Psychotic Disorders Clinical Trial
Official title:
Rapid Tranquilization of Violent or Agitated People in Psychiatric Emergency Settings- A Pragmatic Randomized Controlled Trial of Intramuscular Olanzepine Vs. Intramuscular Haloperidol + Promethazine.
Three hundred consecutive adult patients presenting to the emergency services of the
department of psychiatry and who are diagnosed by the treating doctor to be needing
tranquillization to control agitated or aggressive behavior will be randomized to receive
either Injection Olanzepine I.M. or Injection Haloperidol 10mg + Injection Promethazine 50
mg in this parallel group, block randomized, centrally-randomzed, allocation-concealed,
assessor-blinded pragmatic clinical trial.
The main outcome measure that the two treatments would be compared on would be the clinical
state of the patient 4 hours after intervention, but the rate of tranquillization, degree of
sedation, proportions tranquil and / or asleep at 15, 30, 60 and 240 minutes, need for
additional medication, use of physical restraints, doctors called back, numbers absconding
and adverse effects at each of these time points would also be compared. Compliance with
oral medication and adverse effects at the end of 2 weeks would also be compared.
Participants:
Consecutive adult psychiatric patients presenting to the department of psychiatry as
outpatients, or those who are admitted, who have violent, aggressive or agitated behavior.
Inclusion criteria
1. The attending physician feels that intramuscular sedation is clearly indicated because
of agitation, aggression or violent behaviour, and
2. The physician does not feel that either one of the interventions poses an additional
risk for the patient.
3. The patient or a responsible relative provides informed consent to participate in the
trial.
Exclusion Criteria
1. Patients who lack capacity to give informed consent and who do not have a relative to
obtain consent from will be excluded from the study protocol.
2. The physician feels either one of the interventions poses a risk for the patient.
Ethical considerations Good evidence on the treatment of acutely disturbed patients is
missing because of the perceived difficulty in performing trials in nonconsenting patients.
However, close reading of the recent draft of the Helsinki declaration reveals that trials
in nonconsenting patients are permitted on 2 conditions: (1) no other context exists in
which to answer the question, and (2) all trial participants get clear therapeutic benefit
from whichever arm they are randomized to. So placebos cannot be used in these studies.
The present trial proposes to study the efficacy of two interventions that are reportedly
effective and safe in the management of acute violence, but whose relative merits are
unclear, and shall only enroll participants whose relatives provide consent, if they
themselves are unable to do so, as is likely in this context.
Randomisation and allocation concealment Randomisation will be in accordance with a computer
generated list of random numbers in varying sized blocks of less than 10 prepared by the UK
collaborator. This collaborator will send the randomisation codes electronically to an
investigator with no clinical responsibilities in the trial, who will work with the
pharmacist to prepare sequentially numbered, sealed, opaque, identical cardboard boxes that
will have either Haloperidol 5 mgs × 2 ampoules + promethazine 50 mgs × 1 ampoule or
Olanzepine 10 mg × 1 vial + water for injection, according to the randomisation sequence,
plus a disposable syringe and needle and study forms. The outside of the box will have a
form in which the participants’ ID, scores on the Clinical Global Impression Severity Scale
(Guy, 1976), and clinical diagnosis will be recorded whilst blind to the contents of the
box.
Procedure:
Once eligibility of a patient is ensured, the next consecutive box shall be taken from the
emergency cupboard and this will constitute randomization. The duty doctor shall record the
severity of the episode and the initial diagnosis on the form stuck to the outside of the
sealed intervention pack. The box shall then be opened and the intervention administered.
The patient will then followed up at 15, 30, 60 and 120 min by the treatment team and at 240
min and at 2 weeks by the study coordinators. Data will also obtained from the case notes as
well as from interviews with relatives and the treatment team.
Blinding:
The study will be blind until the point of treatment assignment, which will minimize
selection bias. After assignment, ratings for the first 2 h will not be blind as the
management team will need to know the prescribed medications. This is a pragmatic trial that
evaluates real-world interventions that are not given blind. However, at each of the
assessment points in the first two hours, 30 % of the ratings will be additionally rated by
one of the investigators who will be blind to the interventions. In addition, one of the
investigators who will be blind to interventions given shall undertake ratings at 240 min.
At this time, they will also guess the allocated intervention, to assess their blinding.
Outcomes:
Patients shall be rated at each assessment point on whether they are tranquil or asleep; in
addition, the time of onset of tranquillization and sleep will be noted. Participants will
be considered to be tranquil when they are calm and not exhibiting agitated, aggressive or
dangerous behavior to others, property, or to themselves. They will considered to be asleep
if, on inspection, they appear to be sound asleep and are not aroused by ambient
disturbances; the depth of this apparent slumber will not assessed further. They shall also
be rated on the Clinical Global Impression – Severity (CGI–S) scale at entry, and the
CGI–Improvement (CGI–I) scale (Guy, 1976) with respect to aggression and violence, the
Simpson–Angus extra pyramidal side-effects rating scale (Simpson & Angus, 1970) and the
Barnes Akathisia Scale (Barnes, 1989) at each assessment point; any other clinically
important adverse effect, especially dystonia, will be noted. These assessments shall be
conducted only on participants who are awake, as extra pyramidal symptoms are usually not
apparent during sleep or, in the case of dystonia or akathisia, are likely to prevent sleep.
Other outcomes within the first 4 hours will be the use of additional medication for control
of agitated or aggressive behavior, the use of physical restraints, the need for further
medical attention and numbers absconding. Participants shall also be followed up 2 weeks
later to check for adverse effects. The primary outcome will be ‘tranquil or asleep by 4
hours’.
The inter-rater reliability of the investigators in rating outcomes shall be established to
be satisfactory before the commencement of the trial.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind, Primary Purpose: Treatment
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