Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study

Lone Baandrup; OPTiMiSE study group; Rene Kahn; Iris Sommer; Inge Winter-van Rossum; Metten Somers; Paula C Ywema; Shitisj Kapur; Philip McGuire; Marion Leboyer; Andres Meyer-Lindenberg; Shon W Lewis; Stefan Leucht; Celso Arango; Wolfgang W Fleischhacker; Anne Lotte Meijering; Jocelyn Petter; Resy Van de Brug; Joost Schotsman; Jildou Zwerver; Jos Peuskens; Marc De Hert; Erik Thys; Lucho G Hranov; Valentin Hranov; Jan Libiger; Richard Köhler; Pavel Mohr; Birte Glenthøj; Brian Broberg; Signe Düring; Lone Baandrup; Stephane Jamain; Stephan Heres; Dan Rujescu; Ina Giegling; Mark Weiser; Mor Bar Heim; Michael Davidson; Silvana Galderisi; Paola Bucci; Armida Mucci; Janusz Rybakowski; Agnieszka Remlinger-Molenda; Ilan Gonen; Paull Radu; Marina Díaz-Marsá; Alberto Rodriguez-Jiminez; Tomas Palomo; Roberto Rodriguez-Jiminez; Paz García-Portilla; Miquel Bernado; Julio Bobes; Christina Vilares Oliveira; Gregor Berger; Claudia Wildt; Paola Dazzan; Roccio Perez-Iglesias; Richard Drake; Sarah Gregory; Danielle Wilson; Covadonga M Díaz-Caneja; Marius J C Eijkemans

doi:10.1016/S2215-0366(18)30252-9

Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study

Lone Baandrup (Medlem af forfattergruppering), OPTiMiSE study group, Rene Kahn, Iris Sommer, Inge Winter-van Rossum, Metten Somers, Paula C Ywema, Shitisj Kapur, Philip McGuire, Marion Leboyer, Andres Meyer-Lindenberg, Shon W Lewis, Stefan Leucht, Celso Arango, Wolfgang W Fleischhacker, Anne Lotte Meijering, Jocelyn Petter, Resy Van de Brug, Joost Schotsman, Jildou ZwerverJos Peuskens, Marc De Hert, Erik Thys, Lucho G Hranov, Valentin Hranov, Jan Libiger, Richard Köhler, Pavel Mohr, Birte Glenthøj, Brian Broberg, Signe Düring, Lone Baandrup, Stephane Jamain, Stephan Heres, Dan Rujescu, Ina Giegling, Mark Weiser, Mor Bar Heim, Michael Davidson, Silvana Galderisi, Paola Bucci, Armida Mucci, Janusz Rybakowski, Agnieszka Remlinger-Molenda, Ilan Gonen, Paull Radu, Marina Díaz-Marsá, Alberto Rodriguez-Jiminez, Tomas Palomo, Roberto Rodriguez-Jiminez, Paz García-Portilla, Miquel Bernado, Julio Bobes, Christina Vilares Oliveira, Gregor Berger, Claudia Wildt, Paola Dazzan, Roccio Perez-Iglesias, Richard Drake, Sarah Gregory, Danielle Wilson, Covadonga M Díaz-Caneja, Marius J C Eijkemans

154 Citationer (Scopus)

Abstract

BACKGROUND: No established treatment algorithm exists for patients with schizophrenia. Whether switching antipsychotics or early use of clozapine improves outcome in (first-episode) schizophrenia is unknown.

METHODS: This three-phase study was done in 27 centres, consisting of general hospitals and psychiatric specialty clinics, in 14 European countries and Israel. Patients aged 18-40 years who met criteria of the DSM-IV for schizophrenia, schizophreniform disorder, or schizoaffective disorder were treated for 4 weeks with up to 800 mg/day amisulpride orally in an open-label design (phase 1). Patients who did not meet symptomatic remission criteria at 4 weeks were randomly assigned to continue amisulpride or switch to olanzapine (≤20 mg/day) during a 6-week double-blind phase, with patients and staff masked to treatment allocation (phase 2). Randomisation was done online by a randomisation website; the application implemented stratification by site and sex, and applied the minimisation method for randomisation. Patients who were not in remission at 10 weeks were given clozapine (≤900 mg/day) for an additional 12 weeks in an open-label design (phase 3). The primary outcome was the number of patients who achieved symptomatic remission at the final visits of phases 1, 2, and 3, measured by intention-to-treat analysis. Data were analysed with a generalised linear mixed model, with a logistic link and binomial error distribution. This trial is registered with ClinicalTrials.gov, number NCT01248195, and closed to accrual.

FINDINGS: Between May 26, 2011, and May 15, 2016, we recruited 481 participants who signed informed consent. Of the 446 patients in the intention-to-treat sample, 371 (83%) completed open-label amisulpride treatment, and 250 (56%) achieved remission after phase 1. 93 patients who were not in remission continued to the 6-week double-blind switching trial, with 72 (77%) patients completing the trial (39 on olanzapine and 33 on amisulpride); 15 (45%) patients on amisulpride versus 17 (44%) on olanzapine achieved remission (p=0·87). Of the 40 patients who were not in remission after 10 weeks of treatment, 28 (70%) started on clozapine; 18 (64%) patients completed the 12-week treatment, and five (28%) achieved remission. The number of serious adverse events did not differ between the treatment arms in phase 2: one patient on olanzapine was admitted to hospital because of an epileptic seizure, and one patient on amisulpride was admitted to hospital twice because of exacerbations of psychotic symptoms. Over the course of the trial, two serious suicide attempts were reported.

INTERPRETATION: For most patients in the early stages of schizophrenia, symptomatic remission can be achieved using a simple treatment algorithm comprising the sequential administration of amisulpride and clozapine. Since switching to olanzapine did not improve outcome, clozapine should be used after patients fail a single antipsychotic trial-not until two antipsychotics have been tried, as is the current recommendation.

FUNDING: European Commission Seventh Framework Program.

Originalsprog	Engelsk
Artikelnummer	5
Tidsskrift	The Lancet. Psychiatry
Vol/bind	5
Udgave nummer	10
Sider (fra-til)	797-807
Antal sider	11
ISSN	2215-0366
DOI	https://doi.org/10.1016/S2215-0366(18)30252-9
Status	Udgivet - okt. 2018

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10.1016/S2215-0366(18)30252-9

Citationsformater

Baandrup, L., OPTiMiSE study group, Rene Kahn, Iris Sommer, Inge Winter-van Rossum, Metten Somers, Paula C Ywema, Shitisj Kapur, Philip McGuire, Marion Leboyer, Andres Meyer-Lindenberg, Shon W Lewis, Stefan Leucht, Celso Arango, Wolfgang W Fleischhacker, Anne Lotte Meijering, Jocelyn Petter, Resy Van de Brug, Joost Schotsman, ... Marius J C Eijkemans (2018). Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study. The Lancet. Psychiatry, 5(10), 797-807. Artikel 5. https://doi.org/10.1016/S2215-0366(18)30252-9

Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study. / Baandrup, Lone (Medlem af forfattergruppering); OPTiMiSE study group; Rene Kahn et al.
I: The Lancet. Psychiatry, Bind 5, Nr. 10, 5, 10.2018, s. 797-807.

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

Baandrup, L, OPTiMiSE study group, Rene Kahn, Iris Sommer, Inge Winter-van Rossum, Metten Somers, Paula C Ywema, Shitisj Kapur, Philip McGuire, Marion Leboyer, Andres Meyer-Lindenberg, Shon W Lewis, Stefan Leucht, Celso Arango, Wolfgang W Fleischhacker, Anne Lotte Meijering, Jocelyn Petter, Resy Van de Brug, Joost Schotsman, Jildou Zwerver, Jos Peuskens, Marc De Hert, Erik Thys, Lucho G Hranov, Valentin Hranov, Jan Libiger, Richard Köhler, Pavel Mohr, Birte Glenthøj, Brian Broberg, Signe Düring, Lone Baandrup, Stephane Jamain, Stephan Heres, Dan Rujescu, Ina Giegling, Mark Weiser, Mor Bar Heim, Michael Davidson, Silvana Galderisi, Paola Bucci, Armida Mucci, Janusz Rybakowski, Agnieszka Remlinger-Molenda, Ilan Gonen, Paull Radu, Marina Díaz-Marsá, Alberto Rodriguez-Jiminez, Tomas Palomo, Roberto Rodriguez-Jiminez, Paz García-Portilla, Miquel Bernado, Julio Bobes, Christina Vilares Oliveira, Gregor Berger, Claudia Wildt, Paola Dazzan, Roccio Perez-Iglesias, Richard Drake, Sarah Gregory, Danielle Wilson, Covadonga M Díaz-Caneja & Marius J C Eijkemans 2018, 'Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study', The Lancet. Psychiatry, bind 5, nr. 10, 5, s. 797-807. https://doi.org/10.1016/S2215-0366(18)30252-9

@article{07df6c6f708643f3a17bde76290b717c,

title = "Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study",

abstract = "BACKGROUND: No established treatment algorithm exists for patients with schizophrenia. Whether switching antipsychotics or early use of clozapine improves outcome in (first-episode) schizophrenia is unknown.METHODS: This three-phase study was done in 27 centres, consisting of general hospitals and psychiatric specialty clinics, in 14 European countries and Israel. Patients aged 18-40 years who met criteria of the DSM-IV for schizophrenia, schizophreniform disorder, or schizoaffective disorder were treated for 4 weeks with up to 800 mg/day amisulpride orally in an open-label design (phase 1). Patients who did not meet symptomatic remission criteria at 4 weeks were randomly assigned to continue amisulpride or switch to olanzapine (≤20 mg/day) during a 6-week double-blind phase, with patients and staff masked to treatment allocation (phase 2). Randomisation was done online by a randomisation website; the application implemented stratification by site and sex, and applied the minimisation method for randomisation. Patients who were not in remission at 10 weeks were given clozapine (≤900 mg/day) for an additional 12 weeks in an open-label design (phase 3). The primary outcome was the number of patients who achieved symptomatic remission at the final visits of phases 1, 2, and 3, measured by intention-to-treat analysis. Data were analysed with a generalised linear mixed model, with a logistic link and binomial error distribution. This trial is registered with ClinicalTrials.gov, number NCT01248195, and closed to accrual.FINDINGS: Between May 26, 2011, and May 15, 2016, we recruited 481 participants who signed informed consent. Of the 446 patients in the intention-to-treat sample, 371 (83%) completed open-label amisulpride treatment, and 250 (56%) achieved remission after phase 1. 93 patients who were not in remission continued to the 6-week double-blind switching trial, with 72 (77%) patients completing the trial (39 on olanzapine and 33 on amisulpride); 15 (45%) patients on amisulpride versus 17 (44%) on olanzapine achieved remission (p=0·87). Of the 40 patients who were not in remission after 10 weeks of treatment, 28 (70%) started on clozapine; 18 (64%) patients completed the 12-week treatment, and five (28%) achieved remission. The number of serious adverse events did not differ between the treatment arms in phase 2: one patient on olanzapine was admitted to hospital because of an epileptic seizure, and one patient on amisulpride was admitted to hospital twice because of exacerbations of psychotic symptoms. Over the course of the trial, two serious suicide attempts were reported.INTERPRETATION: For most patients in the early stages of schizophrenia, symptomatic remission can be achieved using a simple treatment algorithm comprising the sequential administration of amisulpride and clozapine. Since switching to olanzapine did not improve outcome, clozapine should be used after patients fail a single antipsychotic trial-not until two antipsychotics have been tried, as is the current recommendation.FUNDING: European Commission Seventh Framework Program.",

author = "Kahn, {Ren{\'e} S} and {Winter van Rossum}, Inge and Stefan Leucht and Philip McGuire and Lewis, {Shon W} and Marion Leboyer and Celso Arango and Paola Dazzan and Richard Drake and Stephan Heres and D{\'i}az-Caneja, {Covadonga M} and Dan Rujescu and Mark Weiser and Silvana Galderisi and Birte Glenth{\o}j and Eijkemans, {Marinus J C} and Fleischhacker, {W Wolfgang} and Shitij Kapur and Sommer, {Iris E} and Lone Baandrup and {OPTiMiSE study group} and {Rene Kahn} and {Iris Sommer} and {Inge Winter-van Rossum} and {Metten Somers} and {Paula C Ywema} and {Shitisj Kapur} and {Philip McGuire} and {Marion Leboyer} and {Andres Meyer-Lindenberg} and {Shon W Lewis} and {Stefan Leucht} and {Celso Arango} and {Wolfgang W Fleischhacker} and {Anne Lotte Meijering} and {Jocelyn Petter} and {Resy Van de Brug} and {Joost Schotsman} and {Jildou Zwerver} and {Jos Peuskens} and {Marc De Hert} and {Erik Thys} and {Lucho G Hranov} and {Valentin Hranov} and {Jan Libiger} and {Richard K{\"o}hler} and {Pavel Mohr} and {Birte Glenth{\o}j} and {Brian Broberg} and {Signe D{\"u}ring} and {Lone Baandrup} and {Stephane Jamain} and {Stephan Heres} and {Dan Rujescu} and {Ina Giegling} and {Mark Weiser} and {Mor Bar Heim} and {Michael Davidson} and {Silvana Galderisi} and {Paola Bucci} and {Armida Mucci} and {Janusz Rybakowski} and {Agnieszka Remlinger-Molenda} and {Ilan Gonen} and {Paull Radu} and {Marina D{\'i}az-Mars{\'a}} and {Alberto Rodriguez-Jiminez} and {Tomas Palomo} and {Roberto Rodriguez-Jiminez} and {Paz Garc{\'i}a-Portilla} and {Miquel Bernado} and {Julio Bobes} and {Christina Vilares Oliveira} and {Gregor Berger} and {Claudia Wildt} and {Paola Dazzan} and {Roccio Perez-Iglesias} and {Richard Drake} and {Sarah Gregory} and {Danielle Wilson} and {Covadonga M D{\'i}az-Caneja} and {Marius J C Eijkemans}",

year = "2018",

month = oct,

doi = "10.1016/S2215-0366(18)30252-9",

language = "English",

volume = "5",

pages = "797--807",

journal = "The Lancet. Psychiatry",

issn = "2215-0366",

publisher = "Elsevier Limited",

number = "10",

}

TY - JOUR

T1 - Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE)

T2 - a three-phase switching study

AU - Kahn, René S

AU - Winter van Rossum, Inge

AU - Leucht, Stefan

AU - McGuire, Philip

AU - Lewis, Shon W

AU - Leboyer, Marion

AU - Arango, Celso

AU - Dazzan, Paola

AU - Drake, Richard

AU - Heres, Stephan

AU - Díaz-Caneja, Covadonga M

AU - Rujescu, Dan

AU - Weiser, Mark

AU - Galderisi, Silvana

AU - Glenthøj, Birte

AU - Eijkemans, Marinus J C

AU - Fleischhacker, W Wolfgang

AU - Kapur, Shitij

AU - Sommer, Iris E

AU - OPTiMiSE study group

AU - Rene Kahn

AU - Iris Sommer

AU - Inge Winter-van Rossum

AU - Metten Somers

AU - Paula C Ywema

AU - Shitisj Kapur

AU - Philip McGuire

AU - Marion Leboyer

AU - Andres Meyer-Lindenberg

AU - Shon W Lewis

AU - Stefan Leucht

AU - Celso Arango

AU - Wolfgang W Fleischhacker

AU - Anne Lotte Meijering

AU - Jocelyn Petter

AU - Resy Van de Brug

AU - Joost Schotsman

AU - Jildou Zwerver

AU - Jos Peuskens

AU - Marc De Hert

AU - Erik Thys

AU - Lucho G Hranov

AU - Valentin Hranov

AU - Jan Libiger

AU - Richard Köhler

AU - Pavel Mohr

AU - Birte Glenthøj

AU - Brian Broberg

AU - Signe Düring

AU - Lone Baandrup

AU - Stephane Jamain

AU - Stephan Heres

AU - Dan Rujescu

AU - Ina Giegling

AU - Mark Weiser

AU - Mor Bar Heim

AU - Michael Davidson

AU - Silvana Galderisi

AU - Paola Bucci

AU - Armida Mucci

AU - Janusz Rybakowski

AU - Agnieszka Remlinger-Molenda

AU - Ilan Gonen

AU - Paull Radu

AU - Marina Díaz-Marsá

AU - Alberto Rodriguez-Jiminez

AU - Tomas Palomo

AU - Roberto Rodriguez-Jiminez

AU - Paz García-Portilla

AU - Miquel Bernado

AU - Julio Bobes

AU - Christina Vilares Oliveira

AU - Gregor Berger

AU - Claudia Wildt

AU - Paola Dazzan

AU - Roccio Perez-Iglesias

AU - Richard Drake

AU - Sarah Gregory

AU - Danielle Wilson

AU - Covadonga M Díaz-Caneja

AU - Marius J C Eijkemans

A2 - Baandrup, Lone

PY - 2018/10

Y1 - 2018/10

N2 - BACKGROUND: No established treatment algorithm exists for patients with schizophrenia. Whether switching antipsychotics or early use of clozapine improves outcome in (first-episode) schizophrenia is unknown.METHODS: This three-phase study was done in 27 centres, consisting of general hospitals and psychiatric specialty clinics, in 14 European countries and Israel. Patients aged 18-40 years who met criteria of the DSM-IV for schizophrenia, schizophreniform disorder, or schizoaffective disorder were treated for 4 weeks with up to 800 mg/day amisulpride orally in an open-label design (phase 1). Patients who did not meet symptomatic remission criteria at 4 weeks were randomly assigned to continue amisulpride or switch to olanzapine (≤20 mg/day) during a 6-week double-blind phase, with patients and staff masked to treatment allocation (phase 2). Randomisation was done online by a randomisation website; the application implemented stratification by site and sex, and applied the minimisation method for randomisation. Patients who were not in remission at 10 weeks were given clozapine (≤900 mg/day) for an additional 12 weeks in an open-label design (phase 3). The primary outcome was the number of patients who achieved symptomatic remission at the final visits of phases 1, 2, and 3, measured by intention-to-treat analysis. Data were analysed with a generalised linear mixed model, with a logistic link and binomial error distribution. This trial is registered with ClinicalTrials.gov, number NCT01248195, and closed to accrual.FINDINGS: Between May 26, 2011, and May 15, 2016, we recruited 481 participants who signed informed consent. Of the 446 patients in the intention-to-treat sample, 371 (83%) completed open-label amisulpride treatment, and 250 (56%) achieved remission after phase 1. 93 patients who were not in remission continued to the 6-week double-blind switching trial, with 72 (77%) patients completing the trial (39 on olanzapine and 33 on amisulpride); 15 (45%) patients on amisulpride versus 17 (44%) on olanzapine achieved remission (p=0·87). Of the 40 patients who were not in remission after 10 weeks of treatment, 28 (70%) started on clozapine; 18 (64%) patients completed the 12-week treatment, and five (28%) achieved remission. The number of serious adverse events did not differ between the treatment arms in phase 2: one patient on olanzapine was admitted to hospital because of an epileptic seizure, and one patient on amisulpride was admitted to hospital twice because of exacerbations of psychotic symptoms. Over the course of the trial, two serious suicide attempts were reported.INTERPRETATION: For most patients in the early stages of schizophrenia, symptomatic remission can be achieved using a simple treatment algorithm comprising the sequential administration of amisulpride and clozapine. Since switching to olanzapine did not improve outcome, clozapine should be used after patients fail a single antipsychotic trial-not until two antipsychotics have been tried, as is the current recommendation.FUNDING: European Commission Seventh Framework Program.

AB - BACKGROUND: No established treatment algorithm exists for patients with schizophrenia. Whether switching antipsychotics or early use of clozapine improves outcome in (first-episode) schizophrenia is unknown.METHODS: This three-phase study was done in 27 centres, consisting of general hospitals and psychiatric specialty clinics, in 14 European countries and Israel. Patients aged 18-40 years who met criteria of the DSM-IV for schizophrenia, schizophreniform disorder, or schizoaffective disorder were treated for 4 weeks with up to 800 mg/day amisulpride orally in an open-label design (phase 1). Patients who did not meet symptomatic remission criteria at 4 weeks were randomly assigned to continue amisulpride or switch to olanzapine (≤20 mg/day) during a 6-week double-blind phase, with patients and staff masked to treatment allocation (phase 2). Randomisation was done online by a randomisation website; the application implemented stratification by site and sex, and applied the minimisation method for randomisation. Patients who were not in remission at 10 weeks were given clozapine (≤900 mg/day) for an additional 12 weeks in an open-label design (phase 3). The primary outcome was the number of patients who achieved symptomatic remission at the final visits of phases 1, 2, and 3, measured by intention-to-treat analysis. Data were analysed with a generalised linear mixed model, with a logistic link and binomial error distribution. This trial is registered with ClinicalTrials.gov, number NCT01248195, and closed to accrual.FINDINGS: Between May 26, 2011, and May 15, 2016, we recruited 481 participants who signed informed consent. Of the 446 patients in the intention-to-treat sample, 371 (83%) completed open-label amisulpride treatment, and 250 (56%) achieved remission after phase 1. 93 patients who were not in remission continued to the 6-week double-blind switching trial, with 72 (77%) patients completing the trial (39 on olanzapine and 33 on amisulpride); 15 (45%) patients on amisulpride versus 17 (44%) on olanzapine achieved remission (p=0·87). Of the 40 patients who were not in remission after 10 weeks of treatment, 28 (70%) started on clozapine; 18 (64%) patients completed the 12-week treatment, and five (28%) achieved remission. The number of serious adverse events did not differ between the treatment arms in phase 2: one patient on olanzapine was admitted to hospital because of an epileptic seizure, and one patient on amisulpride was admitted to hospital twice because of exacerbations of psychotic symptoms. Over the course of the trial, two serious suicide attempts were reported.INTERPRETATION: For most patients in the early stages of schizophrenia, symptomatic remission can be achieved using a simple treatment algorithm comprising the sequential administration of amisulpride and clozapine. Since switching to olanzapine did not improve outcome, clozapine should be used after patients fail a single antipsychotic trial-not until two antipsychotics have been tried, as is the current recommendation.FUNDING: European Commission Seventh Framework Program.

U2 - 10.1016/S2215-0366(18)30252-9

DO - 10.1016/S2215-0366(18)30252-9

M3 - Journal article

C2 - 30115598

SN - 2215-0366

VL - 5

SP - 797

EP - 807

JO - The Lancet. Psychiatry

JF - The Lancet. Psychiatry

IS - 10

M1 - 5

ER -

Amisulpride and olanzapine followed by open-label treatment with clozapine in first-episode schizophrenia and schizophreniform disorder (OPTiMiSE): a three-phase switching study

Abstract

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