Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial

R. A. Harrington; F. Van de Werf; A. Luyten; B. Potkin; N. McIntosh-Yellin; C. Morgan; K. Feskiw; K. Finnie; S. McCreery; J. Diodati; E. Shalit; S. Roth; J. Smith; W. Hui; L. Kvill; M. Senaratne; M. Goeres; P. Greenwood; A. Prosser; A. Kristinsson; V. Runarsdottir; G. Oddsson; H. Plardardottir; A. B. Chandler; M. Edwards; J. Becker; S. Nallcy; R. Becker; S. Ball; E. Bates; T. Johnson; R. Harrington; K. Quintero; A. Paraschos; L. Paraschos; K. Lerrick; B. Spinogatti; N. Bhalodkar; A. Valeria; D. Moliterno; P. Desantis; J. K. White; K. Andreatta; J. Burks; N. Kohler; J. Seaworth; J. Jensen; G. Carreon; T. Nygaard; J. White; J. Puma; L. Jones; P. Armstrong; W. Sutherland; E. Topol; D. Moliterno; R. Califf; R. Harrington; K. Newby; M. Peek; C. Binanay; K. Tinnin; M. Bhapkar; M. Dorsey; J. Parker; B. Tardiff; J. Alexander; B. Crenshaw; C. Green; G. Strand; M. Krucoff; K. Trollinger; C. Green; S. Ellis; T. Ivanc; D. Debowey; W. Hillegass; M. Lincoff; J. Tcheng; A. Rames; B. Steiner; M. Bokslag; D. Marcantuono; E. Luiden; T. Nielsen

doi:10.1016/S0735-1097(98)00474-4

Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial

R. A. Harrington, F. Van de Werf, A. Luyten, B. Potkin, N. McIntosh-Yellin, C. Morgan, K. Feskiw, K. Finnie, S. McCreery, J. Diodati, E. Shalit, S. Roth, J. Smith, W. Hui, L. Kvill, M. Senaratne, M. Goeres, P. Greenwood, A. Prosser, A. KristinssonV. Runarsdottir, G. Oddsson, H. Plardardottir, A. B. Chandler, M. Edwards, J. Becker, S. Nallcy, R. Becker, S. Ball, E. Bates, T. Johnson, R. Harrington, K. Quintero, A. Paraschos, L. Paraschos, K. Lerrick, B. Spinogatti, N. Bhalodkar, A. Valeria, D. Moliterno, P. Desantis, J. K. White, K. Andreatta, J. Burks, N. Kohler, J. Seaworth, J. Jensen, G. Carreon, T. Nygaard, J. White, J. Puma, L. Jones, P. Armstrong, W. Sutherland, E. Topol, D. Moliterno, R. Califf, R. Harrington, K. Newby, M. Peek, C. Binanay, K. Tinnin, M. Bhapkar, M. Dorsey, J. Parker, B. Tardiff, J. Alexander, B. Crenshaw, C. Green, G. Strand, M. Krucoff, K. Trollinger, C. Green, S. Ellis, T. Ivanc, D. Debowey, W. Hillegass, M. Lincoff, J. Tcheng, A. Rames, B. Steiner, M. Bokslag, D. Marcantuono, E. Luiden, T. Nielsen

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135 Citas (Scopus)

Resumen

Objectives. The trial was designed to assess the safety, pharmacodynamies and effects on reperfusion of the platelet glycoprotein (GP) IIb/IIIa inhibitor lamifiban when given with thrombolysis to patients with ST segment elevation acute myocardial infarction. Background. Studies of fibrinolytic agents in acute myocardial infarction have demonstrated a direct relationship between early complete reperfusion and survival. Blockade of the platelet GP IIb/IIIa receptor complex inhibits platelet aggregation and may speed reperfusion when given in conjunction with thrombolysis to patients with acute myocardial infarction. Methods. Patients with ST segment elevation presenting within 12 h of symptom onset who were treated with either tissue- plasminogen activator or streptokinase were enrolled in this three-part Phase II dose exploration study. In Part A, all patients received the GP IIb/IIIa inhibitor lamifiban in an open-label, dose escalation scheme. Parts B and C were a randomized, double-blind Comparison of a bolus plus 24-h infusion of lamifiban versus placebo with patients randomized in a 2:1 ratio. The goal was to identify a dose(s) of lamitiban that provided >85% adenosine diphosphate (ADP)-induced platelet aggregation inhibition. A composite of angiographic, continuous electrocardiographic and clinical markers of reperfusion was the primary efficacy end point, and bleeding was the primary safety end point. Results. Platelet aggregation was inhibited by lamifiban in a dose-dependent manner with the highest doses exceeding 85% ADP-induced platelet aggregation inhibition. There was more bleeding associated with lamifiban (transfusions in 16.1% lamifiban-treated vs. 10.3% placebo-treated patients). Lamifiban induced more rapid reperfusion as measured by all continuous electrocardiographic (ECG) parameters. Conclusions. Lamifiban given with thrombolytic therapy appears to be associated with more rapid and complete reperfusion than placebo. As expected in this small sample, there were no obvious clinical benefits to lamifiban over placebo. Reconciliation of ECG monitoring with clinical outcomes will require a larger, adequately powered clinical trial.

Idioma original	English
Páginas (desde-hasta)	2003-2010
Número de páginas	8
Publicación	Journal of the American College of Cardiology
Volumen	32
N.º	7
DOI	https://doi.org/10.1016/S0735-1097(98)00474-4
Estado	Published - dic 1998

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine

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10.1016/S0735-1097(98)00474-4

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Harrington, R. A., Van de Werf, F., Luyten, A., Potkin, B., McIntosh-Yellin, N., Morgan, C., Feskiw, K., Finnie, K., McCreery, S., Diodati, J., Shalit, E., Roth, S., Smith, J., Hui, W., Kvill, L., Senaratne, M., Goeres, M., Greenwood, P., Prosser, A., ... Nielsen, T. (1998). Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial. Journal of the American College of Cardiology, 32(7), 2003-2010. https://doi.org/10.1016/S0735-1097(98)00474-4

Harrington, R. A. ; Van de Werf, F. ; Luyten, A. et al. / Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban : Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial. En: Journal of the American College of Cardiology. 1998 ; Vol. 32, N.º 7. pp. 2003-2010.

@article{9e347a966ee64b24ae900c4b19db4ab1,

title = "Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial",

abstract = "Objectives. The trial was designed to assess the safety, pharmacodynamies and effects on reperfusion of the platelet glycoprotein (GP) IIb/IIIa inhibitor lamifiban when given with thrombolysis to patients with ST segment elevation acute myocardial infarction. Background. Studies of fibrinolytic agents in acute myocardial infarction have demonstrated a direct relationship between early complete reperfusion and survival. Blockade of the platelet GP IIb/IIIa receptor complex inhibits platelet aggregation and may speed reperfusion when given in conjunction with thrombolysis to patients with acute myocardial infarction. Methods. Patients with ST segment elevation presenting within 12 h of symptom onset who were treated with either tissue- plasminogen activator or streptokinase were enrolled in this three-part Phase II dose exploration study. In Part A, all patients received the GP IIb/IIIa inhibitor lamifiban in an open-label, dose escalation scheme. Parts B and C were a randomized, double-blind Comparison of a bolus plus 24-h infusion of lamifiban versus placebo with patients randomized in a 2:1 ratio. The goal was to identify a dose(s) of lamitiban that provided >85\% adenosine diphosphate (ADP)-induced platelet aggregation inhibition. A composite of angiographic, continuous electrocardiographic and clinical markers of reperfusion was the primary efficacy end point, and bleeding was the primary safety end point. Results. Platelet aggregation was inhibited by lamifiban in a dose-dependent manner with the highest doses exceeding 85\% ADP-induced platelet aggregation inhibition. There was more bleeding associated with lamifiban (transfusions in 16.1\% lamifiban-treated vs. 10.3\% placebo-treated patients). Lamifiban induced more rapid reperfusion as measured by all continuous electrocardiographic (ECG) parameters. Conclusions. Lamifiban given with thrombolytic therapy appears to be associated with more rapid and complete reperfusion than placebo. As expected in this small sample, there were no obvious clinical benefits to lamifiban over placebo. Reconciliation of ECG monitoring with clinical outcomes will require a larger, adequately powered clinical trial.",

author = "Harrington, \{R. A.\} and \{Van de Werf\}, F. and A. Luyten and B. Potkin and N. McIntosh-Yellin and C. Morgan and K. Feskiw and K. Finnie and S. McCreery and J. Diodati and E. Shalit and S. Roth and J. Smith and W. Hui and L. Kvill and M. Senaratne and M. Goeres and P. Greenwood and A. Prosser and A. Kristinsson and V. Runarsdottir and G. Oddsson and H. Plardardottir and Chandler, \{A. B.\} and M. Edwards and J. Becker and S. Nallcy and R. Becker and S. Ball and E. Bates and T. Johnson and R. Harrington and K. Quintero and A. Paraschos and L. Paraschos and K. Lerrick and B. Spinogatti and N. Bhalodkar and A. Valeria and D. Moliterno and P. Desantis and White, \{J. K.\} and K. Andreatta and J. Burks and N. Kohler and J. Seaworth and J. Jensen and G. Carreon and T. Nygaard and J. White and J. Puma and L. Jones and P. Armstrong and W. Sutherland and E. Topol and D. Moliterno and R. Califf and R. Harrington and K. Newby and M. Peek and C. Binanay and K. Tinnin and M. Bhapkar and M. Dorsey and J. Parker and B. Tardiff and J. Alexander and B. Crenshaw and C. Green and G. Strand and M. Krucoff and K. Trollinger and C. Green and S. Ellis and T. Ivanc and D. Debowey and W. Hillegass and M. Lincoff and J. Tcheng and A. Rames and B. Steiner and M. Bokslag and D. Marcantuono and E. Luiden and T. Nielsen",

year = "1998",

month = dec,

doi = "10.1016/S0735-1097(98)00474-4",

language = "English",

volume = "32",

pages = "2003--2010",

number = "7",

}

Harrington, RA, Van de Werf, F, Luyten, A, Potkin, B, McIntosh-Yellin, N, Morgan, C, Feskiw, K, Finnie, K, McCreery, S, Diodati, J, Shalit, E, Roth, S, Smith, J, Hui, W, Kvill, L, Senaratne, M, Goeres, M, Greenwood, P, Prosser, A, Kristinsson, A, Runarsdottir, V, Oddsson, G, Plardardottir, H, Chandler, AB, Edwards, M, Becker, J, Nallcy, S, Becker, R, Ball, S, Bates, E, Johnson, T, Harrington, R, Quintero, K, Paraschos, A, Paraschos, L, Lerrick, K, Spinogatti, B, Bhalodkar, N, Valeria, A, Moliterno, D, Desantis, P, White, JK, Andreatta, K, Burks, J, Kohler, N, Seaworth, J, Jensen, J, Carreon, G, Nygaard, T, White, J, Puma, J, Jones, L, Armstrong, P, Sutherland, W, Topol, E, Moliterno, D, Califf, R, Harrington, R, Newby, K, Peek, M, Binanay, C, Tinnin, K, Bhapkar, M, Dorsey, M, Parker, J, Tardiff, B, Alexander, J, Crenshaw, B, Green, C, Strand, G, Krucoff, M, Trollinger, K, Green, C, Ellis, S, Ivanc, T, Debowey, D, Hillegass, W, Lincoff, M, Tcheng, J, Rames, A, Steiner, B, Bokslag, M, Marcantuono, D, Luiden, E & Nielsen, T 1998, 'Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial', Journal of the American College of Cardiology, vol. 32, n.º 7, pp. 2003-2010. https://doi.org/10.1016/S0735-1097(98)00474-4

Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial. / Harrington, R. A.; Van de Werf, F.; Luyten, A. et al.
En: Journal of the American College of Cardiology, Vol. 32, N.º 7, 12.1998, p. 2003-2010.

Producción científica: Article › revisión exhaustiva

TY - JOUR

T1 - Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban

T2 - Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial

AU - Harrington, R. A.

AU - Van de Werf, F.

AU - Luyten, A.

AU - Potkin, B.

AU - McIntosh-Yellin, N.

AU - Morgan, C.

AU - Feskiw, K.

AU - Finnie, K.

AU - McCreery, S.

AU - Diodati, J.

AU - Shalit, E.

AU - Roth, S.

AU - Smith, J.

AU - Hui, W.

AU - Kvill, L.

AU - Senaratne, M.

AU - Goeres, M.

AU - Greenwood, P.

AU - Prosser, A.

AU - Kristinsson, A.

AU - Runarsdottir, V.

AU - Oddsson, G.

AU - Plardardottir, H.

AU - Chandler, A. B.

AU - Edwards, M.

AU - Becker, J.

AU - Nallcy, S.

AU - Becker, R.

AU - Ball, S.

AU - Bates, E.

AU - Johnson, T.

AU - Harrington, R.

AU - Quintero, K.

AU - Paraschos, A.

AU - Paraschos, L.

AU - Lerrick, K.

AU - Spinogatti, B.

AU - Bhalodkar, N.

AU - Valeria, A.

AU - Moliterno, D.

AU - Desantis, P.

AU - White, J. K.

AU - Andreatta, K.

AU - Burks, J.

AU - Kohler, N.

AU - Seaworth, J.

AU - Jensen, J.

AU - Carreon, G.

AU - Nygaard, T.

AU - White, J.

AU - Puma, J.

AU - Jones, L.

AU - Armstrong, P.

AU - Sutherland, W.

AU - Topol, E.

AU - Moliterno, D.

AU - Califf, R.

AU - Harrington, R.

AU - Newby, K.

AU - Peek, M.

AU - Binanay, C.

AU - Tinnin, K.

AU - Bhapkar, M.

AU - Dorsey, M.

AU - Parker, J.

AU - Tardiff, B.

AU - Alexander, J.

AU - Crenshaw, B.

AU - Green, C.

AU - Strand, G.

AU - Krucoff, M.

AU - Trollinger, K.

AU - Green, C.

AU - Ellis, S.

AU - Ivanc, T.

AU - Debowey, D.

AU - Hillegass, W.

AU - Lincoff, M.

AU - Tcheng, J.

AU - Rames, A.

AU - Steiner, B.

AU - Bokslag, M.

AU - Marcantuono, D.

AU - Luiden, E.

AU - Nielsen, T.

PY - 1998/12

Y1 - 1998/12

N2 - Objectives. The trial was designed to assess the safety, pharmacodynamies and effects on reperfusion of the platelet glycoprotein (GP) IIb/IIIa inhibitor lamifiban when given with thrombolysis to patients with ST segment elevation acute myocardial infarction. Background. Studies of fibrinolytic agents in acute myocardial infarction have demonstrated a direct relationship between early complete reperfusion and survival. Blockade of the platelet GP IIb/IIIa receptor complex inhibits platelet aggregation and may speed reperfusion when given in conjunction with thrombolysis to patients with acute myocardial infarction. Methods. Patients with ST segment elevation presenting within 12 h of symptom onset who were treated with either tissue- plasminogen activator or streptokinase were enrolled in this three-part Phase II dose exploration study. In Part A, all patients received the GP IIb/IIIa inhibitor lamifiban in an open-label, dose escalation scheme. Parts B and C were a randomized, double-blind Comparison of a bolus plus 24-h infusion of lamifiban versus placebo with patients randomized in a 2:1 ratio. The goal was to identify a dose(s) of lamitiban that provided >85% adenosine diphosphate (ADP)-induced platelet aggregation inhibition. A composite of angiographic, continuous electrocardiographic and clinical markers of reperfusion was the primary efficacy end point, and bleeding was the primary safety end point. Results. Platelet aggregation was inhibited by lamifiban in a dose-dependent manner with the highest doses exceeding 85% ADP-induced platelet aggregation inhibition. There was more bleeding associated with lamifiban (transfusions in 16.1% lamifiban-treated vs. 10.3% placebo-treated patients). Lamifiban induced more rapid reperfusion as measured by all continuous electrocardiographic (ECG) parameters. Conclusions. Lamifiban given with thrombolytic therapy appears to be associated with more rapid and complete reperfusion than placebo. As expected in this small sample, there were no obvious clinical benefits to lamifiban over placebo. Reconciliation of ECG monitoring with clinical outcomes will require a larger, adequately powered clinical trial.

AB - Objectives. The trial was designed to assess the safety, pharmacodynamies and effects on reperfusion of the platelet glycoprotein (GP) IIb/IIIa inhibitor lamifiban when given with thrombolysis to patients with ST segment elevation acute myocardial infarction. Background. Studies of fibrinolytic agents in acute myocardial infarction have demonstrated a direct relationship between early complete reperfusion and survival. Blockade of the platelet GP IIb/IIIa receptor complex inhibits platelet aggregation and may speed reperfusion when given in conjunction with thrombolysis to patients with acute myocardial infarction. Methods. Patients with ST segment elevation presenting within 12 h of symptom onset who were treated with either tissue- plasminogen activator or streptokinase were enrolled in this three-part Phase II dose exploration study. In Part A, all patients received the GP IIb/IIIa inhibitor lamifiban in an open-label, dose escalation scheme. Parts B and C were a randomized, double-blind Comparison of a bolus plus 24-h infusion of lamifiban versus placebo with patients randomized in a 2:1 ratio. The goal was to identify a dose(s) of lamitiban that provided >85% adenosine diphosphate (ADP)-induced platelet aggregation inhibition. A composite of angiographic, continuous electrocardiographic and clinical markers of reperfusion was the primary efficacy end point, and bleeding was the primary safety end point. Results. Platelet aggregation was inhibited by lamifiban in a dose-dependent manner with the highest doses exceeding 85% ADP-induced platelet aggregation inhibition. There was more bleeding associated with lamifiban (transfusions in 16.1% lamifiban-treated vs. 10.3% placebo-treated patients). Lamifiban induced more rapid reperfusion as measured by all continuous electrocardiographic (ECG) parameters. Conclusions. Lamifiban given with thrombolytic therapy appears to be associated with more rapid and complete reperfusion than placebo. As expected in this small sample, there were no obvious clinical benefits to lamifiban over placebo. Reconciliation of ECG monitoring with clinical outcomes will require a larger, adequately powered clinical trial.

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JO - Journal of the American College of Cardiology

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Harrington RA, Van de Werf F, Luyten A, Potkin B, McIntosh-Yellin N, Morgan C et al. Combining thrombolysis with the platelet glycoprotein IIb/IIIa inhibitor lamifiban: Results of the platelet aggregation receptor antagonist dose investigation and reperfusion gain in myocardial infarction (PARADIGM) trial. Journal of the American College of Cardiology. 1998 dic;32(7):2003-2010. doi: 10.1016/S0735-1097(98)00474-4