Department of Biology, McMaster University, Hamilton, Ontario, Canada.
Department of Medicine, McMaster University, Hamilton, Ontario, Canada.
J Cell Mol Med. 2009 Aug;13(8B):1775-1783. doi: 10.1111/j.1582-4934.2008.00480.x. Epub 2008 Aug 21.
An increase in cytosolic Ca(2+) concentration in coronary artery smooth muscle causes a contraction but in endothelium it causes relaxation. Na(+)-Ca(2+)-exchanger (NCX) may play a role in Ca(2+) dynamics in both the cell types. Here, the NCX-mediated (45)Ca(2+) uptake was compared in Na(+)-loaded pig coronary artery smooth muscle and endothelial cells. In both the cell types, this uptake was inhibited by KB-R7943, SEA 0400 and by monensin, but not by cariporide. Prior loading of the cells with the Ca(2+) chelator BAPTA increased the NCX-mediated (45)Ca(2+) uptake in smooth muscle but not in endothelial cells. In the presence or absence of BAPTA loading, the Na(+)-mediated (45)Ca(2+) uptake was greater in endothelial than in smooth muscle cells. In smooth muscle cells without BAPTA loading, thapsigargin diminished the NCX-mediated (45)Ca(2+) entry. This effect was not observed in endothelial cells or in either cell type after BAPTA loading. The results in the smooth muscle cells are consistent with a limited diffusional space model in which the NCX-mediated (45)Ca(2+) uptake was enhanced by chelation of cytosolic Ca(2+) or by its sequestration by the sarco/endoplasmic reticulum Ca(2+) pump (SERCA). They suggest a functional linkage between NCX and SERCA in the smooth muscle but not in the endothelial cells. The concept of a linkage between NCX and SERCA in smooth muscle was also confirmed by similar distribution of NCX and SERCA2 proteins when detergent-treated microsomes were fractionated by flotation on sucrose density gradients. Thus, the coronary artery smooth muscle and endothelial cells differ not only in the relative activities of NCX but also in its functional linkage to SERCA.
细胞浆中钙离子浓度的增加会导致冠状动脉平滑肌收缩,但会导致内皮细胞舒张。钠钙交换器(NCX)可能在这两种细胞类型的钙离子动力学中发挥作用。在这里,比较了钠负荷猪冠状动脉平滑肌和内皮细胞中 NCX 介导的(45)Ca(2+)摄取。在这两种细胞类型中,KB-R7943、SEA 0400 和莫能菌素均抑制该摄取,但 cariporide 不抑制。细胞预先用 Ca(2+)螯合剂 BAPTA 负载会增加平滑肌中 NCX 介导的(45)Ca(2+)摄取,但不会增加内皮细胞中的摄取。无论是否存在 BAPTA 负载,内皮细胞中的 Na(+)介导的(45)Ca(2+)摄取均大于平滑肌细胞。在没有 BAPTA 负载的平滑肌细胞中,thapsigargin 减少了 NCX 介导的(45)Ca(2+)进入。在 BAPTA 负载后,在内皮细胞或两种细胞类型中均未观察到这种作用。平滑肌细胞中的结果与有限的扩散空间模型一致,该模型通过螯合细胞浆 Ca(2+)或通过肌浆/内质网 Ca(2+)泵(SERCA)将其隔离来增强 NCX 介导的(45)Ca(2+)摄取。它们表明在平滑肌中存在 NCX 和 SERCA 之间的功能联系,但在内皮细胞中不存在。通过蔗糖密度梯度漂浮对去污剂处理的微粒体进行分级时,发现 NCX 和 SERCA2 蛋白的相似分布也证实了平滑肌中 NCX 和 SERCA 之间的联系概念。因此,冠状动脉平滑肌和内皮细胞不仅在 NCX 的相对活性方面不同,而且在其与 SERCA 的功能联系方面也不同。