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首页> 外文期刊>Cell transplantation >Engineering liver tissues under the kidney capsule site provides therapeutic effects to hemophilia B mice.
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Engineering liver tissues under the kidney capsule site provides therapeutic effects to hemophilia B mice.

机译:在肾囊部位下方工程化肝组织可为血友病B小鼠提供治疗效果。

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摘要

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.
机译:肝组织工程学的最新进展鼓励进一步研究基于动物疾病模型的治疗效果评估。在本研究中,对血友病B的小鼠凝血因子IX敲除(FIX-KO)小鼠进行了肝组织工程研究,以确定组织工程方法是否可提供治疗益处。从野生型小鼠的肝脏中分离出原代肝细胞,并将其悬浮在培养基和细胞外基质成分的混合物中。将肝细胞悬液注射到FIX-KO小鼠双侧肾囊下的空间中,以工程化肝组织。未经处理的FIX-KO小鼠的血浆FIX活性(FIX:C)在任何时间点都无法检测到。相反,经肝脏组织工程改造的FIX-KO小鼠的血浆FIX活性(FIX:C)达到1.5-2.5%,并且这种升高的FIX:C水平在整个90天的实验期间一直持续存在。在工程肝组织中发现了显着的FIX mRNA表达水平,其水平与野生型肝脏相似。本研究表明,肝组织工程学可以在治疗血友病B中提供治疗益处。

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