Your search keyword '"Gundlach CW 4th"' showing total 4 results

1. Identification of Inhibitors of Integrin Cytoplasmic Domain Interactions With Syk.

Author

Bakthavatsalam D, Craft JW Jr, Kazansky A, Nguyen N, Bae G, Caivano AR, Gundlach CW 4th, Aslam A, Ali S, Gupta S, Lin SY, Parthiban HD, Vanderslice P, Stephan CC, and Woodside DG

Subjects

Anti-Inflammatory Agents chemistry, Cefsulodin chemistry, Ceftazidime chemistry, High-Throughput Screening Assays, Humans, Integrin beta Chains chemistry, Integrin beta Chains metabolism, Leukocytes enzymology, Male, Phosphorylation, Protein Binding, Protein Interaction Domains and Motifs, Signal Transduction, Small Molecule Libraries, Syk Kinase chemistry, Syk Kinase metabolism, THP-1 Cells, Anti-Inflammatory Agents pharmacology, Cefsulodin pharmacology, Ceftazidime pharmacology, Integrin beta Chains drug effects, Leukocytes drug effects, Syk Kinase antagonists & inhibitors

Abstract

Leukocyte inflammatory responses require integrin cell-adhesion molecule signaling through spleen tyrosine kinase (Syk), a non-receptor kinase that binds directly to integrin β-chain cytoplasmic domains. Here, we developed a high-throughput screen to identify small molecule inhibitors of the Syk-integrin cytoplasmic domain interactions. Screening small molecule compound libraries identified the β-lactam antibiotics cefsulodin and ceftazidime, which inhibited integrin β-subunit cytoplasmic domain binding to the tandem SH2 domains of Syk (IC 50 range, 1.02-4.9 µM). Modeling suggested antagonist binding to Syk outside the pITAM binding site. Ceftazidime inhibited integrin signaling via Syk, including inhibition of adhesion-dependent upregulation of interleukin-1β and monocyte chemoattractant protein-1, but did not inhibit ITAM-dependent phosphorylation of Syk mediated by FcγRI signaling. Our results demonstrate a novel means to target Syk independent of its kinase and pITAM binding sites such that integrin signaling via this kinase is abrogated but ITAM-dependent signaling remains intact. As integrin signaling through Syk is essential for leukocyte activation, this may represent a novel approach to target inflammation., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Bakthavatsalam, Craft, Kazansky, Nguyen, Bae, Caivano, Gundlach, Aslam, Ali, Gupta, Lin, Parthiban, Vanderslice, Stephan and Woodside.)

Published

2021

2. Small molecule agonist of very late antigen-4 (VLA-4) integrin induces progenitor cell adhesion.

Author

Vanderslice P, Biediger RJ, Woodside DG, Brown WS, Khounlo S, Warier ND, Gundlach CW 4th, Caivano AR, Bornmann WG, Maxwell DS, McIntyre BW, Willerson JT, and Dixon RA

Subjects

CD11a Antigen genetics, CD11a Antigen metabolism, Cell Adhesion drug effects, Cell Adhesion physiology, Cell Movement physiology, Cell- and Tissue-Based Therapy methods, Chemokine CXCL12 genetics, Chemokine CXCL12 metabolism, Heterocyclic Compounds, 4 or More Rings chemistry, Human Umbilical Vein Endothelial Cells, Humans, Integrin alpha4beta1 genetics, Integrin alpha4beta1 metabolism, Integrin alpha5beta1 genetics, Integrin alpha5beta1 metabolism, Jurkat Cells, Stem Cells cytology, Vascular Cell Adhesion Molecule-1 genetics, Vascular Cell Adhesion Molecule-1 metabolism, Cell Movement drug effects, Heterocyclic Compounds, 4 or More Rings pharmacology, Integrin alpha4beta1 agonists, Models, Molecular, Stem Cells metabolism

Abstract

Activation of the integrin family of cell adhesion receptors on progenitor cells may be a viable approach to enhance the effects of stem cell-based therapies by improving cell retention and engraftment. Here, we describe the synthesis and characterization of the first small molecule agonist identified for the integrin α4β1 (also known as very late antigen-4 or VLA-4). The agonist, THI0019, was generated via two structural modifications to a previously identified α4β1 antagonist. THI0019 greatly enhanced the adhesion of cultured cell lines and primary progenitor cells to α4β1 ligands VCAM-1 and CS1 under both static and flow conditions. Furthermore, THI0019 facilitated the rolling and spreading of cells on VCAM-1 and the migration of cells toward SDF-1α. Molecular modeling predicted that the compound binds at the α/β subunit interface overlapping the ligand-binding site thus indicating that the compound must be displaced upon ligand binding. In support of this model, an analog of THI0019 modified to contain a photoreactive group was used to demonstrate that when cross-linked to the integrin, the compound behaves as an antagonist instead of an agonist. In addition, THI0019 showed cross-reactivity with the related integrin α4β7 as well as α5β1 and αLβ2. When cross-linked to αLβ2, the photoreactive analog of THI0019 remained an agonist, consistent with it binding at the α/β subunit interface and not at the ligand-binding site in the inserted ("I") domain of the αL subunit. Co-administering progenitor cells with a compound such as THI0019 may provide a mechanism for enhancing stem cell therapy.

Published

2013

3. Synthesis and evaluation of an anti-MLC1 × anti-CD90 bispecific antibody for targeting and retaining bone-marrow-derived multipotent stromal cells in infarcted myocardium.

Author

Gundlach CW 4th, Caivano A, Cabreira-Hansen Mda G, Gahremanpour A, Brown WS, Zheng Y, McIntyre BW, Willerson JT, Dixon RA, Perin EC, and Woodside DG

Subjects

Animals, Antibodies, Bispecific chemistry, Antibodies, Bispecific immunology, Bone Marrow Cells, Humans, Myocardial Infarction pathology, Myocardium, Swine, Antibodies, Bispecific therapeutic use, Molecular Targeted Therapy methods, Multipotent Stem Cells immunology, Myocardial Infarction drug therapy, Myosin Light Chains immunology, Stromal Cells immunology, Thy-1 Antigens immunology

Abstract

A key issue regarding the use of stem cells in cardiovascular regenerative medicine is their retention in target tissues. Here, we have generated and assessed a bispecific antibody heterodimer designed to improve the retention of bone-marrow-derived multipotent stromal cells (BMMSC) in cardiac tissue damaged by myocardial infarction. The heterodimer comprises an anti-human CD90 monoclonal antibody (mAb) (clone 5E10) and an anti-myosin light chain 1 (MLC1) mAb (clone MLM508) covalently cross-linked by a bis-arylhydrazone. We modified the anti-CD90 antibody with a pegylated-4-formylbenzamide moiety to a molar substitution ratio (MSR) of 2.6 and the anti-MLC1 antibody with a 6-hydrazinonicotinamide moiety to a MSR of 0.9. The covalent modifications had no significant deleterious effect on mAb epitope binding. Furthermore, the binding of anti-CD90 antibody to BMMSCs did not prevent their differentiation into adipo-, chondro-, or osteogenic lineages. Modified antibodies were combined under mild conditions (room temperature, pH 6, 1 h) in the presence of a catalyst (aniline) to allow for rapid generation of the covalent bis-arylhydrazone, which was monitored at A(354). We evaluated epitope immunoreactivity for each mAb in the construct. Flow cytometry demonstrated binding of the bispecific construct to BMMSCs that was competed by free anti-CD90 mAb, verifying that modification and cross-linking were not detrimental to the anti-CD90 complementarity-determining region. Similarly, ELISA-based assays demonstrated bispecific antibody binding to plastic-immobilized recombinant MLC1. Excess anti-MLC1 mAb competed for bispecific antibody binding. Finally, the anti-CD90 × anti-MLC1 bispecific antibody construct induced BMMSC adhesion to plastic-immobilized MLC1 that was resistant to shear stress, as measured in parallel-plate flow chamber assays. We used mAbs that bind both human antigens and the respective pig homologues. Thus, the anti-CD90 × anti-MLC1 bispecific antibody may be used in large animal studies of acute myocardial infarction and may provide a starting point for clinical studies.

Published

2011

4. The hairpin ribozyme substrate binding-domain: a highly constrained D-shaped conformation.

Author

Pinard R, Lambert D, Heckman JE, Esteban JA, Gundlach CW 4th, Hampel KJ, Glick GD, Walter NG, Major F, and Burke JM

Subjects

Base Sequence, Binding Sites, Catalysis, Computer Simulation, Cross-Linking Reagents chemistry, Models, Molecular, Molecular Sequence Data, RNA, Viral chemistry, RNA, Viral metabolism, Substrate Specificity, Nucleic Acid Conformation, RNA, Catalytic chemistry

Abstract

The two domains of the hairpin ribozyme-substrate complex, usually depicted as straight structural elements, must interact with one another in order to form an active conformation. Little is known about the internal geometry of the individual domains in an active docked complex. Using various crosslinking and structural approaches in conjunction with molecular modeling (constraint-satisfaction program MC-SYM), we have investigated the conformation of the substrate-binding domain in the context of the active docked ribozyme-substrate complex. The model generated by MC-SYM showed that the domain is not straight but adopts a bent conformation (D-shaped) in the docked state of the ribozyme, indicating that the two helices bounding the internal loop are closer than was previously assumed. This arrangement rationalizes the observed ability of hairpin ribozymes with a circularized substrate-binding strand to cleave a circular substrate, and provides essential information concerning the organization of the substrate in the active conformation. The internal geometry of the substrate-binding strand places G8 of the substrate-binding strand near the cleavage site, which has allowed us to predict the crucial role played by this nucleotide in the reaction chemistry., (Copyright 2001 Academic Press.)

Published

2001