Benzodiazepina untuk keagresifan atau agitasi akibat psikosis
Abstract
Background
Acute psychotic illness, especially when associated with agitated or violent behaviour, can require urgent pharmacological tranquillisation or sedation. In several countries, clinicians often use benzodiazepines (either alone or in combination with antipsychotics) for this outcome.
Objectives
To examine whether benzodiazepines, alone or in combination with other pharmacological agents, is an effective treatment for psychosis‐induced aggression or agitation when compared with placebo, other pharmacological agents (alone or in combination) or non‐pharmacological approaches.
Search methods
We searched the Cochrane Schizophrenia Group's register (January 2012, 20 August 2015 and 3 August 2016), inspected reference lists of included and excluded studies, and contacted authors of relevant studies.
Selection criteria
We included all randomised controlled trials (RCTs) comparing benzodiazepines alone or in combination with any antipsychotics, versus antipsychotics alone or in combination with any other antipsychotics, benzodiazepines or antihistamines, for people who were aggressive or agitated due to psychosis.
Data collection and analysis
We reliably selected studies, quality assessed them and extracted data. For binary outcomes, we calculated standard estimates of risk ratio (RR) and their 95% confidence intervals (CI) using a fixed‐effect model. For continuous outcomes, we calculated the mean difference (MD) between groups. If there was heterogeneity, this was explored using a random‐effects model. We assessed risk of bias and created a 'Summary of findings' table using GRADE.
Main results
Twenty trials including 695 participants are now included in the review. The trials compared benzodiazepines or benzodiazepines plus an antipsychotic with placebo, antipsychotics, antihistamines, or a combination of these. The quality of evidence for the main outcomes was low or very low due to very small sample size of included studies and serious risk of bias (randomisation, allocation concealment and blinding were not well conducted in the included trials, 30% of trials (six out of 20) were supported by pharmaceutical institutes). There was no clear effect for most outcomes.
Benzodiazepines versus placebo
One trial compared benzodiazepines with placebo. There was no difference in the number of participants sedated at 24 hours (very low quality evidence). However, for the outcome of global state, clearly more people receiving placebo showed no improvement in the medium term (one to 48 hours) (n = 102, 1 RCT, RR 0.62, 95% CI 0.40 to 0.97, very low quality evidence).
Benzodiazepines versus antipsychotics
For the outcome of sedation by 16 hours, there was no difference between haloperidol and benzodiazepine (n = 434, 8 RCTs, RR 1.13, 95% CI 0.83 to 1.54, low quality evidence). There was no difference in the number of participants who had not improved in the medium term (n = 188, 5 RCTs, RR 0.89, 95% CI 0.71 to 1.11, low quality evidence). However, one small study found fewer participants improved when receiving benzodiazepines compared with olanzapine (n = 150, 1 RCT, RR 1.84, 95% CI 1.06 to 3.18, very low quality evidence). People receiving benzodiazepines were less likely to experience extrapyramidal effects in the medium term compared to people receiving haloperidol (n = 233, 6 RCTs, RR 0.13, 95% CI 0.04 to 0.41, low quality evidence).
Benzodiazepines versus combined antipsychotics/antihistamines
When benzodiazepine was compared with combined antipsychotics/antihistamines (haloperidol plus promethazine), there was a higher risk of no improvement in people receiving benzodiazepines in the medium term (n = 200, 1 RCT, RR 2.17, 95% CI 1.16 to 4.05, low quality evidence). However, for sedation, the results were controversial between two groups: lorazepam may lead to lower risk of sedation than combined antipsychotics/antihistamines (n = 200, 1 RCT, RR 0.91, 95% CI 0.84 to 0.98, low quality evidence); while, midazolam may lead to higher risk of sedation than combined antipsychotics/antihistamines (n = 200, 1 RCT, RR 1.13, 95% CI 1.04 to 1.23, low quality evidence).
Other combinations
Data comparing benzodiazepines plus antipsychotics versus benzodiazepines alone did not yield any results with clear differences; all were very low quality evidence. When comparing combined benzodiazepines/antipsychotics (all studies compared haloperidol) with the same antipsychotics alone (haloperidol), there was no difference between groups in improvement in the medium term (n = 185, 4 RCTs, RR 1.17, 95% CI 0.93 to 1.46, low quality evidence), but sedation was more likely in people who received the combination therapy (n = 172, 3 RCTs, RR 1.75, 95% CI 1.14 to 2.67, very low quality evidence). Only one study compared combined benzodiazepine/antipsychotics with antipsychotics; however, this study did not report our primary outcomes. One small study compared combined benzodiazepines/antipsychotics with combined antihistamines/antipsychotics. Results showed a higher risk of no clinical improvement (n = 60, 1 RCT, RR 25.00, 95% CI 1.55 to 403.99, very low quality evidence) and sedation status (n = 60, 1 RCT, RR 12.00, 95% CI 1.66 to 86.59, very low quality evidence) in the combined benzodiazepines/antipsychotics group.
Authors' conclusions
The evidence from RCTs for the use of benzodiazepines alone is not good. There were relatively few good data. Most trials were too small to highlight differences in either positive or negative effects. Adding a benzodiazepine to other drugs does not seem to confer clear advantage and has potential for adding unnecessary adverse effects. Sole use of older antipsychotics unaccompanied by anticholinergic drugs seems difficult to justify. Much more high‐quality research is still needed in this area.
PICO
Plain language summary
Benzodiazepina sahaja atau kombinasi dengan ubat antipsikotik untuk psikosis akut
Soalan ulasan
Tujuan ulasan ini adalah untuk membandingkan kesan penenang (menenangkan) atau sedatif (mengantuk) benzodiazepina, yang diberi bersendirian atau digabung dengan ubat lain berbanding kesan plasebo (rawatan palsu), ubat lain atau rawatan bukan ubatan untuk pesakit yang agresif atau gelisah kerana sedang mengalami psikosis.
Latar belakang
Psikosis akut adalah keadaan mental seseorang yang cepat bertambah teruk di mana sentuhan realiti lazim hilang. Pesakit boleh mengalami khayalan atau halusinasi menakutkan yang meresahkan dan boleh menyebabkan tingkah laku gelisah atau agresif. Dalam kes mendesak, agitasi atau keagresifan boleh mengakibatkan kecederaan kepada orang yang mengalami psikosis atau orang lain di sekitar mereka. Untuk mengelakkan kecederaan sedemikian, penenangan segera atau dengan ubat‐ubatan sedatif mungkin perlu. Ubat yang paling lazim diguna untuk mencapai keadaan tenang atau sedatsi adalah benzodiazepina dan ia boleh diberi sama ada bersendirian atau gabungan dengan antipsikotik.
Carian
Carian asal untuk ulasan ini dijalankan pada Januari 2012 dan kemudiannya dua carian kemaskini seterusnya dijalankan pada Ogos 2015 dan Ogos 2016. Carian tersebut menemui sejumlah 2497 rekod, di mana pengarang ulasan memeriksa untuk inklusi atau eksklusi daripada ulasan. Pengarang hanya memasukkan rekod jika ia adalah kajian rawak (kajian klinikal di mana pesakit dibahagikan secara rambang kepada satu daripada dua atau lebih kumpulan rawatan) yang memperuntukkan orang dengan psikosis akut yang menunjukkan agitasi, tingkah laku agresif ganas (atau gabungan) untuk menerima benzodiazepina yang diberi berasingan atau digabung dengan sebarang antipsikotik, berbanding plasebo, antipsikotik sahaja atau gabungan dengan antipsikotik lain/benzodiazepina/antihistamin atau rawatan bukan ubatan.
Bukti yang ditemui
Sejumlah, 20 kajian telah disertakan. Keseluruhannya, kualiti bukti adalah rendah atau sangat rendah akibat risiko bias yang serius dan saiz kecil kajian yang dimasukkan. Tiada perbezaan ketara dalam pembaikan antara benzodiazepina dan plasebo, benzodiazepina dan antipsikotik atau benzodiazepina ditambah antipsikotik dan benzodiazepina sahaja atau antipsikotik sahaja. Apabila benzodiazepina dibanding dengan gabungan antipsikotik/antihistamin, terdapat risiko bias yang lebih tinggi untuk tiada pembaikan dalam kalangan orang yang menerima benzodiazepina sahaja tetapi bukti adalah berkualiti rendah. Hanya satu kajian menunjukkan kesan gabungan benzodiazepina/antipsikotik yang rendah berbanding gabungan antihistamin/antipsikotik. Walau bagaimanapun, bukti tersebut adalah berkualiti sangat rendah. Dari segi kesan sampingan, orang yang menerima benzodiazepina berbanding antipsikotik berisiko lebih rendah untuk menunjukkan simptom seperti menggeletar, tremor dan percakapan tidak jelas manakala keputusan sedasi adalah tidak jelas.
Kesimpulan
Kajian sedia ada tidak memberi cukup maklumat untuk menyokong atau menyangkal penggunaan benzodiazepina sahaja atau dengan tambahan kepada ubat lain apabila penenangan segera atau sedasi dengan ubat diperlukan. Walaupun benzodiazepina sahaja mungkin menyebabkan kurang kesan sampingan berbanding antipsikotik terdahulu, apabila ia ditambah kepada ubat lain ini mungkin membawa kepada kesan sampingan yang tidak perlu. Kajian lanjutan diperlukan untuk memberi bukti berkualiti bagus dengan kesimpulan kukuh untuk makluman praktis dan polisi tentang penenangan segera untuk orang dengan psikosis yang agresif atau gelisah.
