Abstract

The chemical and biomechanical parameters of implanted blood- contacting biomaterials initiate and/or modulate the resultant inflammatory, regenerative, and thrombotic reactions. These tissue reactions ultimately determine the clinical success of implanted vascular prostheses. Bioresorbable lactide/glycolide copolymeric prostheses which are phagocytized by macrophages lead to extensive myofibroblast and endothelial cell regeneration. The current protocol attempts to clarify the extent of the regenerative capacities of the components of the arterial wall and to analyze the mechanisms by which the prosthetic composition and biomechanical characteristics affect the tissue responses.
Specific aims i nclude (1) the effects of compositional and biomechanical characteristics of bioresorbable prostheses on the rate and extent of regeneration of myofibroblasts, endothelial cells, collagen and elastin, the duratin and extent of cellular proliferative activity, and functionality of these regenerated tissues; (2) the role and identification of specific growth factors as mediators of vascular healing following prosthetic implantation; (3) macrophage-biomaterial interactions inducing release of specific macrophage derived growth factors as mediators of vascular healing; and (4) the efficacy of exogenous growth factors in optimization of vascular healing. This proposal will utilize bioresorble and non-resorbable prostheses woven to defined reproducible parameters from well characterized yarns. Prostheses will be implanted into rabbit and canine models and explants will later be analzyed by histologic, immunocytochemical, and ultrastructural techniques, autoradiography, collagen assays, and functional analyses of compliance, strength, and prostacyclin production rates. Northern blot analyses of explanted tissues will identify mRNA for specific growth factors. The content of growth factors within explanted tissues subjected to elutriation techniques will be determined by bioassays and by biochemical and immunochemical growth factor analyses with results expressed as a function of time following implantation. These results will be temporally related to the histologic analyses and to corrobation tissue culture studies of macrophage-biomaterial interactions. These concurrent analyses will document the differential activation of resident macrophages by biomaterials resulting in their production of growth factor(s) as documented by bioassays and specific growth factor identification will utilize biochemical and immunochemical techniques. A related study will examine the modulation of vascular healing in response to the application of a specific growth factor, HBGF-1, applied to biomaterials. The clarification of these issues should lead to a new generation of small caliber vascular prostheses with greater clinical efficacy as well as an ability to selectively stimulate or inhibit aspects of vascular healing by appropriate use of growth factors and their antagonists.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL041272-04
Application #
3358932
Study Section
Special Emphasis Panel (SRC (18))
Project Start
1988-07-01
Project End
1993-04-30
Budget Start
1991-05-15
Budget End
1992-04-30
Support Year
4
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Loyola University Chicago
Department
Type
Schools of Medicine
DUNS #
791277940
City
Maywood
State
IL
Country
United States
Zip Code
60153

  Publications

Ucuzian, Areck A; Bufalino, Dominick V; Pang, Yonggang et al. (2013) Angiogenic endothelial cell invasion into fibrin is stimulated by proliferating smooth muscle cells. Microvasc Res 90:40-7
Gassman, Andrew A; Kuprys, Tomas; Ucuzian, Areck A et al. (2011) Three-dimensional 10% cyclic strain reduces bovine aortic endothelial cell angiogenic sprout length and augments tubulogenesis in tubular fibrin hydrogels. J Tissue Eng Regen Med 5:375-83
Pang, Yonggang; Wang, Xiaoli; Lee, Dongkeun et al. (2011) Dynamic quantitative visualization of single cell alignment and migration and matrix remodeling in 3-D collagen hydrogels under mechanical force. Biomaterials 32:3776-83
Ucuzian, Areck A; Gassman, Andrew A; East, Andrea T et al. (2010) Molecular mediators of angiogenesis. J Burn Care Res 31:158-75
Ucuzian, Areck A; Brewster, Luke P; East, Andrea T et al. (2010) Characterization of the chemotactic and mitogenic response of SMCs to PDGF-BB and FGF-2 in fibrin hydrogels. J Biomed Mater Res A 94:988-96
Pang, Yonggang; Wang, Xiaoli; Ucuzian, Areck A et al. (2010) Local delivery of a collagen-binding FGF-1 chimera to smooth muscle cells in collagen scaffolds for vascular tissue engineering. Biomaterials 31:878-85
Pang, Yonggang; Greisler, Howard P (2010) Using a type 1 collagen-based system to understand cell-scaffold interactions and to deliver chimeric collagen-binding growth factors for vascular tissue engineering. J Investig Med 58:845-8
Brewster, L P; Ucuzian, A A; Brey, E M et al. (2010) FRNK overexpression limits the depth and frequency of vascular smooth muscle cell invasion in a three-dimensional fibrin matrix. J Cell Physiol 225:562-8
Pang, Yonggang; Ucuzian, Areck A; Matsumura, Akie et al. (2009) The temporal and spatial dynamics of microscale collagen scaffold remodeling by smooth muscle cells. Biomaterials 30:2023-31
Brewster, Luke P; Washington, Cicely; Brey, Eric M et al. (2008) Construction and characterization of a thrombin-resistant designer FGF-based collagen binding domain angiogen. Biomaterials 29:327-36

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