Haemodynamic changes induced by the correction of anaemia by erythropoietin: role of antiplatelet therapy

BACKGROUND.: In a restrospective study, antiplatelet therapy has been shownto be associated with a decreased incidence of erythropoietin-inducedhypertension. In order to ascertain the role of antiplateletdrugs in the haemodynamic response to the correction of anaemiaby rHuEpo, 18 patients on chronic haemodialysis who startedrHuEpo therapy were prospectively studied. METHODS.: The subjects were randomly assigned to receive or not, one ofthe following antiplatelet drugs: ditazole (3 patients), ticlopidine(3 patients) or aspirin plus dipyridamole (3 patients). Cardiacindex (CI) by echo-Doppler, total peripheral resistance (TPR)and mean arterial pressure (MAP) were determined at baseline10 and 20 weeks following the initiation of rHuEpo therapy.rHuEpo therapy was administered subcutaneously at the same dose(40 U/kg thrice weekly) during the first 10 weeks. Ten uraemicpatients on haemodialysis who had never received rHuEpo therapyserved as the control group. RESULTS.: One patient in the group without antiplatelet drugs discontinuedthe study due to the development of severe hypertension after12 weeks on rHuEpo therapy. There were no significant differencesin the haemodynamic parameters at baseline. At 10 weeks, MAPwas higher in patients without than with antiplatelet drugsor controls untreated with rHuEpo (128.5 ± 28 versus100.6 ± 13.5 versus 98.7 ± 14 mmHg respectively,P = 0.0047), TPR was also higher in patients without antiplateletdrugs than in the 2 other groups (1919 ± 433 versus 1576± 359 versus 1418 ± 324 din.seg.cm^–5 m²respectively, P = 0.0231), but CI did not differ among the threegroups. At 20 weeks, MAP was still higher in patients withoutantiplatelet drugs than in patients with antiplatelet drugsor controls not on rHuEpo therapy respectively (112.9 ±24.6 versus 91.0 ± 9.0 versus 101.7 ± 14.1 mmHgrespectively, P = 0.075), but at this stage TPR and Cl did notdiffer among the three groups. CONCLUSIONS.: These data reinforce the previous observation that antiplatelettherapy may prevent the development of rHuEpo-induced hypertension.