首页> 美国卫生研究院文献>Biochemical Journal >Regulation of the gastric microsomal (H+ + K+)-transporting ATPase system by the endogenous activator. Effect of phospholipase A2 treatment.
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Regulation of the gastric microsomal (H+ + K+)-transporting ATPase system by the endogenous activator. Effect of phospholipase A2 treatment.

机译:内源性激活剂调节胃微粒体(H + + K +)转运ATPase系统。磷脂酶A2处理的效果。

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摘要

Pig gastric microsomal (H+ + K+)-stimulated ATPase activity was nearly abolished within 10 min of digestion with phospholipase A2 at room temperature. The enzyme activity could be largely restored by a cytosolic activator protein partially purified from the gastric cells. The K+ sensitivity and turnover of 32P-labelled intermediates produced by the control and the activator-reconstituted microsomal (H+ + K+)-stimulated ATPase were closely similar but were widely different to those from treated membranes without activator reconstitution. The data suggest an essential requirement for the endogenous activator for gastric (H+ + K+)-stimulated ATPase function.
机译:在室温下用磷脂酶A2消化后10分钟内,猪胃微粒体(H + + K +)刺激的ATPase活性几乎消失。从胃细胞中部分纯化的胞质激活蛋白可以大大恢复酶的活性。对照和活化剂重构的微粒体(H + + K +)刺激的ATPase产生的32P标记中间体的K +敏感性和周转率非常相似,但与没有活化剂重构的处理过的膜相比,差异很大。数据表明内源性激活剂对胃(H + + K +)刺激的ATPase功能具有基本要求。

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