Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice
Recent advances in liver tissue engineering have encouraged further investigation into the evaluation of therapeutic benefits based on animal disease models. In the present study, liver tissues were engineered in coagulation factor IX knockout (FIX-KO) mice, a mouse model of hemophilia B, to determi...
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doaj-039435e99b5840289ebaf52a904f4e2d2020-11-25T02:48:36ZengSAGE PublishingCell Transplantation0963-68971555-38922010-06-011910.3727/096368910X508924Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B MiceKazuo Ohashi M.D., Ph.D.0Kohei Tatsum1Rie Utoh2Soichi Takagi3Midori Shima4Teruo Okano5Institute of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University, Tokyo, JapanDepartment of Pediatrics, Nara Medical University, Nara, JapanInstitute of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University, Tokyo, JapanInstitute of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University, Tokyo, JapanDepartment of Pediatrics, Nara Medical University, Nara, JapanInstitute of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University, Tokyo, JapanRecent advances in liver tissue engineering have encouraged further investigation into the evaluation of therapeutic benefits based on animal disease models. In the present study, liver tissues were engineered in coagulation factor IX knockout (FIX-KO) mice, a mouse model of hemophilia B, to determine if the tissue engineering approach would provide therapeutic benefits. Primary hepatocytes were isolated from the liver of wild-type mice and suspended in a mixture of culture medium and extracellular matrix components. The hepatocyte suspension was injected into the space under the bilateral kidney capsules of the FIX-KO mice to engineer liver tissues. The plasma FIX activities (FIX:C) of the untreated FIX-KO mice were undetectable at any time point. In contrast, the liver tissue engineered FIX-KO mice achieved 1.5–2.5% of plasma FIX activities (FIX:C) and this elevated FIX:C level persisted throughout the 90 day experimental period. Significant FIX mRNA expression levels were found in the engineered liver tissues at levels similar to the wild-type livers. The present study demonstrates that liver tissue engineering could provide therapeutic benefits in the treatment of hemophilia B.https://doi.org/10.3727/096368910X508924 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Kazuo Ohashi M.D., Ph.D. Kohei Tatsum Rie Utoh Soichi Takagi Midori Shima Teruo Okano |
spellingShingle |
Kazuo Ohashi M.D., Ph.D. Kohei Tatsum Rie Utoh Soichi Takagi Midori Shima Teruo Okano Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice Cell Transplantation |
author_facet |
Kazuo Ohashi M.D., Ph.D. Kohei Tatsum Rie Utoh Soichi Takagi Midori Shima Teruo Okano |
author_sort |
Kazuo Ohashi M.D., Ph.D. |
title |
Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice |
title_short |
Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice |
title_full |
Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice |
title_fullStr |
Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice |
title_full_unstemmed |
Engineering Liver Tissues under the Kidney Capsule Site Provides Therapeutic Effects to Hemophilia B Mice |
title_sort |
engineering liver tissues under the kidney capsule site provides therapeutic effects to hemophilia b mice |
publisher |
SAGE Publishing |
series |
Cell Transplantation |
issn |
0963-6897 1555-3892 |
publishDate |
2010-06-01 |
description |
Recent advances in liver tissue engineering have encouraged further investigation into the evaluation of therapeutic benefits based on animal disease models. In the present study, liver tissues were engineered in coagulation factor IX knockout (FIX-KO) mice, a mouse model of hemophilia B, to determine if the tissue engineering approach would provide therapeutic benefits. Primary hepatocytes were isolated from the liver of wild-type mice and suspended in a mixture of culture medium and extracellular matrix components. The hepatocyte suspension was injected into the space under the bilateral kidney capsules of the FIX-KO mice to engineer liver tissues. The plasma FIX activities (FIX:C) of the untreated FIX-KO mice were undetectable at any time point. In contrast, the liver tissue engineered FIX-KO mice achieved 1.5–2.5% of plasma FIX activities (FIX:C) and this elevated FIX:C level persisted throughout the 90 day experimental period. Significant FIX mRNA expression levels were found in the engineered liver tissues at levels similar to the wild-type livers. The present study demonstrates that liver tissue engineering could provide therapeutic benefits in the treatment of hemophilia B. |
url |
https://doi.org/10.3727/096368910X508924 |
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