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[氢离子ATP酶在气道平滑肌质膜中的作用]

[Role of H+ ATPases in plasma membranes of airway smooth muscle].

作者信息

Pacheco G, de Alfonzo R G, de Bécemberg I L, Alfonzo M J

机构信息

Cátedra de Bioquímica y Patología General, Universidad Central de Venezuela, Caracas.

出版信息

Acta Cient Venez. 1993;44(2):111-9.

PMID:8085404
Abstract

Protons generated inside the cells during metabolic activity have to be extruded through active mechanisms from the intracellular to the extracellular space. One of the systems involved in proton transport across membranes are the V-ATPases, which are oligomeric complexes that have been found in several subcellular organelles energizing such organelle through a proton gradient and a membrane potential. In this paper, a V-ATPase activity has been described at the plasma membranes fractions isolated from airway smooth muscle. This activity was measured as a Cl- stimulated Mg2+ ATPase. This Cl- activating effect was also shared by others halogens as I- and Br- but not F-. This Cl- stimulated ATPase is a nucleotide triphosphatase being unable to hydrolyze mono and dinucleotides. The divalent cations showed the following sequence of activation (Mg2+ > Mn2+ > Ca2+) of the Cl- activated Mg2+ ATPase. This Cl- stimulated Mg2+ ATPase was insensitive to ouabain, vanadate, sodium azide and rutamicina. NEM (N-ethylmaleimide) partially inhibited this activity but a complete inhibition was observed with p-CMB (p-chloromercurbenzoate ). Several specific proton transport inhibitors were employed to show the presence of a H+ pump activity. Thus, the strong inhibition induced by DCCD suggest the existence of hydrophobic subunits related to a proton channel. In addition, protonophores as 1799 and FCCP stimulated the Cl- stimulated ATPase indicating the presence of a H+ pump in these plasma membranes vesicles. The chloride requirement could be explained by the existence of a chloride conductor coupled to the proton pump (H+ ATPase-type V) due to the inhibitory effect of duramycin.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

代谢活动期间细胞内产生的质子必须通过主动机制从细胞内转运到细胞外空间。参与跨膜质子转运的系统之一是V-ATP酶,它是一种寡聚复合物,存在于几种亚细胞器中,通过质子梯度和膜电位为这些细胞器提供能量。在本文中,已描述了从气道平滑肌分离的质膜组分中的V-ATP酶活性。该活性通过Cl-刺激的Mg2+ ATP酶来测量。这种Cl-激活作用也为其他卤素如I-和Br-所共有,但F-没有。这种Cl-刺激的ATP酶是一种核苷酸三磷酸酶,无法水解单核苷酸和二核苷酸。二价阳离子对Cl-激活的Mg2+ ATP酶显示出以下激活顺序(Mg2+ > Mn2+ > Ca2+)。这种Cl-刺激的Mg2+ ATP酶对哇巴因、钒酸盐、叠氮化钠和鱼藤酮不敏感。N-乙基马来酰亚胺(NEM)部分抑制了该活性,但对氯汞苯甲酸(p-CMB)则观察到完全抑制。使用了几种特异性质子转运抑制剂来显示H+泵活性的存在。因此,二环己基碳二亚胺(DCCD)诱导的强烈抑制表明存在与质子通道相关的疏水亚基。此外,质子载体如1799和羰基氰化物间氯苯腙(FCCP)刺激了Cl-刺激的ATP酶,表明这些质膜囊泡中存在H+泵。由于短杆菌肽的抑制作用,氯离子的需求可以通过与质子泵(V型H+ ATP酶)偶联的氯离子导体的存在来解释。(摘要截短于250字)

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