BioEngineering

Patrick S. Stayton, Professor

Thrust Areas
Engineered Biomaterials and Tissue Bioengineering
Molecular Bioengineering and Nanotechnology

Education
PhD (biochemistry), University of Illinois-Champaign, 1989

 photo of Dr. Stayton

Research Interests
    •  Protein engineering
    •  Biomaterials
    •  Drug delivery
    •  Biomineralization

Contact Information
Department of Bioengineering
University of Washington
Box 355061
William H. Foege Building, Room N530L
Phone: 206-685-8148
E-mail: stayton@u.washington.edu
Web Site: http://www.bioeng.washington.edu/stayton

Research Description

Our research group is interested in elucidating the fundamental mechanisms of biomolecular recognition and applying the unique capabilities of biological molecules to biotechnologies. We would like to bridge the gap between understanding molecular structure-function relationships, and being able to utilize proteins/peptides/DNA for drug therapies, bioanalytics, diagnostics, and biomaterial development.

"Smart" Biotechnology and Nanotechnology: We are developing new biohybrid molecular materials designed to "talk" and "listen". These "smart" materials are designed for applications in the drug delivery and bioanalytical fields. The drug delivery group is working to develop functional and pH-responsive polymeric carriers for biomolecular therapeutics and vaccines, e.g. proteins, antisense oligonucleotides, RNA interference or silencing RNA, and DNA plasmids. Our challenge is to develop carriers that mimic the ability of viruses and pathogens to deliver macromolecules to specific intracellular compartments, while avoiding their immunogenicity and toxicity.

The bioanalytical group is working to develop smart polymer-protein conjugates, smart polymer-DNA conjugates, and smart polymer-bead conjugates as responsive molecular componentry for diagnostics, lab assays, biochips and arrays, and for upstream processing of complex fluids such as blood. We have a focus on point-of-care diagnostics, including with the Distributed Diagnostics and Home Healthcare group and in diagnostics for resource-poor settings, e.g. diagnostics for Africa.

Biomaterials and Tissue Engineering: We are working in collaboration with the Biomaterials and Tissue Engineering group to develop a better understanding of the mechanisms by which materials can be engineered to control cellular responses. A primary focus is on controlling the foreign body reaction to biomaterials. To accomplish this goal, mechanistic studies of macrophage activation on biomaterials are combined with the development of controlled release systems for anti-inflammatory delivery. For the fundamental studies, signaling pathway analysis is being conducted using gene expression profiling and proteomics to identify key molecular targets for controlling cell response to biomaterials. The delivery arm of the project is utilizing new delivery systems for antisense and RNA interference therapeutics that inactivate key macrophage signaling targets or inflammatory cytokines.

Another focus area is controlling vascularization around tissue engineering matrices and tissue regeneration materials. Our work is centered on protein and nucleic acid delivery from hydrogel coatings and matrices. Similar strategies for protein growth factor and nucleic acid delivery from hydrogel matrices are being used to promote hard tissue regeneration for craniofacial and dental applications.

Molecular Recognition Studies: Our applied bioengineering projects benefit from connections to more fundamental biophysical studies of molecular recognition in biology. We have two primary projects, the first in the area of biomineralization. This research is directed toward elucidating the fundamental design principles used by nature to engineer bone and teeth. We are investigating the molecular mechanisms used by proteins to control the hierarchical structure of biological calcium composites such as hydroxyapatite and calcium oxalate. These studies connect to our hard tissue regeneration applications.

The second project studies the detailed molecular mechanisms by which proteins regulate small molecule recognition. We are using a combination of site-directed mutagenesis, biophysical characterization, and high-resolution structural characterization to elucidate how proteins generate high-affinity for small molecule ligands. These studies may illuminate design principles for drug design, where high affinity is generally the desired goal. The central project is directed toward determining the structure-function relationships responsible for high-affinity and slow off-rates in the model streptavidin-biotin system. These studies connect to more applied protein engineering efforts with streptavidin, which is a widely utilized protein in diagnostics and bioanalytical technologies.

Targeted Drug Delivery: Targeting of therapeutics and imaging agents to specific sites in the body is an important aspect of drug delivery systems. We are using genetic engineering techniques to design antibody and streptavidin systems for improved performance in targeted drug delivery systems. Our model systems are designed for in vivo delivery of therapeutics and radionucleotides to carcinomas such as B-cell lymphoma.

Honors and Awards

  • Fellow, American Institute for Medical and Biological Engineering
  • Controlled Release Society, CRS-Cygnus Recognition Award
  • Hunter Visiting Professor, Clemson University
  • Minority Science Engineering Program, Honorary Award

Professional Experience

  • 2001-present: Professor, Department of Bioengineering, University of Washington
  • 1997-2001: Associate Professor, Department of Bioengineering, University of Washington
  • 1996-present: Molecular Materials Thrust Group Leader, UWEB Engineering Research Center
  • 1992-1997: Assistant Professor, Center for Bioengineering, University of Washington
  • 1989-1992: Postdoctoral Research Associate, Beckman Institute for Advanced Science and Technology
  • 1984-1989: Graduate Research Assistant, University of Illinois, Department of Biochemistry

Selected Publications

  • Drobny, G. P., Long, J. R., Karlsson, T., Shaw, W., Popham, J., Oyler, N., Bower, P., Stringer, J., Gregory, D., Mehta, M., and and Stayton, P. S. "Structural studies of biomaterials using double-quantum solid-state NMR Spectroscopy" (2003) Annual Reviews of Physical Chemistry, 54, 531-571.
  • Stayton, P. S., Shaw, W. J., Long, J. R., and Drobny, G. P. (2003) "Molecular Recognition at the Protein-HAP Interface" Critical Reviews in Oral Biology and Medicine, 14, 370-376.
  • Gilbert, M., Giachelli, C. M., and Stayton, P. S. (2003) "Biomimetic peptides that engage specific integrin-dependent signaling pathways and bind to calcium phosphate surfaces" J. Biomed. Mat. Res., 67, 69-77.
  • McDevitt, T. C., Angello, J. C., Whitney, M. L., Reinecke, H., Hauschka, S. D., Murry, C. E., and Stayton, P. S. (2002) " In vitro generation of differentiated cardiac myofibers on micropatterned laminin surfaces." J. Biomed. Mat. Res. 60, 472-479.
  • McDevitt, T. C., Woodhouse, K. A., Murry, C. E., Hauschka, S. D., and Stayton, P. S. (2003) "Spatially Organized Layers of Cardiomyocytes on Biodegradable Polyurethane Films for Myocardial Repair " J. Biomed. Mat. Res. 66, 586-595.
  • Stayton PS. (2003) "Delivering the Vaccination Mail" Trends Biotechnol. 21, 465-467.
  • Malmstadt, N., Yager, P., Hoffman, A. S., and Stayton, P. S. (2003) "A Smart Microfluidic Affinity Chromatography Matrix Composed of Poly(N-isopropylacrylamide)-Coated Beads" Anal. Chem. (Accelerated Article) 75, 2943-2949.
  • Shimoboji, T., Larenas, E., Fowler, T., Kulkarni, S., Hoffman, A. S., and Stayton, P.S. (2002) "Photo-Responsive Polymer-Enzyme Switches" Proc. Natl. Acad. Sci. USA, 99, 16592-6.
  • Murthy, N., Campbell, J., Fausto, N., Hoffman, A. S., and Stayton, P. S. (2003) "Design and synthesis of pH-responsive polymeric carriers that target uptake and enhance the intracellular delivery of oligonucleotides. " J. Cont. Rel., 89, 365-74.
  • Ding, Z., Fong, R. B., Long, C. J., Hoffman, A. S. and Stayton, P. S. (2001) "Size-dependent control of the binding of biotinylated proteins to streptavidin using a polymer shield" Nature 411, 59-62.
  • Lackey, C. A., Press, O. W., Hoffman, A. S., and Stayton, P. S. (2002) "A Biomimetic pH-Responsive Polymer Directs Endosomal Release and Intracellular Delivery of an Endocytosed Antibody Complex" Bioconjugate Chem. 13, 996-1001.
  • Hyre, D. E., Amon, L. K., Le Trong, I., Penzotti, J., Stenkamp, R. E., Lybrand, T. P., and Stayton, P. S. (2002) "The Streptavidin-Biotin Dissociation Reaction is Initiated By Entry of Specific Water Molecules From a Defined Channel" Nature Structural Biology 9, 582-585.
  • Shimoboji, T., Larenas, E., Fowler, T., Hoffman, A. S., and Stayton, P.S. (2003) "Temperature-induced Switching of Enzyme Activity with Smart Polymer-Enzyme Conjugates" Bioconj. Chem. 14, 517-525.
  • Fong, R. B., Ding, Z., Hoffman, A. S., and Stayton, P. S. (2002) "Affinity separation using an Fv antibody fragment-smart polymer conjugate" Biotechnology and Bioengineering 79, 271-276.