Haloperidol blood levels and clinical effects

dc.contributor.author	Volavka J
dc.contributor.author	Cooper T
dc.contributor.author	Czobor, Pál
dc.contributor.author	Bitter, István
dc.contributor.author	Meisner M
dc.contributor.author	Laska E
dc.contributor.author	Gastanaga P
dc.contributor.author	Krakowski M
dc.contributor.author	Chou JCY
dc.contributor.author	Crowner M
dc.contributor.author	Douyon R
dc.date.accessioned	2018-01-03T09:03:30Z
dc.date.available	2018-01-03T09:03:30Z
dc.date.issued	1992
dc.identifier	0026643073
dc.identifier.citation	pagination=354-361; journalVolume=49; journalIssueNumber=5; journalTitle=ARCHIVES OF GENERAL PSYCHIATRY;
dc.identifier.uri	http://repo.lib.semmelweis.hu//handle/123456789/4522
dc.description.abstract	This study explored the relationships between plasma levels and the clinical effects of haloperidol in 176 acutely exacerbated schizophrenic or schizoaffective patients. After a single-blind placebo period of 1 week (period 1), they entered the double-blind period 2 randomly assigned to one of three plasma levels of haloperidol: low (2 to 13 ng/mL), medium (13.1 to 24 ng/mL), or high (24.1 to 35 ng/mL). Patients whose conditions did not improve in period 2 continued on one of the three haloperidol levels (period 3). Periods 2 and 3 lasted 6 weeks each. Only minor differences in clinical responses were noted among the three levels of haloperidol. These results imply that low or moderate doses of neuroleptics are appropriate for many acutely psychotic patients.
dc.relation.ispartof	urn:issn:0003-990X
dc.title	Haloperidol blood levels and clinical effects
dc.type	Journal Article
dc.date.updated	2017-10-10T08:02:20Z
dc.language.rfc3066	en
dc.identifier.mtmt	1494557
dc.identifier.wos	A1992HV12200002
dc.identifier.pubmed	1586270
dc.contributor.department	SE/AOK/K/Pszichiátriai és Pszichoterápiás Klinika [2015.12.31]
dc.contributor.institution	Semmelweis Egyetem