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Zoledronic acid and risedronate in the prevention and treatment of glucocorticoid-induced osteoporosis (HORIZON) : a multicentre, double-blind, double-dummy, randomised controlled trial

Identifieur interne : 002E56 ( PascalFrancis/Corpus ); précédent : 002E55; suivant : 002E57

Zoledronic acid and risedronate in the prevention and treatment of glucocorticoid-induced osteoporosis (HORIZON) : a multicentre, double-blind, double-dummy, randomised controlled trial

Auteurs : David M. Reid ; Jean-Pierre Devogelaer ; Kenneth Saag ; Christian Roux ; Chak-Sing Lau ; Jean-Yves Reginster ; Philemon Papanastasiou ; Alberto Ferreira ; Florian Hartl ; Taiwo Fashola ; Peter Mesenbrink ; Philip N. Sambrook

Source :

RBID : Pascal:09-0189564

Descripteurs français

English descriptors

Abstract

Background Persistent use of glucocorticoid drugs is associated with bone loss and increased fracture risk. Concurrent oral bisphosphonates increase bone mineral density and reduce frequency of vertebral fractures, but are associated with poor compliance and adherence. We aimed to assess whether one intravenous infusion of zoledronic acid was non-inferior to daily oral risedronate for prevention and treatment ofglucocorticoid-induced osteoporosis. Methods This 1-year randomised, double-blind, double-dummy, non-inferiority study of 54 centres in 12 European countries, Australia, Hong Kong, Israel, and the USA, tested the effectiveness of 5 mg intravenous infusion of zoledronic acid versus 5 mg oral risedronate for prevention and treatment of glucocorticoid-induced osteoporosis. 833 patients were randomised 1:1 to receive zoledronic acid (n=416) or risedronate (n=417). Patients were stratified by sex, and allocated to prevention or treatment subgroups dependent on duration of glucocorticoid use immediately preceding the study. The treatment subgroup consisted of those treated for more than 3 months (272 patients on zoledronic acid and 273 on risedronate), and the prevention subgroup of those treated for less than 3 months (144 patients on each drug). 62 patients did not complete the study because of adverse events, withdrawal of consent, loss to follow-up, death, misrandomisation, or protocol deviation. The primary endpoint was percentage change from baseline in lumbar spine bone mineral density. Drug efficacy was assessed on a modified intention-to-treat basis and safety was assessed on an intention-to-treat basis. This trial is registered with ClinicalTrials.gov, number NCT00100620. Findings Zoledronic acid was non-inferior and superior to risedronate for increase of lumbar spine bone mineral density in both the treatment (least-squares mean 4.06% [SE 0.28] vs 2-71% [SE 0.28], mean difference 1-36% [95% CI 0.67-2.05], p=0.0001) and prevention (2.60% [0.45] vs 0.64% [0.46], 1-96% [1.04-2.88], p<0.0001) subgroups at 12 months. Adverse events were more frequent in patients given zoledronic acid than in those on risedronate, largely as a result of transient symptoms during the first 3 days after infusion. Serious adverse events were worsening rheumatoid arthritis for the treatment subgroup and pyrexia for the prevention subgroup. Interpretation A single 5 mg intravenous infusion of zoledronic acid is non-inferior, possibly more effective, and more acceptable to patients than is 5 mg of oral risedronate daily for prevention and treatment of bone loss that is associated with glucocorticoid use.

Notice en format standard (ISO 2709)

Pour connaître la documentation sur le format Inist Standard.

pA  
A01 01  1    @0 0140-6736
A02 01      @0 LANCAO
A03   1    @0 Lancet : (Br. ed.)
A05       @2 373
A06       @2 9671
A08 01  1  ENG  @1 Zoledronic acid and risedronate in the prevention and treatment of glucocorticoid-induced osteoporosis (HORIZON) : a multicentre, double-blind, double-dummy, randomised controlled trial
A11 01  1    @1 REID (David M.)
A11 02  1    @1 DEVOGELAER (Jean-Pierre)
A11 03  1    @1 SAAG (Kenneth)
A11 04  1    @1 ROUX (Christian)
A11 05  1    @1 LAU (Chak-Sing)
A11 06  1    @1 REGINSTER (Jean-Yves)
A11 07  1    @1 PAPANASTASIOU (Philemon)
A11 08  1    @1 FERREIRA (Alberto)
A11 09  1    @1 HARTL (Florian)
A11 10  1    @1 FASHOLA (Taiwo)
A11 11  1    @1 MESENBRINK (Peter)
A11 12  1    @1 SAMBROOK (Philip N.)
A14 01      @1 University of Aberdeen @2 Aberdeen @3 GBR @Z 1 aut.
A14 02      @1 Université Catholique de Louvain @2 Brussels @3 BEL @Z 2 aut.
A14 03      @1 University of Alabama at Birmingham @2 Birmingham, AL @3 USA @Z 3 aut.
A14 04      @1 Paris-Descartes University @2 Paris @3 FRA @Z 4 aut.
A14 05      @1 University of Dundee @2 Dundee @3 GBR @Z 5 aut.
A14 06      @1 University of Liège @2 Liège @3 BEL @Z 6 aut.
A14 07      @1 Novartis Pharma AG @2 Basel @3 CHE @Z 7 aut. @Z 8 aut. @Z 10 aut.
A14 08      @1 F Hoffman-LaRoche AG @2 Basel @3 CHE @Z 9 aut.
A14 09      @1 Novartis Pharmaceuticals Corporation @2 East Hanover, NJ @3 USA @Z 11 aut.
A14 10      @1 University of Sydney @2 Sydney, NSW @3 AUS @Z 12 aut.
A17 01  1    @1 HORIZON investigators @3 INC
A20       @1 1253-1263
A21       @1 2009
A23 01      @0 ENG
A43 01      @1 INIST @2 5004 @5 354000186816280150
A44       @0 0000 @1 © 2009 INIST-CNRS. All rights reserved.
A45       @0 33 ref.
A47 01  1    @0 09-0189564
A60       @1 P
A61       @0 A
A64 01  1    @0 Lancet : (British edition)
A66 01      @0 GBR
C01 01    ENG  @0 Background Persistent use of glucocorticoid drugs is associated with bone loss and increased fracture risk. Concurrent oral bisphosphonates increase bone mineral density and reduce frequency of vertebral fractures, but are associated with poor compliance and adherence. We aimed to assess whether one intravenous infusion of zoledronic acid was non-inferior to daily oral risedronate for prevention and treatment ofglucocorticoid-induced osteoporosis. Methods This 1-year randomised, double-blind, double-dummy, non-inferiority study of 54 centres in 12 European countries, Australia, Hong Kong, Israel, and the USA, tested the effectiveness of 5 mg intravenous infusion of zoledronic acid versus 5 mg oral risedronate for prevention and treatment of glucocorticoid-induced osteoporosis. 833 patients were randomised 1:1 to receive zoledronic acid (n=416) or risedronate (n=417). Patients were stratified by sex, and allocated to prevention or treatment subgroups dependent on duration of glucocorticoid use immediately preceding the study. The treatment subgroup consisted of those treated for more than 3 months (272 patients on zoledronic acid and 273 on risedronate), and the prevention subgroup of those treated for less than 3 months (144 patients on each drug). 62 patients did not complete the study because of adverse events, withdrawal of consent, loss to follow-up, death, misrandomisation, or protocol deviation. The primary endpoint was percentage change from baseline in lumbar spine bone mineral density. Drug efficacy was assessed on a modified intention-to-treat basis and safety was assessed on an intention-to-treat basis. This trial is registered with ClinicalTrials.gov, number NCT00100620. Findings Zoledronic acid was non-inferior and superior to risedronate for increase of lumbar spine bone mineral density in both the treatment (least-squares mean 4.06% [SE 0.28] vs 2-71% [SE 0.28], mean difference 1-36% [95% CI 0.67-2.05], p=0.0001) and prevention (2.60% [0.45] vs 0.64% [0.46], 1-96% [1.04-2.88], p<0.0001) subgroups at 12 months. Adverse events were more frequent in patients given zoledronic acid than in those on risedronate, largely as a result of transient symptoms during the first 3 days after infusion. Serious adverse events were worsening rheumatoid arthritis for the treatment subgroup and pyrexia for the prevention subgroup. Interpretation A single 5 mg intravenous infusion of zoledronic acid is non-inferior, possibly more effective, and more acceptable to patients than is 5 mg of oral risedronate daily for prevention and treatment of bone loss that is associated with glucocorticoid use.
C02 01  X    @0 002B01
C02 02  X    @0 002B30A03
C02 03  X    @0 002B15A
C03 01  X  FRE  @0 Acide zolédronique @2 NK @2 FR @5 01
C03 01  X  ENG  @0 Zoledronic acid @2 NK @2 FR @5 01
C03 01  X  SPA  @0 Acido zoledrónico @2 NK @2 FR @5 01
C03 02  X  FRE  @0 Prévention @5 02
C03 02  X  ENG  @0 Prevention @5 02
C03 02  X  SPA  @0 Prevención @5 02
C03 03  X  FRE  @0 Traitement @5 03
C03 03  X  ENG  @0 Treatment @5 03
C03 03  X  SPA  @0 Tratamiento @5 03
C03 04  X  FRE  @0 Acide risédronique @2 NK @2 FR @5 04
C03 04  X  ENG  @0 Risedronic acid @2 NK @2 FR @5 04
C03 04  X  SPA  @0 Acido risedrónico @2 NK @2 FR @5 04
C03 05  X  FRE  @0 Glucocorticoïde @5 05
C03 05  X  ENG  @0 Glucocorticoid @5 05
C03 05  X  SPA  @0 Glucocorticoide @5 05
C03 06  X  FRE  @0 Etude multicentrique @5 06
C03 06  X  ENG  @0 Multicenter study @5 06
C03 06  X  SPA  @0 Estudio multicéntrico @5 06
C03 07  X  FRE  @0 Ostéoporose @5 07
C03 07  X  ENG  @0 Osteoporosis @5 07
C03 07  X  SPA  @0 Osteoporosis @5 07
C03 08  X  FRE  @0 Essai clinique @5 08
C03 08  X  ENG  @0 Clinical trial @5 08
C03 08  X  SPA  @0 Ensayo clínico @5 08
C03 09  X  FRE  @0 Médecine @5 09
C03 09  X  ENG  @0 Medicine @5 09
C03 09  X  SPA  @0 Medicina @5 09
C03 10  X  FRE  @0 Antirésorptif @5 25
C03 10  X  ENG  @0 Antiresorptive agent @5 25
C03 10  X  SPA  @0 Antirresortivo @5 25
C03 11  X  FRE  @0 Antiostéoporotique @5 26
C03 11  X  ENG  @0 Antiosteoporotic @5 26
C03 11  X  SPA  @0 Antiosteoporótico @5 26
C03 12  X  FRE  @0 Anticancéreux @5 27
C03 12  X  ENG  @0 Antineoplastic agent @5 27
C03 12  X  SPA  @0 Anticanceroso @5 27
C03 13  X  FRE  @0 Antiostéoclastique @5 28
C03 13  X  ENG  @0 Antiosteoclastic agent @5 28
C03 13  X  SPA  @0 Antiosteoclástica @5 28
C07 01  X  FRE  @0 Bisphosphonates @5 37
C07 01  X  ENG  @0 Bisphosphonates @5 37
C07 01  X  SPA  @0 Bisfosfonatos @5 37
C07 02  X  FRE  @0 Dérivé de l'acide diphosphonique @5 38
C07 02  X  ENG  @0 Diphosphonic acid derivatives @5 38
C07 02  X  SPA  @0 Difosfonico ácido derivado @5 38
C07 03  X  FRE  @0 Pathologie du système ostéoarticulaire @5 39
C07 03  X  ENG  @0 Diseases of the osteoarticular system @5 39
C07 03  X  SPA  @0 Sistema osteoarticular patología @5 39
N21       @1 138
N44 01      @1 OTO
N82       @1 OTO

Format Inist (serveur)

NO : PASCAL 09-0189564 INIST
ET : Zoledronic acid and risedronate in the prevention and treatment of glucocorticoid-induced osteoporosis (HORIZON) : a multicentre, double-blind, double-dummy, randomised controlled trial
AU : REID (David M.); DEVOGELAER (Jean-Pierre); SAAG (Kenneth); ROUX (Christian); LAU (Chak-Sing); REGINSTER (Jean-Yves); PAPANASTASIOU (Philemon); FERREIRA (Alberto); HARTL (Florian); FASHOLA (Taiwo); MESENBRINK (Peter); SAMBROOK (Philip N.)
AF : University of Aberdeen/Aberdeen/Royaume-Uni (1 aut.); Université Catholique de Louvain/Brussels/Belgique (2 aut.); University of Alabama at Birmingham/Birmingham, AL/Etats-Unis (3 aut.); Paris-Descartes University/Paris/France (4 aut.); University of Dundee/Dundee/Royaume-Uni (5 aut.); University of Liège/Liège/Belgique (6 aut.); Novartis Pharma AG/Basel/Suisse (7 aut., 8 aut., 10 aut.); F Hoffman-LaRoche AG/Basel/Suisse (9 aut.); Novartis Pharmaceuticals Corporation/East Hanover, NJ/Etats-Unis (11 aut.); University of Sydney/Sydney, NSW/Australie (12 aut.)
DT : Publication en série; Niveau analytique
SO : Lancet : (British edition); ISSN 0140-6736; Coden LANCAO; Royaume-Uni; Da. 2009; Vol. 373; No. 9671; Pp. 1253-1263; Bibl. 33 ref.
LA : Anglais
EA : Background Persistent use of glucocorticoid drugs is associated with bone loss and increased fracture risk. Concurrent oral bisphosphonates increase bone mineral density and reduce frequency of vertebral fractures, but are associated with poor compliance and adherence. We aimed to assess whether one intravenous infusion of zoledronic acid was non-inferior to daily oral risedronate for prevention and treatment ofglucocorticoid-induced osteoporosis. Methods This 1-year randomised, double-blind, double-dummy, non-inferiority study of 54 centres in 12 European countries, Australia, Hong Kong, Israel, and the USA, tested the effectiveness of 5 mg intravenous infusion of zoledronic acid versus 5 mg oral risedronate for prevention and treatment of glucocorticoid-induced osteoporosis. 833 patients were randomised 1:1 to receive zoledronic acid (n=416) or risedronate (n=417). Patients were stratified by sex, and allocated to prevention or treatment subgroups dependent on duration of glucocorticoid use immediately preceding the study. The treatment subgroup consisted of those treated for more than 3 months (272 patients on zoledronic acid and 273 on risedronate), and the prevention subgroup of those treated for less than 3 months (144 patients on each drug). 62 patients did not complete the study because of adverse events, withdrawal of consent, loss to follow-up, death, misrandomisation, or protocol deviation. The primary endpoint was percentage change from baseline in lumbar spine bone mineral density. Drug efficacy was assessed on a modified intention-to-treat basis and safety was assessed on an intention-to-treat basis. This trial is registered with ClinicalTrials.gov, number NCT00100620. Findings Zoledronic acid was non-inferior and superior to risedronate for increase of lumbar spine bone mineral density in both the treatment (least-squares mean 4.06% [SE 0.28] vs 2-71% [SE 0.28], mean difference 1-36% [95% CI 0.67-2.05], p=0.0001) and prevention (2.60% [0.45] vs 0.64% [0.46], 1-96% [1.04-2.88], p<0.0001) subgroups at 12 months. Adverse events were more frequent in patients given zoledronic acid than in those on risedronate, largely as a result of transient symptoms during the first 3 days after infusion. Serious adverse events were worsening rheumatoid arthritis for the treatment subgroup and pyrexia for the prevention subgroup. Interpretation A single 5 mg intravenous infusion of zoledronic acid is non-inferior, possibly more effective, and more acceptable to patients than is 5 mg of oral risedronate daily for prevention and treatment of bone loss that is associated with glucocorticoid use.
CC : 002B01; 002B30A03; 002B15A
FD : Acide zolédronique; Prévention; Traitement; Acide risédronique; Glucocorticoïde; Etude multicentrique; Ostéoporose; Essai clinique; Médecine; Antirésorptif; Antiostéoporotique; Anticancéreux; Antiostéoclastique
FG : Bisphosphonates; Dérivé de l'acide diphosphonique; Pathologie du système ostéoarticulaire
ED : Zoledronic acid; Prevention; Treatment; Risedronic acid; Glucocorticoid; Multicenter study; Osteoporosis; Clinical trial; Medicine; Antiresorptive agent; Antiosteoporotic; Antineoplastic agent; Antiosteoclastic agent
EG : Bisphosphonates; Diphosphonic acid derivatives; Diseases of the osteoarticular system
SD : Acido zoledrónico; Prevención; Tratamiento; Acido risedrónico; Glucocorticoide; Estudio multicéntrico; Osteoporosis; Ensayo clínico; Medicina; Antirresortivo; Antiosteoporótico; Anticanceroso; Antiosteoclástica
LO : INIST-5004.354000186816280150
ID : 09-0189564

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<name sortKey="Papanastasiou, Philemon" sort="Papanastasiou, Philemon" uniqKey="Papanastasiou P" first="Philemon" last="Papanastasiou">Philemon Papanastasiou</name>
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<s1>Novartis Pharma AG</s1>
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<name sortKey="Fashola, Taiwo" sort="Fashola, Taiwo" uniqKey="Fashola T" first="Taiwo" last="Fashola">Taiwo Fashola</name>
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<name sortKey="Mesenbrink, Peter" sort="Mesenbrink, Peter" uniqKey="Mesenbrink P" first="Peter" last="Mesenbrink">Peter Mesenbrink</name>
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<author>
<name sortKey="Sambrook, Philip N" sort="Sambrook, Philip N" uniqKey="Sambrook P" first="Philip N." last="Sambrook">Philip N. Sambrook</name>
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<s1>University of Sydney</s1>
<s2>Sydney, NSW</s2>
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<title level="j" type="main">Lancet : (British edition)</title>
<title level="j" type="abbreviated">Lancet : (Br. ed.)</title>
<idno type="ISSN">0140-6736</idno>
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<date when="2009">2009</date>
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<term>Antineoplastic agent</term>
<term>Antiosteoclastic agent</term>
<term>Antiosteoporotic</term>
<term>Antiresorptive agent</term>
<term>Clinical trial</term>
<term>Glucocorticoid</term>
<term>Medicine</term>
<term>Multicenter study</term>
<term>Osteoporosis</term>
<term>Prevention</term>
<term>Risedronic acid</term>
<term>Treatment</term>
<term>Zoledronic acid</term>
</keywords>
<keywords scheme="Pascal" xml:lang="fr">
<term>Acide zolédronique</term>
<term>Prévention</term>
<term>Traitement</term>
<term>Acide risédronique</term>
<term>Glucocorticoïde</term>
<term>Etude multicentrique</term>
<term>Ostéoporose</term>
<term>Essai clinique</term>
<term>Médecine</term>
<term>Antirésorptif</term>
<term>Antiostéoporotique</term>
<term>Anticancéreux</term>
<term>Antiostéoclastique</term>
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<front>
<div type="abstract" xml:lang="en">Background Persistent use of glucocorticoid drugs is associated with bone loss and increased fracture risk. Concurrent oral bisphosphonates increase bone mineral density and reduce frequency of vertebral fractures, but are associated with poor compliance and adherence. We aimed to assess whether one intravenous infusion of zoledronic acid was non-inferior to daily oral risedronate for prevention and treatment ofglucocorticoid-induced osteoporosis. Methods This 1-year randomised, double-blind, double-dummy, non-inferiority study of 54 centres in 12 European countries, Australia, Hong Kong, Israel, and the USA, tested the effectiveness of 5 mg intravenous infusion of zoledronic acid versus 5 mg oral risedronate for prevention and treatment of glucocorticoid-induced osteoporosis. 833 patients were randomised 1:1 to receive zoledronic acid (n=416) or risedronate (n=417). Patients were stratified by sex, and allocated to prevention or treatment subgroups dependent on duration of glucocorticoid use immediately preceding the study. The treatment subgroup consisted of those treated for more than 3 months (272 patients on zoledronic acid and 273 on risedronate), and the prevention subgroup of those treated for less than 3 months (144 patients on each drug). 62 patients did not complete the study because of adverse events, withdrawal of consent, loss to follow-up, death, misrandomisation, or protocol deviation. The primary endpoint was percentage change from baseline in lumbar spine bone mineral density. Drug efficacy was assessed on a modified intention-to-treat basis and safety was assessed on an intention-to-treat basis. This trial is registered with ClinicalTrials.gov, number NCT00100620. Findings Zoledronic acid was non-inferior and superior to risedronate for increase of lumbar spine bone mineral density in both the treatment (least-squares mean 4.06% [SE 0.28] vs 2-71% [SE 0.28], mean difference 1-36% [95% CI 0.67-2.05], p=0.0001) and prevention (2.60% [0.45] vs 0.64% [0.46], 1-96% [1.04-2.88], p<0.0001) subgroups at 12 months. Adverse events were more frequent in patients given zoledronic acid than in those on risedronate, largely as a result of transient symptoms during the first 3 days after infusion. Serious adverse events were worsening rheumatoid arthritis for the treatment subgroup and pyrexia for the prevention subgroup. Interpretation A single 5 mg intravenous infusion of zoledronic acid is non-inferior, possibly more effective, and more acceptable to patients than is 5 mg of oral risedronate daily for prevention and treatment of bone loss that is associated with glucocorticoid use.</div>
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<s0>Background Persistent use of glucocorticoid drugs is associated with bone loss and increased fracture risk. Concurrent oral bisphosphonates increase bone mineral density and reduce frequency of vertebral fractures, but are associated with poor compliance and adherence. We aimed to assess whether one intravenous infusion of zoledronic acid was non-inferior to daily oral risedronate for prevention and treatment ofglucocorticoid-induced osteoporosis. Methods This 1-year randomised, double-blind, double-dummy, non-inferiority study of 54 centres in 12 European countries, Australia, Hong Kong, Israel, and the USA, tested the effectiveness of 5 mg intravenous infusion of zoledronic acid versus 5 mg oral risedronate for prevention and treatment of glucocorticoid-induced osteoporosis. 833 patients were randomised 1:1 to receive zoledronic acid (n=416) or risedronate (n=417). Patients were stratified by sex, and allocated to prevention or treatment subgroups dependent on duration of glucocorticoid use immediately preceding the study. The treatment subgroup consisted of those treated for more than 3 months (272 patients on zoledronic acid and 273 on risedronate), and the prevention subgroup of those treated for less than 3 months (144 patients on each drug). 62 patients did not complete the study because of adverse events, withdrawal of consent, loss to follow-up, death, misrandomisation, or protocol deviation. The primary endpoint was percentage change from baseline in lumbar spine bone mineral density. Drug efficacy was assessed on a modified intention-to-treat basis and safety was assessed on an intention-to-treat basis. This trial is registered with ClinicalTrials.gov, number NCT00100620. Findings Zoledronic acid was non-inferior and superior to risedronate for increase of lumbar spine bone mineral density in both the treatment (least-squares mean 4.06% [SE 0.28] vs 2-71% [SE 0.28], mean difference 1-36% [95% CI 0.67-2.05], p=0.0001) and prevention (2.60% [0.45] vs 0.64% [0.46], 1-96% [1.04-2.88], p<0.0001) subgroups at 12 months. Adverse events were more frequent in patients given zoledronic acid than in those on risedronate, largely as a result of transient symptoms during the first 3 days after infusion. Serious adverse events were worsening rheumatoid arthritis for the treatment subgroup and pyrexia for the prevention subgroup. Interpretation A single 5 mg intravenous infusion of zoledronic acid is non-inferior, possibly more effective, and more acceptable to patients than is 5 mg of oral risedronate daily for prevention and treatment of bone loss that is associated with glucocorticoid use.</s0>
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<ET>Zoledronic acid and risedronate in the prevention and treatment of glucocorticoid-induced osteoporosis (HORIZON) : a multicentre, double-blind, double-dummy, randomised controlled trial</ET>
<AU>REID (David M.); DEVOGELAER (Jean-Pierre); SAAG (Kenneth); ROUX (Christian); LAU (Chak-Sing); REGINSTER (Jean-Yves); PAPANASTASIOU (Philemon); FERREIRA (Alberto); HARTL (Florian); FASHOLA (Taiwo); MESENBRINK (Peter); SAMBROOK (Philip N.)</AU>
<AF>University of Aberdeen/Aberdeen/Royaume-Uni (1 aut.); Université Catholique de Louvain/Brussels/Belgique (2 aut.); University of Alabama at Birmingham/Birmingham, AL/Etats-Unis (3 aut.); Paris-Descartes University/Paris/France (4 aut.); University of Dundee/Dundee/Royaume-Uni (5 aut.); University of Liège/Liège/Belgique (6 aut.); Novartis Pharma AG/Basel/Suisse (7 aut., 8 aut., 10 aut.); F Hoffman-LaRoche AG/Basel/Suisse (9 aut.); Novartis Pharmaceuticals Corporation/East Hanover, NJ/Etats-Unis (11 aut.); University of Sydney/Sydney, NSW/Australie (12 aut.)</AF>
<DT>Publication en série; Niveau analytique</DT>
<SO>Lancet : (British edition); ISSN 0140-6736; Coden LANCAO; Royaume-Uni; Da. 2009; Vol. 373; No. 9671; Pp. 1253-1263; Bibl. 33 ref.</SO>
<LA>Anglais</LA>
<EA>Background Persistent use of glucocorticoid drugs is associated with bone loss and increased fracture risk. Concurrent oral bisphosphonates increase bone mineral density and reduce frequency of vertebral fractures, but are associated with poor compliance and adherence. We aimed to assess whether one intravenous infusion of zoledronic acid was non-inferior to daily oral risedronate for prevention and treatment ofglucocorticoid-induced osteoporosis. Methods This 1-year randomised, double-blind, double-dummy, non-inferiority study of 54 centres in 12 European countries, Australia, Hong Kong, Israel, and the USA, tested the effectiveness of 5 mg intravenous infusion of zoledronic acid versus 5 mg oral risedronate for prevention and treatment of glucocorticoid-induced osteoporosis. 833 patients were randomised 1:1 to receive zoledronic acid (n=416) or risedronate (n=417). Patients were stratified by sex, and allocated to prevention or treatment subgroups dependent on duration of glucocorticoid use immediately preceding the study. The treatment subgroup consisted of those treated for more than 3 months (272 patients on zoledronic acid and 273 on risedronate), and the prevention subgroup of those treated for less than 3 months (144 patients on each drug). 62 patients did not complete the study because of adverse events, withdrawal of consent, loss to follow-up, death, misrandomisation, or protocol deviation. The primary endpoint was percentage change from baseline in lumbar spine bone mineral density. Drug efficacy was assessed on a modified intention-to-treat basis and safety was assessed on an intention-to-treat basis. This trial is registered with ClinicalTrials.gov, number NCT00100620. Findings Zoledronic acid was non-inferior and superior to risedronate for increase of lumbar spine bone mineral density in both the treatment (least-squares mean 4.06% [SE 0.28] vs 2-71% [SE 0.28], mean difference 1-36% [95% CI 0.67-2.05], p=0.0001) and prevention (2.60% [0.45] vs 0.64% [0.46], 1-96% [1.04-2.88], p<0.0001) subgroups at 12 months. Adverse events were more frequent in patients given zoledronic acid than in those on risedronate, largely as a result of transient symptoms during the first 3 days after infusion. Serious adverse events were worsening rheumatoid arthritis for the treatment subgroup and pyrexia for the prevention subgroup. Interpretation A single 5 mg intravenous infusion of zoledronic acid is non-inferior, possibly more effective, and more acceptable to patients than is 5 mg of oral risedronate daily for prevention and treatment of bone loss that is associated with glucocorticoid use.</EA>
<CC>002B01; 002B30A03; 002B15A</CC>
<FD>Acide zolédronique; Prévention; Traitement; Acide risédronique; Glucocorticoïde; Etude multicentrique; Ostéoporose; Essai clinique; Médecine; Antirésorptif; Antiostéoporotique; Anticancéreux; Antiostéoclastique</FD>
<FG>Bisphosphonates; Dérivé de l'acide diphosphonique; Pathologie du système ostéoarticulaire</FG>
<ED>Zoledronic acid; Prevention; Treatment; Risedronic acid; Glucocorticoid; Multicenter study; Osteoporosis; Clinical trial; Medicine; Antiresorptive agent; Antiosteoporotic; Antineoplastic agent; Antiosteoclastic agent</ED>
<EG>Bisphosphonates; Diphosphonic acid derivatives; Diseases of the osteoarticular system</EG>
<SD>Acido zoledrónico; Prevención; Tratamiento; Acido risedrónico; Glucocorticoide; Estudio multicéntrico; Osteoporosis; Ensayo clínico; Medicina; Antirresortivo; Antiosteoporótico; Anticanceroso; Antiosteoclástica</SD>
<LO>INIST-5004.354000186816280150</LO>
<ID>09-0189564</ID>
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