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哺乳动物壁细胞中酸分泌的部位。

The site of acid secretion in the mammalian parietal cell.

作者信息

Scott D R, Helander H F, Hersey S J, Sachs G

机构信息

Department of Physiology and Medicine, UCLA.

出版信息

Biochim Biophys Acta. 1993 Feb 23;1146(1):73-80. doi: 10.1016/0005-2736(93)90340-6.

Abstract

Initiation of acid secretion in the gastric mucosa is accompanied by a morphological transformation in which the acid pump, the H+/K(+)-ATPase, translocates from a cytoplasmic vesicular location to the secretory surface lining the canaliculi. Associated with the morphological changes, activation of K+ and Cl- pathways are necessary to supply K+ to the extracytoplasmic face of the pump. Although the pump in the secretory membrane is known to secrete acid, it is not known whether activation of the KCl pathway occurs in the tubulovesicular membrane prior to the formation of the canaliculus, or when the pump is in the secretory membrane. The cellular site of activation of acid secretion in the rabbit gastric parietal cell was investigated using the covalent binding of [3H]omeprazole as a probe of acid secretion in rabbit gastric glands that were undergoing stimulation in vitro. This compound depends on an acidic environment for activation and covalent binding to the H+/K(+)-ATPase. Electron microscopic autoradiography showed that activation of the enzyme occurred only when it was present in the canalicular membrane and not when it was present in the cytoplasmic tubulovesicular membrane. Hence there is likely to be a physical separation of K+ and/or Cl- pathways from the ATPase in the resting cell, and stimulation of acid secretion is dependent on colocalization of these pathways in the canalicular membrane.

摘要

胃黏膜中酸分泌的起始伴随着一种形态学转变,其中酸泵,即H⁺/K⁺-ATP酶,从细胞质囊泡位置转运至衬于小管的分泌表面。与形态学变化相关,激活K⁺和Cl⁻途径对于向泵的胞外表面供应K⁺是必要的。虽然已知分泌膜中的泵分泌酸,但尚不清楚KCl途径的激活是在小管形成之前发生于微管泡膜中,还是在泵位于分泌膜时发生。利用[³H]奥美拉唑的共价结合作为体外受刺激的兔胃腺中酸分泌的探针,研究了兔胃壁细胞中酸分泌激活的细胞位点。该化合物依赖酸性环境进行激活并与H⁺/K⁺-ATP酶共价结合。电子显微镜放射自显影显示,该酶仅当其存在于小管膜中时才被激活,而当其存在于细胞质微管泡膜中时则不被激活。因此,在静息细胞中,K⁺和/或Cl⁻途径与ATP酶可能存在物理分离,而酸分泌的刺激取决于这些途径在小管膜中的共定位。

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