首页> 外文期刊>The Journal of Physiology >Atrial natriuretic peptide modulation of albumin clearance and contrast agent permeability in mouse skeletal muscle and skin: role in regulation of plasma volume.
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Atrial natriuretic peptide modulation of albumin clearance and contrast agent permeability in mouse skeletal muscle and skin: role in regulation of plasma volume.

机译:心钠素调节白蛋白清除率和造影剂在小鼠骨骼肌和皮肤中的渗透性:在调节血浆容量中的作用。

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Atrial natriuretic peptide (ANP) via its guanylyl cyclase-A (GC-A) receptor participates in regulation of arterial blood pressure and vascular volume. Previous studies demonstrated that concerted renal diureticatriuretic and endothelial permeability effects of ANP cooperate in intravascular volume regulation. We show that the microvascular endothelial contribution to the hypovolaemic action of ANP can be measured by the magnitude of the ANP-induced increase in blood-to-tissue albumin transport, measured as plasma albumin clearance corrected for intravascular volume change, relative to the corresponding increase in ANP-induced renal water excretion. We used a two-tracer method with isotopically labelled albumin to measure clearances in skin and skeletal muscle of: (i) C57BL6 mice; (ii) mice with endothelium-restricted deletion of GC-A (floxed GC-A x tie2-Cre: endothelial cell (EC) GC-A knockout (KO)); and (iii) control littermates (floxed GC-A mice with normal GC-A expression levels). Comparison of albumin clearances in hypervolaemic EC GC-A KO mice with normovolaemic littermates demonstrated that skeletal muscle albumin clearance with ANP treatment accounts for at most 30% of whole body clearance required for ANP to regulate plasma volume. Skin microcirculation responded to ANP similarly. Measurements of permeability to a high molecular mass contrast agent (35 kD Gadomer) by dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI) enabled repeated measures in individual animals and confirmed small increases in muscle and skin microvascular permeability after ANP. These quantitative methods will enable further evaluation of the contribution of ANP-dependent microvascular beds (such as gastro-intestinal tract) to plasma volume regulation.
机译:心钠素通过鸟苷酸环化酶-A(GC-A)受体参与调节动脉血压和血管容量。先前的研究表明,ANP的协同的肾脏利尿/利尿钠和内皮通透性作用在血管内体积调节中协同作用。我们表明,微血管内皮对ANP的降血容量作用的贡献可以通过ANP诱导的血液向组织白蛋白转运的增加的幅度来衡量,以血浆白蛋白清除率校正为血管内体积变化(相对于相应的增加)来衡量在ANP引起的肾水排泄中。我们使用同位素标记白蛋白的二次示踪法来测量以下动物的皮肤和骨骼肌中的清除率:(i)C57BL6小鼠; (ii)具有内皮细胞限制的GC-A缺失的小鼠(固定的GC-A x tie2-Cre:内皮细胞(EC)GC-A敲除(KO)); (iii)对照同窝仔(具有正常GC-A表达水平的固定GC-A小鼠)。比较高血容量EC GC-A KO小鼠与正绒毛同窝小鼠的白蛋白清除率,结果表明,采用ANP处理的骨骼肌白蛋白清除率最多占ANP调节血浆量所需的全身清除率的30%。皮肤微循环对ANP的反应相似。通过动态对比增强磁共振成像(DCE-MRI)测量对高分子量造影剂(35 kD Gadomer)的渗透性,可以对单个动物进行重复测量,并确认ANP后肌肉和皮肤微血管渗透性的小幅增加。这些定量方法将能够进一步评估依赖ANP的微血管床(例如胃肠道)对血浆容量调节的贡献。

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