Coating PTFE vascular prostheses with a fibroblastic matrix improves cell retention when subjected to blood flow

An investigation was made into the effect of blood flow on endothelial cells (EC) and mesothelial cells (MC) seeded on a vascular expanded polytetrafluoroethylene (ePTFE) prosthesis coated with a fibroblastic matrix. Endothelial cells were obtained from the external jugular vein and MC from the omentum. To test the performance of prostheses, a custom designed, femoral ''ex vivo'' circuit was developed in mongrel dogs. Four study groups were established: a control group, A 1 , where prostheses were uncoated and seeded with EC; a second control group, A 2 , where prostheses were uncoated and seeded with MC; group B 1 where prostheses were coated with a fibroblastic matrix and seeded with EC; and group B 2 where coated prostheses were seeded with MC. All cells were labeled with 111 Indium oxine (10 Ci/mL) before seeding. After the seeded cells had formed a monolayer on the ePTFE prostheses (which took approximately 24 h) the prostheses were placed in the ''ex vivo'' circuit. The rates of blood flow to which prostheses were exposed were measured at the point of inflow (117.5 ± 12.50 mL/min, mean ± SD) and outflow (72.6 ± 14.3 mL/ min). MC showed a greater baseline radionuclide uptake than did EC. The cells of groups B 1 and B 2 adhered sufficiently to the fibroblastic matrix and covered enough of the prosthetic surface to be positioned in the ''ex vivo '' circuit (76.90 ± 8.24% surface covered in EC-seeded prostheses and 71.65 ± 6.23% in MC-seeded prostheses). After exposure to blood flow the quantity of radionuclide-labeled cells and the prosthetic surface covered by them were greatly reduced though the fibroblast-coated prostheses showed greater cell retention.