Abstract

Congenital and acquired disease of the heart valves and great arteries are leading causes of morbidity and mortality. Current prosthetic or bioprosthetic replacement devices are imperfect and subject patients to one or more ongoing risks including thrombosis, limited durability, increased susceptibility to infection, and need for reoperations due to lack of growth. Tissue engineering is a new discipline which offers the potential to create replacement structures from autologous cells and biodegradable polymers. Since tissue engineered (TE) constructs contain living cells, they may have the potential for growth and self-repair and remodeling. Therefore, they could overcome many limitations of existing devices. Cardiac valve leaflets and large conduit arteries have been made with the TE approach. These TE structures have functioned in the pulmonary circulation of growing lambs for up to four months and have demonstrated (1) structural organization to resemble normal valve and artery, (2) satisfactory physiologic function, (3) lack of thrombus formation, and (4) growth. Despite these results, significant questions remain. There is little understanding of cellular interactions and production of extracellular matrix in TE structures. Optimal sources of cells and optimal cell and tissue culture conditions have not been determined. The TE structures created using polyglycolic acid polymer have poor surgical handling characteristics. The longer term fate of TE structures in the circulation is unknown. The proposed studies will attempt to address several issues: (1) the content, structure, and kinetics of degradation of extracellular matrix in normal and TE valve and artery, (2) the influence of anatomic origin and maturation status of cells used to form TE structures, (3) the suitability of new stronger, more flexible polymers in the formation of TE structures, (4) the impact of imposed stretch and shear stress in vitro on developing TE structures. These studies will provide a better understanding of the biological events occurring in the developing TE structures and will guide progress toward the development of clinically useful TE replacements of cardiovascular structures. Abstract)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL060463-04
Application #
6389935
Study Section
Special Emphasis Panel (ZHL1-CSR-F (M1))
Program Officer
Kelley, Christine A
Project Start
1998-07-10
Project End
2003-06-30
Budget Start
2001-07-01
Budget End
2002-06-30
Support Year
4
Fiscal Year
2001
Total Cost
$357,324
Indirect Cost

  Institution

Name
Children's Hospital Boston
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Sales, Virna L; Mettler, Bret A; Engelmayr Jr, George C et al. (2010) Endothelial progenitor cells as a sole source for ex vivo seeding of tissue-engineered heart valves. Tissue Eng Part A 16:257-67
Plouffe, Brian D; Kniazeva, Tatiana; Mayer Jr, John E et al. (2009) Development of microfluidics as endothelial progenitor cell capture technology for cardiovascular tissue engineering and diagnostic medicine. FASEB J 23:3309-14
Mettler, Bret A; Sales, Virna L; Stucken, Chaz L et al. (2008) Stem cell-derived, tissue-engineered pulmonary artery augmentation patches in vivo. Ann Thorac Surg 86:132-40;discussion 140-1
Sales, Virna L; Mettler, Bret A; Lopez-Ilasaca, Marco et al. (2007) Endothelial progenitor and mesenchymal stem cell-derived cells persist in tissue-engineered patch in vivo: application of green and red fluorescent protein-expressing retroviral vector. Tissue Eng 13:525-35
Sales, Virna L; Engelmayr Jr, George C; Johnson Jr, John A et al. (2007) Protein precoating of elastomeric tissue-engineering scaffolds increased cellularity, enhanced extracellular matrix protein production, and differentially regulated the phenotypes of circulating endothelial progenitor cells. Circulation 116:I55-63
Sales, Virna L; Engelmayr Jr, George C; Mettler, Bret A et al. (2006) Transforming growth factor-beta1 modulates extracellular matrix production, proliferation, and apoptosis of endothelial progenitor cells in tissue-engineering scaffolds. Circulation 114:I193-9
Breuer, Christopher K; Mettler, Bret A; Anthony, Tiffany et al. (2004) Application of tissue-engineering principles toward the development of a semilunar heart valve substitute. Tissue Eng 10:1725-36
Perry, Tjorvi E; Kaushal, Sunjay; Sutherland, Fraser W H et al. (2003) Thoracic Surgery Directors Association Award. Bone marrow as a cell source for tissue engineering heart valves. Ann Thorac Surg 75:761-7; discussion 767
Kaushal, S; Amiel, G E; Guleserian, K J et al. (2001) Functional small-diameter neovessels created using endothelial progenitor cells expanded ex vivo. Nat Med 7:1035-40