Assessment scales

Several scales have been developed to provide standardisation of agitation assessment, including, but not limited to, the Overt Agitation Severity Scale (Reference Yudofsky, Kopecky and KunikYudofsky 1997) and the Agitated Behavior Scale (Reference CorriganCorrigan 1989), which are used in the context of traumatic brain injury, and the Positive and Negative Syndrome Scale, Excited Component (PANSS-EC; Reference Kay, Fiszbein and OplerKay 1987), used in the context of psychotic illness. These scales tend to conceptualise agitation on a spectrum, ranging from anxiety to aggression, and reflecting the three major components present in most definitions of agitation: strong emotion, excessive motor/vocal behaviour, and inappropriate or non-purposeful motor/vocal behaviour (Reference CitromeCitrome 2004a). Anxiety, at one end of the spectrum, as defined by DSM-IV (American Psychiatric Association 1994), entails subjective symptoms manifested through a variety of somatic complaints, including distractibility, nervousness and difficulty concentrating. At the other end of the spectrum, aggression is more consistent with verbal abuse, verbal and physical threats, and threats of violence (Reference Ness, House and NessNess 2000). In some cases, agitation may even manifest as explicit violent behaviour directed at others (Reference Kopecky, Kopecky and YudofskyKopecky 1998).

Evolution of management methods

In the USA, as in other countries, early efforts at managing agitation were focused on physically restraining and/or sedating the patient, a form of ‘chemical restraint’ – generating a stuporous or even unconscious state in an agitated patient (Reference WiseWise 2000). Rather than addressing the source of agitation, sedation merely masked it. This masking effect hindered not only agitation management but also diagnostic efforts. Sedation may be mistaken for negative symptoms and/or cognitive deficits (Reference MillerMiller 2004), compromising assessment and diagnosis, and may also contribute to non-adherence to medication because of patients’ negative feelings about taking it (Reference CitromeCitrome 2004a).

Agitation management has evolved significantly, with a strong move away from physical and ‘chemical’ restraints that risk physically injuring (Reference Buckley, Noffsinger and SmithBuckley 2003) or over-sedating patients (Reference Downey, Zun and GonzalesDowney 2007). Nevertheless, these restraint methods continue to be used in about 60% of emergency departments throughout the USA (Reference Downey, Zun and GonzalesDowney 2007).

Non-pharmacological interventions

In the UK, the National Institute for Health and Clinical Excellence (NICE) emphasises the importance of non-pharmacological interventions in managing agitation, recommending that rapid tranquillisation (also known as urgent sedation) be used only ‘in situations requiring the rapid control of agitation, aggression or excitement … when other less coercive techniques of calming … such as verbal de-escalation … have failed’ (National Collaborating Centre for Nursing and Supportive Care 2005: p. 27).

In both the USA and the UK, the primary concern when first approaching an agitated patient is the safety of the patient and those nearby. For this reason, isolation of the patient from others while the crisis is contained is crucial (Reference WiseWise 2000). Stimulation from radio, television and so on may also contribute to an agitated state and should be minimised. Verbal one-on-one interaction (de-escalation) has been demonstrated to reduce anxiety and help patients regain control and should be enacted early in management (Reference FisherFisher 1994).

In the USA, the Joint Commission on Accreditation of Healthcare Organizations (JCAHO) mandated in 2000 that restraint and/or seclusion can only be used in an emergency, when other attempts to manage agitation have failed and there is imminent risk of harm to a patient or others (Reference WiseWise 2000). Therefore, in the USA seclusion and restraints are considered treatments of last resort and should be used as such (Reference Buckley, Noffsinger and SmithBuckley 2003). In the UK, however, the NICE guidelines recommend seclusion if rapid tranquillisation is contraindicated but they note that it should not be considered a therapeutic intervention; rather, it should be seen as allowing a period of calming for the patient.

The UK is in agreement with the USA in recommending that physical restraint (which NICE calls physical intervention) be used only as a last resort, when there is a real possibility of significant harm if it is not used. In most situations, the restraint should be limited to manual holding: mechanical devices such as belts or handcuffs should not be used, except in exceptional circumstances, usually within high-security settings (National Collaborating Centre for Nursing and Supportive Care 2005: p. 26).

Pharmacological interventions (rapid tranquillisation)

Pharmacological management of acute agitation has been typically limited to four classes of medication: barbiturates, benzodiazepines, typical antipsychotics and, more recently, atypical antipsychotics. For years, barbiturates and then typical antipsychotics with or without benzodiazepines (most commonly, intramuscular administration of 5 mg haloperidol and 2 mg lorazepam) have been the mainstay of treatment (Reference BellnierBellnier 2002). However, 93% of patients prefer oral formulations during a behavioural emergency, perceiving parenteral administration as coercive and abusive (Reference Altamura, Sassella and SantiniAltamura 2003). Recent literature has shown that, for patients willing to take them, oral atypical antipsychotics are at least as effective as intramuscular typical antipsychotics in acute psychotic agitation (Reference Currier, Trenton and WalshCurrier 2006a). They should therefore be the first-line method of pharmacological administration (Reference Mohr, Pecenák and SvestkaMohr 2005).

In 2005, the US Journal of Psychiatric Practice published a supplement on the treatment of behavioural emergencies as part of its Expert Consensus Guidelines Series (Expert Consensus Panel for Behavioral Emergencies 2005). It was generated from responses to a survey by 48 of 50 invited leading American experts in psychiatric emergency medicine. The publication received financial support in the form of grants from AstraZeneca, Janssen and Pfizer but, to reduce any possible bias, the experts contacted were not aware of this. The survey resulted in the following recommendation for first-line treatment of acute schizophrenia or mania: oral olanzapine, oral risperidone, or haloperidol plus a benzodiazepine (Expert Consensus Panel for Behavioral Emergencies 2005).

Oral disintegrating (orodispersible) formulations that dissolve in seconds prevent patients from hiding tablets in their mouths and subsequently spitting them out; they are bioequivalent to regular tablets (Reference Van Schaick, Lechat and RemmerieVan Schaick 2003). However, the efficacy of oral formulations is limited by patients’ cooperation in taking them, which is problematic in many severely agitated patients. One literature review found that severe agitation could be managed with oral formulations alone in only 55% of cases (Reference De FruytDe Fruyt 2004).

The NICE guidelines recommend that vital signs be monitored after rapid tranquillisation and that pulse oximeters be available. Blood pressure, pulse, temperature, respiratory rate and hydration should be recorded regularly (National Collaborating Centre for Nursing and Supportive Care 2005: p. 102).

The most commonly used and recommended pharmacological agents for the management of agitation in psychosis are reviewed in the following sections.

Benzodiazepines

Benzodiazepines (Table 1) produce anti-agitation effects via modulation of γ-aminobutyric acid (GABA) neurotransmission and evidence suggests that they are at least as effective as – and at higher doses superior to – typical antipsychotics in agitation treatment (Reference Foster, Kessel and BermanFoster 1997; Reference AllenAllen 2000; Reference BattagliaBattaglia 2005). Benzodiazepines have significantly fewer extrapyramidal side-effects than typical antipsychotics, but they can cause respiratory depression, ataxia and excessive sedation (Reference AllenAllen 2000; Reference BattagliaBattaglia 2005). The sedative effect of benzodiazepines is the major limiting factor in their use for managing agitation: as discussed above, sedation should not be the endpoint of management and may hinder diagnosis.

TabLE 1 Benzodiazepines for acute agitation

Drug (formulation)	Key characteristics	Onset of action	Half-life
Clonazepam (oral/IM)	Not recommended: limited efficacy and may increase psychosis or agitation	20–60 min	19–50 h
Diazepam (oral/IM)	Long-lasting effect Prolonged sedation IM not recommended	0.5–2 h (oral)	30–60 h
Lorazepam (oral/IM)	Preferred benzodiazepine Complete, rapid intramuscular absorption	1–1.5h	12–15 h
Midazolam (oral/IM)	Effective for motor agitation Short-acting Greater sedation	5–15 min (IM) 10–30 min (oral)	1–4 h

Lorazepam is the most popular benzodiazepine for agitation, owing to its complete and rapid intramuscular absorption, onset within 60–90 minutes, half-life of 12–15 hours, and 8–10 hour duration of action (Reference BattagliaBattaglia 2005; Reference Greenblatt, Blaskovich and NuwayserGreenblatt 2005). Diazepam is frequently used for its long-lasting effect, but prolonged sedation of a patient is often not desirable, making shorter-acting benzodiazepines such as lorazepam more attractive. Evidence for the superiority of midazolam over haloperidol for managing motor agitation is encouraging, but it is overly sedating and the majority of patients treated with midazolam fell asleep after intramuscular administration (Reference Mendoza, Djenderedjian and AdamsMendoza 1987). Clonazepam has limited efficacy in treating agitation. It may in fact increase psychosis or agitation in some individuals and is therefore not recommended (Reference BattagliaBattaglia 2005).

Atypical antipsychotics

Atypical antipsychotics (Table 2) are a newer development in the management of agitation. Owing to their action on serotonergic as well as dopaminergic receptors they carry an adverse risk profile distinct from that of typical antipsychotics, with less dysphoria, akathisia and extrapyramidal side-effects (Reference BattagliaBattaglia 2005). Interestingly, some patients have even been reported to request an additional dose of an atypical antipsychotic when being treated for an agitated state in the emergency room (Reference Preval, Klotz and SouthardPreval 2005).

TabLE 2 Atypical antipsychotics for acute agitation

Drug (formulation)	Key characteristics	Onset of action	Half-life
Aripiprazole (oral/IM)	Lower risk of weight gain Delayed onset Possible somnolence	3–5 h	75–146h
Olanzapine (oral/IM)	Rapid onset Greater sedation, somnolence, weight gain Caution in hypotensive patients – avoid parenteral benzodiazepines	15–45 min	21–54 h
Quetiapine (oral)	Useful for aggressive patients	1.5 h	6 h
Risperidone (oral)	Not available in fast-acting IM formulation	1–2 h	20–24h
Ziprasidone (oral/IM)	Lower risk of weight gain Caution in patients with renal impairment Possible QT interval prolongation	30–45 min	2–5 h (IM) 7 h (oral)

Atypicals are available in both oral and intramuscular formulations. Intramuscular ziprasidone was made available in the USA in 2002, with indications for agitation associated with schizophrenia. Intramuscular olanzapine followed in 2004 for agitation associated with schizophrenia and bipolar mania. Finally, in 2006, intramuscular aripiprazole became available for agitation associated with schizophrenia and bipolar mania (Reference CitromeCitrome 2007).

The consensus guidelines mentioned above (Expert Consensus Panel for Behavioral Emergencies 2005) currently recommend atypical anti-psychotics as first-line agents for acute agitation in schizophrenia, although evidence of atypical antipsychotic efficacy in managing agitation in bipolar I disorder has also been established (Reference Meehan, Zhang and DavidMeehan 2001; Reference Zimbroff, Marcus and ManosZimbroff 2007). Olanzapine and risperidone are both available in disintegrating oral tablets and are therefore optimal as first-line interventions for patients who will take them.

Ziprasidone

Ziprasidone primarily acts as a dopamine/ serotonin antagonist. It has low potential for causing extrapyramidal symptoms and was the first atypical antipsychotic made available in rapid-acting intramuscular formulation, with an onset of action of 30–45 minutes (Reference BattagliaBattaglia 2005).

In the USA, the drug was approved for acute agitation in schizophrenia on the basis of two double-blind trials (Reference Daniel, Potkin and ReevesDaniel 2001; Reference Lesem, Zajecka and SwiftLesem 2001). Ziprasidone (10–20 mg) yields an NNT of 3 (95% CI 2–4) with the response criterion defined as at least a 2-point reduction in the Behavioural Activity Rating Scale, 2 hours after injection (Reference CitromeCitrome 2007). Incidence of movement disorders, including akathisia, dystonia and extrapyramidal symptoms, is < 4% compared with 12–38% for haloperidol (Reference MendelowitzMendelowitz 2004).

Safety concerns with intramuscular ziprasidone include caution when treating patients with renal impairment, as the cyclodextrin excipient is cleared by renal filtration. Ziprasidone is also known to cause greater dose-related QT interval prolongation than haloperidol, olanzapine and risperidone. Owing to fatal arrhythmias associated with QT prolongation caused by other drugs, ziprasidone is contraindicated in patients with a known history of QT prolongation, recent myocardial infarction or uncompensated heart failure (Reference GlassmanGlassman 2001; Pfizer 2009).

Olanzapine

Olanzapine, which acts on multiple receptors, has an onset of action of 15–45 minutes (Reference BattagliaBattaglia 2004). Three placebo-controlled trials that showed the superiority of 2.5–10 mg of intramuscular olanzapine over placebo and its non-inferiority to 7.5 mg intramuscular haloperidol provided the basis for olanzapine use in acute agitation associated with schizophrenia (Reference Wright, Birkett and DavidWright 2001; Reference CitromeCitrome 2007). However, placebo-controlled trials have indicated a higher incidence of sedation compared with placebo, with somnolence present in 29% of patients compared with 13% in the placebo arm (Eli Lilly 2006). Olanzapine can be as sedating as haloperidol or lorazepam (Reference Currier, Allen and BunneyCurrier 2004a). In a trial involving patients with schizophrenia, the NNT for 10 mg olanzapine was 3 (95% CI 2–3). In bipolar I mania, 10 mg olanzapine also yielded an NNT of 3 (95% CI 2–5) (Reference Meehan, Zhang and DavidMeehan 2001). Intramuscular olanzapine is as efficacious as haloperidol and has significant advantages in terms of extrapyramidal symptoms: Parkinsonism was avoided in 1 in 7 patients, acute dystonia in 1 in 14, and anticholinergic prescriptions were avoided in 1 in 7 patients (Reference Tulloch and ZedTulloch 2004; Reference CitromeCitrome 2007).

Safety concerns related to olanzapine include hypotension, bradycardia with or without hypotension, tachycardia and syncope. Consequently, parenteral benzodiazepines should be avoided in patients simultaneously receiving intramuscular olanzapine (Eli Lilly 2008). The number needed to harm (NNH) was significant for hypotension, at 50 (95% CI 30–154) compared with placebo (Reference CitromeCitrome 2007).

If possible, an oral formulation should be given at a loading dose of 5 to 20 mg, as this has been shown to be safe and effective at quickly calming acutely agitated psychotic patients (Reference Karagianis, Dawe and ThakurKaragianis 2001). Oral olanzapine can be used alone or with oral lorazepam, which has been shown to be as effective as oral haloperidol plus lorazepam in reducing acute agitation (Reference Escobar, San and PerezEscobar 2008). Oral olanzapine is uniquely advantageous in its efficacy as a monotherapy in both emergency rooms and psychiatric units, which not only contributes to medication adherence and a positive doctor–patient relationship, but also avoids the adverse effects often seen in transition from intramuscular to oral medications (Reference Escobar, San and PerezEscobar 2008).

Risperidone

Risperidone is a potent dopamine antagonist with high affinity for D₂ receptors and action on multiple serotonergic receptors. Despite the fact that risperidone is not currently available in a fast-acting intramuscular formulation, it has been found to be effective in managing agitation in patients willing to take oral medication. Earlier studies found that oral risperidone plus oral lorazepam was tolerable and comparable to intramuscular haloperidol plus lorazepam for short-term treatment of agitated psychosis in patients who accept oral medications (Reference Currier and AllenCurrier 2000, Reference Currier and Simpson2001, Reference Currier, Chou and Feifel2004b). A later study found that oral risperidone plus oral lorazepam was more successful at managing acute psychotic agitation 2 hours after administration when compared with intramuscular conventional antipsychotics such as haloperidol and zuclopenthixol (Reference Lejeune, Larmo and ChrzanowskiLejeune 2004). A meta-analysis found that risperidone yielded superior efficacy to haloperidol in managing hostility and aggression in patients with schizophrenia (Reference Aleman and KahnAleman 2001).

Aripiprazole

Aripiprazole differs pharmacologically from the other atypical antipsychotics in its partial agonism at dopamine D₂ and serotonin 5-HT_1A receptors and antagonism at 5-HT_2a receptors (Reference Burris, Molski and XuBurris 2002). In at least three randomised, double-blind, placebo-controlled studies it was found to be efficacious, safe and tolerable in treating agitation in patients with bipolar I disorder, schizophrenia or schizoaffective disorder (Reference Andrezina, Josiassen and MarcusAndrezina 2006; Reference Currier, Citrome and ZimbroffCurrier 2007; Reference Tran-Johnson, Sack and MarcusTran-Johnson 2007). In one of these studies (Reference Andrezina, Josiassen and MarcusAndrezina 2006) the efficacy of 9.75 mg intramuscular aripiprazole was established v. 6.5 mg intramuscular haloperidol. Aripiprazole demonstrated rapid and effective control of agitation in schizophrenia and schizoaffective disorder with a significant reduction in events involving extrapyramidal side-effects (1.7% v. 12.6%) (Reference CitromeCitrome 2007). A dose of 9.75 mg intramuscular aripiprazole was shown to be the most effective and best tolerated from a range of 1, 5.25, 9.75 and 15 mg (Reference GlassmanGlassman 2001). In schizophrenia, 9.75 mg aripiprazole has an NNT of 6 (95% CI 4–16); in bipolar mania, 10 mg and 15 mg aripiprazole have an NNT of 4 (95% CI 3–10) (Reference CitromeCitrome 2007). Aripiprazole has been associated with reduced sedation compared with placebo (Reference CitromeCitrome 2007), but somnolence has been reported to be marginally higher than with placebo (Bristol-Myers Squibb 2003). Compared with those on haloperidol, patients on aripiprazole had a 10% lower risk of extrapyramidal side-effects (Reference CitromeCitrome 2007).

Quetiapine

In emergency room psychiatric settings, quetiapine at doses ranging from 300 to 800 mg/day has been shown to be as effective as olanzapine and risperidone, and better tolerated than haloperidol (Reference Villari and RoccaVillari 2008), despite preliminary data that suggested it to be less efficacious than olanzapine and risperidone (Reference Raja and AzzoniRaja 2003). Relative to haloperidol, quetiapine at doses ranging from 150 to 750 mg has direct calming effects on agitation independent of its effect in improving psychosis. It demonstrated a reduction in both hostility and agitation among patients experiencing an acute exacerbation of schizophrenia (Reference Chengappa, Goldstein and GreenwoodChengappa 2003). In patients with aggressive psychosis, it has been reported to reduce overall aggression within the first 24 hours of treatment, aggression towards others by 83% within 2 days of treatment, and sustained reduction in overall aggression over 5 days of treatment (Reference Ganesan, Bilsker and KhanbhaiGanesan 2005).

The transition from intramuscular to oral formulations

Consensus guidelines recommend switching from intramuscular medication to oral formulations when managing long-term agitation subsequent to acute episodes (Expert Consensus Panel for Behavioral Emergencies 2005). This transition, although recommended, can engender adverse effects. Such effects are more common with typical than with atypical antipsychotics. In a comparison of haloperidol (without concomitant anticholinergic medication) and olanzapine, dystonia affected 4.3% v. 0% (P = 0.026) and akathisia affected 5.2% v. 0% (P = 0.013) of participants on transition from intramuscular to oral formulations of the respective drugs (Reference Wright, Meehan and BirkettWright 2003). The same study reported that the initial alleviation of agitation was sustained in the transition. The absence of spontaneously reported acute dystonia in the olanzapine-treated patients over several days of continued oral treatment demonstrated its superior extrapyramidal side-effect safety profile compared with haloperidol.

Haloperidol has demonstrated increased rates of events involving extrapyramidal side-effects in transition compared with aripiprazole and ziprasidone and it frequently requires concomitant administration of anticholinergic medications (Reference Daniel, Zimbroff and SwiftDaniel 2004; Reference CitromeCitrome 2007). One of the major benefits of using the more expensive atypical anti-psychotics is the obviation of anticholinergic use both prophylactically and acutely (Reference Raja and AzzoniRaja 2001).

Comparison of atypical antipsychotics

Relative to placebo, the atypical antipsychotics demonstrate notable efficacy in the management of acute agitation in the populations discussed above. Additionally, they significantly reduce the incidence of movement disorders and sedation compared with older treatments. However, there are significant differences between the atypical antipsychotics that should help guide the decision-making process regarding their use. Unfortunately, only a few head-to-head comparisons of the atypicals have been conducted (see below). Most of the comparisons of efficacy have been generated relative to respective comparisons with placebo and older treatments, including haloperidol and lorazepam.

Regarding US Food and Drug Administration (FDA) indications (analogous to ‘licenses’ in the UK), ziprasidone is indicated for agitation in schizophrenia only, while olanzapine and aripiprazole are the only atypical antipsychotics discussed with indications for agitation associated with either schizophrenia or bipolar I mania. Neither risperidone nor quetiapine, despite their established efficacy, currently have specific indications for the treatment of agitation in schizophrenia or bipolar I mania. However, the absence of specific indications for agitation should not necessarily dissuade the provider from choosing a particular agent for the management of agitation, as the process of obtaining additional indications for an already approved medication is both lengthy and costly.

Clinical guidelines

Figure 1 outlines the procedure to follow in managing acute agitation, and medication choices if verbal de-escalation is unsuccessful.

FIG 1 Management of psychotic agitation. Medications are listed in numerical order of preferred use, given demonstrated efficacy while minimising sedation. Medications listed as a, b, c are comparable options with similar efficacy and should be selected on the basis of the patient's medical profile. CNS, central nervous system.

Conclusions

The management of agitation in the context of psychosis presents a challenge that is as multi-faceted as it is prevalent. Over the past decade, there have been significant contributions to the research of agitation which now afford clinicians an extensive assortment of treatment options. However, rather than using the most current, evidence-based practices to tailor customised treatment plans for their agitated patients, clinicians often fall back on ‘what works’ (in their experience). The goal of this article was to provide a thorough and concise review of the literature to enable clinicians to effectively manage agitation with minimal detriment to the diagnostic process, and, most importantly, to the patient.

MCQs

Select the single best option for each question stem

1. 1 The pharmacological agent that has demonstrated particular efficacy in managing hostility/aggression in agitation is:

   1. a risperidone

   2. b midazolam

   3. c lorazepam

   4. d quetiapine.

2. 2 The pharmacological agent with quickest onset of action is:

   1. a olanzapine

   2. b risperidone

   3. c lorazepam

   4. d midazolam.

3. 3 The first step in managing acute agitation should be:

   1. a prepare intramuscular haloperidol and lorazepam

   2. b physically restrain the patient

   3. c offer patient oral risperidone

   4. d isolate patient from other patients.

4. 4 Which of the following has the greatest potential to increase psychosis and/or worsen agitation?

   1. a lorazepam

   2. b midazolam

   3. c diazepam

   4. d clonazepam.

5. 5 Which class of pharmacological agent should be avoided in patients who are being given olanzapine?

   1. a selective serotonin reuptake inhibitors

   2. b typical antipsychotics

   3. c benzodiazepines

   4. d fluoroquinolones.

MCQ answers

1

d

2

d

3

d

4

d

5

c