Abstract

Every year, nearly 100,000 patients need coronary or peripheral revascularization procedures, but have no suitable vein or artery. The tissue engineering of autologous vessels for these patients could have an enormous impact on therapy for cardiovascular disease. We have developed techniques to culture tissue engineered vessels from differentiated vascular cells. Engineered arteries are cultured on degradable polymer scaffolds in pulsatile perfusion systems. Vessels that are produced are strong enough for initial implantation. Completely autologous animals grafts, as well as human engineered vessels, have cultured using these methods. However, implanted autologous vessels dilate significantly over time in vivo, due to limitations in ultimate mechanical strength. In addition, engineered graft survival in animal models is limited by thrombosis. Thus, although significant advances have been made in vascular tissue engineering, mechanical strength and thrombogenicity limit further progress in the field. Collagen determines the ultimate mechanical properties of blood vessels. Engineered blood vessels have less collagen than native vessels, and this collagen has lower load-bearing properties than native. We postulate that the """"""""defective"""""""" collagen in engineered vessels is caused by inadequate cross-linking, and by excessive cleavage by proteases. This proposal will test this overall hypothesis. Specifically, we will study the effects on collagen cross-linking of copper supplementation to increase lysyl oxidase activity. In addition, we will study the effects of metalloproteinase inhibition on collagen accumulation and vessel strength, and we will assess the effects of retinoids on cross- linking activity, metalloproteinases, and cellular quiescence in engineered vessels. These experiments will thus work synergistically to improve tissue engineered collagen, and hence improve vessel mechanical strength. The other important limitation for engineered vessels is early thrombosis. Cultured endothelial cells decrease expression of thrombomodulin, which is an important anti-coagulant in the native arterial system. We will examine the functional significance of thrombomodulin loss in engineered vessels. With the aim of improving the patency of these vascular grafts, we will also quantify the effects of thrombomodulin over-expression on vessel thrombogenicity. Thus, by attacking the two important impediments in vascular tissue engineering, the experiments in this proposal will significantly advance the field.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL063766-02
Application #
6625865
Study Section
Surgery and Bioengineering Study Section (SB)
Program Officer
Lundberg, Martha
Project Start
2002-05-01
Project End
2006-04-30
Budget Start
2003-05-01
Budget End
2004-04-30
Support Year
2
Fiscal Year
2003
Total Cost
$281,000
Indirect Cost

  Institution

Name
Duke University
Department
Biomedical Engineering
Type
Schools of Engineering
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Gong, Zhaodi; Niklason, Laura E (2011) Use of human mesenchymal stem cells as alternative source of smooth muscle cells in vessel engineering. Methods Mol Biol 698:279-94
Solan, Amy; Dahl, Shannon L M; Niklason, Laura E (2009) Effects of mechanical stretch on collagen and cross-linking in engineered blood vessels. Cell Transplant 18:915-21
Gong, Zhaodi; Calkins, Geoffrey; Cheng, Ee-chun et al. (2009) Influence of culture medium on smooth muscle cell differentiation from human bone marrow-derived mesenchymal stem cells. Tissue Eng Part A 15:319-30
Gong, Zhaodi; Niklason, Laura E (2008) Small-diameter human vessel wall engineered from bone marrow-derived mesenchymal stem cells (hMSCs). FASEB J 22:1635-48
Dahl, Shannon L M; Rhim, Caroline; Song, Ying C et al. (2007) Mechanical properties and compositions of tissue engineered and native arteries. Ann Biomed Eng 35:348-55
Dahl, Shannon L M; Vaughn, Megann E; Niklason, Laura E (2007) An ultrastructural analysis of collagen in tissue engineered arteries. Ann Biomed Eng 35:1749-55
Klinger, Rebecca Y; Blum, Juliana L; Hearn, Bevin et al. (2006) Relevance and safety of telomerase for human tissue engineering. Proc Natl Acad Sci U S A 103:2500-5
Solan, Amy; Niklason, Laura (2005) Age effects on vascular smooth muscle: an engineered tissue approach. Cell Transplant 14:481-8
Poh, Melissa; Boyer, Matthew; Solan, Amy et al. (2005) Blood vessels engineered from human cells. Lancet 365:2122-4
Dahl, Shannon L M; Rucker, Robert B; Niklason, Laura E (2005) Effects of copper and cross-linking on the extracellular matrix of tissue-engineered arteries. Cell Transplant 14:367-74

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