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首页> 外文期刊>Tissue engineering, Part C. Methods >Hemodynamic Characterization of a Mouse Model for Investigating the Cellular and Molecular Mechanisms of Neotissue Formation in Tissue-Engineered Heart Valves
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Hemodynamic Characterization of a Mouse Model for Investigating the Cellular and Molecular Mechanisms of Neotissue Formation in Tissue-Engineered Heart Valves

机译:小鼠模型的血液动力学特征,用于研究组织工程性心脏瓣膜中新组织形成的细胞和分子机制

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Decellularized allograft heart valves have been used as tissue-engineered heart valve (TEHV) scaffolds with promising results; however, little is known about the cellular mechanisms underlying TEHV neotissue formation. To better understand this phenomenon, we developed a murine model of decellularized pulmonary heart valve transplantation using a hemodynamically unloaded heart transplant model. Furthermore, because the hemodynamics of blood flow through a heart valve may influence morphology and subsequent function, we describe a modified loaded heterotopic heart transplant model that led to an increase in blood flow through the pulmonary valve. We report host cell infiltration and endothelialization of implanted decellularized pulmonary valves (dPV) and provide an experimental approach for the study of TEHVs using mouse models.
机译:脱细胞的同种异体心脏瓣膜已被用作组织工程心脏瓣膜(TEHV)支架,取得了可喜的结果。然而,关于TEHV新组织形成的细胞机制知之甚少。为了更好地了解这种现象,我们使用血液动力学卸载的心脏移植模型开发了脱细胞肺心瓣膜移植的小鼠模型。此外,由于流经心脏瓣膜的血流动力学可能会影响形态和后续功能,因此我们描述了一种改良的负载异位心脏移植模型,该模型导致流经肺动脉瓣的血流增加。我们报告宿主细胞浸润和植入的脱细胞肺动脉瓣(dPV)的内皮化,并提供了使用小鼠模型研究TEHVs的实验方法。

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