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Does regional norepinephrine spillover represent local sympathetic activity?

机译:区域去甲肾上腺素溢出是否代表局部交感神经活动?

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Regional spillover of norepinephrine (NE), based on isotope dilution and single-compartment steady-state kinetics, is considered one of the best parameters for estimating organ sympathetic activity. However, the effects of local changes in clearance of NE on the spillover have not yet been investigated. We studied local NE kinetics and clearance in the forearm of 10 healthy subjects using intra-arterial infusions of NE, tritiated NE, the neuronal uptake inhibitor desipramine, and tyramine, which competes with NE for the neuronal uptake carrier. Before and during complete blockade of neuronal uptake by desipramine the venous concentration-time curves for tritiated NE and for NE released by tyramine were biexponential, consistent with the presence of (at least) two compartments for circulating tritiated NE and for locally released NE. The time constants for tyramine-induced release of NE and, in the same subjects during desipramine infusion, for tritiated NE were almost equal at the same level of forearm blood flow. This argues against possible diffusion or transport differences for NE to and from the circulation and the synapse. The regional intrinsic clearance capacity (a measure of the maximal ability of an organ to irreversibly remove drug by all pathways in the absence of any flow limitations) for NE decreased in the forearm by 65% (p less than 0.01) during neuronal uptake blockade by desipramine; the forearm clearance decreased by 59% (p less than 0.001), whereas the spillover rate of NE increased from 33 +/- 5 to 63 +/- 11 pmol.min-1 (p less than 0.05). Nitroprusside-induced increments in blood flow increased the spillover of NE from 18 +/- 4 to 35 +/- 6 pmol.min-1 (p less than 0.01); the clearance of circulating NE also increased (by 58%, p less than 0.05), and the intrinsic clearance capacity remained unchanged. This demonstrates that regional spillover of NE is markedly influenced by local changes in clearance and flow. The new parameter plasma appearance rate of NE is proposed. Although also derived from isotope dilution, this parameter may better approximate the regional entry of NE into the blood pool than spillover. This is corroborated by the nonsignificant changes of plasma appearance rate of NE during our desipramine and nitroprusside infusions.
机译:基于同位素稀释和单室稳态动力学的去甲肾上腺素(NE)的区域溢出被认为是估计器官交感活性的最佳参数之一。但是,尚未研究NE清除率局部变化对溢出的影响。我们使用动脉内输注NE,tri化的NE,神经元摄取抑制剂desipramine和酪胺(与NE竞争神经元摄取载体)研究了10名健康受试者的前臂中的局部NE动力学和清除。在去昔帕明完全阻断神经元摄取之前和期间,tri化的NE和酪胺释放的NE的静脉血药浓度-时间曲线是双指数的,这与(至少)两个tri化的NE和局部释放的NE的间隔存在一致。在相同的前臂血流水平下,酪胺诱导的NE释放的时间常数,以及在去甲胺输注期间在同一受试者中,tri化的NE的时间常数几乎相等。这与NE在循环和突触之间可能存在的扩散或运输差异相抵触。 NE的神经元摄取阻滞期间,前臂的NE的区域固有清除能力(一种在没有任何血流限制的情况下通过所有途径不可逆转地去除所有药物的最大能力的一种量度)在神经元摄取阻滞期间降低了65%(p小于0.01)。地昔帕明前臂清除率降低了59%(p小于0.001),而NE的外溢率从33 +/- 5增加到63 +/- 11 pmol.min-1(p小于0.05)。硝普钠引起的血流量增加使NE的溢出从18 +/- 4增加到35 +/- 6 pmol.min-1(p小于0.01);循环NE的清除率也增加了(增加58%,P小于0.05),并且固有清除能力保持不变。这表明,NE的区域溢出明显受到清除率和流量局部变化的影响。提出了新的NE参数等离子体出现率。尽管也来自同位素稀释,但该参数可能比溢流更好地近似了NE进入血池的区域。在我们进行地昔帕明和硝普钠输注期间,NE的血浆出现率无显着变化,这印证了这一点。

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