Low-molecular-weight heparin in the treatment of patients with venous thromboembolism

J. W. tenCate; H. R. Buller; M. Gent; J. Hirsh; M. H. Prins; R. Baildon; A. W. A. Lensing; D. R. Anderson; E. J. R. vanBeek; J. N. Fiesinger; J. G. P. Tijssen; A. vanBarneveld; L. T. Eimers; Y. P. Graafsma; R. Hettiarachchi; B. Hutten; K. Redekop; S. Haley; L. LIberale; T. Finch; S. Whittaker; L. Wilkinson; P. Prandoni; S. Villalta; B. Girolami; P. Bagatella; L. Rossi; A. Girolami; F. Piovella; M. Barone; C. Beltrametti; S. Serafini; S. Siragusa; E. Ascari; M. J. Kovacs; B. Morrow; J. Kovacs; P. M. M. Kuijer; M. M. W. Koopman; H. Jagt; J. Weitz; C. Kearon; L. Biagioni; S. Haas; F. Lossner; F. A. Spengel; M. Berger; C. Demers; J. Poulin; J. vanderMeer; G. T. H. Que; W. M. Smid; K. S. Robinson; E. Boyle; J. R. Leclerc; B. StJacques; S. Finkenbine; A. S. Gallus; D. Cohlan; C. Rich; D. P. M. Brandjes; C. A. Hoefnagel; M. deRijk; F. Turkstra; L. Desjardins; J. CoteDesjardins; L. Couture; M. Ruel; J. Villenueve; W. H. Geerts; R. M. Jay; E. K. I. Code; A. G. G. Turpie; J. Johnson; P. Nguyen; J. R. Cusson; S. Roy; P. S. Wells; J. Bormanis; D. Goudie; M. Cruickshank; M. vonLewinski; M. Monreal; J. C. Sahuquillo; E. Lafoz; G. Simonneau; F. Parent; J. Jagot; J. D. Douketis; K. Kinnon; J. S. Ginsberg; P. BrillEdwards; D. Donovan; P. A. Ockelford; J. Kassis; S. Bornais; B. Planchon; D. Elkouri; M. A. Pistorius; M. Escribano; G. Garrido; C. N. Chesterman; B. H. Chong; S. Pritchard; J. F. Cade; T. Bynon; J. Stanford; W. M. Brien; B. Palmer; R. Faivre; B. Petiteau; P. M. Manucci; M. Moia; P. Bucciarelli; J.W. ten Cate

doi:https://doi.org/10.1056/NEJM199709043371001

Low-molecular-weight heparin in the treatment of patients with venous thromboembolism

J. W. tenCate, H. R. Buller, M. Gent, J. Hirsh, M. H. Prins, R. Baildon, A. W. A. Lensing, D. R. Anderson, E. J. R. vanBeek, J. N. Fiesinger, J. G. P. Tijssen, A. vanBarneveld, L. T. Eimers, Y. P. Graafsma, R. Hettiarachchi, B. Hutten, K. Redekop, S. Haley, L. LIberale, T. FinchS. Whittaker, L. Wilkinson, P. Prandoni, S. Villalta, B. Girolami, P. Bagatella, L. Rossi, A. Girolami, F. Piovella, M. Barone, C. Beltrametti, S. Serafini, S. Siragusa, E. Ascari, M. J. Kovacs, B. Morrow, J. Kovacs, P. M. M. Kuijer, M. M. W. Koopman, H. Jagt, J. Weitz, C. Kearon, L. Biagioni, S. Haas, F. Lossner, F. A. Spengel, M. Berger, C. Demers, J. Poulin, J. vanderMeer, G. T. H. Que, W. M. Smid, K. S. Robinson, E. Boyle, J. R. Leclerc, B. StJacques, S. Finkenbine, A. S. Gallus, D. Cohlan, C. Rich, D. P. M. Brandjes, C. A. Hoefnagel, M. deRijk, F. Turkstra, L. Desjardins, J. CoteDesjardins, L. Couture, M. Ruel, J. Villenueve, W. H. Geerts, R. M. Jay, E. K. I. Code, A. G. G. Turpie, J. Johnson, P. Nguyen, J. R. Cusson, S. Roy, P. S. Wells, J. Bormanis, D. Goudie, M. Cruickshank, M. vonLewinski, M. Monreal, J. C. Sahuquillo, E. Lafoz, G. Simonneau, F. Parent, J. Jagot, J. D. Douketis, K. Kinnon, J. S. Ginsberg, P. BrillEdwards, D. Donovan, P. A. Ockelford, J. Kassis, S. Bornais, B. Planchon, D. Elkouri, M. A. Pistorius, M. Escribano, G. Garrido, C. N. Chesterman, B. H. Chong, S. Pritchard, J. F. Cade, T. Bynon, J. Stanford, W. M. Brien, B. Palmer, R. Faivre, B. Petiteau, P. M. Manucci, M. Moia, P. Bucciarelli, J.W. ten Cate

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Abstract

Background Low-molecular-weight heparin is known to be safe and effective for the initial Treatment of patients with proximal deep-vein thrombosis. However, its application to patients with pulmonary embolism or previous episodes of thromboembolism has not been studied. Methods We randomly assigned 1021 patients with symptomatic venous thromboembolism to fixed-dose, subcutaneous low-molecular-weight heparin (reviparin sodium) or adjusted-dose, intravenous unfractionated heparin. Oral anticoagulant therapy with a coumarin derivative was started concomitantly and continued for 12 weeks, Approximately one third of the patients had associated pulmonary embolism, The outcome events studied over the 12 weeks were symptomatic recurrent venous thromboembolism, major bleeding, and death. We sought to determine whether low-molecular-weight heparin is at least equivalent to unfractionated heparin in patients with venous thromboembolism. Results Twenty-seven of the 510 patients assigned to low-molecular-weight heparin (5.3 percent) had recurrent thromboembolic events, as compared with 25 of the 511 patients assigned to unfractionated heparin (4.9 percent). The difference of 0.4 percentage point indicates that the two therapies have equivalent value according to our predetermined definition of equivalence. Sixteen patients assigned to low-molecular-weight heparin (3.1 percent) and 12 patients assigned to unfractionated heparin (2.3 percent) had episodes of major bleeding (P=0.63), and the mortality rates in the two groups were 7.1 percent and 7.6 percent, respectively (P=0.89). Conclusions Fixed-dose, subcutaneous low-molecular-weight heparin is as effective and safe as adjusted-dose, intravenous unfractionated heparin for the initial management of venous thromboembolism, regardless of whether the patient has pulmonary embolism or a history of venous thromboembolism. (C) 1997, Massachusetts Medical Society

Original language	English
Pages (from-to)	657-662
Journal	New England journal of medicine
Volume	337
Issue number	10
DOIs	https://doi.org/10.1056/NEJM199709043371001
Publication status	Published - 1997

Keywords

AMC wi-co

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tenCate, J. W., Buller, H. R., Gent, M., Hirsh, J., Prins, M. H., Baildon, R., Lensing, A. W. A., Anderson, D. R., vanBeek, E. J. R., Fiesinger, J. N., Tijssen, J. G. P., vanBarneveld, A., Eimers, L. T., Graafsma, Y. P., Hettiarachchi, R., Hutten, B., Redekop, K., Haley, S., LIberale, L., ... ten Cate, J. W. (1997). Low-molecular-weight heparin in the treatment of patients with venous thromboembolism. New England journal of medicine, 337(10), 657-662. https://doi.org/10.1056/NEJM199709043371001

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title = "Low-molecular-weight heparin in the treatment of patients with venous thromboembolism",

abstract = "Background Low-molecular-weight heparin is known to be safe and effective for the initial Treatment of patients with proximal deep-vein thrombosis. However, its application to patients with pulmonary embolism or previous episodes of thromboembolism has not been studied. Methods We randomly assigned 1021 patients with symptomatic venous thromboembolism to fixed-dose, subcutaneous low-molecular-weight heparin (reviparin sodium) or adjusted-dose, intravenous unfractionated heparin. Oral anticoagulant therapy with a coumarin derivative was started concomitantly and continued for 12 weeks, Approximately one third of the patients had associated pulmonary embolism, The outcome events studied over the 12 weeks were symptomatic recurrent venous thromboembolism, major bleeding, and death. We sought to determine whether low-molecular-weight heparin is at least equivalent to unfractionated heparin in patients with venous thromboembolism. Results Twenty-seven of the 510 patients assigned to low-molecular-weight heparin (5.3 percent) had recurrent thromboembolic events, as compared with 25 of the 511 patients assigned to unfractionated heparin (4.9 percent). The difference of 0.4 percentage point indicates that the two therapies have equivalent value according to our predetermined definition of equivalence. Sixteen patients assigned to low-molecular-weight heparin (3.1 percent) and 12 patients assigned to unfractionated heparin (2.3 percent) had episodes of major bleeding (P=0.63), and the mortality rates in the two groups were 7.1 percent and 7.6 percent, respectively (P=0.89). Conclusions Fixed-dose, subcutaneous low-molecular-weight heparin is as effective and safe as adjusted-dose, intravenous unfractionated heparin for the initial management of venous thromboembolism, regardless of whether the patient has pulmonary embolism or a history of venous thromboembolism. (C) 1997, Massachusetts Medical Society",

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author = "tenCate, {J. W.} and Buller, {H. R.} and M. Gent and J. Hirsh and Prins, {M. H.} and R. Baildon and Lensing, {A. W. A.} and Anderson, {D. R.} and vanBeek, {E. J. R.} and Fiesinger, {J. N.} and Tijssen, {J. G. P.} and A. vanBarneveld and Eimers, {L. T.} and Graafsma, {Y. P.} and R. Hettiarachchi and B. Hutten and K. Redekop and S. Haley and L. LIberale and T. Finch and S. Whittaker and L. Wilkinson and P. Prandoni and S. Villalta and B. Girolami and P. Bagatella and L. Rossi and A. Girolami and F. Piovella and M. Barone and C. Beltrametti and S. Serafini and S. Siragusa and E. Ascari and Kovacs, {M. J.} and B. Morrow and J. Kovacs and Kuijer, {P. M. M.} and Koopman, {M. M. W.} and H. Jagt and J. Weitz and C. Kearon and L. Biagioni and S. Haas and F. Lossner and Spengel, {F. A.} and M. Berger and C. Demers and J. Poulin and J. vanderMeer and Que, {G. T. H.} and Smid, {W. M.} and Robinson, {K. S.} and E. Boyle and Leclerc, {J. R.} and B. StJacques and S. Finkenbine and Gallus, {A. S.} and D. Cohlan and C. Rich and Brandjes, {D. P. M.} and Hoefnagel, {C. A.} and M. deRijk and F. Turkstra and L. Desjardins and J. CoteDesjardins and L. Couture and M. Ruel and J. Villenueve and Geerts, {W. H.} and Jay, {R. M.} and Code, {E. K. I.} and Turpie, {A. G. G.} and J. Johnson and P. Nguyen and Cusson, {J. R.} and S. Roy and Wells, {P. S.} and J. Bormanis and D. Goudie and M. Cruickshank and M. vonLewinski and M. Monreal and Sahuquillo, {J. C.} and E. Lafoz and G. Simonneau and F. Parent and J. Jagot and Douketis, {J. D.} and K. Kinnon and Ginsberg, {J. S.} and P. BrillEdwards and D. Donovan and Ockelford, {P. A.} and J. Kassis and S. Bornais and B. Planchon and D. Elkouri and Pistorius, {M. A.} and M. Escribano and G. Garrido and Chesterman, {C. N.} and Chong, {B. H.} and S. Pritchard and Cade, {J. F.} and T. Bynon and J. Stanford and Brien, {W. M.} and B. Palmer and R. Faivre and B. Petiteau and Manucci, {P. M.} and M. Moia and P. Bucciarelli and {ten Cate}, J.W.",

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tenCate, JW, Buller, HR, Gent, M, Hirsh, J, Prins, MH, Baildon, R, Lensing, AWA, Anderson, DR, vanBeek, EJR, Fiesinger, JN, Tijssen, JGP, vanBarneveld, A, Eimers, LT, Graafsma, YP, Hettiarachchi, R, Hutten, B, Redekop, K, Haley, S, LIberale, L, Finch, T, Whittaker, S, Wilkinson, L, Prandoni, P, Villalta, S, Girolami, B, Bagatella, P, Rossi, L, Girolami, A, Piovella, F, Barone, M, Beltrametti, C, Serafini, S, Siragusa, S, Ascari, E, Kovacs, MJ, Morrow, B, Kovacs, J, Kuijer, PMM, Koopman, MMW, Jagt, H, Weitz, J, Kearon, C, Biagioni, L, Haas, S, Lossner, F, Spengel, FA, Berger, M, Demers, C, Poulin, J, vanderMeer, J, Que, GTH, Smid, WM, Robinson, KS, Boyle, E, Leclerc, JR, StJacques, B, Finkenbine, S, Gallus, AS, Cohlan, D, Rich, C, Brandjes, DPM, Hoefnagel, CA, deRijk, M, Turkstra, F, Desjardins, L, CoteDesjardins, J, Couture, L, Ruel, M, Villenueve, J, Geerts, WH, Jay, RM, Code, EKI, Turpie, AGG, Johnson, J, Nguyen, P, Cusson, JR, Roy, S, Wells, PS, Bormanis, J, Goudie, D, Cruickshank, M, vonLewinski, M, Monreal, M, Sahuquillo, JC, Lafoz, E, Simonneau, G, Parent, F, Jagot, J, Douketis, JD, Kinnon, K, Ginsberg, JS, BrillEdwards, P, Donovan, D, Ockelford, PA, Kassis, J, Bornais, S, Planchon, B, Elkouri, D, Pistorius, MA, Escribano, M, Garrido, G, Chesterman, CN, Chong, BH, Pritchard, S, Cade, JF, Bynon, T, Stanford, J, Brien, WM, Palmer, B, Faivre, R, Petiteau, B, Manucci, PM, Moia, M, Bucciarelli, P & ten Cate, JW 1997, 'Low-molecular-weight heparin in the treatment of patients with venous thromboembolism', New England journal of medicine, vol. 337, no. 10, pp. 657-662. https://doi.org/10.1056/NEJM199709043371001

TY - JOUR

T1 - Low-molecular-weight heparin in the treatment of patients with venous thromboembolism

AU - tenCate, J. W.

AU - Buller, H. R.

AU - Gent, M.

AU - Hirsh, J.

AU - Prins, M. H.

AU - Baildon, R.

AU - Lensing, A. W. A.

AU - Anderson, D. R.

AU - vanBeek, E. J. R.

AU - Fiesinger, J. N.

AU - Tijssen, J. G. P.

AU - vanBarneveld, A.

AU - Eimers, L. T.

AU - Graafsma, Y. P.

AU - Hettiarachchi, R.

AU - Hutten, B.

AU - Redekop, K.

AU - Haley, S.

AU - LIberale, L.

AU - Finch, T.

AU - Whittaker, S.

AU - Wilkinson, L.

AU - Prandoni, P.

AU - Villalta, S.

AU - Girolami, B.

AU - Bagatella, P.

AU - Rossi, L.

AU - Girolami, A.

AU - Piovella, F.

AU - Barone, M.

AU - Beltrametti, C.

AU - Serafini, S.

AU - Siragusa, S.

AU - Ascari, E.

AU - Kovacs, M. J.

AU - Morrow, B.

AU - Kovacs, J.

AU - Kuijer, P. M. M.

AU - Koopman, M. M. W.

AU - Jagt, H.

AU - Weitz, J.

AU - Kearon, C.

AU - Biagioni, L.

AU - Haas, S.

AU - Lossner, F.

AU - Spengel, F. A.

AU - Berger, M.

AU - Demers, C.

AU - Poulin, J.

AU - vanderMeer, J.

AU - Que, G. T. H.

AU - Smid, W. M.

AU - Robinson, K. S.

AU - Boyle, E.

AU - Leclerc, J. R.

AU - StJacques, B.

AU - Finkenbine, S.

AU - Gallus, A. S.

AU - Cohlan, D.

AU - Rich, C.

AU - Brandjes, D. P. M.

AU - Hoefnagel, C. A.

AU - deRijk, M.

AU - Turkstra, F.

AU - Desjardins, L.

AU - CoteDesjardins, J.

AU - Couture, L.

AU - Ruel, M.

AU - Villenueve, J.

AU - Geerts, W. H.

AU - Jay, R. M.

AU - Code, E. K. I.

AU - Turpie, A. G. G.

AU - Johnson, J.

AU - Nguyen, P.

AU - Cusson, J. R.

AU - Roy, S.

AU - Wells, P. S.

AU - Bormanis, J.

AU - Goudie, D.

AU - Cruickshank, M.

AU - vonLewinski, M.

AU - Monreal, M.

AU - Sahuquillo, J. C.

AU - Lafoz, E.

AU - Simonneau, G.

AU - Parent, F.

AU - Jagot, J.

AU - Douketis, J. D.

AU - Kinnon, K.

AU - Ginsberg, J. S.

AU - BrillEdwards, P.

AU - Donovan, D.

AU - Ockelford, P. A.

AU - Kassis, J.

AU - Bornais, S.

AU - Planchon, B.

AU - Elkouri, D.

AU - Pistorius, M. A.

AU - Escribano, M.

AU - Garrido, G.

AU - Chesterman, C. N.

AU - Chong, B. H.

AU - Pritchard, S.

AU - Cade, J. F.

AU - Bynon, T.

AU - Stanford, J.

AU - Brien, W. M.

AU - Palmer, B.

AU - Faivre, R.

AU - Petiteau, B.

AU - Manucci, P. M.

AU - Moia, M.

AU - Bucciarelli, P.

AU - ten Cate, J.W.

N1 - cri/13/odp IV

PY - 1997

Y1 - 1997

N2 - Background Low-molecular-weight heparin is known to be safe and effective for the initial Treatment of patients with proximal deep-vein thrombosis. However, its application to patients with pulmonary embolism or previous episodes of thromboembolism has not been studied. Methods We randomly assigned 1021 patients with symptomatic venous thromboembolism to fixed-dose, subcutaneous low-molecular-weight heparin (reviparin sodium) or adjusted-dose, intravenous unfractionated heparin. Oral anticoagulant therapy with a coumarin derivative was started concomitantly and continued for 12 weeks, Approximately one third of the patients had associated pulmonary embolism, The outcome events studied over the 12 weeks were symptomatic recurrent venous thromboembolism, major bleeding, and death. We sought to determine whether low-molecular-weight heparin is at least equivalent to unfractionated heparin in patients with venous thromboembolism. Results Twenty-seven of the 510 patients assigned to low-molecular-weight heparin (5.3 percent) had recurrent thromboembolic events, as compared with 25 of the 511 patients assigned to unfractionated heparin (4.9 percent). The difference of 0.4 percentage point indicates that the two therapies have equivalent value according to our predetermined definition of equivalence. Sixteen patients assigned to low-molecular-weight heparin (3.1 percent) and 12 patients assigned to unfractionated heparin (2.3 percent) had episodes of major bleeding (P=0.63), and the mortality rates in the two groups were 7.1 percent and 7.6 percent, respectively (P=0.89). Conclusions Fixed-dose, subcutaneous low-molecular-weight heparin is as effective and safe as adjusted-dose, intravenous unfractionated heparin for the initial management of venous thromboembolism, regardless of whether the patient has pulmonary embolism or a history of venous thromboembolism. (C) 1997, Massachusetts Medical Society

AB - Background Low-molecular-weight heparin is known to be safe and effective for the initial Treatment of patients with proximal deep-vein thrombosis. However, its application to patients with pulmonary embolism or previous episodes of thromboembolism has not been studied. Methods We randomly assigned 1021 patients with symptomatic venous thromboembolism to fixed-dose, subcutaneous low-molecular-weight heparin (reviparin sodium) or adjusted-dose, intravenous unfractionated heparin. Oral anticoagulant therapy with a coumarin derivative was started concomitantly and continued for 12 weeks, Approximately one third of the patients had associated pulmonary embolism, The outcome events studied over the 12 weeks were symptomatic recurrent venous thromboembolism, major bleeding, and death. We sought to determine whether low-molecular-weight heparin is at least equivalent to unfractionated heparin in patients with venous thromboembolism. Results Twenty-seven of the 510 patients assigned to low-molecular-weight heparin (5.3 percent) had recurrent thromboembolic events, as compared with 25 of the 511 patients assigned to unfractionated heparin (4.9 percent). The difference of 0.4 percentage point indicates that the two therapies have equivalent value according to our predetermined definition of equivalence. Sixteen patients assigned to low-molecular-weight heparin (3.1 percent) and 12 patients assigned to unfractionated heparin (2.3 percent) had episodes of major bleeding (P=0.63), and the mortality rates in the two groups were 7.1 percent and 7.6 percent, respectively (P=0.89). Conclusions Fixed-dose, subcutaneous low-molecular-weight heparin is as effective and safe as adjusted-dose, intravenous unfractionated heparin for the initial management of venous thromboembolism, regardless of whether the patient has pulmonary embolism or a history of venous thromboembolism. (C) 1997, Massachusetts Medical Society

KW - AMC wi-co

U2 - https://doi.org/10.1056/NEJM199709043371001

DO - https://doi.org/10.1056/NEJM199709043371001

M3 - Article

C2 - 9280815

SN - 0028-4793

VL - 337

SP - 657

EP - 662

JO - New England journal of medicine

JF - New England journal of medicine

IS - 10

ER -