Abstract

A major challenge remaining is the reconstruction of damaged and diseased neural pathways. Toward this end, biomaterials have been examined as bridging devices to support directed nerve outgrowth from regenerating or transplanted neurons. A fundamental challenge that remains is in understanding how to engineer bridges that are clinically useful. The proposed project builds on two observations: 1) aligned scar-like astrocytes support and direct neural outgrowth while misaligned astrocytes display minimal outgrowth even though they display similar surface cues, and 2) neurite outgrowth velocity increases when neurons encounter mixtures of permissive ligands and inhibitory proteoglycans presented in a non-physiological pattern. Based on these observations we formulated the central hypothesis of the proposed research: the local composition and spatial distribution of permissive and inhibitory ligands are the signals that underlie directed outgrowth. by astrocytes. Moreover, we believe it is possible to mimic the spatial distribution of permissive and inhibitory molecules on biomaterials, and that such surfaces could be functionally equivalent to astrocytes coated surfaces in terms of supporting and directing neuronal outgrowth. We will test this hypothesis by: (1) mapping the type and distribution of permissive and inhibitory molecules on aligned astrocyte monolayers using high-resolution microscopy to create a large area map that will aid in the design of a new biologically inspired bridging surface. By designing novel biomimetic structures and interfaces presenting permissive and inhibitory molecules with controlled local composition and spatial distribution we will study how such signals on sub-micrometer length-scales influence axonal outgrowth. (2) We propose to study the role(s) that carbohydrates moieties of the three major proteoglycan families play on directing axonal outgrowth using the novel biomimetic structures as test beds. This will be accomplished using two different routes: using (a) enzymatically modified proteoglycans, or (b) glycosaminoglycans re-assembled from oligosaccharide units synthesized from a precursor using recombinant enzymes. Both types of modifications (a) and (b) then will be tested using axonal outgrowth assays. Finally, (3) we will examine the biomimetic structure under conditions likely encountered following implantation in patients, by using a model system that exposes these surfaces to resting and activated macrophages isolated from CNS.

Public Health Relevance

Among the most debilitating and costly human ailments are injuries and diseases of the nervous system. They affect millions of people in the US and represent a large part of the total national health care cost. Currently there are a limited number of available therapies, none of which restore function to injured neurons of the central nervous system. Numerous studies in animals and man strongly suggest that restorative therapies based on cell transplantation are feasible. A major challenge remains is the reconstruction of damaged and diseased neural pathways. Toward this end, biomaterials have been examined as bridging devices to support directed nerve outgrowth from regenerating neurons. A fundamental challenge involves understanding how to engineer such biomaterial bridges. The proposed project's main objective is to evaluate the construction of such bridging devices based on astrocyte-derived distribution of modified neuron-directing molecules from the nervous system. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS057144-01A2
Application #
7526841
Study Section
Biomaterials and Biointerfaces Study Section (BMBI)
Program Officer
Pancrazio, Joseph J
Project Start
2008-08-01
Project End
2012-05-31
Budget Start
2008-08-01
Budget End
2009-05-31
Support Year
1
Fiscal Year
2008
Total Cost
$422,397
Indirect Cost

  Institution

Name
University of Utah
Department
Biomedical Engineering
Type
Schools of Engineering
DUNS #
009095365
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Hsiao, Tony W; Tresco, Patrick A; Hlady, Vladimir (2017) Astrocyte spreading and migration on aggrecan-laminin dot gradients. Biointerphases 13:01A401
Hsiao, Tony W; Swarup, Vimal P; Eichinger, Colin D et al. (2015) Cell substrate patterning with glycosaminoglycans to study their biological roles in the central nervous system. Methods Mol Biol 1229:457-67
Hsiao, Tony W; Tresco, Patrick A; Hlady, Vladimir (2015) Astrocytes alignment and reactivity on collagen hydrogels patterned with ECM proteins. Biomaterials 39:124-30
Hsiao, Tony W; Swarup, Vimal P; Kuberan, Balagurunathan et al. (2013) Astrocytes specifically remove surface-adsorbed fibrinogen and locally express chondroitin sulfate proteoglycans. Acta Biomater 9:7200-8
Swarup, Vimal P; Hsiao, Tony W; Zhang, Jianxing et al. (2013) Exploiting differential surface display of chondroitin sulfate variants for directing neuronal outgrowth. J Am Chem Soc 135:13488-94
Swarup, Vimal P; Mencio, Caitlin P; Hlady, Vladimir et al. (2013) Sugar glues for broken neurons. Biomol Concepts 4:233-57
Hodgkinson, Gerald N; Tresco, Patrick A; Hlady, Vladimir (2012) The role of well-defined patterned substrata on the regeneration of DRG neuron pathfinding and integrin expression dynamics using chondroitin sulfate proteoglycans. Biomaterials 33:4288-97
Eichinger, Colin D; Hsiao, Tony W; Hlady, Vladimir (2012) Multiprotein microcontact printing with micrometer resolution. Langmuir 28:2238-43
Meng, Fanwei; Hlady, Vladimir; Tresco, Patrick A (2012) Inducing alignment in astrocyte tissue constructs by surface ligands patterned on biomaterials. Biomaterials 33:1323-35
Nguyen, Thao Kim Nu; Raman, Karthik; Tran, Vy My et al. (2011) Investigating the mechanism of the assembly of FGF1-binding heparan sulfate motifs. FEBS Lett 585:2698-702

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