Absorption of intramuscularly administered [14C]haloperidol decanoate in rats

Matsunaga, Yoshimasa; Nambu, Keiko; Oh-E, Yoshinori; Miyazaki, Hisashi; Hashimoto, Masahisa

doi:10.1007/bf03189894

Cited by 16 publications

(12 citation statements)

References 6 publications

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“…See the reference for detailed experimental conditions. The half-life of the second phase was 2.0 days (8) and that of the first rapidly decreasing phase (the distribution phase) was calculated to be 1.6 h in this study.…”

Section: Discussionmentioning

confidence: 99%

“…Clinically, the depot antipsychotic haloperidol decanoate is administered intramuscularly as a solution in sesame oil (1,2). In rats, the ester administered intramuscularly was shown to be absorbed first by the lymphatic circulation (8), and this process (whose half-life has been estimated to be around 13 days) was the rate-limiting step in disposition ana metabolism of this ester after this administration route. Therefore, after intramuscular administration of haloperidol decanoate, the hydrolysis of the ester is not the rate-limiting step but the absorption is.…”

Section: Discussionmentioning

confidence: 99%

“…Lymphocytes are trapped in lymph nodes. In fact, haloperidol decanoate (but not hydrolysate haloperidol) was highly concentrated in lymph nodes nearest to the administration site (8).…”

Section: Discussionmentioning

confidence: 99%

“…[Carbonyl-P'Cjhaloperidol decanoate with the specific radioactivity of 31.21lCi/mg, [carbonyl-P'C]-haloperidol of 42.7 IlCi/mg and [carboxyl-v'C]-etofenamate (an ester of [carboxyl-v'C] flufenamic acid and diethyleneglycol, used as a reference compound for ester hydrolysis) of 20.4 IlCilmg were prepared as described previously (4,5). Their radiochemical purities were practically 100% as revealed by thin layer chromatography.…”

Section: Chemicalsmentioning

confidence: 99%

“…polystyrene culture flask), rat and human lymphocytes (2.0)( 10 6 cells in a glass tube) and established cells, WI-38 cells, L6 cells and BGM cells (1.0)( 10 6 , 4.9)( 10 6 and 1.9)( 10 6 cells, respectively, in a polystyrene culture dish), were washed twice with PBS( -) and the medium was replaced with 5 ml of MEM containing FBS. (8,9). The solvent used was chloroform/methanol (9/l) or cyclohexane /chloroform/acetic acid (60/75/16).…”

Section: Cells and Mediamentioning

confidence: 99%

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Hydrolysis of haloperidol decanoatein vitro by cultured cells

Oh-E

Miyazaki

Matsunaga

et al. 1987

European Journal of Drug Metabolism and Pharmacokinetics

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[14C]Haloperidol decanoate was hydrolysed by partially purified carboxylesterase but not in plasma, blood, lymph and lymphatic liquid. These fluids inhibited the enzyme-mediated hydrolysis of the ester. Within the same incubation period as above, the ester was found hydrolysed to various extents in cell cultures of isolated rat liver cells, of human and rat lymphocytes and of established cell lines (BGM cells, WI-38 cells and L6 cells). Thus, the hydrolysis of the ester was demonstrated in vitro with use of viable cell cultures instead of enzyme preparation. From the time course study on the metabolism of haloperidol decanoate in cell cultures, it was concluded that haloperidol decanoate was first concentrated in the cells and hydrolysed to haloperidol. Based on these results, the metabolic sequences in vivo leading to the formation of active principle haloperidol after intramuscular administration of its decanoate were discussed.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

“…Lymphocytes are trapped in lymph nodes. In fact, haloperidol decanoate (but not hydrolysate haloperidol) was highly concentrated in lymph nodes nearest to the administration site (8).…”

Section: Discussionmentioning

confidence: 99%

Section: Chemicalsmentioning

confidence: 99%

Section: Cells and Mediamentioning

confidence: 99%

See 3 more Smart Citations

Hydrolysis of haloperidol decanoatein vitro by cultured cells

Oh-E

Miyazaki

Matsunaga

et al. 1987

European Journal of Drug Metabolism and Pharmacokinetics

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Effects of depot drug formulations in procedures used to evaluate antipsychotic activity in rodents

et al. 1999

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The use of long‐acting depot antipsychotics results in an increase in compliance and significantly decreases rates of relapse and rehospitalization of schizophrenic patients. However, the assessment of activity of such drugs in small animals is not as straightforward as the evaluation of acutely active drugs. Previous studies have investigated the effects of depot formulations by assessing their activity in preclinical methods that examine their striatal dopaminergic components alone. These methods are currently used to examine the extrapyramidal side‐effects of antipsychotic agents. In the light of recent drug developments, however, it is possible that such procedures may no longer be appropriate for testing antipsychotics which produce fewer side effects and which have a broader range of action including nondopaminergic components. Accordingly, the present study aimed to further investigate the activities of clinically used depot antipsychotics by using procedures that are considered more predictive of antipsychotic activity rather than extrapyramidal side‐effect liability. Along with acutely active analogs, flupenthixol decanoate, fluphenazine decanoate, and haloperidol decanoate were examined in the following procedures with rats or mice: antagonism of 1[2,5‐dimethoxy‐4‐iodophenyl]‐2‐aminopropane (DOI) ‐induced behaviors and amphetamine‐stimulated locomotion. Effects of the depot formulations in both procedures were determined at time points ranging from 24 h to 14 days after administration. In general, some antipsychotic‐related effects were observed with the drugs particularly at earlier time points; effects at 14 days were minimal. The results from this study demonstrate that depot formulations of antipsychotic drugs have effects in rodents, but factors possibly related to injection volume, test procedure, and species could limit the duration of action in small laboratory animals. Drug Dev. Res. 47:27–36, 1999. © 1999 Wiley‐Liss, Inc.

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