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J Thorac Cardiovasc Surg 1997;113:611-613
© 1997 Mosby, Inc.

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WHOLE BLOOD HEPARIN CONCENTRATION MEASUREMENTS BY AUTOMATED PROTAMINE TITRATION AGREE WITH PLASMA ANTI-XA MEASUREMENTS

St. Louis, Mo.

J Thorac Cardiovasc Surg 1997;113:611-3Received for publication Sept.23, 1996 accepted for publication Oct. 22, 1996. Findings recently reported by our group indicated that point-of-care monitoring of heparin concentration by an automated protamine sulfate titration (PST) method (Hepcon HMS, Medtronic Hemotec, Inc., Englewood, Colo.) can reduce excessive microvascular bleeding and blood component transfusion. ¹ That study was preceded by another evaluation in which we found a high degree of correlation between heparin concentration determined by plasma anti-Xa and whole blood automated PST. ² Hardy and colleagues ³ recently published a comparison of heparin measurements by Hepcon automated PST and a laboratory-based anti-Xa chromogenic assay in a relatively small number of patients undergoing cardiac operation with the use of cardiopulmonary bypass (CPB). In contrast to our observations of a strong linear relationship between whole blood PST and plasma anti-Xa measurements, ² these investigators found unacceptably high variability between the two heparin concentration measurements. In explaining this discrepancy, Hardy and colleagues ³ suggested that our data analysis was limited and potentially misleading because we did not use bias analysis. We therefore reanalyzed our data with a bias analysis method as used by that group.

Plasma anti-Xa and whole blood PST measurements (duplicate) on blood specimens obtained at sequential operative times (4 to 6 per patient) from 62 patients undergoing cardiac operations were reanalyzed. ² Whole blood (WB) PST heparin values were converted to plasma equivalent values (PE) using concurrently measured hematocrit (Hct) values with the following formula: PE WB PST = (WB PST x 100/[100 – Hct]). The mean difference or bias between plasma anti-Xa and corrected whole blood PST measurements was 0.002 ± 0.53 U/ml. Fig. 1 shows the results of the bias analysis with means and two standard deviation confidence intervals for the 310 measurement pairs. The mean difference obtained using duplicate measurements was similar to those obtained with each of the two individual measurements (measurement 1: 0.008 ± 0.56; measurement 2: –0.004 ± 0.56).

View larger version (25K): [in this window] [in a new window]   Fig. 1. Bias analysis of plasma anti-Xa versus plasma-equivalent whole blood heparin concentration measurements. Heparin concentration in plasma was measured with use of an anti-Xa chromogenic assay and whole blood heparin concentration values were measured with an automated PST method with use of the Hepcon instrument. Whole blood heparin concentration values were converted to plasma equivalent values (PE) with the following formula: PE PST = (PST x 100/[100 – hematocrit]). The differences between anti-Xa and whole blood heparin concentration measurements are plotted on the y axis and the averages of the two heparin concentration values are plotted on the x axis. The mean (bias) and plus or minus two standard deviations of the differences are represented by the horizontal lines. n = 310.

Maintenance of adequate, patient-specific heparin concentrations with the use of the Hepcon instrument has been shown to reduce excessive hemostatic system activation and preserve coagulation factors during CPB, ⁶ which may in part account for the significant reduction in blood component transfusion requirements seen with this approach. ¹ In an attempt to explain the benefits found in our previous studies, Hardy and colleagues ³ suggested that administration of higher heparin and lower protamine doses may have accounted for the improved outcomes. Although these findings may be the result of administration of greater overall heparin doses, the relative importance of administering heparin on the basis of patient-specific requirements cannot be overlooked. In our previous evaluation, ¹ the total heparin dose was directly related to the concentration of heparin maintained during CPB that was designated for each patient on the basis of the patient's anticoagulant response to heparin before CPB by use of a standard assay (activated clotting time). Finally, we have recently evaluated the use of continuous infusions of heparin during CPB to maintain stable, adequate heparin concentrations. Unpublished data from this study confirm the reliability and usefulness of on-site, whole blood heparin concentration measurements by the Hepcon HMS system.

Footnotes

From the Department of Anasthesiology, Internal Medicine, Pathology, and Surgery, Washington University School of Medicine, St. Louis, Mo. and the Departments of Internal Medicine and Pathology, St. Louis University School of Medicine, St. Louis, Mo.

References

1. Despotis GJ, Joist JH, Hogue CW, et al. The impact of heparin concentration and activated clotting time monitoring on blood conservation: a prospective, randomized evaluation in patients undergoing cardiac operations. J Thorac Cardiovasc Surg 1995;110:46-54.[Abstract/Free Full Text]
   
2. Despotis GJ, Summerfield AL, Joist JH, et al. Comparison of activated coagulation time and whole blood heparin measurements with laboratory plasma anti-Xa heparin concentration in patients having cardiac operations. J Thorac Cardiovasc Surg 1994;108:1076-82.[Abstract/Free Full Text]
   
3. Hardy JF, Belisle S, Robitaille D, Perrault J, Roy M, Gragnon L. Measurement of heparin concentration in whole blood with the Hepcon/HMS device does not agree with laboratory determination of plasma heparin concentration using a chromogenic substrate for activated factor X. J Thorac Cardiovasc Surg 1996;112:154-61.[Abstract/Free Full Text]
   
4. Barrowcliffe TW, Curtis AD, Tomlinson TP, Hubbard AR, Johnson EA, Thomas DP. Standardization of low molecular weight heparins: a collaborative study. Thromb Haemost 1985;54:675-9.[Medline]
   
5. Hirsh J. Heparin [Review]. N Engl J Med 1991;324:1565-74.[Medline]
   
6. Despotis GJ, Joist JH, Hogue CW, et al. The effect of higher heparin concentrations on preservation of hemostasis in cardiac surgical patients. Thromb Haemost 1996;76:902-8.[Medline]
   

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