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与校准计划相关的序贯患者GEM血气测量的临床效用受损。

Impaired clinical utility of sequential patient GEM blood gas measurements associated with calibration schedule.

作者信息

Cembrowski George S, Xu Qian, Cembrowski Adam R, Mei Junyi, Sadrzadeh Hossein

机构信息

Department of Laboratory Medicine and Pathology, University of Alberta Hospital, 4B1.24 Walter C. Mackenzie Centre, 8440 - 112 Street, Edmonton, Alberta T6G 2B7, Canada; University of Alberta, 4B1.24 Walter C. Mackenzie Centre, 8440 - 112 Street, Edmonton, Alberta T6G 2B7, Canada; Alberta Health Services, 4B1.24 Walter C. Mackenzie Centre, 8440 - 112 Street, Edmonton, Alberta T6G 2B7, Canada.

University of Manitoba, 66 Chancellors Cir, Winnipeg, MB R3T 2N2, Canada.

出版信息

Clin Biochem. 2017 Nov;50(16-17):936-941. doi: 10.1016/j.clinbiochem.2017.03.014. Epub 2017 Mar 18.

Abstract

BACKGROUND

Within- and/or between-instrument variation may falsely indicate patient trends or obscure real trends. We employ a methodology that transforms sequential intra-patient results into estimates of biologic and analytic variation. We previously derived realistic biologic variation (s) of blood gas (BG) and hematology analytes. We extend this methodology to derive the imprecision of two GEM 4000 BG analyzers.

METHODS

A laboratory data repository provided arterial BG, electrolyte and metabolite results generated by two GEM 4000s on ICU patients in 2012-2013. We tabulated consecutive pairs of intra-patient results separated by increasing time interval between consecutive tests. The average between pair variations were regressed against time with the y-intercept representing the sum of the biologic variation and short term analytic variation: y=s+s. Using an equivalent equation for the Radiometer ABL, the imprecision of the two GEMs was calculated: s=(y-y+s). This analysis was performed for nearly all measurements, regardless of time as well for values obtained over two 12h mutually exclusive periods, starting either at 2am or 2pm.

RESULTS

Regression graphs were derived from 1800 patients' blood gas results with least 10,000 data pairs grouped into 2h intervals. The calculated s exceed the directly measured s with many GEM sigma ratios of biologic variation/analytic variation being close to unity. All of the afternoon s exceeded their morning counterparts with pH, pCO, K and bicarbonate being statistically significant.

CONCLUSION

For many analytes, the average analytical variation of tandem GEMs approximates the biologic variation, indicating impaired clinical usefulness of tandem sequential measurements. A significant component of this variation is due to increased variation of the GEMs between 2pm and 2am.

摘要

背景

仪器内部和/或仪器之间的差异可能会错误地显示患者的病情趋势,或掩盖真实趋势。我们采用一种方法,将患者体内的连续检测结果转化为生物学和分析变异的估计值。我们之前已经得出了血气(BG)和血液学分析物的实际生物学变异(s)。我们扩展了这种方法,以得出两台GEM 4000血气分析仪的不精密度。

方法

一个实验室数据存储库提供了2012 - 2013年两台GEM 4000对重症监护病房患者进行动脉血气、电解质和代谢物检测的结果。我们将患者体内连续检测结果按连续检测之间时间间隔的增加进行列表。将每对结果之间的平均差异与时间进行回归分析,y轴截距代表生物学变异和短期分析变异之和:y = s + s。使用与雷度ABL等效的方程,计算两台GEM的不精密度:s =(y - y + s)。对几乎所有测量值进行了此分析,无论时间如何,对于在两个相互排斥的12小时时间段内获得的值,分别从凌晨2点或下午2点开始。

结果

从1800名患者的血气结果中得出回归图,至少有10000个数据对按2小时间隔分组。计算出的s超过直接测量的s,许多GEM生物学变异/分析变异的西格玛比值接近1。所有下午的s均超过上午的对应值,pH、pCO₂、K和碳酸氢盐具有统计学意义。

结论

对于许多分析物,串联GEM的平均分析变异接近生物学变异,表明串联连续测量的临床实用性受损。这种变异的一个重要组成部分是由于GEM在下午2点至凌晨2点之间的变异增加。

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