首页> 美国卫生研究院文献>Biochemical Journal >Role of membrane-associated thiol groups in the functional regulation of gastric microsomal (H+ + K+)-transporting ATPase system.
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Role of membrane-associated thiol groups in the functional regulation of gastric microsomal (H+ + K+)-transporting ATPase system.

机译:膜相关巯基在胃微粒体(H + + K +)转运ATPase系统功能调节中的作用。

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摘要

The distribution of free thiol groups associated with the membrane proteins of the purified pig gastric microsomal vesicles was quantified, and the relation of thiol groups to the function of the gastric (H+ + K+)-transporting ATPase system was investigated. Two different thiol-specific agents, carboxypyridine disulphide (CPDS) and N-(1-naphthyl)maleimide (NNM) were used for the study. The structure-function relationship of the membrane thiol groups was studied after modification by the probes under various conditions, relating the inhibition of the (H+ + K+)-transporting ATPase to the ATP-dependent H+ accumulation by the gastric microsomal vesicles. On the basis of the extent of stimulation of the microsomal (H+ + K+)-transporting ATPase in the presence and absence of valinomycin (val) about 85% of the vesicles were found to be intact. CPDS at 1 mM completely inhibits the valinomycin-stimulated ATPase and the associated p-nitrophenyl phosphatase with a concomitant inhibition of vesicular H+ uptake. Both the enzyme and dye-uptake activities were fully protected against CPDS inhibition when the treatment with CPDS was carried out in the presence of ATP. ATP also offered protection (about 65%) against NNM inhibition of the (H+ + K+)-transporting ATPase system and vesicular H+ uptake. Under similar conditions ATP also protected about 10 and 6 nmol of thiol groups/mg of protein respectively from CPDS and NNM reaction. Our data suggest that the thiol groups on the outer surface of the vesicles are primarily involved in gastric (H+ + K+)-transporting ATPase function. Furthermore, at least about 15% of the total microsomal thiol groups appear to be associated with the ATPase system. The data have been discussed in terms of the structure-function relationship of gastric microsomes.
机译:定量与纯化的猪胃微粒体膜的膜蛋白相关的游离巯基的分布,并研究了巯基与胃(H + + K +)转运ATPase系统功能的关系。两种不同的巯基特异性试剂,羧基吡啶二硫化物(CPDS)和N-(1-萘基)马来酰亚胺(NNM)用于研究。在各种条件下用探针修饰后,研究了膜硫醇基团的结构-功能关系,将(H + + K +)转运ATPase的抑制作用与胃微粒体小泡对ATP依赖的H +积累有关。根据在存在和不存在缬氨霉素(val)的情况下对微粒体(H + + K +)运输ATP酶的刺激程度,发现约85%的囊泡是完整的。 1 mM的CPDS完全抑制了缬霉素刺激的ATPase和相关的对硝基苯基磷酸酶,同时抑制了水泡H +的吸收。当在ATP的存在下进行CPDS处理时,酶和染料吸收活性均受到CPDS抑制。 ATP还为NNM抑制(H + + K +)转运ATPase系统和水泡H +吸收提供了保护(约65%)。在相似的条件下,ATP还可以保护CPDS和NNM反应分别保护约10和6 nmol / mg蛋白质/毫克蛋白质。我们的数据表明,囊泡外表面的巯基主要参与胃(H + + K +)转运ATPase的功能。此外,总微粒体硫醇基团中至少约15%似乎与ATPase系统有关。已经根据胃微粒体的结构-功能关系讨论了数据。

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