Enhanced pressor response to increased CSF sodium concentration and to central ANG I in heterozygous α2 Na+-K+-ATPase knockout mice

机译：对杂合性α2Na + -K + -ATPase敲除小鼠的CSF钠浓度升高和中枢ANG I的升压反应增强

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Intracerebroventricular (ICV) infusion of NaCl mimics the effects of a high-salt diet in salt-sensitive hypertension, raising the sodium concentration in the cerebrospinal fluid (CSF [Na]) and subsequently increasing the concentration of an endogenous ouabain-like substance (OLS) in the brain. The OLS, in turn, inhibits the brain Na⁺-K⁺-ATPase, causing increases in the activity of the brain renin-angiotensin system (RAS) and blood pressure. The Na⁺-K⁺-ATPase α (catalytic)-isoform(s) that mediates the pressor response to increased CSF [Na] is unknown, but it is likely that one or more isoforms that bind ouabain with high affinity are involved (e.g., the Na⁺-K⁺-ATPase α2- and/or α3-subunits). We hypothesize that OLS-induced inhibition of the α2-subunit mediates this response. Therefore, a chronic reduction in α2 expression via a heterozygous gene knockout (α2 +/−) should enhance the pressor response to increased CSF [Na]. Intracerebroventricular (ICV) infusion of artificial CSF containing 0.225 M NaCl increased mean arterial pressure (MAP) in both wild-type (+/+) and α2 +/− mice, but to a greater extent in α2 +/−. Likewise, the pressor response to ICV ouabain was enhanced in α2 +/− mice, demonstrating enhanced sensitivity to brain Na⁺-K⁺-ATPase inhibition per se. The pressor response to ICV ANG I but not ANG II was also enhanced in α2 +/− vs. α2+/+ mice, suggesting an enhanced brain RAS activity that may be mediated by increased brain angiotensin converting enzyme (ACE). The latter hypothesis is supported by enhanced ACE ligand binding in the organum vasculosum laminae terminalis. These studies demonstrate that chronic downregulation of Na⁺-K⁺-ATPase α2-isoform expression by heterozygous knockout increases the pressor response to increased CSF [Na] and activates the brain RAS. Since these changes mimic those produced by the endogenous brain OLS, the brain α2-isoform may be a target for the brain OLS during increases in CSF [Na], such as in salt-dependent hypertension.

机译：脑室内（ICV）输注NaCl模仿盐敏感型高血压中高盐饮食的作用，增加脑脊髓液（CSF [Na]）中的钠浓度，随后增加内源性哇巴因样物质（OLS）的浓度）在大脑中。 OLS依次抑制脑Na ^{+ -K ^{+ -ATPase，导致脑肾素-血管紧张素系统（RAS）活性和血压升高。 Na ^{+ -K ^{+ -ATPaseα（催化）-亚型介导升压对CSF [Na]的响应，但尚不清楚涉及一种或多种以高亲和力结合哇巴因的同工型（例如，Na ^{+ -K ^{+ -ATPaseα2-和/或α3-亚基）。我们假设OLS诱导的对α2-亚基的抑制介导了这种反应。因此，通过杂合基因敲除（α2+/-）导致α2表达的慢性减少应增强对升高的CSF [Na]的升压反应。含有0.225 M NaCl的人工CSF的脑室内（ICV）输注在野生型（+ / +）和α2+/-小鼠中均增加了平均动脉压（MAP），但在α2+/-中则更大。同样，α2+/-小鼠对ICV哇巴因的升压反应增强，表明对脑Na ^{+ -K ^{+ -ATPase抑制的敏感性增强。与α2+ / +小鼠相比，α2+/-小鼠对ICV ANG I而不是ANG II的压力反应也得到了增强，表明脑RAS活性增强，这可能是由脑血管紧张素转化酶（ACE）的增加介导的。后者的假说是由末端器官中的增强的ACE配体结合所支持的。这些研究表明，杂合敲除对Na ^{+ -K ^{+ -ATPaseα2-同工型表达的慢性下调增加了对升高的CSF [Na]的升压反应并激活了脑RAS。。由于这些变化模拟了内源性大脑OLS产生的变化，因此在CSF [Na]升高（例如盐依赖性高血压）期间，大脑α2-同种型可能成为大脑OLS的靶标。}}}}}}}}}}

著录项

期刊名称 American Journal of Physiology - Regulatory Integrative and Comparative Physiology
作者
Xiaohong Hou; Steven F. Theriault; Iva Dostanic-Larson; Amy E. Moseley; Jerry B Lingrel; Hengwei Wu; Stephanie Dean; James W. Van Huysse;
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作者单位

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年(卷),期 -1(296),5
年度 -1
页码 R1427–R1438
总页数 4
原文格式 PDF
正文语种
中图分类人体生理学;
关键词
α2-isoform gene knockout sodium chloride brain ouabain-like substance brain renin-angiotensin system intracerebroventricular infusion;

机译：α2-同工型;基因敲除;氯化钠;脑哇巴因样物质;脑肾素-血管紧张素系统;脑室内灌注;

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专利

1. Enhanced pressor response to increased CSF sodium concentration and to central ANG I in heterozygous α 2 Na +-K +-ATPase knockout mice [J] . Hou, X., Theriault, American Journal of Physiology . 2009,第5aPta2期

机译：增强的压力响应增加CSF钠浓度和杂合α2NA+ -K + -ATP酶敲除小鼠的COSE ANG I
2. Increased extracellular dopamine concentrations and FosB/DeltaFosB expression in striatal brain areas of heterozygous GDNF knockout mice. [J] . Airavaara M, Planken A, Gaddnas H, The European Journal of Neuroscience . 2004,第9期

机译：杂合的GDNF基因敲除小鼠的纹状体脑区域中的细胞外多巴胺浓度和FosB / DeltaFosB表达增加。
3. Collecting duct prorenin receptor knockout reduces renal function, increases sodium excretion, and mitigates renal responses in ANG II-induced hypertensive mice [J] . Minolfa C. Prieto, Virginia Reverte, Mykola Mainenko, American Journal of Physiology . 2017,第6Pta2期

机译：收集管道Prorenin受体敲除降低肾功能，增加排泄钠，并减轻昂氏诱导的高血压小鼠中的肾反应
4. QUANTIFICATION OF THE BIOMECHANICAL DIFFERENCES IN WILD-TYPE AND HETEROZYGOUS TGF BETA2 KNOCKOUT MICE [C] . Joseph T Keyes, Stacy Borowicz, Urs Utzinger, ASME summer bioengineering conference;SBC2010 . 2010

机译：定量检测野生型和异质TGF BETA2敲除小鼠的生物力学差异
5. A role for the brain sodium, potassium-ATPase alpha2 isoform in salt-sensitive hypertension: Enhanced pressor responses to increased CSF sodium and ouabain concentrations in gene-targeted heterozygous alpha2 sodium, potassium-ATPase knockout mice. [D] . Theriault, Steven F. 2005

机译：盐敏感性高血压中脑钠钾ATP酶α2同工型的作用：基因靶向杂合α2钠钾ATP酶敲除小鼠对增强的CSF钠和哇巴因浓度的升压反应。
6. Collecting duct prorenin receptor knockout reduces renal function increases sodium excretion and mitigates renal responses in ANG II-induced hypertensive mice [O] . Minolfa C. Prieto, Virginia Reverte, Mykola Mamenko, -1

机译：收集导管肾上腺素受体敲除可降低肾功能增加钠排泄并减轻ANG II诱导的高血压小鼠的肾脏反应
7. Enhanced pressor response to increased CSF sodium concentration and to central ANG I in heterozygous α2 Na+-K+-ATPase knockout mice [O] . Hou, Xiaohong, Theriault, Steven F., Dostanic-Larson, Iva, 2009

机译：对杂合性α2Na + -K + -ATPase基因敲除小鼠的CSF钠浓度升高和中枢ANG I的升压反应增强

Enhanced pressor response to increased CSF sodium concentration and to central ANG I in heterozygous α2 Na+-K+-ATPase knockout mice

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