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晶体液输注对酸碱状态的物理化学模型。

A physicochemical model of crystalloid infusion on acid-base status.

机构信息

Alta Bates Summit Medical Center, Oakland, CA, USA.

出版信息

J Intensive Care Med. 2010 Sep;25(5):271-80. doi: 10.1177/0885066610371633.

Abstract

The objective of this study is to develop a physicochemical model of the projected change in standard base excess (SBE) consequent to the infused volume of crystalloid solutions in common use. A clinical simulation of modeled acid-base and fluid compartment parameters was conducted in a 70-kg test participant at standard physiologic state: pH =7.40, partial pressure of carbon dioxide (PCO2) = 40 mm Hg, Henderson-Hasselbalch actual bicarbonate ([HCO3]HH) = 24.5 mEq/L, strong ion difference (SID) = 38.9 mEq/L, albumin = 4.40 g/dL, inorganic phosphate = 1.16 mmol/L, citrate total = 0.135 mmol/L, and SBE =0.1 mEq/L. Simulations of multiple, sequential crystalloid infusions up to 10 L were conducted of normal saline (SID = 0), lactated Ringer's (SID = 28), plasmalyte 148 (SID = 50), one-half normal saline þ 75 mEq/L sodium bicarbonate (NaHCO3; SID = 75), 0.15 mol/L NaHCO3 (SID = 150), and a hypothetical crystalloid solution whose SID = 24.5 mEq/L, respectively. Simulations were based on theoretical completion of steady-state equilibrium and PCO2 was fixed at 40 mm Hg to assess nonrespiratory acid-base effects. A crystalloid SID equivalent to standard state actual bicarbonate (24.5 mEq/L) results in a neutral metabolic acid-base status for infusions up to 10 L. The 5 study solutions exhibited curvilinear relationships between SBE and crystalloid infusion volume in liters. Solutions whose SID was greater than 24.5 mEq/L demonstrated a progressive metabolic alkalosis and less, a progressive metabolic acidosis. In a human model system, the effects of crystalloid infusion on SBE are a function of the crystalloid and plasma SID, volume infused, and nonvolatile plasma weak acid changes. A projection of the impact of a unit volume of various isotonic crystalloid solutions on SBE is presented. The model's validation, applications, and limitations are examined.

摘要

本研究的目的是建立一个物理化学模型,预测在输注常用晶体溶液后标准基础过剩(SBE)的变化。在一个标准生理状态的 70 公斤试验参与者中进行了酸-碱和液体隔室参数的临床模拟:pH = 7.40,二氧化碳分压(PCO2)= 40 mmHg,Henderson-Hasselbalch 实际碳酸氢盐([HCO3]HH)= 24.5 mEq/L,强离子差(SID)= 38.9 mEq/L,白蛋白= 4.40 g/dL,无机磷酸盐= 1.16 mmol/L,柠檬酸总量= 0.135 mmol/L,SBE = 0.1 mEq/L。模拟了多达 10 L 的生理盐水(SID = 0)、乳酸林格氏液(SID = 28)、血浆代用品 148(SID = 50)、半生理盐水+75 mEq/L 碳酸氢钠(NaHCO3;SID = 75)、0.15 mol/L NaHCO3(SID = 150)和假设的晶体溶液(SID = 24.5 mEq/L)的多次连续晶体输注。模拟基于稳态平衡的理论完成,PCO2 固定在 40 mmHg 以评估非呼吸性酸碱平衡的影响。晶体 SID 与标准实际碳酸氢盐(24.5 mEq/L)相等,导致输注 10 L 以下的中性代谢性酸碱平衡状态。5 种研究溶液的 SBE 与晶体输注量呈曲线关系。SID 大于 24.5 mEq/L 的溶液显示出进行性代谢性碱中毒,而 SID 小于 24.5 mEq/L 的溶液则显示出进行性代谢性酸中毒。在人体模型系统中,晶体输注对 SBE 的影响是晶体和血浆 SID、输注体积和非挥发性血浆弱酸变化的函数。提出了各种等渗晶体溶液单位体积对 SBE 影响的预测。检查了模型的验证、应用和局限性。

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