Orthotropic transplantation of the bioengineered lung using a mouse-scale perfusion-based bioreactor and human primary endothelial cells

Author:

Suzuki Takaya1,Tomiyama Fumiko1,Watanabe Tatsuaki1,Miyanaga Jun2,Suzuki Anna2,Murai Sho1,Suzuki Yuyo1,Niikawa Hiromichi1,Oishi Hisashi1,Notsuda Hirotsugu1,Watanabe Yui1,Hirama Takashi1,Onodera Ken1,Togo Takeo1,Noda Masafumi1,Waddell Thomas3,Karoubi Golnaz3,Okada Yoshinori1

Affiliation:

1. Institute of Aging, Development and Cancer, Tohoku University

2. Institute of Fluid Science, Tohoku University

3. University of Toronto

Abstract

Abstract Whole lung engineering and the transplantation of its products is an ambitious goal and ultimately a viable solution for alleviating the donor-shortage crisis for lung transplants. There are several limitations currently impeding progress in the field with a major obstacle being efficient revascularization of decellularized scaffolds, which requires an extremely large number of cells when using larger pre-clinical animal models. Here, we developed a simple but effective experimental pulmonary bioengineering platform by utilizing the lung as a scaffold. Revascularization of pulmonary vasculature using human umbilical cord vein endothelial cells was feasible using a novel in-house developed perfusion-based bioreactor. The endothelial lumens formed in the peripheral alveolar area were confirmed using a transmission electron microscope. The quality of engineered lung vasculature was evaluated using fractal dimension analysis of histological images. The engineered mouse lungs were successfully transplanted into the orthotopic thoracic cavity. The engineered vasculature in the lung scaffold showed blood perfusion after transplantation without significant hemorrhage. The mouse-based lung bioengineering system can be utilized as an efficient ex-vivo screening platform for lung tissue engineering.

Publisher

Research Square Platform LLC

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