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植入鸡胚和大鼠体内的心肌微组织和大组织的组织移植融合及血管化

Tissue-transplant fusion and vascularization of myocardial microtissues and macrotissues implanted into chicken embryos and rats.

作者信息

Kelm Jens M, Djonov Valentin, Hoerstrup Simon P, Guenter Christina I, Ittner Lars M, Greve Frauke, Hierlemann Andreas, Sanchez-Bustamante Carlota Diaz, Perriard Jean-Claude, Ehler Elisabeth, Fussenegger Martin

机构信息

Institute for Chemical and Bio-Engineering, Swiss Federal Institute of Technology, Zurich, Switzerland.

出版信息

Tissue Eng. 2006 Sep;12(9):2541-53. doi: 10.1089/ten.2006.12.2541.

Abstract

Cell-based therapies and tissue engineering initiatives are gathering clinical momentum for next-generation treatment of tissue deficiencies. By using gravity-enforced self-assembly of monodispersed primary cells, we have produced adult and neonatal rat cardiomyocyte-based myocardial microtissues that could optionally be vascularized following coating with human umbilical vein endothelial cells (HUVECs). Within myocardial microtissues, individual cardiomyocytes showed native-like cell shape and structure, and established electrochemical coupling via intercalated disks. This resulted in the coordinated beating of microtissues, which was recorded by means of a multi-electrode complementary metal-oxide-semiconductor microchip. Myocardial microtissues (microm3 scale), coated with HUVECs and cast in a custom-shaped agarose mold, assembled to coherent macrotissues (mm3 scale), characterized by an extensive capillary network with typical vessel ultrastructures. Following implantation into chicken embryos, myocardial microtissues recruited the embryo's capillaries to functionally vascularize the rat-derived tissue implant. Similarly, transplantation of rat myocardial microtissues into the pericardium of adult rats resulted in time-dependent integration of myocardial microtissues and co-alignment of implanted and host cardiomyocytes within 7 days. Myocardial microtissues and custom-shaped macrotissues produced by cellular self-assembly exemplify the potential of artificial tissue implants for regenerative medicine.

摘要

基于细胞的疗法和组织工程计划正在为组织缺陷的下一代治疗积累临床动力。通过利用单分散原代细胞的重力强制自组装,我们制备了基于成年和新生大鼠心肌细胞的心肌微组织,在用人类脐静脉内皮细胞(HUVECs)包被后可选择性地实现血管化。在心肌微组织内,单个心肌细胞呈现出类似天然的细胞形状和结构,并通过闰盘建立了电化学偶联。这导致了微组织的协调搏动,通过多电极互补金属氧化物半导体微芯片进行记录。用HUVECs包被并铸入定制形状琼脂糖模具中的心肌微组织(微米³尺度)组装成连贯的宏观组织(毫米³尺度),其特征是具有典型血管超微结构的广泛毛细血管网络。植入鸡胚后,心肌微组织募集了胚胎的毛细血管,使源自大鼠的组织植入物实现功能性血管化。同样,将大鼠心肌微组织移植到成年大鼠的心包中,在7天内导致心肌微组织的时间依赖性整合以及植入的和宿主心肌细胞的共排列。通过细胞自组装产生的心肌微组织和定制形状的宏观组织例证了人工组织植入物在再生医学中的潜力。

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