Marion Bessin Liver Research Center, Department of Medicine, Albert Einstein College of Medicine, Bronx, NY 10461, USA.
Hepatology. 2012 Apr;55(4):1182-92. doi: 10.1002/hep.24735.
Organs from non-heart-beating donors are attractive for use in cell therapy. Understanding the nature of molecular perturbations following reperfusion/reoxygenation will be highly significant for non-heart-beating donor cells. We studied non-heart-beating donor rats for global gene expression with Affymetrix microarrays, hepatic tissue integrity, viability of isolated hepatocytes, and engraftment and proliferation of transplanted cells in dipeptidyl peptidase IV-deficient rats. In non-heart-beating donors, liver tissue was morphologically intact for >24 hours with differential expression of 1, 95, or 372 genes, 4, 16, or 34 hours after death, respectively, compared with heart-beating donors. These differentially expressed genes constituted prominent groupings in ontological pathways of oxidative phosphorylation, adherence junctions, glycolysis/gluconeogenesis, and other discrete pathways. We successfully isolated viable hepatocytes from non-heart-beating donors, especially up to 4 hours after death, although the hepatocyte yield and viability were inferior to those of hepatocytes from heart-beating donors (P < 0.05). Similarly, although hepatocytes from non-heart-beating donors engrafted and proliferated after transplantation in recipient animals, this was inferior to hepatocytes from heart-beating donors (P < 0.05). Gene expression profiling in hepatocytes isolated from non-heart-beating donors showed far greater perturbations compared with corresponding liver tissue, including representation of pathways in focal adhesion, actin cytoskeleton, extracellular matrix-receptor interactions, multiple ligand-receptor interactions, and signaling in insulin, calcium, wnt, Jak-Stat, or other cascades.
Liver tissue remained intact over prolonged periods after death in non-heart-beating donors, but extensive molecular perturbations following reperfusion/reoxygenation impaired the viability of isolated hepatocytes from these donors. Insights into molecular changes in hepatocytes from non-heart-beating donors offer opportunities for improving donor cell viability, which will advance the utility of non-heart-beating donor organs for cell therapy or other applications.
未心跳供体的器官在细胞治疗中很有吸引力。了解再灌注/再氧合后分子扰动的性质对于非心跳供体细胞非常重要。我们使用 Affymetrix 微阵列研究了非心跳供体大鼠的整体基因表达、肝组织完整性、分离肝细胞的活力以及在二肽基肽酶 IV 缺陷大鼠中移植细胞的植入和增殖。在非心跳供体中,肝组织在形态上完整>24 小时,与心跳供体相比,死亡后 4、16 或 34 小时分别有 1、95 或 372 个基因差异表达。这些差异表达的基因构成了氧化磷酸化、黏附连接、糖酵解/糖异生和其他离散途径的本体论途径中的显著分组。我们成功地从非心跳供体中分离出具有活力的肝细胞,尤其是在死亡后 4 小时内,尽管肝细胞的产量和活力低于心跳供体的肝细胞(P < 0.05)。同样,虽然来自非心跳供体的肝细胞在受体动物中移植后植入和增殖,但这不如来自心跳供体的肝细胞(P < 0.05)。从非心跳供体中分离的肝细胞的基因表达谱显示出比相应肝组织更大的干扰,包括在粘着斑、肌动蛋白细胞骨架、细胞外基质-受体相互作用、多个配体-受体相互作用以及胰岛素、钙、wnt、Jak-Stat 或其他级联中的信号转导途径的代表。
在非心跳供体中,肝组织在死亡后很长一段时间内保持完整,但再灌注/再氧合后的广泛分子干扰损害了这些供体来源的分离肝细胞的活力。对非心跳供体细胞中肝细胞分子变化的深入了解为提高供体细胞活力提供了机会,这将推进非心跳供体器官在细胞治疗或其他应用中的应用。