Your search keyword '"Kentaro, Hozumi"' showing total 5 results

1. The Lutheran/Basal Cell Adhesion Molecule Promotes Tumor Cell Migration by Modulating Integrin-mediated Cell Attachment to Laminin-511 Protein

Author

Kentaro Hozumi, Ryo Sudo, Jeffrey H. Miner, Motoyoshi Nomizu, Takaho Ogawa, Fumihiko Katagiri, Yamato Kikkawa, and Yuji Yamada

Subjects

Integrins, Cell, Integrin, Glycobiology and Extracellular Matrices, Biology, Biochemistry, Basement Membrane, Extracellular matrix, Mice, Cell Movement, Laminin, Cell Line, Tumor, Neoplasms, Cell Adhesion, medicine, Animals, Humans, Cell adhesion, Cell Shape, Molecular Biology, Integrin binding, Mice, Knockout, Membrane Glycoproteins, Cell adhesion molecule, Cell migration, Cell Biology, Lutheran Blood-Group System, Neoplasm Proteins, Cell biology, HEK293 Cells, medicine.anatomical_structure, biology.protein, Cell Adhesion Molecules

Abstract

Cell-matrix interactions are critical for tumor cell migration. Lutheran (Lu), also known as basal cell adhesion molecule (B-CAM), competes with integrins for binding to laminin α5, a subunit of LM-511, a major component of basement membranes. Here we show that the preferential binding of Lu/B-CAM to laminin α5 promotes tumor cell migration. The attachment of Lu/B-CAM transfectants to LM-511 was slightly weaker than that of control cells, and this was because Lu/B-CAM disturbed integrin binding to laminin α5. Lu/B-CAM induced a spindle cell shape with pseudopods and promoted cell migration on LM-511. In addition, blocking with an anti-Lu/B-CAM antibody led to a flat cell shape and inhibited migration on LM-511, similar to the effects of an activating integrin β1 antibody. We conclude that tumor cell migration on LM-511 requires that Lu/B-CAM competitively modulates cell attachment through integrins. We suggest that this competitive interaction is involved in a balance between static and migratory cell behaviors.

Published

2013

2. Identification of Cell Adhesive Sequences in the N-terminal Region of the Laminin α2 Chain

Author

Kentaro Hozumi, Yamato Kikkawa, Yuji Yamada, Takemitsu Hayashi, Masaya Ishikawa, Fumihiko Katagiri, and Motoyoshi Nomizu

Subjects

Integrin, Glycobiology and Extracellular Matrices, Peptide, Biology, PC12 Cells, Peptide Mapping, Biochemistry, Antibodies, Sepharose, Mice, Protein structure, Laminin, Cell Adhesion, Animals, Humans, Amino Acid Sequence, Binding site, Cell adhesion, Molecular Biology, Peptide sequence, chemistry.chemical_classification, Cell Biology, Protein Structure, Tertiary, Rats, chemistry, biology.protein, Integrin alpha2beta1, Peptides

Abstract

The laminin α2 chain is specifically expressed in the basement membrane surrounding muscle and nerve. We screened biologically active sequences in the mouse laminin N-terminal region of α2 chain using 216 soluble peptides and three recombinant proteins (rec-a2LN, rec-a2LN+, and rec-a2N) by both the peptide- or protein-coated plate and the peptide-conjugated Sepharose bead assays. Ten peptides showed cell attachment activity in the plate assay, and 8 peptides were active in the bead assay. Seven peptides were active in the both assays. Five peptides promoted neurite outgrowth with PC12 cells. To clarify the cellular receptors, we examined the effects of heparin and EDTA on cell attachment to 11 active peptides. Heparin inhibited cell attachment to 10 peptides, and EDTA significantly affected only A2-8 peptide (YHYVTITLDLQQ, mouse laminin α2 chain, 117-128)-mediated cell attachment. Cell attachment to A2-8 was also specifically inhibited by anti-integrin β1 and anti-integrin α2β1 antibodies. These results suggest that A2-8 promotes an integrin α2β1-mediated cell attachment. The rec-a2LN protein, containing the A2-8 sequence, bound to integrin α2β1 and cell attachment to rec-a2LN was inhibited by A2-8 peptide. Further, alanine substitution analysis of both the A2-8 peptide and the rec-a2LN+ protein revealed that the amino acids Ile-122, Leu-124, and Asp-125 were involved in integrin α2β1-mediated cell attachment, suggesting that the A2-8 site plays a functional role as an integrin α2β1 binding site in the LN module. These active peptides may provide new insights on the molecular mechanism of laminin-receptor interactions.

Published

2012

3. TM14 Is a New Member of the Fibulin Family (Fibulin-7) That Interacts with Extracellular Matrix Molecules and Is Active for Cell Binding

Author

Yoshihiko Yamada, Susana de Vega, Takashi Nakamura, Kentaro Hozumi, Larry W. Fisher, Tsutomu Iwamoto, Satoshi Fukumoto, and Dianalee A. McKnight

Subjects

DNA, Complementary, Glycosylation, Mesenchyme, Integrin, Protein Sorting Signals, Biochemistry, Mice, stomatognathic system, Dentin sialophosphoprotein, Chlorocebus aethiops, Cell Adhesion, medicine, Animals, Humans, RNA, Messenger, Molecular Biology, In Situ Hybridization, Odontoblasts, biology, Cell adhesion molecule, Chemistry, Integrin beta1, Calcium-Binding Proteins, Gene Expression Regulation, Developmental, Cell Differentiation, Cell Biology, Molecular biology, Recombinant Proteins, Extracellular Matrix, Protein Structure, Tertiary, Fibulin, Fibronectin, stomatognathic diseases, Odontoblast, medicine.anatomical_structure, Organ Specificity, Multigene Family, COS Cells, Dentin, NIH 3T3 Cells, biology.protein, Dentin mineralization, Tooth, HeLa Cells, Protein Modification, Translational

Abstract

We identified a new extracellular protein, TM14, by differential hybridization using mouse tooth germ cDNA microarrays. TM14 cDNA encodes 440 amino acids containing a signal peptide. The protein contains 3 EGF modules at the center, a C-terminal domain homologous to the fibulin module, and a unique Sushi domain at the N terminus. In situ hybridization revealed that TM14 mRNA was expressed by preodontoblasts and odontoblasts in developing teeth. TM14 mRNA was also expressed in cartilage, hair follicles, and extraembryonic tissues of the placenta. Immunostaining revealed that TM14 was localized at the apical pericellular regions of preodontoblasts. When the dentin matrix was fully formed and dentin mineralization occurred, TM14 was present in the predentin matrix and along the dentinal tubules. We found that the recombinant TM14 protein was glycosylated with N-linked oligosaccharides and interacted with heparin, fibronectin, fibulin-1, and dentin sialophosphoprotein. We also found that TM14 preferentially bound dental mesenchyme cells and odontoblasts but not dental epithelial cells or nondental cells such as HeLa, COS7, or NIH3T3 cells. Heparin, EDTA, and anti-integrin beta1 antibody inhibited TM14 binding to dental mesenchyme cells, suggesting that both a heparan sulfate-containing cell surface receptor and an integrin are involved in TM14 cell binding. Our findings indicate that TM14 is a cell adhesion molecule that interacts with extracellular matrix molecules in teeth and suggest that TM14 plays important roles in both the differentiation and maintenance of odontoblasts as well as in dentin formation. Because of its protein characteristics, TM14 can be classified as a new member of the fibulin family: fibulin-7.

Published

2007

4. Laminin α1 Chain LG4 Module Promotes Cell Attachment through Syndecans and Cell Spreading through Integrin α2β1

Author

Motoyoshi Nomizu, Yoshihiko Yamada, Kentaro Hozumi, Nobuharu Suzuki, and Peter K. Nielsen

Subjects

Male, Syndecans, Integrin, Biology, Biochemistry, Cell Line, Syndecan 1, Mice, Cell Movement, Laminin, Heterotrimeric G protein, Cell Adhesion, medicine, Animals, Humans, Binding site, Cell adhesion, Fibroblast, Molecular Biology, Cells, Cultured, Skin, Alanine, Binding Sites, Heparin, Epithelial Cells, Cell Biology, Fibroblasts, Molecular biology, Recombinant Proteins, medicine.anatomical_structure, Amino Acid Substitution, Fluorescent Antibody Technique, Direct, Cell culture, Mutagenesis, Site-Directed, biology.protein, Integrin alpha2beta1

Abstract

The laminin alpha1 chain is a subunit of laminin-1, a heterotrimeric basement membrane protein. The LG4-5 module at the C terminus of laminin alpha1 contains major binding sites for heparin, sulfatide, and alpha-dystroglycan and plays a critical role in early embryonic development. We previously identified active synthetic peptides AG73 and EF-1 from the sequence of laminin alpha1 LG4 for binding to syndecan and integrin alpha2beta1, respectively. However, their activity and functional relationship within the laminin-1 and LG4 as well as the functional relation between these sites and alpha-dystroglycan binding sites in LG4 are not clear. To address these questions, we created mutant recombinant LG4 proteins containing alanine substitutions within the AG73 (M1), EF-1 (M2, M3), and alpha-dystroglycan binding sites (M4, M5) and analyzed their activities. We found that recombinant proteins rec-M1 and rec-M5, containing mutations within M1 and M5, respectively, did not bind heparin or lymphoid cell lines expressing syndecans. These results suggest that LG4 binds to heparin and syndecans through M1 and M5. Rec-M1 and rec-M5 reduced fibroblast attachment, whereas mutant rec-M2 and rec-M3 retained cell attachment activity but did not promote cell spreading. Fibroblast attachment to rec-LG4 was inhibited by heparin but not by integrin antibodies. Spreading of fibroblasts on rec-LG4 was inhibited by anti-integrin alpha2 and beta1 but not by anti-integrin alpha1 and alpha6. These results suggest that the M1 and M5 sites are necessary for cell attachment on LG4 through syndecans and that the EF-1 site is for cell spreading activity through integrin alpha2beta1. In contrast, laminin-1-mediated fibroblast attachment and spreading were not inhibited by heparin or anti-integrin alpha2. Our findings indicate that LG4 has a unique function distinct from laminin-1 and suggest that laminin alpha1 LG4-5 may also be produced by a proteolytic cleavage in certain tissues where it exerts its activity.

Published

2006

5. The Lutheran/Basal Cell Adhesion Molecule Promotes Tumor Cell Migration by Modulating Integrin-mediated Cell Attachment to Laminin-511 Protein.

Author

Yamato Kikkawa, Takaho Ogawa, Ryo Sudo, Yuji Yamada, Fumihiko Katagiri, Kentaro Hozumi, Motoyoshi Nomizu, and Miner, Jeffrey H.

Subjects

*CELL-matrix adhesions, *CELL migration, *CANCER cells, *LAMININS, *INTEGRINS

Abstract

Cell-matrix interactions are critical for tumor cell migration. Lutheran (Lu), also known as basal cell adhesion molecule (B-CAM), competes with integrins for binding to laminin α5, a subunit of LM-511, a major component of basement membranes. Here we show that the preferential binding of Lu/B-CAM to laminin α5 promotes tumor cell migration. The attachment of Lu/B-CAM transfectants to LM-511 was slightly weaker than that of control cells, and this was because Lu/B-CAM disturbed integrin binding to laminin α5. Lu/B-CAM induced a spindle cell shape with pseudopods and promoted cell migration on LM-511. In addition, blocking with an anti-Lu/B-CAM antibody led to a flat cell shape and inhibited migration on LM-511, similar to the effects of an activating integrin β1 anti- body. We conclude that tumor cell migration on LM-511 requires that Lu/B-CAM competitively modulates cell attachment through integrins. We suggest that this competitive interaction is involved in a balance between static and migratory cell behaviors. [ABSTRACT FROM AUTHOR]

Published

2013