首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Effects of osmolality and oxygen availability on soluble cyclic AMP-dependent protein kinase activity of rat renal inner medulla.
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Effects of osmolality and oxygen availability on soluble cyclic AMP-dependent protein kinase activity of rat renal inner medulla.

机译:重量克分子渗透压浓度和氧利用率对大鼠肾内髓质可溶性环AMP依赖性蛋白激酶活性的影响。

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摘要

The renal inner medulla is ordinarily exposed to osmolalities that are much higher and to O2 tensions that are lower than those in other tissues. The effects of media osmolality and O2 availability on basal and arginine vasopressin(AVP)-responsive soluble cyclic (c)AMP-dependent protein kinase activity were examined in slices of rat inner medulla. Increasing total media osmolality from 305 to 750 or 1,650 mosM by addition of urea plas NaCl to standard Krebs-Ringer bicarbonate buffer significantly reduced basal cAMP content and protein kinase activity ratios. This occurred in the presence or absence of O2. Incubation of slices in high osmolality buffer also blunted increases in inner medullary slice cAMP and protein kinase activity ratios induced by O2. These changes reflected predominantly an action of the urea rather than the NaCl content of high osmolality buffers. In contrast to effects on basal activity, high media osmolality significantly enhanced activation of inner medullary protein kinase by AVP. Conversely, increases in media O2 content suppressed AVP stimulation of enzyme activity. This inhibitory effect of O2 was best expressed at low osmolality. Naproxen and ibuprofen, inhibitors of prostaglandin biosynthesis, reduced basal kinase activity ratios and increased AVP responsiveness in the presence, but not in the absence, of O2. Exogenous prostaglandins (PG) modestly increased (PGE2 and PGE1) or did not change (PGF2alpha) cAMP and protein kinase activity ratios in O2-deprived inner medullary slices. Protein kinase activation by PGE2 was not observed in oxygenated inner medulla with high basal activity ratios. The stimulatory effects of PGE2 and PGE1 on protein kinase activity observed in O2-deprived slices were additive with those of submaximal or maximal AVP. PGE2, PGE1, and PGF2alpha all failed to suppress AVP activation of protein kinase. Thus, enhanced endogenous PGE production may contribute to the higher basal protein kinase activity ratios induced by O2. However, the results do not support a role for PGE2, PGE1, or PGF2alpha in O2-mediated inhibition of AVP responsiveness. The present data indicate that both solute content and O2 availability can alter the expression of AVP action on cAMP-dependent protein kinase activity in inner medulla. AVP activation of protein kinase is best expressed when osmolality is high and O2 availability is low, conditions that pertain in inner medulla during hydropenia.
机译:肾内髓质通常暴露于比其他组织更高的渗透压和更低的O2张力。介质渗透压和氧气供应对基础和精氨酸升压素(AVP)响应的可溶性环(c)AMP依赖性蛋白激酶活性的影响在大鼠内延髓切片中进行了检查。通过向标准Krebs-Ringer碳酸氢盐缓冲液中添加尿素pla NaCl,将总介质渗透压从305升至750或1,650 mosM,可以显着降低基础cAMP含量和蛋白激酶活性比。这是在有或没有氧气的情况下发生的。在高渗透压缓冲液中孵育切片也使由O2诱导的内髓切片cAMP和蛋白激酶活性比率的增加受到抑制。这些变化主要反映了尿素的作用,而不是高克分子渗透浓度缓冲液的NaCl含量。与对基础活性的影响相反,高渗透压渗透压显着增强了AVP对内髓质蛋白激酶的激活。相反,培养基中O2含量的增加抑制了AVP对酶活性的刺激。 O2的这种抑制作用在低摩尔渗透压浓度下表现得最好。萘普生和布洛芬是前列腺素生物合成的抑制剂,在存在但不存在氧气的情况下,降低了基础激酶活性比并增加了AVP反应性。在缺氧的内髓质切片中,外源性前列腺素(PG)适度增加(PGE2和PGE1)或不改变(PGF2alpha)cAMP和蛋白激酶活性比率。在具有高基础活性比率的氧化内髓中未观察到PGE2激活的蛋白激酶。在缺氧的切片中观察到的PGE2和PGE1对蛋白激酶活性的刺激作用与亚最大或最大AVP的作用相加。 PGE2,PGE1和PGF2alpha均不能抑制蛋白激酶的AVP激活。因此,增强的内源性PGE产生可能有助于由O2诱导的更高的基础蛋白激酶活性比率。但是,该结果不支持PGE2,PGE1或PGF2alpha在O2介导的AVP响应抑制中的作用。目前的数据表明溶质含量和O2可用性都可以改变内在髓质中对cAMP依赖性蛋白激酶活性的AVP作用的表达。当重量克分子渗透压浓度高和O2利用率低时,蛋白激酶的AVP激活最能表达,这种状态与水培期间内延髓有关。

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