| Literature DB >> 35360387 |
Irina Zakharova1,2,3, Shoraan Saaya2, Alexander Shevchenko1,2,3, Alena Stupnikova1,4, Maria Zhiven'1, Pavel Laktionov2,3, Alena Stepanova2,3, Alexander Romashchenko1, Lyudmila Yanshole5, Alexander Chernonosov3, Alexander Volkov2, Elena Kizilova1,4, Evgenii Zavjalov1, Alexander Chernyavsky2, Alexander Romanov2, Andrey Karpenko2, Suren Zakian1,2,3.
Abstract
In our previous study, we showed that discarded cardiac tissue from the right atrial appendage and right ventricular myocardium is an available source of functional endothelial and smooth muscle cells for regenerative medicine and tissue engineering. In the study, we aimed to find out what benefits are given by vascular cells from cardiac explants used for seeding on vascular patches engrafted to repair vascular defects in vivo. Additionally, to make the application of these cells safer in regenerative medicine we tested an in vitro approach that arrested mitotic division to avoid the potential tumorigenic effect of dividing cells. A tissue-engineered construction in the form of a patch based on a polycaprolactone-gelatin scaffold and seeded with endothelial and smooth muscle cells was implanted into the abdominal aorta of immunodeficient SCID mice. Aortic patency was assessed using ultrasound, MRI, immunohistochemical and histological staining. Endothelial and smooth muscle cells were treated with mitomycin C at a therapeutic concentration of 10 μg/ml for 2 h with subsequent analysis of cell proliferation and function. The absence of the tumorigenic effect of mitomycin C-treated cells, as well as their angiogenic potential, was examined by injecting them into immunodeficient mice. Cell-containing patches engrafted in the abdominal aorta of immunodeficient mice form the vessel wall loaded with the appropriate cells and extracellular matrix, and do not interfere with normal patency. Endothelial and smooth muscle cells treated with mitomycin C show no tumorigenic effect in the SCID immunodeficient mouse model. During in vitro experiments, we have shown that treatment with mitomycin C does not lead to a decrease in cell viability. Despite the absence of proliferation, mitomycin C-treated vascular cells retain specific cell markers, produce specific extracellular matrix, and demonstrate the ability to stimulate angiogenesis in vivo. We pioneered an approach to arresting cell division with mitomycin C in endothelial and smooth muscle cells from cardiac explant, which prevents the risk of malignancy from dividing cells in vascular surgery. We believe that this approach to the fabrication of tissue-engineered constructs based on mitotically inactivated cells from waste postoperative material may be valuable to bring closer the development of safe cell products for regenerative medicine.Entities:
Keywords: endothelial cells; mitomycin C; polycaprolactone; smooth muscle cells; tissue-engineered vascular graft; vascular patch
Year: 2022 PMID: 35360387 PMCID: PMC8963790 DOI: 10.3389/fbioe.2022.772981
Source DB: PubMed Journal: Front Bioeng Biotechnol ISSN: 2296-4185