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人尿中的哇巴因样因子:鉴定一种钠钾ATP酶抑制剂为钒-抗坏血酸加合物。

Ouabain-like factors in human urine: identification of a Na-K-ATPase inhibitor as vanadium-diascorbate adduct.

作者信息

Kramer H J, Krampitz G, Bäcker A, Meyer-Lehnert H

机构信息

Medical Policlinic/Department of Medicine, University of Bonn, Germany.

出版信息

Clin Exp Hypertens. 1998 Jul-Aug;20(5-6):557-71. doi: 10.3109/10641969809053234.

Abstract

We investigated endogenous Na-K-ATPase inhibitors, i.e. ouabain-like factors(OLFs), in the urine of salt-loaded healthy subjects. During an intake of > 30g NaCl/day 24h-urines were collected, lyophilized, redissolved and acidified to pH 3.5. With gelchromatography the inhibitory activity eluted in a post-salt fraction FIV from Sephadex G-25. When this fraction was again passed through Sephadex G-10, one of three OLFs eluted in the early subfractions FIV/1-2 close to H-ouabain and cross-reacted strongly with a ouabain antibody (NEN). Two additional OLFs with Mr around 400 eluted in a late subfraction FIV/8 which resolved after reverse-phase HPLC into a more polar OLF- (water phase) and a more apolar OLF-2 (20% acetonitrile). Only the more apolar OLF-2 cross-reacted with digoxin and ouabain antibodies. OLF-1 and OLF-2 purified to single compounds by preparative thin layer chromatography inhibited Na-K-ATPase with IC50 of around 1.5 x 10(-5) M and 1.5 x 10(-4) M, respectively. Identification of OLF-2 was first attempted because most material was available for further processing. Data from mass-spectroscopy, nuclear magnetic resonance (1H-NMR) and infrared spectroscopy characterized OLF-2 as structurally unrelated to ouabain but resembling ascorbic acid derivatives, i.e. vanadium (V) diascorbates (Mr 403) with similar elution times from RP-HPLC as OLF-2. They inhibited the enzyme in its E2-configuration with IC50 of 9 x 10(-5) M and 2 x 10(-6) M for V(IV)- and V(V)-diascorbate, respectively. OLF-1, OLF-2 and V-diascorbate raise intracellular free calcium in inner medullary collecting duct and vascular smooth muscle cells which also contract in vitro. V-diascorbate was also natriuretic in a bioassay. We suggest that V-diascorbates represent one of several OLFs excreted in human urine.

摘要

我们研究了盐负荷健康受试者尿液中的内源性钠钾ATP酶抑制剂,即哇巴因样因子(OLFs)。在每日摄入超过30g氯化钠期间,收集24小时尿液,冻干,重新溶解并酸化至pH 3.5。通过凝胶色谱法,抑制活性在Sephadex G - 25的盐后级分FIV中洗脱。当该级分再次通过Sephadex G - 10时,三种OLFs之一在接近H - 哇巴因的早期亚级分FIV/1 - 2中洗脱,并与哇巴因抗体(NEN)发生强烈交叉反应。另外两种分子量约为400的OLFs在后期亚级分FIV/8中洗脱,经反相高效液相色谱法分离为极性更强的OLF - 1(水相)和极性更弱的OLF - 2(20%乙腈)。只有极性更弱的OLF - 2与地高辛和哇巴因抗体发生交叉反应。通过制备薄层层析法纯化至单一化合物的OLF - 1和OLF - 2分别以约1.5×10⁻⁵M和1.5×10⁻⁴M的IC50抑制钠钾ATP酶。由于有更多材料可用于进一步处理,首先尝试对OLF - 2进行鉴定。质谱、核磁共振(¹H - NMR)和红外光谱数据表明,OLF - 2在结构上与哇巴因无关,但类似于抗坏血酸衍生物,即钒(V)双抗坏血酸盐(分子量403),其从反相高效液相色谱法洗脱的时间与OLF - 2相似。它们分别以9×10⁻⁵M和2×10⁻⁶M的IC50抑制处于E2构型的酶,对于V(IV) - 双抗坏血酸盐和V(V) - 双抗坏血酸盐而言。OLF - 1、OLF - 2和V - 双抗坏血酸盐可提高髓质内集合管和血管平滑肌细胞内的游离钙,这些细胞在体外也会收缩。在生物测定中,V - 双抗坏血酸盐也具有利钠作用。我们认为V - 双抗坏血酸盐是人类尿液中排泄的几种OLFs之一。

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