Your search keyword '"Sarah C. Bodary"' showing total 24 results

1. Effects of kistrin on bone resorption in vitro and serum calcium in vivo

Author

Kathleen King, Subhash C. Kukreja, Robert M. Pitti, Sarah C. Bodary, Mark S. Dennis, Robert A. Lazarus, Mark Siegel, James J. D'Anza, and R. Glenn Hammonds

Subjects

Male, Alpha-v beta-3, Endocrinology, Diabetes and Metabolism, Molecular Sequence Data, Integrin, Osteoclasts, Bone resorption, Cell Line, Mice, chemistry.chemical_compound, Osteoclast, In vivo, Crotalid Venoms, Cell Adhesion, medicine, Animals, Humans, Orthopedics and Sports Medicine, Amino Acid Sequence, Bone Resorption, Cell adhesion, Cells, Cultured, Mice, Inbred BALB C, Dose-Response Relationship, Drug, biology, Fibrinogen, Rats, Resorption, Cell biology, medicine.anatomical_structure, chemistry, Biochemistry, Microscopy, Electron, Scanning, biology.protein, Calcium, Vitronectin, Peptides, Oligopeptides

Abstract

In many cell systems, cell-cell and cell-matrix interactions are mediated by integrins, a family of cell surface heterodimeric glycoprotein receptors. Osteoclast integrins may play a role in the process of bone resorption. Osteoclasts express the alpha v and beta 3 subunits of the vitronectin receptor and adhere to a wide range of proteins in vitro, all which contain the amino acid sequence Arg-Gly-Asp (RGD), an adhesion site recognition sequence common to many protein ligands that bind to integrins. The effect of kistrin, an RGD-containing snake venom protein, on osteoclast-mediated bone resorption was investigated in vivo and in vitro. When kistrin was infused into normocalcemic and hypercalcemic mice, serum calcium was significantly lowered at 3 and 6 h after the start of infusion, indicating an inhibitory effect on osteoclast activity in vivo. In vitro, kistrin potently inhibited bone resorption by isolated rat osteoclasts cultured on slices of bovine bone, and kistrin also inhibited the attachment of 293 cells expressing recombinant human alpha v beta 3 to fibrinogen (IC50 = 1 nM). These results indicate the potential therapeutic use of RGD-containing molecules for hypercalcemia of malignancy or for other disorders associated with bone loss.

Published

2009

2. Blockade of CD11a by Efalizumab in Psoriasis Patients Induces a Unique State of T-Cell Hyporesponsiveness

Author

Yulia Vugmeyster, Francesca Chamian, Edmund Lee, Toyoko Kikuchi, Wolfgang Dummer, Kathy Howell, Michelle A. Lowes, Emma Guttman-Yassky, James G. Krueger, Sarah C. Bodary, Brisdell Hunte, Patricia Gilleaudeau, and Mark Kagen

Subjects

Adult, Male, Receptor complex, CD3 Complex, CD8 Antigens, T-Lymphocytes, CD3, T cell, Lymphocyte, Efalizumab, CD2 Antigens, Receptors, Antigen, T-Cell, Down-Regulation, CD11a, Dermatology, Integrin alpha4beta1, Antibodies, Monoclonal, Humanized, Lymphocyte Activation, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, CD28 Antigens, Downregulation and upregulation, Psoriasis, medicine, Humans, CD11a Antigen, Molecular Biology, Aged, 030304 developmental biology, 0303 health sciences, biology, business.industry, Antibodies, Monoclonal, Cell Biology, Middle Aged, medicine.disease, Lymphocyte Function-Associated Antigen-1, 3. Good health, medicine.anatomical_structure, 030220 oncology & carcinogenesis, CD4 Antigens, Immunology, biology.protein, Interleukin-2, Female, business, medicine.drug

Abstract

Efalizumab (anti-CD11a) interferes with LFA-1/ICAM-1 binding and inhibits several key steps in psoriasis pathogenesis. This study characterizes the effects of efalizumab on T-cell activation responses and expression of surface markers on human circulating psoriatic T cells during a therapeutic trial. Our data suggest that efalizumab may induce a unique type of T-cell hyporesponsiveness, directly induced by LFA-1 binding, which is distinct from conventional anergy described in animal models. Direct activation of T cells through different activating receptors (CD2, CD3, CD3/28) is reduced, despite T cells being fully viable. This hyporesponsiveness was spontaneously reversible after withdrawal of the drug, and by IL-2 in vitro. In contrast to the state of anergy, Ca(+2) release is intact during efalizumab binding. Furthermore, lymphocyte function-associated antigen-1 (LFA-1) blockade resulted in an unexpected downregulation of a broad range of surface molecules, including the T-cell receptor complex, co-stimulatory molecules, and integrins unrelated to LFA-1, both in the peripheral circulation and in diseased skin tissue. These observations provide evidence for the mechanism of action of efalizumab. The nature of this T-cell hyporesponsiveness suggests that T-cell responses may be reduced during efalizumab therapy, but are reversible after ceasing efalizumab treatment.

Published

2008

3. Elevated Flk1 (Vascular Endothelial Growth Factor Receptor 2) Signaling Mediates Enhanced Angiogenesis in β3-Integrin–Deficient Mice

Author

Stephen D. Robinson, Tobi Nagel, Julie C. Lively, Sarah C. Bodary, Andrew R. Reynolds, Louise E. Reynolds, Daniel J. Hicklin, and Kairbaan Hodivala-Dilke

Subjects

Male, Vascular Endothelial Growth Factor A, Cancer Research, medicine.medical_specialty, Lung Neoplasms, Endothelium, Angiogenesis, Melanoma, Experimental, Cell Growth Processes, Biology, Vascular endothelial growth inhibitor, Mice, chemistry.chemical_compound, Cell Movement, Internal medicine, medicine, Animals, Extracellular Signal-Regulated MAP Kinases, Neovascularization, Pathologic, Integrin beta3, Kinase insert domain receptor, Neoplasms, Experimental, Integrin alphaVbeta3, Vascular Endothelial Growth Factor Receptor-2, Cell biology, Mice, Inbred C57BL, Vascular endothelial growth factor, Vascular endothelial growth factor B, Vascular endothelial growth factor A, Endocrinology, medicine.anatomical_structure, Oncology, chemistry, Vascular endothelial growth factor C, Female, Endothelium, Vascular, Signal Transduction

Abstract

Tumor growth, tumor angiogenesis, and vascular endothelial growth factor (VEGF)–specific angiogenesis are all enhanced in β3-integrin–null mice. Furthermore, endothelial cells isolated from β3-null mice show elevated levels of Flk1 (VEGF receptor 2) expression, suggesting that β3-integrin can control the amplitude of VEGF responses by controlling Flk1 levels or activity. We now show that Flk1 signaling is required for the enhanced tumor growth and angiogenesis seen in β3-null mice. Moreover, β3-null endothelial cells exhibit enhanced migration and proliferation in response to VEGF in vitro, and this phenotype requires Flk1 signaling. Upon VEGF stimulation, β3-null endothelial cells exhibit higher levels of phosphorylated Flk1 and extracellular-related kinases 1 and 2 than wild-type endothelial cells. Furthermore, signaling via ERK1/2 is required to mediate the elevated responses to VEGF observed in β3-null endothelial cells and aortic rings in vitro. These data confirm that VEGF signaling via Flk1 is enhanced in β3-integrin–deficient mice and suggests that this increase may mediate the enhanced angiogenesis and tumor growth observed in these mice in vivo.

Published

2004

4. Efalizumab (anti-CD11a)-induced increase in peripheral blood leukocytes in psoriasis patients is preferentially mediated by altered trafficking of memory CD8+ T cells into lesional skin*1

Author

Sarah C. Bodary, James G. Krueger, Patricia Gilleaudeau, Yulia Vugmeyster, Michelle A. Lowes, Francesca Chamian, Edmund Lee, Kathy Howell, Toyoko Kikuchi, Wolfgang Dummer, and Mark Kagen

Subjects

business.industry, T cell, Immunology, Efalizumab, T lymphocyte, CD11a, medicine.disease, medicine.anatomical_structure, Psoriasis, Immunology and Allergy, Medicine, Cytotoxic T cell, business, Memory T cell, CD8, medicine.drug

Abstract

Therapeutic administration of efalizumab, a humanized antibody to CD11a, induces a marked but reversible increase of peripheral lymphocytes in psoriasis patients. In this study, 13 patients were treated with 12 weekly subcutaneous doses (2 mg/kg/week) of efalizumab, and all 13 patients had increases in leukocyte counts. This increased white blood cell count was mainly due to a 3- to 4-fold increase in the number of circulating CD3+ lymphocytes during active treatment. Both naive and memory populations of CD4+ and CD8+ lymphocytes in the peripheral blood increased, with the largest increase observed in memory CD8+ T cells. This CD8+ memory T cell subset is a prominent T cell population found in psoriatic skin. An increase in Type 1 (IFN-γ producing) T cells was also observed during treatment. Both components of LFA-1, CD11a and CD18, were downregulated during treatment, and surprisingly the integrins CD11b and β7 were similarly reduced. We conclude that efalizumab most likely blocks cutaneous entry of memory CD8+ T cells, a highly disease-relevant cell population. The relatively smaller increase in naive peripheral blood T cells could be attributed to reduced trafficking of naive T cells.

Published

2004

5. ANGPTL3 Stimulates Endothelial Cell Adhesion and Migration via Integrin αvβ3 and Induces Blood Vessel Formation in Vivo

Author

Ming-Hong Xie, Maria Teresa Pisabarro, Joe Kowalski, Phil Hass, Daniel Eric Sherman, Austin L. Gurney, Maureen Beresini, Xiao Huan Liang, Sarah C. Bodary, Napoleone Ferrara, Gieri Camenisch, Mark Nagel, Hans-Peter Gerber, and Kevin R Clark

Subjects

MAP Kinase Signaling System, Angiogenesis, Molecular Sequence Data, Integrin, Neovascularization, Physiologic, Angiopoietin-like 4 Protein, Transfection, Biochemistry, Cell Line, Angiopoietin-2, Cornea, Focal adhesion, Angiopoietin, Mice, Cell Movement, ANGPTL3, Cell Adhesion, Animals, Humans, Receptors, Vitronectin, Amino Acid Sequence, Endothelium, Cloning, Molecular, Growth Substances, Molecular Biology, Protein kinase B, Cells, Cultured, Angiopoietin-Like Protein 3, Sequence Homology, Amino Acid, biology, Fibrinogen, Proteins, Cell Biology, Protein-Tyrosine Kinases, Precipitin Tests, Recombinant Proteins, Protein Structure, Tertiary, Rats, Cell biology, Angiopoietin-like Proteins, Focal Adhesion Kinase 1, Focal Adhesion Protein-Tyrosine Kinases, biology.protein, Intercellular Signaling Peptides and Proteins, Signal transduction, Angiopoietins, Protein Binding

Abstract

The angiopoietin family of secreted factors is functionally defined by the C-terminal fibrinogen (FBN)-like domain, which mediates binding to the Tie2 receptor and thereby facilitates a cascade of events ultimately regulating blood vessel formation. By screening expressed sequence tag data bases for homologies to a consensus FBN-like motive, we have identified ANGPTL3, a liver-specific, secreted factor consisting of an N-terminal coiled-coil domain and the C-terminal FBN-like domain. Co-immunoprecipitation experiments, however, failed to detect binding of ANGPTL3 to the Tie2 receptor. A molecular model of the FBN-like domain of ANGPTL3 was generated and predicted potential binding to integrins. This hypothesis was experimentally confirmed by the finding that recombinant ANGPTL3 bound to alpha(v)beta(3) and induced integrin alpha(v)beta(3)-dependent haptotactic endothelial cell adhesion and migration and stimulated signal transduction pathways characteristic for integrin activation, including phosphorylation of Akt, mitogen-activated protein kinase, and focal adhesion kinase. When tested in the rat corneal assay, ANGPTL3 strongly induced angiogenesis with comparable magnitude as observed for vascular endothelial growth factor-A. Moreover, the C-terminal FBN-like domain alone was sufficient to induce endothelial cell adhesion and in vivo angiogenesis. Taken together, our data demonstrate that ANGPTL3 is the first member of the angiopoietin-like family of secreted factors binding to integrin alpha(v)beta(3) and suggest a possible role in the regulation of angiogenesis.

Published

2002

6. αvβ3 Antagonists Based on a Central Thiophene Scaffold

Author

Thomas R. Gadek, Denis Carniato, Martine Gaillard, Marielle Auberval, Jochen Knolle, Roland Baron, Jean-Marie Ruxer, Karl-Heinz Scheunemann, Jean-Francois Gourvest, Gerhard Breipohl, Hans Ulrich Stilz, Volkmar Wehner, Sarah C. Bodary, Bernard Doucet, David William Will, and Anusch Peyman

Subjects

Scaffold, biology, Stereochemistry, Chemistry, Organic Chemistry, Clinical Biochemistry, Integrin, Pharmaceutical Science, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Drug Discovery, Thiophene, Side chain, biology.protein, Molecular Medicine, Guanidine, Selectivity, Cell adhesion, Molecular Biology

Abstract

A series of novel, highly potent αvβ3 antagonists based on a thiophene scaffold and containing an acylguanidine as an Arg-mimetic is described. A number of structural features, such as cyclic versus open guanidine and a variety of lipophilic side chains, carbamates, sulfonamides and β-amino acids were explored with respect to inhibition of αvβ3 mediated cell adhesion and selectivity versus αIIbβ3 binding. In addition, compound 19 was found to be active in the TPTX model of osteoporosis.

Published

2001

7. RGD Mimetics containing a central hydantoin scaffold: α V β 3 vs α IIb β 3 selectivity requirements

Author

Jochen Knolle, Denis Carniato, Hans Ulrich Stilz, Jean-Marie Ruxer, Karl-Heinz Scheunemann, Anusch Peyman, Gerhard Breipohl, Thomas R. Gadek, Volkmar Wehner, Jean-Francois Gourvest, and Sarah C. Bodary

Subjects

Steric effects, chemistry.chemical_classification, Scaffold, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, Hydantoin, Peptide, Biochemistry, Chemical synthesis, In vitro, chemistry.chemical_compound, Drug Discovery, Side chain, Molecular Medicine, Selectivity, Molecular Biology

Abstract

The synthesis of a series of RGD mimetic α V β 3 antagonists containing a hydantoin scaffold is shown. The results demonstrate some of the structural requirements for the design of selective α V β 3 antagonists (vs α IIb β 3 ) in terms of the Arg-mimetic, the distance between N- and C-terminus and the lipophilic side chain.

Published

2000

8. Kistrin Inhibits Human Smooth Muscle Cell Interaction with Fibrin

Author

Yuji Ikari, Karen O. Yee, Stephen M. Schwartz, and Sarah C. Bodary

Subjects

Integrins, Disintegrins, Cell, Integrin, Peptides, Cyclic, Fibrin, Fibrinolytic Agents, Cell Movement, In vivo, Cell Adhesion, medicine, Disintegrin, Humans, Blood Coagulation, Aorta, biology, Infant, Newborn, Muscle, Smooth, Hematology, Cell biology, Fibronectin, medicine.anatomical_structure, Biochemistry, Cell culture, Snake venom, Sulfoxides, biology.protein, Peptides, Oligopeptides, Platelet Aggregation Inhibitors

Abstract

Because of the lack of function-blocking anti-integrin antibodies that react with nonprimate species, the study of the role of integrins in in vivo animal models of atherosclerosis has been limited. In contrast, peptides or small molecules have shown less species specificity and thus may be better tools to use. In an attempt to identify integrin antagonists of potential use against smooth muscle response to injury, we investigated the role of human smooth muscle cell interactions with fibrin by using a panel of integrin antagonists consisting of the snake venom disintegrin, Kistrin, as well as cyclic peptides with well-defined integrin antagonists activities. We demonstrate that Kistrin, a disintegrin that inhibits beta1, beta2, beta3, and beta5 integrin interactions, had the most potent inhibitory effect. Based on our results, Kistrin or peptides with similar pan-integrin selectivity patterns are prime candidates for use as anti-integrin antagonists in further studies of atherosclerosis and restenosis.

Published

2000

9. Characterization of a candidate Borrelia burgdorferi beta3-chain integrin ligand identified using a phage display library

Author

Wambui Chege, Jenifer Coburn, Sarah C. Bodary, John M. Leong, and Loranne Magoun

Subjects

Phage display, Monosaccharide Transport Proteins, Recombinant Fusion Proteins, Integrin, Porins, Platelet Membrane Glycoproteins, Biology, Ligands, medicine.disease_cause, Microbiology, Bacterial Adhesion, Maltose-Binding Proteins, Cell Line, law.invention, Bacterial Proteins, Borrelia burgdorferi Group, Antigens, CD, Peptide Library, law, Escherichia coli, medicine, Humans, Borrelia burgdorferi, Molecular Biology, Escherichia coli Proteins, Integrin beta3, Transfection, bacterial infections and mycoses, Ligand (biochemistry), biology.organism_classification, Molecular biology, Cell culture, Recombinant DNA, biology.protein, ATP-Binding Cassette Transporters, Carrier Proteins

Abstract

The spirochaetal agents of Lyme disease, Borrelia burgdorferi (sensu lato) bind to integrins alphaIIbbeta3, alphavbeta3 and alpha5beta1 in purified form and on the surfaces of human cells. Using a phage display library of B. burgdorferi (sensu stricto) DNA, a candidate ligand for beta3-chain integrins was identified. The native B. burgdorferi protein, termed p66, is known to be recognized by human Lyme disease patient sera and to be expressed on the surface of the spirochaete. We show here that recombinant p66 binds specifically to beta3-chain integrins and inhibits attachment of intact B. burgdorferi to the same integrins. When expressed on the surface of Escherichia coli, this protein increases the attachment of E. coli to a transfected cell line that expresses alphavbeta3, but not to the parental cell line, which expresses no beta3-chain integrins. Localization of p66 on the surface of B. burgdorferi, the ability of recombinant forms of the protein to bind to beta3-chain integrins and the fact that p66 and B. burgdorferi bind to beta3-chain integrins in a mutually exclusive manner make p66 an attractive candidate bacterial ligand for integrins alphaIIbbeta3 and alphavbeta3.

Published

1999

10. A natural variant of the cysteine protease virulence factor of group A Streptococcus with an arginine-glycine-aspartic acid (RGD) motif preferentially binds human integrins α v β 3 and α IIb β 3

Author

Sarah Renish, Jenifer Coburn, Kathryn E. Stockbauer, Mengyao Liu, Eugene H. Burns, Siddeswar Gubba, Sarah C. Bodary, Loranne Magoun, James M. Musser, John M. Leong, Elizabeth Baker, and Xi Pan

Subjects

Multidisciplinary, Integrin, Virulence, Fibrinogen binding, Biology, medicine.disease_cause, Molecular biology, Virulence factor, Platelet Glycoprotein GPIIb-IIIa Complex, Streptococcus pyogenes, biology.protein, medicine, Vitronectin, RGD motif

Abstract

The human pathogenic bacterium group A Streptococcus produces an extracellular cysteine protease [streptococcal pyrogenic exotoxin B (SpeB)] that is a critical virulence factor for invasive disease episodes. Sequence analysis of the speB gene from 200 group A Streptococcus isolates collected worldwide identified three main mature SpeB (mSpeB) variants. One of these variants (mSpeB2) contains an Arg-Gly-Asp (RGD) sequence, a tripeptide motif that is commonly recognized by integrin receptors. mSpeB2 is made by all isolates of the unusually virulent serotype M1 and several other geographically widespread clones that frequently cause invasive infections. Only the mSpeB2 variant bound to transfected cells expressing integrin α v β 3 (also known as the vitronectin receptor) or α IIb β 3 (platelet glycoprotein IIb-IIIa), and binding was blocked by a mAb that recognizes the streptococcal protease RGD motif region. In addition, mSpeB2 bound purified platelet integrin α IIb β 3 . Defined β 3 mutants that are altered for fibrinogen binding were defective for SpeB binding. Synthetic peptides with the mSpeB2 RGD motif, but not the RSD sequence present in other mSpeB variants, blocked binding of mSpeB2 to transfected cells expressing α v β 3 and caused detachment of cultured human umbilical vein endothelial cells. The results ( i ) identify a Gram-positive virulence factor that directly binds integrins, ( ii ) identify naturally occurring variants of a documented Gram-positive virulence factor with biomedically relevant differences in their interactions with host cells, and ( iii ) add to the theme that subtle natural variation in microbial virulence factor structure alters the character of host-pathogen interactions.

Published

1999

11. Integrins α v β 3 and α 5 β 1 Mediate Attachment of Lyme Disease Spirochetes to Human Cells

Author

John M. Leong, Sarah C. Bodary, Jenifer Coburn, and Loranne Magoun

Subjects

Immunology, Integrin, Spirochaetaceae, Microbiology, Bacterial Adhesion, Cell Line, Receptors, Fibronectin, Lyme disease, Borrelia burgdorferi Group, medicine, Humans, Receptors, Vitronectin, Borrelia burgdorferi, biology, Cell adhesion molecule, bacterial infections and mycoses, biology.organism_classification, medicine.disease, Virology, Fibronectin, Infectious Diseases, Molecular and Cellular Pathogenesis, biology.protein, Parasitology, Vitronectin, Antibody

Abstract

Borrelia burgdorferi (sensu lato), the agent of Lyme disease, is able to cause chronic, multisystemic infections in human and animal hosts. Attachment of the spirochete to host cells is likely to be important for the colonization of diverse tissues. The platelet-specific integrin α IIb β 3 was previously identified as a receptor for all three species of Lyme disease spirochetes ( B. burgdorferi sensu stricto, B. garinii , and B. afzelii ). Here we show that B. burgdorferi also recognizes the widely expressed integrins α v β 3 and α 5 β 1 , known as the vitronectin and fibronectin receptors, respectively. Three representatives of each species of Lyme disease spirochete were tested for the ability to bind to purified α v β 3 and α 5 β 1 . All of the strains tested bound to at least one integrin. Binding to one integrin was not always predictive of binding to other integrins, and several different integrin preference profiles were identified. Attachment of the infectious B. burgdorferi strain N40 to purified α v β 3 and α 5 β 1 was inhibited by RGD peptides and the appropriate receptor-specific antibodies. Binding to α v β 3 was also shown by using a transfected cell line that expresses this receptor but not α IIb β 3 . Attachment of B. burgdorferi N40 to human erythroleukemia cells and to human saphenous vein endothelial cells was mediated by both α 5 β 1 and α v β 3 . Our results show that multiple integrins mediate attachment of Lyme disease spirochetes to host cells.

Published

1998

12. Blocking Monoclonal Antibodies to αVβ3 Integrin: A Unique Epitope of αVβ3 Integrin Is Present on Human Osteoclasts

Author

K. Jin Kim, Anan Chuntharapai, Sarah C. Bodary, and Michael A. Horton

Subjects

chemistry.chemical_classification, medicine.drug_class, Integrin, Fibrinogen binding, Cell Biology, Biology, Monoclonal antibody, Molecular biology, Epitope, Epitope mapping, chemistry, biology.protein, medicine, Vitronectin, Cell adhesion, Glycoprotein

Abstract

Integrins are a family of cell surface glycoproteins that promote cell adhesion. The integrin αVβ3, vitronectin receptor, is a major integrin expressed by osteoclasts. To further investigate the role of αVβ3 in cell adhesion, we generated and characterized monoclonal antibodies to αVβ3 by immunizing BALB/c mice with purified αVβ3 protein. Three monoclonal antibodies (mAbs), 9D4.9.1, 9G2.1.3, and 10C4.1.3, from a total of more than 1100 positive cultures which bound αVβ3, were characterized extensively: mAbs 9G2.1.3 and 10C4.1.3 recognize the αVβ3 complex whereas mAb 9D4.9.1 reacts with the β3-chain shared between the αVβ3 complex and gpIIbIIIa. Further epitope mapping using flow microfluorometry analysis and histochemical staining of various tissues showed that 9D4.9.1 and 10C4.1.3 recognized distinct epitopes. Ligand-binding studies using cell-bound and purified αVβ3 demonstrated that all three mAbs blocked fibrinogen binding. Vitronectin binding was blocked by mAb 9D4.9.1 and, less effectively, by mAb 10C4.1.3; mAb 9G2.1.3 was without effect. All three mAbs recognized osteoclasts from human tissues; mAb 9G2.1.3 also stained osteoclasts from a wide range of nonhuman species. Monoclonal antibodies 9D4.9.1 and 9G2.1.3 bound to a panel of cultured cell lines and various tissues. In contrast, mAb 10C4.1.3 bound only weakly or not at all to tissues expressing αVβ3 with the exception of osteoclasts. Thus, mAb 10C4.1.3 showed a very narrow tissue specificity being restricted to high-level expression on human osteoclasts.

Published

1993

13. cDNA sequence of the human integrin beta 5 subunit

Author

David A. Cheresh, D J Vestal, Sarah C. Bodary, and J. W. McLean

Subjects

Alpha-v beta-3, Retinoic acid receptor beta, Cell Biology, Biology, TGF beta receptor 2, Biochemistry, Molecular biology, Interleukin 10 receptor, alpha subunit, chemistry.chemical_compound, chemistry, Integrin alpha M, biology.protein, Integrin, beta 6, Molecular Biology, Interleukin 12 receptor, beta 1 subunit, G alpha subunit

Abstract

A novel integrin receptor involved in cell adhesion to the matrix protein vitronectin has recently been described from a human lung epithelial-derived cell line (Cheresh, D. A., Smith, J. W., Cooper, H. M., and Quaranta, V. (1989) Cell 57, 59-69). This receptor has an alpha subunit that appears identical to the alpha v of the vitronectin receptor alpha v beta 3 expressed in melanoma and endothelial cells, but is complexed with a distinct beta subunit, beta 5. cDNA clones coding for beta 5 have been isolated and used to determine the mRNA and amino acid sequence of this new subunit. A 3.3-kilobase mRNA was found to code for a mature protein of 775 amino acid residues with a hydrophobic leader sequence of 24 amino acids. A 56% identity was found between the beta 5 and beta 3 protein sequences, making them the most closely related of the integrin beta subunits. Polymerase chain reaction abundance analysis revealed that alpha v and beta 5 mRNAs were found in seven very different cell lines, compared with beta 3 mRNA which was found in only three of the them, indicating that this new integrin receptor may be widely distributed.

Published

1990

14. The integrin beta 1 subunit associates with the vitronectin receptor alpha v subunit to form a novel vitronectin receptor in a human embryonic kidney cell line

Author

Sarah C. Bodary and John W. McLean

Subjects

biology, Alpha-v beta-5, Integrin, Interleukin 5 receptor alpha subunit, Cell Biology, Biochemistry, Molecular biology, Interleukin 10 receptor, alpha subunit, Fibronectin, chemistry.chemical_compound, chemistry, Laminin, biology.protein, Vitronectin, Integrin, beta 6, Molecular Biology

Abstract

We describe a novel integrin heterodimer on the surface of the human embryonic kidney cell line 293. This receptor is comprised of alpha v and beta 1 subunits, each of which has been previously found in association with other integrin subunits. This alpha v.beta 1 complex was identified as the predominant vitronectin receptor (VnR) on the surface of 293 cells by immunoprecipitation with antibodies raised against the alpha v subunit. Polymerase chain reaction analysis detected mRNAs for alpha v and beta 1 subunits while no evidence was obtained for beta 2, beta 3, or alpha IIb integrin subunit mRNA. Immunoprecipitation of surface-iodinated proteins with antibodies to alpha v gave bands of 150 and 120 kDa. The 120-kDa band reacted with antibodies to beta 1 in immunoblotting experiments. 293 cells adhere to vitronectin, fibronectin, laminin, and collagen IV, while von Willebrand factor and fibrinogen, known ligands of the VnR (alpha v.beta 3), did not support adhesion. A polyclonal antibody directed against both subunits of the VnR (alpha v, beta 3) inhibits attachment of 293 cells to vitronectin but not to other adhesive proteins. A beta 1-specific monoclonal inhibited attachment to fibronectin, laminin, and collagen IV, known ligands of beta 1 integrins, as well as vitronectin. This novel (alpha v. beta 1) VnR thus appears to mediate cell adhesion exclusively to vitronectin, in contrast to previously described VnRs which have multiple ligands.

Published

1990

15. Competition between intercellular adhesion molecule-1 and a small-molecule antagonist for a common binding site on the alphal subunit of lymphocyte function-associated antigen-1

Author

Lisa D. Stefanich, Kevin R Clark, Thomas R. Gadek, Maureen Beresini, Susan M. Keating, Caroline P. Edwards, Fred Arellano, Sarah C. Bodary, Steven A. Spencer, and James C. Marsters

Subjects

Recombinant Fusion Proteins, Allosteric regulation, Enzyme-Linked Immunosorbent Assay, Kidney, Ligands, Biochemistry, Binding, Competitive, Article, Allosteric Regulation, Humans, Lymphocyte function-associated antigen 1, Binding site, Molecular Biology, Binding Sites, Photoaffinity labeling, Chemistry, Cooperative binding, Kidney metabolism, Intercellular Adhesion Molecule-1, Small molecule, Lymphocyte Function-Associated Antigen-1, Peptide Fragments, Protein Structure, Tertiary, Protein Subunits, Cross-Linking Reagents, Immunoglobulin G, Biophysics, Binding domain

Abstract

The lymphocyte function-associated antigen-1 (LFA-1) binding of a unique class of small-molecule antagonists as represented by compound 3 was analyzed in comparison to that of soluble intercellular adhesion molecule-1 (sICAM-1) and A-286982, which respectively define direct and allosteric competitive binding sites within LFA-1's inserted (I) domain. All three molecules antagonized LFA-1 binding to ICAM-1-Immunoglobulin G fusion (ICAM-1-Ig) in a competition ELISA, but only compound 3 and sICAM-1 inhibited the binding of a fluorescein-labeled analog of compound 3 to LFA-1. Compound 3 and sICAM-1 displayed classical direct competitive binding behavior with ICAM-1. Their antagonism of LFA-1 was surmountable by both ICAM-1-Ig and a fluorescein-labeled compound 3 analog. The competition of both sICAM-1 and compound 3 with ICAM-1-Ig for LFA-1 resulted in equivalent and linear Schild plots with slopes of 1.24 and 1.26, respectively. Cross-linking studies with a photoactivated analog of compound 3 localized the high-affinity small-molecule binding site to the N-terminal 507 amino acid segment of the alpha chain of LFA-1, a region that includes the I domain. In addition, cells transfected with a variant of LFA-1 lacking this I domain showed no significant binding of a fluorescein-labeled analog of compound 3 or ICAM-1-Ig. These results demonstrate that compound 3 inhibits the LFA-1/ICAM-1 binding interaction in a directly competitive manner by binding to a high-affinity site on LFA-1. This binding site overlaps with the ICAM-1 binding site on the alpha subunit of LFA-1, which has previously been localized to the I domain.

Published

2005

16. Adhesion molecules as therapeutic targets for autoimmune diseases and transplant rejection

Author

Marvin R. Garovoy, Sarah C. Bodary, and Russell L. Dedrick

Subjects

Pharmacology, Autoimmune disease, Graft Rejection, Cell adhesion molecule, Clinical Biochemistry, Soluble cell adhesion molecules, Inflammation, Biology, medicine.disease, Intercellular adhesion molecule, Transplant rejection, Autoimmune Diseases, Biological Therapy, Immune system, Drug Delivery Systems, Drug Discovery, Immunology, medicine, Animals, Humans, medicine.symptom, Cell adhesion, Cell Adhesion Molecules

Abstract

Inflammatory disorders such as autoimmune diseases and graft rejection are mediated by activated leukocytes, particularly T lymphocytes, which penetrate the inflamed tissue and perpetuate or amplify the immune reaction. In an unstimulated state, leukocytes do not readily adhere to the vascular endothelium. However, inflammatory signals induce the expression of proteins on the endothelial cell surface that promote the adhesion and extravasation of activated immune cells from the circulation into the underlying tissues. Key among these molecules are P- and E-selectin, intercellular adhesion molecule-1 (ICAM-1) and vascular cell adhesion molecule-1 (VCAM-1) on the endothelial cells, and their respective counter receptors, P-selectin glycoprotein ligand-1 (PSGL-1), leukocyte function-associated antigen-1 (LFA-1) and very late antigen-4 (VLA-4), on the leukocytes. In vitro blockade of these molecules inhibits the adhesion of leukocytes. In many cases there is attenuation of leukocyte activation as well. Adhesion blockade in animal models prevents or ameliorates graft rejection and disease severity in autoimmune models. Clinical studies with humanised monoclonal antibodies which interfere with LFA-1/ICAM-1 or VLA-4/VCAM-1 interactions have shown significant efficacy and good safety profiles in autoimmune disease, including psoriasis, multiple sclerosis and inflammatory bowel disease. Thus, adhesion blockade is emerging as a useful therapeutic strategy in several inflammatory settings.

Published

2003

17. Anti-CD11a ameliorates disease in the human psoriatic skin-SCID mouse transplant model: comparison of antibody to CD11a with Cyclosporin A and clobetasol propionate

Author

James Varani, Yiqing Chi, Daniel Tumas, Mary E. Zeigler, Sarah C. Bodary, and Haicheng Tang

Subjects

Pathology, medicine.medical_specialty, medicine.drug_class, medicine.medical_treatment, Administration, Topical, Transplantation, Heterologous, Anti-Inflammatory Agents, Human skin, Mice, SCID, Pathology and Forensic Medicine, Mice, Reference Values, Cyclosporin a, Psoriasis, medicine, Animals, Humans, Molecular Biology, Glucocorticoids, Skin, Severe combined immunodeficiency, Clobetasol, integumentary system, business.industry, Antibodies, Monoclonal, Cell Biology, Immunotherapy, Skin Transplantation, medicine.disease, Lymphocyte Function-Associated Antigen-1, Transplantation, Immunology, Cyclosporine, Corticosteroid, Dermatologic Agents, Clobetasol propionate, business, medicine.drug

Abstract

The present study assesses the applicability of human skin–SCID (severe combined immunodeficiency) mouse chimeras in testing antipsoriatic therapeutics. Three agents were examined: (1) a monoclonal antibody to the alpha subunit of leukocyte function associated antigen-1 integrin (CD11a); (2) Cyclosporin A; and (3) clobetasol propionate (Temovate), a potent topical corticosteroid used clinically in the treatment of psoriasis. Skin transplanted to SCID mice from normal human volunteers or from psoriatic lesional skin was allowed to heal for 3 to 5 weeks before application of test reagents. During this period, psoriatic skin, which was 3.8-fold thicker than the corresponding normal skin before transplantation, maintained its phenotype (ie, increased epidermal thickness, rete ridges with blunted ends, and intralesional presence of T lymphocytes). Transplanted normal human skin, however, underwent a hyperplastic response during this period, resulting in a 2.4-fold increase in epidermal thickness. After the healing period, animals transplanted with normal or psoriatic skin were treated for 14 days by daily intraperitoneal injection of either Cyclosporin A or a monoclonal antibody to human CD11a, or by topical application of clobetasol propionate. At the end of the treatment period, the mice were killed and the tissue evaluated morphometrically for changes in epidermal thickness and immunohistologically for the presence of T lymphocytes. Both Cyclosporin A and anti-CD11a reduced the epidermal thickness of transplanted psoriatic skin, whereas neither reagent significantly reduced the thickness of transplanted normal skin. T lymphocytes were detected in the skin from treated animals; there did not seem to be any reduction in the number of T lymphocytes. Clobetasol propionate reduced the epidermal thickness of both normal and psoriatic skin. These data indicate that, in this model, therapies directed against pathophysiologic mechanisms that contribute to psoriasis can be distinguished from treatments that block epidermal hyperplasia occurring as a consequence of xenografting. Our observations provide evidence for the activity of anti-CD11a in an animal model of human psoriasis.

Published

2001

18. Putting the pieces together: contribution of fluorescence polarization assays to small-molecule lead optimization

Author

Susan M. Keating, Kim Zioncheck, Fred Arellano, Sarah C. Bodary, Jim Marsters, Carmen Ladner, Kevin R Clark, and Maureen Beresini

Subjects

chemistry.chemical_compound, chemistry, Biochemistry, Ligand binding assay, Fluorescein, Receptor, Fluorescein isothiocyanate, Ligand (biochemistry), Small molecule, Fluorescence, Fluorescence anisotropy

Abstract

Fluorescence polarization assays with both purified receptor and intact cells have been developed to assess potency and selectivity of antagonists of the interaction of the lymphocyte receptor, LFA-1, and its endothelial ligand, ICAM-1. Fluorescein isothiocyanate conjugated small molecule probes were optimized for use in binding assay with LFA-1 and a closely related receptor, MAC-1. In the assays, the antagonists compete with the fluorescent probe for binding to the receptor. This enables the determination of IC50 and consequently Ki values of the antagonists for each of the receptors. Routine use of polarization assay with tranfected cells, in addition to purified receptors, has become feasible with the availability of sensitive plate readers that are able to detect 1 nM fluorescent probe in 15 (mu) l sample volumes with good signal to noise. These measurements aid in the iterative synthesis of more potent and selective compounds.© (2000) COPYRIGHT SPIE--The International Society for Optical Engineering. Downloading of the abstract is permitted for personal use only.

Published

2000

19. Identification of the binding site in intercellular adhesion molecule 1 for its receptor, leukocyte function-associated antigen 1

Author

L G Presta, Sarah C. Bodary, L Riddle, J Lu, Karen L. Fisher, and K J Kim

Subjects

Models, Molecular, medicine.drug_class, Complement receptor 1, Integrin, Intercellular Adhesion Molecule-1, Vascular Cell Adhesion Molecule-1, chemical and pharmacologic phenomena, Plasma protein binding, Monoclonal antibody, Mice, medicine, Animals, Humans, Lymphocyte function-associated antigen 1, Binding site, Cell adhesion, Molecular Biology, Binding Sites, biology, Antibodies, Monoclonal, hemic and immune systems, Cell Biology, Molecular biology, Lymphocyte Function-Associated Antigen-1, Recombinant Proteins, Protein Structure, Tertiary, biology.protein, Mutagenesis, Site-Directed, Binding Sites, Antibody, biology.gene, Research Article, Protein Binding

Abstract

Intercellular adhesion molecule 1 (ICAM-1, CD54) is a member of the Ig superfamily and is a counterreceptor for the beta 2 integrins: lymphocyte function-associated antigen 1 (LFA-1, CD11a/CD18), complement receptor 1 (MAC-1, CD11b/CD18), and p150,95 (CD11c/CD18). Binding of ICAM-1 to these receptors mediates leukocyte-adhesive functions in immune and inflammatory responses. In this report, we describe a cell-free assay using purified recombinant extracellular domains of LFA-1 and a dimeric immunoadhesin of ICAM-1. The binding of recombinant secreted LFA-1 to ICAM-1 is divalent cation dependent (Mg2+ and Mn2+ promote binding) and sensitive to inhibition by antibodies that block LFA-1-mediated cell adhesion, indicating that its conformation mimics that of LFA-1 on activated lymphocytes. We describe six novel anti-ICAM-1 monoclonal antibodies, two of which are function blocking. Thirty-five point mutants of the ICAM-1 immunoadhesin were generated and residues important for binding of monoclonal antibodies and purified LFA-1 were identified. Nineteen of these mutants bind recombinant LFA-1 equivalently to wild type. Sixteen mutants show a 66-2500-fold decrease in LFA-1 binding yet, with few exceptions, retain binding to the monoclonal antibodies. These mutants, along with modeling studies, define the LFA-1 binding site on ICAM-1 as residues E34, K39, M64, Y66, N68, and Q73, that are predicted to lie on the CDFG beta-sheet of the Ig fold. The mutant G32A also abrogates binding to LFA-1 while retaining binding to all of the antibodies, possibly indicating a direct interaction of this residue with LFA-1. These data have allowed the generation of a highly refined model of the LFA-1 binding site of ICAM-1.

Published

1997

20. Regulation of integrin function by the urokinase receptor

Author

Michael Doyle, Daniel I. Simon, Ying Wei, Steven Rosenberg, Sarah C. Bodary, Matvey Lukashev, and Harold A. Chapman

Subjects

Integrins, Glycosylphosphatidylinositols, Recombinant Fusion Proteins, Integrin, Molecular Sequence Data, Receptors, Cell Surface, Receptors, Cytoadhesin, Ligands, Transfection, Collagen receptor, Cell Line, Receptors, Urokinase Plasminogen Activator, Cell surface receptor, Cell Adhesion, Humans, Amino Acid Sequence, Vitronectin, skin and connective tissue diseases, Cell adhesion, neoplasms, Multidisciplinary, biology, Chemistry, Integrin beta1, Molecular biology, Urokinase-Type Plasminogen Activator, biological factors, Cell biology, Fibronectins, Urokinase receptor, enzymes and coenzymes (carbohydrates), Integrin alpha M, CD18 Antigens, biology.protein, Integrin, beta 6, biological phenomena, cell phenomena, and immunity

Abstract

Integrin function is central to inflammation, immunity, and tumor progression. The urokinase-type plasminogen activator receptor (uPAR) and integrins formed stable complexes that both inhibited native integrin adhesive function and promoted adhesion to vitronectin via a ligand binding site on uPAR. Interaction of soluble uPAR with the active conformer of integrins mimicked the inhibitory effects of membrane uPAR. Both uPAR-mediated adhesion and altered integrin function were blocked by a peptide that bound to uPAR and disrupted complexes. These data provide a paradigm for regulation of integrins in which a nonintegrin membrane receptor interacts with and modifies the function of activated integrins.

Published

1996

21. Antibodies that selectively inhibit leukocyte function-associated antigen 1 binding to intercellular adhesion molecule-3 recognize a unique epitope within the CD11a I domain

Author

Caroline P. Edwards, Mark Champe, Phillip W. Berman, L. G. Presta, M.E. Binnerts, Sarah C. Bodary, Y. van Kooyk, Carl G. Figdor, Molecular cell biology and Immunology, AII - Cancer immunology, and CCA - Cancer biology and immunology

Subjects

Molecular Sequence Data, chemical and pharmacologic phenomena, Plasma protein binding, Biology, Biochemistry, Epitope, Antigen-Antibody Reactions, Mice, Antibody Specificity, Antigens, CD, Cell Adhesion, Animals, Humans, Amino Acid Sequence, Binding site, Cell adhesion, Molecular Biology, Cell adhesion molecule, Antibodies, Monoclonal, hemic and immune systems, Cell Biology, Ligand (biochemistry), Intercellular adhesion molecule, Molecular biology, Antigens, Differentiation, Lymphocyte Function-Associated Antigen-1, Protein Structure, Tertiary, Enzyme Activation, Epitope mapping, Cell Adhesion Molecules, Epitope Mapping, Protein Binding

Abstract

Several studies indicate that the I domain located in the a chain (CD11a) of leukocyte function-associated antigen-1 (LFA-1; CD11a/CD18) plays an essential role in ligand recognition. We recently identified three distinct epitopes (IdeA, IdeB, and IdeC) within the CD11a I domain, recognized by antibodies that block binding of LFA-1 to intercellular adhesion molecules (ICAM) 1, 2, and 3. In the present study, we used a series of human/murine CD11a I domain chimeras, to localize a fourth I domain epitope (IdeD), recognized by three independently derived anti-CD11a antibodies that selectively block the binding of LFA-1 to ICAM-3, but not to ICAM-1. The IdeD epitope depended on human CD11a residues Asp182 and Ser184 and was not present in CD11b or CD11c. Although mutation of Asp182 and Ser184 failed to abolish ICAM-3 adhesion of LFA-1 transfectants, alignment of these residues with the crystal structure of the CD11a I domain suggested that the IdeD epitope is located in close proximity to residues (Ile126 and Asn129) recently implicated in the ICAM-3 binding site (1). Interestingly, the IdeB and IdeC epitopes appeared to be in close proximity of a divalent cation binding pocket within the CD11a I domain that regulates both ICAM-1 and ICAM-3 adhesion. Taken together, these data indicate that distinct regions of the CD11a I domain contain epitopes for antibodies that either selectively inhibit binding of LFA-1 to ICAM-3, or interfere with both ICAM- 1 and ICAM-3 binding of LFA-1.

Published

1996

22. Identification of amino acids in the CD11a I-domain important for binding of the leukocyte function-associated antigen-1 (LFA-1) to intercellular adhesion molecule-1 (ICAM-1)

Author

Phillip W. Berman, Mark Champe, Leonard G. Presta, Mary Ellen Wessinger, Tania Gonzalez, Caroline P. Edwards, Steven A. Spencer, and Sarah C. Bodary

Subjects

Recombinant Fusion Proteins, Intercellular Adhesion Molecule-1, DNA Mutational Analysis, Magnesium Chloride, chemical and pharmacologic phenomena, Plasma protein binding, Biology, Ligands, Biochemistry, Epitope, Epitopes, Mice, Structure-Activity Relationship, Chlorides, Species Specificity, Cell Adhesion, Animals, Humans, Point Mutation, Lymphocyte function-associated antigen 1, Cell adhesion, Molecular Biology, G alpha subunit, Alanine, chemistry.chemical_classification, hemic and immune systems, Cell Biology, Molecular biology, Lymphocyte Function-Associated Antigen-1, Amino acid, chemistry, Manganese Compounds, Protein Binding

Abstract

Leukocyte function-associated antigen-1 (LFA-1) is a cell surface adhesion receptor for intercellular adhesion molecule-1, -2, and -3 (ICAM-1, -2, -3). Using human/murine chimeras of the I-domain of the LFA-1 alpha subunit (CD11a), we recently identified the epitopes recognized by eight monoclonal antibodies against CD11a that inhibit LFA-1 binding to ICAM-1. In this report, we determined that replacement of the entire human I-domain with the entire murine I-domain in CD11a completely abrogated LFA-1 binding to human ICAM-1 without affecting the gross conformation or heterodimer formation of LFA-1, as assayed by antibody binding. In order to assess which residues of the I-domain are responsible for binding to ICAM-1, we tested the ability of a panel of human/murine I-domain chimeras to bind to human ICAM-1. When complexed with CD18, all CD11a chimeras bound ICAM-1 at levels comparable to wild-type CD11a/CD18, indicating that the residues in these chimeras which differ in human and murine I-domains may not play a critical role in LFA-1 binding to ICAM-1. A series of point mutations of residues that are conserved between murine and human CD11a I-domains, as well as between CD11b and CD11c, were also generated. Substitution of alanine for proline at position 192 in the human CD11a I-domain abrogated adhesion of LFA-1 to ICAM-1. Antibody binding data suggested that this was due to conformational changes within the I-domain. Mutation of the aspartic acids at positions 137 and 239 to either alanine or lysine completely destroyed ICAM-1 binding. The conformation of LFA-1 alanine mutants was not significantly altered. This suggests that these aspartic acids are required for binding of human LFA-1 to human ICAM-1.

Published

1996

23. Expression of recombinant platelet glycoprotein IIbIIIa results in a functional fibrinogen-binding complex

Author

Sarah C. Bodary, John W. McLean, and Mary A. Napier

Subjects

Receptor complex, biology, Protein subunit, Integrin, Fibrinogen binding, Cell Biology, Transfection, Platelet membrane glycoprotein, Biochemistry, Molecular biology, Cell surface receptor, hemic and lymphatic diseases, biology.protein, Vitronectin, Molecular Biology

Abstract

The ability of cDNAs encoding the human platelet glycoprotein IIbIIIa to be expressed and assembled into a functional integrin receptor was assessed by transient transfection into a human cell line. Transfection of full length cDNAs resulted in synthesis of high levels of integrin subunits which appear to be stable within the cell for several days. Coexpression of both subunits resulted in a proteolytically processed form of GPIIb that associated with GPIIIa as a heterodimeric complex as the cell surface. Transport to the cell surface required association of these subunits with each other or with endogenous integrin subunits. When expressed alone, the GPIIb subunit remained intracellular, while the GPIIIa subunit was found to complex with endogenous proteins and was mobilized to the cell surface. The GPIIbIIIa receptor complex facilitated attachment of cells to known ligands for GPIIbIIIa: fibrinogen, vitronectin, and von Willebrand factor. This adhesion was sensitive to inhibition by the peptide GRGDV and the monoclonal antibody AP2, known inhibitors of platelet aggregation

Published

1989

24. Regulation of nerve growth factor mRNA levels in developing rat heart ventricle is not altered by sympathectomy

Author

Louis F. Reichardt, Dennis O. Clegg, Thomas H. Large, and Sarah C. Bodary

Subjects

Male, Sympathetic nervous system, medicine.medical_specialty, Aging, Sympathetic Nervous System, medicine.medical_treatment, Heart Ventricles, Biology, Substance P, chemistry.chemical_compound, Norepinephrine, Hydroxydopamines, Internal medicine, medicine, Animals, Nerve Growth Factors, RNA, Messenger, Oxidopamine, Molecular Biology, Neurons, Heart development, Sympathectomy, Chemical, Heart, Rats, Inbred Strains, Cell Biology, Rats, Autonomic nervous system, Nerve growth factor, medicine.anatomical_structure, Endocrinology, nervous system, chemistry, Sympathectomy, Female, Neuron, Developmental Biology, medicine.drug

Abstract

The survival of sympathetic and sensory neurons is known to be controlled by nerve growth factor (NGF) supplied by the targets of innervation, yet little is known about how target NGF synthesis is regulated. We have investigated the pattern of NGF mRNA expression in developing rat heart ventricle using a sensitive RNA blotting procedure. We find that the concentration of NGF mRNA increases steadily from Embryonic Day 17 to peak levels at 10-14 days postnatal and then declines about twofold and stabilizes at the level found in adults. The rise in NGF mRNA concentration correlates with the arrival and differentiation of sympathetic nerve terminals in the heart and the cessation of sympathetic cell death. To assess the role of innervating sympathetic neurons in regulating NGF mRNA expression, neonatal rats were sympathectomized by treatment with 6-hydroxydopamine and heart ventricles were assayed for NGF message. Although this treatment reduced ventricle norepinephrine content by 82%, no significant change in NGF mRNA concentration was observed. These results suggest that the developmental program of NGF mRNA production in the heart is not influenced by innervating sympathetic neurons.

Published

1989