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Protamine Reversal of Heparin After Cardiopulmonary Bypass Increases Lung Resistance, Not Elastance

Department of Anesthesiology, The University of Maryland Medical System

George M. Barnas

Department of Anesthesiology, The University of Maryland Medical System, Department of Physiology, University of Maryland Medical System

David W. Miller

Department of Surgery, The University of Maryland Medical System, Baltimore, Maryland

Alejandro J. Sequeira

Department of Surgery, The University of Maryland Medical System, Baltimore, Maryland

Background: Protamine, an immunologically active, cationic amine, has been suspected of impairing lung mechanics when administered after cardiopulmonary bypass (CPB) to reverse heparin. Whether such adverse changes are an effect of protamine itself, the forma tion of heparin-protamine complexes, the extent of heparin anticoagulation, or its chemical reversal is not known.

Methods and Results: Using a computer-controlled, forced-ventilation method over a vari ety of physiological tidal volume (VT) and frequency (f) combinations, we prospectively studied 18 adult, elective patients before systemic heparinization and after protamine rever sal to confirm and, possibly, elucidate an etiology for any adverse pulmonary effects. Prot amine and heparin doses, their sum (-dose) and differential (-dose) doses, and activated clotting times were tabulated. In all patients, lung resistance (R_L) and, to a lesser extent, elastance (E_L) increased after CPB, compared with pre-CPB values (P < .05). However, R_L particularly increased after CPB with increases correlated to the -dose, where R_{L PRE-POST} = -0.037 [-dose] - 0.56f - 0.019VT + 36.1 (r = .652, P < .05). No other significant correla tions were found among the remaining clinical parameters and changes in either R_L or E _L, or any chest wall component (all P > .05).

Conclusions: The changes seen in R_L after CPB were greatest in those patients receiving the most nearly balanced doses of heparin and protamine, and were not related significantly to the total heparin or protamine doses, or their sum. This suggests that the extent of antico agulation reversal or formation of heparin-protamine complexes, and not protamine itself, are more responsible for changes seen in lung mechanics. The changes seen were limited solely to R_L, and not in either EL nor the chest wall mechanical properties.

Key Words: anticoagulation • cardiopulmonary bypass • lung mechanics • protamine • pulmo nary edema.

Journal of Cardiovascular Pharmacology and Therapeutics, Vol. 4, No. 3, 137-141 (1999)
DOI: 10.1177/107424849900400302


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