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己糖异硫氰酸酯对己糖转运蛋白抑制作用及标记的重新研究。

Re-examination of hexose-transporter inhibition and labelling by hexose isothiocyanates.

作者信息

Rees W D, Gliemann J, Holman G D

出版信息

Biochem J. 1987 Feb 1;241(3):857-62. doi: 10.1042/bj2410857.

Abstract

We have re-examined hexose-transport inhibition by hexose isothiocyanates and find that the inhibition is incomplete, probably because of decomposition of the reagent. The inhibition type is 'mixed', because hexose-transporter ligands such as maltose and cytochalasin B only give partial protection from inhibition. This suggests that a liganded-transporter-hexose isothiocyanate ternary complex is formed. We have compared the labelling of red-blood-cell membranes by [14C]MITC (D-maltose isothiocyanate) with the labelling obtained using a photoaffinity probe (ASA-BMPA [2-N-(4-azidosalicyloyl)-1,3-bis-(D-mannos-4'-yloxy)-2 -propylamine]) which gives specific labelling of the hexose transporter in band 4.5. [14C]MITC gives a partially D-glucose-displaceable labelling of a band 3 component in the same cell preparations which show ASA-BMPA labelling of band 4.5. This eliminates the possibility that band 4.5 labelling can only occur when the HITC (hexose isothiocyanate) binding protein in band 3 is proteolysed. HITC pretreatment does not decrease ASA-BMPA labelling of the exofacial site of band 4.5. This is also consistent with the formation of ternary complex. However, HITC pretreatment inhibits both reversible and photoactivated covalent [3H]cytochalasin B binding to band 4.5. These results suggest that, in the intact cell, interactions between a band 3 HITC-binding component and the inside cytochalasin B-binding site on the hexose transporter in band 4.5 may occur.

摘要

我们重新研究了异硫氰酸己糖对己糖转运的抑制作用,发现这种抑制并不完全,可能是由于试剂分解所致。抑制类型为“混合型”,因为诸如麦芽糖和细胞松弛素B等己糖转运体配体只能提供部分保护以防止抑制。这表明形成了一种配体-转运体-异硫氰酸己糖三元复合物。我们将[¹⁴C]MITC(D-麦芽糖异硫氰酸酯)对红细胞膜的标记与使用光亲和探针(ASA-BMPA [2-N-(4-叠氮水杨酰基)-1,3-双-(D-甘露糖-4'-氧基)-2-丙胺])获得的标记进行了比较,该探针能特异性标记4.5带中的己糖转运体。在显示4.5带ASA-BMPA标记的相同细胞制剂中,[¹⁴C]MITC对3带成分产生了部分可被D-葡萄糖置换的标记。这排除了只有当3带中的HITC(异硫氰酸己糖)结合蛋白被蛋白水解时才会发生4.5带标记的可能性。HITC预处理不会降低4.5带外表面位点的ASA-BMPA标记。这也与三元复合物的形成一致。然而,HITC预处理会抑制[³H]细胞松弛素B与4.5带的可逆结合和光活化共价结合。这些结果表明,在完整细胞中,3带HITC结合成分与4.5带己糖转运体上的细胞松弛素B结合位点内部之间可能会发生相互作用。

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