Siggaard-Andersen algorithm-derived p50 parameters: perturbation by abnormal hemoglobin-oxygen affinity and acid-base disturbances.

T J Morgan, Z H Endre, D M Kanowski, L I Worthley, R D Jones
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Abstract

The p50 and derived indexes, calculated by using the Siggaard-Andersen algorithm from a single measurement of arterial blood gas tensions and hemoglobin-oxygen saturation, are used to assess tissue oxygen availability in critical illness. We tested the accuracy of the Siggaard-Andersen p50 algorithm over a wide range of pathophysiologic conditions. Blood gases, cooximetry, and calculation of standard and in vivo p50 were performed at multiple saturations, CO2 tensions, and H+ concentrations on blood with normal (standard p50 of 26.1 and 26.7 mm Hg), increased (19.0 and 25.4), and reduced (33.9 and 38.2) hemoglobin-oxygen affinity, as well as on high-affinity blood from two patients with diabetic ketoacidosis (16.7 and 20.8). Log p50 in vivo/pH plots were constructed to determine the Bohr effect. Except in the normal affinity specimens (coefficient of variation < 1.7%), standard p50 values showed high variability (coefficient of variation > 5.9%), with saturation-linked bias and distortion of the Bohr effect. Standard p50 was overestimated by up to 11 mm Hg as saturation approached 97%. Although base deficit correction of the stored specimens (6.9 < pH < 7.1) restored the Bohr effect and improved the accuracy of standard p50 calculations (coefficient of variation = 4.4% and 2.9%), saturation-linked bias persisted. We conclude that Siggaard-Andersen p50 calculations may be misleading when there are disturbances of hemoglobin-oxygen affinity and acid-base balance, owing to changes in shape of the hemoglobin-dissociation curve. When metabolic acidosis occurs with high hemoglobin-oxygen affinity, as can occur in critical illness, indexes derived by the Siggaard-Andersen algorithm on arterial blood may greatly overestimate oxygen availability.

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Siggaard-Andersen算法衍生的p50参数:异常血红蛋白-氧亲和和酸碱干扰的扰动。
使用Siggaard-Andersen算法从动脉血气张力和血红蛋白氧饱和度的单一测量中计算p50及其衍生指数,用于评估危重疾病的组织氧可用性。我们在广泛的病理生理条件下测试了Siggaard-Andersen p50算法的准确性。对两例糖尿病酮症酸中毒患者(16.7和20.8)的高亲和血,在多种饱和度、CO2张力和H+浓度下正常(标准p50为26.1和26.7 mm Hg)、升高(19.0和25.4)、降低(33.9和38.2)血红蛋白氧亲和度的血液进行血气、共氧测定和标准和体内p50的计算。构建logp50体内/pH图来确定玻尔效应。除正常亲和样品(变异系数< 1.7%)外,标准p50值表现出高变异性(变异系数> 5.9%),存在饱和相关偏差和玻尔效应失真。当饱和度接近97%时,标准p50被高估了11毫米汞柱。尽管对储存标本进行碱基缺陷校正(6.9 < pH < 7.1)恢复了玻尔效应,提高了标准p50计算的准确性(变异系数= 4.4%和2.9%),但饱和相关偏差仍然存在。我们得出结论,当血红蛋白-氧亲和力和酸碱平衡受到干扰时,由于血红蛋白解离曲线形状的变化,Siggaard-Andersen p50计算可能会产生误导。当代谢性酸中毒发生时,血红蛋白氧亲和力高,如危重疾病时,Siggaard-Andersen算法得出的动脉血指标可能会大大高估氧可用性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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