Department of Medicine/Cardiology, Cardiovascular Research Laboratories, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA.
Eur Heart J. 2009 Sep;30(18):2254-65. doi: 10.1093/eurheartj/ehp267. Epub 2009 Jun 27.
To increase the supply, many countries harvest allograft valves from explanted hearts of transplant recipients with ischaemic (ICM) or dilated cardiomyopathy (DCM). This study determines the structural integrity of valves from cardiomyopathic hearts.
Extracellular matrix (ECM) was examined in human valves obtained from normal, ICM, and DCM hearts. To confirm if ECM changes were directly related to the cardiomyopathy, we developed a porcine model of chronic ICM. Histology and immunohistostaining, as well as non-invasive multiphoton and second harmonic generation (SHG) imaging revealed marked disruption of ECM structures in human valves from ICM and DCM hearts. The ECM was unaffected in valves from normal and acute ICM pigs, whereas chronic ICM specimens showed ECM alterations similar to those seen in ICM and DCM patients. Proteins and proteinases implicated in ECM remodelling, including Tenascin C, TGFbeta1, Cathepsin B, MMP2, were upregulated in human ICM and DCM, and porcine chronic ICM specimens.
Valves from cardiomyopathic hearts showed significant ECM deterioration with a disrupted collagen and elastic fibre network. It will be important to determine the impact of this ECM damage on valve durability and calcification in vivo if allografts are to be used from these donors.
为了增加供应,许多国家从缺血性(ICM)或扩张型心肌病(DCM)的移植受者的已移植心脏中收获同种异体瓣膜。本研究旨在确定心肌病心脏来源的瓣膜的结构完整性。
检查了取自正常、ICM 和 DCM 心脏的人类瓣膜中的细胞外基质(ECM)。为了确认 ECM 变化是否与心肌病直接相关,我们开发了一种慢性 ICM 的猪模型。组织学和免疫组织化学染色以及非侵入性多光子和二次谐波产生(SHG)成像显示,来自 ICM 和 DCM 心脏的人类瓣膜的 ECM 结构明显破坏。来自正常和急性 ICM 猪的瓣膜中 ECM 不受影响,而慢性 ICM 标本显示与 ICM 和 DCM 患者中所见相似的 ECM 改变。涉及 ECM 重塑的蛋白质和蛋白酶,包括 Tenascin C、TGFbeta1、组织蛋白酶 B、MMP2,在人类 ICM 和 DCM 以及慢性 ICM 猪标本中上调。
来自心肌病心脏的瓣膜显示出明显的 ECM 恶化,胶原和弹性纤维网络受到破坏。如果要从这些供体中使用同种异体移植物,那么确定 ECM 损伤对体内瓣膜耐久性和钙化的影响将非常重要。