Zuclopenthixol acetate in Viscoleo® ‐ a new drug formulation

Amdisen, A.; Nielsen, M S; Dencker, S. J.; Fensbo, C.; Ahlfors, U. G.; Gravem, A.; Baastrup, P. C.; Bjerkenstedt, Lars; Gunby, B; Wiesel, F.-A.; Lindholm, H.; Rafaelsen, Ole J.; Fredslund-Andersen, K.; Thomsen, Natasha; Rosell, I.; Pakarinen, Päivi; Harma, Pirjo; Amthor, Karl-Friedrich; Kastberg, S.; Abelskov, J.

doi:10.1111/j.1600-0447.1987.tb02759.x

Cited by 37 publications

(6 citation statements)

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“…Several studies show the efficacy of zuclopenthixol for the treatment of acute psychosis or exacerbated chronic psychosis (Gravem and Bugge, 1981;Sechter et al, 1981;Lang and Winteler, 1983;Mann et al, 1985;Bourdouxheet al, 1987), but little information is yet available about zuclopenthixol acetate (Amdisen et al, 1987;Kuefferle et al, 1987). Our results confirm that this prodrug is a useful antipsychotic medication for the treatment of acute psychotic episodes or acute deteriorations of a chronic psychotic state (Amdisen et al, 1986).…”

Section: Discussionmentioning

confidence: 99%

Clinical and Pharmacokinetic Evaluation of Zuclopenthixol Acetate in Viscoleo®

Ae²,

Eiselé³

et al. 1989

Pharmacopsychiatry

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The purpose of the present study was to evaluate zuclopenthixol acetate in Viscoleo, a new preparation to be administered once every 3 days, in the early treatment of acute psychotic episodes and acute deterioration of chronic psychosis. 21 cases were included in the study: patients received 1 to 3 injections. Clinical evaluation was made at 24, 48 and 72 hours after each injection, using the Clinical Global Impressions (CGI) and the Brief Psychiatric Rating Scale (BPRS). Results at end-point indicated a marked or moderate therapeutic effect in the 11 cases of acute psychosis. A statistically significant decrease was observed for the total BPRS score as well as for its subscales. Among 8 cases of exacerbation of chronic psychosis, 4 patients showed a moderate therapeutic effect, and minimal or no effect was found in the other 4 subjects. The total BPRS decreased significantly, but to a lesser extent than for acute psychosis. Two patients suffering from mania showed a moderate therapeutic effect according to CGI. 8 cases of acute psychosis and 5 cases of chronic psychosis did not suffer from any neurological side-effects. Plasma concentration measurements suggest that a dose of 50 mg per 3 days may be sufficient for early treatment of most acutely ill psychotic patients.

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Section: Discussionmentioning

confidence: 99%

Clinical and Pharmacokinetic Evaluation of Zuclopenthixol Acetate in Viscoleo®

Ae²,

Eiselé³

et al. 1989

Pharmacopsychiatry

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“…Injectable neuroleptics were developed for the management of acute psychoses in people who refused to take oral neuroleptics in the initial stages of their treatment (Amdisen et al, 1987). These drugs are used to alleviate anxiety, have various durations of action depending on formulation, and have few side effects when used appropriately.…”

Section: Introductionmentioning

confidence: 99%

Evaluation of Zuclopenthixol Acetate to Decrease Handling Stress in Wapiti

Read¹,

Caulkett²,

McCallister

2000

Journal of Wildlife Diseases

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Handling stress and capture myopathy are important consequences of intensively managing wildlife species. Over the last 15 yr, the use of long-acting neuroleptic (LAN) drugs in wildlife has increased, and these drugs have become a valuable tool for decreasing capture and handling stress in many species. At this time, reports on the use of these drugs in North American species are limited. The major objective of this study was to evaluate the use of the LAN, zuclopenthixol acetate (Clopixol-Acuphase), to decrease both quantifiable and subjective measurements of stress and activity in wild wapiti (Cervus elaphus, North American elk). This blinded, randomized study took place in February 1999 in Manitoba (Canada) and involved 11 animals receiving the drug and 12 animals acting as controls. At 24 hr after drug administration, there were measurable and significant decreases in the stress and activity of treated animals versus controls during handling.

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“…This is contrary to the recommendations from the manufacturer, and to the guidelines given in prescribing manuals, which suggest a course of injections is usually optimal. [8], [9], [10] Just under half ( n = 40) of the respondents routinely gave ZA with another psychoactive medication, most frequently a benzodiazepine (clonazepam being most frequently used). Sedation was cited as being the most frequent side effect of ZA, and although EPSE were recognised as a complication of treatment, respondents rated this as relatively uncommon (on a linear scale of 1-5, mean score was <3).…”

Section: Establishing a Need For Specific Guidelines For Use Of Zamentioning

confidence: 99%

“…In sum, there was a reasonable consistency between trials on the following: Several studies suggested that, depending on the individual's diagnosis, a differential response to ZA can be expected. That is, those with an exacerbation of chronic psychotic illness or acute mania tended to show a more rapid response, evidenced by decline in clinical global impression (CGI) score ( P < 0.0001) 8 and Bech Rafaelsen Mania scale (BRMAS) scores ( P < 0.001). [8], [14] There was reasonable agreement that the time of onset of sedation was between 15-90 minutes and that this level of sedation increases to reach a maximum after 8 hours.…”

Section: What Does the Literature Say?mentioning

confidence: 99%

“…That is, those with an exacerbation of chronic psychotic illness or acute mania tended to show a more rapid response, evidenced by decline in clinical global impression (CGI) score ( P < 0.0001) 8 and Bech Rafaelsen Mania scale (BRMAS) scores ( P < 0.001). [8], [14] There was reasonable agreement that the time of onset of sedation was between 15-90 minutes and that this level of sedation increases to reach a maximum after 8 hours. The sedative effect decreases with subsequent injections of ZA unless the dose is increased. Those individuals with mania and first episode psychosis were found to have less of a sedative response and took longer to show a sedative response as compared to those with a relapse of chronic psychosis. …”

Section: What Does the Literature Say?mentioning

confidence: 99%

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