Bioengineered uterine tissue supports pregnancy in a rat model
We investigated the functionality of different bioengineered patches for partial uterus repair and conclude that uterine cells and mesenchymal stem cells can reconstruct decellularized uterine tissue and support pregnancy.
Volume 106, Issue 2, Pages 487- 496.e1
Mats Hellström, Ph.D., Juan M. Moreno-Moya, Ph.D., Sara Bandstein, M.Sc., Eva Bom, Ph.D., Randa R. Akouri, M.D., Ph.D., Kaoru Miyazaki, M.D., Ph.D., Tetsuo Maruyama, M.D., Ph.D., Mats Brännström, M.D., Ph.D.
To create a bioengineered uterine patch for uterine repair of a partially defect uterus.
Three different decellularized uterine scaffolds were recellularized in vitro with primary uterine cells and green fluorescent protein– (GPF-) labeled bone marrow–derived mesenchymal stem cells (GFP-MSCs). The patches were transplanted in vivo to investigate their tissue adaptation and supporting capacity during pregnancy.
Female Lewis rats (n = 9) as donors to generate whole-uterus scaffolds using three different protocols (n = 3 per protocol); Sprague Dawley rats (n = 40) for primary uterus cell isolation procedures (n = 10) and for transplantation/pregnancy studies (n = 30); and male Sprague Dawley rats (n = 12) for mating.
Decellularization was achieved by whole-uterus perfusion with buffered or nonbuffered Triton-X100 and dimethyl sulfoxide (DMSO; group P1/P2) or with sodium deoxycholate (group P3). Primary uterine cells and GFP-MSCs were used to develop uterine tissue constructs, which were grafted to uteri with partial tissue defects.
Main Outcome Measure(s)
Recellularization efficiency and graft quality were analyzed morphologically, immunohistochemically, and by real-time quantitative polymerase chain reaction (PCR). The location and number of fetuses were documented during pregnancy days 16–20.
Pregnancy and fetal development were normal in groups P1 and P2, with fetal development over patched areas. Group P3 showed significant reduction of fetal numbers, and embryos were not seen in the grafted area. Quantitative PCR and immunohistochemistry revealed uterus-like tissue in the patches, which had been further reconstructed by infiltrating host cells after transplantation.
Primary uterine cells and MSCs can be used to reconstruct decellularized uterine tissue. The bioengineered patches made from triton-X100+DMSO-generated scaffolds were supportive during pregnancy. These protocols should be explored further to develop suitable grafting material to repair partially defect uteri and possibly to create a complete bioengineered uterus.