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Indicated Prevention With Omega-3 Fatty Acids in Adolescents With 'At-Risk-Mental-State' for Psychosis

Primary Purpose

Schizophrenia, Prodrome

Status
Completed
Phase
Phase 4
Locations
Austria
Study Type
Interventional
Intervention
Omega 3 fatty acids
Sponsored by
Medical University of Vienna
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional prevention trial for Schizophrenia focused on measuring Ultra-High Risk, Psychosis, Schizophrenia, Omega-3 fatty acids, RCT

Eligibility Criteria

13 Years - 25 Years (Child, Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  1. /written informed consent (for individuals under 18 written informed consent of at least one of the parents is required),
  2. /age between 13 and 25 years,
  3. /ARMS as classified by the PACE criteria (Yung et al., 1998)

PACE criteria for ARMS include one or more of following characteristics which must have occurred within the last 12 months:

  • Frank psychotic symptoms < 1 week (Transient psychosis group)
  • Attenuated psychotic symptoms > 1 week, > 2 times per week
  • Decline in global function (drop in GAF of > 30%) plus family history of psychosis or individual has schizotypal personality disorder To operationalize PACE criteria duration and severity ratings of psychotic symptoms will be performed using the Positive and Negative Syndromes of Schizophrenia Scale (PANSS) (Kay et al., 1987) applying following cut-off scores, following Morrison et al (2002): Ad 1) Transient psychosis is defined with the presence of symptoms that score 4 or more on hallucinations, 4 or more on delusions, or 5 or more on conceptual disorganizations, last less than one week and resolve without antipsychotic medication. Ad 2) Attenuated psychotic symptoms are defined by the presence of symptoms that score 3 on delusions, 2-3 on hallucinations, 3-4 on suspiciousness or 3-4 on conceptual disorganization.

Exclusion Criteria:

  1. /Acute suicidal behaviour, aggressive behaviour (PANSS hostility, suicidality = 7),
  2. /Drug abuse that contributed decisively to the presentation of the index episode, (dependency on morphine, cocaine, amphetamine, but not THC),
  3. /Alcohol abuse if considered as major problem,
  4. /Epilepsy,
  5. /Mental Retardation (IQ<80),
  6. /Pregnancy and lactation,
  7. /Structural changes in MRI or CT scan (e.g., tumours), expect for enlargement of ventricles or sulci,
  8. /Previous history of antipsychotic drug (>1 week) or mood stabilizer treatment,
  9. /Laboratory values more than 10% outside the normal range for transaminases, CRP or bleeding parameters,
  10. /Individuals with organic brain syndrome,
  11. /Individuals who are taking anticoagulants,
  12. /Individuals who are taking omega 3 supplements, currently or within 8 weeks of being included in the trial,
  13. /Individuals who have other, severe, intercurrent illness which in the opinion of the investigator may put them at risk or influence the results of the trial or affect ability to take part in the trial.

Sites / Locations

  • Medical University of Vienna, Department of Child and Adolescent Psychiatry

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Placebo Comparator

Arm Label

A

B

Arm Description

Coconut oil

Outcomes

Primary Outcome Measures

Transition to PANSS defined first-episode psychosis

Secondary Outcome Measures

PANSS positive, negative, and global subscales
MADRS
GAF
UKU
Lipid metabolism in peripheral tissue pre/post treatment

Full Information

First Posted
November 6, 2006
Last Updated
December 20, 2007
Sponsor
Medical University of Vienna
Collaborators
Stanley Medical Research Institute
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1. Study Identification

Unique Protocol Identification Number
NCT00396643
Brief Title
Indicated Prevention With Omega-3 Fatty Acids in Adolescents With 'At-Risk-Mental-State' for Psychosis
Official Title
Indicated Prevention With Omega-3 Fatty Acids in Adolescents With 'At-Risk-Mental-State' for Psychosis: A Randomised, Double Blind, Placebo-Controlled Treatment Trial
Study Type
Interventional

2. Study Status

Record Verification Date
December 2007
Overall Recruitment Status
Completed
Study Start Date
May 2004 (undefined)
Primary Completion Date
June 2007 (Actual)
Study Completion Date
June 2007 (Actual)

3. Sponsor/Collaborators

Name of the Sponsor
Medical University of Vienna
Collaborators
Stanley Medical Research Institute

4. Oversight

Data Monitoring Committee
Yes

5. Study Description

Brief Summary
Early intervention in psychosis might be associated with better outcomes. However, intervention in the pre-psychotic phase has been questioned as, using current criteria, only 20-50% of individuals classified as prodromal develop a psychotic disorder within a 1-2 years period. Treatment agents investigated in the pre-psychotic phase of schizophrenia and other psychotic disorders should, therefore, not have major side effects. This proposal investigates omega-3 fatty acids (1.2 gramm per day eicosapentaenoic acid/docosahexaenoic acid;EPA/DHA) as a beneficial and possible preventive therapeutic agent in young people at ultra high-risk for developing a psychotic disorder.
Detailed Description
Aims of the study The principal aim is to test if 1.2 g/day EPA/DHA can prevent transition to first-episode psychosis in 13-25 year old ultra-high risk individuals. Specifically we propose to investigate: The clinical effects of EPA/DHA supplementation as an adjunct to standard therapy in individuals with 'At-Risk Mental State' (ARMS) for psychosis as defined by the PACE criteria (Yung et al., 1998). Lipid metabolism in peripheral tissue pre/post treatment by 1./analyzing bioactive lipid composition of red-blood cell membranes, 2./measuring phospholipase A2 (cPLA2) activity in serum (the enzyme responsible for the cleavage of arachidonic acid (AA) and other precursors of bioactive lipids from glycerophospholipids (GPL) and 3./the topical niacin flush test (a clinical test of the AA-prostaglandin D2 cascade). Background and evidence that bioactive lipids are altered in schizophrenia and can be influenced by EPA/DHA supplementation There is suggestion that early intervention in psychosis might be associated with better outcomes (Norman & Malla, 2001). However, intervention in the pre-psychotic phase has been questioned as, using current criteria, only 20-50% of individuals classified as prodromal develop a psychotic disorder within a 1-2 years period (McGlashan et al., 2001). Treatment agents investigated in the pre-psychotic phase of schizophrenia and other psychotic disorders should, therefore, not have major side effects. This proposal introduces EPA/DHA, two omega-3 essential fatty acids (EFA), as a beneficial and possible preventative therapeutic agent in young people at ultra high-risk for developing a psychotic disorder. Bioactive lipids and their role in the brain Bioactive lipids are molecules that have both intra- and intercellular roles, including mediation, modulation and control of neurobiological processes, such as ion channel and receptor activity, neurotransmitter release, synaptic plasticity, second messenger pathways and neuronal gene expression (Agranoff et al., 1998). Emphasis has been placed on AA and its metabolites, known collectively as eicosanoids. A major proportion of lipids in the brain consist of bioactive lipids such as AA and its metabolites, also referred to as EFA, which are mainly bound to GPL. Bioactive lipids are released through direct and indirect enzymatic pathways (e.g., phospholipases) from membrane GPL. AA is a precursor of prostaglandins, thromboxanes, leukotriens (5-HpETE) and prostacyclins. Animal studies and preliminary studies in humans have shown an association between bioactive lipid metabolism, behaviour and cognition (Zimmer et al., 2000). Reduced membrane EFA in schizophrenia Abnormal membrane GPL EFA metabolism has been suggested to contribute to the aetiopathophysiology of schizophrenia. A recent review of 15 published studies confirmed a depletion of bioactive lipids in cell membranes of patients with schizophrenia (Fenton et al., 2000). The most consistent findings were reductions in AA and its precursors, and these were independent of drug treatment (Yao et al., 1996). Reductions in AA and its precursors have also been found in post mortem brains of patients with schizophrenia, relative to normal control brains [Yao et al., 2000]. Yao and van Kammen (1996) suggested that defective uptake of AA into membrane GPL was a possible aetiopathological mechanism in schizophrenia, whereas Peet et al. (1996), who reported an additional increase of EFA peroxidation products, suggested there was increased breakdown of membrane GPL. Khan et al. (2002) reported on erythrocyte membrane EFA levels and levels of plasma lipid peroxides, products of damaged EFAs, in drug-naive patients within +/-4.5 days of onset of psychosis. The levels of EFAs, particularly AA and docosahexaenoic acid (DHA) were significantly lower in drug-naive patients at the onset of psychosis compared to matched normal controls. These lower EFA levels were associated with significantly higher levels of lipid peroxides in patients. The levels of AA and DHA were also lower and lipid peroxides higher in chronic medicated patients than normal controls. Interestingly in context with this proposal, EFA levels were higher in chronic medicated patients than drug-naive first-episode patients. Khan et al. concluded that these findings could indicate that lower membrane AA and DHA most likely predate the illness and probably contribute to the onset of illness. The lipid peroxidation data suggest that possible increased oxidative stress may be one of the mechanisms of reduced membrane EFAs. The findings also imply that supplementation of EFAs and/or antioxidants might provide effective treatments for early psychosis. This view is supported by Horrobin et al. (2002) who showed that increase in red cell AA levels resulted from treatment with the optimal levels of EPA and that, clinical improvement was highly significantly positively correlated with rises in red cell membrane AA in individuals with schizophrenia. Treatment studies in schizophrenia Three randomized controlled treatment studies conducted over 12 weeks found 2g/day EPA significantly more effective than placebo in reducing psychopathological symptoms in individuals with schizophrenia (Peet et al., 2001; Emsley et al., 2002). Symptom improvements in those studies were both, clinically relevant and statistically significant. A dose-ranging exploratory study of the effects of EPA in individuals with schizophrenia who experienced persistent symptoms found 2 g EPA/day significantly more effective in reducing symptom scores on psychiatric rating scales than 1g and 4g EPA/day (Peet et al., 2002). On the other hand, Fenton et al. (2002) investigated augmentation of neuroleptics with 3 g/day of EPA on symptoms and cognition in patients with schizophrenia or schizoaffective disorder and reported a negative finding. The patients in Fenton et al.s' study had, however, been ill for two decades and had substantial symptoms, despite treatment with newer neuroleptics, including clozapine. The patients described as benefiting from EPA in the other studies were younger and had a shorter duration of illness. It must be emphasized that in all EPA treatment studies, no treatment-related side effects or adverse biochemical or haematological effects have been observed. EPA proved safe to administer to schizophrenic patients as an adjunct therapy. EPA did not cause side effects other than mild gastrointestinal symptoms by itself, nor did it enhance the side effects of existing drugs. Patients found EPA highly tolerable. The proportion of patients who completed 12 weeks (89%) compares favourably with mean withdrawal rates of 54% in the novel neuroleptic groups and 67% in the placebo groups in trials in the FDA database (Peet et al., 2002). Acceptance of a substance which is normally found in the human body without significant side effects, with a potency potentially similar to the antipsychotic drugs in the early phase of psychotic disorders could contribute to reduce the duration of untreated psychosis and to increase compliance. Study design We will use a prospective, randomized, double-blind, placebo-controlled, single-centre study design. Eighty one individuals aged 13-25 will be randomly assigned in two treatment conditions at the University Clinic for Child and Adolescent Neuropsychiatry, Vienna, Austria. Randomization codes will be generated and stored off site. The treatment groups will receive 1.2 gramm per day EPA/DHA or placebo for 12 weeks. Follow-up assessments will be conducted at 1,2,3,4,8,12,26,and 52 weeks. All patients will receive standard treatment, which includes management by a psychiatrist or resident psychiatrist and non-neuroleptic pharmacotherapy as clinically indicated.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Schizophrenia, Prodrome
Keywords
Ultra-High Risk, Psychosis, Schizophrenia, Omega-3 fatty acids, RCT

7. Study Design

Primary Purpose
Prevention
Study Phase
Phase 4
Interventional Study Model
Parallel Assignment
Masking
ParticipantCare ProviderInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
81 (Actual)

8. Arms, Groups, and Interventions

Arm Title
A
Arm Type
Experimental
Arm Title
B
Arm Type
Placebo Comparator
Arm Description
Coconut oil
Intervention Type
Drug
Intervention Name(s)
Omega 3 fatty acids
Intervention Description
The active treatment is a supplement of yellow gelatin 0.5 g fish oil capsules. The daily dose of 4 (2x2) capsules provides 700 mg of eicosapentaenoic acid and 500 mg of docosahexaenoic acid, and 10 mg of Vitamin E. Placebo treatment comprises coconut oil capsules, carefully matched with the active treatment with respect to both appearance and flavor, also containing 10 mg Vitamin E, and 10 mg of fish oil to mimic taste. Coconut oil was chosen as placebo because it does not contain polyunsaturated fatty acids and has no impact on n-3 fatty acid metabolism. The intervention period is 12 weeks.
Primary Outcome Measure Information:
Title
Transition to PANSS defined first-episode psychosis
Time Frame
Baseline, 1, 2, 3, 4, 8, 12 weeks, 6, and 12 months
Secondary Outcome Measure Information:
Title
PANSS positive, negative, and global subscales
Time Frame
Baseline, 1, 2, 3, 4, 8, 12 weeks, 6, and 12 months
Title
MADRS
Time Frame
Baseline, 1, 2, 3, 4, 8, 12 weeks, 6, and 12 months
Title
GAF
Time Frame
Baseline, 1, 2, 3, 4, 8, 12 weeks, 6, and 12 months
Title
UKU
Time Frame
Baseline, 1, 2, 3, 4, 8, 12 weeks
Title
Lipid metabolism in peripheral tissue pre/post treatment
Time Frame
Baseline, 12 weeks

10. Eligibility

Sex
All
Minimum Age & Unit of Time
13 Years
Maximum Age & Unit of Time
25 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: /written informed consent (for individuals under 18 written informed consent of at least one of the parents is required), /age between 13 and 25 years, /ARMS as classified by the PACE criteria (Yung et al., 1998) PACE criteria for ARMS include one or more of following characteristics which must have occurred within the last 12 months: Frank psychotic symptoms < 1 week (Transient psychosis group) Attenuated psychotic symptoms > 1 week, > 2 times per week Decline in global function (drop in GAF of > 30%) plus family history of psychosis or individual has schizotypal personality disorder To operationalize PACE criteria duration and severity ratings of psychotic symptoms will be performed using the Positive and Negative Syndromes of Schizophrenia Scale (PANSS) (Kay et al., 1987) applying following cut-off scores, following Morrison et al (2002): Ad 1) Transient psychosis is defined with the presence of symptoms that score 4 or more on hallucinations, 4 or more on delusions, or 5 or more on conceptual disorganizations, last less than one week and resolve without antipsychotic medication. Ad 2) Attenuated psychotic symptoms are defined by the presence of symptoms that score 3 on delusions, 2-3 on hallucinations, 3-4 on suspiciousness or 3-4 on conceptual disorganization. Exclusion Criteria: /Acute suicidal behaviour, aggressive behaviour (PANSS hostility, suicidality = 7), /Drug abuse that contributed decisively to the presentation of the index episode, (dependency on morphine, cocaine, amphetamine, but not THC), /Alcohol abuse if considered as major problem, /Epilepsy, /Mental Retardation (IQ<80), /Pregnancy and lactation, /Structural changes in MRI or CT scan (e.g., tumours), expect for enlargement of ventricles or sulci, /Previous history of antipsychotic drug (>1 week) or mood stabilizer treatment, /Laboratory values more than 10% outside the normal range for transaminases, CRP or bleeding parameters, /Individuals with organic brain syndrome, /Individuals who are taking anticoagulants, /Individuals who are taking omega 3 supplements, currently or within 8 weeks of being included in the trial, /Individuals who have other, severe, intercurrent illness which in the opinion of the investigator may put them at risk or influence the results of the trial or affect ability to take part in the trial.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
G Paul Amminger, MD
Organizational Affiliation
Medical University of Vienna
Official's Role
Principal Investigator
Facility Information:
Facility Name
Medical University of Vienna, Department of Child and Adolescent Psychiatry
City
Vienna
ZIP/Postal Code
1090
Country
Austria

12. IPD Sharing Statement

Citations:
Citation
Berger GE, Proffitt TM, McConchie M, et al. Ethyl-Eicosapentaenoic acid in first episode psychosis: A randomized, placebo-controlled trial. Journal of Clinical Psychiatry 2007; in press Berger GE, Wood SJ, Wellard RM, et al. In vivo brain effects of ethyl-eicosapentaenoic acid in early psychosis. A 1H-MRS study. Neuropsychopharmacology 2007;in press.
Results Reference
background
PubMed Identifier
28126360
Citation
Smesny S, Milleit B, Schaefer MR, Hesse J, Schlogelhofer M, Langbein K, Hipler UC, Berger M, Cotter DR, Sauer H, McGorry PD, Amminger GP. Effects of omega-3 PUFA on immune markers in adolescent individuals at ultra-high risk for psychosis - Results of the randomized controlled Vienna omega-3 study. Schizophr Res. 2017 Oct;188:110-117. doi: 10.1016/j.schres.2017.01.026. Epub 2017 Jan 23.
Results Reference
derived
PubMed Identifier
27650124
Citation
Focking M, Dicker P, Lopez LM, Cannon M, Schafer MR, McGorry PD, Smesny S, Cotter DR, Amminger GP. Differential expression of the inflammation marker IL12p40 in the at-risk mental state for psychosis: a predictor of transition to psychotic disorder? BMC Psychiatry. 2016 Sep 20;16(1):326. doi: 10.1186/s12888-016-1039-7.
Results Reference
derived
PubMed Identifier
23870722
Citation
Amminger GP, Chanen AM, Ohmann S, Klier CM, Mossaheb N, Bechdolf A, Nelson B, Thompson A, McGorry PD, Yung AR, Schafer MR. Omega-3 fatty acid supplementation in adolescents with borderline personality disorder and ultra-high risk criteria for psychosis: a post hoc subgroup analysis of a double-blind, randomized controlled trial. Can J Psychiatry. 2013 Jul;58(7):402-8. doi: 10.1177/070674371305800705.
Results Reference
derived
PubMed Identifier
20124114
Citation
Amminger GP, Schafer MR, Papageorgiou K, Klier CM, Cotton SM, Harrigan SM, Mackinnon A, McGorry PD, Berger GE. Long-chain omega-3 fatty acids for indicated prevention of psychotic disorders: a randomized, placebo-controlled trial. Arch Gen Psychiatry. 2010 Feb;67(2):146-54. doi: 10.1001/archgenpsychiatry.2009.192.
Results Reference
derived
Links:
URL
http://www.stanleyresearch.org/
Description
The Stanley Medical Research Institute

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Indicated Prevention With Omega-3 Fatty Acids in Adolescents With 'At-Risk-Mental-State' for Psychosis

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