Blaustein M P, Juhaszova M, Golovina V A, Church P J, Stanley E F
Department of Physiology, University of Maryland School of Medical School, Baltimore, Maryland 21210, USA.
Ann N Y Acad Sci. 2002 Nov;976:356-66. doi: 10.1111/j.1749-6632.2002.tb04762.x.
Immunocytochemistry reveals that the Na/Ca exchanger (NCX) in neuronal somata and astrocytes is confined to plasma membrane (PM) microdomains that overlie sub-PM (junctional) endoplasmic reticulum (jER). By contrast, the PM Ca(2+) pump (PMCA) is more uniformly distributed in the PM. At presynaptic nerve terminals, the NCX distribution is consistent with that observed in the neuronal somata, but the PMCA is clustered at the active zones. Thus, the PMCA, with high affinity for Ca(2+) (K(d) congruent with 100 nM), may keep active zone Ca(2+) very low and thereby "reprime" the vesicular release mechanism following activity. NCX, with lower affinity for Ca(2+) (K(d) congruent with 1,000 nM), on the other hand, may extrude Ca(2+) that has diffused away from the active zones and been temporarily sequestered in the endoplasmic reticulum. The PL microdomains that contain the NCX also contain Na(+) pump high ouabain affinity alpha2 (astrocytes) or alpha 3 (neurons) subunit isoforms (IC(50) congruent with 5-50 nM ouabain). In contrast, the alpha1 isoform (low ouabain affinity in rodents; IC(50) >10,000 nM), like the PMCA, is more uniformly distributed in these cells. The sub-PM endoplasmic reticulum in neurons (and probably glia and other cell types as well) and the adjacent PM form junctions that resemble cardiac muscle dyads. We suggest that the PM microdomains containing NCX and alpha 2/alpha 3 Na(+) pumps, the underlying jER, and the intervening tiny volume of cytosol (<10(-18) l) form functional units (PLasmERosomes); diffusion of Na(+) and Ca(2+) between these cytosolic compartments and "bulk" cytosol may be markedly restricted. The activity of the Na(+) pumps with alpha 2/alpha 3 subunits may thus regulate NCX activity and jER Ca(2+) content. This view is supported by studies in mice with genetically reduced (by congruent with 50%) alpha 2 Na(+) pumps: evoked Ca(2+) transients were augmented in these cells despite normal cytosolic Na(+) and resting Ca(2+) concentrations (Na(+) and Ca(2+)). We conclude that alpha 2/alpha 3 Na(+) pumps control PLasmERosome (local) Na(+). This, in turn, via NCX, modulates local Ca(2+), jER Ca(2+) storage, Ca(2+) signaling, and cell responses.
免疫细胞化学分析显示,神经元胞体和星形胶质细胞中的钠钙交换体(NCX)局限于位于突触后膜(junctional)内质网(jER)上方的质膜(PM)微区。相比之下,质膜钙泵(PMCA)在质膜中的分布更为均匀。在突触前神经末梢,NCX的分布与在神经元胞体中观察到的一致,但PMCA聚集在活性区。因此,对钙离子具有高亲和力(K(d)约为100 nM)的PMCA可能使活性区的钙离子浓度保持在极低水平,从而在活动后“重置”囊泡释放机制。另一方面,对钙离子亲和力较低(K(d)约为1000 nM)的NCX可能会排出从活性区扩散并暂时被内质网储存的钙离子。含有NCX的质膜微区还含有钠泵高哇巴因亲和力的α2(星形胶质细胞)或α3(神经元)亚基同工型(IC(50)约为5 - 50 nM哇巴因)。相比之下,α1同工型(在啮齿动物中对哇巴因亲和力低;IC(50) >10000 nM),与PMCA一样,在这些细胞中分布更为均匀。神经元(可能还有胶质细胞和其他细胞类型)中的突触后膜内质网与相邻的质膜形成类似于心肌二联体的连接。我们认为,含有NCX和α2/α3钠泵的质膜微区、其下方的jER以及其间微小的胞质体积(<10(-18) l)形成功能单元(质膜内质网体);钠离子和钙离子在这些胞质区室与“大量”胞质之间的扩散可能受到显著限制。具有α2/α3亚基的钠泵的活性可能因此调节NCX活性和jER钙离子含量。在α2钠泵基因表达减少(约50%)的小鼠中的研究支持了这一观点:尽管胞质钠离子和静息钙离子浓度(Na(+)和Ca(2+))正常,但这些细胞中诱发的钙离子瞬变增强。我们得出结论,α2/α3钠泵控制质膜内质网体(局部)Na(+)。进而,通过NCX,这又调节局部Ca(2+)、jER钙离子储存、钙离子信号传导和细胞反应。
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