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破骨细胞中钠/钙交换体NCX-1的鉴定、特性及其在骨吸收中的作用

Identification and characterization of a sodium/calcium exchanger, NCX-1, in osteoclasts and its role in bone resorption.

作者信息

Moonga B S, Davidson R, Sun L, Adebanjo O A, Moser J, Abedin M, Zaidi N, Huang C L, Zaidi M

机构信息

Mount Sinai Bone Program, Department of Medicine, Mount Sinai School of Medicine, and Bronx Veteran's Affairs Geriatric Research Education and Clinical Center, New York, New York 10029, USA.

出版信息

Biochem Biophys Res Commun. 2001 May 18;283(4):770-5. doi: 10.1006/bbrc.2001.4870.

Abstract

We provide the first demonstration for a Na+/Ca2+ exchanger, NCX-1, in the osteoclast. We speculate that by using Na+ exchange, NCX-1 couples H+ extrusion with Ca2+ fluxes during bone resorption. Microspectrofluorimetry of fura-2-loaded osteoclasts revealed a rapid and sustained, but reversible, cytosolic Ca2+ elevation upon Na+ withdrawal. This elevation was abolished by the cytosolic introduction (by gentle permeabilization) of a highly specific Na+/Ca2+ exchange inhibitor peptide, XIP, but not its inactive analogue, sXIP. Confocal microscopy revealed intense plasma membrane immunofluorescence with an isoform-specific monoclonal anti-NCX-1 antibody applied to gently permeabilized osteoclasts. Electrophysiological studies using excised outside-in membrane patches showed a low-conductance, Na+-selective, dichlorobenzamil-sensitive, amiloride-insensitive channel that we tentatively assigned as being an NCX. Finally, to examine for physiological relevance, an osteoclast resorption (pit) assay was performed. There was a dramatic reduction of bone resorption following NCX-1 inhibition by dichlorobenzamil and XIP (but not with S-XIP). Together, the results suggest that a functional NCX, likely NCX-1, is involved in the regulation of osteoclast cytosolic Ca2+ and bone resorption.

摘要

我们首次在破骨细胞中证实了钠钙交换体NCX-1的存在。我们推测,在骨吸收过程中,NCX-1通过钠交换将氢离子的排出与钙离子的流动联系起来。用fura-2负载破骨细胞进行的显微荧光测定显示,去除钠离子后,细胞溶质钙离子迅速且持续升高,但这种升高是可逆的。通过(轻柔通透处理)向细胞溶质中引入一种高度特异性的钠钙交换抑制剂肽XIP可消除这种升高,但引入其无活性类似物sXIP则无效。共聚焦显微镜检查显示,将一种亚型特异性单克隆抗NCX-1抗体应用于轻柔通透处理的破骨细胞时,质膜出现强烈的免疫荧光。使用切除的外向内膜片进行的电生理研究显示,存在一种低电导、钠选择性、对二氯苯甲酰胺敏感、对氨氯地平不敏感的通道,我们初步将其认定为NCX。最后,为了检验其生理相关性,进行了破骨细胞吸收(凹陷)试验。用二氯苯甲酰胺和XIP抑制NCX-1后(但用S-XIP抑制则无此效果),骨吸收显著减少。总之,这些结果表明,一种功能性的NCX,可能是NCX-1,参与了破骨细胞胞质钙离子的调节和骨吸收过程。

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