Your search keyword '"Ying-Fon Chang"' showing total 4 results

1. Tenascin-C aptamers are generated using tumor cells and purified protein

Author

Paul Schmidt, Ty A. Gould, Chris Marion, Ying-Fon Chang, Steve Warren, Brian Hicke, David Parma, and Cynthia K. Lynott

Subjects

Aptamer, Oligonucleotides, Plasma protein binding, Ligands, Biochemistry, Mice, In vivo, Tumor Cells, Cultured, Animals, Humans, Molecular Biology, biology, Oligonucleotide, Tenascin C, Tenascin, Cell Biology, Surface Plasmon Resonance, Molecular biology, In vitro, Peptide Fragments, Extracellular Matrix, Dissociation constant, biology.protein, Nucleic Acid Conformation, Glioblastoma, Systematic evolution of ligands by exponential enrichment, Protein Binding

Abstract

Tenascin-C (TN-C) is an extracellular matrix protein that is overexpressed during tissue remodeling processes, including tumor growth. To identify an aptamer for testing as a tumor-selective ligand, SELEX (systematic evolution of ligands by exponential enrichment) procedures were performed using both TN-C and TN-C-expressing U251 glioblastoma cells. The different selection techniques yielded TN-C aptamers that are related in sequence. In addition, a crossover procedure that switched from tumor cell to purified protein selections was effective in isolating two high-affinity TN-C aptamers. When targeting tumor cells in vitro, the observed propensity of naive oligonucleotide pools to evolve TN-C aptamers may be due to the abundance of this protein. In vivo, TN-C abundance may also be well suited for aptamer accumulation in the tumor milieu. A size-minimized and nuclease-stabilized aptamer, TTA1, binds to the fibrinogen-like domain of TN-C with an equilibrium dissociation constant (K(d)) of 5 x 10(-9) m. At 13 kDa, this aptamer is intermediate in size between peptides and single chain antibody fragments, both of which are superior to antibodies for tumor targeting because of their smaller size. TTA1 defines a new class of ligands that are intended for targeted delivery of radioisotopes or chemical agents to diseased tissues.

Published

2001

2. Anti-L-selectin aptamers: binding characteristics, pharmacokinetic parameters, and activity against an intravascular target in vivo

Author

Laurie Weigand, David Parma, Steven Ringquist, Ying-Fon Chang, Susan R. Watson, and Dan O'connell

Subjects

Aptamer, Dose-Response Relationship, Immunologic, Oligonucleotides, DNA, Single-Stranded, Plasma protein binding, Mice, SCID, Pharmacology, Biology, Ligands, Binding, Competitive, Rats, Sprague-Dawley, Mice, Pharmacokinetics, In vivo, Cell Movement, PEG ratio, Genetics, Animals, Humans, Nucleotide, Lymphocytes, L-Selectin, chemistry.chemical_classification, Oligonucleotide, In vitro, Rats, Molecular Weight, chemistry, Nucleic Acid Conformation, Lymph Nodes, Protein Binding

Abstract

Therapeutic and diagnostic applications have been envisioned for aptamers, a class of oligonucleotide ligands that bind their target molecules with high affinity and specificity (Gold, J. Biol. Chem. 270, 13581-13584, 1995). To identify parameters that are important for the in vivo activity of aptamers acting on intravascular targets, we have studied binding characteristics in vitro, pharmacokinetic parameters in Sprague-Dawley rats, and inhibitory activity in a SCID mouse/human lymphocyte model of lymphocyte trafficking for both 2'F pyrimidine 2'OH purine RNA and ssDNA anti-human L-selectin aptamers. The data indicate that aptamers with low nanomolar affinity are suitable candidates for use as in vivo reagents and that nonspecific binding to vascular cells is not an issue for efficacy. As is often observed for other reagents, plasma clearance is biphasic. Both the distribution phase and the clearance rate strongly affect in vivo activity. Pharmacokinetic parameters and in vivo activity are significantly improved by conjugating aptamers to a carrier molecule, such as polyethylene glycol (PEG). Most active in vivo is 1d40, a 2'F pyrimidine 2'OH purine aptamer conjugated to 40 kDa PEG. At a dose of 5.4 nmol/kg body weight, its duration of effect (time to 50% inhibition) is 11.2 hours, and at 1 mg or 90 nmol/kg, its plasma clearance rate (CL) is 0.4 ml/min/kg. Its ED50 is estimated to be 80 pmol/kg in preinjection dose-response experiments, compared with 4 pmol/kg for the dimeric anti-L-selectin antibody DREG56. Further improvement of in vivo activity is expected from nucleotide modifications that increase resistance to nuclease digestion for aptamers where mass is not rate limiting for clearance. Because the relationship of clearance to conjugate molecular weight (MW) is not the same for all aptamers, it is advisable to determine the relationship at the outset of in vivo studies. In summary, the data suggest that properly formulated aptamers have the capacity to be effective therapeutic agents against intravascular targets.

Published

2000

3. Site-directed selection of oligonucleotide antagonists by competitive elution

Author

Dan O'connell, Ying-Fon Chang, Ada Velati-Bellini Buvoli, Philippe Bridonneau, and David Parma

Subjects

Erythrocytes, Cations, Divalent, Wheat Germ Agglutinins, Aptamer, Oligonucleotides, Ligands, Binding, Competitive, Genetics, Animals, Binding site, Cloning, Molecular, Gene Library, Pharmacology, Sheep, Base Sequence, Chemistry, Oligonucleotide, Elution, Hemagglutination, Small molecule, Wheat germ agglutinin, Dissociation constant, Molecular Weight, Biochemistry, Carbohydrate Metabolism, Nucleic Acid Conformation, Thermodynamics, Trisaccharides, Systematic evolution of ligands by exponential enrichment

Abstract

Oligonucleotide ligands that bind a protein or a small molecule of interest are readily isolated by in vitro selection and amplification of rare sequences from combinatorial libraries of sequence-randomized oligonucleotides (Gold et al., 1995). Classic systematic evolution of ligands by exponential enrichment (SELEX) protocols are affinity based (Tuerk and Gold, 1990), but because many problems and applications require antagonists, protocols for selecting inhibitors are both desirable and valuable. A widely applicable approach for isolating inhibitors is competitive elution with a molecule that binds the targeted molecule's active or binding site. We have used this approach to isolate antagonists of wheat germ agglutinin (WGA) from a library of 2'NH2-pyrimidine, 2'OH-purine oligonucleotides by elution with N N' N"-triacetylchitotriose, (GlcNAc)3. The highest affinity aptamers have equilibrium dissociation constants of 1 nM-20 nM for WGA, a 10(3)-10(4)-fold improvement relative to (GlcNAc)3, and unlike the carbohydrate, are highly specific. In addition to competing for binding with (GlcNAc)3, aptamers inhibit WGA-mediated agglutination of sheep erythrocytes, demonstrating that they are able to compete with natural ligands presented on the surfaces of cells. These results illustrate the feasibility of isolating high-affinity, high-specificity antagonists by competitive elution with low molecular weight, relatively low-affinity, and low-specificity small molecules.

Published

1999

4. High-affinity aptamers selectively inhibit human nonpancreatic secretory phospholipase A2 (hnps-PLA2)

Author

David W. Snyder, Philippe Bridonneau, Ying-Fon Chang, Lea M. Johnson, Theodore Goodson, David H. Parma, David K. Herron, Dan O'connell, and Stanley C. Gill

Subjects

Male, Indoles, Aptamer, Guinea Pigs, Molecular Sequence Data, Oligonucleotides, In Vitro Techniques, Group II Phospholipases A2, Phospholipases A, chemistry.chemical_compound, Phospholipase A2, Drug Discovery, Animals, Humans, Amino Acid Sequence, Enzyme Inhibitors, IC50, Lung, Gene Library, biology, Base Sequence, Oligonucleotide, Elastase, Muscle, Smooth, Molecular biology, Phospholipases A2, chemistry, Biochemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Nucleic Acid Conformation, Pleura, RNA, lipids (amino acids, peptides, and proteins), Arachidonic acid, Systematic evolution of ligands by exponential enrichment

Abstract

A family of sequence-related 2'-aminopyrimidine, 2'-hydroxylpurine aptamers, developed by oligonucleotide-based combinatorial chemistry, SELEX (systematic evolution of ligand by exponential enrichment) technology, binds human nonpancreatic secretory phospholipase A2 (hnps-PLA2) with nanomolar affinities and inhibits enzymatic activity. Aptamer 15, derived from the family, binds hnps-PLA2 with a Kd equal to 1.7 +/- 0.2 nM and, in a standard chromogenic assay of enzymatic activity, inhibits hnps-PLA2 with an IC50 of 4 nM, at a mole fraction of substrate concentration of 4 x 10(-6) and a calculated Ki of 0.14 nM. Aptamer 15 is selective for hnps-PLA2, having a 25- and 2500-fold lower affinity, respectively, for the unrelated proteins human neutrophil elastase and human IgG. Contractions of guinea pig lung pleural strips induced by hnps-PLA2 are abolished by 0.3 microM aptamer 15, whereas contractions induced by arachidonic acid are not altered. The structure that is essential for binding and inhibition appears to be a 40-base hairpin/loop motif with an asymmetrical internal loop. The affinity and activity of the aptamers demonstrate the ability of the SELEX process to isolate antagonists of nonnucleic-acid-binding proteins from vast oligonucleotide combinatorial libraries.

Published

1998