystrophy (8). So far, 7 glycosyltransferases or glycosyltransferase-like ...

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Loss of α-Dystroglycan Laminin Binding in Epithelium-derived Cancers Is Caused by Silencing of LARGE

Cited by 102 publications

References 32 publications

Human Natural Killer-1 Sulfotransferase (HNK-1ST)-induced Sulfate Transfer Regulates Laminin-binding Glycans on α-Dystroglycan

Human Natural Killer-1 Sulfotransferase (HNK-1ST)-induced Sulfate Transfer Regulates Laminin-binding Glycans on α-Dystroglycan

Absence of Post-phosphoryl Modification in Dystroglycanopathy Mouse Models and Wild-type Tissues Expressing Non-laminin Binding Form of α-Dystroglycan

Tumor suppressor function of laminin-binding α-dystroglycan requires a distinct β3- N -acetylglucosaminyltransferase

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