Your search keyword '"Integrin beta1 physiology"' showing total 33 results

1. Talin-Dependent Integrin Activation Regulates VE-Cadherin Localization and Endothelial Cell Barrier Function.

Author

Pulous FE, Grimsley-Myers CM, Kansal S, Kowalczyk AP, and Petrich BG

Subjects

Animals, Antigens, CD analysis, Cadherins analysis, Female, Human Umbilical Vein Endothelial Cells physiology, Humans, Intercellular Junctions metabolism, Male, Mice, Antigens, CD physiology, Cadherins physiology, Endothelial Cells physiology, Integrin beta1 physiology, Talin physiology

Abstract

Rationale: Endothelial barrier function depends on the proper localization and function of the adherens junction protein VE (vascular endothelial)-cadherin. Previous studies have suggested a functional relationship between integrin-mediated adhesion complexes and VE-cadherin yet the underlying molecular links are unclear. Binding of the cytoskeletal adaptor protein talin to the β-integrin cytoplasmic domain is a key final step in regulating the affinity of integrins for extracellular ligands (activation) but the role of integrin activation in VE-cadherin mediated endothelial barrier function is unknown., Objective: To test the requirement of talin-dependent activation of β1 integrin in VE-cadherin organization and endothelial cell (EC) barrier function., Methods and Results: EC-specific deletion of talin in adult mice resulted in impaired stability of intestinal microvascular blood vessels, hemorrhage, and death. Talin-deficient endothelium showed altered VE-cadherin organization at EC junctions in vivo. shRNA (short hairpin RNA)-mediated knockdown of talin1 expression in cultured ECs led to increased radial actin stress fibers, increased adherens junction width and increased endothelial monolayer permeability measured by electrical cell-substrate impedance sensing. Restoring β1-integrin activation in talin-deficient cells with a β1-integrin activating antibody normalized both VE-cadherin organization and EC barrier function. In addition, VE-cadherin organization was normalized by reexpression of talin or integrin activating talin head domain but not a talin head domain mutant that is selectively deficient in activating integrins., Conclusions: Talin-dependent activation of EC β1-integrin stabilizes VE-cadherin at endothelial junctions and promotes endothelial barrier function.

Published

2019

2. In vivo cleaved CDCP1 promotes early tumor dissemination via complexing with activated β1 integrin and induction of FAK/PI3K/Akt motility signaling.

Author

Casar B, Rimann I, Kato H, Shattil SJ, Quigley JP, and Deryugina EI

Subjects

Animals, Antigens, Neoplasm, Cell Line, Tumor, Cell Movement, Chick Embryo, Endothelial Cells pathology, Humans, Male, Mice, Neoplasm Invasiveness, Neoplasm Metastasis, Phosphorylation, Serine Proteases physiology, Antigens, CD physiology, Cell Adhesion Molecules physiology, Focal Adhesion Kinase 1 physiology, Integrin beta1 physiology, Neoplasm Proteins physiology, Phosphatidylinositol 3-Kinases physiology, Prostatic Neoplasms pathology, Proto-Oncogene Proteins c-akt physiology, Signal Transduction physiology

Abstract

Specific cleavage of the transmembrane molecule, CUB domain-containing protein-1 (CDCP1), by plasmin-like serine proteases induces outside-in signal transduction that facilitates early stages of spontaneous metastasis leading to tumor cell intravasation, namely cell escape from the primary tumor, stromal invasion and transendothelial migration. We identified active β1 integrin as a biochemical and functional partner of the membrane-retained 70-kDa CDCP1 fragment, newly generated from its full-length 135-kDa precursor though proteolytic cleavage by serine proteases. Both in cell cultures and in live animals, active β1 integrin complexed preferentially with functionally activated, phosphorylated 70-kDa CDCP1. Complexing of β1 integrin the 70-kDa with CDCP1 fragment induced intracellular phosphorylation signaling, involving focal adhesion kinase-1 (FAK) and PI3 kinase (PI3K)-dependent Akt activation. Thus, inhibition of FAK/PI3K activities by specific inhibitors as well as short-hairpin RNA downregulation of β1 integrin significantly reduced FAK/Akt phosphorylation under conditions where CDCP1 was processed by serine proteases, indicating that FAK/PI3K/Akt pathway operates downstream of cleaved CDCP1 complexed with β1 integrin. Furthermore, this complex-dependent signaling correlated positively with high levels of tumor cell intravasation and dissemination. Correspondingly, abrogation in vivo of CDCP1 cleavage either by unique cleavage-blocking monoclonal antibody 10-D7 or by inhibition of proteolytic activity of plasmin-like serine proteases with aprotinin prevented β1 integrin/CDCP1 complexing and downstream FAK/Akt signaling concomitant with significant reduction of stromal invasion and spontaneous metastasis. Therefore, β1 integrin appears to serve as a motility-regulating partner mediating cross-talk between proteolytically cleaved, membrane-retained CDCP1 and members of FAK/PI3K/Akt pathway. This CDCP1 cleavage-induced signaling cascade constitutes a unique mechanism, independent of extracellular matrix remodeling, whereby a proteolytically cleaved CDCP1 regulates in vivo locomotion and metastasis of tumor cells through β1 integrin partnering. Our findings indicate that CDCP1 cleavage, occurring at the apex of a β1 integrin/FAK/PI3K/Akt signaling cascade, may represent a therapeutic target for CDCP1-positive cancers.

Published

2014

3. Canine intra-articular multipotent stromal cells (MSC) from adipose tissue have the highest in vitro expansion rates, multipotentiality, and MSC immunophenotypes.

Author

Zhang N, Dietrich MA, and Lopez MJ

Subjects

Animals, Anterior Cruciate Ligament cytology, Antigens, CD immunology, Antigens, CD34 physiology, Cell Count veterinary, Cell Division physiology, Dogs, Female, Hyaluronan Receptors physiology, Immunophenotyping veterinary, Integrin beta1 physiology, Leukocyte Common Antigens physiology, Multipotent Stem Cells cytology, Multipotent Stem Cells immunology, Stifle cytology, Stromal Cells immunology, Stromal Cells physiology, Thy-1 Antigens physiology, Adipose Tissue cytology, Antigens, CD physiology, Multipotent Stem Cells physiology, Stromal Cells cytology

Abstract

Objective: To identify the optimum intra-articular multipotent stromal cell (MSC) tissue source in the canine stifle., Study Design: Experimental., Sample Population: Infrapatellar adipose tissue, synovium lining the joint capsule, and synovium surrounding the cranial cruciate ligament (CrCL) from normal stifles of 6 dogs., Methods: Nucleated cell density for each tissue was determined, and cell doublings (CD) and doubling times (DT) were quantified for expansion rates. Adipogenic, osteogenic, and chondrogenic differentiation was confirmed with light microscopy. Fibroblastic, adipogenic, and osteogenic colony forming unit frequencies were determined for multipotentiality. Tissue-specific target gene expression was assessed, and percentages of CD29(+) , CD34(+) , CD44(+) , CD45(+) , and CD90(+) cells quantified., Results: Adipose tissue had the highest MSC density (ASC). The CD decreased with increasing passages for all cell types, and ASC values tended to be higher. Multipotentiality decreased with passage, but remained highest in ASC. Tissue-specific target gene expression was higher in induced versus noninduced cells, and ASCs had the highest upregulation across passages. Most cells were CD29(+) , CD44(+) , CD90(+) , and percentages decreased with passage. Within cell types, there were more CD29(+) ASC in early passages and more CD44(+) and CD90(+) ASC in later passages., Conclusions: ASC had the highest in vitro expansion rates, CFU frequencies, tissue-specific target gene expression, and percentages of MSC immunophenotypes., (© Copyright 2013 by The American College of Veterinary Surgeons.)

Published

2013

4. CD133(-) cells, derived from a single human colon cancer cell line, are more resistant to 5-fluorouracil (FU) than CD133(+) cells, dependent on the β1-integrin signaling.

Author

Hongo K, Tanaka J, Tsuno NH, Kawai K, Nishikawa T, Shuno Y, Sasaki K, Kaneko M, Hiyoshi M, Sunami E, Kitayama J, Takahashi K, and Nagawa H

Subjects

AC133 Antigen, Adenocarcinoma drug therapy, Adenocarcinoma immunology, Adenocarcinoma physiopathology, Antigens, CD genetics, Antimetabolites, Antineoplastic therapeutic use, Apoptosis physiology, Biomarkers, Tumor immunology, Cell Line, Tumor, Cell Movement physiology, Cell Transformation, Neoplastic immunology, Cell Transformation, Neoplastic pathology, Colorectal Neoplasms immunology, Colorectal Neoplasms physiopathology, Glycoproteins genetics, Humans, Peptides genetics, Treatment Outcome, Antigens, CD metabolism, Colorectal Neoplasms drug therapy, Drug Resistance, Neoplasm immunology, Fluorouracil therapeutic use, Glycoproteins deficiency, Glycoproteins metabolism, Integrin beta1 physiology, Peptides deficiency, Peptides metabolism, Signal Transduction physiology

Abstract

Background and Aim: Recently, the cancer stem cells (CSCs) theory has been proposed, and CD133 has been suggested as a potential marker of CSCs in various cancer types. In the present study, we aimed evaluate CD133 as a potential marker of colorectal CSCs and, for this purpose, isolated CD133(+) and CD133(-) cells from a single colorectal cancer cell line, and compared their features, especially related to the tumor-forming and differentiation abilities, and the sensitivity to chemotherapy., Methods and Results: CD133(+) cells had higher in vivo tumor-forming ability than CD133(-) cells, and in culture, they progressively differentiated into CD133(-) cells, but not vice-versa. On the other hand, CD133(-) cells were more resistant to 5-fluorouracil (FU) treatment than CD133(+) cells, and it was found to be dependent on the higher expression of ß1-integrins, and consequently, higher ability to bind collagen. Disruption of the ß1-integrin function abrogated the chemoresistance., Conclusion: From the present results, we concluded that colorectal cancer CD133(+) cells, although showing some features of CSCs, are not more resistant to 5-FU than CD133(-) cells. Therefore, definite conclusions can not be drawn yet, but it is strongly suggestive that CD133 should not be used as a single CSC marker of colorectal cancer., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

5. Semaphorin 7a promotes spreading and dendricity in human melanocytes through beta1-integrins.

Author

Scott GA, McClelland LA, and Fricke AF

Subjects

Antigens, CD analysis, Cells, Cultured, Fibroblasts metabolism, Fibroblasts radiation effects, GPI-Linked Proteins, Humans, Microscopy, Fluorescence, Nerve Tissue Proteins analysis, Receptors, Cell Surface analysis, Semaphorins analysis, Signal Transduction, Skin chemistry, Ultraviolet Rays, Antigens, CD physiology, Dendrites physiology, Integrin beta1 physiology, Melanocytes cytology, Nerve Tissue Proteins physiology, Receptors, Cell Surface physiology, Semaphorins physiology

Abstract

Described as secreted and membrane-bound proteins important for neural pathfinding, the class of proteins called Semaphorins are expressed in multiple tissue types and are involved in diverse biologic processes. In this study, we describe the function of Semaphorin 7a, a membrane-bound Semaphorin known to stimulate neurite outgrowth, on human melanocytes. We show that Semaphorin 7a is expressed by human keratinocytes and fibroblasts in vitro and in vivo and that melanocytes express Plexin C1, a receptor for Semaphorin 7a. Upregulation of Semaphorin 7a was observed in fibroblasts treated with UV irradiation, a potent stimulus for melanocyte dendricity. Because of the importance of melanocyte dendrites in cutaneous photoprotection, we performed functional studies examining the effect of Semaphorin 7a in melanocyte dendrite formation. We also examined the contribution of beta1-integrin and Plexin C1 receptor signaling in mediating effects of Semaphorin 7a in melanocytes. We show that Semaphorin 7a induces significant melanocyte spreading and dendricity in human melanocytes. Furthermore, we show that beta1-integrins and Plexin C1 receptors are ligands for Semaphorin 7a, and that signaling by these receptors has opposing effects on Semaphorin 7a-induced dendrite formation.

Published

2008

6. Role of beta(1)-integrins and their associated tetraspanin molecules in fibronectin-enhanced megakaryopoiesis.

Author

Han P, Guo X, and Story C

Subjects

Antigens, CD34 metabolism, Cell Differentiation, Cell Proliferation, Fibronectins antagonists & inhibitors, Hematopoiesis, Humans, Membrane Glycoproteins chemistry, Stem Cells physiology, Thrombopoietin antagonists & inhibitors, Thrombopoietin physiology, Antigens, CD physiology, Fibronectins physiology, Integrin beta1 physiology, Megakaryocytes cytology

Abstract

Background: We have shown previously that fibronectin (FN) together with megakaryocyte (Mk) growth and development factor (MGDF) enhanced generation of Mk progenitors determined by colony-forming unit (CFU)-Mk assay. MGDF can activate beta(1)-integrins on progenitor cells and increase binding to FN. We studied the role of beta(1)-integrin-tetraspanin complexes by which FN may enhance megakaryopoiesis., Methods: Cord blood CD34(+) cells were cultured for up to 8 days in serum-free medium containing IL-3, IL-6 and SCF with or without MGDF in the presence or absence of FN. Immunofluorescence flow cytometry was used to monitor changes in beta(1)-integrin-tetraspanin complexes. CFU-Mk assay was used to assess Mk commitment., Results: The cocktail of cytokines irrespective of the presence of MGDF altered the percentage expression of beta(1)-integrins CD49d and CD49e on CD34(+) cells. CD49d expression fell initially (98% to 15%) and then rose to 75%, whereas CD49e progressively increased over the 8 days of culture, from 5.4% to 22%. However, with the addition of FN, similar changes in the expression of beta(1)-integrins were observed but the expression was maintained at a higher level. MGDF and FN increased expression of tetraspanin molecules, CD63 and CD151, as well as their co-expression with the beta(1)-integrins on both the CD34(+) and CD34(-) cells (e.g. and increase from 0% to 80% co-expression of CD49d and CD151 on CD34(+)). Blocking of beta(1)-integrins or the tetraspanin CD151 with the respective MAb reduced Mk progenitor generation in a stromal cell model., Discussion: FN enhanced Mk progenitor generation through modulation of beta(1)-integrin-tetraspanin complexes, such as CD151/CD49d.

Published

2004

7. The functional interactions between CD98, beta1-integrins, and CD147 in the induction of U937 homotypic aggregation.

Author

Cho JY, Fox DA, Horejsi V, Sagawa K, Skubitz KM, Katz DR, and Chain B

Subjects

Antibodies pharmacology, Antigens, CD immunology, Basigin, Carrier Proteins immunology, Cell Adhesion drug effects, Cell Death, Deoxyglucose pharmacology, Edetic Acid pharmacology, Flow Cytometry, Fluorescein-5-isothiocyanate, Fluorescent Dyes, Fusion Regulatory Protein-1, Humans, Integrin beta1 immunology, Membrane Glycoproteins immunology, Phosphorylation, Phosphotyrosine metabolism, U937 Cells, Antigens, CD physiology, Antigens, Neoplasm, Antigens, Surface, Avian Proteins, Blood Proteins, Carrier Proteins physiology, Cell Adhesion physiology, Integrin beta1 physiology, Membrane Glycoproteins physiology, Monocytes physiology

Abstract

CD98 is expressed on both hematopoietic and nonhematopoietic cells and has been implicated in a variety of different aspects of cell physiology and immunobiology. In this study, the functional interactions between CD98 and other adhesion molecules on the surface of the promonocyte line U937 are examined by means of a quantitative assay of cell aggregation. Several of the CD98 antibodies induced homotypic aggregation of these cells without affecting cellular viability or growth. Aggregation induced by CD98 antibodies could be distinguished from that induced by beta1-integrin (CD29) ligation by lack of sensitivity to EDTA and by increased sensitivity to deoxyglucose. Aggregation induced via CD98 and CD29 could also be distinguished by the pattern of protein tyrosine phosphorylation induced. Some CD29 antibodies partially inhibited CD98-induced aggregation, and these antibodies were neither agonistic for aggregation nor inhibitors of beta1-integrin binding to substrates. Conversely, some CD98 antibodies were potent inhibitors of CD29-induced aggregation. Antibodies to beta2 integrins also partially inhibited CD98-induced aggregation. Unexpectedly, 2 antibodies to CD147, an immunoglobulin superfamily member whose function has remained unclear, were also potent inhibitors of both the aggregation and the protein tyrosine phosphorylation induced via CD98 ligation. The results of this study support a central role for CD98 within a multimolecular unit that regulates cell aggregation.

Published

2001

8. Expression and cellular distribution of alpha(v)integrins in beta(1)integrin-deficient embryonic stem cell-derived cardiac cells.

Author

Guan K, Czyz J, Fürst DO, and Wobus AM

Subjects

Animals, Antigens, CD genetics, Cell Adhesion, Cells, Cultured, Heart embryology, Humans, Integrin alphaV, Integrin beta1 metabolism, Integrin beta3, Integrins genetics, Mice, Mice, Knockout, Platelet Membrane Glycoproteins genetics, RNA, Messenger, Stem Cells cytology, Up-Regulation, Antigens, CD metabolism, Integrin beta Chains, Integrin beta1 physiology, Platelet Membrane Glycoproteins metabolism

Abstract

beta(1)integrin-deficient (beta(1)-/-) ES cells showed increased differentiation of cardiac cells characterized by reduced adhesion and high beating frequency. Whereas in whole embryoid body outgrowths of beta(1)-/- cells maximum levels of alpha(v), beta(3)and beta(5)integrin mRNA were delayed and transiently upregulated, in cardiac clusters isolated from beta(1)-/- cells, only beta(3)integrin mRNA levels were enhanced in comparison to wild-type (wt) cells. To answer the question, whether alpha(v)and beta(3)integrins may compensate, at least partially, the loss of beta(1)integrin function during cardiac differentiation, the distribution of alpha(v)and beta(3)integrins in beta(1)-/- and wt pacemaker-like cardiac cells was analyzed. A different distribution of alpha(v)and beta(3)integrins in beta(1)-/- v wt cardiac cells was found. In wt cardiac cells, beta(1)integrin was localized in specialized subsarcolemmal regions, in particular, at focal contacts and costameres, but alpha(v)integrin was diffusely distributed. In contrast, in beta(1)-/- cardiac cells, alpha(v)integrin was preponderantly localized at cell membranes, focal contacts and costameres. beta(3)integrin displayed a diffuse pattern both in wt and in beta(1)-/- pacemaker-like cells at early differentiation stages, whereas at terminal stages, beta(3)was colocalized with sarcomeres in wt, but not in beta(1)-/- pacemaker-like cells. Quantitative immunofluorescence analysis revealed increased alpha(v)and beta(3)integrin levels in beta(1)-/- pacemaker-like cardiac cells. Our results led us to conclude that altered cellular distribution of alpha(v)integrin and upregulation of beta(3)integrin correlate with growth and survival of beta(1)-/- cardiac pacemaker-like cells at an early developmental state. However, alpha(v)and beta(3)integrins cannot functionally compensate the loss of beta(1)integrin during terminal differentiation of cardiac cells implicating that cardiomyocytes require specific beta(1)integrin functions for cardiac specialization., (Copyright 2001 Academic Press.)

Published

2001

9. Potential role of alphav and beta1 integrins as oocyte adhesion molecules during fertilization in pigs.

Author

Linfor J and Berger T

Subjects

Animals, Antigens, CD analysis, Blotting, Western methods, Cell Membrane chemistry, Chromatography, Affinity, Female, Integrin alphaV, Integrin beta1 analysis, Integrins analysis, Male, Antigens, CD physiology, Integrin beta1 physiology, Integrins physiology, Oocytes chemistry, Sperm-Ovum Interactions physiology, Swine physiology

Abstract

Integrin molecules are cell adhesion molecules that are thought to be involved in sperm-oocyte interaction in rodents and humans. The objective of this study was to evaluate whether integrin molecules were present on the surface of pig oocytes, consistent with involvement in sperm-oocyte interaction in this species. Immunocytochemistry and confocal microscopy were used to evaluate the presence of beta1, and alpha1, alpha2, alpha3, alpha4, alpha5, alpha6 and alphav integrin subunits on the plasma membrane of pig oocytes. The beta1 and alphav integrin subunits were present consistently at the surface of pig oocytes; however, the remaining alpha integrin subunits evaluated were not routinely detected. The antibodies to the beta1 and alphav integrin subunits recognized appropriately sized protein bands on western blots of partially purified oocyte plasma membrane. These two antibodies also recognized oocyte plasma membrane protein isolated from a sperm plasma membrane affinity column. Sperm plasma membrane proteins of 137 and 93 kDa appeared to be the ligands for the beta1 integrin subunit as revealed by a western sandwich blot. Antibody to an extracellular domain of the beta1 integrin subunit reduced pig sperm-oocyte binding (P < 0.05), also indicating an assisting role for a beta1 oocyte integrin subunit in sperm-oocyte interaction in pigs. These results are consistent with an alphavbeta1 pig oocyte integrin interacting with a ligand on the sperm plasma membrane during fertilization.

Published

2000

10. Integrin-associated protein/CD47 regulates motile activity in human B-cell lines through CDC42.

Author

Yoshida H, Tomiyama Y, Ishikawa J, Oritani K, Matsumura I, Shiraga M, Yokota T, Okajima Y, Ogawa M, Miyagawa Ji, Nishiura T, and Matsuzawa Y

Subjects

Antibodies, Monoclonal pharmacology, B-Lymphocytes cytology, Burkitt Lymphoma, CD47 Antigen, Cell Polarity, Cross-Linking Reagents, Fibronectins physiology, Humans, Integrin beta1 physiology, Integrin beta3, Platelet Membrane Glycoproteins physiology, Receptors, Fibronectin physiology, Recombinant Proteins metabolism, Signal Transduction, Transfection, Tumor Cells, Cultured, Antigens, CD physiology, B-Lymphocytes physiology, Carrier Proteins physiology, cdc42 GTP-Binding Protein metabolism

Abstract

Cell migration requires a dynamic interaction between the cell, its substrate, and the cytoskeleton-associated motile apparatus. Integrin-associated protein (IAP)/CD47 is a 50-kd cell surface protein that is physically associated with beta3 integrins and that modulates the functions of beta3 integrins in various cells. However, in B-lymphocytes that express beta1 integrins but few beta3 integrins, the roles of IAP/CD47 remain to be determined. Cross-linking of IAP/CD47 by the immobilized anti-IAP/CD47 monoclonal antibody (mAb) B6H12, but not 2D3, produced signals to promote polarization with lamellipodia, a characteristic morphology during leukocyte migration, in pre-B and mature B-cell lines (BALL, Nalm6, ONHL-1, Daudi), but not in myeloma cell lines (RPMI8226, OPM-2). In the presence of the immobilized fibronectin (FN), soluble B6H12 could increase the rate of the polarization and activate migratory activity of BALL cells to FN in a transwell filter assay. Furthermore, the dominant-negative form of CDC42 completely blocked B6H12-induced morphologic and functional changes without inhibiting phorbol 12-myristate 13-acetate-induced spreading on FN in BALL cells, whereas the dominant-negative form of Rac1 inhibited all these changes. These findings demonstrate that in B-lymphocytes, IAP/CD47 may transduce the signals to activate the migratory activity, in which CDC42 may be specifically involved, and that IAP/CD47 shows synergistic effect with alpha4beta1 on B-cell migration. These findings would provide new insight into the role of IAP/CD47 on B-cell function.

Published

2000

11. Interaction between the cytodomains of the alpha 3 and beta 1 integrin subunits regulates remodelling of adhesion complexes on laminin.

Author

Laplantine E, Vallar L, Mann K, Kieffer N, and Aumailley M

Subjects

Amino Acid Sequence, Antigens, CD metabolism, Cell Adhesion Molecules physiology, Cell Line, Cytoplasm physiology, Fibroblasts metabolism, Fibroblasts physiology, Humans, Integrin alpha3, Integrin beta1 metabolism, Integrins metabolism, Laminin physiology, Microinjections, Molecular Sequence Data, Peptide Fragments chemical synthesis, Peptide Fragments isolation & purification, Protein Structure, Tertiary physiology, Surface Plasmon Resonance, Antigens, CD physiology, Cell Adhesion Molecules metabolism, Integrin beta1 physiology, Integrins physiology, Laminin metabolism, Peptide Fragments physiology

Abstract

The first step of laminin 1-induced signal transduction is initiated by the formation of alpha 6 beta 1 integrin-specific adhesion complexes. In contrast, on other laminin isoforms the adhesion complexes are alpha 3 beta 1 integrin-specific due to a transdominant regulation of the alpha 6 beta 1 integrin by the alpha 3 beta 1 integrin. To determine the mechanism of this regulation, peptides representing the cytoplasmic domain of the alpha 3 or alpha 6 integrin subunits were microinjected together with recombinant enhanced green fluorescence protein into live fibroblasts. Microinjection of the alpha 3 integrin peptide to laminin 1-adherent cells displaying alpha 6 beta 1 integrin-specific adhesion complexes resulted in the disengagement of the alpha 6 beta 1 integrin, while microinjection of green fluorescence protein alone or in combination with the alpha 6 integrin cytodomain had no effect. Further surface plasmon resonance studies revealed that the cytodomain of the beta 1 integrin subunit interacts with low affinity with the cytoplasmic tail of the alpha 3 integrin subunit, but not with that of several other alpha subunits including alpha 6. These results imply that the cytoplasmic tails of the integrin alpha subunits play a critical role in the regulation of integrin-induced signal transduction. In particular, the intracellular tail of the alpha 3 integrin subunit controls the formation of adhesion complexes in cells adhering to laminins.

Published

2000

12. Y receptor-mediated induction of CD63 transcripts, a tetraspanin determined to be necessary for differentiation of the intestinal epithelial cell line, hBRIE 380i cells.

Author

Halldén G, Hadi M, Hong HT, and Aponte GW

Subjects

Animals, Cell Adhesion Molecules genetics, Cell Adhesion Molecules physiology, Cell Differentiation, Cell Line, Cytoskeletal Proteins genetics, Cytoskeleton drug effects, Cytoskeleton physiology, Cytoskeleton ultrastructure, Extracellular Matrix Proteins genetics, Gene Expression Regulation drug effects, Hybrid Cells, Integrin beta1 genetics, Integrin beta1 physiology, Intestinal Mucosa, Intestine, Small, Kinetics, RNA, Messenger genetics, Rats, Tetraspanin 30, Antigens, CD genetics, Antigens, CD physiology, Neuropeptide Y pharmacology, Peptide YY pharmacology, Platelet Membrane Glycoproteins genetics, Platelet Membrane Glycoproteins physiology, Receptors, Gastrointestinal Hormone physiology, Receptors, Neuropeptide Y physiology, Transcription, Genetic drug effects

Abstract

Peptide YY (PYY) and neuropeptide Y (NPY) are peptides that coordinate intestinal activities in response to luminal and neuronal signals. In this study, using the rat hybrid small intestinal epithelial cell line, hBRIE 380i cells, we demonstrated that PYY- and NPY-induced rearrangement of actin filaments may be in part through a Y1alpha and/or a nonneuronal Y2 receptor, which were cloned from both the intestinal mucosa and the hBRIE 380i cells. A number of PYY/NPY-responsive genes were also identified by subtractive hybridization of the hBRIE 380i cells in the presence or absence of a 6-h treatment with PYY. Several of these genes coded for proteins associated with the cell cytoskeleton or extracellular matrix. One of these proteins was the transmembrane-4 superfamily protein CD63, previously shown to associate with beta(1)-integrin and implicated in cell adhesion. CD63 immunoreactivity, using antibody to the extracellular domain, was highest in the differentiated cell clusters of the hBRIE 380i cells. The hBRIE 380i cells transfected with antisense CD63 cDNA lost these differentiated clusters. These studies suggest a new role for NPY and PYY in modulating differentiation through cytoskeletal associated proteins.

Published

1999

13. Stromal cell CD9 regulates differentiation of hematopoietic stem/progenitor cells.

Author

Aoyama K, Oritani K, Yokota T, Ishikawa J, Nishiura T, Miyake K, Kanakura Y, Tomiyama Y, Kincade PW, and Matsuzawa Y

Subjects

Animals, Cell Adhesion, Cell Differentiation, Chemotaxis, Coculture Techniques, Erythropoietin pharmacology, Flow Cytometry, Hematopoietic Stem Cells drug effects, Humans, Integrin beta1 physiology, Interleukin-3 pharmacology, Membrane Glycoproteins physiology, Mice, Recombinant Proteins pharmacology, Stem Cell Factor pharmacology, Stromal Cells cytology, Tetraspanin 29, Antigens, CD physiology, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells physiology, Stromal Cells physiology

Abstract

CD9 belongs to the transmembrane 4 superfamily, and has been shown to influence cell proliferation, motility, and adhesion. We show here that ligation of CD9 modifies proliferation and/or differentiation of hematopoietic stem/progenitors. Pluripotent EML-C1 hematopoietic cells were cocultured with MS-5 stromal cells in the presence of KMC8.8, an anti-CD9 antibody. Numbers of recovered EML-C1 cells were slightly reduced and the antibody caused the hematopoietic cells to migrate beneath the adherent stromal cell layer. Of particular interest, EML-C1 cells recovered from CD9-ligated cultures had undifferentiated properties. Separate pretreatment of the two cell types with antibody showed that stromal-cell CD9 mediated these responses. Spontaneous expression of erythroid marker was completely blocked and there was a shift towards undifferentiated clonogenic progenitors. Immunoprecipitation studies showed that stromal-cell CD9 associates with the beta1 subunit of integrin, as well as a novel 100 kD protein. Antibody cross-linking of cell surface CD9 increased the amount of 100 kD protein that was subsequently coprecipitated with CD9. These observations show that stromal-cell CD9 influences physical interactions with hematopoietic cells and may be one factor that determines the degree of stem cell differentiation.

Published

1999

14. alpha1 and alpha2 integrins mediate invasive activity of mouse mammary carcinoma cells through regulation of stromelysin-1 expression.

Author

Lochter A, Navre M, Werb Z, and Bissell MJ

Subjects

Animals, Antibodies, Basement Membrane pathology, Cell Adhesion physiology, Cell Movement physiology, Endopeptidases physiology, Female, Integrin alpha1, Integrin alpha2, Integrin alpha6, Integrin beta1 physiology, Mammary Neoplasms, Experimental genetics, Matrix Metalloproteinase 3 genetics, Matrix Metalloproteinase 3 pharmacology, Mice, Recombinant Proteins pharmacology, Tumor Cells, Cultured, Antigens, CD physiology, Mammary Neoplasms, Experimental pathology, Mammary Neoplasms, Experimental physiopathology, Matrix Metalloproteinase 3 physiology, Neoplasm Invasiveness physiopathology

Abstract

Tumor cell invasion relies on cell migration and extracellular matrix proteolysis. We investigated the contribution of different integrins to the invasive activity of mouse mammary carcinoma cells. Antibodies against integrin subunits alpha6 and beta1, but not against alpha1 and alpha2, inhibited cell locomotion on a reconstituted basement membrane in two-dimensional cell migration assays, whereas antibodies against beta1, but not against alpha6 or alpha2, interfered with cell adhesion to basement membrane constituents. Blocking antibodies against alpha1 integrins impaired only cell adhesion to type IV collagen. Antibodies against alpha1, alpha2, alpha6, and beta1, but not alpha5, integrin subunits reduced invasion of a reconstituted basement membrane. Integrins alpha1 and alpha2, which contributed only marginally to motility and adhesion, regulated proteinase production. Antibodies against alpha1 and alpha2, but not alpha6 and beta1, integrin subunits inhibited both transcription and protein expression of the matrix metalloproteinase stromelysin-1. Inhibition of tumor cell invasion by antibodies against alpha1 and alpha2 was reversed by addition of recombinant stromelysin-1. In contrast, stromelysin-1 could not rescue invasion inhibited by anti-alpha6 antibodies. Our data indicate that alpha1 and alpha2 integrins confer invasive behavior by regulating stromelysin-1 expression, whereas alpha6 integrins regulate cell motility. These results provide new insights into the specific functions of integrins during tumor cell invasion.

Published

1999

15. Role of beta1 and beta3 integrins in human smooth muscle cell adhesion to and contraction of fibrin clots in vitro.

Author

Yee KO, Rooney MM, Giachelli CM, Lord ST, and Schwartz SM

Subjects

Antibodies pharmacology, Antigens, CD immunology, Cell Adhesion drug effects, Cell Line, Cycloheximide pharmacology, Flow Cytometry, Humans, In Vitro Techniques, Infant, Newborn, Integrin beta1 immunology, Integrin beta3, Muscle Contraction, Muscle, Smooth drug effects, Oligopeptides pharmacology, Peptides, Cyclic pharmacology, Platelet Membrane Glycoproteins immunology, Protein Synthesis Inhibitors pharmacology, Receptors, Fibronectin immunology, Receptors, Fibronectin physiology, Receptors, Vitronectin immunology, Receptors, Vitronectin physiology, Recombinant Proteins, Surface Properties, Vitronectin immunology, Antigens, CD physiology, Blood Coagulation physiology, Fibrin, Integrin beta1 physiology, Muscle, Smooth physiology, Platelet Membrane Glycoproteins physiology

Abstract

The degree of lumen narrowing in advanced lesions correlates poorly with the amount of intimal mass accumulated in the atherosclerotic plaque. As an alternate mechanism of stenosis, we propose that human smooth muscle cells bind to fibrin deposited in the matrix and exert contractile forces to cause a narrowing of the lumen. In the present study we demonstrated in vitro that human newborn aortic smooth muscle cell lines can contract and adhere to fibrin clots composed of either fibronectin-depleted plasma ("plasma") or recombinant fibrin. By using neutralizing antibodies and RGD peptides, we showed that members of the integrin family mediated the interaction between human newborn smooth muscle cells and fibrin. Neutralizing antibodies against the integrin alphavbeta3 (c7E3 Fab and LM609) did not inhibit either plasma clot contraction or recombinant fibrin clot contraction by human newborn smooth muscle cells. In contrast, antibodies against alpha5, beta1, and alpha5/beta1 inhibited contraction of clots composed of either plasma or recombinant fibrin. Anti-alphavbeta3, anti-alphav, anti-alpha5, anti-beta1, and anti-alpha5beta1 antibodies inhibited human newborn smooth muscle cell adhesion to plasma clots; however, only anti-alpha5, anti-beta1, and anti-alpha5beta1 antibodies significantly inhibited adhesion to recombinant fibrin. While the linear RGD peptides had no effect, the cyclic peptide penRGD inhibited adhesion to plasma clots and recombinant fibrin. However, it did not block contraction of recombinant fibrin clots. These results suggest that during the interaction of human newborn smooth muscle cell lines with fibrin, alpha5beta1 plays a significant role. This interaction is of potential interest as a target for efforts to block vascular contraction.

Published

1998

16. Regulation of beta 1-integrin-mediated cell adhesion by the Cbl adaptor protein.

Author

Zell T, Warden CS, Chan AS, Cook ME, Dell CL, Hunt SW 3rd, and Shimizu Y

Subjects

Amino Acid Substitution, Antigens, CD biosynthesis, Binding Sites, CD2 Antigens biosynthesis, CD28 Antigens biosynthesis, Flow Cytometry, Green Fluorescent Proteins, HL-60 Cells, Humans, Kinetics, Luminescent Proteins biosynthesis, Luminescent Proteins genetics, Mutagenesis, Site-Directed, Phosphatidylinositol 3-Kinases chemistry, Phosphatidylinositol 3-Kinases metabolism, Phosphotyrosine metabolism, Polymerase Chain Reaction, Proto-Oncogene Proteins c-cbl, Recombinant Fusion Proteins biosynthesis, Tetradecanoylphorbol Acetate pharmacology, Antigens, CD physiology, CD2 Antigens physiology, CD28 Antigens physiology, Cell Adhesion physiology, Integrin beta1 physiology, Proto-Oncogene Proteins metabolism, Ubiquitin-Protein Ligases

Abstract

Background: Leukocyte activation results in a rapid increase in adhesion to the extracellular matrix due to the activation of beta 1 integrin receptors. A role for phosphatidylinositol (PI) 3-kinase in integrin activation has been proposed, as activation of integrins by many receptors can be blocked by PI 3-kinase inhibitors. One receptor that regulates integrins is the CD28 surface antigen; here, we investigated the mechanisms responsible for CD28-mediated integrin activation., Results: CD28-mediated integrin activation was blocked by mutation of the binding site for the p85 catalytic subunit of PI 3-kinase in the CD28 cytoplasmic domain, and by expression of a dominant-negative form of the p85 subunit. Substitution of the Src homology 2 (SH2)-binding motif in the CD28 cytoplasmic domain for the corresponding motif in the CD28-related CTLA-4 surface antigen also blocked integrin activation but did not affect the recruitment and activation of PI 3-kinase. Mutations of the CD28 cytoplasmic domain that blocked integrin activation also impaired the tyrosine phosphorylation of the Cbl adaptor protein and the activation of the PI 3-kinase that was associated with Cbl. This Cbl-associated PI 3-kinase was distinct from the PI 3-kinase that coprecipitated with the CD28 cytoplasmic domain. CD28-mediated activation of beta 1 integrins was inhibited by expression of a mutant Cbl protein that shows reduced association with PI 3-kinase., Conclusions: Cbl is required for PI-3-kinase-dependent regulation of integrin receptors by CD28. Furthermore, CD28 is coupled to two distinct pools of PI 3-kinase, one directly associated with the CD28 cytoplasmic tail and the other associated with Cbl.

Published

1998

17. Beta3-integrins rather than beta1-integrins dominate integrin-matrix interactions involved in postinjury smooth muscle cell migration.

Author

Slepian MJ, Massia SP, Dehdashti B, Fritz A, and Whitesell L

Subjects

Animals, Carotid Arteries pathology, Catheterization adverse effects, Cell Adhesion, Cell Movement, Cells, Cultured, Endothelium, Vascular pathology, Fibronectins pharmacology, Flow Cytometry, Integrin beta1 physiology, Integrin beta3, Microscopy, Fluorescence, Muscle, Smooth chemistry, Oligopeptides pharmacology, Oligopeptides physiology, Rats, Rats, Sprague-Dawley, Vitronectin pharmacology, Wound Healing, Antigens, CD physiology, Carotid Artery Injuries, Endothelium, Vascular injuries, Extracellular Matrix physiology, Muscle, Smooth physiology, Platelet Membrane Glycoproteins physiology

Abstract

Background: Smooth muscle cell (SMC) migration is a vital component in the response of the arterial wall to revascularization injury. Cell surface integrin-extracellular matrix interactions are essential for cell migration. SMCs express both beta1- and beta3-integrins. In this study, we examined the relative functional roles of beta1- and beta3-integrin-matrix interactions in postinjury SMC migration., Methods and Results: Flow cytometry and fluorescence microscopy of migrating SMCs immunostained with anti-beta1 and anti-alpha(v)beta3/5 antibodies (Abs) revealed expression of both beta1- and beta3-integrins, with beta1 observed as linear streaks and beta3 found in focal contacts. In a scrape-wound migration assay, anti-beta1 Abs (92.0+/-10.7% of control, P=.1) and 0.5 mmol/L linear RGD (105+/-5% of control, P=.2) did not alter SMC migration at 48 hours after injury. Beta3-blockade, however, via Abs (anti-beta3/5 35.7+/-4.5% of control, anti-beta3 61+/-12% of control, both P<.001) and cyclic RGD (0.5 mmol/L) (12+/-10% of control, P<.001) decreased migration. Neither beta1- nor beta3-inhibition altered postinjury [3H]thymidine incorporation. In the rat carotid injury model, local adventitial polymer-based delivery of radiolabeled linear or cyclic RGD led to uptake and retention of label, for both peptides, over a 72-hour period after injury. Local arterial wall beta1-blockade via polymer-based delivery of linear RGD had no effect on SMC migration at 4.5 days (11.5+/-3.2 versus 12.8 SMCs per x600 field [control], P=.6) or on neointimal thickening at 14 days (I/M area ratio, 0.664+/-0.328 versus 1.179+/-0.324 [control], P=.6) after injury. In contrast, local beta3-blockade via cRGD limited migration (0.8+/-0.8 versus 12.8+/-4.4 SMCs per x600 field [control], P<.01) and thickening (I/M area ratio, 0.004+/-0.008 versus 1.179+/-0.324 [control], P<.01)., Conclusions: In postinjury migrating SMCs, beta3- rather than beta1-integrin-matrix interactions are of greater functional significance in adhesive processes essential for SMC migration in vitro and in vivo. Blockade of dominant SMC integrin (beta3)-matrix interactions may be a valuable approach for limiting injury-induced SMC migration and late arterial renarrowing.

Published

1998

18. Vitronectin regulates smooth muscle contractility via alphav and beta1 integrin.

Author

Dahm LM and Bowers CW

Subjects

Amnion, Animals, Antigens, CD physiology, Calcium metabolism, Cell Differentiation drug effects, Cells, Cultured, Chick Embryo, Fibroblasts cytology, Integrin alphaV, Integrin beta1 physiology, Ion Transport, Muscle Contraction, Oligopeptides physiology, Phenotype, Receptors, Vitronectin drug effects, Vitronectin blood, Vitronectin physiology, Antigens, CD drug effects, Integrin beta1 drug effects, Muscle, Smooth drug effects, Receptors, Vitronectin physiology, Vitronectin pharmacology

Abstract

Previous work from this laboratory has established a method for maintaining physiological contractility of dissociated avian smooth muscle in a defined medium at low density. The present report emphasizes the dramatic potency of serum to alter smooth muscle phenotype and induce a loss of contractility. Vitronectin, a molecule purified from plasma, mimicked these effects of serum via an integrin that is RGD-sensitive. Studies utilizing blocking antibodies against vitronectin demonstrated that the presence of this specific adhesion molecule was necessary for the serum-induced loss of contractility. Based on the actions of function-blocking antibodies and RGD-containing peptides, the integrin alphavbeta1 appears to be the primary receptor involved in vitronectin's ability to induce phenotypic transformation in amniotic smooth muscle. The influence of vitronectin on smooth muscle contractility is particularly relevant, because this molecule is abundant in whole blood and plasma (approx. 400 microg/ml). The results suggest that smooth muscle needs to be continually protected from normal blood constituents in vivo. The implications of these results for smooth muscle-related diseases like atherosclerosis, restenosis and Kaposi's sarcoma are discussed.

Published

1998

19. Integrin and cadherin synergy regulates contact inhibition of migration and motile activity.

Author

Huttenlocher A, Lakonishok M, Kinder M, Wu S, Truong T, Knudsen KA, and Horwitz AF

Subjects

Animals, Antigens, CD genetics, Cadherins genetics, Cells, Cultured, Chickens, Coturnix, Cytoskeletal Proteins analysis, Cytoskeletal Proteins genetics, Cytoskeletal Proteins physiology, Desmoplakins, Integrin alpha5, Integrin beta1 analysis, Integrin beta1 genetics, Microscopy, Video, Muscle, Skeletal cytology, Paxillin, Phosphoproteins genetics, Phosphoproteins physiology, Signal Transduction physiology, alpha Catenin, beta Catenin, Antigens, CD physiology, Cadherins physiology, Cell Communication physiology, Cell Movement physiology, Integrin beta1 physiology, Trans-Activators

Abstract

Integrin receptors play a central role in cell migration through their roles as adhesive receptors for both other cells and extracellular matrix components. In this study, we demonstrate that integrin and cadherin receptors coordinately regulate contact-mediated inhibition of cell migration. In addition to promoting proliferation (Sastry, S., M. Lakonishok, D. Thomas, J. Muschler, and A. Horwitz. 1996. J. Cell Biol. 133:169-184), ectopic expression of the alpha5 integrin in cultures of primary quail myoblasts promotes a striking contact-mediated inhibition of cell migration. Myoblasts ectopically expressing alpha5 integrin (alpha5 myoblasts) move normally when not in contact, but upon contact, they show inhibition of migration and motile activity (i.e., extension and retraction of membrane protrusions). As a consequence, these cells tend to grow in aggregates and do not migrate to close a wound. This phenotype is also seen with ectopic expression of beta1 integrin, paxillin, or activated FAK (CD2 FAK) and therefore appears to result from enhanced integrin-mediated signaling. The contact inhibition observed in the alpha5 myoblasts is mediated by N-cadherin, whose expression is upregulated more than fivefold. Perturbation studies using low calcium conditions, antibody inhibition, and ectopic expression of wild-type and mutant N-cadherins all implicate N-cadherin in the contact inhibition of migration. Ectopic expression of N-cadherin also produces cells that show inhibited migration upon contact; however, they do not show suppressed motile activity, suggesting that integrins and cadherins coordinately regulate motile activity. These observations have potential importance to normal and pathologic processes during embryonic development and tumor metastasis.

Published

1998

20. Mechanical stressing of integrin receptors induces enhanced tyrosine phosphorylation of cytoskeletally anchored proteins.

Author

Schmidt C, Pommerenke H, Dürr F, Nebe B, and Rychly J

Subjects

Calcium metabolism, Calcium-Calmodulin-Dependent Protein Kinases metabolism, Chelating Agents pharmacology, Cytochalasin D pharmacology, Egtazic Acid analogs & derivatives, Egtazic Acid pharmacology, Integrin alpha2, Integrin beta1 physiology, Phosphorylation, Physical Stimulation, Protein Binding drug effects, Receptors, Transferrin metabolism, Signal Transduction, Tyrosine metabolism, Vibration, Antigens, CD physiology, Cytoskeletal Proteins metabolism, Integrins physiology, Receptors, Cell Surface physiology

Abstract

Physical forces play a fundamental role in the regulation of cell function in many tissues, but little is known about how cells are able to sense mechanical loads and realize signal transduction. Adhesion receptors like integrins are candidates for mechanotransducers. We used a magnetic drag force device to apply forces on integrin receptors in an osteoblastic cell line and studied the effect on tyrosine phosphorylation as a biochemical event in signal transduction. Mechanical stressing of both the beta1 and the alpha2 integrin subunit induced an enhanced tyrosine phosphorylation of proteins compared with integrin clustering. Application of cyclic forces with a frequency of 1 Hz was more effective than a continuous stress. Using Triton X-100 for cell extraction, we found that tyrosine-phosphorylated proteins became physically anchored to the cytoskeleton due to mechanical integrin loading. This cytoskeletal linkage was dependent on intracellular calcium. To see if mechanical integrin stressing induced further downstream signaling, we analyzed the activation of mitogen-activated protein (MAP) kinases and found an increased phosphorylation of MAP kinases due to mechanical stress. We conclude that integrins sense physical forces that control gene expression by activation of the MAP kinase pathway. The cytoskeleton may play a key role in the physical anchorage of activated signaling molecules, which enables the switch of physical forces to biochemical signaling events.

Published

1998

21. Integrators of epidermal growth and differentiation: distinct functions for beta 1 and beta 4 integrins.

Author

Fuchs E, Dowling J, Segre J, Lo SH, and Yu QC

Subjects

Animals, Cell Differentiation, Cell Division, Cell Survival, Cytoskeleton physiology, Desmosomes physiology, Desmosomes ultrastructure, Extracellular Matrix physiology, Humans, Integrin beta4, Mammals, Models, Biological, Morphogenesis, Signal Transduction, Antigens, CD physiology, Epidermal Cells, Epidermis physiology, Integrin beta1 physiology, Skin cytology, Skin Physiological Phenomena

Abstract

Mammalian epithelia are critically dependent on interactions with components in the underlying basal lamina for proper morphogenesis and function. Substratum attachment is essential for survival, proliferation, movement, and differentiation; detachment compromises the cell's ability to perform these functions, often resulting in human disease. Interactions with the extracellular matrix are mediated through transmembrane integrin receptors that transmit signals to the cytoskeleton and to signaling molecules within the proliferating cells of the epithelium. In the past year, novel insights have emerged regarding the specific role of integrins in their attachment to extracellular matrix and in their signal transduction pathways within the epidermis.

Published

1997

22. Modulation of in vivo migratory function of alpha 2 beta 1 integrin in mouse liver.

Author

Ho WC, Heinemann C, Hangan D, Uniyal S, Morris VL, and Chan BM

Subjects

Animals, Antibodies, Monoclonal pharmacology, Cell Adhesion drug effects, Cell Adhesion physiology, Cell Line, Cell Movement drug effects, Cell Movement physiology, Collagen drug effects, Collagen metabolism, Humans, Integrin alpha2, Laminin drug effects, Laminin metabolism, Mice, Tumor Cells, Cultured, Antigens, CD pharmacology, Antigens, CD physiology, Integrin beta1 pharmacology, Integrin beta1 physiology, Liver cytology, Liver physiology

Abstract

We report herein that expression of alpha 2 beta 1 integrin increased human erythroleukemia K562 transfectant (KX2C2) cell movement after extravasation into liver parenchyma. In contrast, a previous study demonstrated that alpha 2 beta 1 expression conferred a stationary phenotype to human rhabdomyosarcoma RD transfectant (RDX2C2) cells after extravasation into the liver. We therefore assessed the adhesive and migratory function of alpha 2 beta 1 on KX2C2 and RDX2C2 cells using a alpha 2 beta 1-specific stimulatory monoclonal antibody (mAb), JBS2, and a blocking mAb, BHA2.1. In comparison with RDX2C2 cells, KX2C2 were only weakly adherent to collagen and laminin. JBS2 stimulated alpha 2 beta 1-mediated interaction of KX2C2 cells with both collagen and laminin resulting in increases in cell movement on both matrix proteins. In the presence of Mn2+, JBS2-stimulated adhesion on collagen beyond an optimal level for cell movement. In comparison, an increase in RDX2C2 cell movement on collagen required a reduction in its adhesive strength provided by the blocking mAb BHA2.1. Consistent with these in vitro findings, in vivo videomicroscopy revealed that alpha 2 beta 1-mediated postextravasation cell movement of KX2C2 cells in the liver tissue could also be stimulated by JBS2. Thus, results demonstrate that alpha 2 beta 1 expression can modulate postextravasation cell movement by conferring either a stationary or motile phenotype to different cell types. These findings may be related to the differing metastatic activities of different tumor cell types.

Published

1997

23. The alpha4beta1 integrin can mediate leukocyte adhesion to casein and denatured protein substrates.

Author

Davis GE, Thomas JS, and Madden S

Subjects

Amino Acid Sequence, Animals, Binding, Competitive, Caseins metabolism, Cations, Divalent, Cattle, Cells, Cultured, Humans, Integrin alpha4, Peptides metabolism, Protein Denaturation, Structure-Activity Relationship, Antigens, CD physiology, Cell Adhesion Molecules physiology, Integrin beta1 physiology, Leukocytes cytology

Abstract

An understanding of the binding specificity of leukocyte integrins is important to determine the range of ligands that interact with these receptors during inflammatory processes. In this study we show that the alpha4beta1 integrin can interact with casein and denatured albumin and promote leukocyte adhesion through these interactions. This was demonstrated with the use of blocking antibodies directed to alpha4beta1 and peptide adhesion competitors containing the alpha4beta1 binding tripeptide, Leu-Asp-Val (LDV). Consistent with this data, the adhesion is completely divalent cation-dependent and is stimulated by known activators of leukocyte integrin function, namely phorbol ester and the beta1 integrin activating antibody, 8A2. It is interesting to note that neither bovine alpha-casein or human albumin contain an LDV site (present in the CS-1 site of alternatively spliced fibronectin) or an IDS site (present in VCAM-1) yet they promote adhesion through this integrin. Furthermore, alpha4beta1 directly binds to Sepharose columns containing casein, casein fragments, or denatured albumin but does not bind columns containing native albumin. These data suggest that the binding specificity for the alpha4beta1 integrin is considerably broader than previously realized. This work has implications for how subsets of leukocytes may interact with damaged proteins during tissue injury and inflammation.

Published

1997

24. Interleukin-1beta-stimulated invasion of articular cartilage by rheumatoid synovial fibroblasts is inhibited by antibodies to specific integrin receptors and by collagenase inhibitors.

Author

Wang AZ, Wang JC, Fisher GW, and Diamond HS

Subjects

Antibodies, Cells, Cultured, Humans, In Vitro Techniques, Integrin alpha4, Integrin alpha5, Integrin alphaV, Interleukin-1 immunology, Interleukin-8 pharmacology, Osteoarthritis pathology, Receptors, Interleukin-1 antagonists & inhibitors, Antigens, CD physiology, Arthritis, Rheumatoid pathology, Cartilage, Articular pathology, Fibroblasts pathology, Integrin beta1 physiology, Integrins physiology, Interleukin-1 pharmacology, Matrix Metalloproteinase Inhibitors, Synovial Membrane pathology

Abstract

Objective: To study the role of integrin receptors in the invasion of cartilage by rheumatoid synovial fibroblasts (RSF)., Methods: RSF were cocultured with cartilage slices alone or in the presence of various potential activators or inhibitors. The penetration of the cartilage surface by RSF was determined by live-cell imaging of fluorescent-labeled cells., Results: Interleukin-1beta (IL-1beta) and IL-8 stimulated the RSF invasion of cartilage. Invasion was specific for RSF and required a concentration gradient of IL-1beta. The IL-1beta-activated invasion of cartilage was inhibited by anti-IL-1 antibodies, IL-1 receptor antagonist, and collagenase inhibitors. RSF invasion was also inhibited by antibodies to alpha4, alpha5, alphaV, and beta1 integrins., Conclusion: In this study, an IL-1beta concentration gradient was required for RSF invasion into cartilage, raising the possibility that in vivo invasion may be induced by IL-1beta released by chondrocytes. The IL-1beta activation of RSF assayed in vitro may contribute to the RSF invasion of cartilage in vivo. Cartilage invasion requires the availability of beta1 and alpha4, alpha5, and alphaV integrins and the presence of collagenase activity.

Published

1997

25. Disruption of integrin alpha 5 beta 1 signaling does not impair PDGF-BB-mediated stimulation of the extracellular signal-regulated kinase pathway in smooth muscle cells.

Author

Hedin UL, Daum G, and Clowes AW

Subjects

Animals, Cell Adhesion drug effects, Cell Adhesion Molecules physiology, Cell Compartmentation, Cell Division drug effects, Cell Nucleus metabolism, DNA biosynthesis, Fibronectins metabolism, Humans, Integrin alpha5, Laminin metabolism, Papio, Signal Transduction, Antigens, CD physiology, Integrin beta1 physiology, Mitogen-Activated Protein Kinases metabolism, Muscle, Smooth, Vascular physiology, Nerve Tissue Proteins metabolism, Platelet-Derived Growth Factor physiology

Abstract

Smooth muscle cell (SMC) proliferation is dependent on both anchorage to the extracellular matrix by integrins and the presence of growth factors. Integrins and growth factor receptors transduce signals that seem to converge on the extracellular signal-regulated (ERK) pathway, but the molecular basis for this interaction is not known. SMC proliferation has previously been shown to be supported by culture on fibronectin (FN), whereas cells cultured on laminin (LN) are growth inhibited. In the present study, we examined the mitogenic response to platelet-derived growth factor BB (PDGF-BB) in baboon SMCs cultured on FN vs. LN. Induction of DNA synthesis and the activity of ERK and the ERK activating kinase MKK-1 were reduced only slightly after stimulation with PDGF-BB in cells cultured on LN vs. those cultured on FN. We tested the possibility that endogenous FN secretion contributes to the ability of the cells to respond to PDGF stimulation during culture on LN. Inhibition of interactions between FN and integrin alpha 5 beta 1 by the competitive GRGDSP-peptide or anti-alpha 5 integrin antibody restricted cell spreading, reduced cell-surface staining for alpha 5 beta 1 and FN fibrils, and inhibited PDGF-BB-induced DNA synthesis. These results showed that SMC growth on LN required a provisional FN matrix. Although disruption of interactions between alpha 5 beta 1 and FN by the GRGDSP-peptide prevented PDGF-BB-induced DNA synthesis, neither ERK activity nor translocation of ERKs into the nucleus was inhibited. These results show that integrins regulate SMC growth through pathways that function in parallel with, but distinct from, growth factor-mediated ERK signaling.

Published

1997

26. Cross talk between adhesion molecules: control of N-cadherin activity by intracellular signals elicited by beta1 and beta3 integrins in migrating neural crest cells.

Author

Monier-Gavelle F and Duband JL

Subjects

Animals, Cattle, Cell Adhesion, Coturnix embryology, Gene Expression Regulation, Developmental, Humans, Integrin beta3, Neural Crest physiology, Signal Transduction, Antigens, CD physiology, Cadherins physiology, Cell Adhesion Molecules physiology, Cell Movement physiology, Integrin beta1 physiology, Neural Crest embryology, Platelet Membrane Glycoproteins physiology

Abstract

During embryonic development, cell migration and cell differentiation are associated with dynamic modulations both in time and space of the repertoire and function of adhesion receptors, but the nature of the mechanisms responsible for their coordinated occurrence remains to be elucidated. Thus, migrating neural crest cells adhere to fibronectin in an integrin-dependent manner while maintaining reduced N-cadherin-mediated intercellular contacts. In the present study we provide evidence that, in these cells, the control of N-cadherin may rely directly on the activity of integrins involved in the process of cell motion. Prevention of neural crest cell migration using RGD peptides or antibodies to fibronectin and to beta1 and beta3 integrins caused rapid N-cadherin-mediated cell clustering. Restoration of stable intercellular contacts resulted essentially from the recruitment of an intracellular pool of N-cadherin molecules that accumulated into adherens junctions in tight association with the cytoskeleton and not from the redistribution of a preexisting pool of surface N-cadherin molecules. In addition, agents that cause elevation of intracellular Ca2+ after entry across the plasma membrane were potent inhibitors of cell aggregation and reduced the N-cadherin- mediated junctions in the cells. Finally, elevated serine/ threonine phosphorylation of catenins associated with N-cadherin accompanied the restoration of intercellular contacts. These results indicate that, in migrating neural crest cells, beta1 and beta3 integrins are at the origin of a cascade of signaling events that involve transmembrane Ca2+ fluxes, followed by activation of phosphatases and kinases, and that ultimately control the surface distribution and activity of N-cadherin. Such a direct coupling between adhesion receptors by means of intracellular signals may be significant for the coordinated interplay between cell-cell and cell-substratum adhesion that occurs during embryonic development, in wound healing, and during tumor invasion and metastasis.

Published

1997

27. Activation of beta1 integrins on CML progenitors reveals cooperation between beta1 integrins and CD44 in the regulation of adhesion and proliferation.

Author

Lundell BI, McCarthy JB, Kovach NL, and Verfaillie CM

Subjects

Antigens, CD34 analysis, Bone Marrow pathology, Cell Adhesion, Cell Culture Techniques methods, Cell Division, Cells, Cultured, HLA-DR Antigens analysis, Hematopoiesis, Hematopoietic Stem Cells pathology, Hematopoietic Stem Cells physiology, Humans, Kinetics, Leukemia, Myelogenous, Chronic, BCR-ABL Positive pathology, Antigens, CD physiology, Hematopoietic Stem Cells immunology, Hyaluronan Receptors physiology, Integrin beta1 physiology, Leukemia, Myelogenous, Chronic, BCR-ABL Positive immunology

Abstract

Adhesion of normal colony-forming cells (CFC) to bone marrow (BM) stroma and the extracellular matrix (ECM) component fibronectin (FN) depends at least in part on the alpha4beta1 and alpha5beta1 integrins and the CD44 receptor. Aside from anchoring progenitors in the marrow microenvironment, beta1 integrin-dependent adhesion of normal CFC is associated with inhibition of their proliferation. In contrast to normal CFC, chronic myelogenous leukemia (CML) Ph+ CFC adhere significantly less to either stroma or FN. CML Ph+ CFC proliferation is also not inhibited by coculture with stroma or FN. However, equal numbers of alpha4, alpha5, and beta1 integrins and CD44 are present on CML and normal CD34+ cells. We have previously demonstrated that beta1-dependent adhesion to and subsequent proliferation inhibition by FN can be restored when CML Ph+ CFC are incubated with the beta1 integrin activating antibody, 8A2, and demonstrated a role for the alpha5beta1 integrin in this phenomenon. Since the integrin alpha4beta1 and the proteoglycan form of CD44 may cooperate in establishing normal CFC adhesion to FN, we examined if treatment of CML Ph+ CFC with 8A2 also restores the cooperativity between beta1 integrins and CD44. We demonstrate that 8A2 induces adhesion of CML Ph+ CFC not only to intact FN but also to alpha4beta1, alpha5beta1, and proteoglycan binding fragments of FN. 8A2-induced adhesion to these fragments and peptides also results in a significant inhibition of the proliferation of CML Ph+ CFC. Addition of antibodies to either the alpha5, alpha4, or beta1 integrins, antibodies against the CD44 receptor, or removal of chondroitin sulfate glycosaminoglycans from the surface of CML CD34+ HLA-DR+ cells significantly reduced the 8A2-induced adhesion to and adhesion-mediated inhibition of proliferation by FN. These studies demonstrate that activation of beta1 integrins on CML Ph+ CFC not only results in upregulation of beta1 integrin-dependent adhesion and adhesion-mediated inhibition of proliferation, but also in the restoration of cooperation between beta1 integrins and CD44. These studies suggest that decreased beta1 integrin avidity may also affect the function of the proteoglycan adhesion receptor CD44, both of which may contribute to the abnormal circulation and expansion of malignant progenitors in CML.

Published

1997

28. Alpha 3 beta 1 integrin has a crucial role in kidney and lung organogenesis.

Author

Kreidberg JA, Donovan MJ, Goldstein SL, Rennke H, Shepherd K, Jones RC, and Jaenisch R

Subjects

Animals, Basement Membrane ultrastructure, Integrin alpha3, Kidney Glomerulus embryology, Mice, Mice, Knockout, Morphogenesis, Antigens, CD physiology, Integrin beta1 physiology, Integrins physiology, Kidney embryology, Lung embryology

Abstract

A mutation was targeted to the murine alpha3 integrin gene. Homozygous mutant mice survived to birth, but died during the neonatal period. The mutation caused abnormal kidney and lung development. Mutant kidneys displayed decreased branching of the medullary collecting ducts, although the number of nephrons was not altered. Proximal tubules exhibited two distinct subsets of abnormalities, with the epithelial cells either containing excess lysosomes or becoming microcystic. In addition, glomerular development was markedly affected. In mutant kidneys, the extent of branching of glomerular capillary loops was decreased, with capillary lumina being wider than normal. The glomerular basement membrane was disorganized and glomerular podocytes were unable to form mature foot processes. Branching of the bronchi in lungs of mutant mice was also decreased and the large bronchi extended to the periphery. These results indicate a role for integrin receptors in basement membrane organization and branching morphogenesis.

Published

1996

29. Identification of a functionally important sequence in the cytoplasmic tail of integrin beta 3 by using cell-permeable peptide analogs.

Author

Liu XY, Timmons S, Lin YZ, and Hawiger J

Subjects

Amino Acid Sequence, Biological Transport, Cell Line, Humans, Integrin beta1 chemistry, Integrin beta1 physiology, Integrin beta3, Leukemia, Erythroblastic, Acute, Male, Molecular Sequence Data, Peptide Fragments chemical synthesis, Peptide Fragments metabolism, Peptide Fragments pharmacology, Peptides chemical synthesis, Peptides metabolism, Peptides pharmacology, Skin, Tumor Cells, Cultured, Antigens, CD chemistry, Antigens, CD physiology, Cell Adhesion drug effects, Endothelium, Vascular physiology, Platelet Membrane Glycoproteins chemistry, Platelet Membrane Glycoproteins physiology

Abstract

Integrins are major two-way signaling receptors responsible for the attachment of cells to the extracellular matrix and for cell-cell interactions that underlie immune responses, tumor metastasis, and progression of atherosclerosis and thrombosis. We report the structure-function analysis of the cytoplasmic tail of integrin beta 3 (glycoprotein IIla) based on the cellular import of synthetic peptide analogs of this region. Among the four overlapping cell-permeable peptides, only the peptide carrying residues 747-762 of the carboxyl-terminal segment of integrin beta 3 inhibited adhesion of human erythroleukemia (HEL) cells and of human endothelial cells (ECV) 304 to immobilized fibrinogen mediated by integrin beta 3 heterodimers, alpha IIb beta 3, and alpha v beta 3, respectively. Inhibition of adhesion was integrin-specific because the cell-permeable beta 3 peptide (residues 747-762) did not inhibit adhesion of human fibroblasts mediated by integrin beta 1 heterodimers. Conversely, a cell-permeable peptide representing homologous portion of the integrin beta 1 cytoplasmic tail (residues 788-803) inhibited adhesion of human fibroblasts, whereas it was without effect on adhesion of HEL or ECV 304 cells. The cell-permeable integrin beta 3 peptide (residues 747-762) carrying a known loss-of-function mutation (Ser752Pro) responsible for the genetic disorder Glanzmann thrombasthenia Paris I did not inhibit cell adhesion of HEL or ECV 304 cells, whereas the beta 3 peptide carrying a Ser752Ala mutation was inhibitory. Although Ser752 is not essential, Tyr747 and Tyr759 form a functionally active tandem because conservative mutations Tyr747Phe or Tyr759Phe resulted in a nonfunctional cell permeable integrin beta 3 peptide. We propose that the carboxyl-terminal segment of the integrin beta 3 cytoplasmic tail spanning residues 747-762 constitutes a major intracellular cell adhesion regulatory domain (CARD) that modulates the interaction of integrin beta 3-expressing cells with immobilized fibrinogen. Import of cell-permeable peptides carrying this domain results in inhibition "from within" of the adhesive function of these integrins.

Published

1996

30. Migration of brain tumor cells on extracellular matrix proteins in vitro correlates with tumor type and grade and involves alphaV and beta1 integrins.

Author

Friedlander DR, Zagzag D, Shiff B, Cohen H, Allen JC, Kelly PJ, and Grumet M

Subjects

Antibodies pharmacology, Antigens, CD immunology, Biopsy, Brain Neoplasms, Breast Neoplasms surgery, Cell Adhesion, Cell Aggregation, Cell Line, Cell Movement, Female, Humans, Immunohistochemistry, Integrin alphaV, Integrin beta1 immunology, Tumor Cells, Cultured, Antigens, CD physiology, Breast Neoplasms pathology, Breast Neoplasms physiopathology, Extracellular Matrix Proteins, Integrin beta1 physiology

Abstract

An important contributor to the malignancy of brain tumors is their ability to infiltrate the brain. Extracellular matrix molecules and cell adhesion molecules on cell surfaces play key roles in cell migration. In the present study, we used reaggregates of dissociated cells from freshly excised human brain tumors to analyze the migration of cells from human brain tumors of different types and grades on many different adhesion proteins adsorbed to glass substrates. Proteins were chosen based on their presence in normal or neoplastic nervous tissue, and included the extra-cellular matrix molecules fibronectin, collagens, fibrinogen, laminin, tenascin-C, thrombospondin, and the neuron-glia cell adhesion molecule, Ng-CAM. Cells from astrocytomas (n = 24) migrated on a variety of substrates, in contrast to cells from primitive neuroectodermal tumors cells (n=6), which only migrated well on laminin, fibronectin, or type IV collagen but not on the other substrates. Typically, migrating cells from astrocytomas of all grades had long, slender processes, were usually bipolar, and their cell bodies did not spread well on any substrate. Although there was variability in the migration of cells from astrocytomas of the same grade, cells from high-grade astrocytomas tended to migrate more extensively (42.3 +/- 4.7 micrometers/16 h: n = 16) than cells from lower grade astrocytomas (28.9 +/- 3.9 micrometers/16 h; P = 0.07; n = 8); the most striking differences were observed for collagen substrates, on which cells from lower grade astrocytomas migrated at very low levels (7.6 +/- 2 .6 micrometers/16 h) and cells from high-grade astrocytomas at higher levels (24.4 +/- 5.2 micrometers;P = 0.01). In contrast to primary cells from glioblastomas (n = 13), glioblastoma cell lines (n = 10) consistently spread on various substrates and migrated at high levels (69.5 +/- 7.6 versus 46.4 +/-5.7 micrometers/16 h; P = 0.03), in particular, on collagens (108.4 +/- 20.2 versus 28.0 +/- 6.1 micrometers/16 h; P= 0.001). Specific monoclonal antibodies to alphaV and beta1 integrin monomers completely inhibited the migration of astrocytoma cells on most substrates, suggesting that alphaV and beta1 integrins play a crucial role in brain tumor infiltration. These studies also suggest that although a large number of extracellular matrix molecules may promote tumor cell migration, disrupting the function of only a few tumor cell receptors may be critical for tumor infiltration in the brain.

Published

1996

31. Studies in vitro on the role of alpha v and beta 1 integrins in the adhesion of human dermal fibroblasts to provisional matrix proteins fibronectin, vitronectin, and fibrinogen.

Author

Gailit J and Clark RA

Subjects

Adult, Cell Adhesion, Extracellular Matrix Proteins physiology, Fibroblasts physiology, Humans, Integrin alphaV, Receptors, Cell Surface metabolism, Antigens, CD physiology, Fibrinogen physiology, Fibronectins physiology, Integrin beta1 physiology, Skin cytology, Vitronectin physiology

Abstract

Fibroblasts that migrate into a wound during the early stages of repair use cell surface integrins to interact with extracellular molecules as they move away from the interstitial matrix of normal tissue and into the provisional matrix of the wound. Therefore, to understand a critical phase of wound healing, it is necessary to understand the details of integrin involvement. Normal adult human dermal fibroblasts in culture express many receptors for the provisional matrix proteins fibronectin, vitronectin, and fibrinogen, including the integrins alpha 3 beta 1, alpha 4 beta 1, alpha 5 beta 1, alpha v beta 1, alpha v beta 3, and alpha v beta 5. We used quantitative flow cytometry to estimate the relative numbers of these receptors and immunoprecipitation to confirm the expression of alpha v beta 1. Adult human dermal fibroblasts primarily use beta 1 integrins, alpha 4 beta 1, alpha 5 beta 1, and possibly alpha v beta 1, for attachment to fibronectin. alpha v beta 3 and perhaps other integrins containing the alpha v subunit serve fibroblasts as secondary or auxiliary receptors for fibronectin. In contrast, these cells use alpha v integrins but probably not beta 1 integrins for attachment to vitronectin. alpha v beta 3 and alpha v beta 5 apparently act in concert to mediate attachment to vitronectin, and these two integrins may perform different functions during wound repair. Fibroblast adhesion to certain preparations of fibrinogen occurs, at least partially, through the small amount of fibronectin present in the preparations. Fibroblast attachment to fibrinogen purified free of fibronectin also occurs, and that was demonstrated with a sensitive new assay called electrical cell-substrate impedance sensing. Fibroblast attachment to pure fibrinogen can be inhibited by RGD peptide, suggesting that integrins are involved.

Published

1996

32. Loss of the tumorigenic phenotype with in vitro, but not in vivo, passaging of a novel series of human bronchial epithelial cell lines: possible role of an alpha 5/beta 1-integrin-fibronectin interaction.

Author

Schiller JH and Bittner G

Subjects

Animals, Antibodies, Monoclonal, Cell Adhesion, Cells, Cultured, Epithelial Cells, Extracellular Matrix physiology, Humans, Integrin alpha5, Mice, Neoplasm Transplantation, Transplantation, Heterologous, Antigens, CD physiology, Bronchi cytology, Fibronectins physiology, Integrin beta1 physiology, Neoplasms, Experimental pathology, Receptors, Cytoadhesin physiology

Abstract

We established an immortalized, nontumorigenic human bronchial epithelial cell line by transfection with the origin of replication-defective SV40 large T plasmid. This line spontaneously became tumorigenic at passage 184 (NL20T), although subsequent passages (passages 189, 200, and 205) failed to form tumors. The tumorigenic cell line NL20T was reinoculated back into athymic nude mice, and the two subsequently derived cell lines (NL20T-A and NL20T-B) have been passaged 85 times in vitro and remain tumorigenic. However, late-passage NL20T cells consistently lose their tumorigenicity when passaged in vitro on tissue culture plastic dishes (NL20T-n cells). Thus, two of the cell lines, NL20 and NL20T, reverted to the nontumorigenic phenotype reproducibly and spontaneously following serial passage on plastic tissue culture plates, whereas cells passaged in mice (NL20T-A and -B) did not. We used these nontumorigenic (NL20 and NL20T-n) and tumorigenic (early passage NL20T, NL20T-A, and NL20T-B) cells to study the role of the alpha 5/beta 1-integrin and attachment to fibronectin in tumorigenicity. The two nontumorigenic cell lines (NL20 and NL20T-n) attached slower to fibronectin-coated plates than the two tumorigenic cell lines in a cellular-extracellular matrix adhesion assay. Attachment was abrogated by exposure to a blocking antibody to the alpha 5/beta 1-integrin, the fibronectin receptor, in the two tumorigenic cell lines. Cell surface expression of the alpha 5/beta 1 cell surface protein by flow cytometry was highest in the tumorigenic NL20T and NL20T-A cells. NL20T-A cells were cultured with an antibody to alpha 5/beta 1 and inoculated s.c. into athymic nude mice; tumorigenicity of the NL20T-A cells was inhibited in a dose-dependent manner. Tumorigenicity was also inhibited partially with monoclonal antibodies to either alpha 5 or beta 1. A mixture of 10% tumorigenic NL20T-A cells and 90% nontumorigenic NL20 cells was cultured on plastic, type IV collagen, laminin, and fibronectin for 9 weeks. Only cells cultured on fibronectin formed tumors when inoculated s.c. into athymic nude mice. We conclude that these data are consistent with the hypothesis that neoplastic transformation in our original cell line arose from in vivo selection of a small mutant clone, which had arisen in culture and was selected subsequently in vivo but was lost with in vitro culture in NL20 cells, and that alpha 5/beta 1-integrin interaction with the extracellular matrix may play a role in tumorigenicity in our system.

Published

1995

33. Ectopic expression of human and feline CD9 in a human B cell line confers beta 1 integrin-dependent motility on fibronectin and laminin substrates and enhanced tyrosine phosphorylation.

Author

Shaw AR, Domanska A, Mak A, Gilchrist A, Dobler K, Visser L, Poppema S, Fliegel L, Letarte M, and Willett BJ

Subjects

Animals, Antibodies, Monoclonal pharmacology, Antigens, CD biosynthesis, Benzoquinones, Cats, Cattle, Cell Line, Enzyme Inhibitors pharmacology, Fibronectins, Flow Cytometry, Gene Expression, Humans, Integrin beta1 physiology, Lactams, Macrocyclic, Laminin, Membrane Glycoproteins biosynthesis, Membrane Glycoproteins physiology, Phosphorylation, Protein-Tyrosine Kinases antagonists & inhibitors, Protein-Tyrosine Kinases metabolism, Quinones pharmacology, Recombinant Proteins, Rifabutin analogs & derivatives, Serum Albumin, Bovine, Signal Transduction, Tetraspanin 29, Transfection, Antigens, CD physiology, B-Lymphocytes immunology, Cell Movement, Phosphotyrosine metabolism

Abstract

Few molecules have been shown to confer cell motility. Although the motility-arresting properties of anti-CD9 monoclonal antibody (mAb) suggest the transmembrane 4 superfamily (TM4SF) member CD9 can induce a motorgenic signal, gene transfection studies have failed to confirm this hypothesis. We report here that ectopic expression of human CD9 (CD9h) and feline CD9 (CD9f) in the CD9-negative, poorly motile, human B cell line Raji dramatically enhances migration across fibronectin- and laminin-coated polycarbonate filters. Migration of Raji/CD9h and Raji/CD9f on either substrate was inhibited by the anti-CD9 mAb 50H.19 and by the anti-beta 1 integrin mAb AP-138. Migration of Raji/CD9h on laminin was potently inhibited by the anti-VLA-6 integrin mAb GoH3 and by the anti-VLA-4 integrin mAb 44H6, whereas migration of Raji/CD9h on fibronectin was inhibited only by mAb 44H6. Since CD9h-transfected Raji cells adhered to fibronectin as effectively as mock transfectants, expression of CD9 enhanced motility, but not adhesion. CD9-enhanced migration was inhibited by the protein tyrosine kinase inhibitor herbimycin A suggesting that tyrosine phosphorylation played a role in the generation of a motorgenic signal. Raji/CD9h transfectants adherent to fibronectin expressed 6-fold higher levels of phosphotyrosine than Raji. Raji/CD9f transfectants also phosphorylated proteins on tyrosine more effectively than Raji including a protein of 110 kDa which was phosphorylated on the motility-inducing substrates laminin and fibronectin, but not on bovine serum albumin. Our results support a role for CD9 in the amplification of a motorgenic signal in B cells involving beta 1 integrins and the activation of protein tyrosine kinases.

Published

1995